Court Opinion

ID: 4675408
Source: CourtListenerOpinion
Date Created: 2021-04-07 20:01:50.402484+00
Date Added: 2024-06-11T08:03:25.926337
License: Public Domain

In the United States Court of Federal Claims
                                       OFFICE OF SPECIAL MASTERS
                                                No. 17-480V
                                              (to be published)

    *************************
    E.S,                    *
                                *                                            Filed: November 13, 2020
                    Petitioner, *
                                *                                            Chief Special Master Corcoran
              v.                *
                                *
    SECRETARY OF HEALTH AND     *                                            Human Papillomavirus Vaccine; Type
    HUMAN SERVICES,             *                                            I Diabetes; Influenza Vaccine;
                                *                                            Narcolepsy; Postural Orthostatic
                                *                                            Tachycardia Syndrome;
                  Respondent.   *                                            Chronic Fatigue; Reliable Theory;
                                *                                            Aggravation of Diabetes; Onset
                                *
    *************************

    Robert J. Krakow, Law Office of Robert J. Krakow, New York, NY, for Petitioner.

    Sarah Duncan, U.S. Department of Justice, Washington, D.C., for Respondent.

                                                       DECISION 1

           On April 4, 2017, E.S             filed this action seeking compensation under the National
    Vaccine Injury Compensation Program (the “Program”). 2 ECF No. 1; see also Amended Petition,
    filed Apr. 4, 2017 (ECF No. 64-1). Petitioner alleges that she suffered autonomic dysfunction,
    manifesting in a wide variety of conditions and symptoms (including headaches, chronic fatigue
    syndrome (“CFS”), postural orthostatic tachycardia syndrome (“POTS”) and small fiber neuropathy
    (“SFN”), after receipt of the human papillomavirus (“HPV”) and hepatitis A vaccines in July 2014,
    with the same symptoms plus a cardiac condition and aggravation of preexisting diabetes mellitus
    after receiving another HPV vaccine dose along with the influenza (“flu”) vaccine in August 2015.

1
  This Decision will be posted on the United States Court of Federal Claims’ website in accordance with the E-
Government Act of 2002, 44 U.S.C. § 3501 (2012). This means the Decision will be available to anyone with access
to the internet. As provided by 42 U.S.C. § 300aa-12(d)(4)(B), however, the parties may object to the published
Decision’s inclusion of certain kinds of confidential information. Specifically, under Vaccine Rule 18(b), each party has
fourteen (14) days within which to request redaction “of any information furnished by that party: (1) that is a trade secret
or commercial or financial in substance and is privileged or confidential; or (2) that includes medical files or similar files,
the disclosure of which would constitute a clearly unwarranted invasion of privacy.” Vaccine Rule 18(b). Otherwise, the
entire Decision will be available to the public in its current form. Id.
2
 The Vaccine Program comprises Part 2 of the National Childhood Vaccine Injury Act of 1986, Pub. L. No. 99-660, 100
Stat. 3758, codified as amended, 42 U.S.C. §§ 300aa-10 through 34 (2012) [hereinafter “The Program” or “Program”].
Individual section references hereafter will be to Section 300aa of the Act.
    Id. at 1. After the filing of multiple expert reports, I invited Respondent to request the claim’s
    dismissal, and the matter is now fully briefed. Resp.’s Brief in Support of Dismissal, filed
    Sept. 13, 2019 (ECF No. 103-1) (“Mot.”); Pet.’s Brief in Opposition of Dismissal, filed Dec.
    2, 2019 (ECF No. 112) (“Opp.”); Resp.’s Reply Brief in Support of Dismissal, filed Feb. 4,
    2020 (ECF No. 114-1)(“Reply”); Pet.’s Sur-Reply Brief in Opposition of Dismissal, filed Apr.
    2, 2020 (ECF No. 118) (“Sur-Reply”).

          Petitioner’s medical history establishes that she has experienced a variety of conditions and
    symptoms, but many of her alleged injuries (in particular POTS and myocardial ischemia) are not
    preponderantly established, nor are all related, as she seems to assume. In addition, those symptoms
    she can establish having experienced appear attributable to her preexisting diabetes, or occurred too
    long after vaccination to be deemed causal. And overall, Petitioner’s theories—that the HPV
    vaccine or flu vaccine can either cause or aggravate (a) dysautonomia and/or POTS, (b) small fiber
    neuropathies, (c) chronic fatigue syndrome, (d) narcolepsy, or (e) diabetes—reiterate contentions
    that have rarely been successful in the Program, and are medically and scientifically unreliable
    based upon the evidence offered in this case. I therefore find that Petitioner’s claim merits no further
    consideration, and dismiss it on the basis of the existing filings.

    I.    Factual Background

          A. Pre-Vaccination Health History

            Ms. E.S.     was born on January 2, 1996 (and was thus eighteen years old when she received
    the first vaccines at issue in this case). Ex. 1 at 1. She was a strong student by her accounts, and an
    accomplished athlete as well, who swam competitively and won top positions at regional swim
    competitions during high school. Ex. 103; Ex. 43; Ex. 44. Ms. E.S.           held summer employment
    as a lifeguard and was reportedly considered for membership on college swim teams, although it is
    unclear from the filed documentary evidence if she did in fact swim for the university she ultimately
    attended (Villanova University). Ex. 103; Ex. 104 at 2.

           The record, however, also reveals that Petitioner had her share of medical problems before
    the relevant vaccinations, and some of these bear on her claim. In particular, Ms. E.S.            was
    diagnosed with type I diabetes mellitus (“DM-1”) when she was five years old (although she had
    good control of it in the time before receiving the first vaccines alleged to have injured her). 3 Her
    medical records also reflect problems with persistent lower back pain, intermittent hematuria,4 flank
    pain, kidney stones, surgery for hemorrhagic right ovarian cyst, irregular menses, selective

3
 See Mot. at 3 n.7 (“Petitioner’s DM-1 was under fair control prior to receiving the first HPV vaccine with a hemoglobin
A1c (“HbA1c”) typically in the range of 7-8% (ideal for a child being <7%) since 2008”) (citing Ex. 19 at 81–110).
4
 Hematuria (or erythrocyturia) is blood (erythrocytes) in the urine. Dorland’s Illustrated Medical Dictionary 824 (33rd
ed. 2020) (hereinafter, “Dorland’s”).

                                                           2
    immunoglobulin A deficiency, and rheumatoid arthritis. Ex. 19 at 50, 54, 66, 69; Ex. 4 at 152; Ex.
    3 at 5, 8; Ex. 23 at 5.

           Additionally, there are several documented instances from the record in which Ms. E.S.
    sought emergency treatment for ambiguous complaints that did not result in any significant findings
    or explanations. Thus, in July 2011, Petitioner visited the emergency room complaining of two days
    of mid-sternal chest pain, weakness, and shortness of breath. Ex. 17 at 198–204. However, her vital
    signs, chest x-ray, and EKG 5 were normal, her chest pain resolved, and she was discharged. Id. at
    198–204, 207, 210. Later on, in the fall of 2012 (now about two years before her relevant
    vaccinations), Ms. E.S.      went two more times to the ER complaining of flank pain. Ex. 4 at 152–
    196. At these visits she recounted similar episodes in the past and a prior history of kidney stones.
    Id. at 152, 159. She also reported that blood in her urine was (at least at that time) a “chronic
    problem.” Id.

           Petitioner reported several health problems to her pediatrician in the months before her July
    2014 receipt of the HPV and hepatitis A vaccines. She complained of recurring headaches and sore
    throat in the fall of 2013. Ex. 3 at 16. A strep test came back negative and her treater diagnosed her
    with adenopathy and acute pharyngitis. Id. She was directed to return if symptoms worsened. Id. In
    March 2014, she visited her pediatrician, Dr. Rebekah Lipstein, for nausea and sore throat, and was
    diagnosed with a viral infection. Ex. 3 at 13–15. She weighed 159 pounds at this visit. Id. Then, in
    April 2014 she went to the ER again, this time complaining of blood in her urine, back and flank
    pain, and hyperglycemia. Ex. 4 at 117–31. Her blood glucose was 349 (an extremely high level for
    a diabetic6), she had glucose and ketones in her urine, and she now weighed 150 pounds. Id. at 118–
    20.

          B. July 15, 2014: Petitioner Receives HPV and Hepatitis A Vaccines

          At a well visit with Dr. Lipstein on July 15, 2014, Ms. E.S.    received the first vaccines at
    issue—the HPV and hepatitis A vaccines. Ex. 3 at 8–12. She weighed 164 pounds at this visit, and
    a urine dipstick test showed trace glucose (an indication of elevated serum glucose levels). Id. at
    11. The record reveals no immediate vaccine reaction. In fact, as indicated below, there was a
    subsequent, several-month gap before Petitioner again sought medical treatment. Thus, there is no
    evidence from this period that she was experiencing symptoms of any kind.

          Ms. E.S.      began college in the fall of 2014. On September 2, 2014, she visited the student
    health center for treatment of increased blood sugars that she had observed from her own self-

5
 Electrocardiogram (“EKG” or ECG) is a graphic tracing of the variations in electrical potential caused by the excitation
of the heart muscle and detected at the body surface. Dorland’s at 593.

6
 In children two years to adult, normal “casual” (meaning any time of day) blood glucose levels are ≤ 200 mg/dL or 11.1
mmol/L. Mosby’s Manual of Diagnostic and Laboratory Tests 253 (6th ed. 2018) (hereinafter, “Mosby’s”).

                                                           3
    monitoring, and a sore throat. Ex. 14 at 88–90. Petitioner tested positive for group A streptococcus
    and was prescribed antibiotics. Id. However, there is no evidence from this particular record that
    any treater associated her strep infection or diabetes resurgence with her July vaccinations (which
    had been administered nearly seven weeks before). Later that same month, from September 22–24,
    2014, Ms. E.S.      visited the health center multiple times for high glucose levels and a cough (later
    diagnosed as bronchitis). Id. at 84–87. About ten days later, on October 2, 2014, she visited the
    emergency room (“ER”) at Bryn Mawr Hospital for an abnormal glucose level of 338. Ex. 9 at 3–
    12. She denied having previous similar symptoms (despite her history in the immediate weeks
    prior), and although she complained of headache and sinus pressure, she did not identify the onset
    of these symptoms occurring much before the ER visit. Id. Four days later, on October 6, 2014,
    Petitioner visited her university health center for nausea and elevated blood sugars. Ex. 14 at 70.
    Meanwhile, more than ten weeks had passed from the time in July when Petitioner received the
    relevant vaccines.

           No records have been filed establishing any additional visits by Ms. E.S.          to medical
    treaters in November 2014. Then, on December 5, 2014, Petitioner made a second visit to the Bryn
    Mawr ER, now complaining of constant vomiting and diarrhea that she reported began about one
    and a half weeks before her visit (late-November). Ex. 9 at 27–35. This was the first time in the
    medical record Petitioner reported this combination of symptoms and based on her presentation she
    was diagnosed with gastroenteritis. Id. Throughout December, Petitioner visited the Villanova
    student health center multiple times for increased glucose levels, diarrhea, vomiting, and abdominal
    pain. See, e.g., Ex. 14 at 68–69; Ex. 17 at 12–21, 102–05.

           On December 11, 2014, Petitioner saw Dr. Keith Benkov, a gastroenterologist. Ex. 11 at 1–
    2. She reported that in late September 2014 she had experienced several viral infections, high blood
    sugars, and back pain. Id. She also told Dr. Benkov that in November 2014 she began vomiting
    daily and having loose stools. Id. Dr. Benkov ordered labs, doubled Petitioner’s Protonix 7 dose,
    considered performing an endoscopy, and took Petitioner’s weight (now 172 pounds). Id.
    Petitioner’s celiac and thyroid profiles were negative, and she was also negative for thyroid
    antibodies, FSH, testosterone, estradiol, and DHEAS. 8 Id. at 6. The records from this time reflect
    some treater concerns that Petitioner may have suffered from a pancreatic condition, although this
    was not confirmed. Id. at 10. Later that same December, Ms. E.S.       was again hospitalized after
    complaining of persistent headaches, and testing performed on her revealed elevated liver enzymes
    plus some evidence of a possibly enlarged liver. Ex. 17 at 97, 99, 113. Dr. Benkov concluded that

7
 Protonix is the trademark for preparations of pantoprazole sodium. Dorland’s at 1513. Pantoprazole sodium is a proton
pump inhibitor used in the treatment of erosive esophagitis associated with gastroesophageal reflux disease. Pantoprazole
Sodium,                     Dorland’s                    Online                    Medical                    Dictionary,
https://www.dorlandsonline.com/dorland/definition?id=36645&searchterm=pantoprazole+sodium (last visited Oct. 9,
2020).
8
  Dehydroepiandrosterone sulfate (“DHEAS”) is a steroid secreted by the adrenal cortex, the major androgen precursor
in females; it is often present in excessive amounts in body fluids of patients with adrenal virilism. Dorland’s at 476.
                                                           4
    Petitioner had poor diabetic control as well as poor gastric emptying, and a fatty liver. Id. at 105.

          On January 6, 2015, Petitioner’s glycated hemoglobin (HbA1c) 9 level was 9.8% and 10.2%
    on different readings taken that day—both highly elevated and evidence of ongoing diabetes. Ex.
    19 at 114, 119. Later that month, on January 27, 2015, she visited Dr. Elizabeth Wallach, an
    endocrinologist. Id. at 28–31. Petitioner’s mother was concerned about Ms. E.S.            ’s increasing
    HbA1c levels (9.8% that day) and increasing weight (12 pounds since she began college). She
    privately discussed with Dr. Wallach that Petitioner was eating a lot and not always testing her
    blood sugar. Id. at 29. Dr. Wallach felt Petitioner was doing well on her insulin pump, but discussed
    the possibility of taking her off it (something Petitioner expressed a desire to do). Id. at 28.

          C. Additional Vaccines Deemed Causal and Onset of Novel Symptoms

           More than three months passed before Ms. E.S.           again required medical treatment. On
    May 1, 2015, Petitioner sought emergency room treatment at Bryn Mawr Hospital for the fourth
    time, complaining of abrupt onset of right flank pain, nausea, and vomiting. Ex. 9 at 54. Petitioner’s
    blood glucose at the point of care was 129 mg/dL, and urine glucose was 500 mg/dL. Id. at 70.
    Three months passed before Petitioner’s next doctor visit which was for her annual pediatric exam
    on August 19, 2015. Ex. 3 at 5–7. She now weighed 168 pounds, and a urine dipstick showed 3+
    blood and no glucose.10 Id. During this exam, she received her second HPV vaccine dose, and a flu
    vaccine. Id. Petitioner’s filed medical history reveals she had in the past repeatedly received the flu
    vaccine with no complications. Ex 2; Ex. 17 at 185. There is no evidence of any immediate/close-
    in-time reaction to these vaccinations.

           Over the fall of 2015 and into early 2016, Ms. E.S.      continued to seek emergency care on
    a regular basis, with most treater visits seemingly oriented toward addressing diabetes-related issues
    or complications. Approximately two months passed since the second set of vaccinations before
    Petitioner had two ER visits. At the first visit (October 10, 2015), she complained of nausea,
    vomiting, loose stools, and high blood sugar. Ex. 9 at 79, 81–82. However, she had a normal EKG,
    and the discharge assessment was nausea and vomiting. Id. at 83. She was instructed to drink plenty
    of fluids, avoid alcohol and certain over-the-counter pain relievers, and to adjust her insulin pump

9
 In adults, about 98 percent of the hemoglobin in the red blood cell is hemoglobin A. About seven percent of hemoglobin
A consists of a type of hemoglobin (HbA1) that can combine strongly with glucose in a process called glycosylation. As
the red blood cell circulates, it combines its HbA1 with some of the glucose in the bloodstream to form glycohemoglobin
(GHb). The amount of GHb depends on the amount of glucose available in the bloodstream over the RBC’s 120-day life
span. Therefore, determination of the GHb value reflects the average blood sugar level for the 100- to 120-day period
before the test. The more glucose to which the RBC is exposed, the greater the percentage. Mosby’s at 266.
10
  Urine reagent strips or dipsticks are used for the estimation of glucose, albumin, hemoglobin, and bile concentrations,
as well as urinary pH, specific gravity, protein, ketone bodies, nitrates, and leukocyte esterase. Mosby’s at 909. Dipstick
testing is considered preliminary or for screening. Id. Often more definitive and quantitative studies are necessary to
confirm the results. Id.

                                                            5
 as directed by her diabetes physician. Id. Similarly, on her second ER visit (October 21, 2015) she
 presented with high blood sugar and abdominal pain occurring since the prior visit. Ex. 12 at 1, 10,
 75. A CT scan of the abdomen and pelvis was performed with no significant findings. Id.
 Petitioner’s treater noted that her symptoms sounded like acid reflux and that she had a positive
 response to such treatment. Id. at 36.

        Vomiting and diarrhea prompted a third ER visit in early December 2015, and although
 Petitioner’s blood sugar was now a bit lower, she was diagnosed with hypokalemia, 11 and instructed
 to follow-up with her GI doctor about her visit and her potassium levels. Ex. 9 at 106, 108, 109.
 Petitioner reported a similar constellation of symptoms at a January 10, 2016 visit. Ex. 7 at 5, 8–9.
 None of the relevant treaters proposed that Petitioner’s receipt of the second HPV dose or flu
 vaccine in August 2015 might have played a role in Petitioner’s illness, however, treaters did
 consider her high blood sugar as causal. Ex. 12 at 39.

       Petitioner again sought specialized treatment in early 2016. On February 16, 2016, she saw
 Dr. David Lefkowitz, a cardiologist, for evaluation of chest pain. Ex. 5 at 1–4. She reported the pain
 she was experiencing was “generally exertional” in nature, and that she also suffered from
 occasional night sweats, decreased exercise tolerance, new onset migraines, and episodes of
 tachycardia not experienced in the past. 12 Id. She also claimed that she had felt poorly since
 receiving the HPV vaccine, two other vaccines, and a tuberculosis skin test. Id. at 1.

        A physical exam performed by Dr. Lefkowitz showed regular heart rhythm, a mid-systolic
 click, absent jugular venous pressure, normal carotid upstrokes and no lower extremity edema.13
 Ex. 5 at 2. Pericardial 14 thickening was noted on Petitioner’s echocardiogram, and an EKG showed
 “sinus rhythm, inferior and lateral repolarization abnormality compatible with pericarditis 15 versus
 early repolarization.” Id. at 3–4, 13. A stress EKG revealed distal inferoseptal hypokinesis 16 at peak
 stress, which (as Dr. Lefkowitz noted) might suggest a possible jeopardized myocardium,17

11
  Hypokalemia is abnormally low potassium concentration in the blood resulting from excessive potassium loss by the
renal or the gastrointestinal route, from decreased intake, or from transcellular shifts. Dorland’s at 891.

 Tachycardia is excessive rapidity in the action of the heart and is usually applied to a heart rate above 100 beats per
12

minute in an adult. Dorland’s at 1838.
13
   Edema is the presence of abnormally large amounts of fluid in the intercellular tissue spaces of the body, usually
referring to subcutaneous tissues, which may be localized. Dorland’s at 587.
14
  The pericardium is the fibroserous sac that surrounds the heart and the roots of the great vessels, comprising an external
layer of fibrous tissue and an inner serous layer. Dorland’s at 1391.
15
     Pericarditis is inflammation of the pericardium. Dorland’s at 1391.

16
     Hypokinesis or hypokinesia is abnormally decreased mobility/motor function or activity. Dorland’s at 891.

17
     The myocardium is the middle and thickest layer of the heart wall, composed of cardiac muscle. Dorland’s at 1204.

                                                              6
 although the stress test was cut short when Petitioner complained of chest pain. Id. at 2, 4, 15. The
 positive stress test prompted the doctor to order cardiac CT angiography, 18 but that test produced
 normal results. Id. at 16–18 (performed on March 3, 2016). There was no immediate follow-up with
 Dr. Lefkowitz (moreover, Petitioner did not return to him for an entire year).

        On February 17, 2016, Petitioner visited Dr. Benkov again (whom it does not appear from
 the records she had seen for more than a year). Ex. 11 at 3. Although she reported experiencing less
 severe gastrointestinal issues overall, she still had occasional episodes of nausea, diarrhea, and
 vomiting. Id. Records from this visit establish that Petitioner’s mother now expressed the view that
 Ms. E.S.     ’s symptoms were associated with the second HPV dose she had received in August
 2015. Id. The medical record, as discussed above, does not support this conclusion. However, it
 does reveal that throughout this time period Ms. E.S. ’s diabetes was not under good control. Id.
 Additionally, Petitioner reported that she continued to gain weight despite monitoring of her diet.
 Id. Moreover, Petitioner’s mother informed Dr. Benkov that Petitioner’s sister seemed to have
 gotten sick after receiving the HPV vaccine, 19 and that both sisters had developed pericarditis as a
 result. Id.

        In contrast to the mother’s statements, Dr. Benkov noted on exam that Petitioner “actually
 looked pretty well off.” Ex. 11 at 3. However, she now weighed 177 pounds and her hemoglobulin
 A1C was elevated (9.8%), and remained so even when tested again in early March. 20 Id. at 3, 7; Ex.
 19 at 145. An abdominal ultrasound revealed two non-obstructing stones in Petitioner’s right renal
 collecting system. Ex. 11 at 10. Dr. Benkov noted that Petitioner’s condition “could be some form
 of pancreatitis” and suggested doubling her current dose of Protonix. Id. at 1, 2.

        On May 12, 2016, Ms. E.S.        visited Dr. Edith Schussler, a Clinical Fellow in the Division
 of Allergy and Immunology at Icahn School of Medicine at Mount Sinai, for an immune
 dysfunction consultation. Ex. 23 at 5–8. The records from this visit include a condensed medical
 history, addressing her long-standing struggle with diabetes among other things. Id. at 5. The history
 also stated that beginning in the summer of 2014, Petitioner had started to experience repeated throat
 infections, cyclic vomiting (four times a day), diarrhea, racing heart, and fatigue. Id. During this
 period, her athletic pursuits were curtailed, she experienced extreme weight gain and poor glucose
 control, and she now claimed she had been diagnosed with a non-alcoholic fatty liver. Id.

           Petitioner asserts she had improved the following summer, but then worsened after receiving

18
  Angiography is the radiographic visualization of blood vessels following introduction of contrast material; used as a
diagnostic aid in such conditions as stroke syndrome and myocardial infarction. Dorland’s at 83.
19
     See Opp. at 15.
20
  Petitioner visited the ER on March 2, 2016 for non-radiating, waxing and waning abdominal pain that was aggravated
by menstruation diagnosed as a ruptured ovarian cyst. Ex. 14 at 13–14.

                                                          7
 her second HPV vaccine in August 2015. She also reported “running in the 300-400 glucose range,”
 but had better control after recently seeing her endocrinologist. Ex. 23 at 5. A physical examination
 was mostly normal, although Dr. Schussler recommended that Petitioner not get the Rubella or
 hepatitis B vaccines—the only two she needed at the time—while she was not feeling well. Id. at
 7–8. 21 Dr. Schussler, based on HLA testing, 22 concluded that Petitioner did not appear to be a
 vaccine “non-responder,” and that she should continue to be vaccinated in the future. Id. at 13.

        At the end of May 2016, Petitioner visited Dr. John Wells for a neurologic evaluation. Ex. 24
 at 6–7. She reported a number of medical problems within the last year. Id. at 6. Her primary
 neurological complaint was a headache sensation, which had been persistent since starting college
 and was characterized by constant pressure and “weird feelings in her head that come and go.” Id.
 Ms. E.S.       recounted the same general medical history post-2014 vaccinations, adding that she
 had taken a leave of absence from school starting in March 2016. Id. Her neurological exam and
 brain MRI/MRA were normal. Id. at 7 (MRI/MRA performed on June 27, 2016). Dr. Wells
 concluded that Petitioner had persistent headaches despite a normal neurological exam and a normal
 brain MRI/MRA, and suggested that she follow up with her cardiologist and endocrinologist and
 try therapy for her anxiety. Id. at 7 (MRI/MRA performed on June 27, 2016).

        In August 2016, Petitioner followed up with Dr. Wallach, her endocrinologist. Ex. 19 at 2–
 3. She generally reported doing better, with an improved HbA1C level of 8.7%, down from more
 than 9%, and some weight loss. Id. at 2. Dr. Wallach noted that Petitioner was ready to go back to
 college after taking the prior semester off for health issues. Id. A treater thereafter (whom Petitioner
 first saw that spring—and hence long after the vaccinations in question) recommended that
 Petitioner not receive the flu vaccine again due to a “history of adverse reaction,” although (as
 revealed by the record above) this assertion is not well-supported by either the bare medical record
 or any informed treater opinion not solely reliant on Petitioner’s self-reported history. Ex. 15 at 1.

        Petitioner obtained some mental health counseling in October 2016. Ex. 13 at 5–6. Later that
 same month, Petitioner visited Dr. Sanjeev Kothare at NYU’s Langone Health System for
 evaluation of possible seizures and sleep problems. Ex. 22 at 5. Although this is the first time such
 symptoms are mentioned in Petitioner’s medical record, she now reported daytime sleepiness and
 insomnia for the past two years (which would place onset in October 2014, or nearly three months
 after the first vaccines in dispute), plus sleep paralysis, vivid/violent dreams, panic attacks, and
 depressed mood—all of which she attributed to her receipt of the flu vaccine in 2015. Id. at 6;

21
   Notes from that visit also briefly discussed Petitioner’s sister—who allegedly had her own reaction to the HPV vaccine
and has filed a petition in the Program. Ex. 23 at 8 (“[t]here is some confusion about what the sister had, and what
[Petitioner] has had: while racing heart was noted as ventricular tachycardia in the sister by a monitor, [Petitioner] who
has similar complaints has not had this. . . . The relationship between the reactions to Gard[a]sil [sic] in the sisters, if any
is also unclear”).
22
   Human leukocyte antigen (HLA) testing is a blood test that identifies antigens on the surface of cells and tissues.
Mosby’s at 306–07. These antigens can identify patients who are allergic to certain medications or to confirm diagnosis
of certain diseases in which the antigens are present. Id. at 306.
                                                               8
 Statement of Pet., filed Apr. 14, 2017 (ECF No. 7-1), at 3.

         Dr. Kothare noted a history of snoring, dry mouth, mouth breathing, leg twitching, abnormal
 arousals (sleep walking and confusional arousals), and daytime sleepiness were also present. Ex.
 22 at 6. However, Petitioner had a normal neurological exam with no evidence of sensory deficits
 in response to light touch, pin prick, position, and vibration. Id. at 8. It was also noted (at a follow-
 up visit in December 2016) that there were no reported instances of cataplexy. 23 Id. at 11. As of the
 initial visit, Dr. Kothare diagnosed Petitioner with narcolepsy type 2, non-REM parasomnia, and
 REM sleep disorder. Id. at 9.

       Petitioner underwent a nocturnal polysomnography test on November 21, 2016. Ex. 22 at 27.
 The results were interpreted to reveal the existence of mild sleep apnea and “upper airway resistance
 syndrome,” both of which were considered treatable. Id. Then, in January 2017, Ms. E.S.           had
 a multiple sleep latency test (“MSLT”). Ex. 36 at 33, 35. The results were deemed by Dr. Kothare
 to reveal “evidence of excessive daytime sleepiness” which “could be consistent with narcolepsy
 under the appropriate clinical circumstances,” leading him to propose follow-up clinical
 confirmation. Id. at 35. Dr. Kothare noted mild obstructive sleep apnea but normal baseline
 oxygenation, normal CO2, normal EKG, and no significant periodic leg movements. Id. at 24. Dr.
 Kothare saw Petitioner again in March 2017, and after review of the MSLT results and another
 exam, he again confirmed his earlier diagnosis of type 2 narcolepsy (i.e. without cataplexy). Ex. 36
 at 46–50.

         D. 2017 and Post-Filing Treatment

       In January 2017, laboratory results from CellTrend and GmbH were sent to Petitioner’s
 mother. Ex. 16 at 1. Ms. E.S.      was found to be positive for anti α-1-adrenergic antibodies and
 anti-muscarinic cholinergic receptor 4 antibodies. 24 Ex. 16 at 1. She was also “at risk” for anti-
 muscarinic cholinergic receptor 3 antibodies. Id.

        On February 23, 2017, Petitioner saw Dr. Lefkowitz again, who expressed the view that the
 potentially cardiac-associated symptoms were not likely the product of coronary disease. Ex. 18 at
 14 (“[s]he had a thorough workup which revealed ultimately that she had no evidence of coronary
 artery disease on CT angiography”). Dr. Lefkowitz concluded that any cardiac risk factors that Ms.
  E.S.     faced were most credibly associated with her existing diabetes. Id. Petitioner still sought
 treatment for her overall complaints, however, with some treaters allowing the possibility of a link

23
  Cataplexy is a condition in which there are abrupt attacks of muscular weakness and hypotonia triggered by an
emotional stimulus such as mirth, anger, fear, or surprise and is often associated with narcolepsy. Dorland’s at 298.

24
  Dr. Steinman (one of Petitioner’s experts) has referenced a recent study that associates certain autoantibodies, including
adrenergic receptor antibodies, with ME/CFS and fibromyalgia. Steinman Second Report, filed on Jan. 14, 2019 (ECF
No. 85-1), at 26. Dr. Steinman has also maintained that elevated muscarinic receptor antibodies are also associated with
ME/CFS, POTS, CRPS, and fibromyalgia. Id.
                                                             9
     to the HPV vaccine. See, e.g., Ex. 19 at 3 (March 2017 visit to Dr. Wallach).

           This case was subsequently initiated in April 2017, although the period thereafter continued
     to be punctuated by urgent care or emergency treater visits, as Petitioner grappled with the same
     overall constellation of symptoms that she had confronted since the fall of 2014. In May 2017, for
     example, Petitioner visited the ER for chest pain—described as sharp, mild, ongoing, and
     exacerbated by movement and palpitation. Ex. 33 at 57–71. An EKG showed possible left arterial
     enlargement but no evidence of ischemia. Id. at 65. Ms. E.S.     was diagnosed with non-specific
                                   25
     chest pain and hypoglycemia. Id. at 71.

           Four days later, on May 24, 2017, Petitioner returned to the ER. Ex. 33 at 24. She stated that
     “[s]he drank a lot and her insulin pump is going crazy.” Id. On intake, Petitioner reported a tingling
     in her chest and chest pain for the last two days. Id. 24–25. Labs reported that Petitioner’s blood
     alcohol level was 0.137, 26 and a urine screen was positive for cannabinoid. Id. at 17, 21, 40. An
     EKG mostly was normal but did detect a prolonged QT. 27 Id. at 8, 23. Petitioner was discharged
     and diagnosed with hypoglycemia and nausea. Id. at 11.

            There is a lengthy records gap through January 2018, when Petitioner returned to the ER with
     abdominal, rectal, and chest pain with nausea. Ex. 34 at 1. An EKG test was borderline but showed
     normal sinus rhythm and a rightward axis. Id. at 72. A few months later, in April 2018, Petitioner
     sought more treatment for her purported narcolepsy and sleep issues. Ex. 102 at 1. Dr. Rodriguez,
     a board-certified sleep medicine specialist, noted that Petitioner had paralysis and hallucinations at
     night. Id. He recommended 0.25-0.5 mg of Clonazepam, and Petitioner was advised to follow up in
     three months. Id.

            Then, in late June 2018, Ms. E.S.       visited Dr. Susan Levine, a specialist in infectious
     disease and internal medicine. Ex. 98 at 27. A subjective exam showed weakness, fatigue,
     palpitations, upset GI, and numbness of lower extremities. Id. During an objective exam, Dr. Levine
     noted that Petitioner had “[n]euro-diminished sensory over L4/L5 and L5/S1 deformities; 5/+5 good
     motor strength in both lower extremities; [and] slightly diminished patellar reflexes bilaterally.” Id.

25
  Hypoglycemia is an abnormally diminished concentration of glucose in the blood, which may lead to tremulousness,
cold sweat, piloerection, hypothermia, and headache; when chronic and severe it may cause central nervous system
manifestations that in rare cases can even be fatal. Dorland’s at 890.
26
  A blood alcohol concentration (“BAC”) of 0.10-0.12 causes significant impairment of motor coordination, including
balance, speech, vision, and control, as well as loss of judgment. Stanford University, Office of Alcohol Policy and
Education, What is BAC?, https://alcohol.stanford.edu/alcohol-drug-info/buzz-buzz/what-bac (last visited Nov. 2, 2020).
A BAC of 0.13-0.15 causes gross impairment of motor control, blurred vision, and major loss of balance, as well as
dysphoria, which includes anxiety and restlessness. Id.

27
  Long QT syndrome (“LQTS” or “prolonged QT”) is a heart rhythm condition that can potentially cause fast, chaotic
heartbeats. These rapid heartbeats might trigger you to suddenly faint. Mayo Clinic, Long QT syndrome,
https://www.mayoclinic.org/diseases-conditions/long-qt-syndrome/symptoms-causes/syc-20352518 (last visited Nov.
10, 2020).
                                                          10
     Relying on the above, but also on prior test results, Dr. Levine assessed Ms. E.S.                 with
                                                         28
     inflammatory neuropathy, autonomic dysfunction, gastroparesis, and endometriosis. Id. Notably,
     EMG and nerve conduction study tests performed on September 12, 2018 only supported a mild
     radiculopathy rather than true neuropathy. Ex. 49 at 27. Not long after this visit, Dr. Levine prepared
     the one-page report that Petitioner has submitted in support of her claim. Ex. 85.

        Petitioner followed up with Dr. Levine in August 2018. Ex. 98 at 26. She now reported
continuing daily weakness, fatigue, palpitations, worsening ability to function, and increased panic.
Id. Dr. Levine assessed Petitioner with ME/CFS, 29 DM1, post-HPV vaccine onset of CFS symptoms,
dysautonomia, and POTS. 30 Id. However, the record does not include evidence of confirmatory
testing for the POTS diagnosis.

        In the fall of 2018, Petitioner visited Dr. Russell Chin, a neurologist at Weill Cornell
 medicine, for “suspected neuropathy” upon referral by Dr. Levine. Ex. 49 at 1; Ex. 48 at 1. Dr. Chin
 ordered EMG testing and epidermal nerve fiber density testing via skin biopsy. Ex. 48 at 1; Ex. 49
 at 27. Petitioner reported that since 2015, she had noticed some intermittent tingling sensations in
 her mid-chest region, and since early 2018 tingling and “chilled” sensations to her scalp, neck, and
 shoulders (complaints that, as the review of records to this date should reveal, are not especially
 reflected in her overall history). Ex. 49 at 2. Although Petitioner has claimed that Dr. Chin
 “suspected” she had progressing small fiber neuropathy in her body since 2015, Dr. Chin merely
 expressed the view that her symptoms were possibly related to other dysautonomic/autoimmune
 issues (such as her diabetes, inflammatory arthritis, or an IgA deficiency). Ex. 86 at 34–37.
 However, he ultimately acknowledged that the “[e]tiology of these symptoms is unknown.” Ex. 49
 at 7.

        An EMG/nerve conduction study performed at this time suggested to Dr. Chin carpal tunnel
 and ulnar entrapment of the right arm, a mild radiculopathy of the lower extremities, but no evidence
 of neuropathy. Ex. 49 at 27–34. However, extensive laboratory tests for causes of neuropathy
 yielded normal results with the exception of Petitioner’s known diabetes and elevated cholesterol
 levels. Id. at 21–26. The two skin biopsies performed at this time showed reduced sweat gland nerve
 fiber density and a reduced intra-epidermal nerve fiber density at one site. Ex. 48. A brain MRI

28
  The autonomic nervous system is the portion of the nervous system concerned with regulation of the activity of cardiac
muscle, smooth muscle, and glandular epithelium; usually restricted to the two visceral efferent peripheral components,
the sympathetic nervous system, and the parasympathetic nervous system. Autonomic nervous system, Dorland’s
Medical Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=111779 (last visited Oct. 26, 2020).

29
  People with myalgic encephalomyelitis/chronic fatigue syndrome (ME/CFS) have overwhelming fatigue that is not
improved by rest. ME/CFS may get worse after any activity, whether it’s physical or mental. Other symptoms can include
problems with sleep, thinking and concentrating pain, and dizziness. Centers for Disease Control and Prevention, Myalgic
Encephalomyelitis/Chronic Fatigue Syndrome, What is ME/CFS? (last visited Nov. 10, 2020).
30
     At a December 2018 follow-up Dr. Levine’s assessment was ME/CFS and dysautonomia. Ex. 98 at 26.

                                                          11
     performed on Ms. E.S.       on September 24, 2018 revealed “a 4 X 4 X 3 mm nonenhancing lesion
     along the pituitary gland” and a “punctate focus of T2 hypointensity.” Ex. 49 at 20. The radiologist
     who obtained the imaging deemed it to potentially “reflect the provided history of a pituitary
     adenoma,”31 adding that no prior imaging was available to make any comparisons or further
     assessments. Id. at 21. I am unaware of any additional documents filed in this case relating to any
     subsequent exams or treatments conducted by Dr. Chin.

         On August 12, 2019, Petitioner saw Dr. David S. Younger, a neurologist, for additional
evaluation. Dr. Younger reviewed Petitioner’s medical history and past studies as well as performed
a physical examination. Ex. 105 at 3. The examination showed sensory loss, hyporeflexia, distal leg
weakness, Romberg sign, 32 and tandem imbalance. Id. Upon review of past studies, Dr. Younger
noted that a 2012 MRI showed degenerative changes. Id. Although, tests from 2016 appeared normal,
the 2018 pituitary MRI studies suggested a microadenoma. Id. at 2. Dr. Younger recommended
additional screening studies. Id. On November 7, 2019, Dr. Younger saw Petitioner for a follow-up
visit. Id. at 6. Dr. Younger now reported that skin changes suggested possible vasculopathy. Id.
Petitioner’s neck and shoulder pain and chest discomfort suggested combined cervicogenic and
autonomic disturbances. Id. Dr. Younger again recommended additional screening studies as well as
a psychiatric assessment. Id.

 II.      Expert Reports and Other Evidence

       Thirteen expert reports have been filed in this matter, totaling more than 200 pages of opinion.
 Hundreds, if not thousands, of pages in supporting medical research and literature have also been
 offered. As of today, Petitioner has presented six reports from three different experts, and
 Respondent has filed seven reports from four individual experts. Each expert, their credentials, and
 opinions are considered in turn.

          A.      Petitioner’s Experts

                  1.       Dr. Lawrence Steinman

       Dr. Steinman prepared three reports in support of Petitioner’s claim. Report, dated Mar. 2,
 2018, filed as Ex. 39 (ECF No. 47-1) (“First Steinman Rep.”); Report, dated Jan. 14, 2019, filed
 as Ex. 86 (ECF No. 85-1) (“Second Steinman Rep.”); Report, dated Feb. 15, 2019, filed as Ex. 99
 (ECF No. 90-1) (“Third Steinman Rep.”). Dr. Steinman inconsistently focuses on different aspects

31
  A pituitary adenoma is a slow-expanding growth deemed benign in the vast majority of cases. Mayo Clinic, Pituitary
Tumors, https://www.mayoclinic.org/diseases-conditions/pituitary-tumors/symptoms-causes/syc-20350548 (last visited
Oct. 26, 2020).
32
  Romberg sign/syndrome, or facial hemiatrophy, is a condition of unknown etiology, characterized by progressive
atrophy of the tissues of one side of the face, frequently with pigmentation disorders and alopecia. Sometimes it can
spread to involve both sides of the face or the ipsilateral trunk, viscera, or limbs.
                                                           12
     of Petitioner’s case, depending on the date of his report and whether the report was reacting to the
     assertions of one of Respondent’s experts.

            Dr. Steinman currently serves as the chairman in immunology and professor in the
     departments of neurology, pediatrics, and genetics at Stanford University. Steinman Curriculum
     Vitae, filed as Ex. 40 (ECF No. 52-1) (“Steinman CV”) at 1. He obtained his bachelor’s degree
     from Dartmouth College before earning his medical degree from Harvard University. Id. He then
     completed his internship and residency in surgery, pediatrics, and pediatric and adult neurology at
     Stanford University. Id. He has also completed several fellowships in the area of immunology. Id.
     He is board certified in neurology, though much of his work in the field also involves
     immunological concepts and theories. Id. at 2. However, he has no demonstrated expertise in
     treating or diagnosing diabetes or conditions attributable to autonomic dysfunction.

                            a. First Steinman Report

            In his first report, Dr. Steinman limited his opinion solely to whether the HPV vaccine doses
     Petitioner received in 2014 and 2015 and/or the flu vaccine from 2015, could have caused the
     narcolepsy and headaches Petitioner asserts she experienced. First Steinman Rep. at 1. He began by
     considering when such symptoms likely first manifested. Dr. Steinman opined that onset of Ms.
          E.S.’s headaches could be placed in early October 2014 (based on an ER note associated with
     that visit). Ex. 9 at 3. Other medical records, however, reveal that Petitioner complained of
     headaches well before her first HPV dose in July 2014. Id. at 30; Ex. 3 at 16 (headache listed among
     chief complaints on September 19, 2013). Onset of narcolepsy, in contrast, was by Dr. Steinman’s
     admission harder to pinpoint. Id. at 30–31. The first mention of any sleep issues appears in an
     October 2016 record—where Petitioner reported that she had been experiencing such symptoms in
     the two-plus years since receiving the flu vaccine. Id. at 31. This contention is not only
     uncorroborated by the record but is partially in conflict with it (since Petitioner had received the flu
     vaccine in August 2015—hence only 14 months prior). Ex. 22 at 5.

            Dr. Steinman proposed that Petitioner’s narcolepsy could have been caused specifically by
     the HPV vaccine. First Steinman Rep. at 6. He relied on molecular mimicry as the biologic
     mechanism for how this occurred, basing this contention on what is known about how narcolepsy
     likely occurs. Id. at 22. Dr. Steinman explained that decreased levels of hypocretin 33 and/or
     abnormalities in hypocretin receptor 2 in the brain are scientifically understood to play a central
     role in the occurrence of narcolepsy. Id. at 8 (citing Ex. 39, references 9 and 10). Aberrant immune
     responses are thought to possibly explain such circumstances. First Steinman Rep. at 8 (discussing

33
  Hypocretin, also known as orexin, is “either of two neuropeptides (orexin A ad orexin B) produced in the hypothalamus
and regulating behavior as well as the sleep-wake cycle.” Orexin, Dorland’s Medical Dictionary Online,
https://www.dorlandsonline.com/dorland/definition?id=35458 (last visited Aug. 13, 2020).

                                                          13
     references 11–17). Decreased hypocretin neurotransmission is thought to be due to autoimmune-
     mediated destruction of hypocretin-containing neurons in the lateral hypothalamus. Ex. 39, Ref. 9,
     at 39.

            One possible way the immune response could create conditions for narcolepsy would be
     where an antigen presenting to the immune system (whether from a wild virus or vaccine) might
     mimic “various components of the hypocretin pathway, including hypocretin itself and the HCRT-
     R2 receptor.” First Steinman Rep. at 9. Dr. Steinman estimated the HPV vaccine could accomplish
     this—but to bulwark this contention he relied significantly on “BLAST” searches 34 he personally
     performed, looking for homology between HPV vaccine components and hypocretin pathway
     structures. Id. 35 In so doing, Dr. Steinman explained that his criteria for “a meaningful molecular
     mimic” relied on evidence of five or more amino acids that were identical (although fewer could
     also trigger a cross-reaction, and the amino acids did not in his view need to be identical in
     sequence). Id. (citing Exhibit 39, references 18–20).

            Based on electronic database research performed specifically for this case, Dr. Steinman
     maintained that several proteins in the HPV vaccine had sufficient homology to hypocretin to have
     the potential to induce an autoimmune cross-reaction that would trigger narcolepsy. First Steinman
     Rep. at 11–22. For support, he referenced a study finding increased incidence of narcolepsy
     following receipt of the HPV vaccination. Id. at 25 (citing L. Arnheim-Dahlstrom et al.,
     Autoimmune, Neurological, and Venous Thromboembolic Adverse Events After Immunization of
     Adolescent Girls with Quadrivalent Human Papillomavirus in Denmark and Sweden: Cohort Study,
     British Med. J. 1, 1–11 (2013), filed as Ex. 39, Ref. 24 (ECF No. 50-4) (“Arnheim-Dahlstrom”)).
     However, Arnheim-Dahlstrom found no supporting associations between exposure to the
     quadrivalent HPV vaccine and autoimmune, neurological, or venous thromboembolic adverse
     events. Although associations for three autoimmune events were initially observed, on further
     assessment these associations proved weak, and not temporally related to vaccine exposure.
     Arnheim-Dahlstrom at 1. Dr. Steinman acknowledged that this observed increase did not reach a
     level of statistical significance—but proposed (based on his layman’s understanding of the legal
     standards applicable to Vaccine Program cases) that it was sufficient to meet the preponderance test
     relevant to fact determinations in this case. First Steinman Rep. at 27. 36

34
   Basic Local Alignment Search Tool (“BLAST”) is a medical/scientific internet resource that assists researchers in
finding regions of similarity between biological sequences of amino acids. The program compares nucleotide or protein
sequences to sequence databases and calculates the statistical significance. BLAST, U.S. National Library of Medicine,
https://blast.ncbi.nlm.nih.gov/Blast.cgi (last visited Oct. 6, 2020).
35
   In other cases, Dr. Steinman has characterized the research undertaken to identify such homology as an “in silica”
study—by which he means that he used a desktop or personal computer, and access to scientific databases, to identify
the comparable amino acid sequences that he references to establish homology. See, e.g., Blackburn v. Sec. of Health &
Hum. Servs., No. 10-410V, 2015 WL 425935, at *10 (Fed. Cl. Spec. Mstr. Jan. 9, 2015). This kind of research is clearly
case-oriented, and is not equivalent to lab or clinical research that an expert might perform and/or rely upon for an
opinion.

36
     In his second report, Dr. Steinman went to great lengths to cast doubt on the lack of statistical significance he had
                                                            14
           In addition, Dr. Steinman generally seemed to embrace a loose timeframe for narcolepsy
     onset as medically acceptable—in effect suggesting that any onset “weeks to months” from the date
     of vaccination to the time Petitioner obtained a formal sleep test confirmed narcolepsy diagnosis
     was reasonable, since it was literally after the vaccines were administered in 2014 and 2015. Id. at
     31. Dr. Steinman more specifically suggested that onset within eight months of vaccination would
     be a generally reasonable timeframe for narcolepsy to first manifest (relying on studies about the
     flu vaccine and narcolepsy). Id.

            Further, Dr. Steinman opined that Petitioner’s headaches were attributable to the HPV
     vaccine. First Steinman Rep. at 30. In support, he noted that the vaccine’s package insert lists
     headaches as a frequent symptom (although it specifically envisions them as a transient response,
     likely occurring close in time to vaccination, and does not identify headache as a chronic post-
     vaccination concern). Id.; Gardasil [Package Insert]. Whitehouse Station, NJ: Merck & Co., Inc.;
     2011, filed as Ex. 39, Ref. 7 (ECF No. 48-7) (“Gardasil Package Insert”).

            Dr. Steinman also noted the existence of “strong evidence that calcitonin-gene-related-
     peptide (CGRP) is involved in chronic headache, particularly migraine.” First Steinman Rep. at 28.
     Based on sufficient evidence of homology between the antigenic components of the HPV vaccine
     and CGRP, Dr. Steinman reasoned that the vaccine might plausibly trigger an autoimmune cross-
     reaction sufficient to produce headaches. Id. at 28–29. The headaches could later become chronic,
     due to the fact that the vaccine’s alum additive (used as an adjuvant, to cause a more robust immune
     response) 37 has been demonstrated to persist for up to a year (albeit in animal studies). Id. at 30
     (citing Z. Khan et al., Slow CCL2 Translocation of Biopersistent Particles from Muscle to Brain,
     11 BMC Medicine (2013), filed Mar. 5, 2018 as Ex. 39, Ref. 27 (ECF No. 50-7)). This, plus the
     fact that the immune response to HPV vaccine itself can be long-lasting, lent further support to his
     conclusion that chronic headaches could be propagated by the vaccine. First Steinman Rep. at 30
     (citing C. MacIntyre et al., Immunogenicity and Persistence of Immunity of a Quadrivalent Human

seemingly admitted in his first report about Arnheim-Dahlstrom’s conclusions, making arguments about the mathematic
guidelines used in evaluating whether a given statistical finding had significance that (by his own admission) exceeded
his expertise. Second Steinman Rep. at 22–23.
37
  The argument that the alum adjuvant ingredient in a vaccine can remain in the body for extended periods of time post-
vaccination, and thereafter cause or contribute to immunologic harm, is perilously close to a discredited theory often
posed by unsuccessful petitioners, termed “ASIA,” or “autoimmune/inflammatory syndrome induced by adjuvants.” See,
e.g., Yalacki v. Sec’y of Health & Hum. Servs., No. 14-278V, 2019 WL 1061429, at *24 n.30 (Fed. Cl. Spec. Mstr. Jan.
31, 2019), mot. for review den’d, 146 Fed. Cl. 80 (2019) (noting several prior decisions in which special masters rejected
the ASIA theory as scientifically unreliable). The evidence that a vaccine’s adjuvants can act in this manner (as opposed
to merely increase the immunogenicity of the vaccine generally) is thin to none and has little acceptance in the medical
community otherwise as a reputable theory. See, e.g., Rowan v. Sec'y of Health & Hum. Servs., No. 10–272V, 2014 WL
7465661 (Fed. Cl. Spec. Mstr. Dec. 8, 2014); mot. for review den'd, 2015 WL 3562409 (Fed. Cl. 2015); D'Angiolini v.
Sec'y of Health & Hum. Servs., No 99–578V, 2014 WL 1678145 (Fed. Cl. Spec. Mstr. Mar. 27, 2014), mot. for review
den'd, 122 Fed. Cl. 86 (2015), aff'd, 645 F. App'x 1002 (Fed. Cir. 2016).

                                                           15
 Papillomavirus (HPV) Vaccine in Immunocompromised Children, 34 Vaccine 4343, 4343–45
 (2016), filed Mar. 5, 2018 as Ex. 39, Ref. 28 (ECF No. 50-8)).

                           b. Second Steinman Report

       Dr. Steinman’s second report was of comparable length to his first, but largely aimed at
 responding to counter-arguments (discussed in more detail below) that had been lodged by two of
 Respondent’s experts. See generally Second Steinman Rep.

        Dr. Steinman began by referencing some new research relevant to the biological processes
 underlying narcolepsy (specifically pertaining to the hypocretin pathway) that he maintained was
 additionally supportive of his previously-asserted opinion. Second Steinman Rep. at 1–4; D.
 LaTorre et al., T cells in Patients with Narcolepsy Target Self-Antigens of Hypocretin Neurons,
 Nature 1, 1–23 (2018), filed Jan. 14, 2019 as Ex. 87 (ECF No. 85-2) (“Latorre”). Latorre observed
 the existence of “peptides that attacked orexin [another term for hypocretin] and were found in the
 spinal fluid,” and that these amino acid sequences showed homology with HPV vaccine antigens
 (based on Dr. Steinman’s BLAST searches). Second Steinman Rep. at 1–3; Latorre at 538. As a
 result, Dr. Steinman concluded that “this degree of homology is sufficient to induce clinically
 relevant neuroinflammation.” Second Steinman Rep. at 3. He later emphasized literature he felt
 underscored the legitimacy of BLAST searches to establish potentially significant homologies (for
 purposes of establishing the potentiality of pathologic autoimmune cross-reactions). Id. at 16–18.

        Next, Dr. Steinman attempted to rebut arguments attacking various aspects of his theory. He
 acknowledged that Petitioner did not have (and was never diagnosed with) type I narcolepsy—the
 kind that is more definitively understood to have an autoimmune character. Thus, she was not
 positive for the HLA molecules most associated with type I narcolepsy, and had otherwise not been
 tested for hypocretin levels either. Second Steinman Rep. at 7. However, Dr. Steinman still
 contended that type II narcolepsy could have an autoimmune character or etiology—although in
 doing so he devoted many pages of his second report to a detailed defense of research he had
 previously cited, or had been involved with, rather than citing evidence that more directly supported
 his opinion. Id. at 5–15. At bottom, Dr. Steinman proposed that the rarity of a vaccine-induced
 narcolepsy excused the need for more statistically-significant or robust evidence supporting his
 argument. Id. at 14, 22.39

38
  Page five of the Latorre article filed by Petitioner appears to be blank. Dr. Steinman, however, provides a copy of the
referenced table on page two of his second report.
39
  Dr. Steinman similarly diminished the need for epidemiologic evidence linking the HPV vaccine to narcolepsy,
maintaining that it was “not the proper tool to decide whether, in a given individual with a given disease, the vaccine did
NOT trigger the disease in that individual.” Second Steinman Rep. at 18. This completely misstates the relevant
evidentiary burden (and underscores why Dr. Steinman should avoid commenting on the legal standards employed in
adjudicating Program claims). Although it is very true that petitioners are never compelled to present epidemiologic
evidence, and can thus prevail without it, it is a petitioner’s ultimate burden to establish preponderantly that a vaccine
caused an injury. The Respondent is not tasked with proving a negative (that the vaccine could not have caused the
                                                            16
             Dr. Steinman reiterated prior arguments regarding the purported link between the HPV
     vaccine and Petitioner’s chronic headaches. He emphasized that an association between the two
     was not only established by the vaccine’s package insert, but also by VAERS 40 reports identifying
     headache as a commonly reported adverse event. Second Steinman Rep. at 18–19. He elaborated
     on how he proposed the headaches could become chronic, noting that the vaccine’s antigenic
     particles would bind with alum contained in it, and thereby persist in the body for as long as the
     alum did. Id. at 19–20. This argument seems to assume that because there is some limited evidence
     that alum can persist, that the vaccine’s initial immune-stimulative impact would last for the same
     timeframe; however, Dr. Steinman did not offer evidence showing this beyond items referenced in
     his initial report suggesting that the vaccine had created long-lasting immunity against HPV (not
     that its components would continuously stimulate the immune system in a pathologic manner, and
     specifically cause chronic headaches in the process).

            In addition to defending previously expressed opinions regarding Petitioner’s purported
     narcolepsy and headaches, Dr. Steinman addressed some of the additional diagnoses she had
     obtained after the case’s filing (including CFS and SFN). Second Steinman Rep. at 24. He noted
     that testing performed on Ms. E.S.       in the fall of 2016 (over a year from the time she received
     the second HPV dose) and obtained in January 2017 established she possessed elevated levels of
     muscarinic41 antibodies associated with CFS. Second Steinman Rep. at 24–25. He maintained that
     these antibodies played a significant role in the pathogenesis of CFS. Id. In contrast, the literature
     offered for this proposition was less certain. M. Loebel et al., Antibodies to β Adrenergic and
     Muscarinic Cholinergic Receptors in Patients with Chronic Fatigue Syndrome, 52 Brain, Behavior,
     and Immunity 32–39 (2016), filed Jan. 15, 2019 as Ex. 97 (ECF No. 42-4) (“Loebel”). Loebel, for
     example, noted that there was evidence of elevated levels of these antibodies in only a “subset” of
     CFS patients, and also that the function of the antibodies remained unclear (and thus could not

injury), but may offer evidence that undercuts the success of a claimant’s showing. As a result, reliable epidemiologic
studies can be evaluated—and can undermine a petitioner’s showing—even if they cannot preponderantly disprove the
possibility of causation by itself.
40
  The Vaccine Adverse Event Reporting System (“VAERS”) is a national early warning system to detect possible safety
problems in U.S.-licensed vaccines. VAERS, https://vaers.hhs.gov/about.html (last visited Oct. 7, 2020). VAERS was
established in 1990 and is co-sponsored by the Centers for Disease Control and Prevention (CDC), and the Food and
Drug Administration (FDA), agencies of the U.S. Department of Health and Human Services (HHS). Id.
41
   Muscarinic receptors are a type of cholinergic receptor that is stimulated by the alkaloid muscarine and blocked by
atropine; it is found on autonomic effector cells as well as central neurons in the thalamus and cerebral cortex. Muscarinic
Receptor, Dorland’s Medical Dictionary Online, https://www.dorlandsonline.com/dorland/definition?id=102569 (last
visited Oct. 7, 2020). Different types may be distinguished on the basis of pharmacologic specificity or molecular
structure; a number of differing nomenclatures have been applied to these types. Id. Cholinergic receptors are a type of
cell-surface receptor that binds the neurotransmitter acetylcholine and mediates its action on postjunctional cells.
Cholinergic               Receptor,              Dorland’s               Medical              Dictionary            Online,
https://www.dorlandsonline.com/dorland/definition?id=102541 (last visited Oct. 7, 2020). Types include
parasympathetic autonomic effector cells, sympathetic and parasympathetic autonomic ganglion cells, striated muscle,
and certain central neurons. Id.

                                                            17
     definitely be said to contribute to CFS’s pathogenesis). Loebel at 38.

            Dr. Steinman also proposed that these antibodies (that would potentially attack the same
     neuroreceptors relevant to autonomic dysfunction that could in turn produce CFS, POTS, or other
     similar conditions) could be produced as part of an autoimmune, cross-reactive process instigated
     by the HPV vaccine, and cited literature purportedly to that effect. S. Ikeda et al., Autoantibodies
     against Autonomic Nerve Receptors in Adolescent Japanese Girls after Immunization with Human
     Papillomavirus Vaccine, 2 Annals of Arthritis and Clinical Rheumatology 1, 1–6 (2019), filed Nov.
     24, 2019 as Ex. 107 (ECF No. 106-1) (“Ikeda”). Ikeda (in a case-control comparison of young girls
     who received the HPV vaccine versus those who did not) did observe increased levels of these
     autoantibodies directed against the relevant nerve receptors in those who had received the HPV
     vaccine. Ikeda at 3. However, Ikeda’s authors also frankly admitted that “[t]here was no significant
     association between the major symptoms including dysautonomic symptoms and the serum levels
     of autoantibodies” (Id. at 4)—a lynchpin of the argument that these autoantibodies are pathogenic.42

            Nevertheless, Dr. Steinman proposed that the antibodies associated with chronic fatigue were
     also mimics of HPV antigens, similarly citing additional BLAST search evidence in support as with
     prior representations about homology between HPV vaccine components and hypocretin pathway-
     associated amino acid sequences. Second Steinman Rep. at 26–33. Thus, this could again establish
     a mechanism by which the vaccine might promote this additional injury. Dr. Steinman also noted
     that Petitioner’s visit to Dr. Chin in the fall of 2018 (after his first report was prepared and filed)
     corroborated the chronic fatigue and small fiber neuropathy diagnoses with reliable testing (such as
     a skin biopsy for the latter). Id. at 35–38.

                             c. Third Steinman Report

            A month after his second report had been filed, Dr. Steinman prepared an additional, final
     report solely to address the question of onset of Petitioner’s CFS or SFN. See generally Third
     Steinman Rep. He asserted that the onset of these conditions (which were not even diagnosed until
     three years after the second round of relevant vaccines administered in August 2015) was medically
     acceptable, invoking his prior findings about post-vaccine headache onset (early October 2014,
     hence two and one-half months after vaccination), and narcolepsy (in the fourteen months after
     receipt of the flu vaccine in August 2015). Id. at 1–2.

           To support the medical acceptability of onset for such varied conditions, Dr. Steinman
     referenced an item of literature specific to the HPV vaccine. Third Steinman Rep. at 2; K. Ozawa

42
   In addition, further undercutting the reliability of any determinations in Ikeda is the fact that its authors approvingly
cited to the ASIA theory discussed above to support the contention that vaccines can “occasionally trigger the
development of POTS, CRPS, and CFS.” Ikeda at 5 n.38 (referencing an article written by the creator of the ASIA theory,
Dr. Yehuda Shoenfeld). Dr. Shoenfeld is a frequent Program expert, and has offered the opinion that the HPV vaccine
can cause dysautonomic injuries like POTS or chronic fatigue—although not credibly. See, e.g., Johnson v. Sec’y of
Health & Hum. Servs., No. 14-254V, 2018 WL 2051760, at *22–23 (Fed. Cl. Spec. Mstr. March 23, 2018).
                                                            18
et al., Suspected Adverse Effects After Human Papillomavirus Vaccination: A Temporal
Relationship Between Vaccine Administration and the Appearance of Symptoms in Japan, 40 Drug
Safety 1, 1–11 (2017), filed Feb 15, 2019 as Ex. 100 (ECF No. 90-2) (“Ozawa”). Ozawa was an
observational study from Japan that considered the symptoms reported by 120 female subjects who
had received the HPV vaccine in the 2013-16 timeframe. Ozawa at 1. Ozawa observed that certain
symptoms (including fatigue, headaches, sleep disturbance, and autonomic dysfunction) manifested
on average within 360 days of vaccination—supporting a lengthy, post-vaccination timeframe.
Ozawa at 9. Ozawa itself, however, notes that the average time for onset observed was “very long
in comparison with the adverse effects of conventional vaccinations,” and attributed this in part to
the fact that “it is rather difficult to determine the exact time of onset” for the symptoms it
considered. Id. More importantly, the overall probative value of Ozawa’s findings was limited by
other deficiencies in the study readily acknowledged by its authors, including but not limited to (a)
a lack of an unvaccinated control group, (b) its generally small sample size, and (c) the self-selection
of studied subjects, all of whom specifically sought out the medical institution for which Ozawa’s
authors worked to report their concerns that the vaccine had caused their symptoms. Id. at 2, 9.

              2.      Dr. Sin Hang Lee

      Dr. Lee, a pathologist, prepared two expert reports on Petitioner’s behalf, both of which
sought to establish that (a) her preexisting diabetes was exacerbated by the two HPV vaccine doses
she received in 2014 and 2015, and (b) she developed myocardial ischemia due to those same
vaccines. Report, dated Mar. 23, 2018, filed as Ex. 41 (ECF No. 55-1) (“First Lee Rep.”); Report,
dated Oct. 30, 2018, filed as Ex. 50 (ECF No. 78-1) (“Second Lee Rep.”).

       Dr. Lee studied at Wuhan Medical College and Tongji University College of Medicine from
1951 to 1956. Sin Hang Lee Curriculum Vitae at 1, filed on Mar. 23, 2018 (ECF No. 61-1). In 1966,
he earned his F.R.C.P. (C) from the Royal College of Physicians and Surgeons of Canada. Id. He
participated in several post-graduate training programs and held several teaching positions in China,
Hong Kong, Canada, and the United States—several of which focused on pathology. Id. at 1–2. He
is licensed to practice medicine in Connecticut and is boarded in pathology. Id. at 2. Dr. Lee is
currently the director of Milford Molecular Diagnostics Laboratory, in Milford, Connecticut, which
performs DNA sequencing-based diagnostic testing to confirm conditions like Lyme disease. Id.;
Milford Molecular Diagnostics, http://www.dnalymetest.com/ (last visited Oct. 6, 2020). His first
report acknowledges that the opinions he has provided were based on a review of Petitioner’s
medical history and his own research into “the science available in the public domain,” (as opposed
to professional research or expertise pertaining to the issues in dispute). First Lee Rep. at 1.

                     a. First Lee Report

     Dr. Lee described type 1 (or “insulin-dependent”) diabetes generally as an autoimmune-
                                                 19
     induced condition, mediated by T cells and autoantibodies, in which insulin-producing beta cells
     (responsible for regulating blood sugar) in the pancreas are destroyed, resulting in downstream
     sequela attributable to the inability of the body in the absence of insulin to monitor and control
     blood sugar levels. First Lee Rep. at 6; M. Cnop et al., Mechanisms of Pancreatic β-Cell Death in
     Type 1 and Type 2 Diabetes: Many Differences, Few Similarities, 54 Diabetes S97, S97–S107
     (2005), filed Mar. 23, 2018 as Ex. 41, Ref. 6 (ECF No. 56-6). Dr. Lee proposed that the HPV
     vaccine had significantly exacerbated Petitioner’s DM-1, based on several independent points. First
     Lee Rep. at 5.

             First, Dr. Lee noted that federal safety disclosures relating to the HPV vaccine’s approval for
     use revealed instances in which the vaccine may have been associated with new cases of diabetes—
     although to reach this conclusion, Dr. Lee relied on tortuous math that is almost facially incorrect
     from a scientific/epidemiologic standpoint. He cited to the fact that in the HPV vaccine’s clinical
     trials, the same number of vaccinated individuals (two out of 10,706) reported new cases of type 1,
     insulin-dependent diabetes (measured at fourteen days after each vaccine dose administration) as
     the unvaccinated placebo group (two out of 9,412)—suggesting no statistically-significant greater
     incidence of vaccine-associated cases (18.7 cases per 100,000 for vaccinated individuals, versus
     21.2 for the control group). Id.; Gardasil [Package Insert]. Whitehouse Station, NJ: Merck & Co.,
     Inc.; 2011, filed as Ex. 41, Ref. 4 at 8 (“Gardasil Package Insert”). This finding might seem not to
     support Petitioner’s overall claim.

            Dr. Lee, however, compared these rates to a “national statistics report” from 2016, which
     showed an incidence of 19.9 cases of diabetes total per 100,000 unvaccinated individuals for the
     entirety of 2005 (prior to the HPV vaccine’s approval). Although this earlier incidence rate exceeds
     what was observed for even vaccinated individuals from the HPV vaccine trials, Dr. Lee maintained
     (without demonstrating his methodology)43 that this figure “translates” into a far lower incidence
     of .74 cases per 100,000 after two weeks—thus establishing a “25 fold” increase in the incidence
     rate for vaccinated individuals as reflected in the safety study data. How this calculation can be
     possibly reliable (since Dr. Lee has not shown that the 2005 data identifies diabetes onset as
     reasonably occurring in the span of two weeks—and if so, based on what starting point, since it
     does not measure time from a vaccination or placebo event) is not explained, although Dr. Lee’s
     report rapidly moves on.

          Next, Dr. Lee maintained that based upon what was understood about how the HPV vaccine
     mechanistically “works” (coupled with some speculative points of his own about an inadvertent
     byproduct of its manufacture), a reliable theory could be proposed for how the vaccine’s
     components might worsen a preexisting case of DM-1. First Lee Rep. at 6–14. The relevant
     formulation of the HPV vaccine, he contended, contains purified “virus-like particles,” or VLPs,

43
  Presumably, Dr. Lee took the data for 2005, divided it by 365 (for the total days in a year), and then multiplied that
sum by 14—although doing so does not precisely produce the rate he cites in his report.

                                                          20
     derived from the L1 capsid 44 for the HPV wild virus. Id. at 6; Gardasil Package Insert at 12. To
     provoke an immune response to the presentation of these VLP antigens after vaccination, the HPV
     vaccine includes alum as an adjuvant. First Lee Rep. at 7–9. Some vaccines have also begun to
     incorporate toll-like receptor (“TLR”) agonists, a different kind of biologic adjuvant that helps
     stimulate a greater immune response (although this distinct form of adjuvant has primarily been
     used to date in anticancer therapies). Id. at 8–10. However, Dr. Lee admitted TLR agonists are not
     an intentional component of the HPV vaccine’s formulation. Id. Nevertheless, Dr. Lee maintained
     that the process by which HPV vaccine was manufactured likely resulted (inadvertently) in the
     inclusion of some “viral DNA fragments” that would in effect “serve as potent long-acting TLR9
     agonist”—and hence acting as “the actual functional adjuvant.” Id. at 12.

           From the above, Dr. Lee attempted to explain how the HPV vaccine could aggravate type I
     diabetes. Although much remains unknown about the pathogenesis of this form of diabetes, Dr. Lee
     proposed that some new research establishes that TLR ligands (which can function like agonists)
     play a “key role in initiation or aggravation of type 1 diabetes.” First Lee Rep. at 13 (citing A.
     Limmer et al., Stimulation of Autoimmunity by Toll-like Receptor Ligands, 64 Annals Rheumatic
     Diseases 15, 15–18 (2005), filed Mar. 23, 2018 as Ex. 41, Ref. 31 (ECF No. 59-1); S. Ferris et al.,
     The Islet-Resident Macrophage is in an Inflammatory State and Senses Microbial Products in
     Blood, 7;214(8) J. Experimental Med. 1, 1–17 (2017), filed Mar. 23, 2018 as Ex. 41, Ref. 32 (ECF
     No. 59-2) (“Ferris”); J. Dowling & A. Mansell, Toll-like Receptors: The Swiss Army Knife of
     Immunity and Vaccine Development, 5 Clinical Translational Immunology 1, 1–10 (2016), filed
     Mar. 23, 2018 as Ex. 41, Ref. 33 (ECF No. 59-3)).

           Of these cited articles, only Ferris addresses diabetes head-on. In Ferris, researchers
     examined the transcriptional profiles of macrophages in diabetic mice. The mice demonstrated an
     increased inflammatory signature, including elevated expression of chemokines 45 and chemokine
     receptors and an oxidative response. Ferris at 1. Researchers concluded, among other things, that
     macrophages have the capacity to sense blood-born stimuli. Id. at 10. Nevertheless, because type I
     diabetes is believed to have an autoimmune component, activation of TLRs in such a person would
     (in Dr. Lee’s view) occur by “augment[ing] production of all autoantibodies against self-antigens,”
     including those autoantibodies thought to attack the insulin-producing beta cells—thus exacerbating
     an existing case of diabetes. First Lee Rep. at 14.

          Dr. Lee attempted to set his theory within the context of Ms. E.S.’s actual experience. First
     Lee Rep. at 14–15. Relying on an overview of the medical history (Id. at 1–4), he observed that

44
  Gardasil is the trade name for the Human Papillomavirus Quadrivalent (Types 6, 11, 16, and 18) Vaccine, Recombinant,
a non-infectious recombinant quadrivalent vaccine prepared from the purified virus-like particles (VLSs) of the major
capsid (L1) protein of HPV Types 6, 11, 16, and 18. The L1 proteins are produced by separate fermentations in
recombinant Saccharomysces cervisiae and self-assembled into VLPs. Gardasil Package Insert at 12.
45
  Chemokines are regulators of the immune system and may also play a role in the circulatory and central nervous
systems. Dorland’s at 335.
                                                         21
  Petitioner appeared to have fair control of her diabetes prior to her receipt of an initial HPV vaccine
  dose. Id. at 1–2, 14. But, her diabetic-associated symptoms greatly worsened in the months thereafter,
  as reflected in the many ER and doctor visits she had (at which time her glucose levels were
  consistently determined to be high). Id. Then, after her second HPV vaccine dose in August 2015,
  Petitioner started to develop chest pain and experienced additional worsening symptoms, including
  vomiting. Id. at 14. He specifically deemed the timeframe between the second HPV dose
  (administered August 19, 2015) and her October 10, 2015 ER visit—a more than seven-week
  period—as medically acceptable, although (incongruously) in so doing he referenced his prior
  arguments about the HPV clinical trials revealing post-vaccination onset as possible within two
  weeks. Id.; Gardasil Package Insert at 14–21.

         Besides exacerbation of type I diabetes, Dr. Lee’s first report included the opinion that the
HPV vaccine could outright trigger a myocardial ischemia due to low blood perfusion, and did so to
Petitioner. First Lee Rep. at 15. Dr. Lee explained that if and when immune cells are activated as a
result of receipt of the HPV vaccine, and then reach sufficient number in the myocardium, the
cytotoxic cytokines generated by these immune cells can cause myocardial depression with reduced
cardiac outputs and low blood profusion through the myocardium, leading to irreversible myocardial
damage in certain genetically and physically predisposed individuals. Id. at 16–17; See also Second
Lee Rep. at 7. He noted that (again referencing the HPV vaccine package insert) syncope (resulting
from insufficient blood flow to the brain attributable in turn to low blood pressure (hypotension) is
the most commonly-reported adverse reaction after receipt of the vaccine. Id; Gardasil Package Insert
at 27. He did not, however, specify the expected timeframe for such an adverse event (and syncope
itself is expected to occur very close-in-time, if at all, to vaccination—not months or years later).
Gardasil Package Insert at 1.

        Syncope is a feature of orthostatic intolerance—a category that includes POTS, and that has
been associated with receipt of the HPV vaccine. However, by Dr. Lee’s admission this association
“has not received much attention of [sic] the medical community.” First Lee Rep. at 15. Dr. Lee cited
a post-licensure survey study observing (for a 2006 to 2008 timeframe) that out of 12,424 reported
adverse events, there were 32 deaths, six of which could be shown to have been cardiac-related. First
Lee Rep. at 15; B. Slade et al., Postlicensure Safety Surveillance for Quadrivalent Human
Papillomavirus Recombinant Vaccine, 302 JAMA 750–57 (2009), filed Mar. 23, 2018 as Ex. 41,
Ref. 36 (ECF No. 59-6) (“Slade”) (medical and autopsy reports on 20 of the 32 deaths confirmed
there were 4 unexplained deaths and 6 cardiac-related deaths). From this, Dr. Lee concluded that
vaccine-induced hypotension could in turn reduce blood flow to the heart, thereby incurring a
“jeopardized myocardium.” First Lee Rep. at 15.

        Dr. Lee offered a causation theory for how the HPV vaccine might initiate such a process,
 which paralleled or relied on his theory addressing aggravation of diabetes. He reiterated his prior
 contention that the vaccine likely contained “a set of ready-made instant DNA immune ‘mediators’”
 (in the form of the purported TLR agonist attributable solely to the vaccine’s manufacture, rather
                                                  22
     than an actual ingredient), which enabled the innate immune system’s macrophages to transport
     vaccine antigens throughout the body—including across the blood-brain barrier. First Lee Rep. at
     16. He offered a case report as evidence of the latter. F. DiMario et al., A 16-year-old Girl with
     Bilateral Visual Loss and Left Hemiparesis Following an Immunization Against Human
     Papillomavirus, 25 J. Child Neurology 321–27 (2010), filed Mar. 23, 2018 as Ex. 41, Ref. 39 (ECF
     No. 59-9) (“DiMario”). However, DiMario is factually distinct in that it involved localized
     encephalomyelitis and a biopsy-confirmed tumefactive demyelinating lesion. In addition, Dr. Lee
     referenced a Program case in which it was purportedly established that the HPV vaccine caused a
     child’s death from a silent myocardial infarction (however, the facts and circumstances of that case
     are readily distinguishable). First Lee Rep. at 18; Gomez v. Sec’y of Health & Hum. Servs., No. 15-
     160V, 2016 WL 6072391 (Fed. Cl. Spec. Mstr. Sept. 21, 2016). 46

            Dr. Lee proposed that the stimulation of TLRs induced by vaccination could equally promote
     upregulation of a variety of proinflammatory cytokines, some of which (like tumor necrosis factor
     alpha (TNF-α or Il-1β)) are “recognized myocardial depressants” which can cause damage to the
     myocardium in physically predisposed individuals. First Lee Rep. at 16–17; J. Parrillo et al., A
     Circulating Myocardial Depressant Substance in Humans with Septic Shock: Septic Shock Patients
     with Reduced Ejection Fraction have a Circulating Factor that Depresses in Vitro Myocardial Cell
     Performance, 76 J. Clinical Investigation 1539–53 (1985), filed Mar. 23, 2018 as Ex. 41, Ref. 40
     (ECF No. 59-10). A sufficient number of these “cytotoxic cytokines” would be capable of causing
     myocardial depression and low blood perfusion, resulting in “irreversible myocardial damage.”
     First Lee Rep. at 16–17.

            Dr. Lee supported his theory pertaining to Petitioner’s purported heart issues with the medical
     record. As before, he deemed significant the before/after vaccination distinction in Ms.        E.S.’s
     health, focusing particularly on the growing evidence that she might have a cardiac disorder after
     the August 2015 second HPV vaccine dose. First Lee Rep. at 17. He took particular note of the
     cardiac consultation Petitioner received from Dr. Lefkowitz in the winter of 2016 (six months from
     receipt of the second dose), at which time a stress EKG revealed the possibility of a jeopardized
     myocardium. Id; Ex. 5 at 3. However, Dr. Lee acknowledged that this determination was not
     conclusively made at this time. Id. Nevertheless, Dr. Lee maintained that literature supported an
     association of the kind of abnormality observed at this time with moderate ischemia. First Lee Rep.
     at 17; L. Shaw et al., Comparative Definitions for Moderate-Severe Ischemia in Stress Nuclear,
     Echocardiography, and Magnetic Resonance Imaging, 7 JACC Cardiovascular Imaging 593–604
     (2014), filed Mar. 23, 2018 as Ex. 41, Ref. 50 (ECF No. 60-7). In addition, Dr. Lee drew attention
     to the fact that as of March 2016, Petitioner’s serologic testing revealed heightened levels of white
     blood cells, which he deemed “indicative of an augmented immune reaction . . . probably with
     associated increased discharge” of the cytokines he previously maintained were known myocardial

46
  In Gomez (a matter in which Dr. Lee also offered an expert report), a 14-year old male died a day after receipt of a
second dose of HPV vaccine—a far cry from the present facts. Moreover, that case settled, and therefore no reasoned
causal determination was issued that could shed light on this matter’s disposition. Gomez, 2016 WL 6072391, at *1.
                                                         23
     depressants. First Lee Rep. at 18.

            To support the timing for an association between the August 2015 second HPV dose and the
     February 2016 diagnostic evidence as proof of Petitioner’s vaccine-caused cardiac issues, Dr. Lee
     noted again the post-licensure studies, like Slade. First Lee Rep. at 18; Slade at 750. Of the 32 post-
     HPV vaccine deaths observed (approximately .26 percent of the 12,424 reported adverse events),
     the timeframes for fatality were from 2 to 405 days. Slade at 755. As a result (although without any
     showing specific to the cardiac-associated deaths), Dr. Lee concluded that a six-month lag in this
     case was medically acceptable.

                            b. Second Lee Report

            In reaction to arguments lodged by Respondent’s experts in opposition to his theories, Dr.
     Lee prepared a second report even lengthier than his first (although it was padded with large sections
     featuring wholesale reproduction of other articles, portions of websites, or similar authorities). See
     generally Second Lee Rep. 47

            Much of the supplemental report addresses Dr. Lee’s prior contentions that Petitioner’s
     alleged cardiac injuries were caused by the HPV vaccine. Second Lee Rep. at 1–16. He strenuously
     defended his conclusion that Petitioner had in fact experienced an “untoward cardiac event,”
     referencing the February 2016 stress test cited in his first report, and noting that Dr. LaRue
     (Respondent’s cardiologist expert) had acknowledged that some “ST segment elevation” was
     observed from the stress test, which could “represent acute ischemia.” Id. at 1–2. Dr. Lee (who lacks
     comparable cardiac expertise) fiercely attacked Dr. LaRue’s diminishment of the importance of
     these findings as medically incorrect. Id. at 2–5; A. Ali et al., Early Repolarization Syndrome: A
     Cause of Sudden Cardiac Death, 7 World J. Cardiology 466, 466–75 (2015), filed Nov. 16, 2018
     as Ex. 51 (ECF No. 79-1). He also observed that Petitioner had additional abnormal EKG results
     after her ER visits in May 2017 and January 2018, thus corroborating the proposed diagnosis.
     Second Lee Rep. at 4; Ex. 33 at 8; Ex. 34 at 72. Ultimately, he accused Respondent’s expert of
     relying on “half-truth and twisted science” in rejecting the conclusion that Petitioner had
     experienced myocardia ischemia. Second Lee Rep. at 7. And he went to great lengths to defend his
     conclusion that the test results set forth in the record were a sufficient basis for his diagnostic
     opinion. Id. at 7–10.

           To bulwark his prior contentions that Petitioner’s purported myocardial ischemia occurred in
     a medically acceptable timeframe, Dr. Lee noted that the two cytokines even Respondent’s experts
     admitted were associated with it (TNF-α and Il-1β) had been established to persist even six months

47
   Indeed, Dr. Lee attempted to rebut some of the criticisms and questions that Respondent’s experts lodged against his
first report mainly by repeating verbatim the arguments he had already set forth (rather than by homing in on how the
objections were unreasonable or wrong). See, e.g., Second Lee Rep. at 41 (“I have copied and pasted below the most
relevant part” of prior report), 42–49 (reproducing five pages of the first report in the second).
                                                          24
from the date of vaccination. Second Lee Rep. at 14; Report, dated July 2, 2018, filed as Ex. A
(ECF No. 68-1), at 6, 8; D. Herrin et al., Comparison of Adaptive and Innate Immune Responses
Induced by Licensed Vaccines for Human Papillomavirus, 10 Hum. Vaccines Immunotherapies
3446–54 (2014), filed Mar. 23, 2018 as Ex. 41, Ref. 29 (ECF No. 58-9) (“Herrin”). In Herrin,
however, blood plasma was analyzed for ten circulating cytokines and chemokines, including TNf,
at pre-vaccination and post-first and third vaccination at days 1, 2, 5, 14 and 28 and at month seven,
but no statistically significant trends were observed that would corroborate the conclusion that these
two particular cytokines were likely to persist for as long as Dr. Lee assumed. Herrin at 3449–50.

       Dr. Lee expanded on his causation theory, offering additional support for his general assertion
that “aluminum adjuvant-laden macrophages” travel in the body (and thus transport the adjuvant
away from the site of vaccine administration) but also could conceivably cluster in the myocardium,
causing a sufficiently-harmful concentration of the cytokines specific to myocardial ischemia to
propagate the condition. Second Lee Rep. at 16; M. Mold et al., Insight into the Cellular Fate and
Toxicity of Aluminium Adjuvants Used in Clinically Approved Human Vaccinations, Nature:
Science Reports 1, 1–13 (2016), filed Mar. 23, 2018 as Ex. 41, Ref. 34 (ECF No. 59-4) (“Mold”).
In Mold, a comparative study was undertaken to monitor the particle size distributions of aluminum
adjuvants through the process of vaccine formulation using dynamic light scattering. Id. at 1.
Results suggested that the particle size distributions may be important for its immunological
recognition and subsequent clearance from the injection site. Id. Dr. Lee deemed this
“straightforward science.” Second Lee Rep. at 16.

       In addition, Dr. Lee maintained his contentions (relating type I diabetes to the HPV vaccine)
in the face of Respondent’s experts’ criticisms. First, he strenuously argued that his treatment of the
HPV vaccine licensing data (which he had cited as proof that the vaccine was associated with an
increased incidence of diabetes) was legitimate (despite the obvious mistakes in his reading of this
data that Respondent’s experts readily pointed out). Second Lee Rep. at 17–18, 20–21. He attacked
other epidemiologic studies referenced by Respondent which credibly undercut the HPV vaccine-
diabetes association as biased or merely “observational” and thus not worthy of significant weight.
Id. at 18–20; C. Chao et al., Surveillance of Autoimmune Conditions Following Routine Use of
Quadrivalent Human Papillomavirus Vaccine, 271 J. Internal Med. 193–203 (2012), filed July 27,
2018 as Ex. C, Tab 18 (ECF No. 70-9) (“Chao”). At the same time, he referenced again Arnheim-
Dahlstrom as bulwarking his argument (even though in comparison it dealt with a drastically
smaller sample size of only 23 individuals). Second Lee Rep. at 18–20; Arnheim-Dahlstrom at 4.

       Second, Dr. Lee reiterated his argument about the mechanism by which the HPV vaccine
would theoretically cause injury, explaining the extent to which his theory was adjuvant-based. He
repeated arguments contained in his first report about how a “proprietary aluminum salt” used in
HPV vaccine’s manufacture could only act as an adjuvant in concert with a TLR agonist—
something purportedly found in the vaccine due to the presence of “gene DNA fragments” left over
in the process of manufacture. Second Lee Rep. at 49. He referenced two items of literature he had
                                                25
     himself authored to support this argument. S. Lee, Detection of Human Papillomavirus (HPV) L1
     Gene DNA Possibly Bound to Particulate Aluminum Adjuvant in the HPV Vaccine Gardasil, 117
     J. Inorganic Biochemistry 85, 85–92 (2012), filed Nov. 16, 2018 as Ex. 66 (ECF No. 80-6); S. Lee,
     Guidelines for the Use of Molecular Tests for the Detection and Genotyping of Human
     Papillomavirus from Clinical Specimens, 903 Methods Molecular Biology 65–101 (2012), filed
     Nov. 16, 2018 as Ex. 67 (ECF No. 80-7); Second Lee Rep. at 49–52. As indirect support for these
     overall contentions, Dr. Lee referenced Nobel prize-winning research into the role that TLRs play
     “as the sensors of innate immunity.” Second Lee Rep. at 52; Press Release, The Nobel Assembly at
     Karolinksa Institutet, The Nobel Prize in Physiology or Medicine 2011 (Oct. 3, 2011),
     https://www.nobelprize.org/prizes/medicine/2011/press-release/ (last visited Oct. 13, 2020).

            Moreover, Dr. Lee revisited different elements of the medical record to defend his opinion.
     He argued, for example, that the flank pain Ms. E.S.          frequently reported was reflective of
     hyperglycemia related to her diabetes—and thus spikes in glycated hemoglobin levels caused (in
     his view) by the HPV vaccine would explain such symptoms. Second Lee Rep. at 24. He rejected
     attributing the worsening of Petitioner’s diabetes to adolescence, arguing that she lacked other
     important risk factors linked to worsening such as an eating disorder, treatment-associated insulin
     restriction, or other disruptions in medical monitoring that might occur when a young person goes
     to college. Id. at 25–27. He maintained that evidence of inflammation taken from testing performed
     on Petitioner in March 2016, at which time she had been diagnosed with a ruptured ovarian cyst,
     was independent of the cyst (since the type of inflammation associated with such a cyst was
     absent 48) and instead attributable to “autoimmune reaction” begun by the vaccines received no
     earlier than seven months before (the time of the second HPV vaccine dose). Id. at 29–33.

            Besides defending his own conclusions, Dr. Lee endeavored to rebut the suggestions of
     Respondent’s experts that the general picture of Petitioner’s overall post-vaccination worsening
     (evidenced in her repeated returns to the ER beginning in the fall of 2014) could be explained by a
     “selective IgA [antibody] deficiency,” thereby producing more frequent viral infections that could
     in turn trigger loss of control of blood glucose. Second Lee Rep. at 36, 37. Dr. Lee countered by
     pointing out the limited number of pre- versus post-vaccination ER visits (Id. at 37), and also that

48
   Specifically, Dr. Lee opined that in cases of what he termed “acute abdomen,” an afflicted individual would display
high levels of neutrophils in the blood and site of infection/injury, but normal to below-normal lymphocytes in blood
tests. Second Lee Rep. at 28–30. Petitioner’s CBC differential from March 6, 2016 showed the opposite, in his reading.
Id. at 31–32. However, the article Dr. Lee cited for this proposition (although never filed into the record) related to
abdominal pain generally rather than a burst cyst. Id. at 30; J. Deibener-Kaminsky, Leukocyte Differential for Acute
Abdominal Pain in Adults, 17 Lab Hematology 1, 1–5 (2011). Moreover, one of Respondent’s experts, Dr. MacGinnitie,
observed that a CBC count performed just two days before the cyst incident showed no lymphocyte increase, consistent
with an earlier blood test in November 2015—and thus totally rebutting Dr. Lee’s supposition that the CBC reading he
called attention to reflected some ongoing and chronic condition consistent with his theory. Ex. 19 at 142. Dr. Lee
explained away these contrary results, arguing that lymphocyte levels could naturally fluctuate, and adding that the
evidence he had previously offered establishing that the HPV vaccine generally caused sustained levels of inflammatory
cytokines ultimately supported his contentions (disregarding the fact that the two other blood tests referenced by Dr.
MacGinnitie were inconsistent with the idea that the HPV vaccine would lead to persistently-elevated inflammation due
to the cytokines it encouraged). Second Lee Rep. at 33–36.
                                                          26
some of the support for Respondent’s argument was derived from a case control study with a
distinguishable study sample group (males considerably older than Petitioner). Id. at 38–39. He
emphasized that the GI symptoms Petitioner often experienced were common by-products of
uncontrolled diabetes, further limiting the likelihood that they reflected something else (although
not making it more likely that the vaccine itself was to blame for the diabetes-related flares). Id. at
39–40.

       Regarding onset, Dr. Lee acknowledged (in effect) that type I diabetes would not literally
“begin” within two weeks of vaccination, but clarified that he meant to argue that its impact on a
person’s insulin-producing pancreatic beta cells could be discerned in such a short timeframe.
Second Lee Rep. at 21. He also disputed the contention of Respondent’s experts that glycated
hemoglobin levels were themselves a strong biomarker for destruction of such beta cells, proposing
instead that these levels were only proof of a “general trend” and not a predictor independent from
the impact of vaccination. Id. at 23–24. He nevertheless attempted to link record instances in which
testing exposed a spike in these levels to prior receipt of the HPV vaccine, maintaining that the
process would “take a few months to express.” Id. at 24.

       Finally, Dr. Lee attempted to defend his opinion that the HPV vaccine could cause orthostatic
intolerance (manifesting in different ways, like syncope or POTS) by arguing that it could occur on
a transient basis, and thus the record (which does not establish persistent instances of POTS close
in time to vaccination, or regular events comparable to it) supported his contention. Second Lee
Rep. at 13–14. He again referenced VAERS reporting of such instances, along with the vaccine’s
package insert. Second Lee Rep. at 28.

              3.      Dr. Susan Levine

       Dr. Levine, a board-certified specialist in infectious diseases, and one of Petitioner’s more
recent treaters, offered a one-page letter in support of Petitioner’s claim. Letter, dated September
28, 2020, filed as Ex. 47 (ECF No. 75-1). The letter was derived from Dr. Levine’s treatment of
Ms. E.S.       well after the filing of this case. Dr. Levine opined that Petitioner suffers from CFS,
orthostatic intolerance, “brain fog,” and migraine headaches, all of which interfere with her ability
to “function in a predictable and consistent manner.” Letter at 1. The bases for Dr. Levine’s opinion
seem to be derived from a review of Petitioner’s medical history. Ex. 98 at 27. Dr. Levine has not
provided any substantiation for these diagnoses outside of her record review, nor does her one-page
letter propose that Petitioner’s illnesses are attributable to the HPV or flu vaccines.

     B.      Respondent’s Experts

             1.      Dr. Shane LaRue

     Dr. LaRue is a cardiologist by training and teaches at the Washington University School of
                                                27
Medicine. He prepared two reports in support of Respondent’s position in this case. See generally
Report, dated July 2, 2018, filed as Ex. A (ECF No. 68-1) (“First LaRue Rep.”); Report, dated May
3, 2019, filed as Ex. G (ECF No. 94-1) (“Second LaRue Rep.”). Dr LaRue maintains that Ms.
 E.S.    does not suffer from myocardial ischemia, and denies that any of the relevant vaccines she
received could cause it.

      Dr. LaRue studied at the University of Wisconsin-Madison where he obtained his bachelor’s
degree in biochemistry before earning his medical degree from the Medical College of Wisconsin.
LaRue Curriculum Vitae at 1, filed on July 27, 2018 (ECF No. 68-9). He then obtained a master’s
degree in population health sciences from Washington University School of Medicine. Id.
Currently, Dr. LaRue is Assistant Professor of Medicine, Section of Heart Failure and Cardiac
Transplantation, in the Cardiovascular Division at Washington University School of Medicine. Id.
He is board certified by the American Board of Internal Medicine in Advanced Heart Failure and
Transplant Cardiology. Id. at 2. And has authored numerous peer-reviewed manuscripts concerning
various aspects of cardiology. Id. at 5–11.

       Dr. LaRue’s first report began with consideration of some of the instances of cardiac-oriented
treatment documented in Petitioner’s medical records. He noted the July 2011 instance (three years
prior to the first HPV dose) when Ms. E.S.           first appeared to complain of chest pain and
associated symptoms, and at that time received some degree of medical work-up (including an
EKG). First LaRue Rep.at 2; Ex. 17 at 198. Not only did treaters identify no underlying explanation
for her complaints, but the EKG was deemed normal. At most, it included evidence of “early
repolarization”—a benign finding that is common in young people (especially those who are
athletic like Petitioner), even though the shape of the relevant wave recorded on the EKG looks
similar to the pathologic wave elevation that can be seen during acute myocardial infarction or
pericarditis. Id; Second LaRue Rep. at 1; Ex. 17 at 198; A. Goldberger, et al., Electrocardiogram
in the Diagnosis of Myocardial Ischemia and Infarction, uptodate.com 36 (2019), Ex. G1, filed on
May 7, 2019 (ECF No. 94-2). This early EKG was also in Dr. LaRue’s view consistent with
Petitioner’s two later EKGs. Second LaRue Rep. at 1.

       Thereafter, the record revealed that Petitioner next obtained treatment for possibly heart-
related symptoms in February 2016, when she saw Dr. Lefkowitz. Ex. 5 at 2. However, Dr. LaRue’s
detailed evaluation of the records from this treatment event (as well as testing performed in its wake)
suggested to him no evidence of anything significant from a cardiac standpoint, let alone myocardial
ischemia. In particular, he highlighted the fact that Petitioner’s pain was initially considered
“exertional in nature,” and thus had not appeared spontaneously, and also that her initial physical
exam was normal. First LaRue Rep. at 2; Ex. 5 at 2. Dr. LaRue admitted that the 2016 EKG did
reveal the possibility of an abnormality, but opined that (comparing this one to the 2011 EKG and
one other Petitioner received in October 2015—both of which were deemed normal) it also included
wave shapes consistent with the (normal) “early repolarization” he saw in all three EKGs. First

                                                28
     LaRue Rep. at 2–3, 6–7. 49

            Dr. LaRue conceded that Petitioner also received a positive EKG stress test 50, but emphasized
     his view that it only supported the “possible” existence of a jeopardized myocardium, adding that
     the stress test generally only serves as a screening device that should prompt additional testing and
     analysis. First LaRue Rep. at 4; see also Second LaRue Rep. at 4 (“positive findings of a wall
     motion abnormality on a stress [EKG] may not be the result of ischemia”). Its sensitivity was
     correlated to the general incidence for coronary issues in the relevant population—and here,
     Petitioner’s youth made it unlikely that the result would have much predictive value. Id. Moreover,
     as a result of the positive stress test result (and consistent with its very purpose), Petitioner was
     subsequently referred for a cardiac CT angiography 51—which in Dr. LaRue’s reading revealed no
     evidence at all of “significant coronary artery disease,” myocardial ischemia, or a “jeopardized”

49
   In response to Dr. Lee’s argument that the “early polarization” justification for all three EKGs’ reported normal findings
did not hold up (because Petitioner was no longer a college athlete as of 2016), Dr. LaRue maintained that (a) she had
been a consistent athlete when the 2011 EKG was performed, and (b) the repolarization pattern was far more prevalent
than the incidence of observable EKG abnormalities, thus allowing for the conclusion that the possible abnormality
suggested by the repolarization pattern was only an “incidental [EKG] finding with no clinical implications.” Second
LaRue Rep. at 3. He also proposed that the finding in 2016 was not new in light of the two earlier EKGs, further reducing
its overall significance. Id. at 2.

I need not decide the evidentiary significance or meaning of this aspect of the EKG performed on Petitioner in 2016. It
cannot be disputed that the EKG resulted in a subsequent positive stress test, followed by a negative CT angiography,
and that treating cardiologists like Dr. Lefkowitz did not (after consideration of all of the above) ultimately diagnose
Petitioner with myocardial ischemia, or any other significant cardiac condition. The weight of the evidence is thus against
the Petitioner on this aspect of her claim no matter which expert is more “right” about the significance of repolarization
patterns specifically (although Dr. LaRue’s demonstrated greater expertise in the field gives his opinions on these subjects
additional heft).

50
  Dr. LaRue also speculated that the stress test constituted a false positive, noting that the low likelihood of obstructive
coronary disease in a woman in her early twenties, even with type I diabetes, and the fact that prior studies have noted a
false-positive rate of approximately 30% for stress echocardiography. First LaRue Rep. at 4. Dr. Lee termed this argument
a straw man, reflective of an effort by Dr. LaRue to distract from the real issue under discussion while admitting that
Petitioner did show inferior ST elevation. But (just like my evaluation of the purported early polarization evidence from
the EKG) because my analysis turns on test results collectively and what on-the-ground treaters determined, the accuracy
of the stress test in that process (which unquestionably led Dr. Lefkowitz to order follow-up testing) need not be
evaluated, but instead can be presumed to support only the possibility of a cardiac problem—as in fact it was read.

51
  As noted above, Dr. Lee contested whether the testing Petitioner received constituted the best means of evaluating the
presence of myocardial ischemia, noting (as Dr. LaRue acknowledged) that a different diagnostic test—coronary
angiography—was the true “gold standard.” First LaRue Rep. at 5. But Dr. LaRue went on to explain why a CT
angiography was still a perfectly valid test when (as here) the likelihood of coronary disease was not high to begin with,
and that this kind of test was generally sufficiently sensitive to identify the presence (or absence) of a more serious
coronary problem. Id. Dr. LaRue also noted that Ms. E.S.        would not have been a proper recipient for a more accurate
but invasive test, and also that her treaters (who could have ordered any testing they thought appropriate) did not pursue
additional testing. Second LaRue Rep. at 6.

I find that Dr. LaRue persuasively established the legitimacy of the CT angiography test that Petitioner received, and its
reliable scientific value under the circumstances (especially given the lack of other evidence corroborating Petitioner’s
assertions in this regard).

                                                             29
     myocardium. Id. at 2, 3, 5; Ex. 5 at 18. (“[a]ll coronaries are patent without evident atherosclerotic
     plaque”). Indeed, based on such results, Dr. Lefkowitz made no negative diagnostic finding close,
     in any respect, to what Petitioner alleges. Id. at 5; Second LaRue Rep. at 2, 5–6. 52 Thus, Dr. LaRue
     considered Petitioner’s 2016 stress test result a false positive. First LaRue Rep. at 6.

            Moving beyond Dr. Lefkowitz’s 2016 exam, Dr. LaRue saw little from the subsequent
     records that would support the conclusion that Petitioner ever suffered from any meaningful form
     of cardiac issue, vaccine-caused or not. At the first of Petitioner’s May 2017 ER visits (when she
     complained of chest pain, among other things), for example, she received a largely normal EKG
     result (except for the possibility of left atrial enlargement), First LaRue Rep. at 3. Her second May
     2017 visit (facially prompted by an incident of drinking that caused her insulin pump to overreact)
     also resulted in an EKG result deemed normal, with no findings of cardiac-related problems upon
     discharge. Id.; Ex. 33 at 23. 53 Her January 2017 ER visit was comparable, with a similar nonspecific
     EKG (beyond the same evidence of early polarization that Dr. LaRue observed in Petitioner’s prior
     EKGs). Id. at 4. And he discounted the probative value of a January 2018 EKG that was at the time
     interpreted as “borderline-abnormal” (Ex. 34 at 72), noting that his reading of the results did not
     convince him that it was in fact properly understood in this manner, and that her primary symptoms
     as of the date of this EKG pertained to abdominal pain ultimately attributable to a ruptured cyst.
     First LaRue Rep. at 6; Second LaRue Rep. at 4. Petitioner otherwise never displayed other objective
     evidence of ischemia, such as “elevated serum cardiac biomarkers or an abnormality seen on cardiac
     CT or cardiac MRI.” Second LaRue Rep. at 3, 5.

           Dr. LaRue commented on the persuasiveness of Dr. Lee’s arguments that the HPV vaccine
     could be associated with myocardial ischemia (although he admitted in so doing that immunologic
     issues were in fact outside of his primary expertise). Second LaRue Rep. at 10. He agreed that
     cytokines like TNF-α and IL-1β did play a role in myocardial depression, but questioned whether
     they would remain sufficiently elevated months after vaccination to effect such injury (adding that
     the record did not establish that Petitioner had experienced other impacts of cytokine-driven
     inflammation that would be expected to exist under such circumstances, like low cardiac output or
     damage). First LaRue Rep. at 6, 8. He also disputed that the record supported the conclusion that
     these cytokines were in fact elevated as of March 2016. Id. at 8–9.

52
  Indeed—as Dr. LaRue observed, Petitioner was not even complaining of symptoms of ischemia at the time of her
March 2016 exam, when Dr. Lee maintains the ischemia diagnosis was confirmed by EKG and other testing. Second
LaRue Rep. at 2.
53
   In discussing the May 24, 2017 EKG, Dr. LaRue noted (as he did when discussing the February 2016 EKG) another
reason to doubt that it evidenced any potential problems. In Dr. LaRue’s experience, an “auto-generated [EKG] machine”
can produce unreliable results—in particular when the machine itself (via its computer programming) deems a result
suggestive of injury, independent of a human treater’s read of the findings. Second LaRue Rep. at 2, 5; M.E. Guglin et
al., Common errors in computer electrocardiogram interpretation, 106 Int. J. Cardiol. 232–37 (2006). Thus, the first
evidence of a problem from the February 2016 EKG was derived from the “computer generated reading” from the EKG
machine (which itself included the heading “UNCONFIRMED INTERPRETATION”) rather than Dr. Lefkowitz. Second
LaRue Rep. at 2; Ex. 5 at 5. The same was true, in Dr. LaRue’s review, of the subsequent May 2017 EKG report. Second
LaRue Rep. at 4.
                                                         30
            Besides opining on causal allegations specific to Petitioner’s alleged cardiac injury, Dr.
     LaRue reviewed some of her other claimed vaccine-caused harms. For example, his review of the
     record did not lead him to conclude that Petitioner ever experienced persistent or significant
     hypotension. First LaRue Rep. at 6. He agreed hypotension could be a transient post-vaccination
     concern, but challenged that a valid and reliable mechanism existed for explaining how the HPV
     vaccine could produce circumstances in which it would be “transiently” experienced six to nineteen
     months post-vaccination. Second LaRue Rep. at 9. He also noted that Ms. E.S.    ’s blood pressure
     was measured in connection with Petitioner’s March 2016 stress test, but that her readings even
     after the stress of exercise never measured below normal such that an orthostatic hypotension
     diagnosis could be supported. Id. Nor could the condition of cardiac ischemia be deemed to be
     caused by hypotension (although hypotension could result from “cardiac abnormalities”). Id. at 10.

                  2.       Dr. Andrew MacGinnitie

            Dr. MacGinnitie, a pediatrician and immunologist/allergist, prepared two reports for
     Respondent. Report, dated May 1, 2018, filed as Ex. C (ECF No. 69-1) (“First MacGinnitie Rep.”);
     Report, dated May 3, 2019 filed as Ex. H (ECF No. 95-1) (“Second MacGinnitie Rep.”). Dr.
     MacGinnitie’s opinions mostly focused on Petitioner’s alleged narcolepsy, POTS, and headaches,
     and whether the HPV vaccine could cause any of the above, nevertheless he did also address some
     of Dr. Lee’s contentions specific to cardiac issues or mechanisms for vaccine causation.

        Dr. MacGinnitie is currently an attending physician as well as Clinical Director for the
Division of Immunology at Boston’s Children’s Hospital, where he oversees clinical operations for
Allergy/Immunology, Rheumatology, and Dermatology. First MacGinnitie Rep. at 1. He obtained
his medical degree and Ph.D. in Pathology from the University of Chicago Pritzker School of
Medicine. Id. Dr. MacGinnitie is board certified in both Allergy/Immunology and Pediatrics and
maintains an active clinical practice seeing more than 1,600 patients annually. Id. at 2. He also
performs research and has published numerous articles in areas relating to Allergy/Immunology,
including vaccine reactions. Id.

                          a. MacGinnitie First Report

         After a brief overview of Petitioner’s medical history, Dr. MacGinnitie endeavored to rebut
 Dr. Steinman’s narcolepsy theory. First MacGinnitie Rep. at 4. He noted a diagnostic issue that
 undermined Dr. Steinman’s causation theory as presented in this case. Dr. MacGinnitie conceded
 that at least a “plausible case” existed for the contention that a specific formulation of the flu vaccine
 (one that is adjuvanted—a form rarely administered in the U.S., and not received by Ms. E.S.
 in this case) could trigger narcolepsy with cataplexy, or “type 1” narcolepsy, 54 via an autoimmune

54
  Type 1 narcolepsy is caused by extensive loss of hypothalamic neurons that produce the neuropeptides orexin-A and -
B (also referred to as hypocretin-1 and -2). Narcolepsy type 2 includes most of the same symptoms, but its cause is
                                                         31
     process in which antibodies triggered by vaccine antigen presentation cross-react with the
     hypocretin pathway. 55 Id. However, Ms. E.S.          had at best been diagnosed only with type 2
     narcolepsy56—a less severe form not accompanied by cataplexy, and not also believed to be
     autoimmune-driven. Id. at 4–5, 7; T. Scammell, Narcolepsy, 373 New Eng. J. Med. 2654–62
     (2015), filed July 27, 2018 as Ex. C, Tab 1 (ECF No. 69-2). As a result, Dr. Steinman’s entire
     causal explanation was inapplicable to the facts of this case.

            In addition, Dr. MacGinnitie questioned whether (independent of the version of narcolepsy
     Petitioner allegedly had experienced) Dr. Steinman had even established that narcolepsy could be
     driven by an autoimmune process that was vaccine-triggered. First MacGinnitie Rep. at 5–6. Thus,
     he pointed out that many of the individual items of literature Dr. Steinman had cited did not
     demonstrate that persons with narcolepsy possessed sufficient amounts of the purportedly
     hypocretin-oriented autoantibodies for a cross-reaction, while individuals without narcolepsy had
     comparable quantities of the antibodies. Id. at 6; S. Ahmed et al., Antibodies to Influenza
     Nucleoprotein Cross-React with Human Hypocretin Receptor 2, 7 Sci. Translational Med. 1, 1–15
     (2015), filed July 27, 2018 as Ex. C, Tab 3 (ECF No. 69-4). Dr. MacGinnitie deemed this to cast
     “considerable doubt on the importance of these antibodies.” First MacGinnitie Rep. at 6.

            Dr. MacGinnitie raised several other technical objections to the reliability of the causation
     theory that vaccination could provoke an autoimmune response sufficient to interfere with
     hypocretin pathways and thereby cause narcolepsy. First MacGinnitie Rep. at 6–9. But in his view
     a more fundamental flaw in the theory arose from the fact that such evidence, reliable or not,
     involved an adjuvanted flu vaccine—not the HPV vaccine. Regarding the latter, Dr. MacGinnitie
     noted that Dr. Steinman’s argument relied heavily on the contention that mimicry existed between
     HPV vaccine amino acid sequences (the building-blocks of proteins) sufficient to interfere with
     hypocretin pathways, but without reliable evidence (in the form of experimentation or other
     research) showing this actually could occur. Instead, Dr. Steinman relied on animal studies relevant
     to autoimmune-driven demyelination generally, a disease pathogenesis wholly distinguishable from

unknown, and it does not feature cataplexy. T.E. Scammell, Narcolepsy, 373 N. Engl. J. Med. 2654-62 (2015), filed July
27, 2018 as Ex. C, Tab 1 (ECF No. 69-2).
55
  In his second report, Dr. MacGinnitie devoted greater attention to the argument that the flu vaccine could be credibly
associated with any form of narcolepsy, offering two 2018 articles that he proposed diminished the significance of prior
research linking certain formulations of the H1N1 fly vaccine to type 1 narcolepsy. Second MacGinnitie Rep. at 5–8
(references omitted). But because Petitioner did not receive the form of flu vaccine even arguably associated with
narcolepsy, and based on my prior reasoned determinations (mentioned below) that the non-adjuvanted flu vaccine
commonly administered in the U.S. is highly unlikely to cause the condition, I do not herein devote extensive discussion
to these issues. Of the theories advanced in this case, the contention that type II narcolepsy can be caused by the flu or
HPV vaccines was among the least well-substantiated—no matter how robust the association between type I narcolepsy
and some versions of the flu vaccine might be.
56
  People with type 2 narcolepsy do not have cataplexy and have normal orexin-A levels. Scammell, at 4. Type 2
narcolepsy may be caused by less extensive injury to orexin-A and -B transmitters, but data on the disease process are
quite limited. Id.
                                                           32
the receptor blocking at issue in narcolepsy. Id. at 9–10. Dr. MacGinnitie also pointed out that there
were in nature numerous examples of possible molecular mimicry between amino acid sequences
and self-structures (“this level of overlap in protein sequence is common”), yet autoimmune
diseases were not regular occurrences (thus suggesting that homology between sequences alone was
no guarantee of an autoimmune/pathologic reaction). Id. at 10.

       More significantly, Dr. MacGinnitie observed that several large epidemiologic studies (one
of which Dr. Steinman himself cited in his own report) did not demonstrate any significant
incidence of narcolepsy after receipt of the HPV vaccine. First MacGinnitie Rep. at 11; Arnheim-
Dahlstrom at 1. Chao—a study referenced by Dr. Lee, and in Dr. MacGinnitie’s report (and which
has been offered in many other Program decisions)—reached a similar conclusion. Chao at 193.
Chao was a peer-reviewed observational study analyzing a database comprised of the medical
histories of approximately 189,000 women in California to determine whether the studied
population had developed a variety of autoimmune conditions after receiving the HPV vaccine.
Chao at 194.

       Next, Dr. MacGinnitie evaluated the strength of Dr. Steinman’s arguments that Petitioner’s
reported headaches could be associated with the HPV vaccine. He noted that the record did not offer
substantiation for a migraine headache diagnosis for Petitioner, and also that the vaccine package
inserts (which Dr. Steinman purported established headache as an expected post-vaccination
adverse event) described “almost certainly acute events occurring immediately after vaccination,”
rather than a chronic occurrence manifesting long after. First MacGinnitie Rep. at 11. Dr.
MacGinnitie expressed doubt about the proposed mechanism for the headaches, arguing that the
likelihood of the small amount of presenting antigen in the vaccine could travel into the central
nervous system (the “CNS”) to bind with or activate receptors there associated with headache was
low, and that other evidence cited by Dr. Steinman to substantiate persistence of effect over time
(whether due to the alum included in the vaccine as an adjuvant, or evidence that the immunity
effect of the vaccine could last) did not amount to a showing that the “vaccine proteins themselves”
(which constituted tiny amounts of the vaccine) would remain in the body for the same period. Id.
at 12; Second MacGinnitie Rep. at 12.

      Besides his review of Dr. Steinman’s opinion, Dr. MacGinnitie critiqued elements of Dr.
Lee’s arguments about the association between the HPV vaccine and worsening of diabetes or heart
damage. He deemed the former to suffer from “a number of glaring weaknesses,” including but not
limited to the following:

     •   The table referenced from the HPV vaccine safety trials did not establish an increased,
         post-vaccination incidence of new-onset type 1 diabetes, and also used as a control group
         subjects who received a placebo (as opposed to the general population) (First
         MacGinnitie Rep. at 13);

                                                33
         •    Epidemiologic studies like Chao or Arnheim-Dahlstrom showed no association between
              the HPV vaccine and type 1 diabetes (Id. at 13-14 (citing Chao at 201; Arnheim-
              Dahlstrom at 5)); and

         •    Dr. Lee’s incidence calculation was not only mathematically erroneous, but proposed an
              unlikely, drastically high level that “if it were accurate, we would be observing an
              epidemic of [type 1 diabetes] in adolescent boys and girls” (First MacGinnitie Rep. at
              14).

        In addition, Dr. MacGinnitie offered to show, via the filed medical records, that in fact
 Petitioner’s “worsened control” of her diabetes was not likely vaccine-related. First MacGinnitie
 Rep. at 14. As he observed, Ms. E.S.         had one of her highest glycated hemoglobin readings in
 early July 2014—before receipt of the first HPV vaccine dose. Id.; see also Second MacGinnitie
 Rep. at 3 (“her control was worsening prior [to] receiving her fist HPV vaccine”). In contrast, one
 of her best readings came in December 2016, by which time she had received both doses at issue,
 undercutting Dr. Lee’s contention that her levels would be expected to be persistently high due to
 vaccination. Id. at 14–15. Dr. MacGinnitie felt the onset of Petitioner’s late adolescence, with the
 attendant “life changes” that might make monitoring more difficult, or other unhealthy behaviors”
 that occur at the college level (pointing specifically to the instance in which a drinking bout resulted
 in an ER visit), better explained her experiences. Id. at 15; Second MacGinnitie Rep. at 4. 57

       Regarding Petitioner’s purported myocardial ischemia, Dr. MacGinnitie echoed Dr. LaRue,
 maintaining that the medical record (and more specifically EKG and CT testing Petitioner had
 received) did not establish either evidence of decreased blood flow or a jeopardized myocardium,
 nor had any treaters ultimately found otherwise. First MacGinnitie Rep. at 16-17. He disputed Dr.
 Lee’s effort to link such problems to syncope or POTS, noting that (a) at most, the vaccine was
 associated with acute (one-time) episodes of post-vaccination syncope rather than chronic blood
 flow issues, and (b) the HPV vaccine was only linked to POTS by a single four-patient case study.
 First MacGinnitie Rep. at 16. Dr. Lee offered little to no other evidence reliably establishing the
 vaccine could injure the heart. Id. And the record did not suggest that Ms. E.S.  had experienced
 heightened levels of inflammation around the time of her March 2016 cardiac consultation, with
 some testing done before this time revealing no abnormalities, and any higher levels revealed in

57
  As an alternative explanation for Ms.        E.S. ’s diabetes-related post-vaccination symptoms and associated ER visits,
Dr. MacGinnitie proposed “selective IgA deficiency”—a deficiency in an immunoglobulin protective against infection
that Petitioner was diagnosed with as a younger child. First MacGinnitie Rep. at 15. Dr. Lee argued in response that
selective IgA deficiency could not be the cause because Ms.          E.S. ’s relevant ER visits were post-vaccination and not
throughout her childhood. Second Lee Rep. at 37. Further, Ms.            E.S ’s chronic tonsillitis was a health care issue only
after vaccination and obviously unrelated to her SIgAD. Id. at .38. Both sides make reasonable points about the
significance of the levels of this particular antibody, but my decision does not turn on who is “more” correct on this issue,
since (as discussed in detail throughout) I ultimately do not find that any vaccine Petitioner received likely caused the
exacerbation of her type I diabetes.

                                                              34
 March 2016 likely attributable to the ruptured cyst she had experienced. Id. at 16–17. 58

                          b. MacGinnitie Second Report

        Dr. MacGinnitie’s second report contained some more detailed evaluations of theories
 presented by Petitioner’s experts. First, he questioned Dr. Lee’s contention that the HPV vaccine
 doses Petitioner received in 2014 and 2015 could later cause elevated cytokine levels persisting into
 the winter of 2016. He highlighted the fact that articles, like Herrin, explicitly stated that they did
 not find that the specific proinflammatory cytokines (identified by Dr. Lee) became elevated over
 long periods of time after receipt of the HPV vaccine. Second MacGinnitie Rep. at 1–2; Herrin at
 3449–50.

        Dr. MacGinnitie also noted that the mere production of proinflammatory cytokines by
 macrophages was not a “controversial” point, but it did not mean that vaccines encouraged this
 process or could cause it to persist. In so arguing, Dr. MacGinnitie specifically challenged Dr. Lee’s
 assertion that macrophages bearing alum would likely travel into the CNS, noting that the literature
 cited for this concept by Dr. Lee was speculative rather than supported with “actual data.” Second
 MacGinnitie Rep. at 3. And he distinguished literature establishing that the HPV vaccine could
 promote a subsequent increased T-cell/immune response to the vaccine’s proteins (the very purpose
 of vaccination) from a demonstration that the “immune system in general shows increased activity
 after vaccination,” and that this increase would persist for long periods of time. Id. at 4 (emphasis
 in original).

        In addition, Dr. MacGinnitie attempted to address head-on Dr. Lee’s contentions about DNA
 matter persisting in the HPV vaccine formulation—a condition for Dr. Lee’s overall causal theory
 that a “silent” adjuvant (the TLR agonist) found its way into the vaccine and would thereafter
 amplify its pathologic impact. He noted that this element of Dr. Lee’s opinion was only supported
 by two articles Dr. Lee himself authored plus his own experiment, adding that the technique used
 to sense the presence of this DNA was so sensitive that it would pick up the presence of “miniscule”
 amounts, thereby producing false positives. Second MacGinnitie Rep. at 4–5. And in any event, Dr.
 Lee had offered “no evidence that the amount [of cell-free DNA] in the HPV vaccine is sufficient
 to stimulate a significant immune response,” as his theory posited. Id. at 5. 59

58
   Inflammation is a localized protective response elicited by injury or destruction of tissue. Dorland’s at 935.
Inflammation can be acute, usually of sudden onset and predominated by vascular and exudative processes. Id. When
chronic and slow in its progression, it is marked chiefly by the formation of new connective tissue; it may be a
continuation of an acute form or a prolonged low-grade form, and usually causes permanent tissue damage. Id. Dr.
MacGinnitie later partially granted Dr. Lee’s contention that the ruptured cyst might exhibit different kinds of
inflammatory immune cells, but insisted nonetheless that there was overall little evidence of “persistent inflammation.”
Second MacGinnitie Rep. at 4.
59
  Dr. MacGinnitie added that as a general matter, “trace amounts” of DNA in a vaccine were simply unlikely to be
harmful, noting that humans already are exposed to similar DNA from bacteria and micro-organisms without aberrant
impacts, and the blood itself also contains cell-free DNA. Second MacGinnitie Rep. at 5. And vaccine development
                                                          35
         Because chronic fatigue had not been alleged as an additional vaccine injury at the time of
 his first report, Dr. MacGinnitie only addressed it in the second report, emphasizing that the
 diagnosis post-dated the vaccinations at issue by three to four years. Second MacGinnitie Rep. at
 12. Also, he noted that Dr. Steinman’s support for the association between the HPV vaccine and
 chronic fatigue came from a four-person case study, contrasting the embrace of such limited
 evidence (since case studies at bottom only demonstrated a temporal relationship) with Dr.
 Steinman’s arguments that large-scale epidemiologic studies were not sufficiently powered to
 suggest the absence of an association. Id. at 13. Dr. MacGinnitie cited additional epidemiologic
 evidence undercutting a relationship between the HPV vaccine and chronic fatigue. Id.; J. Skufca
 et al., The Association of Adverse Events With Bivalent Human Papillomavirus Vaccination: A
 Nationwide Register-Based Cohort Study in Finland, 36 Vaccine 5226–33 (2018), filed May 7,
 2019 as Ex. H, Tab 17 (ECF No. 96-8) (“Skufca”). Skufca (evaluating a different formulation of
 the HPV vaccine) considered the evidence of adverse outcomes for more than 240,000 females in
 Finland aged 11-15 who received the vaccine, finding no statistically-significant increased
 incidence rate for CRPS or POTS; while a slight increase was observed for chronic fatigue, it was
 consistent with what boy subjects experienced. Skufca at 3. Dr. MacGinnitie otherwise disputed
 that chronic fatigue could even be understood as an autoimmune condition in the first place. Second
 MacGinnitie Rep. at 13–14.

                 3.       Dr. David Raizen

        A neurologist and medical professor with specific training and expertise in sleep medicine
 issues, Dr. Raizen offered two written reports. Report, dated May 24, 2018, filed as Ex. E (ECF No.
 72-1) (“First Raizen Rep.”); Report, dated May 4, 2019, filed as Ex. I (ECF No. 97-1) (“Second
 Raizen Rep.”). Dr. Raizen mainly addressed Dr. Steinman’s contentions pertaining to narcolepsy,
 although he expanded his focus to include Petitioner’s allegations of chronic fatigue in his second
 report.

        Dr. Raizen is an associate professor at the Perelman School of Medicine for the University
 of Pennsylvania, and a practicing neurologist with a sub-specialty in sleep medicine. First Raizen
 Rep. at 1. He is board certified in psychiatry and neurology as well board certified in sleep medicine.
 Id. Dr. Raizen has been treating patients with sleep disorders for the past fourteen years and
 currently follows approximately 50 patients with narcolepsy in an outpatient clinic. Id. In addition,
 he directs a research group aimed at understanding the fundamental mechanisms regulating sleep
 and wake. Id. at 2. Dr. Raizen’s reports were based on consideration of the reports offered from
 Drs. Steinman and Lee, his review of the medical record, and a variety of medical and scientific
 articles bearing on the diagnoses in question and what is known about the pathogenesis of each.
 First Raizen Rep. at 2–3; Second Raizen Rep. at 1.

efforts that seek to rely on the stimulative, adjuvant-like effect of this DNA employ amounts far in excess of the trace
levels that would be found in the HPV vaccine. Id.
                                                          36
                      a. Raizen First Report

        In discussing narcolepsy, Dr. Raizen noted that the “presence of cataplexy” (which he defined
 as “the sudden loss of muscle tone during wakefulness”) was the main distinguishing feature
 between types 1 and 2. First Raizen Rep. at 4. Diagnosing narcolepsy requires consideration of
 medical history, a physical exam, and then the combination of a polysomnography test and a MSLT.
 Id. A sleep latency of eight minutes or less, plus proof of two or more sleep onset REM periods, is
 supportive of a narcolepsy diagnosis. Id. From a pathophysiologic perspective, Dr. Raizen
 emphasized that more was known scientifically about type 1 narcolepsy, and his explanation for it
 (loss of brain neurons that produce hypocretin, plus association with HLA antigen) was consistent
 with what Drs. MacGinnitie and Steinman agreed upon—as was his admission that evidence existed
 associating an adjuvanted form of the flu vaccine that was only administered in Europe (Pandemrix)
 with an increased incidence of type 1 narcolepsy. Id. at 5–6.

       In this case, Dr. Raizen disputed the legitimacy the MSLT Ms. E.S.     underwent in January
 2017, arguing that critical protocols needed to ensure the accuracy of results did not occur. First
 Raizen Rep. at 5. In particular,

      •   performance of the polysomnography the night before the MSLT (“to ensure that proper
          sleep amount was achieved” before the MSLT) did not occur—instead, the two were
          performed two months apart;

      •   sleep logs were not obtained for the week before the MSLT;

      •   a urine drug screening (for medications that might impact sleep) was not performed; and

      •   the sleep apnea diagnosis Petitioner had previously obtained provided an alternative
          explanation for daytime sleepiness that undercut the MSLT findings.

Id. at 6–7. Thus, he disputed that the MSLT test, coupled with other exam and testing results
considered by Ms.      E.S.’s treaters, in fact supported the narcolepsy diagnosis she received.

       Moreover, assuming the diagnosis was substantively supported, Dr. Raizen pointed out
(consistent with Dr. MacGinnitie) that the distinction between types 1 and 2 narcolepsy was harmful
to Petitioner’s causation theory. He noted that there was “essentially no evidence for autoimmunity
in the pathogenesis of type 2 narcolepsy,” and therefore, what was believed plausible about the
pathogenesis of type 1 narcolepsy had no relevance in explaining Petitioner’s case. First Raizen
Rep. at 7, 8. And (referencing Arnheim-Dahlstrom) he denied that reliable evidence connecting the
HPV vaccine to any form of narcolepsy existed, noting that “the ratio of narcolepsy incidence
between those vaccinated and those unvaccinated has a mean that is less (and not more) than 1.” Id.

                                                37
 at 8 (emphasis in original); Arnheim-Dahlstrom at 5. 60

                           b. Raizen Second Report

       Dr. Raizen’s second report focused on Ms.            E.S.’s chronic fatigue diagnosis and its
purported causal association with the HPV vaccine. He observed that the diagnosis (which came
from Dr. Levine’s treatment of Ms. E.S.          in 2018) often featured “unrefreshing sleep” as a
symptom. Second Raizen Rep. at 1–2. But he disputed that there was any overlap between this feature
of chronic fatigue and narcolepsy, noting that those diagnosed with the latter often reported feeling
refreshed after the instances in which they slept normally, with ever-present sleepiness more the
problem they faced. Id. at 2; C. Baumann et al., Challenges in Diagnosing Narcolepsy without
Cataplexy: A Consensus Statement, 37 Sleep 1035–42 (2014), filed July 27, 2018 as Ex. E, Tab 12
(ECF No. 73-3). As a result, he rejected the contention that chronic fatigue sleep-related symptoms
would corroborate a narcolepsy diagnosis (and in fact maintained that Dr. Levine’s findings further
undercut the accuracy of Petitioner’s earlier narcolepsy diagnosis). Id. at 2.

        Dr. Raizen otherwise (consistent with his arguments about the narcolepsy-HPV vaccine
causal relationship) contested Petitioner’s allegations that the HPV vaccine was associated with
chronic fatigue. He noted that science still did not fully understand the pathogenesis of chronic
fatigue. Second Raizen Rep. at 5. As a result, he rejected Petitioner’s argument that it was more likely
than not an autoimmune condition. In addition, he noted that reliable studies from Europe did not
observe an association between the HPV vaccine and an increased risk of chronic fatigue. Id; B.
Feiring et al., HPV Vaccination and Risk of Chronic Fatigue Syndrome/Myalgic Encephalomyelitis:
A Nationwide Register-Based Study from Norway, 35 Vaccine 4203–12 (2017), filed May 7, 2019
as Ex. I, Tab 5 (ECF No. 97-6); K. Donegan et al., Bivalent Human Papillomavirus Vaccine and the
Risk of Fatigue Syndromes in Girls in the UK, 31 Vaccine 4961–67 (2013), filed May 7, 2019 as Ex.
I, Tab 6 (ECF No. 97-7).

                  4.       Dr. Christopher Gibbons

        Dr. Gibbons, a board-certified neurologist with specific expertise in both diabetes and small
 fiber neuropathies, prepared a single report. Report, dated May 3, 2019, filed as Ex. J (ECF No. 98-
 1) (“Gibbons Rep.”). In it, he set forth his dim view of Dr. Steinman’s contention that Ms.    E.S.’s
 purported small fiber neuropathy was caused by the HPV vaccine.

         Dr. Gibbons is an Associate Professor of Neurology at Harvard Medical School. Gibbons

60
   In his second report, Dr. Raizen revisited Arnheim-Dahlstrom in light of arguments Dr. Steinman had made about his
interpretation of its findings (in particular criticisms he leveled at how the raw data was adjusted). Second Steinman Rep.
at 21–22. Dr. Raizen admitted his lack of expertise in statistics or epidemiology (which Dr. Steinman shares), but deemed
the adjusted figures (which he placed more faith in) to be common in reliable epidemiologic studies, and otherwise argued
the results that supported his contentions were scientifically reasonable. Second Raizen Rep. at 3–4.
                                                            38
     Rep. at 1. He completed neurological training at Johns Hopkins Hospital and subspecialty training
     in Clinical Neurophysiology at Harvard Medical School and Beth Israel Deaconess Medical Center.
     Id. Dr. Gibbons has previously served as the Chair of the Autonomic Section of the American
     Academy of Neurology and Chair of the Clinical Affairs Committee of the American Autonomic
     Society. Id. He is currently the Director of the Beth Israel Deaconess Medical Center
     Neurocutaneous Laboratory—the diagnostic laboratory for small fiber neuropathy—and has treated
     thousands of patients with small fiber neuropathy and reviewed tens of thousands of skin biopsy
     slides for evaluation of small fiber neuropathy. Id. at 2. Of particular note, Dr. Gibbons reports that
     he personally published the “seminal articles” on both small fiber neuropathy as well as the use of
     skin biopsies as a diagnostic tool, and that he has over the years treated thousands of individuals
     suffering from small fiber neuropathy. Id. at 1–2; C. Gibbons et al., Quantification of Sudomotor
     Innervation: a Comparison of Three Methods, 42 Muscle Nerve 112–119 (2009), filed May 7, 2019
     as Ex. J, Tab 4 (ECF No. 98-5); C. Gibbons, et al., Quantification of Sweat Gland Innervation: a
     Clinical-Pathologic Correlation, 72 Neurology 1479–86 (2009), filed May 7, 2019 as Ex. J, Tab 5
     (ECF No. 98-6).

            Like the other experts before him, Dr. Gibbons initiated his report with an overview of
     Petitioner’s medical history, noting in particular that (a) Ms. E.S.    had struggled controlling her
     diabetes, and (b) her small fiber neuropathy diagnosis came from the time period when she began
     seeing Dr. Chin in September 2018 (three-plus years after the last vaccinations at issue) and was
     based on two skin biopsies performed at that time. Gibbons Rep. at 3; Ex. 48. He challenged the
     diagnosis, arguing (despite the fact that the test results themselves were in the abnormal range (Ex.
     48 at 2)) that the underlying records for the actual results had not been provided, making it
     impossible for him to evaluate the accuracy of the diagnosis in light of the proper reading of the
     results. Gibbons Rep. at 4.

            More so, Dr. Gibbons maintained that Petitioner had received normal neurologic exams from
     2016 until her visits with Dr. Chin, that there was no filed record establishing follow-up with Dr.
     Chin that would confirm the accuracy of the diagnosis, and that overall the record lacked sufficient
     clinical proof to corroborate the small fiber neuropathy diagnosis. Gibbons Rep. at 5. In addition,
     Dr. Gibbons maintained that the diagnosis could not be based solely on biopsy results, which could
     constitute a false positive. Id.; B. Callaghan et al., Better Diagnostic Accuracy of Neuropathy in
     Obesity: A New Challenge for Neurologists, 129 Clinical Neurophysiology: Official J. of the Int’l
     Federation of Clinical Neurophysiology 654–62 (2018), filed May 7, 2019 as Ex. J, Tab 5 (ECF
     No. 98-6).

            Dr. Gibbons highlighted the significance of Petitioner’s preexisting type 1 diabetes.
     Neuropathies are well-known to be highly associated with diabetes (as well as other risk factors
     Petitioner possessed, such as an elevated body mass index and hypercholesterolemia 61). Gibbons

61
     Hypercholesterolemia is excessive cholesterol in the blood. Dorland’s at 876.
                                                            39
     Rep. at 6. Indeed, the association between diabetes and any form of neuropathy was far better
     established by medical science than a link to the HPV vaccine. Id. Dr. Gibbons therefore opined
     that assuming the small fiver neuropathy diagnosis was correct, it was still far more likely that it
     was explained by her diabetes than her receipt of the HPV vaccine. Id.

            Regarding Petitioner’s causal theory, Dr. Gibbons rejected the contention that the HPV
     vaccine was associated with small fiber neuropathy. He noted that (based on his own research) there
     were exceedingly few publicly available articles involving the topic, no research evaluating how
     the vaccine would cause such a form of neuropathy, and no case reports. Gibbons Rep. at 4. At
     most, Petitioner had referenced “a case series from Japan with an enormous array of symptoms”
     from a pool of individuals who received the vaccine. T. Kinoshita et al., Peripheral Sympathetic
     Nerve Dysfunction in Adolescent Japanese Girls Following Immunization with the Human
     Papillomavirus Vaccine, 53 Internal Med. 2185–2200 (2014), filed May 7, 2019 as Ex. J, Tab 1
     (ECF No. 98-2) (“Kinoshita”). But, Dr. Gibbons opined that Kinoshita may not even have identified
     actual incidents of small fiber neuropathy (conflating them with biopsy evidence of purported
     “nerve” damage that in his reading was merely proof of damage to nerve myelin), adding that its
     findings otherwise had been cast in doubt. Id.; S. Hanley et al., Peripheral Sympathetic Nerve
     Dysfunction in Adolescent Japanese Girls Following Immunization with the Human Papillomavirus
     Vaccine, 54 Internal Med. 1953 (2015), filed May 7, 2019 as Ex. J, Tab 2 (ECF No. 98-3) (letter
     criticizing Kinoshita as not “demonstrat[ing] any relationship between vaccination and adverse
     events, which are [in Kinoshita] poorly-defined and include an eclectic range of symptoms”).

           Dr. Gibbons also proposed that the reasonableness of the timeframe in which Petitioner’s
     onset occurred had not been established. The earliest evidence of a diagnosis of small fiber
     neuropathy was from 2018—three years after the last HPV dose Petitioner received. Moreover (and
     contrary to the history provided to Dr. Chin), the record for the intervening period of 2015 to 2018
     showed numerous instances in which Ms. E.S.          received normal neurologic exams. As a result,
     the period from last HPV dose to when Dr. Gibbons speculated Petitioner might have developed a
     small fiber neuropathy was too lengthy to be medically acceptable. Gibbons Rep. at 6–7.

           C.      Other Scientific or Medical Evidence Pertaining to Petitioner’s Case

           Petitioner filed some additional items of literature (15 in all) in the course of briefing
     Respondent’s dismissal motion. Only a small few, however, plowed new ground, and therefore
     merit discussion.62 One such article was only published in the late summer of 2019, and purports to

62
   Illustrative of the misguided, “more heat than light” nature of Petitioner’s overall showing in this case, the Sur-Reply
was filed with seven additional items of literature—most of which could have been offered far earlier in the matter’s life,
since all but one were published before 2018, and did not otherwise reflect new scientific findings. One of the newly-
filed items, Exhibit 117, was a nearly nine-hundred-page excerpt from the Institute of Medicine’s treatise Adverse Effects
of Vaccines: Evidence and Causality—essentially the entirety of the work. The filing of whole texts into the record of a
Vaccine Act case is not a practice reflective of careful lawyering aimed at persuading the special master through focused
reference to helpful evidence.
                                                            40
     support Petitioner’s contentions about the autoimmune character of POTS. See, e.g., W. Gunning
     et al., Postural Orthostatic Tachycardia Syndrome is Associated with Elevated G-Protein Coupled
     Receptor Autoantibodies, 8 J. Am. Heart Assoc. 1–10 (2019), filed Nov. 24, 2019 as Ex. 109 (ECF
     No. 107-1) (“Gunning”). Gunning observed the presence of elevated G-protein coupled adrenergic
     autoantibodies or muscarinic autoantibodies in the majority of a group of 55 patients. Gunning at
     5–6. However, its authors conceded that the significance of its findings remained “unknown” (Id.
     at 7), and although Gunning purported that an association between vaccination and POTS was
     “well-documented,” it based this proposition on articles written by some of the same individuals
     that have been found unpersuasive in past cases. Id. at 8 fn. 47–50 (citing an article written by Dr.
     Shoenfeld). 63 Gunning otherwise is not strong evidence for the conclusion that all cases of POTS
     are autoimmune in origin or nature—let alone a subset.

            Respondent similarly filed some additional articles bearing on the resolution of the case. First,
     he filed a 2019 statement from the American Autonomic Society (the “AAS”), written by certain
     individuals deemed leaders in the field, 64 finding specifically that “there are no data [at this time]
     to support a causal relationship between HPV vaccination and CRPS, chronic fatigue, and [POTS]
     to other forms of dysautonomia.” A. Barboi et al., Human Papillomavirus (HPV) Vaccine and
     Autonomic Disorders: A Position Statement from the American Autonomic Society, Clinical
     Autonomic Res. 1, 1–6 (2019), filed Feb. 4, 2020 as Ex. M (ECF No. 115-2) (the “AAS Statement”),
     at 1. The AAS Statement references L. Brinth et al., Orthostatic Intolerance and postural
     tachycardia syndrome as suspected adverse effects of vaccination against human papilloma virus,
     33 Vaccine 2602–05 (“Brinth”).

            Second, Respondent filed a response to the AAS Statement written by a medical expert whose
     work has been favorably cited by Petitioner in this case as supportive of the relationship between
     the HPV vaccine and POTS. S. Blitshteyn, Human Papillomavirus (HPV) Vaccine Safety
     Concerning POTS, CRPS and Related Conditions, Clinical Autonomic Res. (2019), filed Feb. 4,
     2020 as Ex. N (ECF No. 115-3) (“Blitshteyn”). Dr. Blitshteyn’s article proposes that vaccine-
     triggered, immune-mediated autonomic dysfunction could possibly lead to the development of de
     novo post-HPV vaccination syndrome in genetically susceptible individuals. Blitshetyn, et al.,
     Autonomic dysfunction and HPV immunization: an overview, Immunologic Res., filed as Ex. 96 on
     January 15, 2019 (ECF No. 88-1). But in her letter, (and while maintaining that the concept of
     dysautonomia induced by the HPV vaccine should be taken seriously and be made the subject of

63
  Once again, reference is made to an article on the propensity of vaccination to cause autoimmune disease written by
Dr. Shoenfeld—the same expert who (a) came up with the discredited ASIA theory discussed in footnote 56 above, and
(b) has repeatedly, but unpersuasively, testified that the HPV vaccine can cause POTS and other purportedly autoimmune
conditions. See Gunning at 8.
64
  The AAS Statement’s 22 authors include one of Respondent’s experts, Dr. Gibbons, as well as Dr. Philip Low, a
nationally-recognized expert on the autonomic nervous system who has testified previously in the Program for
Respondent in cases involving POTS as a claimed vaccine injury. See, e.g. Yalacki, 2019 WL 1061429, at *18.
                                                         41
 further research), Dr. Blitshteyn acknowledged the accuracy of the AAS’s conclusions. Blitshteyn
 Letter at 1 (noting that Dr. Blitshteyn “agree[s] with [the AAS’s] conclusion that given the existing
 evidence to date, a causal relationship has not been supported”) (the “Blitshteyn Letter”).

       Finally, Respondent offered a 2018 statistical analysis from Japan (source of articles like
 Ozawa and Kinoshita) of approximately 30,000 female recipients of the HPV vaccine and 24 kinds
 of post-vaccination symptoms commonly reported in studies claiming an association between the
 vaccine and the kinds of injuries claimed in this case. S. Suzuki et al., No Association Between HPV
 Vaccine and Reported Post-Vaccination Symptoms in Japanese Young Women: Results of the
 Nagoya Study, 5 Papillomavirus Res. 96–103 (2018), filed Feb. 4, 2020 as Ex. L (ECF No. 115-1)
 (“Suzuki”). The sample group in Suzuki is far larger than the number of individuals considered in
 Ozawa, Kinoshita, or even Brinth. Suzuki’s authors only noted statistically relevant increases in
 complaints of headache or hospitalization due to menstrual bleeding, but not the kind of symptoms
 that might be deemed autonomic in character (e.g., fatigue, dizziness, weakness, brain fog, etc.).
 Suzuki at 98–100.

III.   Procedural History

      The Petition was initiated in April 2017. By September of that year, after the filing of medical
records and a substitution of counsel, Respondent filed his Rule 4(c) Report opposing an entitlement
award. ECF No. 27. For nearly two years thereafter, the parties filed back-and-forth expert reports
as discussed above. By May 2019, however, I had determined (given misgivings I had regarding
some aspects of the case) that certain elements of the matter might be amenable to disposition via
ruling on the record. To that end, I set up an initial schedule for briefing the matter. Docket Entry
Order, dated May 15, 2019. The parties completed briefing the matter with the filing of Petitioner’s
Sur-Reply in April 2020, and the matter is fully ripe for resolution.

IV.    Parties’ Respective Arguments

       Respondent’s Motion attacks both the adequacy of evidence establishing certain of
Petitioner’s claimed injuries, as well as her success in demonstrating that the HPV and/or flu
vaccines could cause them in the first place. He disputes that the record supports Petitioner’s claim
of chronic headaches, noting a lack of such a diagnosis (Mot. at 18), and also similarly contests that
the record establishes that Ms. E.S.     experienced myocardial ischemia. Mot. at 28–30. He also
maintains that Petitioner’s type 2 narcolepsy diagnosis was based on incomplete testing (Mot. at
33–34), adding that preponderant evidence does not establish that this form of narcolepsy (which
cannot be assumed to be autoimmune, in comparison to the first form) has not reliably been
associated with the HPV or flu vaccine. Id. at 34–36.

       In addition, Respondent similarly observes that Petitioner’s purported diagnoses for chronic
                                                 42
fatigue, small fiber neuropathy, and POTS were all obtained long after the vaccinations at issue
(calling into question how they could be reasonably associated with vaccines), and that the evidence
offered to support each either lacks corroboration in the record or reflects an incomplete
determination. Mot. at 37–42. And Respondent challenges Petitioner’s ability to show that her DM1
could be significantly aggravated by either relevant vaccine, arguing that (a) no Program decision
has ever held that diabetes can be caused or aggravated by any vaccine, (b) Petitioner’s course did
not necessarily reveal consistent worsening, but instead was characterized by numerous ups and
downs (as reflected in varying blood sugar testing results in the timeframe after vaccination), and
(c) Dr. Lee’s causation theory is not credible or reliable, and comes from an individual lacking the
expertise to so opine. Id. at 21–28.

       In reaction, Petitioner opposes dismissal, arguing instead that ample matters have been
presented warranting a hearing. She consistently takes note of the difference in her health overall
pre- versus post-vaccination. Opp. at 3–4, 5–6. After a lengthy review of her medical history, she
emphasizes the diagnostic support for autonomic-related injuries from Dr. Levine in 2018, followed
by Drs. Chin and Younger. Id. at 17–23. The narcolepsy diagnosis, she maintains, similarly finds
support in Dr. Kothare’s evaluation, and she proposes that the testing evidence (that she possesses
the autoantibodies that are key to her theory for how these injuries came about) is sound. Id. at 23–
24, 29. She makes a similar argument to vouch for the skin biopsy findings of small fiber
neuropathy, over the objections of Dr. Gibbons. Id. at 34. These injuries are all related and are in
Petitioner’s view bulwarked by reliable recent literature underscoring the significance of anti-
adrenergic antibodies in causing autonomic harm, such as Ikeda. Opp. at 27–28.

      Ms. E.S.      also maintains that her myocardial ischemia and DM1 significant aggravation
claims are supported by the record and reliable science and medical evidence, including the
testimony of Dr. Lee. To do so, she relies on inclusion of large block-quoted sections from Dr.
Lee’s reports. Opp. at 36–40. And as further support for her significant aggravation of diabetes
claim, Petitioner revisits again her argument that her health took a noticeable turn for the worse
post-vaccination, and emphasizes Dr. Lee’s assertion (logically questioned by Respondent’s
experts, as noted above) that there was a “25-fold increase” in the incidence of diabetes after
administration of the HPV vaccine. Id. at 40–42.

       Respondent filed a succinct reply. It emphasized my authority to resolve this matter without
a hearing, noting that none of the “new” articles or more recent treatment records Petitioner filed
established persuasive grounds for a hearing. Reply at 2–3. Respondent made specific comment
about the unpersuasive or unreliable character of articles filed in conjunction with the Opposition
Brief, like Kinoshita and Gunning, while highlighting his own newly-filed articles, such as the AAS
Statement or Suzuki. Id. at 4–5.

       Given the opportunity to offer a sur-reply, Petitioner prepared and filed a brief twice as long
as the Reply, but which largely repeated arguments already lodged in opposing Respondent’s initial
                                                43
     dismissal motion. Petitioner admitted that the evidence for a POTS diagnosis might not be
     preponderant (Sur-Reply at 3 (“Dr. Younger’s medical record and testing points in the direction of
     a POTS diagnosis”) (emphasis added)), but claimed the evidence suggestive of that diagnosis had
     to be considered in light of the other record evidence supportive of some kind of dysautonomia,
     which was likely related to Petitioner’s receipt of the HPV vaccine. Id. at 3–4. The “newly emerged”
     evidence associating the two marshaled in favor of a hearing. Id. at 4. She reiterated her arguments
     about a decline in health post-vaccination (Id. at 5–9). She also raised two somewhat new injury
     complaints that she had not emphasized before: (1) that she had showed “[s]ymptoms of ovarian
     failure” after vaccination—a condition she maintained is associated with the HPV vaccine; 65 and
     (2) that 2018 MRI results revealed a pituitary lesion that could be associated with HPV infection.
     Id. at 9–11.

 V.       Applicable Law

          A.      Petitioner’s Overall Burden in Vaccine Program Cases

        To receive compensation in the Vaccine Program, a petitioner must prove either: (1) that he
suffered a “Table Injury”—i.e., an injury falling within the Vaccine Injury Table—corresponding to
one of the vaccinations in question within a statutorily prescribed period of time or, in the alternative,
(2) that his illnesses were actually caused by a vaccine (a “Non-Table Injury”). See Sections
13(a)(1)(A), 11(c)(1), and 14(a), as amended by 42 C.F.R. § 100.3; § 11(c)(1)(C)(ii)(I); see also
Moberly v. Sec’y of Health & Hum. Servs., 592 F.3d 1315, 1321 (Fed. Cir. 2010); Capizzano v. Sec’y
of Health & Hum. Servs., 440 F.3d 1317, 1320 (Fed. Cir. 2006). 66 In this case, Petitioner does not
assert a Table claim.

        For both Table and Non-Table claims, Vaccine Program petitioners bear a “preponderance of
the evidence” burden of proof. Section 13(1)(a). That is, a petitioner must offer evidence that leads
the “trier of fact to believe that the existence of a fact is more probable than its nonexistence before
[he] may find in favor of the party who has the burden to persuade the judge of the fact’s existence.”
Moberly, 592 F.3d at 1322 n.2; see also Snowbank Enter. v. United States, 6 Cl. Ct. 476, 486 (1984)
(mere conjecture or speculation is insufficient under a preponderance standard). Proof of medical
certainty is not required. Bunting v. Sec’y of Health & Hum. Servs., 931 F.2d 867, 873 (Fed. Cir.
1991). In particular, a petitioner must demonstrate that the vaccine was “not only [the] but-for cause

65
   In fact, claims of post-HPV vaccine ovarian failure have been litigated several times in the Program—never to success.
See, e.g. Wright v. Sec. of Health & Hum. Servs., No. 15-851V, 2017 WL 8218937 (Fed. Cl. Spec. Mstr. Dec. 28, 2017);
Culligan v. Sec. of Health & Hum. Servs., No. 14-318V, 2016 WL 3101981 (Fed. Cl. Spec. Mstr. June 2, 2016); Laughlin
v. Sec. of Health & Hum. Servs., No. 13-289V, 2016 WL 3101977 (Fed. Cl. Spec. Mstr. June 2, 2016).

66
   Decisions of special masters (some of which I reference in this ruling) constitute persuasive but not binding authority.
Hanlon v. Sec’y of Health & Hum. Servs., 40 Fed. Cl. 625, 630 (1998). By contrast, Federal Circuit rulings concerning
legal issues are binding on special masters. Guillory v. Sec’y of Health & Hum. Servs., 59 Fed. Cl. 121, 124 (2003), aff’d
104 F. Appx. 712 (Fed. Cir. 2004); see also Spooner v. Sec’y of Health & Hum. Servs., No. 13-159V, 2014 WL 504728,
at *7 n.12 (Fed. Cl. Spec. Mstr. Jan. 16, 2014).
                                                            44
of the injury but also a substantial factor in bringing about the injury.” Moberly, 592 F.3d at 1321
(quoting Shyface v. Sec’y of Health & Hum. Servs., 165 F.3d 1344, 1352–53 (Fed. Cir. 1999));
Pafford v. Sec’y of Health & Hum. Servs., 451 F.3d 1352, 1355 (Fed. Cir. 2006). A petitioner may
not receive a Vaccine Program award based solely on his assertions; rather, the petition must be
supported by either medical records or by the opinion of a competent physician. Section 13(a)(1).

        In attempting to establish entitlement to a Vaccine Program award of compensation for a
Non-Table claim, a petitioner must satisfy all three of the elements established by the Federal Circuit
in Althen v. Sec’y of Health & Hum. Servs, 418 F.3d 1274, 1278 (Fed. Cir. 2005): “(1) a medical
theory causally connecting the vaccination and the injury; (2) a logical sequence of cause and effect
showing that the vaccination was the reason for the injury; and (3) a showing of proximate temporal
relationship between vaccination and injury.”

        Each of the Althen prongs requires a different showing. Under Althen prong one, petitioners
must provide a “reputable medical theory,” demonstrating that the vaccine received can cause the
type of injury alleged. Pafford, 451 F.3d at 1355–56 (citations omitted). To satisfy this prong, a
petitioner’s theory must be based on a “sound and reliable medical or scientific explanation.”
Knudsen v. Sec’y of Health & Hum. Servs., 35 F.3d 543, 548 (Fed. Cir. 1994). Such a theory must
only be “legally probable, not medically or scientifically certain.” Id. at 549.

         Petitioners may satisfy the first Althen prong without resort to medical literature,
epidemiological studies, demonstration of a specific mechanism, or a generally accepted medical
theory. Andreu v. Sec’y of Health & Hum. Servs., 569 F.3d 1367, 1378–79 (Fed. Cir. 2009) (citing
Capizzano, 440 F.3d at 1325–26). Special masters, despite their expertise, are not empowered by
statute to conclusively resolve what are essentially thorny scientific and medical questions, and thus
scientific evidence offered to establish Althen prong one is viewed “not through the lens of the
laboratorian, but instead from the vantage point of the Vaccine Act’s preponderant evidence
standard.” Id. at 1380. Accordingly, special masters must take care not to increase the burden placed
on petitioners in offering a scientific theory linking vaccine to injury. Contreras, 121 Fed. Cl. at 245
(“[p]lausibility . . . in many cases may be enough to satisfy Althen prong one” (emphasis in original)).

        In discussing the evidentiary standard applicable to the first Althen prong, the Federal Circuit
has consistently rejected the contention that it can be satisfied merely by establishing the proposed
causal theory’s scientific or medical plausibility. See Boatmon v. Sec’y of Health & Hum. Servs., 941
F.3d 1351, 1359 (Fed. Cir. 2019); see also LaLonde v. Sec’y of Health & Hum. Servs., 746 F.3d 1334,
1339 (Fed. Cir. 2014) (“[h]owever, in the past we have made clear that simply identifying a
‘plausible’ theory of causation is insufficient for a petitioner to meet her burden of proof.” (citing
Moberly, 592 F.3d at 1322)). And petitioners always have the ultimate burden of establishing their
overall Vaccine Act claim with preponderant evidence. W.C. v. Sec’y of Health & Hum. Servs., 704
F.3d 1352, 1356 (Fed. Cir. 2013) (citations omitted); Tarsell v. United States, 133 Fed. Cl. 782, 793

                                                 45
(2017) (noting that Moberly “addresses the petitioner’s overall burden of proving causation-in-fact
under the Vaccine Act” by a preponderance standard).

        The second Althen prong requires proof of a logical sequence of cause and effect, usually
supported by facts derived from a petitioner’s medical records. Althen, 418 F.3d at 1278; Andreu,
569 F.3d at 1375–77; Capizzano, 440 F.3d at 1326; Grant v. Sec’y of Health & Hum. Servs., 956
F.2d 1144, 1148 (Fed. Cir. 1992). In establishing that a vaccine “did cause” injury, the opinions and
views of the injured party’s treating physicians are entitled to some weight. Andreu, 569 F.3d at 1367;
Capizzano, 440 F.3d at 1326 (“medical records and medical opinion testimony are favored in vaccine
cases, as treating physicians are likely to be in the best position to determine whether a ‘logical
sequence of cause and effect show[s] that the vaccination was the reason for the injury’”) (quoting
Althen, 418 F.3d at 1280). Medical records are generally viewed as particularly trustworthy evidence,
since they are created contemporaneously with the treatment of the patient. Cucuras v. Sec’y of
Health & Hum. Servs., 993 F.2d 1525, 1528 (Fed. Cir. 1993).

         Medical records and statements of a treating physician, however, do not per se bind the
special master to adopt the conclusions of such an individual, even if they must be considered and
carefully evaluated. Section 13(b)(1) (providing that “[a]ny such diagnosis, conclusion, judgment,
test result, report, or summary shall not be binding on the special master or court”); Snyder v. Sec’y
of Health & Hum. Servs., 88 Fed. Cl. 706, 746 n.67 (2009) (“there is nothing . . . that mandates that
the testimony of a treating physician is sacrosanct—that it must be accepted in its entirety and cannot
be rebutted”). As with expert testimony offered to establish a theory of causation, the opinions or
diagnoses of treating physicians are only as trustworthy as the reasonableness of their suppositions
or bases. The views of treating physicians should be weighed against other, contrary evidence also
present in the record—including conflicting opinions among such individuals. Hibbard v. Sec’y of
Health & Hum. Servs., 100 Fed. Cl. 742, 749 (2011) (not arbitrary or capricious for special master to
weigh competing treating physicians’ conclusions against each other), aff’d, 698 F.3d 1355 (Fed. Cir.
2012); Veryzer v. Sec’y of Dept. of Health & Hum. Servs., No. 06-522V, 2011 WL 1935813, at *17
(Fed. Cl. Spec. Mstr. Apr. 29, 2011), mot. for review denied, 100 Fed. Cl. 344, 356 (2011), aff’d
without opinion, 475 F. Appx. 765 (Fed. Cir. 2012).

        The third Althen prong requires establishing a “proximate temporal relationship” between the
vaccination and the injury alleged. Althen, 418 F.3d at 1281. That term has been equated to the phrase
“medically-acceptable temporal relationship.” Id. A petitioner must offer “preponderant proof that
the onset of symptoms occurred within a timeframe which, given the medical understanding of the
disorder’s etiology, it is medically acceptable to infer causation.” de Bazan v. Sec’y of Health & Hum.
Servs., 539 F.3d 1347, 1352 (Fed. Cir. 2008). The explanation for what is a medically acceptable
timeframe must align with the theory of how the relevant vaccine can cause an injury (Althen prong
one’s requirement). Id. at 1352; Shapiro v. Sec’y of Health & Hum. Servs., 101 Fed. Cl. 532, 542
(2011), recons. denied after remand, 105 Fed. Cl. 353 (2012), aff’d mem., 503 F. Appx. 952 (Fed.
Cir. 2013); Koehn v. Sec’y of Health & Hum. Servs., No. 11-355V, 2013 WL 3214877 (Fed. Cl. Spec.
                                                 46
Mstr. May 30, 2013), mot. for rev. denied (Fed. Cl. Dec. 3, 2013), aff’d, 773 F.3d 1239 (Fed. Cir.
2014).

       B.      Significant Aggravation Claims

        Besides arguing that the HPV and/or hepatitis A vaccines directly caused her injuries,
Petitioner’s experts have also allowed for the possibility that the vaccines significantly aggravated
her preexisting diabetes mellitus. Where a petitioner so alleges, the Althen test is expanded, and the
petitioner has additional evidentiary burdens to satisfy. See generally Loving v. Sec’y of Health &
Hum. Servs., 86 Fed. Cl. 135, 144 (2009). In Loving, the Court of Federal Claims combined the
Althen test with the test from Whitecotton v. Sec’y of Health & Hum. Services, 81 F.3d 1099, 1107
(Fed. Cir. 1996), which related to on-Table significant aggravation cases. The resultant “significant
aggravation” test has six components, which require establishing:

       (1) the person’s condition prior to administration of the vaccine, (2) the person’s current
       condition (or the condition following the vaccination if that is also pertinent), (3) whether
       the person’s current condition constitutes a “significant aggravation” of the person’s
       condition prior to vaccination, (4) a medical theory causally connecting such a
       significantly worsened condition to the vaccination, (5) a logical sequence of cause and
       effect showing that the vaccination was the reason for the significant aggravation, and (6)
       a showing of a proximate temporal relationship between the vaccination and the
       significant aggravation.

Loving, 86 Fed. Cl. at 144; see also W.C., 704 F.3d at 1357 (holding that “the Loving case provides
the correct framework for evaluating off-table significant aggravation claims”). In effect, the last
three prongs of the Loving test correspond to the three Althen prongs.

        In Sharpe v. Sec’y of Health & Hum. Servs., 964 F.3d 1072 (Fed. Cir. 2020), the Federal
Circuit further elaborated on the Loving framework. Under prong (3) of the Loving test, the Petitioner
need not demonstrate an expected outcome, but merely that her current-post vaccination condition
was worse than pre-vaccination. Sharpe, 964 F.3d at 1081. And a claimant may make out a prima
facie case of significant aggravation overall without eliminating a preexisting condition as the cause
of her significantly aggravated injury (although the Circuit did not alter the ability of Respondent to
so prove in cases where the burden shifts). Id. at 1083.

       C.      Legal Standards Governing Factual Determinations

       The process for making determinations in Vaccine Program cases regarding factual issues
begins with consideration of the medical records. Section 11(c)(2). The special master is required to
consider “all [] relevant medical and scientific evidence contained in the record,” including “any
diagnosis, conclusion, medical judgment, or autopsy or coroner’s report which is contained in the
                                                  47
record regarding the nature, causation, and aggravation of the petitioner’s illness, disability, injury,
condition, or death,” as well as the “results of any diagnostic or evaluative test which are contained
in the record and the summaries and conclusions.” Section 13(b)(1)(A). The special master is then
required to weigh the evidence presented, including contemporaneous medical records and
testimony. See Burns v. Sec’y of Health & Hum. Servs., 3 F.3d 415, 417 (Fed. Cir. 1993) (it is within
the special master’s discretion to determine whether to afford greater weight to contemporaneous
medical records than to other evidence, such as oral testimony surrounding the events in question
that was given at a later date, provided that such determination is evidenced by a rational
determination).

         Medical records that are created contemporaneously with the events they describe are
presumed to be accurate and “complete” (i.e., presenting all relevant information on a patient’s health
problems). Cucuras, 993 F.2d at 1528; Doe/70 v. Sec’y of Health & Hum. Servs., 95 Fed. Cl. 598,
608 (2010) (“[g]iven the inconsistencies between petitioner’s testimony and his contemporaneous
medical records, the special master’s decision to rely on petitioner’s medical records was rational
and consistent with applicable law”), aff’d sub nom. Rickett v. Sec’y of Health & Hum. Servs., 468
F. Appx. 952 (Fed. Cir. 2011) (non-precedential opinion). This presumption is based on the linked
propositions that (i) sick people visit medical professionals; (ii) sick people honestly report their
health problems to those professionals; and (iii) medical professionals record what they are told or
observe when examining their patients in as accurate a manner as possible, so that they are aware of
enough relevant facts to make appropriate treatment decisions. Sanchez v. Sec’y of Health & Hum.
Servs., No. 11-685V, 2013 WL 1880825, at *2 (Fed. Cl. Spec. Mstr. Apr. 10, 2013); Cucuras v. Sec’y
of Health & Hum. Servs., 26 Cl. Ct. 537, 543 (1992), aff’d, 993 F.2d at 1525 (Fed. Cir. 1993) (“[i]t
strains reason to conclude that petitioners would fail to accurately report the onset of their daughter’s
symptoms”).

       Accordingly, if the medical records are clear, consistent, and complete, then they should be
afforded substantial weight. Lowrie, 2005 WL 6117475, at *20. Indeed, contemporaneous medical
records are generally found to be deserving of greater evidentiary weight than oral testimony—
especially where such testimony conflicts with the record evidence. Cucuras, 993 F.2d at 1528; see
also Murphy, 23 Cl. Ct. at 733 (citing United States v. United States Gypsum Co., 333 U.S. 364, 396
(1947) (“[i]t has generally been held that oral testimony which is in conflict with contemporaneous
documents is entitled to little evidentiary weight.”)).

        There are, however, situations in which compelling oral testimony may be more persuasive
than written records, such as where records are deemed to be incomplete or inaccurate. Campbell v.
Sec’y of Health & Hum. Servs., 69 Fed. Cl. 775, 779 (2006) (“like any norm based upon common
sense and experience, this rule should not be treated as an absolute and must yield where the factual
predicates for its application are weak or lacking”); Lowrie, 2005 WL 6117475, at *19 (“’[w]ritten
records which are, themselves, inconsistent, should be accorded less deference than those which are
internally consistent’”) (quoting Murphy, 23 Cl. Ct. at 733)). Ultimately, a determination regarding
                                                  48
 a witness’s credibility is needed when determining the weight that such testimony should be afforded.
 Andreu, 569 F.3d at 1379; Bradley v. Sec’y of Health & Hum. Servs., 991 F.2d 1570, 1575 (Fed. Cir.
 1993).

          When witness testimony is offered to overcome the presumption of accuracy afforded to
 contemporaneous medical records, such testimony must be “consistent, clear, cogent, and
 compelling.” Sanchez, 2013 WL 1880825, at *3 (citing Blutstein v. Sec’y of Health & Hum. Servs.,
 No. 90-2808V, 1998 WL 408611, at *5 (Fed. Cl. Spec. Mstr. June 30, 1998)). In determining the
 accuracy and completeness of medical records, the Court of Federal Claims has listed four possible
 explanations for inconsistencies between contemporaneously created medical records and later
 testimony: (1) a person’s failure to recount to the medical professional everything that happened
 during the relevant time period; (2) the medical professional’s failure to document everything
 reported to her or him; (3) a person’s faulty recollection of the events when presenting testimony; or
(4) a person’s purposeful recounting of symptoms that did not exist. Lalonde v. Sec’y of Health &
Hum. Servs., 110 Fed. Cl. 184, 203-04 (2013), aff’d, 746 F.3d 1334 (Fed. Cir. 2014). In making a
determination regarding whether to afford greater weight to contemporaneous medical records or
other evidence, such as testimony at hearing, there must be evidence that this decision was the result
of a rational determination. Burns, 3 F.3d at 417.

       D.      Analysis of Expert Testimony

        Establishing a sound and reliable medical theory often requires a petitioner to present expert
testimony in support of his claim. Lampe v. Sec’y of Health & Hum. Servs., 219 F.3d 1357, 1361
(Fed. Cir. 2000). Vaccine Program expert testimony is usually evaluated according to the factors for
analyzing scientific reliability set forth in Daubert v. Merrell Dow Pharmaceuticals, Inc., 509 U.S.
579, 594–96 (1993). See Cedillo v. Sec’y of Health & Hum. Servs., 617 F.3d 1328, 1339 (Fed. Cir.
2010) (citing Terran v. Sec’y of Health & Hum. Servs., 195 F.3d 1302, 1316 (Fed. Cir. 1999)). “The
Daubert factors for analyzing the reliability of testimony are: (1) whether a theory or technique can
be (and has been) tested; (2) whether the theory or technique has been subjected to peer review and
publication; (3) whether there is a known or potential rate of error and whether there are standards
for controlling the error; and (4) whether the theory or technique enjoys general acceptance within a
relevant scientific community.” Terran, 195 F.3d at 1316 n.2 (citing Daubert, 509 U.S. at 592–95).

        The Daubert factors play a slightly different role in Vaccine Program cases than they do when
applied in other federal judicial fora (such as the district courts). Daubert factors are usually
employed by judges (in the performance of their evidentiary gatekeeper roles) to exclude evidence
that is unreliable and/or could confuse a jury. In Vaccine Program cases, by contrast, these factors
are used in the weighing of the reliability of scientific evidence proffered. Davis v. Sec’y of Health
& Hum. Servs., 94 Fed. Cl. 53, 66–67 (2010) (“uniquely in this Circuit, the Daubert factors have
been employed also as an acceptable evidentiary-gauging tool with respect to persuasiveness of
expert testimony already admitted”). The flexible use of the Daubert factors to evaluate the
                                                 49
 persuasiveness and reliability of expert testimony has routinely been upheld. See, e.g., Snyder, 88
 Fed. Cl. at 742–45. In this matter (as in numerous other Vaccine Program cases), Daubert has not
 been employed at the threshold, to determine what evidence should be admitted, but instead to
 determine whether expert testimony offered is reliable and/or persuasive.

         Respondent frequently offers one or more experts of his own in order to rebut a petitioner’s
 case. Where both sides offer expert testimony, a special master’s decision may be “based on the
 credibility of the experts and the relative persuasiveness of their competing theories.” Broekelschen,
 618 F.3d at 1347 (citing Lampe, 219 F.3d at 1362). However, nothing requires the acceptance of an
 expert’s conclusion “connected to existing data only by the ipse dixit of the expert,” especially if
 “there is simply too great an analytical gap between the data and the opinion proffered.” Snyder, 88
 Fed. Cl. at 743 (quoting Gen. Elec. Co. v. Joiner, 522 U.S. 136, 146 (1997)); see also Isaac v. Sec’y
 of Health & Hum. Servs., No. 08-601V, 2012 WL 3609993, at *17 (Fed. Cl. Spec. Mstr. July 30,
 2012), mot. for rev. denied, 108 Fed. Cl. 743 (2013), aff’d, 540 F. Appx. 999 (Fed. Cir. 2013) (citing
 Cedillo, 617 F.3d at 1339). Weighing the relative persuasiveness of competing expert testimony,
 based on a particular expert’s credibility, is part of the overall reliability analysis to which special
 masters must subject expert testimony in Vaccine Program cases. Moberly, 592 F.3d at 1325–26
 (“[a]ssessments as to the reliability of expert testimony often turn on credibility determinations”);
 see also Porter v. Sec’y of Health & Hum. Servs., 663 F.3d 1242, 1250 (Fed. Cir. 2011) (“this court
 has unambiguously explained that special masters are expected to consider the credibility of expert
 witnesses in evaluating petitions for compensation under the Vaccine Act”).

         Expert opinions based on unsupported facts may be given relatively little weight. See
 Dobrydnev v. Sec’y of Health & Hum. Servs., 556 F. Appx. 976, 992–93 (Fed. Cir. 2014) (“[a]
 doctor’s conclusion is only as good as the facts upon which it is based”) (citing Brooke Group Ltd.
 v. Brown & Williamson Tobacco Corp., 509 U.S. 209, 242 (1993) (“[w]hen an expert assumes facts
 that are not supported by a preponderance of the evidence, a finder of fact may properly reject the
 expert’s opinion”)). Expert opinions that fail to address or are at odds with contemporaneous medical
 records may therefore be less persuasive than those which correspond to such records. See Gerami
v. Sec’y of Health & Hum. Servs., No. 12-442V, 2013 WL 5998109, at *4 (Fed. Cl. Spec. Mstr. Oct.
11, 2013), aff’d, 127 Fed. Cl. 299 (2014).

        E.      Consideration of Medical Literature

        Both parties filed medical and scientific literature in this case, but not every filed item factors
into the outcome of this decision. While I have reviewed all the medical literature submitted in this
case, I discuss only those articles that are most relevant to my determination and/or are central to
Petitioner’s case—just as I have not exhaustively discussed every individual medical record filed.
Moriarty v. Sec’y of Health & Hum. Servs., 844 F.3d 1322, 1328 (Fed. Cir. 2016) (“[w]e generally
presume that a special master considered the relevant record evidence even though he does not
explicitly reference such evidence in his decision”) (citation omitted); see also Paterek v. Sec’y of
                                                    50
Health & Hum. Servs., 527 F. Appx. 875, 884 (Fed. Cir. 2013) (“[f]inding certain information not
relevant does not lead to—and likely undermines—the conclusion that it was not considered”).

         F.       Consideration of Comparable Special Master Decisions

        In reaching a decision in this case, I have considered other decisions issued by special masters
(including my own) involving similar injuries, vaccines, or circumstances. I also reference some of
those cases in this Decision, in an effort to establish common themes, as well as demonstrate how
prior determinations impact my thinking on the present case.

        There is no error in doing so. It is certainly correct that prior decision in different cases do
not control the outcome herein. 67 Boatmon, 941 F.3d at 1358-59; Hanlon v. Sec’y of Health & Hum.
Servs., 40 Fed. Cl. 625, 630 (1998). Thus, the fact that another special master reasonably determined
elsewhere, on the basis of facts not in evidence in this case, that preponderant evidence supported the
conclusion that vaccine X caused petitioner’s injury Y does not compel me to reach the same
conclusion in this case. Different actions present different background medical histories, different
experts, and different items of medical literature, and therefore can reasonably result in contrary
determinations.

        However, it is equally the case that special masters draw upon their experience in resolving
Vaccine Act claims. Doe v. Sec’y of Health & Hum. Servs., 76 Fed. Cl. 328, 338-39 (2007) (“[o]ne
reason that proceedings are more expeditious in the hands of special masters is that the special
masters have the expertise and experience to know the type of information that is most probative of
a claim”) (emphasis added). They would therefore be remiss in ignoring prior cases presenting
similar theories or factual circumstances, along with the reasoning employed in reaching such
decisions. This is especially so given that special masters not only routinely hear from the same
experts in comparable cases but are also repeatedly offered the same items of medical literature
regarding certain common causation theories. It defies reason and logic to obligate special masters
to “reinvent the wheel”, so to speak, in each new case before them, paying no heed at all to how their
colleagues past and present have addressed similar causation theories or fact patterns. It is for this
reason that prior decisions can have high persuasive value—and why special masters often explain
how a new determination relates to such past decisions. 68 Even if the Federal Circuit does not require

67
   By contrast, Federal Circuit rulings concerning legal issues are binding on special masters. Guillory v. Sec’y of Health
& Hum. Servs., 59 Fed. Cl. 121, 124 (2003), aff’d 104 F. Appx. 712 (Fed. Cir. 2004); see also Spooner v. Sec’y of Health
& Hum. Servs., No. 13-159V, 2014 WL 504728, at *7 n.12 (Fed. Cl. Spec. Mstr. Jan. 16, 2014). Special masters are also
bound within a specific case by determinations made by judges of the Court of Federal Claims after a motion for review
is resolved.
68
  Consideration of prior determinations is a two-way street that does not only inure to the benefit of one party. Thus, I
would likely take into account the numerous decisions finding no association between vaccination and autism when
confronted with a new claim asserting autism as an injury, and I have informed such claimants early in the life of their
case that the claim was not viable for just that reason. But I would also deem a non-Table claim asserting GBS after
receipt of the flu vaccine as not requiring extensive proof on Althen prong one “can cause” matters, for the simple reason
that the Program has repeatedly litigated the issue in favor of petitioners.
                                                            51
special masters to distinguish other relevant cases (Boatmon, 941 F.3d at 1358), it is still wise to do
so.

       G.      Determining Matter on Record Rather Than at Hearing

         I have opted to decide this case based on written submissions and evidentiary filings,
 including the numerous expert reports that have been submitted. The Vaccine Act and Rules not
 only contemplate but encourage special masters to decide petitions (or components of a claim) on
 the papers rather than via evidentiary hearing, where (in the exercise of their discretion) they
 conclude that the former means of adjudication will properly and fairly resolve the case. Section
 12(d)(2)(D); Vaccine Rule 8(d). The Federal Circuit has recently affirmed this practice.
 Kreizenbeck v. Sec’y of Health & Hum. Servs., 945 F.3d 1362, 1365–66 (Fed. Cir. 2020). It simply
 is not the case that every Vaccine Act claim need be resolved by hearing—even where the petitioner
 explicitly so requests.

                                             ANALYSIS

 I.    Several of Petitioner’s Alleged Injuries Have Not Been Preponderantly Established

         As reasoned Program case law instructs, a petitioner’s vaccine injury claim is premised on
 first establishing the underlying existence of the claimed injury. The inability to establish an injury
 by preponderant evidence is fatal to the portion of a claim so dependent, since a vaccine could not
 have caused a non-existent injury. Broekelschen, 618 F.3d at 1346. It is also true in many cases that
 the claimant’s causation theory only pertains to a particular injury, and/or the one articulated in the
 case. As a result, it is often necessary at the outset of analyzing a vaccine injury claim to determine
 whether a given alleged injury has been preponderantly established.

        This case features a lengthy, ample medical record that strongly establishes that Petitioner
 (who unquestionably had preexisting type 1 diabetes that was not completely controlled in the time
 period prior to her first vaccination at issue) regularly sought medical treatment, often on an
 emergency basis, after her vaccinations in 2014 and 2015. However, other than complications
 attributable to her ongoing struggle with diabetes, the record does not preponderantly support some
 of the diagnoses that Petitioner purports to have received, and that she claims are the product of a
 vaccine injury. There is simply far less here than meets the eye, and certainly less proof of harm if
 petitioner-reported diagnoses (recounted to new treaters) contained in medical histories are ignored
 (as they rightfully should be).

       The injuries asserted by Petitioner that find insufficient support in the record, and therefore
 have not been preponderantly established, include the following:

                                                   52
        Myocardial Ischemia — the record does not preponderate whatsoever in support of the
conclusion that Ms. Hughes has myocardial ischemia, or any comparable heart condition. The
evidence supporting this diagnosis comes from a single encounter with a cardiologist in February
2016. Although there is some proof suggestive of a problem from the testing performed at that visit,
the treater in question (Dr. Lefkowitz) ultimately did not diagnose Petitioner consistent with what
she argues, as his follow-up visit with her a year later corroborates. See Ex. 18 at 14. Moreover, as
ably demonstrated by Dr. LaRue, the overall picture (when EKGs obtained before and after the
February 2016 visit are considered) does not reveal an actual cardiac problem. In contrast, Dr. Lee
(who has no specific cardiac expertise) has offered an opinion on this matter that (like the larger
problems his reports reflect, discussed below) is wholly unpersuasive. For this reason, I give no
further consideration to arguments that the HPV vaccine could cause this kind of injury—the injury
itself has not been proven preponderantly.

      Headache — there are intermittent references in the record to Ms. Hughes experiencing
headaches, whether migraine in nature or not. See, e.g., Ex. 9 at 3 (On October 2, 2014 Petitioner
was seen at student health center for uncontrollable high blood sugars and headache); Ex. 24 at 7
(On May 31, 2016, Petitioner was evaluated for headaches, neurological exam and brain MRI/MRA
were normal). However, the thrust of her complaints, beginning in the fall of 2014, relate to other
symptoms (abdominal pain in particular) that are distinguishable. There is also evidence of
headaches predating vaccination (see, e.g., Ex. 3 at 16), and no preponderant evidence that her
headache complaints became more frequent beginning in the fall of 2014.

       Headaches are simply not a consistent complaint herein—unlike other cases, where a
claimant squarely maintains that he or she incurred a persistent and debilitating course of headaches
due to the HPV vaccine. See B.A. v. Sec’y of Health & Hum. Servs., No. 11-51V, 2018WL 6985218
(Fed. Cl. Spec. Mstr. Dec. 6, 2018) (petitioner suffered from chronic (at least every few days)
headaches of gradual onset of 4-5 weeks within 9-10 days of vaccination). Thus, I do not find
chronic headaches to have been preponderantly established such that they could be an independent
basis for a finding of entitlement.

              Injuries Highlighted in Sur-Reply

       The claims of a pituitary injury or possible ovarian damage reflective of premature ovarian
failure were not squarely posed in this case any time before Petitioner’s Sur-Reply, but are no better
substantiated by the medical record than those she alleged earlier in the case’s existence. Petitioner
maintains that either could be associated with her overall decline in health post-vaccination. Sur-
Reply at 11; Ex. 121. But the former has not been demonstrated to be malign or a confirmed
pathologic finding, with MRI evidence from Dr. Chin’s evaluations in 2018 providing the primary
evidence for it. Petitioner has not otherwise explained the pathologic impact of this purported injury
(let alone how the HPV vaccine led to it). At most, she maintains that her “low cortisol levels” (Ex.
19 at 140) could be the product of pituitary failure—but no treaters seem to have embraced that
                                                53
diagnostic view, or characterized the lesion as harmful. And its temporal distance from even the
second dose of the vaccine in August 2015 make it highly improbable the lesion could be
attributable to vaccination. In any event, the record does not preponderantly support pituitary failure
as a cognizable injury in this case.

       The arguments about ovarian failure rely too much on incidents experienced by Ms. E.S.
involving ruptured cysts, and do not come close to the circumstances in other cases (cases which
did not result in entitlement findings) in which petitioners far more credibly established some form
of ovarian failure injury. See, e.g., Culligan v. Sec’y of Health & Hum. Servs., No. 14-318V, 2016
WL 3101981 (Fed. Cl. Spec. Mstr. June 2, 2016) (ovarian failure injury was characterized by
markedly irregular periods, following a year of regular periods; periods that occurred less frequently
than every 35 days; and heavier and longer periods, which may have lasted more than seven days);
Meylor v. Sec’y of Health & Hum. Servs., No. 10-770V, 2016 WL 3165774 (Fed. Cl. Spec. Mstr.
May 16, 2016) (ovarian failure injury was characterized by irregular periods that became more
irregular between first and second HPV vaccinations; sleep disturbances, including insomnia and
night sweats; and depression and joint pain). Moreover, the record establishes menses issues well
prior to the first vaccinations.

       Purported ovarian failure is also unpersuasively intertwined with claims of an active HPV
infection based on testing from Milford Molecular Diagnostics (Ex. 32 at 14), somehow interacting
with the observed adenoma. But if this is an actual cognizable injury, there is scant treater support
identifying it as such, let alone associating it with vaccination. Overall, these two late-alleged
injuries simply typify Petitioner’s overall effort to fashion her claim in the course of its adjudication,
adding new arguments to replace old as the latter show weakness, and simply trying to keep the
claim viable by looking for “new” injuries to allege as time passes.

       By contrast, other injuries alleged in the Petition have just enough evidence supporting their
existence to justify an Althen analysis (although some of them barely cross the preponderant line).
Petitioner has unquestionably struggled with diabetes complications throughout her post-
vaccination life, making it a reasonable injury for evaluation as part of a significant aggravation
claim (given the undisputed fact that she had been diagnosed with type I diabetes long before the
vaccinations at issue). Her claim of type 2 narcolepsy is also supported by some record proof.
Respondent’s experts raised reasonable objections to the overall validity of the testing that produced
the diagnosis, but there is sufficient support for it to evaluate if her diagnosed sleep problems were

                                                  54
     in fact vaccine-caused. In addition, diagnosis of chronic fatigue69 and small fiber neuropathy 70 both
     are bulwarked by recent testing results. Although Dr. Gibbons raised credible and persuasive
     reasons to doubt that the uncorroborated skin biopsy results were sufficient for the latter diagnosis,
     these two diagnoses have reliable evidence behind them for purposes of moving forward.

            The POTS injury, by contrast, is far less robustly supported by the record, and arguably
     should not be deemed to have been preponderantly established. It has never been corroborated by a
     true tilt table test (the gold standard for diagnosing POTS). 71 More significantly, Petitioner
     acknowledges that she has never even been diagnosed with POTS. Sur-Reply at 3. She maintains,
     however, that her POTS-like presentation is reflective of overall autonomic dysfunction, especially
     in light of her alleged chronic fatigue syndrome and small fiber neuropathy, all of which she
     considers part of the same vaccine response. Id. Thus, for sake of argument, and to give some credit
     to the “big picture” contention Petitioner advances with regard to her various autonomic-oriented
     symptoms, I will treat POTS as if it had been evidentiarily substantiated (although I expressly do
     not so rule), and will evaluate Petitioner’s subsequent success in preponderantly establishing that
     the HPV vaccine could cause it.

II.       Petitioner’s Various Causation Theories are Unreliable and/or not Preponderantly
          Supported by the Evidence

        Although I am considering a large number of alleged injuries (including several that arguably
lack preponderant support), I universally find that Petitioner has not in any instance established that
the HPV or flu vaccines “can cause” the relevant injury. (I consider separately whether these vaccines
could have aggravated type I diabetes below).

69
   Chronic fatigue syndrome is persistent debilitating fatigue lasting longer than 6 months, with other known medical
conditions having been ruled out by clinical diagnosis, accompanied by at least four of the following: significantly
impaired short-term memory or concentration, muscle weakness, pain in multiple joints without swelling or redness, sore
throat, tender lymph nodes, headaches, unrefreshing sleep, and malaise that lasts more than 24 hours following exertion.
Chronic           fatigue         syndrome,            Dorland’s           Medical          Dictionary          Online,
https://www.dorlandsonline.com/dorland/definition?id=110414 (last visited Oct. 28, 2020). The cause is unknown and
may be multifactorial; immune dysfunction has been suggested, and viral infection may be associated with it, although
no causal relationship has been demonstrated. Id.
70
   Small fiber neuropathy is a type of neuropathy in which only the small sensory cutaneous nerves are affected. Small
fiber             neuropathy,               Dorland’s             Medical               Dictionary             Online,
https://www.dorlandsonline.com/dorland/definition?id=137479&searchterm=small+fiber+neuropathy (last visited Oct.
28, 2020). The majority of patients experience sensory disturbances that start in the feet and progress upwards. John
Hopkins       Medicine,      Neurology       and      Neurosurgery,     Small      Fiber      Sensory     Neuropathy,
https://www.hopkinsmedicine.org/neurology_neurosurgery/centers_clinics/peripheral_nerve/conditions/small_fiber_se
nsory_neuropathy.html (last visited Oct. 28, 2020).
71
   The standard tilt table test entails the patient remaining in a supine position for twenty minutes, followed by ten minutes
tilted upright, and that the heart rate and blood pressure should be measured minute by minute. Yalacki, 2019 WL
1061429, at *40, n.10.

                                                             55
          A.        POTS

          POTS is a circulation disorder characterized by a group of symptoms (not including
 hypotension) that sometimes occur when a person assumes an upright position, including tachycardia,
 tremulousness, lightheadedness, sweating, and hyperventilation. Postural orthostatic tachycardia
 syndrome,                   Dorland’s              Medical              Dictionary               Online,
 https://www.dorlandsonline.com/dorland/definition?id=111236 (last visited Oct. 26, 2020). POTS is
 seen more often in women than in men, and its etiology remains uncertain. Id. It implicates the
 function of the autonomic nervous system, since it involves involuntary physical processes like heart
 rate. A tilt table test is often used to diagnose POTS. John Hopkins Medicine, Health Conditions and
 Diseases,            Postural         Orthostatic       Tachycardia          Syndrome          (POTS),
 https://www.hopkinsmedicine.org/health/conditions-and-diseases/postural-orthostatic-tachycardia-
 syndrome-pots (last visited Oct. 26, 2020). 72 Treaters may diagnose a patient with POTS if all three
 of these criteria are met: (i) abnormal heart rate response to being upright; (ii) symptoms that worsen
 when upright; and (iii) orthostatic hypotension (i.e. a drop in blood pressure) does not develop in the
 first three minutes of testing. Id.

         This is not the first case in which a claimant before me has alleged that POTS was vaccine-
 caused (and usually by the HPV vaccine). But I have never so found. See e.g., McKown v. Sec’y of
 Health & Hum. Servs., No. 15-1451V, 2019 WL 4072113 (Fed. Cl. Spec. Mstr. July 15, 2019); Combs
 v. Sec’y of Health & Hum. Servs., No. 14-878V, 2018 WL 1581672 (Fed. Cl. Spec. Mstr. Feb. 15,
 2018); see also Otto v. Sec’y of Health & Hum. Servs., No. 16-1144V, 2020 WL 4719285 (Fed. Cl.
 Spec. Mstr. June 17, 2020) (case dismissed after hearing on claimant’s request).

         In deciding these prior claims, I have generally noted that POTS is most commonly not
 considered attributable to an autoimmune process interfering with the autonomic nervous system.
 Rather, it is thought to reflect the autonomic system functioning properly in response to stressors (for
 example, hypovolemia, in which a person’s dehydrated states produces orthostatic imbalance). See,
 e.g., McKown, 2019 WL 4072113, at *52. Thus, POTS can occur in the context of a functioning
 autonomic nervous system. Moreover, while it is true that some evidence has emerged in the last ten
 years that in rare cases POTS might sometimes be attributable to an autoimmune process involving
 anti-adrenergic antibodies (which can cause heart rate increases), this is the exception to the rule—
 and to date, not nearly enough is known about how this process works or what would initiate it, to
 draw conclusions in Program cases sufficient to meet the preponderance level of evidence.73 Further,

72
  During the test, the patient is secured on a table while lying flat. Id. The table is then raised to an almost upright
position. Id. The patient’s heart rate, blood pressure, and often blood oxygen and exhaled carbon dioxide levels are
measured during this test. Id.

73
  Another case I decided (although not involving the HPV vaccine specifically) is instructive on this point. See Yalacki,
2019 WL 1061429, at *18. In Yalacki, Dr. Philip Low (a world-renowned expert on the autonomic nervous system)
testifying on Respondent’s behalf, noted that he previously believed that a different kind of autoantibody might be
important in POTS (although in only 10 percent of cases). Id. However, subsequent research disproved any correlation
                                                           56
 in none of these cases was it preponderantly established, through citation to reliable scientific
 evidence or expert testimony, that the HPV vaccine could cause the production of anti-adrenergic
 autoantibodies posited to cause POTS in some limited circumstances. 74

         Against this backdrop, nothing offered in this case by Petitioner or her experts provides more
 recent or more reliable evidence supporting the conclusion that the HPV vaccine might cause POTS
 (or any associated autonomic-associated symptoms for that matter). Dr. Steinman, for example,
 makes the same literal arguments about theoretical homology between components of the HPV
 vaccine and muscarinic receptors that are always presented in such cases—but with insufficient
 reliable corroborative proof supporting the conclusion that the homology is meaningful from a
 pathogenic sense. Establishing the existence of potential homology based on internet-driven research
 performed solely for this case is not enough to meet the preponderant burden of establishing it more
 likely than not that the vaccine would cross-react as proposed. Sullivan v. Sec’y of Health & Hum.
 Servs., No. 10-398V, 2015 WL 1404957, at *17–18, n. 30 (Fed. Cl. Spec. Mstr. Feb. 13, 2015) (while
 the law does not require Petitioner to “prove” homology in a Program case, mere assertion that HPV
 strain shares sequences with human body such that molecular mimicry might occur resulting in injury
 was by itself insufficient to satisfy burden). Indeed, as Dr. MacGinnitie noted, homologies are easily
 demonstrated to exist in nature, but they do not always establish the likelihood of concurrent cross-
 reactivity. First MacGinnitie Rep. at 4. Petitioner’s experts also purport to show an HPV relationship
 to POTS and autonomic dysfunction generally by relying on the same items of literature I have
 reviewed numerous times in the past but found wanting. Ozawa; Kinoshita; Johnson, 2018 WL
 2051760, at *24.

         Arguments about the autoimmune character of POTS, or the possibility that the HPV Vaccine
 could encourage the production of autoantibodies thought to be POTS-associated, were also
 unreliably established. Articles like Ikeda simply demonstrated that a group of individuals possessed
 the proposed autonomic system-impacting autoantibodies after vaccination, not that they were
 caused by it (and Ikeda did not even establish the autoantibodies were likely pathogenic). By contrast,
 other recent articles undermine Petitioner’s arguments about the significance of these autoantibodies,
 (some of which were even offered by her own experts). See, e.g., Loebel at 38. At the same time,
 other evidence established a consensus in the relevant medical community that the vaccine is not
 associated with autonomic injury or interference, or that the kinds of injuries alleged herein have not
 been convincingly associated with the vaccine from an epidemiologic standpoint. See Suzuki at 1;

to POTS. Id. Today, Dr. Low does not routinely test POTS patients for particular autoantibodies, “because we have not
been able to demonstrate any causative antibody.” Id.

74
  In Yalacki, the petitioner’s experts proposed that an “adrenergic antibody,” presumably produced in response to the
hepatitis B vaccine, was the most likely mechanistic causal element in triggering Petitioner’s POTS. Yalacki, 2019 WL
1061429 at *20. However, the literature offered to support this contention did not involve an actual measurement of the
antibody in questions in humans. Id. While the petitioner was able to offer some reliable literature exploring the
possibility that some cases of POTS might be autoimmune-mediated, Petitioner acknowledged that more recent research
moved away from autoimmunity as the most likely explanation for POTS, in the majority of individuals. Id. at *31.
                                                          57
 AAS Statement at 1. Large, reliable epidemiologic studies further undermine this conclusion. And it
 remains true that the majority of cases of POTS are likely not mediated by an autoimmune process—
 and that rare subset that might be would not likely occur months to years after the purported
 instigating event, such as of receipt of a vaccine. All of the above precludes me from determining
 that the HPV vaccine likely can cause POTS.

          B.       Narcolepsy

         Several years ago, I wrote a lengthy decision evaluating the claim that the unadjuvanted flu
 vaccine could cause narcolepsy. D’Toile v. Sec’y of Health & Hum. Servs., No. 15-085V, 2016 WL
 7664475 (Fed. Cl. Spec. Mstr. Nov. 28, 2016) mot. for review den’d, 132 Fed. Cl. 421 (2017), aff’d,
 726 F. App’x 809 (Fed. Cir. 2018). I denied entitlement (in a case featuring Dr. Steinman as the
 petitioner’s primary expert), finding that although there was reliable and persuasive evidence that a
 different form of the flu vaccine (one that was adjuvanted and administered only in Europe) had
 credibly been associated with narcolepsy, the same was not true of the version widely administered
 in the United States and received by the petitioner in question.

         Petitioner now tries to breathe new life into the same theory rejected in D’Toile—but with an
 overall weaker argument, supplemented by no new articles or evidence that might suggest a
 persuasive reason to revisit my prior rejection of the theory. She thus focuses on the HPV vaccine,75
 but without showing any literature akin to what was offered previously (and repeated in this case by
 Dr. Steinman). Worse, Petitioner’s diagnosed version of narcolepsy, type II, is even less considered
 autoimmune in nature than type I, which the literature filed discusses at length. See National Institute
 of Neurological Disorders and Stroke, Narcolepsy Fact Sheet, available at
 https://www.ninds.nih.gov/Disorders/Patient-Caregiver-Education/Fact-Sheets/Narcolepsy-Fact-
 Sheet (last visited Mar. 2, 2018), filed on Mar. 3, 2018 as Ex. 39, Ref. 6 at 2; Ex. 97. And Dr.
 Steinman’s fallback is to rely on homology arguments proposing theoretical bases for an autoimmune
 cross-reaction incited by the HPV vaccine that find no real-world basis in research. In short,
 Petitioner’s argument that the HPV vaccine can cause type II narcolepsy was woefully unsupported
 with reliable proof to be deemed a preponderant showing.

         C.       Chronic Fatigue Syndrome

       Petitioner is on slightly more firm ground in arguing that vaccination can cause chronic
 fatigue. However, claimants have not been routinely successful in so arguing. See, e.g., McCabe v.
 Sec’y of Health & Hum. Servs., No. 13-570V, 2018 WL 3029175 (Fed. Cl. Spec. Mstr. May 17,
 2018) (denying entitlement for CFS allegedly caused by influenza vaccinations); D’Angiolini v.

75
  Perhaps mindful of my prior decisions involving the flu vaccine and narcolepsy, Petitioner does not ask me to consider
again the same issue based on her receipt of the flu vaccine in 2015.

                                                          58
     Sec’y of Health & Hum. Servs., No. 99-5788V, 2014 WL 1678145 (Fed. Cl. Spec. Mstr. March 27,
     2014) (denying entitlement for adverse reaction, including CFS, allegedly caused by hepatitis B
     vaccination). I have also previously considered the issue but not found it preponderantly established.
     Yalacki v. Sec’y of Health & Hum. Servs., No. 14-278V, 2019 WL 1061429, at *38–39 (Fed. Cl.
     Spec. Mstr. Jan. 31, 2019), mot. for review den’d, 146 Fed. Cl. 80 (2019) (hepatitis B vaccine was
     not shown to be capable of causing CFS); Johnson v. Sec. of Health & Human Servs., No. 14-
     254V, 2018 WL 2051760 (Fed. Cl. Spec. Mstr. Mar. 23, 2018) (denying entitlement in case
     alleging CFS and POTS caused by HPV vaccination).

            Petitioner has not succeeded here where others have failed, largely for the same reasons that
     her POTS-related causal theory is unpersuasive. She simply cannot establish with reliable scientific
     evidence of any kind (expert testimony, articles, etc.) that there is a likely association between the
     HPV vaccine and chronic fatigue.76 Those articles or case studies she attempts to cite for this
     assertion do not reflect medically/scientifically reliable determinations, and are rebutted by larger-
     scale epidemiologic proof offered by Respondent, such as Chao.

            D. Small Fiber Neuropathy

            Dr. Gibbons (unquestionably the expert in this case most qualified to comment on Petitioner’s
     small fiber neuropathy-based claim) raised reasonable points about the evidentiary strength of the
     diagnosis obtained when Petitioner saw Dr. Chin in 2018. But even if I assume for sake of argument
     that the small fiber neuropathy diagnosis has reliable/substantive medical support, the underlying
     claim that the HPV vaccine could cause small fiber neuropathy has itself not been reliably
     established.

            As already noted, merely showing via BLAST searches that some homology exists between
     amino acid sequences in the HPV vaccine components and nerve cells does not amount to a
     preponderant showing that the vaccine can produce antibodies that will cross-react against those
     cells. Moreover, it is far from certain that small fiber neuropathy is an autoimmune-driven
     condition 77, as noted in other decisions. See, e.g., Todd v. Sec’y of Health & Hum. Servs., No. 15-

76
   At the same time, this set of symptoms could also be associated with Petitioner’s diabetes. Fatigue is a common
symptom in several medical conditions, including diabetes. Mayo Clinic, Chronic fatigue syndrome,
https://www.mayoclinic.org/diseases-conditions/chronic-fatigue-syndrome/diagnosis-treatment/drc-20360510         (last
visited Oct. 30, 2020). Some of signs and symptoms of type 1 diabetes are: extreme hunger, presence of ketones in the
urine, fatigue, and frequent infections. Mayo Clinic, Diabetes, https://www.mayoclinic.org/diseases-
conditions/diabetes/symptoms-causes/syc-20371444 (last visited Oct. 30, 2020).
77
   It should also be noted that small fiber neuropathy is a type of nerve damage that can occur as a result of uncontrolled
diabetes.     Mayo      Clinic,    Diabetic     Neuropathy,      https://www.mayoclinic.org/diseases-conditions/diabetic-
neuropathy/symptoms-causes/syc-20371580 (last visited Oct. 30, 2020). This nerve damage, sometimes called diabetic
neuropathy, is the result of high blood sugar and most often damages nerves in the legs and feet. Id. Depending on the
affected nerves, diabetic neuropathy symptoms can range from pain and numbness in your legs and feet to problems with
your digestive system, urinary tract, blood vessels, and heart. Id. This record is just as consistent with Petitioner’s small
fiber neuropathy being related to her diabetes as the result of vaccination, if not more so.
                                                             59
  860V, 2020 WL 727973 at *21 (Fed. Cl. Spec. Mstr. Jan. 8, 2020) (denying entitlement for SFN
  allegedly caused by flu vaccination; petitioner failed to establish the existence of systemic
  inflammation that would be associated with a chronic autoimmune neuropathy); LaPierre v. Sec’y
  of Health & Hum. Servs., No. 17-227V, 2019 WL 6490730 at *17 (Fed. Cl. Spec. Mstr. Oct. 18,
  2019) (finding that Petitioner’s non-specific symptoms were not a basis for entitlement despite
  possible overlap with known symptoms of other peripheral neuropathies). And evidence offered to
  suggest a case study-oriented association, like Kinoshita, is weak, dependent on self-selected patient
  populations rather than scientifically-reliable studies. Johnson, 2018 WL 2051760, at *9, 17.

III.   The Medical Record Does Not Support the Conclusion that Petitioner Experienced Any
       of her Allegedly Vaccine-Related Injuries in a Medically-Acceptable Timeframe

        For each claimed injury other than diabetes exacerbation, Petitioner asks that I find that her
onset was medically reasonable. In so doing, however, she frequently relies on diagnoses made long
after vaccination—between two and three years after, depending upon whether 2014 or 2015 are the
focus. Thus, she implicitly relies on the idea that she was experiencing an interrelated, autoimmune-
caused course of symptoms that began close in time to receipt of the HPV and flu vaccines (as
evidenced by her first hospital visits in October 2014 after beginning college), but which occasionally
blossomed into more self-evident.

        But for none of these injuries has Petitioner reliably demonstrated that the HPV or flu
vaccines could have produced the symptoms in a medically-acceptable timeframe. Her narcolepsy,
for example, was not diagnosed until 2016—and although she claims her sleep problems began in
the fall of 2014 (and hence a few months after receipt of the first HPV dose), the record does not
reveal any sleep-related complaint prior to seeing Dr. Kothare. In addition, some of the same
problems with her HPV-narcolepsy theory that plague her showing on the first Althen prong impact
this one as well. Thus, since the type of narcolepsy with which Petitioner was diagnosed is different
from the one that has been deemed autoimmune, scientific understanding about the process for
hypocretin path interference that might be consistent with a lengthy post-vaccination onset is not
automatically relevant herein. Dr. Steinman (the primary expert offering testimony for Petitioner on
this aspect of her claim) did not provide a reliable basis for concluding that type 2 narcolepsy could
be subclinical for so long before manifesting more overtly, even if difficulties in diagnosis are taken
into account. He simply assumed that any period “weeks to months” after vaccination is medically
acceptable.

        The timeframes for Petitioner’s development of chronic fatigue and small fiber neuropathy
are even more problematic. Both were diagnosed no less than three years after receipt of the second
HPV vaccine (and even after this case had been filed), and the record does not contain consistent
evidence of complaints by Petitioner (who certainly sought medical care on a regular basis
throughout) that might reflect incipient presentation of either injury, or that she was experiencing
these symptoms throughout. Indeed, although these conditions are neurologic (with the latter more
                                                  60
 specific to sensory nerves), Petitioner received normal neurologic workups in 2016-2018, before
 either diagnosis was ever considered. And Petitioner’s meta-explanation for her course—that the
 HPV vaccine was somehow initiative of a pathologic process featuring interference with the
 autonomic nervous system, the manifestations of which unfolded over time—is not backed up by
 reliable and persuasive expert testimony or any other form of reasonable proof (i.e. treater views,
 medical record evidence of persistent/common symptoms complaints, medical or scientific articles,
 etc.)

         Petitioner’s alleged nascent POTS is also temporally attenuated from the vaccination, without
 a showing that a vaccination even years before it could initiate a chronic process that would manifest
 as it purportedly did long after. This is especially true if the timeframe inquiry focuses on the
 existence of the anti-adrenergic antibodies that Petitioner alleges were causal. Petitioner was not
 apparently tested for these before the fall of 2016, obtaining the evidence that she possessed them in
 January 2017. Ex. 16 at 1; Second Steinman Rep. at 24–25. Because the shortest period from the
 time the testing occurred to the last relevant vaccination (August 2015) was over one year, how can
 Petitioner’s theory account for vaccine causality given that length of time? Could other factors have
 generated the autoantibodies in a period of time exceeding one year? And why has her POTS not yet
 fully manifested, such that the diagnosis could be made later? This was not the case even as of August
 2018 (when Dr. Levine raised the topic)—more than eighteen months after Petitioner received the
 positive test results. These are not quibbles—they are reasonable questions, and the inability of
 Petitioner to answer them with reliable and persuasive evidence compels a finding that the timeframe
 is simply too long to be medically acceptable.

         The lack of preponderant proof setting forth a medically-acceptable timeframe for injury due
 to vaccination is consistent with my overall impression of this case. Here, a person with severe and
 recurrent illnesses—illnesses most credibly associated with her preexisting diabetes—seeks to
 establish intervening vaccines as responsible for everything that came thereafter. That may have been
 enough of a basis for filing the claim—but a temporal association is unquestionably not enough for
 a finding of entitlement, or at a minimum for showing that the timeframe in which the (alleged)
 injuries occurred was medically acceptable. Petitioner simply has not demonstrated that all of these
 symptoms she experienced can be “tied together,” such that it is medically acceptable to conclude
 that conditions diagnosed years after vaccination are the end-result of pathologic processes she
 experienced in the lead time up to diagnosis. This is especially so given my finding (discussed below)
 that most of what Petitioner experienced far closer in time to the relevant vaccinations reflected her
 worsening diabetes—and the symptoms associated with that have not been shown to be vaccine-
 caused.

IV.    Petitioner’s Preexisting Diabetes Has Not Been Shown to have Been Exacerbated
       by Any Vaccines She Received

        Certain of Petitioner’s evidentiary showing obligations for a significant aggravation claim
                                                  61
     have readily been met. Thus, Ms. Hughes unquestionably was diabetic before her vaccinations
     (Loving prong one). Moreover, although her symptoms did plainly fluctuate over time (with her
     blood sugar levels inconsistently revealing the extent of her problem), 78 her overall health declined
     post-vaccination—satisfying the third Loving prong. 79 But she has not successfully shown that her
     DM1 could be worsened after receipt of the flu or HPV vaccines—or that in this case it likely was
     so worsened.

             First, I note that it has repeatedly been determined in Program cases that vaccination does
     not likely worsen DM1. See, e.g., Hennessey v. Sec’y of Health & Hum. Servs., No. 01-190V, 2009
     WL 1709053 (Fed. Cl. Spec. Mstr. May 29, 2009), mot. for review den’d, Fed. Cl. 126 (2010)
     (affirming the special master’s opinion including that the petitioner had “failed to establish any
     logical connection between his hepatitis B vaccinations and his T1D [type 1 diabetes]” and this his
     deteriorated condition was caused by “the natural progression of insulin dependence, rather than his
     vaccines”); Meyers v. Sec’y of Health & Hum. Servs., No. 04–1771V, 2006 WL 1593947 (Fed. Cl.
     Spec. Mstr. May 22, 2006) (petitioner failed to establish a causal link between DTP vaccine and
     type 1 diabetes); Baker v. Sec’y of Health & Hum. Servs., No. 99–653V, 2003 WL 22416622 (Fed.
     Cl. Spec. Mstr. Sept. 26, 2003) (rejecting claim that multiple vaccinations caused type 1 diabetes).
     Although these decisions do not bind resolution of this case, they have persuasive value—and I am
     aware of no cases standing for the contrary conclusion.

              Second, even if I ignore such older cases, I find that Petitioner did not establish in this case
     that the HPV vaccine itself could worsen DM1. Dr. Lee’s opinion was the primary source of support
     for this contention, but it was poorly-reasoned, and supported by unreliable science or facially-
     inaccurate suppositions. Thus, Dr. Lee made arguments about the post-vaccination incidence of
     diabetes that were facially illogical and numerically/mathematically incorrect. He also contended
     that the HPV vaccine could have a pathologic impact based on assumptions about the inadvertent
     inclusion in it of immune mediators resulting in a specific kind of adjuvant (TLR agonists) that the
     vaccine does not likely contain—and which if it does, are found only in non-pathologic amounts.

78
  As Respondent points out, Petitioner’s diabetes was not under fair control prior to vaccination. Regular testing also
shows that her HbA1c levels spiked shortly before vaccination, returned to previous levels, and then increased again. See
Table 2 Ex. 19 at 109; see also Exhibit C at 14. Her pre-vaccination glucose levels were also frequently higher than or
similar to her post-vaccination levels.

79
  My determination arises somewhat from the restated legal standard for significant aggravation that the Federal Circuit
established in Sharpe, under which a Petitioner need only establish post-vaccination worsening of the preexisting
condition, and not that her course was worse than would otherwise be expected—with Respondent required (once the
burden shifts due to Petitioner’s success in setting forth a prima facie case) to preponderantly demonstrate that the injured
party’s course was actually consistent with her preexisting condition (thus making it and not vaccination responsible).
Here, however, I do not find that Petitioner overall has carried her burden of establishing that the HPV or flu vaccines
worsened her DM1 (since she cannot demonstrate that the vaccines at issue could worsen DM1 symptoms, or did so on
this fact pattern in a medically-acceptable timeframe), and thus I do not reach the question of whether Ms. Hughes’s post-
vaccination course varied from what would be expected for a person with DM1. (I also do take into account fluctuations
in Petitioner’s symptoms, and periods in which she reported good health, since these undermine her “did cause” showing
under Loving prong five).
                                                             62
He otherwise relied on long-rejected arguments about the role of alum in encouraging pathologic
processes. He could not bulwark his theory with sufficient reliable evidence, drawn from his own
experience or otherwise. The two articles he authored and cited for this component of his opinion
were persuasively rebutted by Respondent’s experts.

         The “did cause” Althen prong two/Loving prong five evidence supporting the significant
aggravation claim is also quite limited to nonexistent. There is no medical record proof that
Petitioner was experiencing some kind of initial, if incomplete reaction to her first HPV dose before
her October 2014 hospital visit—and no evidence from that visit, or several thereafter, that would
corroborate the concept that the vaccine was responsible. The record reveals no undercurrent of an
inflammatory response, or aberrant immune reaction, in the months from July 2014 to Petitioner’s
September 2014 treater visits, and the same is true when the August 2015 to October 2015 period
is reviewed. Rather, it simply appears from the record that Ms. E.S.         more likely experienced
diabetes-related symptoms. Thus, I cannot ascertain support for the conclusion that either vaccine
initiated an immune process (evidenced by signs of inflammation or otherwise) that later manifested
in the spike in diabetes-related symptoms for which Petitioner sought repeated treatment.

        In addition, no treaters who saw Petitioner at any time close to the date of vaccination (and
in this case I will define “close” to mean even within six months) ever opined there could be a
relationship between the vaccine and her flares—unlike cases in which treaters readily so speculate.
See, e.g., R.B. v. Sec’y of Health & Hum. Servs., No. 13-956V, 2017 1713113, at *17 (Fed. Cl. Spec.
Mstr. Feb. 22, 2017) (finding that treater’s opinion can have evidentiary value in establishing a
causation theory). And as Respondent notes, Petitioner’s symptoms course was not consistently
trending downward—in contradiction to her theory that her immune reactions were invariably
negatively impacted by two HPV vaccine doses received months prior to the instances she
references. The explanation offered by Dr. Lee—that blood sugar levels could fluctuate even if the
effects of HPV vaccine doses remained persistently pathologic over the course of years—was not
only inconsistent with his overall theory but facile as well.

         Dr. MacGinnitie also persuasively explained that deterioration of diabetes control of the
kind Petitioner experienced is often seen in late adolescence—an unrebutted point that (while not
established to a sufficient degree to make a formal “factor unrelated” finding) diminished what
evidence Petitioner did offer. Indeed, the record itself contains direct instances in which Petitioner
acknowledged the role her own conduct played in causing symptoms flares (see, e.g., Ex. 31 at 122
(Petitioner presented to the ER with the chief complaint of “intoxication” and reports of repetitive
vomiting)). Even though not every occurrence in which Petitioner wound up in the ER for reasons
associated with her DM1 could be so easily explained, self-monitoring or control of the condition
is as likely to cause declines in health as other factors, further limiting the likelihood that a vaccine
dose received months or years prior to a particular instance of a diabetes symptom flare was causal
of it.

                                                 63
             Finally, even if the fourth and fifth Loving prongs could be met, Petitioner has not shown
     that her DM1 aggravation occurred in a medically-acceptable timeframe. Petitioner’s experts did
     not persuasively explain why the pathologic process leading to a decline in blood sugar control she
     experienced would reasonably have started in the two months from her first receipt of the HPV
     vaccine in July 2014 to her first medical visits in September 2014, especially given the lack of
     record suggestion of any problem in this period. The timeframe from Petitioner’s receipt of a second
     HPV vaccine dose (August 2015) to new medical interventions that October was not much shorter,
     and thus does not provide the kind of “challenge-rechallenge” evidence of a faster reaction that
     might bulwark the purported causal role of the HPV vaccine. 80

             In addition, no medically reliable explanation has been provided for how long it would take
     a person with DM1 to have their disease aggravated after receipt of the HPV vaccine, or how the
     process would thereafter become chronic. Arguments about the persistence of alum in the body are
     reflective of previously-rejected claims in other cases. Olson v. Sec’y of Health & Hum. Servs., No.
     13-439, 2017 WL 3624085 at *20 (Fed. Cl. Spec. Mstr. July 14, 2017), aff’d, 758 Fed. Appx. 919
     (Fed. Cl. 2018).

 V.       Petitioner’s Experts Were Unpersuasive and/or Offered Unreliable Opinions

        My determination to decide this case on the papers was motivated in no small part by the
overall unpersuasive character of Petitioner’s expert opinions. Her experts covered ground that they
have in prior cases, to no success, or made facially-unreliable contentions that greatly diminished
their credibility. The paper copies of such deficient reports told me all I needed to decide the matter—
there was no need to hear from the experts directly.

        Dr. Steinman’s opinion, as set forth in his three written reports, illuminates the various
 evidentiary deficiencies that hampered Petitioner’s case. As a well-credentialed immunologist, Dr.
 Steinman was unquestionably qualified to offer an opinion in this case, and what is more he has
 conducted direct research into some of the alleged injuries, such as narcolepsy. However, the
 substance of the opinion offered was almost identical to opinions he has offered repeatedly in prior
 Program cases, often in cases I have decided—and he employed argument and reasoning that I have
 consistently rejected as medically or scientifically unreliable. See, e.g., D’Toile, 2016 WL 7664475,
 at *14 (discussing Dr. Steinman’s opinion on the association between the flu vaccine and
 narcolepsy). Indeed, in this case he attempted to shoehorn a theory that had reliable scientific
 support in one context (the association between a version of the flu vaccine and narcolepsy) to a
 case involving a different vaccine, and where the evidence is substantially less robust.

80
  Challenge-rechallenge happens when a person (1) is exposed to an antigen, (2) reacts to that antigen in a particular
way, (3) is given the same antigen again, and (4) reacts to that antigen similarly. Nussman v. Sec’y of Health & Hum.
Servs., 83 Fed. Cl. 111, 119 (Fed. Cl. 2008). Typically, the second reaction is faster and more severe. Id.
                                                           64
        Dr. Steinman also referenced items of literature that I have in the past (and in comparable
cases) noted were not deserving of substantial weight. See, e.g., Johnson, 2018 WL 2051760, at
*12, 16, and 24 (petitioner did not preponderantly establish that HPV vaccine was responsible for
POTS or other autonomic dysfunction). And he repeated arguments about general homology in
service of his mechanistic theory of molecular mimicry that, while somewhat logical and not outside
the realm of possibility, do no more than raise plausible points that cannot satisfy the preponderant
evidentiary standard required for an entitlement award. Boatmon, 941 F.3d 1351 at 1355. It may,
for example, be scientifically plausible that the HPV vaccine could promote the creation of
antibodies that could in turn cross-react in an autoimmune attack against self-structures in the body,
but it has not preponderantly been shown that this is likely, given a total absence of reliable research
evidence (whether drawn from Dr. Steinman’s own work, other Program decisions, or articles
discussing scientific/medical research bearing on the matter).

       If Dr. Steinman’s opinion was frequently conclusory or unconcerned with its unreliability,
Dr. Lee’s was far worse. To begin with, Dr. Lee is not an immunologist, cardiologist, or trained in
the analysis or treatment of diabetes, rendering his insights into these general matters (which
dominate this case) somewhat unpersuasive from the outset. But even ignoring his lack of relevant
experience, his theory specific to the HPV vaccine barely rose to the level of plausibility, relying
on the contention that a vaccine with one kind of adjuvant might inadvertently contain, through its
processing, another kind (TLR agonists) that the vaccine itself is not intended to include—and that
this would then be the lynchpin for the pathologic mechanistic processes allegedly occurring
thereafter. Such a theory would require either an expert with more experience in treating or
researching the illnesses alleged (such that a connection could be made between opinions about the
vaccine’s functioning and the injuries in question), or reference to some persuasive and reliable
literature suggesting that vaccine manufacture has been shown to have this effect. Yet, Dr. Lee only
proposed that general research he had performed was enough. He additionally over-relied on the
role the aluminum adjuvant could play pathogenically—an erroneous contention that has repeatedly
been rejected in prior Program cases. McKown, 2019 WL 4072113 at *16; Rothenberg v. Sec’y of
Health & Hum. Servs., No. 15-696V, 2018 WL 2731639 at *7 (Fed. Cl. Spec. Mstr. April 19, 2018);
Wolf v. Sec’y of Health & Hum. Servs., No. 14-342V, 2016 WL 6518581 at *4 (Fed. Cl. Spec. Mstr.
Sept. 15, 2016).

       Dr. Lee’s opinion is also run-through with erroneous calculations and bald assumptions that
collapse on close analysis. For example, his effort to contrast vaccine safety trial evidence of
adverse events like diabetes against similar evidence derived from the time before the HPV vaccine
was approved caused him to make an apples-to-oranges numeric comparison that shed no light at
all on the actual risk posed by vaccination—especially since evidence from the safety trial itself
showed no greater incidence of type 1 diabetes new onset for vaccinated individuals in comparison
to a control group. Ex. 41, reference 4 at 8. Similarly, Dr. Lee proposed acceptable timeframes for
onset of cardiac issues after HPV vaccine administration merely through reference to a tiny sample
of semi-comparable instances, none of which helped establish anything other than the fact that
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  certain vaccinated individuals died of cardiac-related injuries at some time after vaccination.

         Further detracting from Dr. Lee’s opinions was the poor construction of his two written
  reports. His contentions were set forth in a garbled, scattershot manner, and relied on cut-and-pasted
  copies of articles and texts—adding considerably to each report’s length, but without increasing
  their persuasiveness or clarity. He also repeatedly attempted to rebut in granular detail certain points
  raised by Respondent’s more facially-qualified experts—but in so doing chased point after point
  down the proverbial rabbit hole, with no obvious benefit to the Petitioner. Compare Second Lee
  Rep. at 8 (disputing what Dr. LaRue defined as the “gold standard” test for diagnosing a coronary
  artery disease), with LaRue Second Rep. at 6 (explaining why Dr. Lee’s points about diagnostic
  methods herein were unpersuasive in establishing Petitioner’s alleged ischemia). These wasted,
  bickering efforts exemplify circumstances where an expert misses the forest for the trees—and
  underscore why I have deemed this matter appropriate for dismissal merely on the basis of the
  record.

VI.     This Claim was Properly Resolved Without a Hearing

       In ruling on the record, I am opting against holding a hearing. The choice of how best to
 resolve this case is a matter that lies generally within my discretion, but because Petitioner
 challenges this manner of disposition in opposing Respondent’s request for dismissal, I shall explain
 my reasoning.

         Prior decisions have recognized that a special master’s discretion in deciding whether to
conduct an evidentiary hearing “is tempered by Vaccine Rule 3(b),” or the duty to afford each party
a “full and fair opportunity to present its case.” Hovey v. Sec’y of Health & Hum. Servs., 38 Fed. Cl.
397, 400–01 (citing Rule 3(b)). But that rule also includes the obligation of creation of a record
“sufficient to allow review of the special master’s decision.” Hovey, 38 Fed. Cl. at 401; see also
Kreizenbeck, 945 F.3d at 1366. Thus, the fact that a claim is legitimately disputed, such that the
special master must exercise his intellectual faculties in order to decide a matter, is not itself grounds
for a trial (for if it were, trials would be required in every disputed case). Special masters are expressly
empowered to resolve fact disputes without a hearing—although they should only so act if a party
has been given the proper “full and fair” chance to prove their claim.

        In this case, no hearing was required to resolve fairly Petitioner’s claim. I was able to evaluate
the evidentiary strength of her expert’s theories and opinions simply based on the written reports,
and did not require credibility determinations to weigh the medical/scientific reliability of the
theories espoused. Petitioner’s arguments to the contrary are not persuasive. That part of her claim
reliant on proving the aggravation of preexisting diabetes, for example, ventured into seas that
numerous prior claimants have unsuccessfully navigated, without offering scientifically-reliable
grounds reflecting new research or thinking on the subject that would counsel for reconsideration of
the issue. The arguments Petitioner makes about the autoimmune nature, in whole or part, of that
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 basket of other symptoms she complains of, and their autonomic nature, is similarly not supported
 by new discoveries or research—as the 2019 AAS Statement makes clear. And her purported “new”
 diagnoses from 2018 or 2019 are either substantively less certain than meets the eye (like POTS and
 CFS), or reflect occurrences that cannot reliably or medically acceptably be linked to vaccines
 received three or more years before.

         The fact that this matter resulted in the filing of numerous expert reports on both sides also is
 not a compelling reason to hold a hearing. Even the most obviously flimsy of theories could be
 “supported” with multiple experts willing to put their reputations on the line, so the fact that expert
 reports pile up in a case is not by itself a compelling reason to hold a trial. Indeed, I have resolved
 by ruling on the record science-dense cases in which both sides made credible, reasonably-contested
 arguments arising from multiple expert reports. See, e.g., D’Toile, 2016 WL 7664475. 81 Here, after
 close review of all reports filed, I was able to discern either obvious deficiencies in the Petitioner’s
 proffered opinion, or that the opinions repeated arguments I have rejected in the past. And these
 opinions were not rooted in new, previously-unconsidered scientific or medical evidence that would
 support re-evaluating my prior determinations on these topics.

                                                   CONCLUSION

       Although some of Petitioner’s purported injuries lack medical record or diagnostic
 substantiation, she has clearly experienced a number of overlapping symptoms and conditions over
 many years (most likely attributable to her struggles with DM1) that have caused her and her family
 considerable anguish—in their efforts to treat as well as to identify some unifying explanation for
 her constant need for medical care. She also no doubt has a good faith belief that the HPV and flu
 vaccines had to have some relationship to her injuries—if for no other reason than the increased
 tempo of her symptoms post-dated her receipt of the vaccines.

       Nevertheless, the overall picture painted herein by the objective medical record is
 unsupportive of the conclusion that the HPV or flu vaccines were causal of any of her post-
 vaccination symptoms, despite their complex array and convoluted progression. The timeframes
 from vaccine to injury are too attenuated, the causation theories not persuasively established, and
 the expert support, plus other independent medical or scientific literature, offered for the claim
 largely unreliable (especially to the extent it repeats causation theories that have proven fruitless in
 numerous prior Program cases). The deficiencies of this claim were self-evident enough that a
 hearing was not required to adjudicate the matter.

81
  By contrast, I have also dismissed cases like this one, where the filing of multiple reports masked what was determined
to be a wholly unreliable claim. Kreizenbeck, 945 F.3d at 1365–66 (dismissing on record case in which parties together
offered opinions from six experts in total; petitioner attempted to convert abandoned autism injury claim into assertion
that vaccines precipitated encephalopathic reaction resulting in developmental regression).

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    Accordingly, for the reasons set forth above, I deny compensation in this case and dismiss the
 matter. In the absence of a timely-filed motion for review (see Appendix B to the Rules of the
 Court), the Clerk shall enter judgment in accord with this decision. 82

     IT IS SO ORDERED.

                                                                         /s/ Brian H. Corcoran
                                                                           Brian H. Corcoran
                                                                           Chief Special Master

82
   Pursuant to Vaccine Rule 11(a), the parties may expedite entry of judgment by filing a joint notice renouncing their
right to seek review.

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