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二元肽凝聚物作为生物分子凝聚物的活性模型。

Binary peptide coacervates as an active model for biomolecular condensates.

作者信息

Cao Shoupeng, Zhou Peng, Shen Guizhi, Ivanov Tsvetomir, Yan Xuehai, Landfester Katharina, Caire da Silva Lucas

机构信息

College of Polymer Science and Engineering, State Key Laboratory of Polymer Materials Engineering, Sichuan University, Chengdu, 610065, PR China.

Max Planck Institute for Polymer Research, 55128, Mainz, Germany.

出版信息

Nat Commun. 2025 Mar 11;16(1):2407. doi: 10.1038/s41467-025-57772-z.

Abstract

Biomolecular condensates formed by proteins and nucleic acids are critical for cellular processes. Macromolecule-based coacervate droplets formed by liquid-liquid phase separation serve as synthetic analogues, but are limited by complex compositions and high molecular weights. Recently, short peptides have emerged as an alternative component of coacervates, but tend to form metastable microdroplets that evolve into rigid nanostructures. Here we present programmable coacervates using binary mixtures of diphenylalanine-based short peptides. We show that the presence of different short peptides stabilizes the coacervate phase and prevents the formation of rigid structures, allowing peptide coacervates to be used as stable adaptive compartments. This approach allows fine control of droplet formation and dynamic morphological changes in response to physiological triggers. As compartments, short peptide coacervates sequester hydrophobic molecules and enhance bio-orthogonal catalysis. In addition, the incorporation of coacervates into model synthetic cells enables the design of Boolean logic gates. Our findings highlight the potential of short peptide coacervates for creating adaptive biomimetic systems and provide insight into the principles of phase separation in biomolecular condensates.

摘要

由蛋白质和核酸形成的生物分子凝聚物对细胞过程至关重要。通过液-液相分离形成的基于大分子的凝聚层液滴可作为合成类似物,但受到复杂组成和高分子量的限制。最近,短肽已成为凝聚层的一种替代成分,但往往会形成亚稳态微滴,进而演变成刚性纳米结构。在此,我们展示了使用基于二苯基丙氨酸的短肽二元混合物形成的可编程凝聚层。我们表明,不同短肽的存在稳定了凝聚层相并防止了刚性结构的形成,使肽凝聚层能够用作稳定的适应性隔室。这种方法能够精确控制液滴形成以及响应生理触发因素的动态形态变化。作为隔室,短肽凝聚层能够隔离疏水分子并增强生物正交催化作用。此外,将凝聚层整合到模型合成细胞中能够设计布尔逻辑门。我们的研究结果突出了短肽凝聚层在创建适应性仿生系统方面的潜力,并为生物分子凝聚物中的相分离原理提供了见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e16e/11897134/741210bbddaa/41467_2025_57772_Fig1_HTML.jpg

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