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亚细胞聚集体和信号通路中的液-液相分离:染色质修饰诱导基因调控细胞生理和功能,包括癌变。

Liquid-liquid phase separation in subcellular assemblages and signaling pathways: Chromatin modifications induced gene regulation for cellular physiology and functions including carcinogenesis.

机构信息

Epigenetics and Cancer Research Laboratory, Biochemistry and Molecular Biology Group, Department of Life Science, National Institute of Technology, Rourkela, India.

Department of Chemical Engineering, Maulana Azad National Institute of Technology, Bhopal, India.

出版信息

Biochimie. 2024 Aug;223:74-97. doi: 10.1016/j.biochi.2024.05.007. Epub 2024 May 7.

DOI:10.1016/j.biochi.2024.05.007
Abstract

Liquid-liquid phase separation (LLPS) describes many biochemical processes, including hydrogel formation, in the integrity of macromolecular assemblages and existence of membraneless organelles, including ribosome, nucleolus, nuclear speckles, paraspeckles, promyelocytic leukemia (PML) bodies, Cajal bodies (all exert crucial roles in cellular physiology), and evidence are emerging day by day. Also, phase separation is well documented in generation of plasma membrane subdomains and interplay between membranous and membraneless organelles. Intrinsically disordered regions (IDRs) of biopolymers/proteins are the most critical sticking regions that aggravate the formation of such condensates. Remarkably, phase separated condensates are also involved in epigenetic regulation of gene expression, chromatin remodeling, and heterochromatinization. Epigenetic marks on DNA and histones cooperate with RNA-binding proteins through their IDRs to trigger LLPS for facilitating transcription. How phase separation coalesces mutant oncoproteins, orchestrate tumor suppressor genes expression, and facilitated cancer-associated signaling pathways are unravelling. That autophagosome formation and DYRK3-mediated cancer stem cell modification also depend on phase separation is deciphered in part. In view of this, and to linchpin insight into the subcellular membraneless organelle assembly, gene activation and biological reactions catalyzed by enzymes, and the downstream physiological functions, and how all these events are precisely facilitated by LLPS inducing organelle function, epigenetic modulation of gene expression in this scenario, and how it goes awry in cancer progression are summarized and presented in this article.

摘要

液-液相分离 (LLPS) 描述了许多生化过程,包括水凝胶的形成,在大分子组装体的完整性和无膜细胞器的存在下,包括核糖体、核仁、核斑点、核旁斑点、早幼粒细胞白血病 (PML) 体、Cajal 体(所有这些在细胞生理学中都起着至关重要的作用),并且证据每天都在涌现。此外,相分离在质膜亚域的形成和膜性细胞器与无膜细胞器之间的相互作用中也有很好的记录。生物聚合物/蛋白质的无序区域 (IDR) 是最关键的粘性区域,加剧了这种凝聚物的形成。值得注意的是,相分离的凝聚物也参与基因表达的表观遗传调控、染色质重塑和异染色质化。DNA 和组蛋白上的表观遗传标记与 RNA 结合蛋白通过其 IDR 合作,引发 LLPS 以促进转录。相分离如何凝聚突变癌蛋白、协调肿瘤抑制基因表达、并促进癌症相关信号通路,正在逐步揭示。部分阐明了自噬体的形成和 DYRK3 介导的癌症干细胞修饰也依赖于相分离。有鉴于此,深入了解细胞内无膜细胞器的组装、酶催化的基因激活和生物反应以及下游生理功能,以及所有这些事件如何通过诱导细胞器功能的 LLPS、这种情况下的基因表达的表观遗传调控以及它在癌症进展中如何出错,都在本文中进行了总结和介绍。

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