Investigating the Context-Dependent Phase Separation of Human HOX Transcription Factors.

IF 3.2 4区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Srijeeb Karmakar, Jishnu Manglam, Krishna Kant, Soumya De
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Abstract

Homeobox (HOX) transcription factors are essential for gene expression during embryonic development and hematopoiesis, and their dysregulation is potentially linked to several types of cancer. Recently, liquid-liquid phase separation (LLPS) has been proposed as a key mechanism in various physiological processes. Using computational tools and molecular dynamics (MD) simulations, we found that the human HOX transcription factors have a strong propensity to undergo phase separation. The large disordered regions of the HOX factors drive phase separation via a fly-casting like mechanism, where the terminal segments of the disordered regions extend out to interact with and draw in neighboring molecules. Also, formation of short transient secondary structures in the disordered regions was observed in MD simulations. The sequences of the transient structures match short linear motifs (SliMs), which are hotspots for interaction with partner molecules. Thus, the HOX transcription factors may act as scaffold proteins and recruit partner molecules, such as TALE proteins, in the biomolecular cocondensates, via interaction with these preformed structural elements. A total of 352 SliMs were mapped with the droplet-promoting disordered regions of the human HOX transcription factors, which indicated an abundance of possible binding sites. These results have been curated in an interactive webpage (https://pel.iitkgp.ac.in/) that generates motif maps, indicating the location of the motifs in the disordered regions of the HOX transcription factors. Overall, this work highlights the potential of phase separation of the human HOX factors, particularly through the lens of context-dependent interactions, which may lead to novel insights into HOX-related processes.

研究人类HOX转录因子的环境依赖相分离。
同源盒(HOX)转录因子对胚胎发育和造血过程中的基因表达至关重要,它们的失调可能与几种类型的癌症有关。近年来,液-液相分离(LLPS)被认为是多种生理过程的关键机制。利用计算工具和分子动力学(MD)模拟,我们发现人类HOX转录因子有很强的相分离倾向。HOX因子的大无序区域通过类似飞铸的机制驱动相分离,其中无序区域的末端片段向外延伸,与邻近分子相互作用并吸引邻近分子。此外,在MD模拟中还观察到在无序区形成了短暂的瞬态二级结构。瞬态结构的序列匹配短线性基序(SliMs),这是与伙伴分子相互作用的热点。因此,HOX转录因子可以作为支架蛋白,并通过与这些预制结构元件的相互作用,在生物分子共凝物中招募伴侣分子,如TALE蛋白。共有352个slim与人类HOX转录因子的促液滴紊乱区域相关联,这表明可能存在丰富的结合位点。这些结果已经在一个交互式网页(https://pel.iitkgp.ac.in/)上进行了整理,该网页生成了基序图,表明了基序在HOX转录因子紊乱区域的位置。总的来说,这项工作强调了人类HOX因素相分离的潜力,特别是通过上下文依赖的相互作用,这可能会导致对HOX相关过程的新见解。
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来源期刊
Proteins-Structure Function and Bioinformatics
Proteins-Structure Function and Bioinformatics 生物-生化与分子生物学
CiteScore
5.90
自引率
3.40%
发文量
172
审稿时长
3 months
期刊介绍: PROTEINS : Structure, Function, and Bioinformatics publishes original reports of significant experimental and analytic research in all areas of protein research: structure, function, computation, genetics, and design. The journal encourages reports that present new experimental or computational approaches for interpreting and understanding data from biophysical chemistry, structural studies of proteins and macromolecular assemblies, alterations of protein structure and function engineered through techniques of molecular biology and genetics, functional analyses under physiologic conditions, as well as the interactions of proteins with receptors, nucleic acids, or other specific ligands or substrates. Research in protein and peptide biochemistry directed toward synthesizing or characterizing molecules that simulate aspects of the activity of proteins, or that act as inhibitors of protein function, is also within the scope of PROTEINS. In addition to full-length reports, short communications (usually not more than 4 printed pages) and prediction reports are welcome. Reviews are typically by invitation; authors are encouraged to submit proposed topics for consideration.
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