Claims for Patent: 10,280,209
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Summary for Patent: 10,280,209
| Title: | Reduction of inflammatory disease symptoms by short peptides that inhibit signaling through CD28 |
| Abstract: | The present disclosure relates to a method for the treatment of a non-pathogen associated inflammatory disorders in a subject in need thereof, comprising administering to said subject an isolated peptide which specifically binds to an amino acid sequence within the dimer interface of a T cell costimulatory pathway member, particularly the T cell costimulatory pathway members CD28 and CTLA4. The present disclosure also relates to pharmaceutical compositions comprising the isolated peptide and to use of the peptide in treating of a non-pathogen associated inflammatory disorders. |
| Inventor(s): | Kaempfer; Raymond (Jerusalem, IL), Shirvan; Anat (Kfar-Saba, IL), Arad; Gila (Mevasseret Zion, IL) |
| Assignee: | ATOX BIO LTD. (Ness Ziona, IL) YISSUM RESEARCH DEVELOPMENT COMPANY OF THE HEBREW UNIVERSITY OF JERUSALEM LTD (Jerusalem, IL) |
| Application Number: | 15/936,686 |
| Patent Claims: | 1. A method for the treatment of a non-pathogen associated acute inflammatory disorder in a human subject in need thereof, said method comprising administering to said
subject a therapeutically effective amount of an isolated peptide which specifically binds to CD28, or a pharmaceutical composition comprising the same, wherein said isolated peptide is (a) selected from the group consisting of the amino acid sequences
His Val Lys Gly Lys His Leu Cys Pro (designated p1TA as denoted by SEQ ID NO: 3), Ser Pro Met Leu Val Ala Tyr Asp (designated p2TA as denoted by SEQ ID NO: 4), His Lys Gly Leu Asp Ser Ala Val (designated p3TA as denoted by SEQ ID NO: 5), Tyr Val Asn Gln
Thr Asp Ile Tyr (designated p4TA as denoted by SEQ ID NO:6), Asn Gly Thr Ile His Val Lys Gly (designated p5TA as denoted by SEQ ID NO: 7), Tyr Val Ile Asp Pro Glu Pro Cys Pro (designated p1TB as denoted by SEQ ID NO: 8), Pro Ala Val Val Leu Ala Ser Ser
(designated p2 TB as denoted by SEQ ID NO: 9), Ser His Phe Thr His Asn Arg His Gly His Ser Thr (designated pe12 as denoted by SEQ ID NO: 12, or (b) a functional derivative of a peptide of (a), wherein said functional derivative maintains the ability to
specifically bind to the CD28 homodimer interface and to inhibit said acute inflammation, said functional derivatives being selected from the group consisting of: (i) a peptide of (a) that has a substitution at one or more amino acid residues, each of
which being a conservative amino acid replacement, the functional derivative with said substitution(s) maintaining at least 80% homology to the corresponding peptide of (a); (ii) a peptide of (a) or (b)(i) that is extended at the N terminus and/or the C
terminus (1) by a lauryl cysteine at the N terminus and a cysteine at the C terminus; or (2) by an organic moiety that is not a naturally occurring or synthetic amino acid residue; or (3) by identical hydrophobic amino acid residue(s) which may be
naturally occurring or synthetic amino acid residues; or (4) by a palmitoyl-lysine tail, wherein said tail is at the N terminus; and (iii) a peptide of (a) that is p1TA, p2TA, p3TA, p4TA or p5TA that is extended at the N-terminus and/or C-terminus
thereof with 1-3 consecutive amino acid residues present in corresponding adjacent positions of the amino acid sequence of SEQ ID NO:1, or a peptide of (a) that is p1TB or p2 TB that is extended at the N-terminus and/or C-terminus thereof with 1-3
consecutive amino acid residues present in corresponding adjacent positions of the amino acid sequence of SEQ ID NO:2.
2. The method according to claim 1, wherein said isolated peptide is the amino acid sequence Ser Pro Met Leu Val Ala Tyr Asp denoted by SEQ ID NO: 4 (designated p2TA) or, as a functional derivative of said p2TA, the amino acid sequence (D-Ala) Ser Pro Met Leu Val Ala Tyr Asp (D-Ala) denoted by SEQ ID NO: 47 (designated (D-A)-p2TA-(D-A). 3. The method according to claim 1, wherein said isolated peptide comprises the amino acid sequence Pro Ala Val Leu Ala Ser (designated p2 TB as denoted by SEQ ID NO: 9), or, as functional derivatives of said p2 TB, (D-Ala)PAVVLASS(D-Ala) (designated (D-A)-p2 TB-(D-A) as denoted by SEQ ID NO: 48) or (palmitoyl-lysine) Pro Ala Val Leu Ala Ser (D-Ala) (designated (pal)-p2 TB-(D-A) as denoted by SEQ ID NO: 50). 4. The method according to claim 1, wherein said isolated peptide is a peptide consisting of the amino acid sequence Ser His Phe Thr His Asn Arg His Gly His Ser Thr (designated pe12 as denoted by SEQ ID NO: 12), or as functional derivatives of said pe12, (D-Ala) Ser His Phe Thr His Asn Arg His Gly His Ser Thr (D-Ala) (designated pe12-(D-A) as denoted by SEQ ID NO: 49) or (palmitoyl-lysine) Ser His Phe Thr His Asn Arg His Gly His Ser Thr D-Ala) (designated pe12-pal as denoted by SEQ ID NO: 51). 5. The method according to claim 1, wherein said isolated peptide is a peptide of (a) extended at the N-terminus and/or the C-terminus by one or more D-Ala residues. 6. The method according to claim 1, wherein said isolated peptide is a peptide of (a) extended at the N-terminus by a palmitoyl-lysine tail. 7. The method according to claim 1, wherein said non-pathogen associated acute inflammatory disorder is selected from the group consisting of non-pathogen associated acute gastrointestinal inflammation, non-pathogen associated acute inflammatory bowel disease (IBD), non-pathogen associated acute peritonitis, non-pathogen associated acute pancreatitis, non-pathogen associated cirrhosis, non-pathogen associated appendicitis, non-pathogen associated colitis, non-pathogen associated acute arthritis, non-pathogen associated rheumatoid arthritis, non-pathogen associated osteoarthritis, and non-pathogen associated multiple sclerosis. 8. The method according to claim 1, wherein said non-pathogen associated acute inflammatory disorder is selected from the group consisting of non-pathogen associated acute gastrointestinal inflammation, non-pathogen associated acute inflammatory bowel disease (IBD), non-pathogen associated acute peritonitis, and non-pathogen associated acute pancreatitis. 9. The method according to claim 8, wherein said isolated peptide comprises the amino acid sequence Ser Pro Met Leu Val Ala Tyr Asp denoted by SEQ ID NO: 4 or, as a functional derivative thereof, the amino acid sequence (D-Ala) Ser Pro Met Leu Val Ala Tyr Asp (D-Ala) denoted by SEQ ID NO: 47. 10. The method according to claim 1, wherein said isolated peptide or pharmaceutical composition is administered by a route selected from the group consisting of intravenous, intramuscular or intraperitoneal administration, intrathecal or subcutaneous injection, oral, intrarectal, intranasal, ocular and topical administration. 11. The method according to claim 1, wherein said isolated peptide is administered at an amount of from about 0.05 mg to about 5.0 mg peptide/kg body weight of a subject in need thereof. 12. The method according to claim 1, wherein said method comprises a single administration of said therapeutically effective dose of said isolated peptide or pharmaceutical composition. 13. The method according to claim 1, wherein said method comprises administering said therapeutically effective dose of said isolated peptide or pharmaceutical composition during one or more identical or different treatment periods by a single daily administration, wherein said treatment periods are consecutive or are set apart from each other by non-treatment intervals. 14. The method according to claim 1, wherein said isolated peptide or pharmaceutical composition is administered in combination with at least one additional therapeutically active agent, which may be administered simultaneously, or at different time points, in any order, in identical or different frequencies, for identical or different durations of time. 15. The method according to claim 14, wherein said additional therapeutically active agent is a steroid, a nonsteroidal anti-inflammatory agent or an immunosuppressive agent. 16. The method according to claim 14, wherein said non-pathogen associated acute inflammatory disorder is non-pathogen associated acute rheumatoid arthritis and wherein said additional therapeutically active agent is selected from the group consisting of Abatacept, a TNF blocker, an IL-1 blocker, an IL-6 blocker, an anti-CD20 agent, and a combination thereof. 17. The method according to claim 1, wherein said non-pathogen associated acute inflammatory disorder is non-pathogen associated acute multiple sclerosis and wherein said additional therapeutically active agent is selected from the group consisting of interferon-.beta., Copaxon; natalizumab and a combination thereof. |
Details for Patent 10,280,209
| Applicant | Tradename | Biologic Ingredient | Dosage Form | BLA | Approval Date | Patent No. | Expiredate |
|---|---|---|---|---|---|---|---|
| Biogen Inc. | TYSABRI | natalizumab | Injection | 125104 | 11/23/2004 | ⤷ Try a Trial | 2039-05-19 |
| Bristol-myers Squibb Company | ORENCIA | abatacept | For Injection | 125118 | 12/23/2005 | ⤷ Try a Trial | 2039-05-19 |
| Bristol-myers Squibb Company | ORENCIA | abatacept | Injection | 125118 | 07/29/2011 | ⤷ Try a Trial | 2039-05-19 |
| >Applicant | >Tradename | >Biologic Ingredient | >Dosage Form | >BLA | >Approval Date | >Patent No. | >Expiredate |
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Preferred Citation:
Friedman, Yali. "DrugPatentWatch" DrugPatentWatch, thinkBiotech, 2024, www.DrugPatentWatch.com.
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