Patent Description:
Some lubricants include a lecithin, which contains a hydrophobic tail and hydrophilic head, similar in nature to the components of the cellular lipid bilayer or soap. This arrangement allows half of the molecule to embed in the aqueous cellular environment, leaving the hydrophobic head exposed, which does not bond to the surface of the surgical instrument, thus preventing the tissue from adhering to the instrument. This mechanism is effective but is limited by heat sensitivity. However, lecithin may be a relatively heat-sensitive compound, which may break down into a residue that does not retain its non-stick properties. As such, lecithin may degrade through the course of the intrinsically thermal process of electro-cautery. In addition, as the residue may build up on the probe, the transfer of energy from the probe to the tissue may become increasingly inefficient, resulting in longer burn-times. Furthermore, the charred residue may not remove easily, and so the further addition of fresh lubricant may not provide improved performance once the residue begins to accumulate. Improved lubricants may aid the surgical process.

<CIT> discloses known lubricants for coating electro-cautery probes.

The invention is a formulation, method and kit as defined in the appended claims. Any of the following not falling within the scope of the claims is comparative.

A medical lubricant may include a base oil. The medical lubricant can be used on a surgical device.

A formulation for a lubricant includes a base oil comprising a compound of the formula I:
<CHM>
In formula I, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>; R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with hydroxy, or OR<NUM>; or a salt thereof. The formulation does further include a phospholipid; or a salt thereof; and a salt of the formula M<NUM>(R<NUM>)(R<NUM>) (II). M<NUM> can be a divalent cation, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, -OC(O)C<NUM>-C<NUM> alkenyl, or - OC(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted OR<NUM>. Each of R<NUM>, R<NUM>, and R<NUM> is independently H, C<NUM>-C<NUM> alkyl , C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, - C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, - C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl,.

A method of coating an electrocautery device includes contacting a surface of the electrocautery device with a formulation. The formulation includes a base oil comprising a compound of the formula I:
<CHM>
In formula I, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>; R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with hydroxy, or OR<NUM>; or a salt thereof. The formulation does further include a phospholipid; or a salt thereof; and a salt of the formula M<NUM>(R<NUM>)(R<NUM>) (II). M<NUM> can be a divalent cation, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, -OC(O)C<NUM>-C<NUM> alkenyl, or - OC(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted OR<NUM>. Each of R<NUM>, R<NUM>, and R<NUM> is independently H, C<NUM>-C<NUM> alkyl , C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, - C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, - C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl.

A method of preparing a formulation is disclosed. The formulation includes a base oil comprising a compound of the formula I:
<CHM>
In formula I, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>; R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with hydroxy, or OR<NUM>; or a salt thereof. The formulation does further include a phospholipid; or a salt thereof; and a salt of the formula M<NUM>(R<NUM>)(R<NUM>) (II). M<NUM> can be a divalent cation, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, -OC(O)C<NUM>-C<NUM> alkenyl, or - OC(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted OR<NUM>. Each of R<NUM>, R<NUM>, and R<NUM> is independently H, C<NUM>-C<NUM> alkyl , C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, - C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, - C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl.

A kit includes formulation for a lubricant that includes a base oil comprising a compound of the formula I:
<CHM>
In formula I, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>; R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with hydroxy, or OR<NUM>; or a salt thereof. The formulation does further include a phospholipid; or a salt thereof; and a salt of the formula M<NUM>(R<NUM>)(R<NUM>) (II). M<NUM> can be a divalent cation, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, -OC(O)C<NUM>-C<NUM> alkenyl, or - OC(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted OR<NUM>. Each of R<NUM>, R<NUM>, and R<NUM> is independently H, C<NUM>-C<NUM> alkyl , C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, - C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, - C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl,. The kit further includes a cautery probe.

A method of cauterization includes applying a formulation to a cautery probe and cauterizing tissue with the cautery probe. The formulation includes a base oil comprising a compound of the formula I:
<CHM>.

In formula I, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted OR<NUM>; R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with hydroxy, or OR<NUM>; or a salt thereof. The formulation does further include a phospholipid; or a salt thereof; and a salt of the formula M<NUM>(R<NUM>)(R<NUM>) (II). M<NUM> can be a divalent cation, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, -OC(O)C<NUM>-C<NUM> alkenyl, or - OC(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted OR<NUM>. Each of R<NUM>, R<NUM>, and R<NUM> is independently H, C<NUM>-C<NUM> alkyl , C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl. The kit further includes a cautery probe.

As used herein, the term "alkyl" includes a chain of carbon atoms, which is optionally branched and contains from <NUM> to <NUM> carbon atoms. It is to be further understood that in certain embodiments, alkyl may be advantageously of limited length, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustratively, such particularly limited length alkyl groups, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>, and the like may be referred to as "lower alkyl. " In some embodiments, alkyl may be C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustrative alkyl groups include, but are not limited to, methyl, ethyl, n-propyl, isopropyl, n-butyl, isobutyl, sec-butyl, tert-butyl, pentyl, <NUM>-pentyl, <NUM>-pentyl, neopentyl, hexyl, heptyl, octyl, nonyl, decyl, and the like. Alkyl may be substituted or unsubstituted. Typical substituent groups include cycloalkyl, aryl, heteroaryl, heteroalicyclic, hydroxy, alkoxy, aryloxy, mercapto, alkylthio, arylthio, cyano, halo, carbonyl, oxo, (=O), thiocarbonyl, O-carbamyl, N-carbamyl, O-thiocarbamyl, N-thiocarbamyl, C-amido, N-amido, C-carboxy, O-carboxy, nitro, and amino, or as described in the various embodiments provided herein. It will be understood that "alkyl" may be combined with other groups, such as those provided above, to form a functionalized alkyl. By way of example, the combination of an "alkyl" group, as described herein, with a "carboxy" group may be referred to as a "carboxyalkyl" group. Other nonlimiting examples include hydroxyalkyl, aminoalkyl, and the like.

As used herein, the term "alkylene" refers to a divalent -alkylgroup in which alkyl is as defined previously. Exemplary alkylene groups include -CH<NUM>-, -(CH<NUM>)<NUM>- and -C(CH<NUM>)HCH<NUM>-.

As used herein, the term "alkenyl" includes a chain of carbon atoms, which is optionally branched, and contains from <NUM> to <NUM> carbon atoms, and also includes at least one carbon-carbon double bond (i.e. C=C). It will be understood that in certain embodiments, alkenyl may be advantageously of limited length, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustratively, such particularly limited length alkenyl groups, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM> may be referred to as lower alkenyl. In some embodiments, alkenyl may be C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Alkenyl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative alkenyl groups include, but are not limited to, ethenyl, <NUM>-propenyl, <NUM>-propenyl, <NUM>-, <NUM>-, or <NUM>-butenyl, and the like.

As used herein, the term "alkenylene" refers to a divalent - alkenyl- group in which alkenyl is as defined previously. Exemplary alkenylene groups include -CH=CH-, -CH=CHCH<NUM>-, and -CH<NUM>CH=CH-.

As used herein, the term "alkynyl" includes a chain of carbon atoms, which is optionally branched, and contains from <NUM> to <NUM> carbon atoms, and includes at least one carbon-carbon triple bond (i.e. C=C). It will be understood that in certain embodiments alkynyl may each be advantageously of limited length, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustratively, such particularly limited length alkynyl groups, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM> may be referred to as lower alkynyl. In some embodiments, alkynyl may be C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Alkynyl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative alkynyl groups include, but are not limited to, ethynyl, <NUM>-propynyl, <NUM>-propynyl, <NUM>-, <NUM>-, or <NUM>-butynyl, and the like.

As used herein, the term "alkynylene" refers to a divalent - alkynyl- group in which - alkynyl - is as defined previously. Exemplary alkynylene groups include ethynyl and propargyl.

As used herein, the term "aryl" refers to an all-carbon monocyclic or fused-ring polycyclic groups of <NUM> to <NUM> carbon atoms having a completely conjugated pi-electron system. It will be understood that in certain embodiments, aryl may be advantageously of limited size such as C<NUM>-C<NUM> aryl. Illustrative aryl groups include, but are not limited to, phenyl, naphthalenyl, and anthracenyl. The aryl group may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein.

As used herein, the term "arylene" refers to a divalent - aryl - group in which aryl is as defined previously. Exemplary arylene groups include - phenylene - and - napthalenylene -.

As used herein, the term "cycloalkyl" refers to a <NUM> to <NUM> member all-carbon monocyclic ring, an all-carbon <NUM>-member/<NUM>-member or <NUM>-member/<NUM>-member fused bicyclic ring, or a multicyclic fused ring (a "fused" ring system means that each ring in the system shares an adjacent pair of carbon atoms with each other ring in the system) group where one or more of the rings may contain one or more double bonds but the cycloalkyl does not contain a completely conjugated pi-electron system. It will be understood that in certain embodiments, cycloalkyl may be advantageously of limited size such as C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM> and C<NUM>-C<NUM>. The cycloalkyl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative cycloalkyl groups include, but are not limited to, cyclopropyl, cyclobutyl, cyclopentyl, cyclopentenyl, cyclopentadienyl, cyclohexyl, cyclohexenyl, cycloheptyl, adamantyl, norbornyl, norbornenyl, <NUM>-fluoren-<NUM>-yl, and the like.

As used herein, the term "cycloalkylene" refers to a divalent - cycloalkyl-group in which cycloalkyl is as defined previously. Exemplary cycloalkylene groups include -cyclohexylene- and -cylcopentylene-.

In accordance with the invention, the term "heteroalkyl" includes a chain of atoms that includes both carbon and at least one heteroatom, and is optionally branched. It is to be further understood that in certain embodiments, heteroalkyl may be advantageously of limited length, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustratively, such particularly limited length heteroalkyl groups, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>, and the like may be referred to as "lower heteroalkyl. " In some embodiments, heteroalkyl may be C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustrative heteroatoms include nitrogen, oxygen, and sulfur. In certain variations, illustrative heteroatoms also include phosphorus and selenium.

As used herein, the term "heteroalkylene" refers to a divalent - heteroalkyl- group in which heteroalkyl is as defined previously. Exemplary heteroalkylene groups include -ethoxylene-.

As used herein, the term "heteroalkenyl" includes both a chain of carbon atoms which is optionally branched and at least one heteroatom, and also includes at least one carbon-carbon double bond (i.e. C=C). It will be understood that in certain embodiments, heteroalkenyl may be advantageously of limited length, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustratively, such particularly limited length heteroalkenyl groups, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM> may be referred to as lower heteroalkenyl. In some embodiments, heteroalkenyl may be C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Heteroalkenyl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative heteroatoms include nitrogen, oxygen, and sulfur. In certain variations, illustrative heteroatoms also include phosphorus and selenium.

As used herein, the term "heteroalkynyl" includes both a chain of carbon atoms which is optionally branched and at least one heteroatom and also includes at least one carbon-carbon double bond (i.e. C≡C). It will be understood that in certain embodiments, heteroalkynyl may be advantageously of limited length, including C<NUM>-C<NUM>, C<NUM>-C<NUM>,C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Illustratively, such particularly limited length heteroalkynyl groups, including C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM> may be referred to as lower heteroalkynyl. In some embodiments, heteroalkynyl may be C<NUM>-C<NUM>, C<NUM>-C<NUM>, C<NUM>-C<NUM>, and C<NUM>-C<NUM>. Heteroalkynyl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative heteroatoms include nitrogen, oxygen, and sulfur. In certain variations, illustrative heteroatoms also include phosphorus and selenium.

As used herein, the term "heteroalkynylene" refers to a divalent - heteroalkynyl - group in which heteroalkynyl is as defined previously.

As used herein, the term "cycloheteroalkyl" including heterocyclyl and heterocycle, includes a chain of atoms that includes both carbon, such as heteroalkyl, and at least one heteroatom, and is optionally branched, where at least a portion of the chain is cyclic. Illustrative heteroatoms include nitrogen, oxygen, and sulfur. In certain variations, illustrative heteroatoms also include phosphorus and selenium. Illustrative cycloheteroalkyl include, but are not limited to, tetrahydrofuryl, pyrrolidinyl, tetrahydropyranyl, piperidinyl, morpholinyl, piperazinyl, homopiperazinyl, quinuclidinyl, and the like. As used herein, the term "heterocycloalkyl" refers to a monocyclic or fused ring group having in the ring(s) from <NUM> to <NUM> ring atoms, in which at least one ring atom is a heteroatom, such as nitrogen, oxygen or sulfur, the remaining ring atoms being carbon atoms. Heterocycloalkyl may optionally contain <NUM>, <NUM>, <NUM> or <NUM> heteroatoms. Heterocycloalkyl may also have one or more double bonds, including double bonds to nitrogen (e.g. C=N or N=N) but does not contain a completely conjugated pi-electron system. It will be understood that in certain embodiments, heterocycloalkyl may be advantageously of limited size such as <NUM>-to <NUM>-membered heterocycloalkyl, <NUM>- to <NUM>-membered heterocycloalkyl, and the like. Heterocycloalkyl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative heterocycloalkyl groups include, but are not limited to, oxiranyl, thianaryl, azetidinyl, oxetanyl, tetrahydrofuranyl, pyrrolidinyl, tetrahydropyranyl, piperidinyl, <NUM>,<NUM>-dioxanyl, morpholinyl, <NUM>,<NUM>-dithianyl, piperazinyl, oxepanyl, <NUM>,<NUM>-dihydro-<NUM>-pyranyl, <NUM>,<NUM>-dihydro-<NUM>-pyranyl, <NUM>-pyranyl, <NUM>, <NUM>, <NUM>, <NUM>-tetrahydropyridinyl, and the like.

As used herein, the term "cycloheteroalkylene" refers to a divalent - cycloheteroalkyl - group in which cycloheteroalkyl is as defined previously. Exemplary cycloheteroalkylene groups include - morpholinylene - and - piperazinylene -.

As used herein, the term "heteroaryl" refers to a monocyclic or fused ring group of <NUM> to <NUM> ring atoms containing one, two, three, or four ring heteroatoms selected from nitrogen, oxygen, and sulfur, the remaining ring atoms being carbon atoms, and also having a completely conjugated pi-electron system. It will be understood that in certain embodiments, heteroaryl may be advantageously of limited size such as <NUM>- to <NUM>-membered heteroaryl, <NUM>- to <NUM>-membered heteroaryl, and the like. Heteroaryl may be unsubstituted or substituted as described for alkyl or as described in the various embodiments provided herein. Illustrative heteroaryl groups include, but are not limited to, pyrrolyl, furanyl, thiophenyl, imidazolyl, oxazolyl, thiazolyl, pyrazolyl, pyridinyl, pyrimidinyl, quinolinyl, isoquinolinyl, purinyl, tetrazolyl, triazinyl, pyrazinyl, tetrazinyl, quinazolinyl, quinoxalinyl, thienyl, isoxazolyl, isothiazolyl, oxadiazolyl, thiadiazolyl, triazolyl, benzimidazolyl, benzoxazolyl, benzthiazolyl, benzisoxazolyl, benzisothiazolyl, carbazoloyl, and the like.

As used herein, the term "heteroarylene" refers to a divalent - heteroaryl - group in which heteroaryl is as defined previously. Exemplary heteroarylene groups include - imidazoylene - and - furanylene -.

As used herein, "hydroxy" or "hydroxyl" refers to an -OH group.

As used herein, "alkoxy" refers to both an -O-(alkyl) or an -O-(unsubstituted cycloalkyl) group. Representative examples include, but are not limited to, methoxy, ethoxy, propoxy, butoxy, cyclopropyloxy, cyclobutyloxy, cyclopentyloxy, cyclohexyloxy, and the like.

As used herein, "halo" or "halogen" refers to fluorine, chlorine, bromine or iodine.

As used herein, "bond" refers to a covalent bond.

As used herein, "amino" refers to an -NR"R" group, where R" is any R group as described in the various embodiments provided herein.

As used herein, "optional" or "optionally" means that the subsequently described event or circumstance may but need not occur, and that the description includes instances where the event or circumstance occurs and instances in which it does not. For example, "heterocycle group optionally substituted with an alkyl group" means that the alkyl may, but need not be present, and the description includes situations where the heterocycle group is substituted with an alkyl group and situations where the heterocycle group is not substituted with the alkyl group.

As used herein, "independently" means that the subsequently described event or circumstance is to be read on its own relative to other similar events or circumstances. For example, in a circumstance where several equivalent hydrogen groups are optionally substituted by another group described in the circumstance, the use of "independently optionally" means that each instance of a hydrogen atom on the group may be substituted by another group, where the groups replacing each of the hydrogen atoms may be the same or different. Or for example, where multiple groups exist all of which can be selected from a set of possibilities, the use of "independently" means that each of the groups can be selected from the set of possibilities separate from any other group, and the groups selected in the circumstance may be the same or different.

For the purposes of promoting an understanding of the principles of the disclosure, reference will now be made to a number of illustrative embodiments illustrated in the drawings and specific language will be used to describe the same.

Lubricants may be used in medical procedures, such as cauterization, to reduce the build-up of material on cautery probes. Illustrative cautery probes include electrocautery probes, heated scalpels, and those capable for use in robotic procedures. Illustrative embodiments of a lubricant may comprise a formulation comprising a base oil, a phospholipid, a salt, or a combination thereof. In some embodiments, a lubricant in accordance with the present disclosure uses a multi-phase non-stick mechanism. In some embodiments, the lubricant more than doubles the number of electro-cautery burns per application compared to a comparative lubricant before the lubricant is exhausted and tissue sticking begins to occur (see <FIG>). Additionally, in some embodiments, a lubricant may retain a transparent appearance during use, preventing the tissue discoloration noted with a comparative lubricant formula (see <FIG>). In some embodiments, the formulation also comprises natural fragrance oils, which assist in offsetting a foul odor that can be generated by the electrocautery process.

The formulation for a lubricant may comprise a certain percentage of a base oil. The percentage of the base oil for the formulation for a lubricant is at least about <NUM>%, at least about <NUM>%, at least about <NUM>%, or at least about <NUM>% by weight of the formulation. In some embodiments, the base oil is about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. The base oil is about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation. In some embodiments, the formulation may comprise one, two, or three base oils. In some embodiments, the formulation comprises a mixture of base oils.

In some illustrative embodiments, the base oil comprises a compound of the formula I
<CHM>
or a salt thereof. In some embodiments, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl. Illustratively, each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with halo, hydroxy, amino, oxo, or OR<NUM>. In some embodiments, R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with halo, hydroxy, amino, oxo, or OR<NUM>. In some embodiments, each of R<NUM> and R<NUM> is independently H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, - C(O)C<NUM>-C<NUM> alkynyl is independently optionally substituted with halo, hydroxy, or amino or a salt thereof.

In some embodiments, R<NUM> is H and the compound of formula I is a carboxylic acid. In some embodiments, R<NUM> is an optionally substituted C<NUM>-C<NUM> alkyl, and the compound of formula I is an ester. Optional substitutions of the C<NUM>-C<NUM> alkyl include OR<NUM>. In some embodiments each R<NUM> is independently H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, - C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, or -C(O)C<NUM>-C<NUM> alkynyl.

In some embodiments, each R<NUM> is independently -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl. In some other embodiments, each R<NUM> is independently -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl,.

In some embodiments, the compound of formula I is triolein. In some embodiments, the compound of formula I is trimyristicin or isopropyl myristate. In some embodiments, the compound of formula I is derived from avocado oil, canola oil, castor oil, coconut oil, olive oil, palm oil, safflower oil, or sunflower, high-oleic oil. In some embodiments, the formulation comprises more than one compound of formula I. In some embodiments, the formulation comprises two or at least two compounds of formula I.

The base oil may comprise a certain percentage of the compound of formula I. The percentage of the compound of formula I in the base oil may be at least about <NUM>%, at least about <NUM>%, at least about <NUM>%, at least about <NUM>%, or at least about <NUM>% by weight of the base oil. In some embodiments, the compound of formula I is about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the base oil. In some embodiments, the compound of formula I is about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the base oil.

In some embodiments, the base oil may be a vegetable oil. In some embodiments, the base oil may be selected from the group consisting of avocado oil, grapeseed oil, canola oil, coconut oil, castor oil, olive oil, palm oil, safflower oil, sunflower oil, and triolein. The base oil may comprise fatty acids that are unsaturated, saturated, or polyunsaturated. In some embodiments, the base oil is avocado oil. In some embodiments, the base oil is grape seed oil.

According to some aspects of the present disclosure, the base oil has a smoke point. In some embodiments, the smoke point of the base oil is at least about <NUM> (<NUM> °F), at least about <NUM> (<NUM> °F), at least about <NUM> (<NUM> °F), at least about <NUM> (<NUM> °F), at least about <NUM> (<NUM> °F), at least about <NUM> (<NUM> °F), at least about <NUM> (<NUM> °F), or at least about <NUM> (<NUM> °F). In some embodiments, the base oil has a smoke point less than about <NUM> (<NUM> °F), less than about <NUM> (<NUM> °F), or less than about <NUM> (<NUM> °F). In some embodiments, the base oil has a smoke point in a range of about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), or about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F). In some embodiments, the base oil is avocado oil (smoke point about <NUM> or <NUM> °F), canola oil (smoke point about <NUM> or <NUM> °F), coconut oil (smoke point about <NUM> or <NUM> °F), castor oil (smoke point about <NUM> or <NUM> °F), olive oil (smoke point about <NUM>-<NUM> or <NUM>-<NUM> °F), palm oil (smoke point about <NUM> or <NUM> °F), safflower oil (smoke point about <NUM> or <NUM> °F), or sunflower, high-oleic oil (smoke point about <NUM> or <NUM> °F). In some embodiments, the base oil is isopropyl myristate.

In some embodiments, the formulation for the lubricant comprises a phospholipid or an equivalent thereof. Illustratively, the phospholipid comprises a lecithin, a choline, lipid, or a combination thereof. In some embodiments, the lipid is hydrogenated. In some embodiments, the lecithin has been processed by acetylation, hydrogenation, phosphatidyl choline enrichment, or a combination thereof to improve heat resistance. In some embodiments, the lecithin is in the form of a liquid or a solid.

In some illustrative embodiments, the phospholipid comprises a compound according to formula IV
<CHM>
or a salt thereof. In some embodiments, each of R<NUM> and R<NUM> is independently C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, and C<NUM>-C<NUM> alkynyl is independently optionally substituted with halo, hydroxy, amino, oxo, or OR<NUM>. In illustrative embodiments, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM>. In some embodiments, the phospholipid or a salt thereof comprises at least one C<NUM>-C<NUM> alkyl. In some embodiments, the phospholipid or a salt thereof is substantially free from a C<NUM>-C<NUM> alkenyl.

The formulation for a lubricant may comprise a certain percentage of a phospholipid or salt thereof. The percentage of phospholipid or salt thereof for the formulation for a lubricant is at least about <NUM>%, at least about <NUM>%, at least about <NUM>%, or at least about <NUM>% by weight of the formulation. In some embodiments, the phospholipid or salt thereof is less than about <NUM>%, less than about <NUM>%, or less than about <NUM>% by weight of the formulation. In some embodiments, the phospholipid or salt thereof is about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. In some embodiments, the phospholipid or salt thereof is about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation.

In some embodiments, the formulation comprises a component that may promote or participate in the formation of a non-stick surface on the probe. In some embodiments, this component may be suspended in the formulation. In some embodiments, the formulation for the lubricant comprises a salt of the formula.

M<NUM>(R<NUM>)(R<NUM>) (calcium stearate)     (II).

In some embodiments, M<NUM> is a divalent cation. In some embodiments, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, -OC (O)C<NUM>-C<NUM> alkenyl, or -OC(O)C<NUM>-C<NUM> alkynyl. In some embodiments, each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>. In some embodiments, R<NUM> is independently H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl, - C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl. In some embodiments, the divalent cation is magnesium, calcium, or iron. In some embodiments, the salt of formula II comprises a stearate. In some embodiments, the salt of formula II is calcium stearate.

In some embodiments, M<NUM> is a monovalent cation and is associated with only one of R<NUM> or R<NUM>. In some embodiments, the formulation comprises a stearate. In some embodiments, the formulation comprises sodium stearate.

The formulation for a lubricant may comprise a certain percentage of the salt of formula II. The percentage of the salt of formula II for the formulation for a lubricant is at least about <NUM>%, at least about <NUM>%, at least about <NUM>%, or at least about <NUM>% by weight of the formulation. In some embodiments, the salt of formula II for the formulation for a lubricant is less than about <NUM>%, less than about <NUM>%, or less than about <NUM>% by weight of the formulation. In some embodiments, the salt of formula II is about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. In some embodiments, the salt of formula II is about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation.

In some embodiments, the formulation comprises a component that modifies the thickness of the formulation, the texture of the formulation, or both, while maintaining heat tolerance. In some embodiments, the formulation for a lubricant comprises a compound of formula V
<CHM>
or a salt thereof. In some embodiments, each of R<NUM>, R<NUM>, and R<NUM> is independently C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl. In some embodiments, each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with halo, hydroxy, amino, oxo, or OR<NUM>. In some embodiments, R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, and C<NUM>-C<NUM> alkynyl is independently optionally substituted with a halo, hydroxy, or an amino. In some embodiments, each of R<NUM>, R<NUM>, and R<NUM> is independently C<NUM>-C<NUM> alkyl or C<NUM>-C<NUM> alkenyl. In some embodiments, each of R<NUM>, R<NUM>, and R<NUM> is independently C<NUM>-C<NUM> alkyl. In some embodiments, the compound of formula V comprises a stearate. In some embodiments, the compound of formula V is glyceryl tristearate. In some embodiments, the compound of formula V is found in the base oil.

In some embodiments, the formulation for a lubricant comprises a saturated fatty acid. In some embodiments, the formulation for a lubricant comprises a myristic acid.

In some embodiments, the formulation comprises a long chain alcohol. Illustratively, the alcohol may be a primary alcohol or a secondary alcohol. Illustratively, the alcohol may be saturated or unsaturated. In some embodiments, the formulation comprises an alcohol of the formula HO(CH<NUM>)dCH<NUM>, where d is an integer from <NUM> to <NUM>. In some embodiments, the alcohol is stearyl alcohol. In some embodiments, the alcohol is cetyl alcohol.

The formulation for a lubricant may comprise a certain percentage of the compound of formula V, a long chain alcohol, a saturated fatty acid, or salts thereof. The percentage of compound of formula V, a long chain alcohol, a saturated fatty acid, or salts thereof for the formulation for a lubricant may be at least about <NUM>%, at least about <NUM>%, at least about <NUM>%, or at least about <NUM>% by weight of the formulation. In some embodiments, the compound of formula V, a long chain alcohol, a saturated fatty acid, or salts thereof for the formulation for a lubricant may be less than about <NUM>%, less than about <NUM>%, or less than about <NUM>% by weight of the formulation. In some embodiments, the compound of formula V, a long chain alcohol, a saturated fatty acid, or salts thereof is about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. In some embodiments, the compound of formula V, a long chain alcohol, a saturated fatty acid, or salts thereof is about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation.

In some embodiments, the formulation for the lubricant comprises a fragrance. In some embodiments, the fragrance comprises an essential oil. In some embodiments, the essential oil is mace essential oil.

The formulation may comprise a certain percentage by weight of the fragrance. In some embodiments, the fragrance is at least about <NUM> %, at least about <NUM>%, at least about <NUM>%, or at least about <NUM>% by weight of the formulation. In some embodiments, the fragrance is up to about <NUM>%, up to about <NUM>%, or up to about <NUM>% by weight of the formulation. The fragrance may be about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. The fragrance may be about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation.

In some embodiments, the formulation for the lubricant comprises at least one anti-oxidant. The anti-oxidant may provide protection for the fatty components against heat-degradation. In addition, the anti-oxidant may act as a preservative and may assist the body's healing processes. In some embodiments, the at least one anti-oxidant comprises a tocopherol or a lipoic acid. In some embodiments, the anti-oxidant comprises a blend of tocopherols. In some embodiments, the lipoic acid is an alpha-lipoic acid.

The formulation may comprise a certain percentage by weight of the at least one anti-oxidant. In some embodiments, the at least one anti-oxidant is at least about <NUM>% or at least about <NUM>% by weight of the formulation. In some embodiments, the at least one anti-oxidant is up to about <NUM>%, up to about <NUM>%, or up to about <NUM>% by weight of the formulation. The at least one anti-oxidant may be about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. The at least one anti-oxidant may be about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation.

In some embodiments, the formulation for the lubricant comprises at least one anti-inflammatory. In some embodiments, the at least one anti-inflammatory comprises a caryophyllene or a phyto-aromatic. In some embodiments, the phyto-aromatic comprises a terpene.

The formulation may comprise a certain percentage by weight of the at least one anti-inflammatory. In some embodiments, the at least one anti-inflammatory is at least about <NUM>% or at least <NUM>% by weight of the formulation. In some embodiments, the at least one anti-inflammatory is up to about <NUM>%, up to about <NUM>%, or up to about <NUM>% by weight of the formulation. The at least one anti-inflammatory may be about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, about <NUM>%, or about <NUM>% by weight of the formulation. The at least one anti-inflammatory may be about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, about <NUM>% to about <NUM>%, or about <NUM>% to about <NUM>% by weight of the formulation.

In some embodiments, the formulation may comprise a scented component. In some embodiments, the scented component is a fragrance oil. In some embodiments, the scented component is biocompatible. In some embodiments, the scented component is selected from the group consisting of hexyl acetate, fructone, ethyl methylphenylglycidate, and combinations thereof. In some embodiments, the scented component is hexyl acetate. In some embodiments, the scented component is fructone. In some embodiments, the scented component is ethyl methylphenylglycidate. In some embodiments, the scented component comprises a lactone. Additional disclosure related to scented components can be found in <CIT>.

Another aspect of the present disclosure is a method of preparing a formulation for a lubricant. Illustratively, the method may comprise heating a base oil, mixing the base oil with a compound of formula V, and mixing the base oil with a phospholipid.

In some embodiments, the step of heating comprises heating the base oil to a temperature of about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), or about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F).

In some embodiments, the step of mixing is performed by stirring at a rate of about <NUM> to about <NUM>,<NUM> RPMs, about <NUM> to about <NUM>,<NUM> RPMs, about <NUM> to about <NUM> RPMs, about <NUM> to about <NUM> RPMs, about <NUM> to about <NUM> RPMs, or about <NUM> to about <NUM> RPMs. In some embodiments, the step of mixing the base oil with the compound of formula V occurs before the step of mixing the base oil with the phospholipid.

In some embodiments, the method comprises mixing at least one antioxidant, at least one anti-inflammatory, or a mixture of both with the base oil. In some embodiments, the step of mixing produces a suspension.

In some embodiments, the method further comprises de-gassing the suspension. Illustratively, the step of de-gassing may be performed by applying a vacuum to the suspension.

In some illustrative embodiments, the method further comprises a cooling the suspension to a temperature of about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F). In some embodiments, the suspension is de-gassed prior to cooling.

In some embodiments, the method comprising mixing the cooled suspension with a fragrance, at least one anti-oxidant, at least one anti-inflammatory, or a mixture thereof.

Illustratively, stearic acid is a fully saturated fat and esterified stearic acid may be a primary component of avocado oil. Adding glyceryl tristearate to a base oil comprising stearic acid may modify the thickness of the oil and calibrate it to a desired texture while retaining the high-heat tolerance. These properties may allow for greater self-healing. In some illustrative embodiments, the formulation comprises hydrogenated phosphatidylcholine. In some embodiments, the formulation comprises d-alpha tocopherol oil, which may provide protection for the fatty components against heat-degradation. This protection may be due to its potent anti-oxidant properties, which may also allow it to act as a preservative and may assist the body's healing processes. In some illustrative embodiments, these four components may comprise a first-phase of the non-stick mechanism. Illustratively, these components may provide improved thermal stability and survive a greater number of burns before degradation compared to a comparative lubricant. A possible benefit to an exemplary formulation may be a change in viscosity upon heating. A comparative lubricant remained relatively viscous even upon heating, which restricted its self-healing capacity on the probe. A formulation in accordance with the present disclosure readily flowed on the surface of the probe when heated, which may allow bare-spots to recover quickly. This is also marked by the observation of a large amount of comparative lubricant remaining on the probe even though it has been depleted on the working-side of the probe (see <FIG>). A lubricant in accordance with the present disclosure may become largely depleted off the probe, but thanks to the second-phase mechanism, it may continue to retain non-stick properties.

In some embodiments, the formulation may provide a second nonstick phase that may prolong the performance of the formulation and may be unrelated to the hydrophobic/hydrophilic nature of lecithin. The second phase may instead rely on the properties of a salt (e.g. calcium stearate) as an anti-caking, a mold-release agent, and a water-repelling agent. As a salt, this molecule may be able to tolerate immense amounts of heat before degrading and may be used throughout the food and pharmaceutical industry for mold-release and anti-caking applications. In some formulations in accordance with the present disclosure, the calcium stearate may be suspended in the solution and may become deposited onto the probe. As the fatty components of the formulation may be lost to heat, the calcium stearate may form a protective barrier on the probe, which may provide a non-stick surface that may be highly resilient against heat. Furthermore, the mix of fatty components in the new formulation may have less propensity to accumulate char, and so may be less susceptible to decreased performance after several cautery applications in comparison to a comparative lubricant. Instead, a relatively thin layer of residue is left behind which may minimally impede the transfer of energy from the probe to the tissue. Because the salt (e.g. calcium stearate) may be effective at preventing sticking, little additional residue accumulates with continued usage. Additionally, the amount of tissue adhering to the probe with some formulations in accordance with the present disclosure tended to be much smaller than what was typical of the original formulation (see <FIG>).

In some embodiments, the formulation comprises a fragrance, such as a fragrance oil. In some embodiments, the fragrance oil is mace oil and is derived from the aril of the nutmeg (M. Illustratively, mace oil may be preferred due to its availability, lack of known-allergens, low sensitization potential, strong-but-pleasing odor, and the high boiling point, which may allow it to persist for a long period before it, is depleted. Additionally, mace oil is of relatively low volatility compared to many other plant essential oils, which will facilitate the manufacturing process and minimize evaporative loss of oil due to the necessary heating of the product for bottling.

In some embodiments, the formulation for a lubricant comprises a phospholipid such as a fully hydrogenated phosphatidylcholine. In some illustrative embodiments, the phospholipid may be dissolved in a mix of saturated fats with high boiling points. In some embodiments, the base oil comprises avocado oil and the formulation comprises of glyceryl tristearate, which are both known for their unusually high smoke points and boiling points, respectively. Illustratively, using fully hydrogenated compounds may provide greater heat-stability.

A formulation for a lubricant included a base oil, a tristearate, a stearate salt, a phospholipid, an anti-oxidant, a fragrance, and an anti-inflammatory. The base oil was avocado oil, the tristearate was glyceryl tristearate, the stearate salt was calcium stearate, the phospholipid was hydrogenated phosphatidyl choline, the anti-oxidant was mixed tocopherol oil, the fragrance was mace essential oil, and the anti-inflammatory was beta-caryophyllene. The components were combined in the amounts described below via blending to prepare the lubricant.

The resulting lubricant was generally a liquid at room temperature and generally colorless.

The base oil (e.g. avocado) is added to a container under stirring of ~<NUM> - <NUM> RPMs and brought to a temperature of ~ <NUM> - <NUM> (~<NUM> °F - <NUM> °F). Secondly, with continued heating and stirring, the oil-soluble compounds are added in no specific order, including glyceryl tristearate and the tocopherols. Stirring and heating are continued until the components are generally dissolved. Next, calcium stearate and hydrogenated phosphatidylcholine are added to create a suspension and stirring is continued. The heat is reduced to allow the mixture to slowly cool while stirring is continued. At this stage, a de-gassing vacuum-procedure may be conducted in order to remove small air-bubbles that may have become entrapped during the stirring and additions.

Once the mixture has cooled to about <NUM> (<NUM> °F) to about <NUM> (<NUM> °F), the caryophyllenes and mace oil are added. Heat is removed, but stirring continues until the mixture has fallen to about <NUM> (<NUM> °F), whereupon stirring can cease and the mixture is allowed to set into its final cream-lie consistency.

Application to the electrocautery tips consists of a simple dipping of the probe into a reservoir of a formulation according to Example <NUM> or <NUM>, followed by a gentle shaking or tapping of the probe to loosen any excess. Wiping will also be possible, as in the case of the current Electro-Lube formulation.

The following experimental conditions were devised to compare the performance of a comparative lubricant formulation against the formulation prepared in Example <NUM> accordance with the present disclosure. A stainless-steel spatula probe was evenly coated in either a comparative lubricant (Electro-Lube®) or the lubricant of Example <NUM> (see <FIG>) and was subjected to repeated coagulation electrocautery at full power against the "skin-side" of a fresh chicken breast. The probe was positioned against the surface of the chicken in a manner that generated continuous arcing between the probe and flesh, and lasted about <NUM>-<NUM> seconds each. After each burn, the probe was moved to an adjacent un-affected area and repeated (see <FIG>). This continued until flesh adhered to the probe, at which point the trial was considered complete. The number of burns achieved was recorded, and the probe was photographed for documentation. The probe was then cleaned using a wire-wheel and wiped. The same probe was used for all trials. Eleven trials were conducted each for the original and revised formula.

Data was analyzed with a Welch's t-test using the statistics program R, see <FIG>. The number of burns per application was greater when using the lubricant of Example <NUM> (M = <NUM>, SD= <NUM>) than the comparative lubricant (M = <NUM>, SD= <NUM>). This difference is statistically significant (t(<NUM>) = -<NUM>, p<<NUM>), confirming that the lubricant of Example <NUM> confers on average an additional <NUM> electrocautery burns per application.

The lubricant for this example was Electrolube® available from Mectra Labs.

A formulation for a lubricant the following components. The components were combined as described above in the amounts described below to prepare the lubricant.

A formulation for a lubricant included the following components. The components were combined as described above in the amounts described below to prepare the lubricant.

The lubricants described in Examples <NUM>-<NUM> were tested as described in Example <NUM>. The results are shown in <FIG>.

A formulation for a lubricant included a base oil, a tristearate, and a fragrance. The components were combined in the amounts described below via blending to prepare the lubricant.

The liquid lecithin was heated to about <NUM> (<NUM> °F) and the stearin is added. The mixture is then stirred at temp until the stearin has fully dissolved. Then the temp is lowered to about <NUM> - about <NUM> (<NUM> °F - about <NUM> °F) where the fragrance oil is added before letting cool to room temp.

Claim 1:
A formulation for a lubricant comprising
a base oil, in a range of from <NUM>% by weight to <NUM>% by weight of the formulation and comprising a compound of the formula I
<CHM>
wherein R<NUM> is H, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>; R<NUM> is C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with hydroxy, or OR<NUM>;
a phospholipid, or a salt thereof, in a range from <NUM>% by weight to <NUM>% by weight of the formulation; and
<NUM>% by weight to <NUM>% by weight of the formulation of a salt of the formula

        M<NUM>(R<NUM>)(R<NUM>)     (II)

wherein M<NUM> is a divalent cation, R<NUM> and R<NUM> are independently -OC(O)C<NUM>-C<NUM> alkyl, - OC(O)C<NUM>-C<NUM> alkenyl, or - OC(O)C<NUM>-C<NUM> alkynyl, and wherein each hydrogen atom in C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, or C<NUM>-C<NUM> alkynyl is independently optionally substituted with OR<NUM>,
wherein each of R<NUM>, R<NUM>, and R<NUM> is independently H, C<NUM>-C<NUM> alkyl , C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, C<NUM>-C<NUM> alkyl, C<NUM>-C<NUM> alkenyl, C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, - C(O)C<NUM>-C<NUM> alkynyl, -C(O)C<NUM>-C<NUM> alkyl, -C(O)C<NUM>-C<NUM> alkenyl, -C(O)C<NUM>-C<NUM> alkynyl.