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通过同分子 FRET 进行分子间能量迁移,捕获了相分离生物分子凝聚物的材料性质的调制。

Intermolecular energy migration via homoFRET captures the modulation in the material property of phase-separated biomolecular condensates.

机构信息

Centre for Protein Science, Design and Engineering, Indian Institute of Science Education and Research (IISER) Mohali, Mohali, India.

Department of Biological Sciences, Indian Institute of Science Education and Research (IISER) Mohali, Mohali, India.

出版信息

Nat Commun. 2024 Oct 25;15(1):9215. doi: 10.1038/s41467-024-53494-w.

Abstract

Physical properties of biomolecular condensates formed via phase separation of proteins and nucleic acids are associated with cell physiology and disease. Condensate properties can be regulated by several cellular factors including post-translational modifications. Here, we introduce an application of intermolecular energy migration via homo-FRET (Förster resonance energy transfer), a nanometric proximity ruler, to study the modulation in short- and long-range protein-protein interactions leading to the changes in the physical properties of condensates of fluorescently-tagged FUS (Fused in Sarcoma) that is associated with the formation of cytoplasmic and nuclear membraneless organelles. We show that homoFRET captures modulations in condensate properties of FUS by RNA, ATP, and post-translational arginine methylation. We also extend the homoFRET methodology to study the in-situ formation of cytoplasmic stress granules in mammalian cells. Our studies highlight the broad applicability of homoFRET as a potent generic tool for studying intracellular phase transitions involved in function and disease.

摘要

生物分子凝聚物的物理性质通过蛋白质和核酸的相分离形成,与细胞生理学和疾病有关。凝聚物的性质可以通过几种细胞因子调节,包括翻译后修饰。在这里,我们介绍了通过分子间能量迁移(同分子Förster 共振能量转移,Homo-FRET)进行的应用,这是一种纳米级近程标尺,用于研究导致荧光标记的 FUS(肉瘤融合)凝聚物的物理性质变化的短程和长程蛋白质-蛋白质相互作用的调节,FUS 与细胞质和核无膜细胞器的形成有关。我们表明,Homo-FRET 可通过 RNA、ATP 和翻译后精氨酸甲基化来捕获 FUS 凝聚物性质的调节。我们还将 Homo-FRET 方法扩展到研究哺乳动物细胞中细胞质应激颗粒的原位形成。我们的研究强调了 Homo-FRET 作为一种通用的研究功能和疾病相关细胞内相变的强大工具的广泛适用性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5d96/11511825/6b3bed3c1cd8/41467_2024_53494_Fig1_HTML.jpg

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