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CD28/B7 regulation of autoimmune diabetes

被引:16
作者
Herold, KC
Lenschow, DJ
Bluestone, JA
机构
[1] UNIV ILLINOIS, COMM IMMUNOL, CHICAGO, IL 60612 USA
[2] UNIV ILLINOIS, BEN MAY INST, CHICAGO, IL 60612 USA
来源
IMMUNOLOGIC RESEARCH | 1997年 / 16卷 / 01期
关键词
autoimmune diabetes; CD28; B7; costimulation; NOD mouse; streptozotocin; tolerance;
D O I
10.1007/BF02786324
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
The initiation and progression of autoimmune diseases, such as insulin-dependent diabetes mellitus (IDDM), are complex processes that depend on autoantigen exposure, genetic susceptibility, and secondary events that promote autoaggression. T-cell costimulation, largely mediated by CD28/B7 interactions, is a major regulatory pathway in the activation and differentiation of T-cells that cause IDDM in murine models. In this article, we summarize our results in two models of IDDM: the nonobese diabetic (NOD) mouse and diabetes induced with multiple low doses of streptozotocin (MDSDM). In both of these models, blockade of CD28/B7 costimulation regulates the development of disease. The effects of blockade vary with the intensity of cognate signal delivered to the T-cells, the timing of the costimulatory signal, and perhaps even the CD28 ligand expressed on antigen-presenting cells (APCs). Our results suggest that targeting CD28/B7 signals is a feasible approach for treatment and prevention of recurrence of autoimmune diabetes. However, the dynamic nature of these interactions highlights the importance of a clear understanding of their role in regulation of the disease.
引用
收藏
页码:71 / 84
页数:14
相关论文
共 78 条
[61]   DIFFERENTIAL T-CELL COSTIMULATORY REQUIREMENTS IN CD28-DEFICIENT MICE [J].
SHAHINIAN, A ;
PFEFFER, K ;
LEE, KP ;
KUNDIG, TM ;
KISHIHARA, K ;
WAKEHAM, A ;
KAWAI, K ;
OHASHI, PS ;
THOMPSON, CB ;
MAK, TW .
SCIENCE, 1993, 261 (5121) :609-612
[62]   ALTERED CYTOKINE ACTIVITY IN ADJUVANT INHIBITION OF AUTOIMMUNE DIABETES [J].
SHEHADEH, NN ;
LAROSA, F ;
LAFFERTY, KJ .
JOURNAL OF AUTOIMMUNITY, 1993, 6 (03) :291-300
[63]   IMMUNOTHERAPY OF THE NONOBESE DIABETIC MOUSE - TREATMENT WITH AN ANTIBODY TO T-HELPER LYMPHOCYTES [J].
SHIZURU, JA ;
TAYLOREDWARDS, C ;
BANKS, BA ;
GREGORY, AK ;
FATHMAN, CG .
SCIENCE, 1988, 240 (4852) :659-662
[64]   IMMUNE-RESPONSE TO GLUTAMIC-ACID DECARBOXYLASE CORRELATES WITH INSULITIS IN NONOBESE DIABETIC MICE [J].
TISCH, R ;
YANG, XD ;
SINGER, SM ;
LIBLAU, RS ;
FUGGER, L ;
MCDEVITT, HO .
NATURE, 1993, 366 (6450) :72-75
[65]   LOSS OF CTLA-4 LEADS TO MASSIVE LYMPHOPROLIFERATION AND FATAL MULTIORGAN TISSUE DESTRUCTION, REVEALING A CRITICAL NEGATIVE REGULATORY ROLE OF CTLA-4 [J].
TIVOL, EA ;
BORRIELLO, F ;
SCHWEITZER, AN ;
LYNCH, WP ;
BLUESTONE, JA ;
SHARPE, AH .
IMMUNITY, 1995, 3 (05) :541-547
[66]   BOTH CD28 LIGANDS CD80 (B7-1) AND CD86 (B7-2) ACTIVATE PHOSPHATIDYLINOSITOL 3-KINASE, AND WORTMANNIN REVEALS HETEROGENEITY IN THE REGULATION OF T-CELL IL-2 SECRETION [J].
UEDA, Y ;
LEVINE, BL ;
HUANG, ML ;
FREEMAN, GJ ;
NADLER, LM ;
JUNE, CH ;
WARD, SG .
INTERNATIONAL IMMUNOLOGY, 1995, 7 (06) :957-966
[67]   DEVELOPMENT OF HUMAN TH1 AND TH2 CYTOKINE RESPONSES - THE CYTOKINE PRODUCTION PROFILE OF T-CELLS IS DICTATED BY THE PRIMARY INVITRO STIMULUS [J].
VANDERPOUWKRAAN, T ;
DEJONG, R ;
AARDEN, L .
EUROPEAN JOURNAL OF IMMUNOLOGY, 1993, 23 (01) :1-5
[68]   CTLA-4 ligation blocks CD28-dependent T cell activation [J].
Walunas, TL ;
Bakker, CY ;
Bluestone, JA .
JOURNAL OF EXPERIMENTAL MEDICINE, 1996, 183 (06) :2541-2550
[69]   CTLA-4 CAN FUNCTION AS A NEGATIVE REGULATOR OF T-CELL ACTIVATION [J].
WALUNAS, TL ;
LENSCHOW, DJ ;
BAKKER, CY ;
LINSLEY, PS ;
FREEMAN, GJ ;
GREEN, JM ;
THOMPSON, CB ;
BLUESTONE, JA .
IMMUNITY, 1994, 1 (05) :405-413
[70]   LYMPHOPROLIFERATIVE DISORDERS WITH EARLY LETHALITY IN MICE DEFICIENT IN CTLA-4 [J].
WATERHOUSE, P ;
PENNINGER, JM ;
TIMMS, E ;
WAKEHAM, A ;
SHAHINIAN, A ;
LEE, KP ;
THOMPSON, CB ;
GRIESSER, H ;
MAK, TW .
SCIENCE, 1995, 270 (5238) :985-988
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