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1Cardiovascular Research Group, School of Medicine, University of Manchester, Manchester, United Kingdom; 2Kagawa Prefectural College of Health Sciences, Mure, Kagawa, Japan; 3Faculty of Biological Sciences, University of Leeds, Leeds, United Kingdom; and 4Department of Physiology, University of British Columbia, Vancouver, British Columbia, Canada
Submitted 7 December 2005 ; accepted in final form 27 September 2006
In the heart, ACh activates the ACh-activated K+ current (IK,ACh) via the M2 muscarinic receptor. The relationship between desensitization of IK,ACh and internalization of the M2 receptor has been studied in rat atrial cells. On application of the stable muscarinic agonist carbachol for 2 h, IK,ACh declined by 
62% with time constants of 1.5 and 26.9 min, whereas 83% of the M2 receptor was internalized from the cell membrane with time constants of 2.9 and 51.6 min. Transfection of the cells with 
-adrenergic receptor kinase 1 (G protein-receptor kinase 2) and -arrestin 2 significantly increased IK,ACh desensitization and M2 receptor internalization during a 3-min application of agonist. Internalized M2 receptor in cells exposed to carbachol for 2 h was colocalized with clathrin and not caveolin. It is concluded that a G protein-receptor kinase 2- and -arrestin 2-dependent internalization of the M2 receptor into clathrin-coated vesicles could play a major role in IK,ACh desensitization.
acethylcholine-activated potassium current; acetylcholine; Kir3.1; Kir3.4; caveolin
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