B-cell epitope peptides of HSP 65

Drug – bio-affecting and body treating compositions – Antigen – epitope – or other immunospecific immunoeffector – Amino acid sequence disclosed in whole or in part; or...

Reexamination Certificate

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C424S248100, C424S278100, C530S326000, C530S402000, C530S806000, C530S820000, C514S013800

Reexamination Certificate

active

06770281

ABSTRACT:

FIELD OF THE INVENTION
The present invention relates to various peptides homologous to regions of heat shock protein (HSP), to DNA sequences encoding such peptides, to DNA constructs comprising the DNA sequences, and to antibodies directed against peptides of the invention. The invention also relates to active vaccines comprising a peptide, a DNA sequence or a DNA construct of the invention, and to a passive immunization composition comprising an antibody of the invention.
BACKGROUND
Throughout this application, various publications are referred to by Arabic numerals in parentheses. These publications are incorporated herein in their entireties and constitute part of the description.
Adjuvant Arthritis (AA) is an experimental model of autoimmune arthritis which can be induced in susceptible strains of rats such as inbred Lewis or Wistar strains upon vaccination with heat-killed
Mycobacterium tuberculosis
(MT) in complete Freund's Adjuvant (CFA) [1-3]. The disease cannot be induced in resistant strains of rats (e.g., Brown-Norway; Fisher [5, 6]), and Lewis rats develop resistance to re-induction of the disease after recovery from arthritis.
The inventors have previously shown that resistance to AA can be transferred to a susceptible strain of rats by intravenous infusion of immunoglobulins from the resistant strains, and that resistance is associated with the presence of antibodies against the 65 kD MT heat shock protein (HSP 65) [4].
Heat shock proteins are a family of highly conserved proteins. There is ~50% amino acid identity between the mycobacterial HSP 65 and the mammalian HSP 60 [21]. The role of the 65 kD heat shock protein (HSP 65) of MT in the pathogenesis of autoimmune arthritis, both in experimental animals [7, 8], as well as in humans [9-11], has been investigated intensively in the past several years. For example, Barker et al. [32] describes the suppression of arthritogenic immune responses in mice given HSP 65 and pristane. The antigen used to elicit the response was full-length HSP 65, and no attempt was made to investigate the effect of specific sub-domains or peptides deriving from this protein.
AA can be passively transferred by a T-cell clone reactive to residues 180-188 of the MT HSP 65, and in patients suffering from rheumatoid arthritis (RA), an association between T-cell responses to HSP 65 and early stages of joint inflammation has been found [7, 12-14]. Paradoxically, pre-immunization with the mycobacterial HSP 65 leads to resistance to induction of the disease by MT, and this protective effect is believed to be mediated by T-cells specific for HSP 65 [7, 15-16]. Likewise, although arthritic rats develop vigorous T-cell responses to self-HSP and to peptide 180-188 of the MT HSP, neither of these is arthritogenic when injected to arthritis-susceptible rats [15, 17]. These and other results suggest that HSP may contain epitopes that are disease-related and other epitopes that confer resistance [5, 19, 20]. Both the pathogenic immune response and the protective effect were attributed to anti-HSP T-cells. The following Examples illustrate the fine epitope specificity of the anti-HSP antibodies of arthritis-susceptible and resistant rats.
In addition, the inventors have found that naive Lewis rats lack antibodies to certain epitopes of the mycobacterial HSP 65 which are found naturally in young BN and old naive Lewis rats, and that are acquired by young Lewis rats after recovery from the disease. Analysis of the primary and tertiary structure of the whole MT HSP 65 molecule indicated that these “protective” epitopes are potential B-cell epitopes with non-conserved amino acid sequences which are found on the outer surface of the molecule.
Pre-immunization of Lewis rats with one of the “protective” epitopes prior to induction of the disease induced antibodies against the whole molecule as well as resistance to disease induction. This peptide corresponds also to the self-HSP 60 epitope to which antibodies were found in the arthritis-resistant rats, but not in the arthritis-susceptible naive Lewis rats.
SUMMARY
The present invention relates to a peptide comprising the amino acid sequence. substantially as denoted by SEQ ID NO:1 and biologically functional homologues and derivatives thereof.
More particularly, the invention relates to a peptide having the amino acid sequence substantially as denoted by SEQ ID NO:2 and biologically functional homologues and derivatives thereof and to a peptide having the amino acid sequence substantially as denoted by SEQ ID NO:3 and biologically functional homologues and derivatives thereof.
In addition, the invention relates to a peptide comprising the amino acid sequence substantially as denoted by SEQ ID NO:4 and biologically functional homologues and derivatives thereof.
The peptides of the invention can be synthetic peptides and chemically modified peptides.
The peptides of the invention are capable of conferring immunity against autoimmune and/or inflammatory disorders.
In a further aspect, the invention relates to a nucleic acid sequence encoding a peptide of the invention and to DNA constructs comprising the same.
In yet a further aspect, the invention relates to vaccines comprising as an active ingredient an effective vaccinating amount of at least one peptide of the invention, or a nucleic acid according to the invention. The vaccines of the invention are particularly useful in conferring immunity against autoimmune or inflammatory disorders.
Still further, the invention relates to antibodies directed against the peptides of the invention and to compositions comprising them. The compositions of the invention are particularly useful for passive vaccination against autoimmune or inflammatory disorders.
The details of one or more embodiments of the invention are set forth in the accompanying drawings and the description below. Other features, objects, and advantages of the invention will be apparent from the description and drawings, and from the claims.


REFERENCES:
patent: 5780034 (1998-07-01), Cohen et al.
patent: 5985287 (1999-11-01), Tan et al.
patent: WO 95/25744 (1995-09-01), None
patent: WO 96/10039 (1996-04-01), None
Lederman et al. Molecular Immunology 1991; 28: 1171-1181.*
Li et al. Proc. Natl. Acad. Sci. USA 1980; 77: 3211-3214.*
Van Regenmortel “Methods: A Companion to Methods of Enzymology” 1996; 9:465-472.*
Anderton et al., “Inflammation activates self hsp60-specific T cells”,Eur. J. Immuno., 23:33-38, 1993.
Anderton et al., “Activation of T Cells Recognizing Self 60-kD Heat Shock Protein Can Protect against Experimental Arthritis”,J. Exp. Med., 181:943-952, 1995.
Anderton et al., “Differential Mycobacterial 65-kDa Heat Shock Protein T Cell Epitope Recognition after Adjuvant Arthritis-Inducing or Protective Immunization Protocols”,Journal of Immunology, 152:3656-3664, 1994.
Barker et al., “Differential Effects of Immunisation with Mycobacterial 65 kD Heat Shock Protein on Two Models of Autoimmunity”,Immunity, 14:73-77, 1992.
Billingham et al., “A Mycobacterial 65-kD Heat Shock Protein Induces Antigen-Specific Suppression Of Adjuvant Arthritis, But Is Not Itself Arthritogenic”,J. Exp. Med., 171:339-344, 1990.
Chen et al., “Human 60-kDa Heat-Shock Protein: A Danger Signal to the Innate Immune System”,The Journal of Immunology, 162:3212-3219, 1999.
Elias, D and Cohen, IR, “The hsp60 Peptide p277 Arrests the Autoimmune Diabetes Induced by the Toxin Streptozotocin”,Diabetes, 45:1168-1172, 1996.
Elais, D and Cohen, IR, “Peptide therapy for diabetes in NOD mice”,The Lancet, 343:704-706, 1994.
Friedland et al., “Mycobacterial 65-kD heat shock protein induces release of proinflammatory cytokines from human monocytic cell”,Clin. Exp. Immunol., 91:58-62, 1993.
Ghoraishian et al., “Comparison between the protective effects of mycobacterial 65-kD heat shock protein and ovomucoid in pristane-induced arthritis: relationship with agalactosyl IgC”,Clin. Exp. Immunol., 94:247-251, 1993.
Griffiths et al., “

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