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DNA mismatch repair enzymes: Genetic defects and autoimmunity

机译:DNA错配修复酶:遗传缺陷和自身免疫

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摘要

DNA mismatch repair (MMR) is one of the several DNA repair pathways conserved from bacteria to humans. The primary function of MMR is to eliminate the mismatch of base-base insertions and deletions that appear as a consequence of DNA polymerase errors at DNA synthesis. The genes encoding the DNA MMR enzymes (MMREs) are highly conserved throughout evolution. In humans, there are two sets of MMREs, corresponding to homologues of the bacterial MutLS systems. The human MutS enzymes consist of MSH2, MSH3 and MSH6, and the human MutL enzymes include MLH1, MLH3, PMS1 and PMS2. Since the beginning of this century, a few reports on autoantibodies to some MMREs have been reported in autoimmune inflammatory myopathy, cancer and hematological disorders. This review charts the functional structures of MMREs, their genetic defects and associated disorders, and autoimmunity to MMREs, including our recent data that was the first to analyze autoantibodies against all seven kinds of MMREs in systemic autoimmune diseases, including idiopathic inflammatory myopathies. (C) 2015 Elsevier B.V. All rights reserved.
机译:DNA错配修复(MMR)是从细菌到人类保守的几种DNA修复途径之一。 MMR的主要功能是消除DNA合成中DNA聚合酶错误导致的碱基插入和缺失不匹配。编码DNA MMR酶(MMRE)的基因在整个进化过程中高度保守。在人类中,有两组MMRE,分别对应于细菌MutLS系统的同源物。人MutS酶由MSH2,MSH3和MSH6组成,人MutL酶包括MLH1,MLH3,PMS1和PMS2。自本世纪初以来,已报道了一些针对一些MMRE自身抗体的报道,涉及自身免疫性炎性肌病,癌症和血液系统疾病。这篇综述绘制了MMRE的功能结构,它们的遗传缺陷和相关疾病以及对MMRE的自身免疫性,包括我们最近的数据,这是第一个分析针对全身性自身免疫性疾病包括特发性炎症性肌病的所有7种MMRE自身抗体的数据。 (C)2015 Elsevier B.V.保留所有权利。

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