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锌指蛋白143在染色质环化与基因调控中的作用

ZNF143 in Chromatin Looping and Gene Regulation.

作者信息

Ye Bingyu, Yang Ganggang, Li Yuanmeng, Zhang Chunyan, Wang Qiwen, Yu Guoying

机构信息

State Key Laboratory of Cell Differentiation and Regulation, Henan Normal University, Xinxiang, China.

Henan International Joint Laboratory of Pulmonary Fibrosis, Henan Normal University, Xinxiang, China.

出版信息

Front Genet. 2020 Apr 7;11:338. doi: 10.3389/fgene.2020.00338. eCollection 2020.

Abstract

ZNF143, a human homolog of the transcriptional activator Staf, is a C2H2-type protein consisting of seven zinc finger domains. As a transcription factor (TF), ZNF143 is sequence specifically binding to chromatin and activates the expression of protein-coding and non-coding genes on a genome scale. Although it is ubiquitous expressed, its expression in cancer cells and tissues is usually higher than that in normal cells and tissues. Therefore, abnormal expression of ZNF143 is related to cancer cell survival, proliferation, differentiation, migration, and invasion, suggesting that new small molecules can be designed by targeting ZNF143 as it may be a good potential biomarker and therapeutic target for related cancers. However, the mechanism on how ZNF143 regulates its targeting gene remains unclear. Recently, with the development of chromatin conformation capture (3C) and its derivatives, and highthroughput sequencing technology, new findings have been obtained in the study of ZNF143. Pioneering studies have showed that ZNF143 binds directly to promoters and contributes to chromatin interactions connecting promoters to distal regulatory elements, such as enhancers. Further, it has proved that ZNF143 is involved in CCCTC-binding factor (CTCF) in establishing the conserved chromatin loops by cooperating with cohesin and other partners. These results indicate that ZNF143 is a key loop formation factor. In addition, we report ZNF143 is dynamically bound to chromatin during the cell cycle demonstrated that it is a potential mitotic bookmarking factor. It may be associated with CTCF for mitosis-to-G1 phase transition and chromatin loop re-establishment in early G1 phase. In the future, researchers could further clarify the fine mechanism of ZNF143 in mediating chromatin loops with the help of CUT&RUN (CUT&Tag) and Cut-C technology. Thus, in this review, we summarize the research progress of TF ZNF143 in detail and also predict the potential functions of ZNF143 in cell fate and identity based on our recent discoveries.

摘要

ZNF143是转录激活因子Staf的人类同源物,是一种由七个锌指结构域组成的C2H2型蛋白质。作为一种转录因子(TF),ZNF143能序列特异性地结合染色质,并在基因组范围内激活蛋白质编码基因和非编码基因的表达。尽管它在各处都有表达,但其在癌细胞和组织中的表达通常高于正常细胞和组织。因此,ZNF143的异常表达与癌细胞的存活、增殖、分化、迁移和侵袭有关,这表明可以通过靶向ZNF143设计新的小分子,因为它可能是相关癌症的一个良好潜在生物标志物和治疗靶点。然而,ZNF143如何调节其靶向基因的机制仍不清楚。最近,随着染色质构象捕获(3C)及其衍生技术以及高通量测序技术的发展,在ZNF143的研究中获得了新的发现。开创性研究表明,ZNF143直接结合启动子,并有助于染色质相互作用,将启动子与远端调控元件(如增强子)连接起来。此外,已经证明ZNF143通过与黏连蛋白和其他伙伴合作,参与CCCTC结合因子(CTCF)建立保守的染色质环。这些结果表明ZNF143是一个关键的环形成因子。此外,我们报告ZNF143在细胞周期中动态结合染色质,这表明它是一个潜在的有丝分裂书签因子。它可能与CTCF一起参与有丝分裂到G1期的转变以及G1早期染色质环的重新建立。未来,研究人员可以借助CUT&RUN(CUT&Tag)和Cut-C技术进一步阐明ZNF143介导染色质环的精细机制。因此,在本综述中,我们详细总结了转录因子ZNF143的研究进展,并根据我们最近的发现预测了ZNF143在细胞命运和特性方面的潜在功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/727c/7154149/3c8697a16dbd/fgene-11-00338-g001.jpg

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