New paradigms of CFTR chloride channel regulation

被引:0
|
作者
K. L. Kirk
机构
[1] Gregory Fleming James Cystic Fibrosis Research Center,
[2] UAB Dept of Physiology and Biophysics,undefined
[3] MCLM 738,undefined
[4] 1918 University Blvd.,undefined
[5] 1530 3rd Ave S.,undefined
[6] Birmingham (Alabama 35294-0005,undefined
[7] USA),undefined
[8] Fax +1 205 934 1445,undefined
[9] e-mail: Kirk@physiology.uab.edu ,undefined
关键词
Key words. Cystic fibrosis; ion channels; membrane traffic; syntaxins; PDZ domains; epithelial cells; ABC transporters; cystic fibrosis transmembrane; conductance regulator.;
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摘要
The Cystic fibrosis transmembrane conductance regulator (CFTR) chloride channel controls salt and water transport across epithelial tissues. Alterations in the activity of this ion channel lead to two major human diseases: cystic fibrosis (low CFTR activity) and secretory diarrhea (excessive CFTR activity). The goal of this article is to review recent developments in our understanding of two aspects of CFTR biology: (i) interactions between CFTR domains (intramolecular interactions) that control the gating of this epithelial chloride channel and (ii) interactions between CFTR and other proteins (intermolecular interactions) that couple the activity of this ion channel to additional cellular processes in epithelial cells (e.g. membrane traffic). Clarifying the nature of these interactions may lead to the development of novel strategies for treating diseases that involve the CFTR chloride channel.
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页码:623 / 634
页数:11
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