Referenced in: Kv7.4

Automatically associated channels: Kv7.2 , Kv7.4 , Kv7.5

Title: Downregulation of Kv7.4 channel activity in primary and secondary hypertension.

Authors: Thomas A Jepps, Preet S Chadha, Alison J Davis, Maksym I Harhun, Gillian W Cockerill, Søren P Olesen, Rie S Hansen, Iain A Greenwood

Journal, date & volume: Circulation, 2011 Aug 2 , 124, 602-11

PubMed link: http://www.ncbi.nlm.nih.gov/pubmed/21747056

Abstract
Voltage-gated potassium (K(+)) channels encoded by KCNQ genes (Kv7 channels) have been identified in various rodent and human blood vessels as key regulators of vascular tone; however, nothing is known about the functional impact of these channels in vascular disease. We ascertained the effect of 3 structurally different activators of Kv7.2 through Kv7.5 channels (BMS-204352, S-1, and retigabine) on blood vessels from normotensive and hypertensive animals.Precontracted thoracic aorta and mesenteric artery segments from normotensive rats were relaxed by all 3 Kv7 activators, with potencies of BMS-204352=S-1>retigabine. We also tested these agents in the coronary circulation using the Langendorff heart preparation. BMS-204352 and S-1 dose dependently increased coronary perfusion at concentrations between 0.1 and 10 μmol/L, whereas retigabine was effective at 1 to 10 μmol/L. In addition, S-1 increased K(+) currents in isolated mesenteric artery myocytes. The ability of these agents to relax precontracted vessels, increase coronary flow, or augment K(+) currents was impaired considerably in tissues isolated from spontaneously hypertensive rats (SHRs). Of the 5 KCNQ genes, only the expression of KCNQ4 was reduced (≈3.7 fold) in SHRs aorta. Kv7.4 protein levels were ≈50% lower in aortas and mesenteric arteries from spontaneously hypertensive rats compared with normotensive vessels. A similar attenuated response to S-1 and decreased Kv7.4 were observed in mesenteric arteries from mice made hypertensive by angiotensin II infusion compared with normotensive controls.In 2 different rat and mouse models of hypertension, the functional impact of Kv7 channels was dramatically downregulated.