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先天性免疫与适应性免疫之间可能存在的新桥梁:抗线粒体柠檬酸合酶自身抗体是天然抗体网络的组成部分吗?

A possible new bridge between innate and adaptive immunity: Are the anti-mitochondrial citrate synthase autoantibodies components of the natural antibody network?

作者信息

Czömpöly Tamás, Olasz Katalin, Simon Diána, Nyárády Zoltán, Pálinkás László, Czirják László, Berki Tímea, Németh Péter

机构信息

Department of Immunology and Biotechnology, Faculty of Medicine, University of Pécs, Szigeti út 12., Pécs H-7643, Hungary.

出版信息

Mol Immunol. 2006 Apr;43(11):1761-8. doi: 10.1016/j.molimm.2005.11.004. Epub 2005 Dec 20.

Abstract

Natural antibody (nAb) producing B-1 B cells are considered an intermediate stage of evolution between innate and adaptive immunity. nAbs are immunoglobulins that are produced without antigen priming. nAbs can recognize foreign targets and may serve in the first line of immune defense during an infection. Natural autoantibodies (nAAbs) present in the serum of both healthy humans and patients suffering from systemic autoimmune diseases recognize a set of evolutionarily conserved self-structures. Because of their endosymbiotic evolutionary origin, proteins compartmentalized into mitochondria represent an interesting transition from prokaryotic foreign (non-self) to essential (self) molecules. We investigated the possible overlap in recognized epitopes of innate and self-reactive nAbs and surveyed changes in physiological autoreactivity under pathological autoimmune conditions. Epitope mapping analysis of a mitochondrial inner membrane enzyme, citrate synthase (CS) (EC 2.3.3.1) by synthetic overlapping peptides and phage display libraries using sera from healthy individuals and from patients having systemic autoimmune disease revealed CS recognizing nAAbs with IgM isotype. We analyzed cross reactive epitopes on human CS, bacterial CS, and various standard autoantigens. The anti-CS nAAbs by participating in the nAb network, could function in innate defense mechanisms and at the same time recognize a target antigen (nucleosome) in a systemic autoimmune disease. Thus, at the level of recognized epitopes there is a possible new link between the innate like component and the adaptive-autoimmune arm of the humoral immune system.

摘要

产生天然抗体(nAb)的B - 1 B细胞被认为是先天免疫和适应性免疫之间的一个进化中间阶段。天然抗体是在没有抗原启动的情况下产生的免疫球蛋白。天然抗体可以识别外来靶点,并可能在感染期间充当免疫防御的第一道防线。健康人和患有系统性自身免疫疾病的患者血清中存在的天然自身抗体(nAAb)可识别一组进化上保守的自身结构。由于其共生进化起源,定位于线粒体的蛋白质代表了从原核外来(非自身)分子到必需(自身)分子的有趣转变。我们研究了先天和自身反应性天然抗体识别表位的可能重叠,并调查了病理自身免疫条件下生理自身反应性的变化。使用健康个体和患有系统性自身免疫疾病患者的血清,通过合成重叠肽和噬菌体展示文库对线粒体内膜酶柠檬酸合酶(CS)(EC 2.3.3.1)进行表位图谱分析,发现CS可识别IgM同种型的天然自身抗体。我们分析了人CS、细菌CS和各种标准自身抗原上的交叉反应表位。抗CS天然自身抗体通过参与天然抗体网络,可在先天防御机制中发挥作用,同时在系统性自身免疫疾病中识别靶抗原(核小体)。因此,在识别表位水平上,体液免疫系统的先天样成分与适应性自身免疫分支之间可能存在新的联系。

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