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RAG重组酶的调控与进化

Regulation and Evolution of the RAG Recombinase.

作者信息

Teng Grace, Schatz David G

机构信息

Department of Immunobiology, Yale University School of Medicine, New Haven, Connecticut, USA.

Department of Immunobiology, Yale University School of Medicine, New Haven, Connecticut, USA; Howard Hughes Medical Institute, Chevy Chase, Maryland, USA.

出版信息

Adv Immunol. 2015;128:1-39. doi: 10.1016/bs.ai.2015.07.002. Epub 2015 Aug 4.

Abstract

The modular, noncontiguous architecture of the antigen receptor genes necessitates their assembly through V(D)J recombination. This program of DNA breakage and rejoining occurs during early lymphocyte development, and depends on the RAG1 and RAG2 proteins, whose collaborative endonuclease activity targets specific DNA motifs enriched in the antigen receptor loci. This essential gene shuffling reaction requires lymphocytes to traverse several developmental stages wherein DNA breakage is tolerated, while minimizing the expense to overall genome integrity. Thus, RAG activity is subject to stringent temporal and spatial regulation. The RAG proteins themselves also contribute autoregulatory properties that coordinate their DNA cleavage activity with target chromatin structure, cell cycle status, and DNA repair pathways. Even so, lapses in regulatory restriction of RAG activity are apparent in the aberrant V(D)J recombination events that underlie many lymphomas. In this review, we discuss the current understanding of the RAG endonuclease, its widespread binding in the lymphocyte genome, its noncleavage activities that restrain its enzymatic potential, and the growing evidence of its evolution from an ancient transposase.

摘要

抗原受体基因的模块化、非连续结构使其必须通过V(D)J重组进行组装。这种DNA断裂和重新连接程序发生在淋巴细胞早期发育过程中,并且依赖于RAG1和RAG2蛋白,它们的协同内切核酸酶活性靶向富含抗原受体基因座的特定DNA基序。这种至关重要的基因重排反应要求淋巴细胞经历几个发育阶段,在这些阶段中DNA断裂是可容忍的,同时将对整个基因组完整性的损害降至最低。因此,RAG活性受到严格的时间和空间调控。RAG蛋白本身也具有自我调节特性,可将其DNA切割活性与靶染色质结构、细胞周期状态和DNA修复途径协调起来。即便如此,在许多淋巴瘤所基于的异常V(D)J重组事件中,RAG活性的调控限制失误依然明显。在这篇综述中,我们讨论了目前对RAG内切核酸酶的理解、它在淋巴细胞基因组中的广泛结合、抑制其酶活性的非切割活性,以及越来越多关于它从古老转座酶进化而来的证据。

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