Herkel J, Erez-Alon N, Mimran A, Wolkowicz R, Harmelin A, Ruiz P, Rotter V, Cohen I R
Department of Immunology, Weizmann Institute of Science, Rehovot, Israel.
Eur J Immunol. 2000 Apr;30(4):977-84. doi: 10.1002/(SICI)1521-4141(200004)30:4<977::AID-IMMU977>3.0.CO;2-A.
The tumor suppressor molecule p53 features a regulatory domain at the C terminus that recognizes damaged DNA. Since damaged DNA might be involved in activating anti-DNA autoantibodies, we tested whether autoimmunity to the C terminus of p53 might mark murine systemic lupus erythematosus (SLE). We now report that MRL / MpJ-Fas(lpr) mice, which spontaneously develop SLE, produce antibodies both to the C terminus of p53 and to a monoclonal antibody (PAb-421) that binds the p53 C terminus. Anti-idiotypic antibodies to PAb-421 (sampled as monoclonal antibodies) could also bind DNA. Thus, the PAb-421 antibody mimics DNA, and the anti-idiotypic antibody to PAb-421 mimics the p53 DNA-binding site. This mimicry was functional; immunization of BALB / c mice to PAb-421 induced anti-DNA antibodies and antibodies to the C terminus of p53, and most of the mice developed an SLE-like disease. Immunization of C57BL / 6 mice to PAb-421 induced antibodies to p53, but not to its C-terminal domain. The C57BL / 6 mice also did not develop anti-DNA antibodies or the SLE-like disease. Thus, network autoimmunity to the domain of p53 that recognizes damaged DNA can be a pathogenic feature in SLE in genetically susceptible strains of mice.
肿瘤抑制分子p53在其C末端有一个识别受损DNA的调节结构域。由于受损DNA可能参与激活抗DNA自身抗体,我们测试了针对p53 C末端的自身免疫是否可能是小鼠系统性红斑狼疮(SLE)的标志。我们现在报告,自发发生SLE的MRL / MpJ-Fas(lpr)小鼠产生了针对p53 C末端以及针对结合p53 C末端的单克隆抗体(PAb-421)的抗体。针对PAb-421的抗独特型抗体(作为单克隆抗体取样)也能结合DNA。因此,PAb-421抗体模拟了DNA,而针对PAb-421的抗独特型抗体模拟了p53的DNA结合位点。这种模拟是有功能的;用PAb-421免疫BALB / c小鼠可诱导产生抗DNA抗体和针对p53 C末端的抗体,并且大多数小鼠发展出类似SLE的疾病。用PAb-421免疫C57BL / 6小鼠可诱导产生针对p53的抗体,但不产生针对其C末端结构域的抗体。C57BL / 6小鼠也未产生抗DNA抗体或类似SLE的疾病。因此,针对p53识别受损DNA结构域的网络自身免疫可能是基因易感小鼠品系中SLE的致病特征。
