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小鼠狼疮中的组蛋白自身抗原。染色质可及区域内主要表位的定义。

Histone autoantigens in murine lupus. Definition of a major epitope within an accessible region of chromatin.

作者信息

Portanova J P, Cheronis J C, Blodgett J K, Kotzin B L

机构信息

Department of Pediatrics, National Jewish Center for Immunology and Respiratory Medicine, Denver, CO 80206.

出版信息

J Immunol. 1990 Jun 15;144(12):4633-40.

PMID:1693638
Abstract

In SLE and in the (NZB x NZW)F1 murine model of this disease, IgG autoantibodies are frequently produced to DNA and histones. In the present study, we define a linear epitope on histone H2B that is recognized by (NZB x NZW)F1 mice. IgG antibodies from anti-H2B positive (but not anti-H2B negative) mice bound strongly to a peptide containing the first 15 N-terminal amino acids, a region that is exposed in chromatin. Competitive inhibition studies showed that the binding of autoantibodies to H2B in ELISA as well as the binding to soluble H2B was substantially blocked by this peptide. Studies with smaller peptides mapped the epitope to residues 3-12. Individual mice recognized different residues within this region, and a sequence search did not reveal proteins other than H2B that could elicit this spectrum of antibodies. Interestingly, these autoantibody specificities were not a component of those induced in preautoimmune mice by immunization with H2B/RNA complexes or with H2B peptide 1-30 containing the autoantigenic sequence. These findings argue that recognition of a specific N-terminal region of self histone contributes to the anti-H2B autoantibody response in lupus. Autoreactive B cells with specificity for this sequence seem to develop only after the autoimmune process has been initiated.

摘要

在系统性红斑狼疮(SLE)以及该疾病的(新西兰黑鼠×新西兰白鼠)F1小鼠模型中,经常会产生针对DNA和组蛋白的IgG自身抗体。在本研究中,我们确定了组蛋白H2B上一个被(新西兰黑鼠×新西兰白鼠)F1小鼠识别的线性表位。来自抗H2B阳性(而非抗H2B阴性)小鼠的IgG抗体与包含前15个N端氨基酸的肽段强烈结合,该区域在染色质中是暴露的。竞争性抑制研究表明,该肽段在酶联免疫吸附测定(ELISA)中可显著阻断自身抗体与H2B的结合以及与可溶性H2B的结合。对较小肽段的研究将表位定位到第3至12位氨基酸残基。个体小鼠识别该区域内不同的氨基酸残基,序列搜索未发现除H2B以外能引发这种抗体谱的蛋白质。有趣的是,这些自身抗体特异性并非在用H2B/RNA复合物或含自身抗原序列的H2B肽段1 - 30免疫自身免疫前小鼠时所诱导的特异性的组成部分。这些发现表明,对自身组蛋白特定N端区域的识别促成了狼疮中抗H2B自身抗体反应。对该序列具有特异性的自身反应性B细胞似乎仅在自身免疫过程启动后才发育。

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