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将大颗粒可控且正交地分隔到生物分子凝聚物中。

Controlled and orthogonal partitioning of large particles into biomolecular condensates.

作者信息

Kelley Fleurie M, Ani Anas, Pinlac Emily G, Linders Bridget, Favetta Bruna, Barai Mayur, Ma Yuchen, Singh Arjun, Dignon Gregory L, Gu Yuwei, Schuster Benjamin S

机构信息

Department of Chemical and Biochemical Engineering, Rutgers, The State University of New Jersey, Piscataway, NJ, USA.

Department of Chemistry and Chemical Biology, Rutgers, The State University of New Jersey, Piscataway, NJ, USA.

出版信息

Nat Commun. 2025 Apr 14;16(1):3521. doi: 10.1038/s41467-025-58900-5.

Abstract

Partitioning of client molecules into biomolecular condensates is critical for regulating the composition and function of condensates. Previous studies suggest that client size limits partitioning. Here, we ask whether large clients, such as macromolecular complexes and nanoparticles, can partition into condensates based on particle-condensate interactions. We seek to discover the fundamental biophysical principles that govern particle inclusion in or exclusion from condensates, using polymer nanoparticles surface-functionalized with biotin or oligonucleotides. Based on our experiments, coarse-grained molecular dynamics simulations, and theory, we conclude that arbitrarily large particles can controllably partition into condensates given sufficiently strong condensate-particle interactions. Remarkably, we also observe that beads with distinct surface chemistries partition orthogonally into immiscible condensates. These findings may provide insights into how various cellular processes are achieved based on partitioning of large clients into biomolecular condensates, and they offer design principles for drug delivery systems that selectively target disease-related condensates.

摘要

客体分子分配到生物分子凝聚物中对于调节凝聚物的组成和功能至关重要。先前的研究表明客体大小限制了分配。在此,我们探讨诸如大分子复合物和纳米颗粒等大型客体是否能基于颗粒 - 凝聚物相互作用分配到凝聚物中。我们试图发现决定颗粒被凝聚物包含或排斥的基本生物物理原理,使用用生物素或寡核苷酸进行表面功能化的聚合物纳米颗粒。基于我们的实验、粗粒度分子动力学模拟和理论,我们得出结论,在凝聚物 - 颗粒相互作用足够强的情况下,任意大小的颗粒都能可控地分配到凝聚物中。值得注意的是,我们还观察到具有不同表面化学性质的珠子正交分配到互不相溶的凝聚物中。这些发现可能为基于大型客体分配到生物分子凝聚物中如何实现各种细胞过程提供见解,并且它们为选择性靶向疾病相关凝聚物的药物递送系统提供了设计原则。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f2fe/11997106/05a2c0282f30/41467_2025_58900_Fig1_HTML.jpg

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