Cloning and function of the rat colonic epithelial K+ channel K(V)LQT1
Contribuinte(s) |
WR Loewenstein |
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Data(s) |
01/01/2001
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Resumo |
K(V)LQT1 (K(V)LQ1) is a voltage-gated K+ channel essential for repolarization of the heart action potential that is defective in cardiac arrhythmia. The channel is inhibited by the chromanol 293B, a compound that blocks cAMP-dependent electrolyte secretion in rat and human colon, therefore suggesting expression of a similar type of K+ channel in the colonic epithelium. We now report cloning and expression of K(V)LQT1 from rat colon. Overlapping clones identified by cDNA-library screening were combined to a full length cDNA that shares high sequence homology to K(V)LQT1 cloned from other species. RT-PCR analysis of rat colonic musoca demonstrated expression of K(V)LQT1 in crypt cells and surface epithelium. Expression of rK(V)LQT1 in Xenopus oocytes induced a typical delayed activated K+ current. that was further activated by increase of intracellular cAMP but not Ca2+ and that was blocked by the chromanol 293B. The same compound blocked a basolateral cAMP-activated K+ conductance in the colonic mucosal epithelium and inhibited whole cell K+ currents in patch-clamp experiments on isolated colonic crypts. We conclude that K(V)QT1 is forming an important component of the basolateral cAMP-activated K+ conductance in the colonic epithelium and plays a crucial role in diseases like secretory diarrhea and cystic fibrosis. |
Identificador | |
Idioma(s) |
eng |
Publicador |
Springer Verlag |
Palavras-Chave | #Biochemistry & Molecular Biology #Cell Biology #Physiology #Rk(v)lqt1 #Rkcnq1 #Rat Colon #K+ Channel #Epithelium #Electrolyte Secretion #Ion Transport #Xenopus Oocytes #Expression #Cloning #Ussing Chamber #Dogfish Squalus-acanthias #Rectal Gland Tubules #Potassium Channel #Ion-transport #Cyclic-amp #Idiopathic Epilepsy #Cystic-fibrosis #Nacl Secretion #Cl Secretion #Conductance #C1 #270104 Membrane Biology #730110 Respiratory system and diseases (incl. asthma) |
Tipo |
Journal Article |