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稀相中的异型相互作用可驱动FET蛋白的朊病毒样低复杂性结构域与哺乳动物SWI/SNF复合物的共凝聚。

Heterotypic interactions in the dilute phase can drive co-condensation of prion-like low-complexity domains of FET proteins and mammalian SWI/SNF complex.

作者信息

Davis Richoo B, Supakar Anushka, Ranganath Aishwarya Kanchi, Moosa Mahdi Muhammad, Banerjee Priya R

机构信息

Department of Physics, University at Buffalo, Buffalo NY 14260, USA.

Department of Biological Sciences, University at Buffalo, Buffalo NY 14260, USA.

出版信息

bioRxiv. 2023 Nov 22:2023.04.12.536623. doi: 10.1101/2023.04.12.536623.

Abstract

Prion-like domains (PLDs) are low-complexity protein sequences enriched within nucleic acid-binding proteins including those involved in transcription and RNA processing. PLDs of FUS and EWSR1 play key roles in recruiting chromatin remodeler mammalian SWI/SNF complex to oncogenic FET fusion protein condensates. Here, we show that disordered low-complexity domains of multiple SWI/SNF subunits are prion-like with a strong propensity to undergo intracellular phase separation. These PLDs engage in sequence-specific heterotypic interactions with the PLD of FUS in the dilute phase at sub-saturation conditions, leading to the formation of PLD co-condensates. In the dense phase, homotypic and heterotypic PLD interactions are highly cooperative, resulting in the co-mixing of individual PLD phases and forming spatially homogeneous co-condensates. Heterotypic PLD-mediated positive cooperativity in protein-protein interaction networks is likely to play key roles in the co-phase separation of mSWI/SNF complex with transcription factors containing homologous low-complexity domains.

摘要

朊病毒样结构域(PLD)是低复杂性的蛋白质序列,在包括参与转录和RNA加工的蛋白质在内的核酸结合蛋白中富集。FUS和EWSR1的PLD在将染色质重塑因子哺乳动物SWI/SNF复合物募集到致癌性FET融合蛋白凝聚物中起关键作用。在这里,我们表明多个SWI/SNF亚基的无序低复杂性结构域是朊病毒样的,具有很强的细胞内相分离倾向。这些PLD在亚饱和条件下的稀相中与FUS的PLD进行序列特异性异型相互作用,导致PLD共凝聚物的形成。在浓相中,同型和异型PLD相互作用高度协同,导致各个PLD相的共混合并形成空间均匀的共凝聚物。蛋白质-蛋白质相互作用网络中异型PLD介导的正协同作用可能在mSWI/SNF复合物与含有同源低复杂性结构域的转录因子的共相分离中起关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/600b/10680506/b858b20c1c68/nihpp-2023.04.12.536623v2-f0001.jpg

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