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Nat Commun. 2020 Mar 6;11(1):1229. doi: 10.1038/s41467-020-15007-3.
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Mechanosensation of Tight Junctions Depends on ZO-1 Phase Separation and Flow.机械感知紧密连接取决于 ZO-1 的相分离和流动。
Cell. 2019 Oct 31;179(4):937-952.e18. doi: 10.1016/j.cell.2019.10.006.
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Phase Separation of Zonula Occludens Proteins Drives Formation of Tight Junctions.连接蛋白相分离驱动紧密连接的形成。
Cell. 2019 Oct 31;179(4):923-936.e11. doi: 10.1016/j.cell.2019.10.011.
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Phase Separation-Mediated TARP/MAGUK Complex Condensation and AMPA Receptor Synaptic Transmission.相分离介导的 TARP/MAGUK 复合物凝聚和 AMPA 受体突触传递。
Neuron. 2019 Nov 6;104(3):529-543.e6. doi: 10.1016/j.neuron.2019.08.001. Epub 2019 Sep 3.
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Selective effects of ginseng pectins on galectin-3-mediated T cell activation and apoptosis.人参果胶对半乳糖凝集素-3 介导的 T 细胞激活和凋亡的选择性作用。
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ALS-Linked Mutations Affect UBQLN2 Oligomerization and Phase Separation in a Position- and Amino Acid-Dependent Manner.ALS 相关突变以位置和氨基酸依赖性方式影响 UBQLN2 寡聚化和相分离。
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Considerations and Challenges in Studying Liquid-Liquid Phase Separation and Biomolecular Condensates.研究液-液相分离和生物分子凝聚物的考虑因素和挑战。
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RIM and RIM-BP Form Presynaptic Active-Zone-like Condensates via Phase Separation.RIM 和 RIM-BP 通过相分离形成类似于突触前活性区的凝聚物。
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Cancer Mutations of the Tumor Suppressor SPOP Disrupt the Formation of Active, Phase-Separated Compartments.肿瘤抑制因子 SPOP 的癌症突变破坏了活性、相分离隔间的形成。
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半乳糖凝集素-3 N 端尾部脯氨酸调控细胞活性和糖基介导的寡聚化/相分离。

Galectin-3 N-terminal tail prolines modulate cell activity and glycan-mediated oligomerization/phase separation.

机构信息

Engineering Research Center of Glycoconjugates Ministry of Education, Jilin Provincial Key Laboratory of Chemistry and Biology of Changbai Mountain Natural Drugs, School of Life Sciences, Northeast Normal University, 130024 Changchun, China.

Department of Biochemistry, Molecular Biology and Biophysics, University of Minnesota, Minneapolis, MN 55455.

出版信息

Proc Natl Acad Sci U S A. 2021 May 11;118(19). doi: 10.1073/pnas.2021074118.

DOI:10.1073/pnas.2021074118
PMID:33952698
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8126832/
Abstract

Galectin-3 (Gal-3) has a long, aperiodic, and dynamic proline-rich N-terminal tail (NT). The functional role of the NT with its numerous prolines has remained enigmatic since its discovery. To provide some resolution to this puzzle, we individually mutated all 14 NT prolines over the first 68 residues and assessed their effects on various Gal-3-mediated functions. Our findings show that mutation of any single proline (especially P37A, P55A, P60A, P64A/H, and P67A) dramatically and differentially inhibits Gal-3-mediated cellular activities (i.e., cell migration, activation, endocytosis, and hemagglutination). For mechanistic insight, we investigated the role of prolines in mediating Gal-3 oligomerization, a fundamental process required for these cell activities. We showed that Gal-3 oligomerization triggered by binding to glycoproteins is a dynamic process analogous to liquid-liquid phase separation (LLPS). The composition of these heterooligomers is dependent on the concentration of Gal-3 as well as on the concentration and type of glycoprotein. LLPS-like Gal-3 oligomerization/condensation was also observed on the plasma membrane and disrupted endomembranes. Molecular- and cell-based assays indicate that glycan binding-triggered Gal-3 LLPS (or LLPS-like) is driven mainly by dynamic intermolecular interactions between the Gal-3 NT and the carbohydrate recognition domain (CRD) F-face, although NT-NT interactions appear to contribute to a lesser extent. Mutation of each proline within the NT differentially controls NT-CRD interactions, consequently affecting glycan binding, LLPS, and cellular activities. Our results unveil the role of proline polymorphisms (e.g., at P64) associated with many diseases and suggest that the function of glycosylated cell surface receptors is dynamically regulated by Gal-3.

摘要

半乳糖凝集素-3(Gal-3)具有长的、非周期性的和富含脯氨酸的 N 端尾部(NT)。自发现以来,其富含脯氨酸的 NT 的功能作用一直是个谜。为了解决这个难题,我们分别突变了前 68 个残基中所有 14 个 NT 脯氨酸,并评估了它们对各种 Gal-3 介导的功能的影响。我们的研究结果表明,突变任何单个脯氨酸(特别是 P37A、P55A、P60A、P64A/H 和 P67A)都会显著且不同地抑制 Gal-3 介导的细胞活性(即细胞迁移、激活、内吞作用和血凝作用)。为了深入了解机制,我们研究了脯氨酸在介导 Gal-3 寡聚化中的作用,这是这些细胞活动所必需的基本过程。我们表明,Gal-3 通过与糖蛋白结合而引发的寡聚化是一个类似于液-液相分离(LLPS)的动态过程。这些异源寡聚体的组成取决于 Gal-3 的浓度以及糖蛋白的浓度和类型。LLPS 样 Gal-3 寡聚体/凝聚也在质膜和内体膜上观察到。基于分子和细胞的测定表明,糖结合触发的 Gal-3 LLPS(或 LLPS 样)主要由 Gal-3 NT 与碳水化合物识别域(CRD)F 面之间的动态分子间相互作用驱动,尽管 NT-NT 相互作用似乎贡献较小。NT 内的每个脯氨酸的突变会以不同的方式控制 NT-CRD 相互作用,从而影响糖结合、LLPS 和细胞活性。我们的结果揭示了与许多疾病相关的脯氨酸多态性(例如 P64)的作用,并表明糖基化细胞表面受体的功能受 Gal-3 的动态调节。