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微尺度隔室内表面催化的液-液相分离和类淀粉样组装。

Surface-catalyzed liquid-liquid phase separation and amyloid-like assembly in microscale compartments.

机构信息

Department Biological, Chemical and Pharmaceutical Sciences and Technologies (STEBICEF), University of Palermo, Viale delle Scienze, 16, 90128, Palermo, Italy; Department of Physics and Chemistry - Emilio Segrè, University of Palermo, Viale delle Scienze, 18, 90128, Palermo, Italy.

Department of Physics and Chemistry - Emilio Segrè, University of Palermo, Viale delle Scienze, 18, 90128, Palermo, Italy.

出版信息

J Colloid Interface Sci. 2024 Dec 15;676:569-581. doi: 10.1016/j.jcis.2024.07.135. Epub 2024 Jul 18.

DOI:10.1016/j.jcis.2024.07.135
PMID:39053405
Abstract

Liquid-liquid phase separation is a key phenomenon in the formation of membrane-less structures within the cell, appearing as liquid biomolecular condensates. Protein condensates are the most studied for their biological relevance, and their tendency to evolve, resulting in the formation of aggregates with a high level of order called amyloid. In this study, it is demonstrated that Human Insulin forms micrometric, round amyloid-like structures at room temperature within sub-microliter scale aqueous compartments. These distinctive particles feature a solid core enveloped by a fluid-like corona and form at the interface between the aqueous compartment and the glass coverslip upon which they are cast. Quantitative fluorescence microscopy is used to study in real-time the formation of amyloid-like superstructures. Their formation results driven by liquid-liquid phase separation process that arises from spatially heterogeneous distribution of nuclei at the glass-water interface. The proposed experimental setup allows modifying the surface-to-volume ratio of the aqueous compartments, which affects the aggregation rate and particle size, while also inducing fine alterations in the molecular structures of the final assemblies. These findings enhance the understanding of the factors governing amyloid structure formation, shedding light on the catalytic role of surfaces in this process.

摘要

液-液相分离是细胞内无膜结构形成的关键现象,表现为液态生物分子凝聚物。由于其生物学相关性以及倾向于进化的特性,蛋白质凝聚物是研究最多的,导致形成具有高度有序性的聚集体,称为淀粉样蛋白。在这项研究中,证明人胰岛素在室温下在亚微米级的水相小室中形成微米级的圆形类似淀粉样结构。这些独特的颗粒具有固体核心,被类似流体的外壳包裹,并在水相小室和玻璃盖玻片之间的界面上形成,玻璃盖玻片是它们被浇铸的地方。定量荧光显微镜用于实时研究类似淀粉样的超结构的形成。它们的形成是由液-液相分离过程驱动的,该过程源于核在玻璃-水界面上的空间不均匀分布。所提出的实验装置允许改变水相小室的表面积与体积比,这会影响聚集速率和颗粒大小,同时也会对最终组装体的分子结构产生细微的改变。这些发现增强了对控制淀粉样结构形成的因素的理解,揭示了表面在该过程中的催化作用。

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