Rapid Endosomal Recycling

Hana Mahmutefendic, Gordana Blagojević Zagorac, S. Macesic, P. Lučin
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引用次数: 3

Abstract

Peripheral membrane proteins are endocytosed by constitutive processes of membrane invaginations, followed by internalization driven by diverse endocytic machinery available at the cell surface. It is believed that after endocytic uptake, cargo proteins proceed either through the endosomal recycling circuit of the cell or travel toward late endosomes for degradation. In this chapter, we analyzed trafficking of seven cargo molecules (transferrin receptor, fully conformed MHC-I, non-conformed MHC-I, cholera-toxin B subunit, CD44, ICAM1, and G-protein-coupled receptor Rae-1) known to use the distinct endocytic route. For that purpose, we developed the software for multicompartment analysis of intracellular trafficking. We demonstrate that all endocytosed molecules are rapidly recycled and propose that the rapid recycling is a constitutive process that should be considered in the analysis of intracellular trafficking of peripheral membrane proteins.
内体快速循环
外周膜蛋白通过膜内陷的组成过程被内吞,随后由细胞表面多种内吞机制驱动的内化。据信,在内吞摄取后,货物蛋白要么通过细胞的内体再循环回路进行,要么前往内体的晚期进行降解。在本章中,我们分析了七种已知的货物分子(转铁蛋白受体、完全符合MHC-I、不符合MHC-I、霍乱毒素B亚基、CD44、ICAM1和g蛋白偶联受体Rae-1)的运输,它们使用不同的内噬途径。为此,我们开发了用于细胞内运输的多室分析的软件。我们证明了所有的内吞分子都是快速循环的,并提出快速循环是一个组成过程,在分析外周膜蛋白的细胞内运输时应该考虑到这一点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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