Contribution of 20-HETE to Augmented Myogenic Constriction in Coronary Arteries of Endothelial NO Synthase Knockout Mice

doi:10.1161/01.HYP.0000176745.04393.4d

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Hypertension. 2005;46:607-613
Published online before print July 25, 2005, doi: 10.1161/01.HYP.0000176745.04393.4d

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	Coronary circulation
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(Hypertension. 2005;46:607.)
© 2005 American Heart Association, Inc.

Original Articles

Contribution of 20-HETE to Augmented Myogenic Constriction in Coronary Arteries of Endothelial NO Synthase Knockout Mice

An Huang; Dong Sun; Changdong Yan; John R. Falck; Gabor Kaley

From the Department of Physiology (A.H., D.S., C.Y., G.K.), New York Medical College, Valhalla; and Department of Biochemistry (J.R.F.), University of Texas, Southwestern Medical Center, Dallas.

Correspondence to An Huang, MD, PhD, Department of Physiology, New York Medical College, Valhalla, NY 10595. E-mail an_huang{at}nymc.edu

Previous studies suggested an important role for 20-HETE inthe regulation of myogenic responses. Thus, pressure–diameterrelationships were investigated in isolated, cannulated coronaryarteries ( ${approx}$ 100µm) from male endothelial NO synthase knockout(eNOS-KO) and wild-type (WT) mice. All arteries constrictedin response to step increases in perfusate pressure from 20to 100 mm Hg. This constriction was significantly enhanced from40 to 100 mm Hg in arteries of eNOS-KO compared with those ofWT mice. For example, at 60 and 100 mm Hg, respectively, thenormalized diameter (expressed as a percentage of the correspondingpassive diameter) of arteries of eNOS-KO mice was 10% and 12%smaller than that of WT mice. Removal of the endothelium didnot significantly affect the responses of vessels from eitherstrain of mice. However, N-methylsulfonyl-12,12-dibromododec-11-enamide(5x10^–6 M), an inhibitor of cytochrome P-450 (CYP)/ ${omega}$ -hydroxylase,significantly attenuated the greater myogenic constriction ofarteries from eNOS-KO mice by ${approx}$ 12% at each pressure step butdid not significantly affect responses of those from WT mice,leading to a comparable myogenic response in the 2 strains.Western blot analysis demonstrated a comparable CYP4A proteincontent in coronary arteries of the 2 strains of mice. However,production of 20-HETE, measured by fluorescent high-performanceliquid chromatography assay was ${approx}$ 2.7-fold greater in eNOS-KOcompared to WT mice. Thus, as a function of eNOS deficiency,the enhanced coronary artery constriction to pressure is attributableto an increased activity of ${omega}$ -hydroxylase, which, consequently,increases the synthesis of 20-HETE in vascular smooth muscle.

Key Words: constriction • nitric oxide • coronary artery disease