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βIII spectrin 调节高尔基体复合物的结构完整性和分泌蛋白运输。

βIII spectrin regulates the structural integrity and the secretory protein transport of the Golgi complex.

机构信息

Department de Biologia Cel·lular, Immunologia i Neurociències, Facultat de Medicina, Universitat de Barcelona, 08036 Barcelona, Spain.

出版信息

J Biol Chem. 2013 Jan 25;288(4):2157-66. doi: 10.1074/jbc.M112.406462. Epub 2012 Dec 11.

Abstract

A spectrin-based cytoskeleton is associated with endomembranes, including the Golgi complex and cytoplasmic vesicles, but its role remains poorly understood. Using new generated antibodies to specific peptide sequences of the human βIII spectrin, we here show its distribution in the Golgi complex, where it is enriched in the trans-Golgi and trans-Golgi network. The use of a drug-inducible enzymatic assay that depletes the Golgi-associated pool of PI4P as well as the expression of PH domains of Golgi proteins that specifically recognize this phosphoinositide both displaced βIII spectrin from the Golgi. However, the interference with actin dynamics using actin toxins did not affect the localization of βIII spectrin to Golgi membranes. Depletion of βIII spectrin using siRNA technology and the microinjection of anti-βIII spectrin antibodies into the cytoplasm lead to the fragmentation of the Golgi. At ultrastructural level, Golgi fragments showed swollen distal Golgi cisternae and vesicular structures. Using a variety of protein transport assays, we show that the endoplasmic reticulum-to-Golgi and post-Golgi protein transports were impaired in βIII spectrin-depleted cells. However, the internalization of the Shiga toxin subunit B to the endoplasmic reticulum was unaffected. We state that βIII spectrin constitutes a major skeletal component of distal Golgi compartments, where it is necessary to maintain its structural integrity and secretory activity, and unlike actin, PI4P appears to be highly relevant for the association of βIII spectrin the Golgi complex.

摘要

一种基于血影蛋白的细胞骨架与内质网相关,包括高尔基体复合体和细胞质小泡,但它的作用仍不清楚。使用针对人βIII 血影蛋白的特定肽序列的新生成抗体,我们在此显示了它在高尔基体复合体中的分布,在那里它在顺面高尔基体和高尔基体网络中丰富。使用一种诱导药物的酶测定法来消耗与高尔基体相关的 PI4P 池,以及表达专门识别这种磷酸肌醇的高尔基体蛋白的 PH 结构域,这两种方法都将βIII 血影蛋白从高尔基体中置换出来。然而,使用肌动蛋白毒素干扰肌动蛋白动力学不会影响βIII 血影蛋白在高尔基体膜上的定位。使用 siRNA 技术耗尽βIII 血影蛋白和将抗βIII 血影蛋白抗体微注射到细胞质中会导致高尔基体碎裂。在超微结构水平上,高尔基体片段显示出扩张的远端高尔基体潴泡和小泡结构。使用各种蛋白质运输测定法,我们表明内质网到高尔基体和高尔基体后蛋白质运输在βIII 血影蛋白耗尽的细胞中受损。然而,Shiga 毒素亚基 B 到内质网的内化不受影响。我们声明βIII 血影蛋白构成远端高尔基体隔室的主要骨架成分,在那里它需要保持其结构完整性和分泌活性,并且与肌动蛋白不同,PI4P 似乎与βIII 血影蛋白与高尔基体复合体的关联高度相关。

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