A disordered region controls cBAF activity via condensation and partner recruitment

生物 染色质 内在无序蛋白质 功能(生物学) 染色质重塑 计算生物学 嘉雅宠物 细胞生物学 遗传学 生物化学 基因
作者
Ajinkya Patil,Amy R. Strom,João A. Paulo,Clayton K. Collings,Kiersten M. Ruff,Min Kyung Shinn,Akshay Sankar,Kasey S. Cervantes,Tobias Wauer,Jessica D. St. Laurent,Grace Xu,Lindsay A. Becker,Steven P. Gygi,Rohit V. Pappu,Clifford P. Brangwynne,Cigall Kadoch
出处
期刊:Cell [Cell Press]
卷期号:186 (22): 4936-4955.e26 被引量:17
标识
DOI:10.1016/j.cell.2023.08.032
摘要

Intrinsically disordered regions (IDRs) represent a large percentage of overall nuclear protein content. The prevailing dogma is that IDRs engage in non-specific interactions because they are poorly constrained by evolutionary selection. Here, we demonstrate that condensate formation and heterotypic interactions are distinct and separable features of an IDR within the ARID1A/B subunits of the mSWI/SNF chromatin remodeler, cBAF, and establish distinct "sequence grammars" underlying each contribution. Condensation is driven by uniformly distributed tyrosine residues, and partner interactions are mediated by non-random blocks rich in alanine, glycine, and glutamine residues. These features concentrate a specific cBAF protein-protein interaction network and are essential for chromatin localization and activity. Importantly, human disease-associated perturbations in ARID1B IDR sequence grammars disrupt cBAF function in cells. Together, these data identify IDR contributions to chromatin remodeling and explain how phase separation provides a mechanism through which both genomic localization and functional partner recruitment are achieved.
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