ADJUVANT ARTHRITIS AND IMMUNITY TO THE MYCOBACTERIAL 65-KDA HEAT-SHOCK PROTEIN

被引:34
|
作者
HOGERVORST, EJM
WAGENAAR, JPA
BOOG, CJP
VANDERZEE, R
VANEMBDEN, JDA
VANEDEN, W
机构
[1] UNIV UTRECHT,FAC VET MED,DEPT IMMUNOL,DIV INFECT DIS & IMMUNOL,UTRECHT,NETHERLANDS
[2] NATL INST PUBL HLTH & ENVIRONM PROTECT,DEPT BACTERIOL,BILTHOVEN,NETHERLANDS
来源
INTERNATIONAL IMMUNOLOGY | 1992年 / 4卷 / 07期
关键词
AUTOIMMUNITY; T-CELL PROLIFERATION; IMMUNOMODULATION; ANTIBODY PRODUCTION;
D O I
10.1093/intimm/4.7.719
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 mycobacterial 65 kDa heat shock protein (HSP65) is of critical significance in the model of adjuvant arthritis (AA). Arthritogenic and protective T cell clones obtained from arthritic rats recognized the 180 - 188 sequence of HSP65. Previous reports have shown that administration of HSP65 prior to disease induction led to resistance to arthritis in the AA model and in several other models of experimental arthritis. Here, we report the development of immunity to HSP65 and the critical 180 - 188 epitope during the course of AA. Following Mycobacterium tuberculosis (MT) immunization both antibodies and T cell responses to HSP65 were detected. Proliferative responses to the 180 - 188 epitope were seen exclusively in the local draining lymph node cells at day 14 after immunization. The anatomical distribution and course of T cell responses to HSP65 and its 180 - 188 epitope are compatible with T cell regulated control of the disease. Although lower HSP65 antibody levels were observed in the animals with severe arthritis, in individual animals no evidence was obtained for a relationship between development of HSP65 humoral immunity and arthritis severity. Nevertheless, during disease exacerbation, elicited by HSP65 immunization during disease development, elevated T cell responses against HSP65 and its 180 - 188 epitope were found. In contrast, we obtained evidence that successful transfer of arthritis resistance to naive recipients depends on the transfer of HSP65 specific T cells. On the basis of these results, it seems that HSP65 plays a crucial role in the T cell regulatory events involved in both the induction of, and protection against, AA. Although, these findings offer perspectives for immunological intervention of arthritis using HSP65 itself or HSP65 specific T cells, the present findings on the versatile aspects of the immunomodulatory qualities of HSP65 should be taken into account in designing protocols for triggering protective T cell regulation.
引用
收藏
页码:719 / 727
页数:9
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