US2021308252A1PendingUtilityA1
Liposome compositions comprising pam2cys or pam3cys adjuvant and methods for inducing a humoral immune response
Assignee: IMMUNOVACCINE TECHNOLOGIES INCPriority: Oct 6, 2011Filed: Jun 17, 2021Published: Oct 7, 2021
Est. expiryOct 6, 2031(~5.2 yrs left)· nominal 20-yr term from priority
A61P 35/00A61P 31/00A61P 31/12A61P 37/08A61K 2039/55511A61K 2039/55566A61P 25/28A61K 9/127A61P 43/00A61P 37/04A61K 2039/5252A61P 31/04A61K 39/07A61P 31/16A61K 39/099A61K 2039/55555A61K 39/145A61K 39/12C12N 2760/16134A61K 39/39
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Claims
Abstract
The invention provides compositions comprising liposomes, an antigen capable of inducing a humoral immune response, a carrier comprising a continuous phase of a hydrophobic substance, and an adjuvant that activates or increases the activity of TLR2. The invention also provides uses for such compositions in inducing a humoral response and methods for their use in the treatment of a disease, disorder or ailment ameliorated by a humoral immune response.
Claims
exact text as granted — not AI-modified1 - 20 . (canceled)
21 . A water-free composition comprising an adjuvant that activates or increases the activity of toll-like receptor 2 (TLR2), dehydrated liposomes, and an antigen, reconstituted in a carrier comprising a continuous phase of a hydrophobic substance,
wherein the antigen comprises a B cell epitope and is capable of inducing a humoral immune response; wherein the adjuvant comprises dipalmitoyl-S-glyceryl-cysteine (PAM 2 Cys) or tripalmitoyl-S-glyceryl-cysteine (PAM 3 Cys); and wherein the antigen is not coupled covalently to the adjuvant.
22 . The water-free composition of claim 21 , wherein the antigen is an antigen of a pathogenic biological agent; a surface-bound cancer antigen; or an antigen associated with a neurodegenerative disease.
23 . The water-free composition of claim 21 , wherein the composition is capable of inducing a humoral immune response to generate neutralizing antibodies against a toxin, virus, bacterium or allergen.
24 . The water-free composition of claim 21 , wherein the adjuvant activates or increases the activity of TLR2 by interacting with a TLR2 dimer of TLR1/2 or TLR2/6.
25 . The water-free composition of claim 21 , wherein the adjuvant is PAM 2 Cys-Ser-(Lys)4 (SEQ ID NO:1), PAM 3 Cys-Ser-(Lys)4 (SEQ ID NO:1), PAM 3 Cys-SKKKK(SEQ ID NO:1) (β-irradiated), R-PAM 3 Cys-SKKKK (SEQ ID NO:1), S-PAM 3 Cys-SKKKK (SEQ ID NO:1), PAM 3 Cys-SKKKK(Biotin-Aca-Aca) (SEQ ID NO:1), PAM 3 Cys-SKKKK (Fluorescein-Aca-Aca) (SEQ ID NO:1), PAM 3 Cys-SKKKK (Rhodamine-Aca-Aca) (SEQ ID NO:1), PAM 3 Cys-SKKKK-FLAG-tag (SEQ ID NO:1), PAM 3 Cys-SSNAKIDQLSSDVQT (SEQ ID NO:4), PAM 3 Cys-SSNKSTTGSGETTTA (SEQ ID NO:5), PAM 3 Cys-SSTKPVSQDTSPKPA (SEQ ID NO:6), PAM 3 Cys-SSGSKPSGGPLPDAK (SEQ ID NO:7), PAM 3 Cys-SSGNKSAPSSSASSS (SEQ ID NO:8), PAM 3 Cys-GSHQMKSEGHANMQL (SEQ ID NO:9), PAM 3 Cys-SSSNNDAAGNGAAQT (SEQ ID NO:10), PAM 3 Cys-KQNVSSLDEKNSVSV (SEQ ID NO:11), PAM 3 Cys-NNSGKDGNTSANSAD (SEQ ID NO:12), PAM 3 Cys-NNGGPELKSDEVAKS (SEQ ID NO:13), PAM 3 Cys-SQEPAAPAAEATPAG (SEQ ID NO:14), PAM 3 Cys-SSSKSSDSSAPKAYG (SEQ ID NO:15), PAM 3 Cys-AQEKEAKSELDYDQT (SEQ ID NO:16), PAM 2 Cys-SKKKK (mixture of RR and RS stereoisomers) (SEQ ID NO:1), R-PAM 2 Cys-SKKKK (RR stereoisomer) (SEQ ID NO:1), S-PAM 2 Cys-SKKKK (RS stereoisomer) (SEQ ID NO:1), PAM 2 Cys-SKKKK(Biotin-Aca-Aca)-NH 2 (SEQ ID NO:1), PAM 2 Cys-SKKKK(Fluorescein-Aca-Aca)-NH 2 (SEQ ID NO:1), PAM 2 Cys-SKKKK(Rhodamine-Aca-Aca)-NH 2 (SEQ ID NO:1), PAM 2 Cys-SKKKK-FLAG-tag (SEQ ID NO:1), FSL-1 (Pam 2 CGDPKHPKSF) (SEQ ID NO:2), or FSL-1-Ala.
26 . The water-free composition of claim 21 , wherein the adjuvant is PAM 2 Cys-Ser-(Lys)4 (SEQ ID NO: 1).
27 . The water-free composition of claim 21 , wherein the adjuvant is PAM 3 Cys-Ser-(Lys)4 (SEQ ID NO:1).
28 . The water-free composition of claim 21 , wherein the antigen is a polypeptide or a carbohydrate.
29 . The water-free composition of claim 21 , wherein the B cell epitope is derived from a virus or bacteria.
30 . The water-free composition of claim 29 , wherein the B cell epitope is derived from influenza virus, Bordetella pertussis , or Bacillus anthracis.
31 . The water-free composition of claim 30 , wherein the B cell epitope is an epitope of a hemagglutinin protein of H5N1 influenza virus, an epitope of pertussis toxoid protein, or an epitope of an anthrax recombinant protective antigen.
32 . The water-free composition of claim 21 , wherein the antigen is encapsulated within the dehydrated liposomes or both the antigen and the adjuvant are encapsulated in the dehydrated liposomes, reconstituted in the continuous phase of a hydrophobic substance.
33 . The water-free composition of claim 21 , wherein the liposomes are non-cationic liposomes, wherein the lipids of the liposomes consist of neutral lipids, negatively charged lipids or a mixture thereof.
34 . The water-free composition of claim 21 , wherein the composition is capable of inducing a humoral immune response with a single dose.
35 . The water-free composition of claim 22 , wherein the pathogenic biological agent is selected from the group consisting of influenza virus, respiratory syncytial virus, Bordetella pertussis, Bacillus anthracis , and species of the genus Plasmodium.
36 . The water-free composition of claim 21 , wherein the liposomes are comprised of phospholipids and cholesterol.
37 . The water-free composition of claim 21 , wherein the carrier is a mannide oleate in mineral oil solution.
38 . The water-free composition of claim 37 , wherein the carrier is Montanide® ISA 51.
39 . The water-free composition of claim 21 , wherein the antigen is selected from the group consisting of H5N1 recombinant hemagglutinin protein, pertussis toxoid protein, anthrax recombinant Protective Antigen and heat inactivated Influenza strain A/PR/8/34 (H1N1).
40 . The water-free composition of claim 21 , wherein the liposomes comprise S100 lecithin and cholesterol or dioleoyl-phosphatidylcholine (DOPC) and cholesterol; the carrier is Montanide® ISA 51; and the adjuvant is PAM 3 Cys-Ser-(Lys)4 (SEQ ID NO:1).
41 . The water-free composition of claim 40 , wherein the antigen is selected from the group consisting of H5N1 recombinant hemagglutinin protein, pertussis toxoid protein, anthrax recombinant Protective Antigen and heat inactivated Influenza strain A/PR/8/34 (H1N1).Cited by (0)
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