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拓扑异构酶 2β 和 B 细胞发育过程中的 DNA 拓扑结构。

Topoisomerase 2β and DNA topology during B cell development.

机构信息

Molecular Cell Biology and Immunology, Amsterdam University Medical Centers (UMC), Vrije Universiteit Amsterdam, Amsterdam, Netherlands.

Amsterdam Infection and Immunity, Infectious Diseases, Amsterdam, Netherlands.

出版信息

Front Immunol. 2022 Aug 15;13:982870. doi: 10.3389/fimmu.2022.982870. eCollection 2022.

Abstract

Topoisomerase 2β (TOP2B) introduces transient double strand breaks in the DNA helix to remove supercoiling structures and unwind entangled DNA strains. Advances in genomic technologies have enabled the discovery of novel functions for TOP2B in processes such as releasing of the paused RNA polymerase II and maintaining the genome organization through DNA loop domains. Thus, TOP2B can regulate transcription directly by acting on transcription elongation and indirectly by controlling interactions between enhancer and promoter regions through genome folding. The identification of TOP2B mutations in humans unexpectedly revealed a unique role of TOP2B in B-cell progenitors. Here we discuss the functions of TOP2B and the mechanisms leading to the B-cell development defect in patients with TOP2B deficiency.

摘要

拓扑异构酶 2β(TOP2B)在 DNA 螺旋中引入瞬时双链断裂,以去除超螺旋结构并解开纠缠的 DNA 链。基因组技术的进步使人们发现了 TOP2B 在一些过程中的新功能,例如释放暂停的 RNA 聚合酶 II 和通过 DNA 环域维持基因组组织。因此,TOP2B 可以通过作用于转录延伸直接调节转录,也可以通过控制增强子和启动子区域之间的相互作用间接控制基因组折叠。人类 TOP2B 突变的鉴定出人意料地揭示了 TOP2B 在 B 细胞前体中的独特作用。在这里,我们讨论了 TOP2B 的功能以及导致 TOP2B 缺乏症患者 B 细胞发育缺陷的机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1603/9423374/94a23f594799/fimmu-13-982870-g001.jpg

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