2009年8月1日 星期六

Vascular oxidative stress and nitric oxide depletion in HIV-1 transgenic rats are reversed by glutathione restoration [2008](IR90)

Vascular oxidative stress and nitric oxide depletion in HIV-1 transgenic rats are reversed by glutathione restoration [2008](IR90)

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(Memo Item created on August 2, 2009 12:28 PM)

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Vascular oxidative stress and nitric oxide depletion in HIV-1 transgenic rats are reversed by glutathione restoration

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Am J Physiol Heart Circ Physiol 294: H2792-H2804, 2008. First published May 2, 2008; doi:10.1152/ajpheart.91447.2007

0363-6135/08 $8.00

Vascular oxidative stress and nitric oxide depletion in HIV-1 transgenic rats are reversed by glutathione restoration

Erik R. Kline,1 Dean J. Kleinhenz,1 Bill Liang,1,3 Sergey Dikalov,2 David M. Guidot,1 C. Michael Hart,1 Dean P. Jones,1,3 and Roy L. Sutliff1

1Division of Pulmonary, Allergy and Critical Care Medicine, Free Radicals in Medicine Core, 2Division of Cardiology, and 3Center for Clinical and Molecular Nutrition, Emory University School of Medicine/Atlanta Veterans Affairs Medical Center, Atlanta, Georgia

Submitted 12 December 2007 ; accepted in final form 17 April 2008

Human immunodeficiency virus (HIV)-infected patients have a higher incidence of oxidative stress, endothelial dysfunction, and cardiovascular disease than uninfected individuals. Recent reports have demonstrated that viral proteins upregulate reactive oxygen species, which may contribute to elevated cardiovascular risk in HIV-1 patients. In this study we employed an HIV-1 transgenic rat model to investigate the physiological effects of viral protein expression on the vasculature. Markers of oxidative stress in wild-type and HIV-1 transgenic rats were measured using electron spin resonance, fluorescence microscopy, and various molecular techniques. Relaxation studies were completed on isolated aortic rings, and mRNA and protein were collected to measure changes in expression of nitric oxide (NO) and superoxide sources. HIV-1 transgenic rats displayed significantly less NO-hemoglobin, serum nitrite, serum S-nitrosothiols, aortic tissue NO, and impaired endothelium-dependent vasorelaxation than wild-type rats. NO reduction was not attributed to differences in endothelial NO synthase (eNOS) protein expression, eNOS-Ser1177 phosphorylation, or tetrahydrobiopterin availability. Aortas from HIV-1 transgenic rats had higher levels of superoxide and 3-nitrotyrosine but did not differ in expression of superoxide-generating sources NADPH oxidase or xanthine oxidase. However, transgenic aortas displayed decreased superoxide dismutase and glutathione. Administering the glutathione precursor procysteine decreased superoxide, restored aortic NO levels and NO-hemoglobin, and improved endothelium-dependent relaxation in HIV-1 transgenic rats. These results show that HIV-1 protein expression decreases NO and causes endothelial dysfunction. Diminished antioxidant capacity increases vascular superoxide levels, which reduce NO bioavailability and promote peroxynitrite generation. Restoring glutathione levels reverses HIV-1 protein-mediated effects on superoxide, NO, and vasorelaxation.

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acquired immunodeficiency syndrome; antioxidants; superoxide

Address for reprint requests and other correspondence: R. L. Sutliff, Emory Univ./Atlanta VAMC, Rm. 12C-104 (Mailstop 151-P), 1670 Clairmont Rd., Decatur, GA 30033 (e-mail: rsutlif@emory.edu)

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