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单组分生物分子凝聚物中的聚集

Clustering within a single-component biomolecular condensate.

作者信息

Sharma Ankith, Sau Abhishek, Dave Sandeep, Roychowdhury Sumangal, Schnorrenberg Sebastian, Chowdhury Rajdeep, Hutten Saskia, Dormann Dorothee, Musser Siegfried M

机构信息

Department of Cell Biology and Genetics, Texas A&M University; College Station, TX, USA.

Equal Contributions.

出版信息

bioRxiv. 2025 Aug 22:2025.08.18.670948. doi: 10.1101/2025.08.18.670948.

DOI:10.1101/2025.08.18.670948
PMID:40894708
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12393318/
Abstract

Biomolecular condensates (BMCs) are assemblies of hundreds to many thousands of macromolecules within cells that are organized without physical barriers. Condensate function is dictated not only by its molecular composition, but also by substructural organization and molecular mobility. One hypothesis for the onset of multiple protein aggregation diseases is that the increased densities of specific proteins within BMCs promotes the formation of solid inclusions. However, deciphering the internal structural and functional properties of BMCs at the nanoscale and identifying the initiating events of inclusion formation requires tools with high spatiotemporal precision. Here we show using single molecule and other microscopy approaches that single component Fused in Sarcoma (FUS) condensates exhibit confinement and contain clusters with higher FUS density even at early timepoints. Upon aging, condensates displayed altered physical properties and reduced monomer mobility, and yet most FUS monomers diffused throughout the condensate within seconds. While an increase in connectivity over time explains reduced mobility, the large fraction of molecules retaining high mobility suggests a sponge-like structure rather than a system-spanning network. These findings indicate that a pseudo-equilibrium between distinct structural connectivities can exist within simple condensates, suggesting the potential for substantial structural and functional complexity of BMCs at the nanoscale.

摘要

生物分子凝聚物(BMCs)是细胞内由数百到数千个大分子组成的集合体,其组织方式没有物理屏障。凝聚物的功能不仅取决于其分子组成,还取决于亚结构组织和分子流动性。关于多种蛋白质聚集疾病发病的一种假说认为,BMCs内特定蛋白质密度的增加会促进固体包涵体的形成。然而,要在纳米尺度上解析BMCs的内部结构和功能特性,并确定包涵体形成的起始事件,需要具有高时空精度的工具。在这里,我们使用单分子和其他显微镜方法表明,单组分肉瘤融合蛋白(FUS)凝聚物表现出受限性,并且即使在早期时间点也包含FUS密度更高的簇。随着时间的推移,凝聚物的物理性质发生改变,单体流动性降低,然而大多数FUS单体在几秒钟内就会在整个凝聚物中扩散。虽然随着时间的推移连接性增加可以解释流动性降低,但大部分分子保持高流动性表明其结构类似海绵而非跨越整个系统的网络。这些发现表明,在简单的凝聚物中可能存在不同结构连接性之间的准平衡,这表明BMCs在纳米尺度上可能具有相当大的结构和功能复杂性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/75e5/12393318/8cde271c4ab3/nihpp-2025.08.18.670948v1-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/75e5/12393318/8cde271c4ab3/nihpp-2025.08.18.670948v1-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/75e5/12393318/8cde271c4ab3/nihpp-2025.08.18.670948v1-f0001.jpg

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本文引用的文献

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Overlapping nuclear import and export paths unveiled by two-colour MINFLUX.双色MINFLUX揭示的重叠核输入和输出路径
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