Methods and compositions for treating viral, fungal, and bacterial infections
IPC분류정보
국가/구분
United States(US) Patent
등록
국제특허분류(IPC7판)
C11D-007/18
C11D-007/02
C11D-003/48
출원번호
UP-0514722
(2006-08-31)
등록번호
US-7553805
(2009-07-09)
발명자
/ 주소
Tichy, Daryl J.
Larson, Brian G.
출원인 / 주소
Solutions Biomed, LLC
대리인 / 주소
Thorpe North & Western LLP
인용정보
피인용 횟수 :
4인용 특허 :
47
초록▼
The present invention is drawn to methods of treating disease or injury. In particular, the invention provides methods for treating viral infections, bacterial infections, fungal infections, and cancerous tissue. The methods include the administration of an aqueous composition that can comprise an a
The present invention is drawn to methods of treating disease or injury. In particular, the invention provides methods for treating viral infections, bacterial infections, fungal infections, and cancerous tissue. The methods include the administration of an aqueous composition that can comprise an aqueous vehicle, including water, from 0.0001 wt % to 10.0 wt % of a peroxygen, and optionally, an alcohol. Additionally, from 0.0001 ppm to 50,000 ppm by weight of a transition metal based on the aqueous vehicle content can also be present. Alternatively or additionally, the transition metal can be in the form of a colloidal transition metal, such as colloidal silver or alloy thereof.
대표청구항▼
What is claimed is: 1. A method of treating cancerous tissue, comprising: administering an aqueous composition to a subject afflicted with cancerous tissue, said aqueous composition comprising: a) an aqueous vehicle, including: i) water, and ii) from 0.0001 wt % to 10.0 wt % of a peroxygen; and b)
What is claimed is: 1. A method of treating cancerous tissue, comprising: administering an aqueous composition to a subject afflicted with cancerous tissue, said aqueous composition comprising: a) an aqueous vehicle, including: i) water, and ii) from 0.0001 wt % to 10.0 wt % of a peroxygen; and b) from 0.0001 ppm to 50,000 ppm by weight of a transition metal or alloy thereof based on the aqueous vehicle content. 2. A method as in claim 1, wherein the aqueous composition is administered by injection. 3. A method as in claim 1, wherein the aqueous composition is administered by injection. 4. A method as in claim 1, wherein the aqueous composition is administered topically. 5. A method as in claim 1, wherein the aqueous composition is administered intravenously. 6. A method as in claim 1, wherein the administration is over a period of 1 hour to 7 days. 7. A method as in claim 1, wherein the aqueous composition is formulated for administration in the form of an ointment, cream, mouth rinse, gel, lozenge, gum, wipe, dermal patch, foam, powder, aerosol, or bandage dressings. 8. A method as in claim 1, wherein an alcohol is present in the aqueous composition. 9. A method as in claim 8, wherein the alcohol is present at from 0.001 wt % to 40 wt %. 10. A method as in claim 8, wherein the alcohol is present in the aqueous composition at from 0.1 wt % to 10 wt %. 11. A method as in claim 8, wherein the alcohol is selected from the group consisting of methanol, ethanol, propanols, butanols, pentanols, and mixtures thereof. 12. A method as in claim 8, wherein the alcohol is a polyhydric alcohol. 13. A method as in claim 1, wherein the transition metal or alloy thereof is selected from the group consisting of ruthenium, rhodium, osmium, iridium, palladium, platinum, copper, gold, silver, manganese, zinc, alloys thereof, and mixtures thereof. 14. A method as in claim 1, wherein the transition metal or alloy thereof is a colloidal transition metal or alloy thereof. 15. A method as in claim 14, wherein the colloidal transition metal is colloidal silver. 16. A method as in claim 14, wherein the colloidal transition metal or alloy thereof has an average particle size of from 0.03 μm to 0.5 μm. 17. A method as in claim 1, wherein the transition metal or alloy thereof is an ionic transition metal. 18. A method as in claim 1, wherein the transition metal or alloy thereof is present at from 0.0001 ppm to 1,500 ppm by weight. 19. A method as in claim 1, wherein the peroxygen is a peracid. 20. A method as in claim 19, wherein the peracid is selected from the group consisting of peroxyformic acid, peroxyacetic acid, peroxyoxalic acid, peroxypropanoic acid, perlactic acid, peroxybutanoic acid, peroxypentanoic acid, peroxyhexanoic acid, peroxyadipic acid, peroxycitric, peroxybenzoic acid, and mixtures thereof. 21. A method as in claim 1, wherein the peroxygen is a peroxide. 22. A method as in claim 1, wherein the peroxygen includes a peracid and a peroxide. 23. A method as in claim 1, wherein the peroxygen is present at from 0.05 wt % to 5.0 wt % as part of the aqueous vehicle. 24. A method as in claim 1, wherein the peroxygen is present at from 0.1 wt % to 1.5 wt % as part of the aqueous vehicle. 25. A method as in claim 1, wherein the cancerous tissue is a dermal cancer. 26. A method as in claim 1, wherein the cancerous tissue is prostate cancer. 27. A method as in claim 1, wherein the cancerous tissue is an internal cancer. 28. A method of treating a subject of bacterial, viral, or fungal infection, comprising: administering an aqueous composition to a subject in an amount sufficient to prevent or treat the viral infection, said aqueous composition comprising: a) an aqueous vehicle, including: i) water, and ii) from 0.0001 wt % to 10.0 wt % of a peroxygen, wherein the peroxygen includes a peracid; and b) from 0.0001 ppm to 50,000 ppm by weight of a colloidal transition metal or alloy thereof based on the aqueous vehicle content. 29. A method as in claim 28, wherein the aqueous composition is administered orally. 30. A method as in claim 28, wherein the aqueous composition is administered by injection. 31. A method as in claim 28, wherein the aqueous composition is administered topically. 32. A method as in claim 28, wherein the aqueous composition is administered intravenously. 33. A method as in claim 28, wherein the administration is over a period of 1 hour to 7 days. 34. A method as in claim 28, wherein the aqueous composition is formulated for administration in the form of an ointment, cream, mouth rinse, gel, lozenge, gum, wipe, dermal patch, foam, powder, aerosol, or bandage dressings. 35. A method as in claim 28, wherein an alcohol is present in the aqueous composition. 36. A method as in claim 35, wherein the alcohol is present at from 0.001 wt % to 40 wt %. 37. A method as in claim 35, wherein the alcohol is present in the aqueous composition at from 0.1 wt % to 10 wt %. 38. A method as in claim 35, wherein the alcohol is selected from the group consisting of methanol, ethanol, propanols, butanols, pentanols, and mixtures thereof. 39. A method as in claim 35, wherein the alcohol is a polyhydric alcohol. 40. A method as in claim 28, wherein the transition metal or alloy thereof is selected from the group consisting of ruthenium, rhodium, osmium, iridium, palladium, platinum, copper, gold, silver, manganese, zinc, alloys thereof, and mixtures thereof. 41. A method as in claim 28, wherein the colloidal transition metal is colloidal silver. 42. A method as in claim 28, wherein the colloidal transition metal or alloy thereof has an average particle size of from 0.03 μm to 0.5 μm. 43. A method as in claim 28, wherein the transition metal or alloy thereof is present at from 0.0001 ppm to 1,500 ppm by weight. 44. A method as in claim 28, wherein the peracid is selected from the group consisting of peroxyformic acid, peroxyacetic acid, peroxyoxalic acid, peroxypropanoic acid, perlactic acid, peroxybutanoic acid, peroxypentanoic acid, peroxyhexanoic acid, peroxyadipic acid, peroxycitric, peroxybenzoic acid, and mixtures thereof. 45. A method as in claim 28, wherein the peroxygen includes a peroxide. 46. A method as in claim 28, wherein the peroxygen includes a peracid and a peroxide. 47. A method as in claim 28, wherein the peroxygen is present at from 0.05 wt % to 5.0 wt % as part of the aqueous vehicle. 48. A method as in claim 28, wherein the peroxygen is present at from 0.1 wt % to 1.5 wt % as part of the aqueous vehicle. 49. A method as in claim 28, wherein the step of administering is to prevent the viral infection from infecting the subject. 50. A method as in claim 28, wherein the step of administering is to treat the viral infection present in the subject. 51. A method as in claim 28, wherein the viral infection is selected from the group consisting of molluscum contagiosum infection, HTLV infection, HTLV-1 infection, HIV/AIDS infection, human papilloma virus infection, herpes virus infection, genital herpes infection, viral dysentery, flu, measles, rubella, chickenpox, mumps, polio, rabies, mononucleosis, ebola, respiratory syncytial virus, dengue fever, yellow fever, lassa fever, arena virus, bunyavirus, filovirus, flavivirus, hantavirus, rotavirus, viral meningitis, west Nile fever, arbovirus, parainfluenza, smallpox, epstein-barr virus, dengue hemorrhagic fever, cytomegalovirus, infant cytomegalic virus, progressive multifocal leukoencephalopathy, viral gastroenteritis, a hepatitis, cold sores, ocular herpes, meningitis, encephalitis, shingles, encephalitis, california serogroup viral, St. Louis encephalitis, rift valley fever, hand, foot, & mouth disease, hendra virus, enteroviruses, astrovirus, adenoviruses, Japanese encephalitis, lymphocytic choriomeningitis, roseola infantum, sandfly fever, SARS, warts, cat scratch disease, slap-cheek syndrome, orf, pityriasis rosea, or lyssavirus. 52. A method as in claim 28, wherein the virus is small pox. 53. A method as in claim 28, wherein the virus is H5N1 virus. 54. A method as in claim 28, wherein the virus is human papilloma virus. 55. A method as in claim 28, wherein the step of administering is to prevent the bacterial infection from infecting the subject. 56. A method as in claim 28, wherein the subject has a skin injury, and wherein the aqueous composition is applied to the skin injury. 57. A method as in claim 28, wherein the step of administering is to treat the bacterial infection present in the subject. 58. A method as in claim 28, wherein the bacterial infection is selected from the group consisting of e. coli infections, Yersinia pestis, staphylococcal infection, streptococcal infection, mycobacteria infection, bacterial pneumonia, shigella dysentery, serratia infection, candida infection, or cryptococcal infection, or tuberculosis. 59. A method as in claim 28, wherein the bacterial infection is methicillin resistant staphylococcus aureus. 60. A method as in claim 28, wherein the bacterial infection is anthrax. 61. A method as in claim 28, wherein the step of administering is to prevent the fungal infection from infecting the subject. 62. A method as in claim 28, wherein the step of administering is to treat the fungal infection present in the subject. 63. A method as in claim 28, wherein the fungal infection is selected from the group consisting of thrush, candidiasis, cryptococcosis, histoplasmosis, blastomycosis, aspergillosis, coccidioidomycosis, paracoccidiomycosis, sporotrichosis, zygomycosis, chromoblastomycosis, lobomycosis, mycetoma, onychomycosis, piedra pityriasis versicolor, tinea barbae, tinea capitis, tinea corporis, tinea cruris, tinea favosa, tinea nigra, tinea pedis, otomycosis, phaeohyphomycosis, or rhinosporidiosis. 64. A method as in claim 28, wherein the fungal infection is a yeast infection. 65. A method as in claim 28, wherein the fungal infection is a vaginal infection. 66. A method as in claim 28, wherein the fungal infection is a vaginal infection. 67. A method as in claim 28, wherein the fungal infection is a skin, hair, or nail infection. 68. A method of treating a subject for bacterial, viral, or fungal infection, comprising: orally administering an aqueous composition to the subject in an amount sufficient to prevent or treat the viral infection, said aqueous composition comprising: a) an aqueous vehicle, including: i) water, and ii) from 0.0001 wt % to 10.0 wt % of a peroxygen; and b) from 0.0001 ppm to 50,000 ppm by weight of a colloidal transition metal or alloy thereof based on the aqueous vehicle content. 69. A method as in claim 68, wherein the administration is over a period of 1 hour to 7 days. 70. A method as in claim 68, wherein the aqueous composition is formulated for oral administration in the form of a gel, lozenge, gum, foam, powder, or aerosol. 71. A method as in claim 68, wherein an alcohol is present in the aqueous composition. 72. A method as in claim 71, wherein the alcohol is present at from 0.001 wt % to 40 wt %. 73. A method as in claim 71, wherein the alcohol is present in the aqueous composition at from 0.1 wt % to 10 wt %. 74. A method as in claim 71, wherein the alcohol is selected from the group consisting of methanol, ethanol, propanols, butanols, pentanols, and mixtures thereof. 75. A method as in claim 71, wherein the alcohol is a polyhydric alcohol. 76. A method as in claim 68, wherein the transition metal or alloy thereof is selected from the group consisting of ruthenium, rhodium, osmium, iridium, palladium, platinum, copper, gold, silver, manganese, zinc, alloys thereof, and mixtures thereof. 77. A method as in claim 68, wherein the colloidal transition metal is colloidal silver. 78. A method as in claim 68, wherein the colloidal transition metal or alloy thereof has an average particle size of from 0.03 μm to 0.5 μm. 79. A method as in claim 68, wherein the transition metal or alloy thereof is present at from 0.0001 ppm to 1,500 ppm by weight. 80. A method as in claim 68, wherein the peracid is selected from the group consisting of peroxyformic acid, peroxyacetic acid, peroxyoxalic acid, peroxypropanoic acid, perlactic acid, peroxybutanoic acid, peroxypentanoic acid, peroxyhexanoic acid, peroxyadipic acid, peroxycitric, peroxybenzoic acid, and mixtures thereof. 81. A method as in claim 68, wherein the peroxygen includes a peroxide. 82. A method as in claim 68, wherein the peroxygen includes a peracid and a peroxide. 83. A method as in claim 68, wherein the peroxygen is present at from 0.05 wt % to 5.0 wt % as part of the aqueous vehicle. 84. A method as in claim 68, wherein the peroxygen is present at from 0.1 wt % to 1.5 wt % as part of the aqueous vehicle. 85. A method as in claim 68, wherein the step of orally administering is to prevent the viral infection from infecting the subject. 86. A method as in claim 68, wherein the viral infection is selected from the group consisting of molluscum contagiosum infection, HTLV infection, HTLV-1 infection, HIV/AIDS infection, human papilloma virus infection, herpes virus infection, genital herpes infection, viral dysentery, flu, measles, rubella, chickenpox, mumps, polio, rabies, mononucleosis, ebola, respiratory syncytial virus, dengue fever, yellow fever, lassa fever, arena virus, bunyavirus, filovirus, flavivirus, hantavirus, rotavirus, viral meningitis, west Nile fever, arbovirus, parainfluenza, smallpox, epstein-barr virus, dengue hemorrhagic fever, cytomegalovirus, infant cytomegalic virus, progressive multifocal leukoencephalopathy, viral gastroenteritis, a hepatitis, cold sores, ocular herpes, meningitis, encephalitis, shingles, encephalitis, california serogroup viral, St. Louis encephalitis, rift valley fever, hand, foot, & mouth disease, hendra virus, enteroviruses, astrovirus, adenoviruses, Japanese encephalitis, lymphocytic choriomeningitis, roseola infantum, sandfly fever, SARS, warts, cat scratch disease, slap-cheek syndrome, orf, pityriasis rosea, or lyssavirus. 87. A method as in claim 68, wherein the virus is small pox. 88. A method as in claim 68, wherein the virus is H5N1 virus. 89. A method as in claim 68, wherein the virus is human papilloma virus. 90. A method as in claim 68, wherein the step of orally administering is to prevent the bacterial infection from infecting the subject. 91. A method as in claim 68, wherein the step of orally administering is to treat the bacterial infection present in the subject. 92. A method as in claim 68, wherein the bacterial infection is selected from the group consisting of e. coli infections, Yersinia pestis, staphylococcal infection, streptococcal infection, mycobacteria infection, bacterial pneumonia, shigella dysentery, serratia infection, candida infection, or cryptococcal infection, or tuberculosis. 93. A method as in claim 68, wherein the bacterial infection is methicillin resistant staphylococcus aureus. 94. A method as in claim 68, wherein the bacterial infection is anthrax. 95. A method as in claim 68, wherein the step of orally administering is to prevent the fungal infection from infecting the subject. 96. A method as in claim 68, wherein the step of orally administering is to treat the fungal infection present in the subject. 97. A method as in claim 68, wherein the fungal infection is selected from the group consisting of thrush, candidiasis, cryptococcosis, histoplasmosis, blastomycosis, aspergillosis, coccidioidomycosis, paracoccidiomycosis, sporotrichosis, zygomycosis, chromoblastomycosis, lobomycosis, mycetoma, onychomycosis, piedra pityriasis versicolor, tinea barbae, tinea capitis, tinea corporis, tinea cruris, tinea favosa, tinea nigra, tinea pedis, otomycosis, phaeohyphomycosis, or rhinosporidiosis. 98. A method as in claim 68, wherein the fungal infection is a yeast infection. 99. A method as in claim 68, wherein the fungal infection is a vaginal infection. 100. A method as in claim 68, wherein the fungal infection is a skin, hair, or nail infection. 101. A method of treating a subject for bacterial, viral, or fungal infection, comprising: intravenously administering an aqueous composition to the subject in an amount sufficient to prevent or treat the viral infection, said aqueous composition comprising: a) an aqueous vehicle, including: i) water, and ii) from 0.0001 wt % to 10.0 wt % of a peroxygen; and b) from 0.0001 ppm to 50,000 ppm by weight of a colloidal transition metal or alloy thereof based on the aqueous vehicle content. 102. A method as in claim 101, wherein the intravenous administration is over a period of 1 hour to 7 days. 103. A method as in claim 101, wherein an alcohol is present in the aqueous composition. 104. A method as in claim 103, wherein the alcohol is present at from 0.001 wt % to 40 wt %. 105. A method as in claim 103, wherein the alcohol is present in the aqueous composition at from 0.1 wt % to 10 wt %. 106. A method as in claim 103, wherein the alcohol is selected from the group consisting of methanol, ethanol, propanols, butanols, pentanols, and mixtures thereof. 107. A method as in claim 103, wherein the alcohol is a polyhydric alcohol. 108. A method as in claim 101, wherein the transition metal or alloy thereof is selected from the group consisting of ruthenium, rhodium, osmium, iridium, palladium, platinum, copper, gold, silver, manganese, zinc, alloys thereof, and mixtures thereof. 109. A method as in claim 101, wherein the colloidal transition metal is colloidal silver. 110. A method as in claim 101, wherein the colloidal transition metal or alloy thereof has an average particle size of from 0.03 μm to 0.5 μm. 111. A method as in claim 101, wherein the transition metal or alloy thereof is present at from 0.0001 ppm to 1,500 ppm by weight. 112. A method as in claim 101, wherein the peracid is selected from the group consisting of peroxyformic acid, peroxyacetic acid, peroxyoxalic acid, peroxypropanoic acid, perlactic acid, peroxybutanoic acid, peroxypentanoic acid, peroxyhexanoic acid, peroxyadipic acid, peroxycitric, peroxybenzoic acid, and mixtures thereof. 113. A method as in claim 101, wherein the peroxygen includes a peroxide. 114. A method as in claim 101, wherein the peroxygen includes a peracid and a peroxide. 115. A method as in claim 101, wherein the peroxygen is present at from 0.05 wt % to 5.0 wt % as part of the aqueous vehicle. 116. A method as in claim 101, wherein the peroxygen is present at from 0.1 wt % to 1.5 wt % as part of the aqueous vehicle. 117. A method as in claim 101, wherein the step of intravenously administering is to prevent the viral infection from infecting the subject. 118. A method as in claim 101, wherein the step of intravenously administering is to treat the viral infection present in the subject. 119. A method as in claim 101, wherein the viral infection is selected from the group consisting of molluscum contagiosum infection, HTLV infection, HTLV-1 infection, HIV/AIDS infection, human papilloma virus infection, herpes virus infection, genital herpes infection, viral dysentery, flu, measles, rubella, chickenpox, mumps, polio, rabies, mononucleosis, ebola, respiratory syncytial virus, dengue fever, yellow fever, lassa fever, arena virus, bunyavirus, filovirus, flavivirus, hantavirus, rotavirus, viral meningitis, west Nile fever, arbovirus, parainfluenza, smallpox, epstein-barr virus, dengue hemorrhagic fever, cytomegalovirus, infant cytomegalic virus, progressive multifocal leukoencephalopathy, viral gastroenteritis, a hepatitis, cold sores, ocular herpes, meningitis, encephalitis, shingles, encephalitis, california serogroup viral, St. Louis encephalitis, rift valley fever, hand, foot, & mouth disease, hendra virus, enteroviruses, astrovirus, adenoviruses, Japanese encephalitis, lymphocytic choriomeningitis, roseola infantum, sandfly fever, SARS, warts, cat scratch disease, slap-cheek syndrome, orf, pityriasis rosea, or lyssavirus. 120. A method as in claim 101, wherein the virus is small pox. 121. A method as in claim 101, wherein the virus is H5N1 virus. 122. A method as in claim 101, wherein the virus is human papilloma virus. 123. A method as in claim 101, wherein the step of intravenously administering is to prevent the bacterial infection from infecting the subject. 124. A method as in claim 101, wherein the step of intravenously administering is to treat the bacterial infection present in the subject. 125. A method as in claim 101, wherein the bacterial infection is selected from the group consisting of e. coli infections, Yersinia pestis, staphylococcal infection, streptococcal infection, mycobacteria infection, bacterial pneumonia, shigella dysentery, serratia infection, candida infection, or cryptococcal infection, or tuberculosis. 126. A method as in claim 101, wherein the bacterial infection is methicillin resistant staphylococcus aureus. 127. A method as in claim 101, wherein the bacterial infection is anthrax. 128. A method as in claim 101, wherein the step of intravenously administering is to prevent the fungal infection from infecting the subject. 129. A method as in claim 101, wherein the step of intravenously administering is to treat the fungal infection present in the subject. 130. A method as in claim 101, wherein the fungal infection is selected from the group consisting of thrush, candidiasis, cryptococcosis, histoplasmosis, blastomycosis, aspergillosis, coccidioidomycosis, paracoccidiomycosis, sporotrichosis, zygomycosis, chromoblastomycosis, lobomycosis, mycetoma, onychomycosis, piedra pityriasis versicolor, tinea barbae, tinea capitis, tinea corporis, tinea cruris, tinea favosa, tinea nigra, tinea pedis, otomycosis, phaeohyphomycosis, or rhinosporidiosis. 131. A method as in claim 101, wherein the fungal infection is a yeast infection. 132. A method as in claim 101, wherein the fungal infection is a vaginal infection. 133. A method as in claim 101, wherein the fungal infection is a skin, hair, or nail infection. 134. A method of treating a subject for bacterial, viral, or fungal infection, comprising: administering by injection an aqueous composition to the subject in an amount sufficient to prevent or treat the viral infection, said aqueous composition comprising: a) an aqueous vehicle, including: i) water, and ii) from 0.0001 wt % to 10.0 wt % of a peroxygen; and b) from 0.0001 ppm to 50,000 ppm by weight of a colloidal transition metal or alloy thereof based on the aqueous vehicle content. 135. A method as in claim 134, wherein the administration by injection is over a period of 1 hour to 7 days. 136. A method as in claim 134, wherein an alcohol is present in the aqueous composition. 137. A method as in claim 136, wherein the alcohol is present at from 0.001 wt % to 40 wt %. 138. A method as in claim 136, wherein the alcohol is present in the aqueous composition at from 0.1 wt % to 10 wt %. 139. A method as in claim 136, wherein the alcohol is selected from the group consisting of methanol, ethanol, propanols, butanols, pentanols, and mixtures thereof. 140. A method as in claim 136, wherein the alcohol is a polyhydric alcohol. 141. A method as in claim 134, wherein the transition metal or alloy thereof is selected from the group consisting of ruthenium, rhodium, osmium, iridium, palladium, platinum, copper, gold, silver, manganese, zinc, alloys thereof, and mixtures thereof. 142. A method as in claim 134, wherein the colloidal transition metal is colloidal silver. 143. A method as in claim 134, wherein the colloidal transition metal or alloy thereof has an average particle size of from 0.03 μm to 0.5 μm. 144. A method as in claim 134, wherein the transition metal or alloy thereof is present at from 0.0001 ppm to 1,500 ppm by weight. 145. A method as in claim 134, wherein the peracid is selected from the group consisting of peroxyformic acid, peroxyacetic acid, peroxyoxalic acid, peroxypropanoic acid, perlactic acid, peroxybutanoic acid, peroxypentanoic acid, peroxyhexanoic acid, peroxyadipic acid, peroxycitric, peroxybenzoic acid, and mixtures thereof. 146. A method as in claim 134, wherein the peroxygen includes a peroxide. 147. A method as in claim 134, wherein the peroxygen includes a peracid and a peroxide. 148. A method as in claim 134, wherein the peroxygen is present at from 0.05 wt % to 5.0 wt % as part of the aqueous vehicle. 149. A method as in claim 134, wherein the peroxygen is present at from 0.1 wt % to 1.5 wt % as part of the aqueous vehicle. 150. A method as in claim 134, wherein the step of administering by injection is to prevent the viral infection from infecting the subject. 151. A method as in claim 134, wherein the step of administering by injection is to treat the viral infection present in the subject. 152. A method as in claim 134, wherein the viral infection is selected from the group consisting of molluscum contagiosum infection, HTLV infection, HTLV-1 infection, HIV/AIDS infection, human papilloma virus infection, herpes virus infection, genital herpes infection, viral dysentery, flu, measles, rubella, chickenpox, mumps, polio, rabies, mononucleosis, ebola, respiratory syncytial virus, dengue fever, yellow fever, lassa fever, arena virus, bunyavirus, filovirus, flavivirus, hantavirus, rotavirus, viral meningitis, west Nile fever, arbovirus, parainfluenza, smallpox, epstein-barr virus, dengue hemorrhagic fever, cytomegalovirus, infant cytomegalic virus, progressive multifocal leukoencephalopathy, viral gastroenteritis, a hepatitis, cold sores, ocular herpes, meningitis, encephalitis, shingles, encephalitis, california serogroup viral, St. Louis encephalitis, rift valley fever, hand, foot, & mouth disease, hendra virus, enteroviruses, astrovirus, adenoviruses, Japanese encephalitis, lymphocytic choriomeningitis, roseola infantum, sandfly fever, SARS, warts, cat scratch disease, slap-cheek syndrome, orf, pityriasis rosea, or lyssavirus. 153. A method as in claim 134, wherein the virus is small pox. 154. A method as in claim 134, wherein the virus is H5N1 virus. 155. A method as in claim 134, wherein the virus is human papilloma virus. 156. A method as in claim 134, wherein the step of administering by injection is to prevent the bacterial infection from infecting the subject. 157. A method as in claim 134, wherein the step of administering by injection is to treat the bacterial infection present in the subject. 158. A method as in claim 134, wherein the bacterial infection is selected from the group consisting of e. coli infections, Yersinia pestis, staphylococcal infection, streptococcal infection, mycobacteria infection, bacterial pneumonia, shigella dysentery, serrate infection, candida infection, or cryptococcal infection, or tuberculosis. 159. A method as in claim 134, wherein the bacterial infection is methicillin resistant staphylococcus aureus. 160. A method as in claim 134, wherein the bacterial infection is anthrax. 161. A method as in claim 134, wherein the step of administering by injection is to prevent the fungal infection from infecting the subject. 162. A method as in claim 134, wherein the step of administering by injection is to treat the fungal infection present in the subject. 163. A method as in claim 134, wherein the fungal infection is selected from the group consisting of thrush, candidiasis, cryptococcosis, histoplasmosis, blastomycosis, aspergillosis, coccidioidomycosis, paracoccidiomycosis, sporotrichosis, zygomycosis, chromoblastomycosis, lobomycosis, mycetoma, onychomycosis, piedra pityriasis versicolor, tinea barbae, tinea capitis, tinea corporis, tinea cruris, tinea favosa, tinea nigra, tinea pedis, otomycosis, phaeohyphomycosis, or rhinosporidiosis. 164. A method as in claim 134, wherein the fungal infection is a yeast infection. 165. A method as in claim 134, wherein the fungal infection is a vaginal infection. 166. A method as in claim 134, wherein the fungal infection is a skin, hair, or nail infection. 167. A method as in claim 68, wherein the step of orally administering is to treat the viral infection present in the subject.
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