Abstract:
A breath testing apparatus is provided with a mouthpiece, a collection chamber, and a discharge chute. A breath sample is captured within the collection chamber and transferred to an evacuated container through the discharge chute by a sample transfer assembly.

Description:
BACKGROUND OF THE INVENTION 
       [0001]    This invention relates to the field of sampling air from the lungs and specifically to the field of obtaining a sample of a person&#39;s air, including alveolar air from the alveoli of the lungs of a person. 
         [0002]    Air from the lungs of a person can be used for many different types of testing that would otherwise require the person to undergo an invasive procedure. For example, alveolar air can be analyzed for, but not limited to, the noninvasive diagnosis of a wide variety of conditions including the noninvasive diagnosis of stomach infections related to a high incidence of ulcers, enzymatic deficiencies, and metabolic conditions and/or abnormalities. Crucial to any such testing is the ability to get an accurate sample containing a sufficient volume of air representative of true alveolar air, necessary for specific testing. 
         [0003]    Hydrogen and methane are produced in the digestive system primarily only by the bacterial fermentation of carbohydrates (sugars, starches or vegetable fibers), so either of these gases appear in the expired air, it is usually a signal that carbohydrates or carbohydrate fragments have been exposed to bacteria, permitting such fermentation to take place. Levitt, M. D. Production and excretion of hydrogen gas in man. New Engl. J. Med 1968; 281:122 (incorporated herein by reference). The generation of H2 and/or CH4 will result in the reabsorption of some of these gases into the blood stream from the site of their digestion, and they will appear in the expired air. 
         [0004]    Bacteria are ordinarily not present in significant numbers in the small intestine, where digestion and absorption of sugars take place. Therefore, when a challenge dose (eg. lactose) is ingested, the level of hydrogen in alveolar air will rise significantly within one to two hours (depending on the intestinal transit time) only if the sugar is not digested and, therefore reaches the colon. 
         [0005]    The breath-H2 test is a simple non-invasive procedure which is readily accepted by patients and staff (Metz, G.; Jenkins, D. L.; Peters, T. J,; Newman, A.; Blendis, L. M. Breath hydrogen as a diagnostic method for hypolactasia. Lancet. 1975; 1 (7917) : 1155-7, incorporated herein by reference), and which has greater reliability and acceptability than the blood test, according to most reports in the literature (DiPalma, J. A.; Narvaez, R. M. Prediction of lactose malabsorption in referral patients. Dig Dis Sci. 1988; 33:303, incorporated herein by reference, and Davidson, G. P.; Robb, T. A.. Value of breath hydrogen analysis in management of diarrheal illness in childhood: Comparison with duodenal biopsy. J Ped Gastroenterol Nutr. 1985; 4:381-7; Fernandes, J.; Vos, C. E.; Douwes, A, C,; Slotema, E.; Degenhart, H. J. Respiratory hydrogen excretion as a parameter for lactose malabsorption in children. Amer J Clin Nutr. 1978; 31:597-602; Newcomer, A. D.; McGill, D. B.; Thomas, R. J.; Hofmann, A. F. Prospective comparison of indirect methods for detecting lactase deficiency. New Engl J Med. 1975; 293:1232-6; Douwes, A. C.; Fernandes, J.; Degenhart H. J. Improved accuracy of lactose tolerance test in children, using expired H2 measurement. Arch Dis Child. 1978; 53:939-42; Solomons, N. W.; Garcia-Ibanez, R.; Viteri, F. E. Hydrogen breath test of lactose absorption in adults: The application of physiological doses and whole cow&#39;s milk sources. Amer J Clin Nutr. 1980; 33:545-54; each incorporated by reference). 
         [0006]    The lower dose of lactose usually does not cause the discomfort and explosive diarrhea frequently seen by malabsorbers who are given the large dose required for the blood test. 
         [0007]    A study with over 300 patients showed that G-I symptoms after a lactose challenge are strongly associated with the amount of H2 excreted, and the relationship between blood glucose change and symptom-severity was less evident. Jones, D. V.; Latham, M. C.; Kosikowski, F. V.; Woodward, G. Symptom response to lactosereduced milk in lactose-intolerant adults. Amer J Clin Nutr. 1976; 29(6):633-8, incorporated by reference. 
         [0008]    False-positive breath-tests are rare, and when they occur they are usually caused by improperly doing the test—allowing the subject to smoke, to sleep or to eat shortly before or during the test11. Bacterial overgrowth (from the colon retrograde into the small intestine) can also produce a false-positive breath-test, but it is usually preceded by an elevated fasting breath-H2 level and the response is seen soon after the sugar is ingested (within 20-30 minutes). 
         [0009]    The incidence of false-negative results with the breath-test is well below that seen with the blood test. False-negative results are reported to be from 5-15% of all lactose malabsorbers. Filali, A.; Ben Hassine, L.; Dhouib, H.; Matri, S.; Ben Ammar, A.; Garoui, H. Study of malabsorption of lactose by the hydrogen breath test in a population of 70 Tunisian adults. Gastroenterol Clin Biol. 1987; 11:554-7; Douwes, A. C.; Schaap, C.; van der Kleivan Moorsel, J. M. Hydrogen breath test in school children. Arch Dis Child. 1985; 60:333-7; Rogerro, P.; Offredi, M. L.; Mosca, F.; Perazzani, M.; Mangiaterra, V.; Ghislanzoni, P.; Marenghi, L.; Careddu, P. Lactose absorption and malabsorption in healthy Italian children: Do the quantity of malabsorbed sugar and the small bowel transit time play roles in symptom production? J Pediatr Gastroenterol Nutr. 1985 (February); 4(1):82-614; each incorporated by reference. This is due to a variety of causes. Many of the false-negative reports can be avoided by measuring methane in addition to hydrogen because some methanogenic flora convert colonic H2 to CH4. Cloarac, D.; Bornet, F.; Gouilloud, S.; Barry, J. Ll.; Salim, B.; Galmiche, J. P. Breath hydrogen response to lactulose in healthy subjects: relationship to methane producing status. Gut. 1990 (March); 31:300-4; incorporated by reference. 
       SUMMARY OF THE INVENTION 
       [0010]    In accordance with the present invention, a testing apparatus is provided. A breath collection apparatus comprising a breath entryway or mouthpiece is coupled to a first one-way coupling, which is preferably, but not necessarily, a flutter valve. Breath is expelled into the mouthpiece and through the one-way coupling. A collection chamber is coupled to said breath entryway by said first one-way coupling, and a second one-way coupling, also which is preferably, but not necessarily, a flutter valve coupled to said collection chamber to allow a first waste portion of exhaled breath to escape the collection chamber. When the breath is completed, both one-way couplings will close, trapping an end-expiration breath sample within the collection chamber. A sample transfer assembly coupled to said collection chamber allows for an evacuated air chamber to be selectively coupled to said sample transfer assembly, and the evacuated air chamber recovers a portion of the end-expiration breath sample within the collection chamber. In a preferred embodiment, a discharge chute is coupled to said collection chamber about said sample transfer assembly, said discharge chute comprising a proximal end for coupling to said collection chamber, and a distal end for receiving said evacuated air chamber. 
     
    
     
       BRIEF DESCRIPTION OF THE DRAWINGS 
         [0011]      FIG. 1  is a perspective view of a sample collection apparatus of the present invention, with an evacuated air chamber inserted into a distal end of a discharge chute. 
           [0012]      FIG. 2  is an exploded perspective view of a sample collection apparatus of the present invention. 
           [0013]      FIG. 3  is an in-use side cross-sectional view of a sample collection apparatus, shown collecting a breath sample; 
           [0014]      FIG. 4  is a side cross-sectional view of a sample collection apparatus, with an evacuated air chamber being inserted into a distal end of the discharge chute; 
           [0015]      FIG. 5  is a side cross-sectional view of a sample collection apparatus, with an evacuated air chamber being inserted onto a discharge needle within the discharge chute; 
           [0016]      FIG. 6  shows a collected an end-expiration breath sample. 
       
    
    
     DESCRIPTION OF THE PREFERRED EMBODIMENT 
       [0017]    Although the disclosure hereof is detailed and exact to enable those skilled in the art to practice the invention, the physical embodiments herein disclosed merely exemplify the invention which may be embodied in other specific structures. While the preferred embodiment has been described, the details may be changed without departing from the invention. 
         [0018]    Referring now to  FIG. 1  a perspective view of a sample collection apparatus  10  of the present invention is shown. A mouthpiece  12  comprising a breath entryway is shown, to allow breath to pass to collection chamber  14 . A breath discharge chute  16  receives an evacuated air chamber  100  that receives an end-expiration breath sample (described later) from within the collection chamber  14 . 
         [0019]    Referring now to  FIG. 2 , an exploded perspective view of a sample collection apparatus  10  of the present invention is shown. Mouthpiece  12  is either integrally formed or coupled with a one-way discharge assembly  26 . Positive pressure from a breath, through the mouthpiece  12 , causes flexible ring  24  to flex, and allow air to pass into collection chamber  14  at an upstream end of collection chamber  14 . Flexible ring  24 , is preferably, but not necessarily, a flutter valve. Another one-way discharge structure  24 , again coupled to a flexible ring  24  (and again preferably, but not necessarily, a flutter valve), is coupled to a downstream end of collection chamber  14 . Coupled to the interior of collection chamber  14  is discharge needle  22 , which provides a selective passageway from breath between collection chamber  14  and ultimately evacuated air chamber  100 , which is coupled to discharge needle  22  through discharge chute  16 . 
         [0020]    Referring now to  FIG. 3 , an in-use side cross-sectional view of sample collection apparatus  10  is shown. A patient has pressed a mouth to mouthpiece  12  and began exhalation. The first volume of breath  42  evacuates background air from within collection  14 , and first volume of breath  42 , being not the most desirable for alveolar air sampling, is expelled through discharge chute  16  without capture. Positive pressure from the breath sample flexes flexible rings  24 , allowing air to continue to flow through collection chamber  14 , into discharge chute  16 . 
         [0021]    As the breath stops, the positive pressure from the breathing stops as well, allowing flexible rings  24  to return to their static position, flush against one-way discharge structures  26  at the upstream and downstream ends of collection chamber  14 . As the flexible rings  24  seal the collection chamber  14 , end-expiration breath sample  40  is captured in collection chamber  14 . To retrieve the end-expiration breath sample  40  for convenient sampling by gas chromatography equipment, it is desirable to collect end-expiration breath sample  40  in an evacuated air chamber  100  (a test tube) . Evacuated air chamber  100  is of a volume V 1 , which is preferably a smaller volume than volume V 2  of the collection chamber  14 , so that evacuated air chamber  100  collects only end-expiration breath sample  40  from the collection chamber  14 , and not outside air drawn through collection chamber  14 . 
         [0022]    Evacuated air chamber  100  is inserted into a distal end of the discharge chute  16  as shown in  FIG. 4 , and as shown in  FIG. 5 , evacuated air chamber  100  is inserted onto discharge needle  22 , piercing a septum  20  (preferably self-sealing) of air chamber  100 . The evacuated air chamber  100  then retrieves end-expiration breath sample  40  from collection chamber  14 . After air chamber  100  has retrieved end-expiration breath sample  40  from collection chamber  14 , the air chamber  100  can be withdrawn from the discharge needle  22  within discharge chute  16 . The air chamber  100  containing end-expiration breath sample  40  can then be processed in a laboratory for target analytes as desired. 
         [0023]    The foregoing is considered as illustrative only of the principles of the invention. Furthermore, since numerous modifications and changes will readily occur to those skilled in the art, it is not desired to limit the invention to the exact construction and operation shown and described. While the preferred embodiment has been described, the details may be changed without departing from the invention.