SIMILAR PEPTIDES FROM 2 BETA-CELL AUTOANTIGENS, PROINSULIN AND GLUTAMIC-ACID DECARBOXYLASE, STIMULATE T-CELLS OF INDIVIDUALS AT RISK FOR INSULIN-DEPENDENT DIABETES

被引：88

作者：

RUDY, G ^{[1
]}

STONE, N ^{[1
]}

HARRISON, LC ^{[1
]}

COLMAN, PG ^{[1
]}

MCNAIR, P ^{[1
]}

BRUSIC, V ^{[1
]}

FRENCH, MB ^{[1
]}

HONEYMAN, MC ^{[1
]}

TAIT, B ^{[1
]}

LEW, AM ^{[1
]}

机构：

[1] WALTER & ELIZA HALL INST MED RES,MELBOURNE,VIC 3050,AUSTRALIA

来源：

MOLECULAR MEDICINE | 1995年 / 1卷 / 06期

关键词：

D O I：

10.1007/BF03401603

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Background: Insulin (1) and glutamic acid decarboxylase (GAD) (2) are both autoantigens in insulin-dependent diabetes mellitus (IDDM), but no molecular mechanism has been proposed for their association. We have identified a 13 amino acid peptide of proinsulin (amino acids 24-36) that bears marked similarity to a peptide of GAD65 (amino acids 506-518) (G. Rudy, unpublished). In order to test the hypothesis that this region of similarity is implicated in the pathogenesis of IDDM, we assayed T cell reactivity to these two peptides in subjects at risk for IDDM. Materials and Methods: subjects at risk for IDDM were islet cell antibody (ICA)-positive, first degree relatives of people with insulin-dependent diabetes. Peripheral blood mononuclear cells from 10 pairs of at-risk and HLA-DR matched control subjects were tested in an in vitro proliferation assay. Results: Reactivity to both proinsulin and GAD peptides was significantly greater among at-risk subjects than controls (proinsulin; p < 0.008; GAD: p < 0.018). In contrast to reactivity to the GAD peptide, reactivity to the proinsulin peptide was almost entirely confined to the at-risk subjects. Conclusions: This is the first demonstration of T cell reactivity to a proinsulin-specific peptide. In addition, it is the first example of reactivity to a minimal peptide region shared between two human autoimmune disease-associated self antigens. Mimicry between these similar peptides may provide a molecular basis for the conjoint autoantigenicity of proinsulin and GAD in IDDM.

引用

页码：625 / 633

页数：9

共 44 条

[1] CELLULAR-IMMUNITY TO A DETERMINANT COMMON TO GLUTAMATE-DECARBOXYLASE AND COXSACKIE-VIRUS IN INSULIN-DEPENDENT DIABETES [J].

ATKINSON, MA ;

BOWMAN, MA ;

CAMPBELL, L ;

DARROW, BL ;

KAUFMAN, DL ;

MACLAREN, NK .

JOURNAL OF CLINICAL INVESTIGATION, 1994, 94 (05) :2125-2129

[2] IDENTIFICATION OF THE 64K AUTOANTIGEN IN INSULIN-DEPENDENT DIABETES AS THE GABA-SYNTHESIZING ENZYME GLUTAMIC-ACID DECARBOXYLASE [J].

BAEKKESKOV, S ;

AANSTOOT, HJ ;

CHRISTGAU, S ;

REETZ, A ;

SOLIMENA, M ;

CASCALHO, M ;

FOLLI, F ;

RICHTEROLESEN, H ;

CAMILLI, PD .

NATURE, 1990, 347 (6289) :151-156

[3] PROINSULIN AUTOANTIBODIES ARE MORE CLOSELY ASSOCIATED WITH TYPE-1 (INSULIN-DEPENDENT) DIABETES-MELLITUS THAN INSULIN AUTOANTIBODIES [J].

BOHMER, K ;

KEILACKER, H ;

KUGLIN, B ;

HUBINGER, A ;

BERTRAMS, J ;

GRIES, FA ;

KOLB, H .

DIABETOLOGIA, 1991, 34 (11) :830-834

[4] INSITU CHARACTERIZATION OF AUTOIMMUNE PHENOMENA AND EXPRESSION OF HLA MOLECULES IN THE PANCREAS IN DIABETIC INSULITIS [J].

BOTTAZZO, GF ;

DEAN, BM ;

MCNALLY, JM ;

MACKAY, EH ;

SWIFT, PGF ;

GAMBLE, DR .

NEW ENGLAND JOURNAL OF MEDICINE, 1985, 313 (06) :353-360

[5] IDENTIFICATION OF A DOMINANT EPITOPE OF GLUTAMIC-ACID DECARBOXYLASE (GAD-65) RECOGNIZED BY AUTOANTIBODIES IN STIFF-MAN SYNDROME [J].

BUTLER, MH ;

SOLIMENA, M ;

DIRKX, R ;

HAYDAY, A ;

DECAMILLI, P .

JOURNAL OF EXPERIMENTAL MEDICINE, 1993, 178 (06) :2097-2106

[6] INTERCELLULAR-ADHESION MOLECULE-1 IS INDUCED ON ISOLATED ENDOCRINE ISLET CELLS BY CYTOKINES BUT NOT BY REOVIRUS INFECTION [J].

CAMPBELL, IL ;

CUTRI, A ;

WILKINSON, D ;

BOYD, AW ;

HARRISON, LC .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (11) :4282-4286

[7]

CAMPBELL IL, 1988, MOL ENDOCRINOL, V2, P101

[8] INTRAORGANELLAR CALCIUM AND PH CONTROL PROINSULIN CLEAVAGE IN THE PANCREATIC BETA-CELL VIA 2 DISTINCT SITE-SPECIFIC ENDOPEPTIDASES [J].

DAVIDSON, HW ;

RHODES, CJ ;

HUTTON, JC .

NATURE, 1988, 333 (6168) :93-96

[9] DETERMINANT CAPTURE AS A POSSIBLE MECHANISM OF PROTECTION AFFORDED BY MAJOR HISTOCOMPATIBILITY COMPLEX CLASS-II MOLECULES IN AUTOIMMUNE-DISEASE [J].

DENG, HK ;

APPLE, R ;

CLARESALZLER, M ;

TREMBLEAU, S ;

MATHIS, D ;

ADORINI, L ;

SERCARZ, E .

JOURNAL OF EXPERIMENTAL MEDICINE, 1993, 178 (05) :1675-1680

[10]

DUPRE J, 1989, IMMUNOTHERAPY TYPE 1, P125

← 1 2 3 4 5 →