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-EWS 蛋白 N 端低复杂度区的乙酰葡萄糖胺化降低相分离并增强液滴动力学。

-Linked--Acetylglucosaminylation of the RNA-Binding Protein EWS N-Terminal Low Complexity Region Reduces Phase Separation and Enhances Condensate Dynamics.

机构信息

Molecular Medicine Program, The Hospital for Sick Children, Toronto, ON M5G 0A4, Canada.

Department of Biochemistry, University of Toronto, Toronto, ON M5S 1A8, Canada.

出版信息

J Am Chem Soc. 2021 Aug 4;143(30):11520-11534. doi: 10.1021/jacs.1c04194. Epub 2021 Jul 25.

Abstract

Many membraneless organelles are thought to be biomolecular condensates formed by phase separation of proteins and other biopolymers. Post-translational modifications (PTMs) can impact protein phase separation behavior, although for many PTMs this aspect of their function is unknown. -linked β-D--acetylglucosaminylation (-GlcNAcylation) is an abundant form of intracellular glycosylation whose roles in regulating biomolecular condensate assembly and dynamics have not been delineated. Using an approach, we found that -GlcNAcylation reduces the phase separation propensity of the EWS -terminal low complexity region (LCR) under different conditions, including in the presence of the arginine- and glycine-rich RNA-binding domains (RBD). -GlcNAcylation enhances fluorescence recovery after photobleaching (FRAP) within EWS LCR condensates and causes the droplets to exhibit more liquid-like relaxation following fusion. Following extended incubation times, EWS LCR+RBD condensates exhibit diminished FRAP, indicating a loss of fluidity, while condensates containing the -GlcNAcylated LCR do not. In HeLa cells, EWS is less -GlcNAcylated following knockdown, which correlates with its increased accumulation in a filter retardation assay. Relative to the human proteome, -GlcNAcylated proteins are enriched with regions that are predicted to phase separate, suggesting a general role of -GlcNAcylation in regulation of biomolecular condensates.

摘要

许多无膜细胞器被认为是蛋白质和其他生物聚合物相分离形成的生物分子凝聚物。翻译后修饰 (PTM) 可以影响蛋白质相分离行为,但对于许多 PTM 来说,其功能的这一方面尚不清楚。链接的 β-D--乙酰氨基葡萄糖基化 (-GlcNAcylation) 是一种丰富的细胞内糖基化形式,其在调节生物分子凝聚物组装和动力学中的作用尚未确定。使用一种方法,我们发现 -GlcNAcylation 降低了 EWS 末端低复杂度区域 (LCR) 在不同条件下的相分离倾向,包括在存在精氨酸和甘氨酸丰富的 RNA 结合结构域 (RBD) 的情况下。-GlcNAcylation 增强了 EWS LCR 凝聚物中的荧光恢复后漂白 (FRAP),并导致液滴在融合后表现出更类似液体的松弛。经过长时间孵育后,EWS LCR+RBD 凝聚物的 FRAP 减少,表明流动性降低,而含有 -GlcNAcylated LCR 的凝聚物则不会。在 HeLa 细胞中, 敲低后 EWS 的 -GlcNAcylation 减少,这与其在过滤阻滞测定中的积累增加有关。与人类蛋白质组相比,-GlcNAcylated 蛋白质富含预测会相分离的区域,这表明 -GlcNAcylation 在调节生物分子凝聚物方面具有普遍作用。

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