Diabetic HDL-associated myristic acid inhibits acetylcholine-induced nitric oxide generation by preventing the association of endothelial nitric oxide synthase with calmodulin

doi:10.1152/ajpcell.00042.2007

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Am J Physiol Cell Physiol 294: C295-C305, 2008. First published October 31, 2007; doi:10.1152/ajpcell.00042.2007
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VASCULAR BIOLOGY

Diabetic HDL-associated myristic acid inhibits acetylcholine-induced nitric oxide generation by preventing the association of endothelial nitric oxide synthase with calmodulin

James White,¹ Theresa Guerin,¹ Hollie Swanson,² Steven Post,² Haining Zhu,³ Ming Gong,⁴ Jun Liu,¹ William V. Everson,¹ Xiang-An Li,¹ Gregory A. Graf,⁵ Hubert O. Ballard,¹ Stuart A. Ross,¹ and Eric J. Smart¹^,4

Departments of ¹Pediatrics and Kentucky Pediatric Research Institute, ²Pharmacology, ³Molecular and Cellular Biochemistry, ⁴Physiology, and ⁵Pharmaceutical Sciences, University of Kentucky, Lexington, Kentucky

Submitted 30 January 2007 ; accepted in final form 12 October 2007

In the current study, we examined whether diabetes affectedthe ability of HDL to stimulate nitric oxide (NO) production.Using HDL isolated from both diabetic humans and diabetic mousemodels, we found that female HDL no longer induced NO synthesis,despite containing equivalent amounts of estrogen as nondiabeticcontrols. Furthermore, HDL isolated from diabetic females andmales prevented acetylcholine-induced stimulation of NO generation.Analyses of both the human and mouse diabetic HDL particlesshowed that the HDLs contained increased levels of myristicacid. To determine whether myristic acid associated with HDLparticles was responsible for the decrease in NO generation,myristic acid was added to HDL isolated from nondiabetic humansand mice. Myristic acid-associated HDL inhibited the generationof NO in a dose-dependent manner. Importantly, diabetic HDLdid not alter the levels of endothelial NO synthase or acetylcholinereceptors associated with the cells. Surprisingly, diabeticHDL inhibited ionomycin-induced stimulation of NO productionwithout affecting ionomycin-induced increases in intracellularcalcium. Further analysis indicated that diabetic HDL preventedcalmodulin from interacting with endothelial NO synthase (eNOS)but did not affect the activation of calmodulin kinase or calcium-independentmechanisms for stimulating eNOS. These studies are the firstto show that a specific fatty acid associated with HDL inhibitsthe stimulation of NO generation. These findings have importantimplications regarding cardiovascular disease in diabetic patients.

fatty acid; lipoprotein; diabetes; signaling

Address for reprint requests and other correspondence: E. J. Smart, Kentucky Pediatric Research Institute, Univ. of Kentucky, 423 Sanders-Brown, 800 South Limestone St., Lexington, KY 40536-0230 (e-mail: ejsmart{at}email.uky.edu)