Pathways That Control Cortical F-Actin Dynamics During Secretion

被引:0
|
作者
J.-M. Trifaró
T. Lejen
S. D. Rosé
T. Dumitrescu Pene
N. D. Barkar
E. P. Seward
机构
[1] University of Ottawa,Secretory Process Research Program, Department of Cellular and Molecular Medicine, Faculty of Medicine
来源
Neurochemical Research | 2002年 / 27卷
关键词
Chromaffin cell; cortical f-actin; secretion scinderin; MARCKS; PKC;
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学科分类号
摘要
Chromaffin cells possess a mesh of filamentous actin underneath the plasma membrane which acts as a barrier to the chromaffin vesicles access to exocytotic sites. Disassembly of cortical F-actin in response to stimulation allows the movement of vesicles from the reserve pool to the release-ready vesicle pool and, therefore, to exocytotic sites. The dynamics of cortical F-actin is controlled by two mechanisms: a) stimulation-induced Ca2+ entry and scinderin activation and b) protein kinase C (PKC) activation and MARCKS phosphorylation as demonstrated here by experiments with recombinant proteins, antisense olygodeoxynucleotides and vector mediated transient expressions. Under physiological conditions (i.e., cholinergic receptor stimulation followed by Ca2+ entry), mechanism (a) is the most important for the control of cortical F-actin network whereas when Ca2+ is released from intracellular stores (i.e., histamine stimulation) cortical F-actin is regulated mainly by mechanism b.
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页码:1371 / 1385
页数:14
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