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布雷菲德菌素A通过阻断MDCK细胞共同内体中的极性分选,迅速破坏质膜极性。

Brefeldin A rapidly disrupts plasma membrane polarity by blocking polar sorting in common endosomes of MDCK cells.

作者信息

Wang E, Pennington J G, Goldenring J R, Hunziker W, Dunn K W

机构信息

Department of Medicine, Division of Nephrology, Indiana University Medical Center, Indianapolis, IN 46202, USA.

出版信息

J Cell Sci. 2001 Sep;114(Pt 18):3309-21. doi: 10.1242/jcs.114.18.3309.

Abstract

Recent studies showing thorough intermixing of apical and basolateral endosomes have demonstrated that endocytic sorting is critical to maintaining the plasma membrane polarity of epithelial cells. Our studies of living, polarized cells show that disrupting endocytosis with brefeldin-A rapidly destroys the polarity of transferrin receptors in MDCK cells while having no effect on tight junctions. Brefeldin-A treatment induces tubulation of endosomes, but the sequential compartments and transport steps of the transcytotic pathway remain intact. Transferrin is sorted from LDL, but is then missorted from common endosomes to the apical recycling endosome, as identified by its nearly neutral pH, and association with GFP chimeras of Rabs 11a and 25. From the apical recycling endosome, transferrin is then directed to the apical plasma membrane. These data are consistent with a model in which polarized sorting of basolateral membrane proteins occurs via a brefeldin-A-sensitive process of segregation into basolateral recycling vesicles. Although disruption of polar sorting correlates with dissociation of gamma-adaptin from endosomes, gamma-adaptin does not appear to be specifically involved in sorting into recycling vesicles, as we find it associated with the transcytotic pathway, and particularly to the post-sorting transcytotic apical recycling endosome.

摘要

近期研究表明,顶端和基底外侧内体存在彻底的混合,这证明内吞分选对于维持上皮细胞的质膜极性至关重要。我们对活的极化细胞的研究表明,用布雷菲德菌素A破坏内吞作用会迅速破坏MDCK细胞中转铁蛋白受体的极性,而对紧密连接没有影响。布雷菲德菌素A处理会诱导内体形成管状结构,但转胞吞途径的连续区室和运输步骤仍保持完整。转铁蛋白与低密度脂蛋白分离,但随后会从共同内体错误分选至顶端回收内体,这可通过其接近中性的pH值以及与Rabs 11a和25的绿色荧光蛋白嵌合体的结合来确定。然后,转铁蛋白从顶端回收内体被导向顶端质膜。这些数据与一个模型一致,即基底外侧膜蛋白的极化分选通过一个对布雷菲德菌素A敏感的过程发生,该过程将其分离到基底外侧回收小泡中。尽管极性分选的破坏与γ-衔接蛋白从内体的解离相关,但γ-衔接蛋白似乎并未特别参与分选进入回收小泡,因为我们发现它与转胞吞途径相关,尤其是与分选后转胞吞的顶端回收内体相关。

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