Chromatin-IgG complexes activate B cells by dual engagement of IgM and Toll-like receptors

被引:1503
作者
Leadbetter, EA
Rifkin, IR
Hohlbaum, AM
Beaudette, BC
Shlomchik, MJ
Marshak-Rothstein, A [1 ]
机构
[1] Boston Univ, Sch Med, Dept Microbiol, Boston, MA 02118 USA
[2] Boston Univ, Sch Med, Dept Med, Boston, MA 02118 USA
[3] Yale Univ, Sch Med, Dept Lab Med, New Haven, CT 06520 USA
[4] Yale Univ, Sch Med, Dept Immunobiol, New Haven, CT 06520 USA
关键词
D O I
10.1038/416603a
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Autoreactive B cells are present in the lymphoid tissues of healthy individuals, but typically remain quiescent. When this homeostasis is perturbed, the formation of self-reactive antibodies can have serious pathological consequences. B cells expressing an antigen receptor specific for self-immunoglobulin-g (IgG) make a class of autoantibodies known as rheumatoid factor (RF). Here we show that effective activation of RF+ B cells is mediated by IgG2a-chromatin immune complexes and requires the synergistic engagement of the antigen receptor and a member of the MyD88-dependent Toll-like receptor (TLR) family. Inhibitor studies implicate TLR9. These data establish a critical link between the innate and adaptive immune systems in the development of systemic autoimmune disease and explain the preponderance of autoantibodies reactive with nucleic acid-protein particles. The unique features of this dual-engagement pathway should facilitate the development of therapies that specifically target autoreactive B cells.
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页码:603 / 607
页数:5
相关论文
共 40 条
[1]   Targeted disruption of the MyD88 gene results in loss of IL-1- and IL-18-mediated function [J].
Adachi, O ;
Kawai, T ;
Takeda, K ;
Matsumoto, M ;
Tsutsui, H ;
Sakagami, M ;
Nakanishi, K ;
Akira, S .
IMMUNITY, 1998, 9 (01) :143-150
[2]   Disruption of the Cr2 locus results in a reduction in B-1a cells and in an impaired B cell response to T-dependent antigen [J].
Ahearn, JM ;
Fischer, MB ;
Croix, D ;
Goerg, S ;
Ma, MH ;
Xia, JR ;
Zhou, XN ;
Howard, RG ;
Rothstein, TL ;
Carroll, MC .
IMMUNITY, 1996, 4 (03) :251-262
[3]   Toll-like receptors: critical proteins linking innate and acquired immunity [J].
Akira, S ;
Takeda, K ;
Kaisho, T .
NATURE IMMUNOLOGY, 2001, 2 (08) :675-680
[4]   THE SPONTANEOUS APOPTOTIC CELL-DEATH OF NORMAL HUMAN-LYMPHOCYTES INVITRO - THE RELEASE OF, AND IMMUNOPROLIFERATIVE RESPONSE TO, NUCLEOSOMES INVITRO [J].
BELL, DA ;
MORRISON, B .
CLINICAL IMMUNOLOGY AND IMMUNOPATHOLOGY, 1991, 60 (01) :13-26
[5]   IMMUNOGENIC DNA-RELATED FACTORS - NUCLEOSOMES SPONTANEOUSLY RELEASED FROM NORMAL MURINE LYMPHOID-CELLS STIMULATE PROLIFERATION AND IMMUNOGLOBULIN-SYNTHESIS OF NORMAL MOUSE LYMPHOCYTES [J].
BELL, DA ;
MORRISON, B ;
VANDENBYGAART, P .
JOURNAL OF CLINICAL INVESTIGATION, 1990, 85 (05) :1487-1496
[6]   HOW MHC CLASS-II MOLECULES REACH THE ENDOCYTIC PATHWAY [J].
BENAROCH, P ;
YILLA, M ;
RAPOSO, G ;
ITO, K ;
MIWA, K ;
GEUZE, HJ ;
PLOEGH, HL .
EMBO JOURNAL, 1995, 14 (01) :37-49
[7]   Serum amyloid P component controls chromatin degradation and prevents antinuclear autoimmunity [J].
Bickerstaff, MCM ;
Botto, M ;
Hutchinson, WL ;
Herbert, J ;
Tennent, GA ;
Bybee, A ;
Mitchell, DA ;
Cook, HT ;
Butler, PJG ;
Walport, MJ ;
Pepys, MB .
NATURE MEDICINE, 1999, 5 (06) :694-697
[8]   Homozygous C1q deficiency causes glomerulonephritis associated with multiple apoptotic bodies [J].
Botto, M ;
Dell'Agnola, C ;
Bygrave, AE ;
Thompson, EM ;
Cook, HT ;
Petry, F ;
Loos, M ;
Pandolfi, PP ;
Walport, MJ .
NATURE GENETICS, 1998, 19 (01) :56-59
[9]  
CARTER RH, 1988, J IMMUNOL, V141, P457
[10]  
EMLEN W, 1992, J IMMUNOL, V148, P3042