EFFECT OF ANTI-CD4 ANTIBODY TREATMENT ON INFLAMMATORY ARTHRITIS IN MRL-LPR/LPR MICE

被引:26
作者
GILKESON, GS
SPURNEY, R
COFFMAN, TM
KURLANDER, R
RUIZ, P
PISETSKY, DS
机构
[1] DURHAM VET ADM HOSP,MED RES SERV,DURHAM,NC
[2] DUKE UNIV,MED CTR,DIV NEPHROL,DURHAM,NC 27710
[3] DUKE UNIV,MED CTR,DIV HEMATOL & ONCOL,DURHAM,NC 27710
[4] UNIV MIAMI,DEPT PATHOL,MIAMI,FL 33152
来源
CLINICAL IMMUNOLOGY AND IMMUNOPATHOLOGY | 1992年 / 64卷 / 02期
关键词
D O I
10.1016/0090-1229(92)90195-T
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
MRL- lpr lpr mice develop an inflammatory arthritis in association with other manifestations of autoimmunity. Although a variety of immune cell disturbances have been described in these mice, the relationship of these abnormalities to the pathogenesis of arthritis has not yet been determined; the role of T cells is especially unclear since synovial hypertrophy and joint erosions have been noted in some studies in the absence of a significant T cell infiltrate. Therefore, to determine if T cells are required for arthritis in MRL- lpr lpr mice, we evaluated the effects of prolonged treatment with a monoclonal anti-CD4 antibody. Knee joints from treated mice had markedly reduced arthritis compared to saline-treated control animals as measured by the degree of synovial hypertrophy and inflammation. Nephritis in these mice was concomitantly reduced. In contrast, rheumatoid factor levels were not affected by CD4+ cell depletion, despite significant effects on anti-DNA. These results indicate that in MRL- lpr lpr mice anti-CD4 therapy can inhibit arthritis, suggesting an important role of T cells in the pathogenesis of this lesion. © 1992.
引用
收藏
页码:166 / 172
页数:7
相关论文
共 30 条
[1]   SPONTANEOUS MURINE LUPUS-LIKE SYNDROMES - CLINICAL AND IMMUNOPATHOLOGICAL MANIFESTATIONS IN SEVERAL STRAINS [J].
ANDREWS, BS ;
EISENBERG, RA ;
THEOFILOPOULOS, AN ;
IZUI, S ;
WILSON, CB ;
MCCONAHEY, PJ ;
MURPHY, ED ;
ROTHS, JB ;
DIXON, FJ .
JOURNAL OF EXPERIMENTAL MEDICINE, 1978, 148 (05) :1198-1215
[2]   EXPRESSION OF INTERLEUKIN-2 RECEPTORS AS A DIFFERENTIATION MARKER ON INTRATHYMIC STEM-CELLS [J].
CEREDIG, R ;
LOWENTHAL, JW ;
NABHOLZ, M ;
MACDONALD, HR .
NATURE, 1985, 314 (6006) :98-100
[3]   B220 - A B-CELL-SPECIFIC MEMBER OF THE T200 GLYCOPROTEIN FAMILY [J].
COFFMAN, RL ;
WEISSMAN, IL .
NATURE, 1981, 289 (5799) :681-683
[4]  
COHEN P L, 1989, Arthritis and Rheumatism, V32, pS52
[5]   CHARACTERIZATION OF FUNCTIONAL T-CELL LINES DERIVED FROM MRL MICE [J].
COHEN, PL ;
RAPOPORT, R ;
EISENBERG, RA .
CLINICAL IMMUNOLOGY AND IMMUNOPATHOLOGY, 1986, 40 (03) :485-496
[6]   LPR AND GLD - SINGLE GENE MODELS OF SYSTEMIC AUTOIMMUNITY AND LYMPHOPROLIFERATIVE DISEASE [J].
COHEN, PL ;
EISENBERG, RA .
ANNUAL REVIEW OF IMMUNOLOGY, 1991, 9 :243-269
[7]   SELECTIVE PRODUCTION OF INTERLEUKIN-3 (IL-3) AND GRANULOCYTE-MACROPHAGE COLONY-STIMULATING FACTOR (GM-CSF) INVITRO BY MURINE L3T4+ T-CELLS - LACK OF SPONTANEOUS IL-3 AND GM-CSF PRODUCTION BY LY-2-/L3T4- LPR SUBSET [J].
DAVIGNON, JL ;
KIMOTO, M ;
KINDLER, V ;
DEKOSSODO, S ;
VASSALLI, P ;
IZUI, S .
EUROPEAN JOURNAL OF IMMUNOLOGY, 1988, 18 (09) :1367-1372
[8]  
FINKELMAN FD, 1988, J IMMUNOL, V140, P1022
[9]   GENETIC-CONTROL OF INFLAMMATORY ARTHRITIS IN CONGENIC IPR MICE [J].
GILKESON, GS ;
RUIZ, P ;
GRUDIER, JP ;
KURLANDER, RJ ;
PISETSKY, DS .
CLINICAL IMMUNOLOGY AND IMMUNOPATHOLOGY, 1989, 53 (03) :460-474
[10]   GENETIC-CONTROL OF INFLAMMATORY ARTHRITIS AND GLOMERULONEPHRITIS IN CONGENIC LPR MICE AND THEIR F1 HYBRIDS [J].
GILKESON, GS ;
RUIZ, P ;
PRITCHARD, AJ ;
PISETSKY, DS .
JOURNAL OF AUTOIMMUNITY, 1991, 4 (04) :595-606
123