Claims
- 1. A pharmaceutical combination useful for treating exposure to a cholinesterase inhibitor, the pharmaceutical combination comprising:
a 2-PAM cation or a source of a 2-PAM cation; and a facilitating anion or a source of a facilitating anion, wherein: the facilitating anion is less hydrophilic than a chloride anion; and the 2-PAM cation or the source of the 2-PAM cation and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 2. A pharmaceutical combination as set forth in claim 1 wherein the combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the 2-PAM cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 3. A pharmaceutical combination as set forth in claim 2, wherein said combination further comprises an anti-cholinergic agent.
- 4. A pharmaceutical combination as set forth in claim 3, wherein said anti-cholinergic agent comprises atropine.
- 5. A pharmaceutical combination as set forth in claim 2, wherein said combination further comprises a neutralizing agent.
- 6. A pharmaceutical combination as set forth in claim 5, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 7. A pharmaceutical combination as set forth in claim 5, wherein said combination further comprises a buffering agent.
- 8. A pharmaceutical combination as set forth in claim 7, wherein said buffering agent comprises citric acid.
- 9. A pharmaceutical combination as set forth in claim 2, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 10. A pharmaceutical combination as set forth in claim 2 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 0.5 to about 2.
- 11. A pharmaceutical combination as set forth in claim wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 1.0 to about 1.5.
- 12. A pharmaceutical combination as set forth in claim wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 1.0 to about 1.1.
- 13. A pharmaceutical combination as set forth in claim 2, wherein, when the combination is orally administered to a human, the 2-PAM cation is absorbed into the bloodstream from the gastrointestinal tract.
- 14. A pharmaceutical combination as set forth in claim 2, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 15. A pharmaceutical composition as set forth in claim 14, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 16. A pharmaceutical composition as set forth in claim 15, wherein said facilitating anion comprises salicylate.
- 17. A pharmaceutical combination as set forth in claim 32, wherein said combination comprises a compound which comprises both said 2-PAM cation and said facilitating anion.
- 18. A pharmaceutical combination as set forth in claim 2, wherein said combination comprises 2-PAM di(2-ethylhexyl)sulfosuccinate, 2-PAM salicylate, 2-PAM acetylsalicylate, 2-PAM lauryl sulfate, 2-PAM di(2-ethylhexyl) phosphate, or 2-PAM hexadecylsulfonate.
- 19. A pharmaceutical combination as set forth in claim 2, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 20. A pharmaceutical combination as set forth in claim 2, wherein said combination is in a form comprising a tablet or a capsule.
- 21. A pharmaceutical combination as set forth in claim 2, wherein said combination is in a form comprising a solution or suspension.
- 22. A pharmaceutical combination as set forth in claim 2, wherein said combination is in a form suitable for administering via injection.
- 23. A pharmaceutical combination as set forth in claim 22, wherein said combination is suitable for intravenous or intramuscular injection.
- 24. A pharmaceutical combination as set forth in claim 22 further comprising a buffer.
- 25. A pharmaceutical combination as set forth in claim 24 further comprising a bulking, dispersing, wetting or suspending agent.
- 26. A pharmaceutical combination as set forth in claim 2, wherein said combination comprises a pharmaceutical composition comprising:
0.5% to 60% 2-PAM cation, and 0.3% to 60% facilitating anion.
- 27. A pharmaceutical combination as set forth in claim 26, wherein said combination further comprises 0.02% to 99% of a neutralizing agent and/or buffering agent.
- 28. A pharmaceutical combination as set forth in claim 2, wherein said combination comprises a pharmaceutical composition comprising:
5% to 20% 2-PAM cation, and 15% to 45% facilitating anion.
- 29. A pharmaceutical combination as set forth in claim 28, wherein said combination further comprises 35% to 80% of a neutralizing agent and/or buffering agent.
- 30. A pharmaceutical combination as set forth in claims 1-2, wherein said combination comprises a pharmaceutical composition comprising:
10% to 15% 2-PAM cation, and 30% to 40% facilitating anion.
- 31. A pharmaceutical combination as set forth in claim 30, wherein said combination further comprises 45% to 60% of a neutralizing agent and/or buffering agent.
- 32. A pharmaceutical combination as set forth in claim 1 wherein the combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the source of the 2-PAM cation and the source of the facilitating anion together are present in the pharmaceutical kit in a therapeutically effective amount.
- 33. A pharmaceutical combination as set forth in claim 32, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said 2-PAM cation and said facilitating anion.
- 34. A pharmaceutical combination as set forth in claim 32, wherein said combination further comprises a source of an anti-cholinergic agent, a neutralizing agent and/or a buffering agent.
- 35. A pharmaceutical combination as set forth in claim 34, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the 2-PAM cation, the facilitating anion, and the anti-cholinergic agent, neutralizing agent and/or buffering agent.
- 36. A pharmaceutical combination as set forth in claim 32, wherein said pharmaceutical kit further comprises a source of a neutralizing agent and a source of a buffering agent.
- 37. A pharmaceutical combination as as set forth in claim 36 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 38. A pharmaceutical combination as set forth in claim 37 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 39. A pharmaceutical combination as set forth in claim 32, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 40. A pharmaceutical combination as set forth in claim 1, wherein the pharmaceutical combination comprises:
a 2-PAM cation or a source of a 2-PAM cation; and a facilitating anion or a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the 2-PAM cation or the source of the 2-PAM cation and the facilitating anion or the source of the facilitating anion are, in combination, suitable for oral ingestion; the 2-PAM cation or the source of the 2-PAM cation and the facilitating anion or the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the 2-PAM cation or the source of the 2-PAM cation and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 41. A pharmaceutical combination as set forth in claim 40 wherein the combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the 2-PAM cation and the facilitating anion are, in combination, suitable for oral ingestion; the 2-PAM cation and the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the 2-PAM cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 42. A pharmaceutical combination as set forth in claim 41, wherein said combination further comprises an anti-cholinergic agent.
- 43. A pharmaceutical combination as set forth in claim 42, wherein said anti-cholinergic agent comprises atropine.
- 44. A pharmaceutical combination as set forth in claim 41, wherein said combination further comprises a neutralizing agent.
- 45. A pharmaceutical combination as set forth in claim 44, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 46. A pharmaceutical combination as set forth in claim 44, wherein said combination further comprises a buffering agent.
- 47. A pharmaceutical combination as set forth in claim 46, wherein said buffering agent comprises citric acid.
- 48. A pharmaceutical combination as set forth in claim 41, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 49. A pharmaceutical combination as set forth in claim 41 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 0.5 to about 2.
- 50. A pharmaceutical combination as set forth in claim 49 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 1.0 to about 1.5.
- 51. A pharmaceutical combination as set forth in claim 49 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 1.0 to about 1.1.
- 52. A pharmaceutical combination as set forth in claim 41, wherein, when the combination is orally administered to a human, the 2-PAM cation is absorbed into the bloodstream from the gastrointestinal tract.
- 53. A pharmaceutical combination as set forth in claim 41, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 54. A pharmaceutical composition as set forth in claim 53, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 55. A pharmaceutical composition as set forth in claim 54, wherein said facilitating anion comprises salicylate.
- 56. A pharmaceutical combination as set forth in claim 41, wherein said combination comprises a compound which comprises both said 2-PAM cation and said facilitating anion.
- 57. A pharmaceutical combination as set forth in claim 41, wherein said combination comprises 2-PAM di(2-ethylhexyl)sulfosuccinate, 2-PAM salicylate, 2-PAM acetylsalicylate, 2-PAM lauryl sulfate, 2-PAM di(2-ethylhexyl) phosphate, or 2-PAM hexadecylsulfonate.
- 58. A pharmaceutical combination as set forth in claim 41, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 59. A pharmaceutical combination as set forth in claim 41, wherein said combination is in a form comprising a tablet or a capsule.
- 60. A pharmaceutical combination as set forth in claim 41, wherein said combination is in a form comprising a solution or suspension.
- 61. A pharmaceutical combination as set forth in claim 41, wherein said combination is in a form suitable for administering via injection.
- 62. A pharmaceutical combination as set forth in claim 61, wherein said combination is suitable for intravenous or intramuscular injection.
- 63. A pharmaceutical combination as set forth in claim 61 further comprising a buffer.
- 64. A pharmaceutical combination as set forth in claim 63 further comprising a bulking, dispersing, wetting or suspending agent.
- 65. A pharmaceutical combination as set forth in claim 41, wherein said combination comprises a pharmaceutical composition comprising:
0.5% to 60% 2-PAM cation, and 0.3% to 60% facilitating anion.
- 66. A pharmaceutical combination as set forth in claim 65, wherein said combination further comprises 0.02% to 99% of a neutralizing agent and/or buffering agent.
- 67. A pharmaceutical combination as set forth in claim 41, wherein said combination comprises a pharmaceutical composition comprising:
5% to 20% 2-PAM cation, and 15% to 45% facilitating anion.
- 68. A pharmaceutical combination as set forth in claim 67, wherein said combination further comprises 35% to 80% of a neutralizing agent and/or buffering agent.
- 69. A pharmaceutical combination as set forth in claim 41, wherein said combination comprises a pharmaceutical composition comprising:
10% to 15% 2-PAM cation, and 30% to 40% facilitating anion.
- 70. A pharmaceutical combination as set forth in claim 69, wherein said combination further comprises 45% to 60% of a neutralizing agent and/or buffering agent.
- 71. A pharmaceutical combination as set forth in claim 40 wherein the combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the source of the 2-PAM cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the 2-PAM cation and the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the 2-PAM cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 72. A pharmaceutical combination as set forth in claim 71, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said 2-PAM cation and said facilitating anion.
- 73. A pharmaceutical combination as set forth in claim 71, wherein said combination further comprises a source of an anti-cholinergic agent, a neutralizing agent and/or a buffering agent.
- 74. A pharmaceutical combination as set forth in claim 73, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the 2-PAM cation, the facilitating anion, and the anti-cholinergic agent, neutralizing agent and/or buffering agent.
- 75. A pharmaceutical combination as set forth in claim 71, wherein said pharmaceutical kit further comprises a source of a neutralizing agent and a source of a buffering agent.
- 76. A pharmaceutical combination as set forth in claim 75 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 77. A pharmaceutical combination as set forth in claim 76 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 78. A pharmaceutical combination as set forth in claim 71, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 79. A pharmaceutical combination useful for treating exposure to a cholinesterase inhibitor, the pharmaceutical combination comprising:
a 2-PAM cation or a source of a 2-PAM cation; and an anion or a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 3a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 80. A pharmaceutical combination as set forth in claim 79 wherein the combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; and an anion comprising an anion selected from the group consisting of: 4a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R3, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 81. A pharmaceutical combination as set forth in claim 80, wherein the anion comprises R1OSO3− and R1 is hydrocarbyl or substituted hydrocarbyl.
- 82. A pharmaceutical combination as set forth in claim 81, wherein R1 is hydrocarbyl.
- 83. A pharmaceutical combination as set forth in claim 80, wherein the anion comprises the formula:
- 84. A pharmaceutical combination as set forth in claim 83, wherein R1 is hydrocarbyl.
- 85. A pharmaceutical combination as set forth in claim 80 wherein the anion comprises a compound having the formula:
- 86. A pharmaceutical combination as set forth in claim 85, wherein R17 is hydrocarbyl and R18 is hydrogen.
- 87. A pharmaceutical combination as set forth in claim 85, wherein the pharmaceutical combination comprises aspirin.
- 88. A pharmaceutical combination as set forth in claim 85, wherein the pharmaceutical composition is in a form suitable for administering orally.
- 89. A pharmaceutical combination as set forth in claim 79 wherein the combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; and a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 7a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 90. A pharmaceutical combination as set forth in claim 89, wherein the anion comprises R1OSO3− and R1 is hydrocarbyl or substituted hydrocarbyl.
- 91. A pharmaceutical combination as set forth in claim 90, wherein R1 is hydrocarbyl.
- 92. A pharmaceutical combination as set forth in claim 89, wherein the anion comprises a compound having the formula:
- 93. A pharmaceutical combination as set forth in claim 92, wherein R1 is hydrocarbyl.
- 94. A pharmaceutical combination as set forth in claim 89, wherein the anion comprises a compound having the formula:
- 95. A pharmaceutical combination as set forth in claim 94, wherein R17 is hydrocarbyl and R18 is hydrogen.
- 96. A pharmaceutical combination as set forth in claim 89, wherein the pharmaceutical kit comprises aspirin.
- 97. A pharmaceutical combination as set forth in claim 89, wherein the components of the pharmaceutical kit are each in a form suitable for administering orally.
- 98. A pharmaceutical combination useful for treating exposure to a cholinesterase inhibitor, the pharmaceutical combination comprising:
a 2-PAM cation or a source of a 2-PAM cation; a facilitating anion or a source of a facilitating anion; and an anticholinergic agent or a source of an anticholinergic agent, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the 2-PAM cation or the source of the 2-PAM cation and the facilitating anion or the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the 2-PAM cation or the source of the 2-PAM cation, the facilitating anion or the source of the facilitating anion and the anticholinergic agent or the source of the anticholinergic agent together are present in the pharmaceutical combination in a therapeutically effective amount.
- 99. A pharmaceutical combination as set forth in claim 98 wherein the combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; a facilitating anion; and an anticholinergic agent, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the 2-PAM cation and the facilitating anion are, in combination, suitable for oral ingestion; the 2-PAM cation and the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the 2-PAM cation, the facilitating anion and the anticholinergic agent together are present in the pharmaceutical combination in a therapeutically effective amount.
- 100. A pharmaceutical combination as set forth in claim 99, wherein said anti-cholinergic agent comprises atropine.
- 101. A pharmaceutical combination as set forth in claim 99, wherein said combination further comprises a neutralizing agent.
- 102. A pharmaceutical combination as set forth in claim 101, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 103. A pharmaceutical combination as set forth in claim 101, wherein said combination further comprises a buffering agent.
- 104. A pharmaceutical combination as set forth in claim 103, wherein said buffering agent comprises citric acid.
- 105. A pharmaceutical combination as set forth in claim 99, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 106. A pharmaceutical combination as set forth in claim 99 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 0.5 to about 2.
- 107. A pharmaceutical combination as set forth in claim 106 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 1.0 to about 1.5.
- 108. A pharmaceutical combination as set forth in claim 106 wherein the molar ratio of said facilitating anion to said 2-PAM cation is from about 1.0 to about 1.1.
- 109. A pharmaceutical combination as set forth in claim 99, wherein, when the combination is orally administered to a human, the 2-PAM cation is absorbed into the bloodstream from the gastrointestinal tract.
- 110. A pharmaceutical combination as set forth in claim 99, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 111. A pharmaceutical composition as set forth in claim 110, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 112. A pharmaceutical composition as set forth in claim 111, wherein said facilitating anion comprises salicylate.
- 113. A pharmaceutical combination as set forth in claim 99, wherein said combination comprises a compound which comprises both said 2-PAM cation and said facilitating anion.
- 114. A pharmaceutical combination as set forth in claim 99, wherein said combination comprises 2-PAM di(2-ethylhexyl)sulfosuccinate, 2-PAM salicylate, 2-PAM acetylsalicylate, 2-PAM lauryl sulfate, 2-PAM di(2-ethylhexyl) phosphate, or 2-PAM hexadecylsulfonate.
- 115. A pharmaceutical combination as set forth in claim 99, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 116. A pharmaceutical combination as set forth in claim 99, wherein said combination is in a form comprising a tablet or a capsule.
- 117. A pharmaceutical combination as set forth in claim 99, wherein said combination is in a form comprising a solution or suspension.
- 118. A pharmaceutical combination as set forth in claim 99, wherein said combination is in a form suitable for administering via injection.
- 119. A pharmaceutical combination as set forth in claim 118, wherein said combination is suitable for intravenous or intramuscular injection.
- 120. A pharmaceutical combination as set forth in claim 118 further comprising a buffer.
- 121. A pharmaceutical combination as set forth in claim 120 further comprising a bulking, dispersing, wetting or suspending agent.
- 122. A pharmaceutical combination as set forth in claim 99, wherein said combination comprises a pharmaceutical composition comprising:
0.5% to 60% 2-PAM cation, and 0.3% to 60% facilitating anion.
- 123. A pharmaceutical combination as set forth in claim 122, wherein said combination further comprises 0.02% to 99% of a neutralizing agent and/or buffering agent.
- 124. A pharmaceutical combination as set forth in claim 99, wherein said combination comprises a pharmaceutical composition comprising:
5% to 20% 2-PAM cation, and 15% to 45% facilitating anion.
- 125. A pharmaceutical combination as set forth in claim 124, wherein said combination further comprises 35% to 80% of a neutralizing agent and/or buffering agent.
- 126. A pharmaceutical combination as set forth in claim 99, wherein said combination comprises a pharmaceutical composition comprising:
10% to 15% 2-PAM cation, and 30% to 40% facilitating anion.
- 127. A pharmaceutical combination as set forth in claim 126, wherein said combination further comprises 45% to 60% of a neutralizing agent and/or buffering agent.
- 128. A pharmaceutical combination as set forth in claim 98 wherein the combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; a source of a facilitating anion; and a source of an anticholinergic agent, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the source of the 2-PAM cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the 2-PAM cation and the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the 2-PAM cation, the source of the facilitating anion and the source of the anticholinergic agent together are present in the pharmaceutical combination in a therapeutically effective amount.
- 129. A pharmaceutical combination as set forth in claim 128, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said 2-PAM cation and said facilitating anion.
- 130. A pharmaceutical combination as set forth in claim 128, wherein said combination further comprises a source of a neutralizing agent and/or a buffering agent.
- 131. A pharmaceutical combination as set forth in claim 130, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the 2-PAM cation, the facilitating anion, and the anti-cholinergic agent, neutralizing agent and/or buffering agent.
- 132. A pharmaceutical combination as set forth in claim 128, wherein said pharmaceutical kit further comprises a source of a neutralizing agent and a source of a buffering agent.
- 133. A pharmaceutical combination as as set forth in claim 132 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 134. A pharmaceutical combination as set forth in claim 133 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 135. A pharmaceutical combination as set forth in claim 128, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 136. A method of treating exposure to a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 1 to a subject in need thereof.
- 137. A method as set forth in claim 136 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the 2-PAM cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 138. A method as set forth in claim 136 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the source of the 2-PAM cation and the source of the facilitating anion together are present in the pharmaceutical kit in a therapeutically effective amount.
- 139. A method of treating exposure to a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 40 to a subject in need thereof.
- 140. A method as set forth in claim 139 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the 2-PAM cation and the facilitating anion are, in combination, suitable for oral ingestion; the 2-PAM cation and the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the 2-PAM cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 141. A method as set forth in claim 139 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the source of the 2-PAM cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the 2-PAM cation and the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the the source of the 2-PAM cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the 2-PAM cation and the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the 2-PAM cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 142. A method of treating exposure to a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 79 to a subject in need thereof.
- 143. A method as set forth in claim 142 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; and a anion selected from the group consisting of: 10a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 144. A method as set forth in claim 142 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; and a source of a anion, wherein:
the anion comprises an anion selected from the group consisting of: 11a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 145. A method of treating exposure to a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 98 to a subject in need thereof.
- 146. A method as set forth in claim 145 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a 2-PAM cation; a facilitating anion; and an anticholinergic agent, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the 2-PAM cation and the facilitating anion are, in combination, suitable for oral ingestion; the 2-PAM cation and the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the 2-PAM cation, the facilitating anion and the anticholinergic agent together are present in the pharmaceutical combination in a therapeutically effective amount.
- 147. A method as set forth in claim 145 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a 2-PAM cation; a source of a facilitating anion; and a source of an anticholinergic agent, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the source of the 2-PAM cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the 2-PAM cation and the source of the facilitating anion are capable of forming a mixture comprising a 2-PAM cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the 2-PAM cation, the source of the facilitating anion and the source of the anticholinergic agent together are present in the pharmaceutical combination in a therapeutically effective amount.
- 148. A pharmaceutical combination useful for potentiating clearance of a cholinesterase inhibitor, the pharmaceutical combination comprising:
a pyridostigmine cation or a source of a pyridostigmine cation; and a facilitating anion or a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the pyridostigmine cation or the source of the pyridostigmine cation and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 149. A pharmaceutical combination as set forth in claim 148 wherein the combination comprises a pharmaceutical composition comprising:
a pyridostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the pyridostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 150. A pharmaceutical combination as set forth in claim 149, wherein said combination further comprises a neutralizing agent.
- 151. A pharmaceutical combination as set forth in claim 150, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 152. A pharmaceutical combination as set forth in claim 150, wherein said combination further comprises a buffering agent.
- 153. A pharmaceutical combination as set forth in claim 152, wherein said buffering agent comprises citric acid.
- 154. A pharmaceutical combination as set forth in claim 149, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 155. A pharmaceutical combination as set forth in claim 149 wherein the molar ratio of said facilitating anion to said pyridostigmine cation is from about 0.5 to about 2.
- 156. A pharmaceutical combination as set forth in claim 155 wherein the molar ratio of said facilitating anion to said pyridostigmine cation is from about 1.0 to about 1.5.
- 157. A pharmaceutical combination as set forth in claim 155 wherein the molar ratio of said facilitating anion to said pyridostigmine cation is from about 1.0 to about 1.1.
- 158. A pharmaceutical combination as set forth in claim 149, wherein, when the combination is orally administered to a human, the pyridostigmine cation is absorbed into the bloodstream from the gastrointestinal tract.
- 159. A pharmaceutical combination as set forth in claim 149, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 160. A pharmaceutical composition as set forth in claim 159, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 161. A pharmaceutical composition as set forth in claim 160, wherein said facilitating anion comprises salicylate.
- 162. A pharmaceutical combination as set forth in claim 149, wherein said combination comprises a compound which comprises both said pyridostigmine cation and said facilitating anion.
- 163. A pharmaceutical combination as set forth in claim 149, wherein said combination comprises pyridostigmine di(2-ethylhexyl)sulfosuccinate, pyridostigmine salicylate, pyridostigmine acetylsalicylate, pyridostigmine lauryl sulfate, pyridostigmine di(2-ethylhexyl) phosphate, or pyridostigmine hexadecylsulfonate.
- 164. A pharmaceutical combination as set forth in claim 149, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 165. A pharmaceutical combination as set forth in claim 149, wherein said combination is in a form comprising a tablet or a capsule.
- 166. A pharmaceutical combination as set forth in claim 149, wherein said combination is in a form comprising a solution or suspension.
- 167. A pharmaceutical combination as set forth in claim 149, wherein said combination is in a form suitable for administering via injection.
- 168. A pharmaceutical combination as set forth in claim 167, wherein said combination is suitable for intravenous or intramuscular injection.
- 169. A pharmaceutical combination as set forth in claim 167 further comprising a buffer.
- 170. A pharmaceutical combination as set forth in claim 169 further comprising a bulking, dispersing, wetting or suspending agent.
- 171. A pharmaceutical combination as set forth in claim 149, wherein said combination comprises a pharmaceutical composition comprising:
1% to 60% pyridostigmine cation, and 1% to 60% facilitating anion.
- 172. A pharmaceutical combination as set forth in claim 171, wherein said composition further comprises 0.01% to 90% neutralizing agent and/or buffering agent.
- 173. A pharmaceutical combination as set forth in claim 148 wherein the combination comprises a pharmaceutical kit comprising:
a source of a pyridostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the source of the pyridostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 174. A pharmaceutical combination as set forth in claim 173, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said pyridostigmine cation and said facilitating anion.
- 175. A pharmaceutical combination as set forth in claim 173, wherein said combination further comprises a source of a neutralizing agent and/or a buffering agent.
- 176. A pharmaceutical combination as set forth in claim 175, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the pyridostigmine cation, the facilitating anion, and the neutralizing agent and/or buffering agent.
- 177. A pharmaceutical combination as set forth in claim 175 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 178. A pharmaceutical combination as set forth in claim 177 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 179. A pharmaceutical combination as set forth in claim 173, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 180. A pharmaceutical combination as set forth in claim 148, the pharmaceutical combination comprising:
a pyridostigmine cation or a source of a pyridostigmine cation; and a facilitating anion or a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the pyridostigmine cation or the source of the pyridostigmine cation and the facilitating anion or the source of the facilitating anion are, in combination, suitable for oral ingestion; the pyridostigmine cation or the source of the pyridostigmine cation and the facilitating anion or the source of the facilitating anion are capable of forming a mixture comprising a pyridostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the pyridostigmine cation or the source of the pyridostigmine cation and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 181. A pharmaceutical combination as set forth in claim 180 wherein the combination comprises a pharmaceutical composition comprising:
a pyridostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the pyridostigmine cation and the facilitating anion are, in combination, suitable for oral ingestion; the pyridostigmine cation and the facilitating anion are capable of forming a mixture comprising a pyridostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the pyridostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 182. A pharmaceutical combination as set forth in claim 181, wherein said combination further comprises a neutralizing agent.
- 183. A pharmaceutical combination as set forth in claim 182, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 184. A pharmaceutical combination as set forth in claim 182, wherein said combination further comprises a buffering agent.
- 185. A pharmaceutical combination as set forth in claim 184, wherein said buffering agent comprises citric acid.
- 186. A pharmaceutical combination as set forth in claim 181, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 187. A pharmaceutical combination as set forth in claim 181 wherein the molar ratio of said facilitating anion to said pyridostigmine cation is from about 0.5 to about 2.
- 188. A pharmaceutical combination as set forth in claim 187 wherein the molar ratio of said facilitating anion to said pyridostigmine cation is from about 1.0 to about 1.5.
- 189. A pharmaceutical combination as set forth in claim 187 wherein the molar ratio of said facilitating anion to said pyridostigmine cation is from about 1.0 to about 1.1.
- 190. A pharmaceutical combination as set forth in claim 181, wherein, when the combination is orally administered to a human, the pyridostigmine cation is absorbed into the bloodstream from the gastrointestinal tract.
- 191. A pharmaceutical combination as set forth in claim 181, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 192. A pharmaceutical composition as set forth in claim 191, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 193. A pharmaceutical composition as set forth in claim 192, wherein said facilitating anion comprises salicylate.
- 194. A pharmaceutical combination as set forth in claim 181, wherein said combination comprises a compound which comprises both said pyridostigmine cation and said facilitating anion.
- 195. A pharmaceutical combination as set forth in claim 181, wherein said combination comprises pyridostigmine di(2-ethylhexyl)sulfosuccinate, pyridostigmine salicylate, pyridostigmine acetylsalicylate, pyridostigmine lauryl sulfate, pyridostigmine di(2-ethylhexyl) phosphate, or pyridostigmine hexadecylsulfonate.
- 196. A pharmaceutical combination as set forth in claim 181, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 197. A pharmaceutical combination as set forth in claim 181, wherein said combination is in a form comprising a tablet or a capsule.
- 198. A pharmaceutical combination as set forth in claim 181, wherein said combination is in a form comprising a solution or suspension.
- 199. A pharmaceutical combination as set forth in claim 181, wherein said combination is in a form suitable for administering via injection.
- 200. A pharmaceutical combination as set forth in claim 199, wherein said combination is suitable for intravenous or intramuscular injection.
- 201. A pharmaceutical combination as set forth in claim 199 further comprising a buffer.
- 202. A pharmaceutical combination as set forth in claim 201 further comprising a bulking, dispersing, wetting or suspending agent.
- 203. A pharmaceutical combination as set forth in claim 181, wherein said combination comprises a pharmaceutical composition comprising:
1% to 60% pyridostigmine cation, and 1% to 60% facilitating anion.
- 204. A pharmaceutical combination as set forth in claim 203, wherein said composition further comprises 0.01% to 90% neutralizing agent and/or buffering agent.
- 205. A pharmaceutical combination as set forth in claim 180 wherein the combination comprises a pharmaceutical kit comprising:
a source of a pyridostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the source of the pyridostigmine cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the pyridostigmine cation and the source of the facilitating anion are capable of forming a mixture comprising a pyridostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the pyridostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 206. A pharmaceutical combination as set forth in claim 204, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said pyridostigmine cation and said facilitating anion.
- 207. A pharmaceutical combination as set forth in claim 204, wherein said combination further comprises a source of a neutralizing agent and/or a buffering agent.
- 208. A pharmaceutical combination as set forth in claim 207, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the pyridostigmine cation, the facilitating anion, and the neutralizing agent and/or buffering agent.
- 209. A pharmaceutical combination as set forth in claim 207 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 210. A pharmaceutical combination as set forth in claim 209 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 211. A pharmaceutical combination as set forth in claim 204, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 212. A pharmaceutical combination useful for potentiating clearance of a cholinesterase inhibitor, the pharmaceutical combination comprising:
a pyridostigmine cation or a source of a pyridostigmine cation; and an anion or a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 12a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 213. A pharmaceutical combination as set forth in claim 212 wherein the combination comprises a pharmaceutical composition comprising:
a pyridostigmine cation and an anion comprising an anion selected from the group consisting of: 13a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 214. A pharmaceutical combination as set forth in claim 213, wherein the anion comprises R1OSO3− and R1 is hydrocarbyl or substituted hydrocarbyl.
- 215. A pharmaceutical combination as set forth in claim 214, wherein R1 is hydrocarbyl.
- 216. A pharmaceutical combination as set forth in claim 213, wherein the anion comprises the formula:
- 217. A pharmaceutical combination as set forth in claim 216, wherein R5 is hydrocarbyl.
- 218. A pharmaceutical combination as set forth in claim 213 wherein the anion comprises a compound having the formula:
- 219. A pharmaceutical combination as set forth in claim 218, wherein R17 is hydrocarbyl and R18 is hydrogen.
- 220. A pharmaceutical combination as set forth in claim 218, wherein the pharmaceutical combination comprises aspirin.
- 221. A pharmaceutical combination as set forth in claim 218, wherein the pharmaceutical composition is in a form suitable for administering orally.
- 222. A pharmaceutical combination as set forth in claim 212 wherein the combination comprises a pharmaceutical kit comprising:
a source of a pyridostigmine cation; and a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 16wherein R5 is hydrocarbyl or substituted hydrocarbyl.
- 226. A pharmaceutical combination as set forth in claim 92, wherein R5 is hydrocarbyl.
- 227. A pharmaceutical combination as set forth in claim 89, wherein the anion comprises a compound having the formula:
- 228. A pharmaceutical combination as set forth in claim 227, wherein R17 is hydrocarbyl and R18 is hydrogen.
- 229. A pharmaceutical combination as set forth in claim 222, wherein the pharmaceutical kit comprises aspirin.
- 223. A pharmaceutical combination as set forth in claim 222, wherein the anion comprises R1OSO3− and R1 is hydrocarbyl or substituted hydrocarbyl.
- 224. A pharmaceutical combination as set forth in claim 223, wherein R1 is hydrocarbyl.
- 225. A pharmaceutical combination as set forth in claim 222, wherein the anion comprises a compound having the formula:
- 230. A pharmaceutical combination as set forth in claim 222, wherein the components of the pharmaceutical kit are each in a form suitable for administering orally.
- 231. A pharmaceutical combination useful for potentiating clearance of a cholinesterase inhibitor, the pharmaceutical combination comprising:
a potentiating agent or a source of a potentiating agent; and a facilitating anion or a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the potentiating agent or the source of the potentiating agent and the facilitating anion or the source of the facilitating anion are, in combination, suitable for oral ingestion; the potentiating agent or the source of the potentiating agent and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount; and when the pharmaceutical combination is orally administered to a human, the potentiating agent is absorbed into the bloodstream from the gastrointestinal tract.
- 232. A pharmaceutical combination as set forth in claim 231 wherein said potentiating agent comprises a hydrophilic potentiating agent.
- 233. A pharmaceutical combination as set forth in claim 231 wherein said potentiating agent comprises a carbamate of a primary alcohol.
- 234. A pharmaceutical combination as set forth in claim 231 wherein said potentiating agent comprises a quaternary ammonium ion.
- 235. A pharmaceutical combination as set forth in claim 231 wherein said potentiating agent comprises pyridostigmine.
- 236. A pharmaceutical combination as set forth in claim 231, wherein the combination comprises a pharmaceutical composition comprising:
a potentiating agent; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the potentiating agent and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 237. A pharmaceutical combination as set forth in claim 236, wherein said combination further comprises a neutralizing agent.
- 238. A pharmaceutical combination as set forth in claim 237, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 239. A pharmaceutical combination as set forth in claim 237, wherein said combination further comprises a buffering agent.
- 240. A pharmaceutical combination as set forth in claim 239, wherein said buffering agent comprises citric acid.
- 241. A pharmaceutical combination as set forth in claim 236, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 242. A pharmaceutical combination as set forth in claim 236 wherein the molar ratio of said facilitating anion to said potentiating agent is from about 0.5 to about 2.
- 243. A pharmaceutical combination as set forth in claim 242 wherein the molar ratio of said facilitating anion to said potentiating agent is from about 1.0 to about 1.5.
- 244. A pharmaceutical combination as set forth in claim 242 wherein the molar ratio of said facilitating anion to said potentiating agent is from about 1.0 to about 1.1.
- 245. A pharmaceutical combination as set forth in claim 236, wherein, when the combination is orally administered to a human, the potentiating agent is absorbed into the bloodstream from the gastrointestinal tract.
- 246. A pharmaceutical combination as set forth in claim 236, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 247. A pharmaceutical composition as set forth in claim 246, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 248. A pharmaceutical composition as set forth in claim 247, wherein said facilitating anion comprises salicylate.
- 249. A pharmaceutical combination as set forth in claim 236, wherein said combination comprises a compound which comprises both said potentiating agent and said facilitating anion.
- 250. A pharmaceutical combination as set forth in claim 236, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 251. A pharmaceutical combination as set forth in claim 236, wherein said combination is in a form comprising a tablet or a capsule.
- 252. A pharmaceutical combination as set forth in claim 236, wherein said combination is in a form comprising a solution or suspension.
- 253. A pharmaceutical combination as set forth in claim 236, wherein said combination is in a form suitable for administering via injection.
- 254. A pharmaceutical combination as set forth in claim 253, wherein said combination is suitable for intravenous or intramuscular injection.
- 255. A pharmaceutical combination as set forth in claim 253 further comprising a buffer.
- 256. A pharmaceutical combination as set forth in claim 255 further comprising a bulking, dispersing, wetting or suspending agent.
- 257. A pharmaceutical combination as set forth in claim 231, wherein the combination comprises a pharmaceutical kit comprising:
a source of a potentiating agent; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the source of the potentiating agent and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 258. A pharmaceutical combination as set forth in claim 257, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said potentiating agent and said facilitating anion.
- 259. A pharmaceutical combination as set forth in claim 257, wherein said combination further comprises a source of a neutralizing agent and/or a buffering agent.
- 260. A pharmaceutical combination as set forth in claim 259, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the potentiating agnet, the facilitating anion, and the neutralizing agent and/or buffering agent.
- 261. A pharmaceutical combination as set forth in claim 259 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 262. A pharmaceutical combination as set forth in claim 261 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 263. A pharmaceutical combination as set forth in claim 257, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 264. A method for potentiating clearance of a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 148 to a subject in need thereof.
- 265. A method as set forth in claim 264 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a pyridostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the pyridostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 266. A method as set forth in claim 264 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a pyridostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the source of the pyridostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 267. A method for potentiating clearance of a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 180 to a subject in need thereof.
- 268. A method as set forth in claim 267 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a pyridostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the pyridostigmine cation and the facilitating anion are, in combination, suitable for oral ingestion; the pyridostigmine cation and the facilitating anion are capable of forming a mixture comprising a pyridostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the pyridostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 269. A method as set forth in claim 267 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a pyridostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the source of the pyridostigmine cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the pyridostigmine cation and the source of the facilitating anion are capable of forming a mixture comprising a pyridostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the pyridostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 270. A method for potentiating clearance of a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 212 to a subject in need thereof.
- 271. A method as set forth in claim 270 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a pyridostigmine cation and an anion selected from the group consisting of: 19a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 272. A method as set forth in claim 270 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a pyridostigmine cation; and a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 20a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 273. A method of potentiating clearance of a cholinesterase inhibitor, the method comprising administering a pharmaceutical combination of claim 231 to a subject in need thereof.
- 274. A method as set forth in claim 273 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a potentiating agent; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the potentiating agent and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 275. A method as set forth in claim 273 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a potentiating agent; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the source of the potentiating agent and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 276. A pharmaceutical combination useful for treating nerve conditions such as pseudoobstruction of the bowel, paralytic ileus and/or urinary retention, or myasthenia gravis, the pharmaceutical combination comprising:
a neostigmine cation or a source of a neostigmine cation; and a facilitating anion or a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the neostigmine cation or the source of the neostigmine cation and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 277. A pharmaceutical combination as set forth in claim 276 wherein the combination comprises a pharmaceutical composition comprising:
a neostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the neostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 278. A pharmaceutical combination as set forth in claim 277, wherein the combination is used to treat myasthenia gravis.
- 279. A pharmaceutical combination as set forth in claim 277, wherein the combination is used to treat paralytic ileus and/or urinary retention or pseudoobstruction of the bowel.
- 280. A pharmaceutical combination as set forth in claim 277, wherein said combination further comprises a neutralizing agent.
- 281. A pharmaceutical combination as set forth in claim 280, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 282. A pharmaceutical combination as set forth in claim 280, wherein said combination further comprises a buffering agent.
- 283. A pharmaceutical combination as set forth in claim 282, wherein said buffering agent comprises citric acid.
- 284. A pharmaceutical combination as set forth in claim 277, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 285. A pharmaceutical combination as set forth in claim 277 wherein the molar ratio of said facilitating anion to said neostigmine cation is from about 0.5 to about 2.
- 286. A pharmaceutical combination as set forth in claim 285 wherein the molar ratio of said facilitating anion to said neostigmine cation is from about 1.0 to about 1.5.
- 287. A pharmaceutical combination as set forth in claim 285 wherein the molar ratio of said facilitating anion to said neostigmine cation is from about 1.0 to about 1.1.
- 288. A pharmaceutical combination as set forth in claim 277, wherein, when the combination is orally administered to a human, the neostigmine cation is absorbed into the bloodstream from the gastrointestinal tract.
- 289. A pharmaceutical combination as set forth in claim 277, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 290. A pharmaceutical composition as set forth in claim 289, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 291. A pharmaceutical composition as set forth in claim 290, wherein said facilitating anion comprises salicylate.
- 292. A pharmaceutical combination as set forth in claim 277, wherein said combination comprises a compound which comprises both said neostigmine cation and said facilitating anion.
- 293. A pharmaceutical combination as set forth in claim 277, wherein said combination comprises neostigmine di(2-ethylhexyl)sulfosuccinate, neostigmine salicylate, neostigmine acetylsalicylate, neostigmine lauryl sulfate, neostigmine ne di(2-ethylhexyl)phosphate, or neostigmine hexadecylsulfonate.
- 294. A pharmaceutical combination as set forth in claim 277, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 295. A pharmaceutical combination as set forth in claim 277, wherein said combination is in a form comprising a tablet or a capsule.
- 296. A pharmaceutical combination as set forth in claim 277, wherein said combination is in a form comprising a solution or suspension.
- 297. A pharmaceutical combination as set forth in claim 277, wherein said combination is in a form suitable for administering via injection.
- 298. A pharmaceutical combination as set forth in claim 297, wherein said combination is suitable for intravenous or intramuscular injection.
- 299. A pharmaceutical combination as set forth in claim 297 further comprising a buffer.
- 300. A pharmaceutical combination as set forth in claim 299 further comprising a bulking, dispersing, wetting or suspending agent.
- 301. A pharmaceutical combination as set forth in claim 276 wherein the combination comprises a pharmaceutical kit comprising:
a source of a neostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; and the source of the neostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 302. A pharmaceutical combination as set forth in claim 301, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said neostigmine cation and said facilitating anion.
- 303. A pharmaceutical combination as set forth in claim 301, wherein said combination further comprises a source of a neutralizing agent and/or a buffering agent.
- 304. A pharmaceutical combination as set forth in claim 303, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the neostigmine cation, the facilitating anion, and the neutralizing agent and/or buffering agent.
- 305. A pharmaceutical combination as set forth in claim 303 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 306. A pharmaceutical combination as set forth in claim 305 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 307. A pharmaceutical combination as set forth in claim 301, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 308. A pharmaceutical combination as set forth in claim 276, wherein the combination comprises:
a neostigmine cation or a source of a neostigmine cation; and a facilitating anion or a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the neostigmine cation or the source of the neostigmine cation and the facilitating anion or the source of the facilitating anion are, in combination, suitable for oral ingestion; the neostigmine cation or the source of the neostigmine cation and the facilitating anion or the source of the facilitating anion are capable of forming a mixture comprising a neostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the neostigmine cation or the source of the neostigmine cation and the facilitating anion or the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 309. A pharmaceutical combination as set forth in claim 308 wherein the combination comprises a pharmaceutical composition comprising:
a neostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the neostigmine cation and the facilitating anion are, in combination, suitable for oral ingestion; the neostigmine cation and the facilitating anion are capable of forming a mixture comprising a neostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the neostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 310. A pharmaceutical combination as set forth in claim 309, wherein the combination is used to treat myasthenia gravis.
- 311. A pharmaceutical combination as set forth in claim 309, wherein the combination is used to treat paralytic ileus and/or urinary retention or pseudoobstruction of the bowel.
- 312. A pharmaceutical combination as set forth in claim 309, wherein said combination further comprises a neutralizing agent.
- 313. A pharmaceutical combination as set forth in claim 312, wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate.
- 314. A pharmaceutical combination as set forth in claim 312, wherein said combination further comprises a buffering agent.
- 315. A pharmaceutical combination as set forth in claim 314, wherein said buffering agent comprises citric acid.
- 316. A pharmaceutical combination as set forth in claim 309, wherein said facilitating anion has an organic/aqueous phase distribution equilibrium constant of greater than about 320 when introduced into a mixture comprising water, 1-decanol, methyltridecylammonium chloride, and a methyltridecylammonium salt.
- 317. A pharmaceutical combination as set forth in claim 309 wherein the molar ratio of said facilitating anion to said neostigmine cation is from about 0.5 to about 2.
- 318. A pharmaceutical combination as set forth in claim 317 wherein the molar ratio of said facilitating anion to said neostigmine cation is from about 1.0 to about 1.5.
- 319. A pharmaceutical combination as set forth in claim 1317 wherein the molar ratio of said facilitating anion to said neostigmine cation is from about 1.0 to about 1.1.
- 320. A pharmaceutical combination as set forth in claim 309, wherein, when the combination is orally administered to a human, the neostigmine cation is absorbed into the bloodstream from the gastrointestinal tract.
- 321. A pharmaceutical combination as set forth in claim 309, wherein said facilitating anion comprises an anion selected from the group consisting of alkylsulfate, alkylsulfonate, alkylsulfosuccinate, salicylate, alkylsalicylate, alkylphosphate, dialkylphosphate, and dialkanoylphosphatidate.
- 322. A pharmaceutical composition as set forth in claim 321, wherein said facilitating anion comprises di(2-ethylhexyl)sulfosuccinate, salicylate, di(2-ethylhexyl) phosphate, hexadecylsulfonate, or dipalmitoyl phosphatidate.
- 323. A pharmaceutical composition as set forth in claim 322, wherein said facilitating anion comprises salicylate.
- 324. A pharmaceutical combination as set forth in claim 309, wherein said combination comprises a compound which comprises both said neostigmine cation and said facilitating anion.
- 325. A pharmaceutical combination as set forth in claim 309, wherein said combination comprises neostigmine di(2-ethylhexyl)sulfosuccinate, neostigmine salicylate, neostigmine acetylsalicylate, neostigmine lauryl sulfate, neostigmine ne di(2-ethylhexyl)phosphate, or neostigmine hexadecylsulfonate.
- 326. A pharmaceutical combination as set forth in claim 309, wherein said pharmaceutical combination comprises a pharmaceutical composition comprising at least 2 types of facilitating anions.
- 327. A pharmaceutical combination as set forth in claim 309, wherein said combination is in a form comprising a tablet or a capsule.
- 328. A pharmaceutical combination as set forth in claim 309, wherein said combination is in a form comprising a solution or suspension.
- 329. A pharmaceutical combination as set forth in claim 309, wherein said combination is in a form suitable for administering via injection.
- 330. A pharmaceutical combination as set forth in claim 329, wherein said combination is suitable for intravenous or intramuscular injection.
- 331. A pharmaceutical combination as set forth in claim 329 further comprising a buffer.
- 332. A pharmaceutical combination as set forth in claim 331 further comprising a bulking, dispersing, wetting or suspending agent.
- 333. A pharmaceutical combination as set forth in claim 308 wherein the combination comprises a pharmaceutical kit comprising:
a source of a neostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a bromide anion; the source of the neostigmine cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the neostigmine cation and the source of the facilitating anion are capable of forming a mixture comprising a neostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the neostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 334. A pharmaceutical combination as set forth in claim 333, wherein said combination comprises a pharmaceutical kit comprising at least 2 separate unit dosages, said unit dosages independently comprising said neostigmine cation and said facilitating anion.
- 335. A pharmaceutical combination as set forth in claim 333, wherein said combination further comprises a source of a neutralizing agent and/or a buffering agent.
- 336. A pharmaceutical combination as set forth in claim 335, wherein said combination comprises a pharmaceutical kit comprising at least three separate unit dosages, said unit dosages independently comprising the neostigmine cation, the facilitating anion, and the neutralizing agent and/or buffering agent.
- 337. A pharmaceutical combination as set forth in claim 335 wherein said neutralizing agent comprises sodium bicarbonate or sodium citrate and said buffering agent comprises citric acid.
- 338. A pharmaceutical combination as set forth in claim 337 wherein said sources of said neutralizing agent and said buffering agent are in combination and comprise a commercially available Alka Seltzer® tablet.
- 339. A pharmaceutical combination as set forth in claim 333, wherein said pharmaceutical combination comprises a pharmaceutical kit comprising at least 2 types of facilitating anions.
- 340. A pharmaceutical combination useful for treating nerve conditions such as pseudoobstruction of the bowel, paralytic ileus and/or urinary retention, or myasthenia gravis, the pharmaceutical combination comprising:
a neostigmine cation or a source of a neostigmine cation; and an anion or a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 21a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 341. A pharmaceutical combination as set forth in claim 340 wherein the combination comprises a pharmaceutical composition comprising:
a neostigmine cation; and an anion, wherein:
the anion comprises an anion selected from the group consisting of: 22a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 342. A pharmaceutical combination as set forth in claim 341, wherein the anion comprises R1OSO3− and R1 is hydrocarbyl or substituted hydrocarbyl.
- 343. A pharmaceutical combination as set forth in claim 342, wherein R1 is hydrocarbyl.
- 344. A pharmaceutical combination as set forth in claim 341, wherein the facilitating anion comprises the formula:
- 345. A pharmaceutical combination as set forth in claim 344, wherein R5 is hydrocarbyl.
- 346. A pharmaceutical combination as set forth in claim 341, wherein the anion comprises a compound of the the formula:
- 347. A pharmaceutical combination as set forth in claim 346, wherein R17 is hydrocarbyl and R18 is hydrogen.
- 348. A pharmaceutical combination as set forth in claim 346, wherein the pharmaceutical composition comprises aspirin.
- 349. A pharmaceutical combination as set forth in claim 346, wherein the pharmaceutical composition is in a form suitable for administering orally.
- 350. A pharmaceutical combination as set forth in claim 340 wherein the combination comprises a pharmaceutical kit comprising:
a source of a neostigmine cation; and a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 25a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 351. A pharmaceutical combination as set forth in claim 350, wherein the anion comprises R1OSO3− and R1 is hydrocarbyl or substituted hydrocarbyl.
- 352. A pharmaceutical combination as set forth in claim 351, wherein R1 is hydrocarbyl.
- 353. A pharmaceutical combination as set forth in claim 352, wherein the anion comprises a compound of the formula:
- 354. A pharmaceutical combination as set forth in claim 353, wherein R5 is hydrocarbyl.
- 355. A pharmaceutical combination as set forth in claim 350, wherein the anion comprises a compound having the formula:
- 356. A pharmaceutical combination as set forth in claim 355, wherein R17 is hydrocarbyl and R18 is hydrogen.
- 357. A pharmaceutical combination as set forth in claim 355, wherein the pharmaceutical composition comprises aspirin.
- 358. A pharmaceutical combination as set forth in claim 355, wherein the pharmaceutical composition is in a form suitable for administering orally.
- 359. A method for treating nerve conditions such as pseudoobstruction of the bowel, paralytic ileus and/or urinary retention, or myasthenia gravis, the method comprising administering a pharmaceutical combination of claim 276 to a subject in need thereof.
- 360. A method as set forth in claim 359 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a neostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the neostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 361. A method as set forth in claim 359 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a neostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; and the source of the neostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 362. A method for treating nerve conditions such as pseudoobstruction of the bowel, paralytic ileus and/or urinary retention, or myasthenia gravis, the method comprising administering a pharmaceutical combination of claim 308 to a subject in need thereof.
- 363. A method as set forth in claim 362 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a neostigmine cation; and a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the neostigmine cation and the facilitating anion are, in combination, suitable for oral ingestion; the neostigmine cation and the facilitating anion are capable of forming a mixture comprising a neostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the neostigmine cation and the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 364. A method as set forth in claim 362 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a neostigmine cation; and a source of a facilitating anion, wherein:
the facilitating anion is less hydrophilic than a chloride anion; the source of the neostigmine cation and the source of the facilitating anion are, in combination, suitable for oral ingestion; the source of the neostigmine cation and the source of the facilitating anion are capable of forming a mixture comprising a neostigmine cation and a facilitating anion within the gastrointestinal tract of a subject upon ingestion by the subject; and the source of the neostigmine cation and the source of the facilitating anion together are present in the pharmaceutical combination in a therapeutically effective amount.
- 365. A method for treating nerve conditions such as pseudoobstruction of the bowel, paralytic ileus and/or urinary retention, or myasthenia gravis, the method comprising administering a pharmaceutical combination of claim 340 to a subject in need thereof.
- 366. A method as set forth in claim 365 wherein said pharmaceutical combination comprises a pharmaceutical composition comprising:
a neostigmine cation; and an anion, wherein:
the anion comprises an anion selected from the group consisting of: 28a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 367. A method as set forth in claim 365 wherein said pharmaceutical combination comprises a pharmaceutical kit comprising:
a source of a neostigmine cation; and a source of an anion, wherein:
the anion comprises an anion selected from the group consisting of: 29a pseudo-icosahedral carboranes anion (CB11H12−), and a substituted pseudo-icosahedral carborane anion, wherein R1, R2, R3, R4, R6, R7, R8, R9, R10, R11, R12, R13, R14, R15, R16, R17, and the substituent (or substituents) of the substituted pseudo-icosahedral carborane anion are independently hydrocarbyl or substituted hydrocarbyl; and R5 and R18 are independently hydrogen, hydrocarbyl, or substituted hydrocarbyl.
- 368. A process for the preparation of a salt of a quaternary ammonium cation and an anion that is more hydrophobic than chloride ion, the process comprising:
mixing an aqueous solution of a mineral acid salt of the cation with a source of alkali metal or alkaline earth metal salt of the anion; and contacting the resulting mixture with a substantially water-immiscible organic solvent, thereby transferring the salt of the quaternary ammonium cation and the more hydrophobic anion to the solvent phase and producing an organic extract comprising the transferred salt.
- 369. A process as set forth in claim 368 wherein the transferred salt is recovered from the extract.
- 370. A process as set forth in claim 369 wherein recovery of transferred salt from the extract comprises:
dehydrating the extract; and removing solvent from the dehydrated extract to yield a residue comprising the salt of the quaternary ammonium cation and the more hydrophobic anion.
- 371. A process as set forth in claim 368 wherein the quaternary ammonium cation is selected from the group consisting of 2-PAM, pyridostigmine and neostigmine.
- 372. A process as set forth in claim 368 wherein the more hydrophobic anion is selected from the group consisting of alkylsulfonate, alkylsulfosuccinate, alkylphosphate, dialkylphosphate, dialkanoylphosphatidate, dialkylsulfosuccinate, salicylate, and alkylsulfate.
- 373. A process as set forth in claim 368 wherein the mineral acid salt is selected from the group consisting of halide and sulfate salts.
- 374. A process as set forth in claim 373 wherein the mineral acid salt comprises a chloride salt.
- 375. The process as set forth in claim 368 wherein the anion is more hydrophobic than toluenesulfonate.
- 376. A pharmaceutical composition comprising 2-PAM di(2-ethylhexyl)sulfosuccinate
- 377. A pharmaceutical composition comprising 2-PAM salicylate
- 378. A pharmaceutical composition comprising 2-PAM di(2-ethylhexyl)phosphate
- 379. A pharmaceutical composition comprising 2-PAM @ lauryl sulfate
- 380. A pharmaceutical composition comprising 2-PAM hexadecylsulfonate
- 381. A pharmaceutical composition comprising 2-PAM acetyl salicylate
- 382. A pharmaceutical composition comprising pyridostigmine hexadecylsulfonate
- 383. A pharmaceutical composition comprising pyridostigmine di(2-ethylhexyl)sulfosuccinate
- 384. A pharmaceutical composition comprising pyridostigmine salicylate
- 385. A pharmaceutical composition comprising pyridostigmine di(2-ethylhexyl)phosphate
- 386. A pharmaceutical composition comprising pyridostigmine lauryl sulfate
- 387. A pharmaceutical composition comprising pyridostigmine acetyl salicylate
- 388. A pharmaceutical composition comprising neostigmine hexadecylsulfonate
- 389. A pharmaceutical composition comprising neostigmine di(2-ethylhexyl)sulfosuccinate
- 390. A pharmaceutical composition comprising neostigmine salicylate
- 391. A pharmaceutical composition comprising neostigmine di(2-ethylhexyl)phosphate
- 392. A pharmaceutical composition comprising neostigmine lauryl sulfate
- 393. A pharmaceutical composition comprising neostigmine acetyl salicylate
CROSS REFERENCE TO RELATED APPLICATIONS
[0001] This application claims priority from U.S. Provisional Application Serial No. 60/290,456, filed May 11, 2001, the entire text of which is hereby incorporated herein by reference.
Provisional Applications (1)
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Number |
Date |
Country |
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60290456 |
May 2001 |
US |