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Shedding light on the dynamics of endocytosis and viral budding

机译:揭示内吞作用和病毒出芽的动力学

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Endocytosis is used by eukaryotic cells to perform a wide range of functions, including the uptake of extracellular nutrients and the regulation of cell-surface receptors, as well as by toxins, viruses, and microorganisms to gain entry into cells (1). Endocytosis actually encompasses many different processes, such as phagocytosis of large (>250 nm) particles as well as pinocytosis of large volumes of fluid (2). One of the most important endocytic mechanisms is a receptor-mediated process whereby the plasma membrane binds specific macromolecules and smaller particles by means of specialized receptors, invaginates around those particles, and then pinches off to form small vesicles. Receptor-mediated endocytosis had been thought to be assisted by specific proteins, either clathrin or caveolin, polymerizing into a spherical shell around the invagination (3). Recently, however, evidence has arisen for a different, clathrin- and caveolin-independent route by which endocytosis may occur (4, 5): The understanding and quantitative analysis of the mechanisms underlying receptor-mediated endocytosis have important implications for not only viral pathogenesis but also the delivery of macromolecules and nanoparticles for intracellular imaging and targeted therapies (6).
机译:真核细胞利用胞吞作用执行多种功能,包括摄取细胞外营养和调节细胞表面受体,以及毒素,病毒和微生物进入细胞(1)。胞吞作用实际上包含许多不同的过程,例如大颗粒(> 250 nm)的吞噬作用以及大量液体的胞吞作用(2)。最重要的内吞机制之一是受体介导的过程,其中质膜通过专门的受体结合特定的大分子和较小的颗粒,在这些颗粒周围侵入,然后收缩形成小囊泡。受体介导的内吞作用被认为是由特定蛋白(网格蛋白或小窝蛋白)协助而形成的,这些蛋白在内陷周围聚合成球形外壳(3)。然而,最近,已经出现了一种证据,表明存在一种与网格蛋白和小窝蛋白无关的不同途径,可能通过这种途径发生内吞作用(4,5):受体介导的内吞作用机理的理解和定量分析不仅对病毒的发病机理有重要意义。而且还提供用于细胞内成像和靶向治疗的大分子和纳米颗粒(6)。

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