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肽免疫后免疫球蛋白表位扩展与自身免疫性疾病:Sm B/B'衍生的PPPGMRPP和PPPGIRGP诱导剪接体自身免疫。

Immunoglobulin epitope spreading and autoimmune disease after peptide immunization: Sm B/B'-derived PPPGMRPP and PPPGIRGP induce spliceosome autoimmunity.

作者信息

James J A, Gross T, Scofield R H, Harley J B

机构信息

Department of Medicine, University of Oklahoma Health Sciences Center, Oklahoma City.

出版信息

J Exp Med. 1995 Feb 1;181(2):453-61. doi: 10.1084/jem.181.2.453.

Abstract

Autoantibodies from many patients with systemic lupus erythematosus bind the Sm autoantigen B/B' polypeptide. The binding of serial serum specimens to the 233 overlapping octapeptides of Sm B/B' have shown that of the B/B'-derived octapeptides, PPPGMRPP and PPPGIRGP are early targets of the autoimmune response in some lupus patients. Rabbits immunized with PPPGMRPP and PPPGIRGP develop antibodies which not only bind these octapeptides, but also subsequently bind many other octapeptides of Sm B/B'. Eventually, the rabbits immunized with one octapeptide develop autoantibodies that bind other spliceosomal proteins including D, 70K, A, and C. Any mechanisms that operate to maintain tolerance or anergy for the spliceosome are thus overcome. Features considered typical of human systemic lupus erythematosus are also found in these peptide-immunized animals, such as antinuclear antibodies, anti-Sm precipitins, anti-double-stranded DNA, thrombocytopenia, seizures, and proteinuria. This disease model provides access to a mechanism for the development of humoral autoimmunity and may provide a basis to explain the immunopathogenesis of lupus in humans.

摘要

许多系统性红斑狼疮患者的自身抗体可结合Sm自身抗原B/B'多肽。对一系列血清标本与Sm B/B'的233个重叠八肽的结合情况进行检测发现,在一些狼疮患者中,源自B/B'的八肽PPPGMRPP和PPPGIRGP是自身免疫反应的早期靶点。用PPPGMRPP和PPPGIRGP免疫的兔子产生的抗体不仅能结合这些八肽,随后还能结合Sm B/B'的许多其他八肽。最终,用一种八肽免疫的兔子会产生能结合其他剪接体蛋白(包括D、70K、A和C)的自身抗体。因此,任何维持对剪接体耐受性或无反应性的机制都会被克服。在这些经肽免疫的动物中也发现了被认为是人类系统性红斑狼疮典型特征的表现,如抗核抗体、抗Sm沉淀素、抗双链DNA、血小板减少、癫痫发作和蛋白尿。这种疾病模型为体液自身免疫的发展机制提供了研究途径,可能为解释人类狼疮的免疫发病机制提供依据。

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