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翻译后修饰、亚细胞定位及在凋亡微粒中的释放:凋亡将核蛋白转变为自身抗原。

Post-translational modifications, subcellular relocation and release in apoptotic microparticles: apoptosis turns nuclear proteins into autoantigens.

作者信息

Dieker Jürgen, Muller Sylviane

机构信息

Centre National de la Recherche Scientifique, Institut de Biologie Moléculaire et Cellulaire, Strasbourg, France.

出版信息

Folia Histochem Cytobiol. 2009 Jan;47(3):343-8. doi: 10.2478/v10042-009-0068-1.

Abstract

Autoantibodies against particular nuclear components, such as chromatin and snRNPs, are a characteristic feature of the autoimmune disease systemic lupus erythematosus. The last decade, evidence has suggested that apoptotic cells are the main source of autoantigens in this disease. Therefore, it has been proposed that protein modifications occurring during apoptosis lead to the formation of neo-epitopes, which can break the tolerance when apoptotic cells are not properly cleared. Indeed, many lupus autoantigens are prone to apoptosis-associated post-translational modifications and/or cleavage by caspases. In addition, lupus autoantigens are relocated from the nucleus to apoptotic blebs on the cell surface of early apoptotic cells. Therefore, to understand why certain nuclear proteins become autoantigens during apoptosis, it is important to know the apoptotic processing of these proteins. This review summarizes the current knowledge of apoptotic processing of lupus autoantigens and the possible effects on their encounter with the immune system in normal and autoimmune situations.

摘要

针对特定核成分(如染色质和小核核糖核蛋白)的自身抗体是自身免疫性疾病系统性红斑狼疮的一个特征。在过去十年中,有证据表明凋亡细胞是这种疾病中自身抗原的主要来源。因此,有人提出凋亡过程中发生的蛋白质修饰会导致新表位的形成,当凋亡细胞未被妥善清除时,这些新表位会打破免疫耐受。事实上,许多狼疮自身抗原易于发生与凋亡相关的翻译后修饰和/或被半胱天冬酶切割。此外,狼疮自身抗原会从细胞核重新定位到早期凋亡细胞表面的凋亡小泡上。因此,要理解为什么某些核蛋白在凋亡过程中会成为自身抗原,了解这些蛋白质的凋亡过程很重要。这篇综述总结了目前关于狼疮自身抗原凋亡过程的知识以及在正常和自身免疫情况下它们与免疫系统相遇时可能产生的影响。

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