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ZBTB 转录因子的二聚化选择和其他功能。

Dimerization choice and alternative functions of ZBTB transcription factors.

机构信息

Department of Molecular Biology and Genetics, Faculty of Arts and Sciences, Boğaziçi University, Istanbul, Turkey.

出版信息

FEBS J. 2024 Jan;291(2):237-255. doi: 10.1111/febs.16905. Epub 2023 Jul 21.

Abstract

Zinc Finger DNA-binding domain-containing proteins are the most populous family among eukaryotic transcription factors. Among these, members of the BTB domain-containing ZBTB sub-family are mostly known for their transcriptional repressive functions. In this Viewpoint article, we explore molecular mechanisms that potentially diversify the function of ZBTB proteins based on their homo and heterodimerization, alternative splicing and post-translational modifications. We describe how the BTB domain is as much a scaffold for the assembly of co-repressors, as a domain that regulates protein stability. We highlight another mechanism that regulates ZBTB protein stability: phosphorylation in the zinc finger domain. We explore the non-transcriptional, structural roles of ZBTB proteins and highlight novel findings that describe the ability of ZBTB proteins to associate with poly adenosine ribose in the nucleus during the DNA damage response. Herein, we discuss the contribution of BTB domain scaffolds to the formation of transcriptional repressive complexes, to chromosome compartmentalization and their non-transcriptional, purely structural functions in the nucleus.

摘要

锌指 DNA 结合域蛋白是真核转录因子中最丰富的家族。在这些蛋白中,BTB 结构域蛋白家族的成员以其转录抑制功能而闻名。在这篇观点文章中,我们探讨了基于同源和异源二聚化、选择性剪接和翻译后修饰的分子机制,这些机制可能使 ZBTB 蛋白的功能多样化。我们描述了 BTB 结构域既是共抑制因子组装的支架,也是调节蛋白稳定性的结构域。我们强调了另一种调节 ZBTB 蛋白稳定性的机制:锌指结构域中的磷酸化。我们探讨了 ZBTB 蛋白的非转录、结构作用,并强调了新的发现,这些发现描述了 ZBTB 蛋白在 DNA 损伤反应过程中能够与细胞核中的多聚腺苷酸核糖结合的能力。本文讨论了 BTB 结构域支架在转录抑制复合物形成、染色体区室化以及细胞核中非转录、纯粹的结构功能中的贡献。

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