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狼疮自身免疫起始中的自身肽。

Self-peptides in the initiation of lupus autoimmunity.

作者信息

Bockenstedt L K, Gee R J, Mamula M J

机构信息

Department of Internal Medicine, Yale University School of Medicine, New Haven, CT 06520.

出版信息

J Immunol. 1995 Apr 1;154(7):3516-24.

PMID:7534800
Abstract

Systemic lupus erythematosus is characterized by high titers of autoantibodies directed at multiple proteins of the U1/Sm small nuclear ribonucleoproteins (snRNPs). The origin of this type of autoimmunity, that is, whether it is initiated by foreign molecular mimics or by the self-snRNPs, is not known. In this study using normal mice, we investigated the presence of autoreactive B and T cells to the D protein of murine snRNPs. Although neither B nor T cell responses could be detected after immunization with native self-snRNPs, two synthetic self-peptides corresponding to amino acids 26-40 and 56-70 of the snRNP D protein elicited strong autoreactive T cell proliferation as well as a limited Ab response that bound the self-protein in immunoblots. T cells elicited by these peptides did not respond to stimulation with native snRNPs, suggesting that the peptides are cryptic and are not processed from the native protein for presentation by APCs. After priming with either of these cryptic self-peptides, exposure of the immune system to native murine snRNPs resulted in a diversified response with Abs that immunoprecipitated snRNPs and that produced an antinuclear immunofluorescence pattern on murine cell substrates. These studies demonstrate that autoreactive B and T cells specific for self-snRNPs are components of the normal repertoire of mouse lymphocytes; they have been neither deleted nor irreversibly anergized. Furthermore, we show that a diverse autoimmune response to lupus autoantigens, snRNPs, can originate from self-peptides without the influence of foreign Ags or molecular mimics.

摘要

系统性红斑狼疮的特征是针对U1/Sm小核核糖核蛋白(snRNP)多种蛋白质的高滴度自身抗体。这种自身免疫类型的起源,即它是由外来分子模拟物还是自身snRNP引发,尚不清楚。在这项使用正常小鼠的研究中,我们调查了针对小鼠snRNP D蛋白的自身反应性B细胞和T细胞的存在情况。尽管用天然自身snRNP免疫后未检测到B细胞或T细胞反应,但对应于snRNP D蛋白氨基酸26 - 40和56 - 70的两种合成自身肽引发了强烈的自身反应性T细胞增殖以及有限的抗体反应,该抗体在免疫印迹中与自身蛋白结合。这些肽引发的T细胞对天然snRNP的刺激无反应,表明这些肽是隐蔽的,不会从天然蛋白加工后由抗原呈递细胞(APC)呈递。用这些隐蔽自身肽中的任何一种进行致敏后,免疫系统暴露于天然小鼠snRNP会导致多样化反应,产生能免疫沉淀snRNP并在小鼠细胞底物上产生抗核免疫荧光模式的抗体。这些研究表明,针对自身snRNP的自身反应性B细胞和T细胞是小鼠淋巴细胞正常库的组成部分;它们既未被删除也未不可逆地失能。此外,我们表明对狼疮自身抗原snRNP的多样化自身免疫反应可以源自自身肽,而不受外来抗原或分子模拟物的影响。

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