Corruption of coronary collateral growth in metabolic syndrome: Role of oxidative stress

doi:10.4330/wjc.v2.i12.421

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Dec 26, 2010 (publication date) through Apr 26, 2024

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World Journal of Cardiology

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1949-8462

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Baishideng Publishing Group Inc, 7041 Koll Center Parkway, Suite 160, Pleasanton, CA 94566, USA

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World J Cardiol. Dec 26, 2010; 2(12): 421-427
Published online Dec 26, 2010. doi: 10.4330/wjc.v2.i12.421

Corruption of coronary collateral growth in metabolic syndrome: Role of oxidative stress

Yuh Fen Pung, William M Chilian

Yuh Fen Pung, William M Chilian, Department of Integrative Medical Sciences, Northeastern Ohio Universities College of Medicine and Pharmacy, Rootstown, OH 44272, United States

Author contributions: Pung YF and Chilian WM contributed to the manuscript equally.

Supported by National Institute of Health Grants No. HL32788, R01 83366, RC1HL100828 (to Chilian WM); and an American Heart Association Post-doctoral Fellowship, No. 09POST2290021 (to Pung YF)

Correspondence to: William M Chilian, PhD, Department of Integrative Medical Sciences, Northeastern Ohio Universities College of Medicine and Pharmacy, Rootstown, OH 44272, United States. wchilian@neoucom.edu

Telephone: +1-330-3255912 Fax: +1-330-3255912

Received: August 2, 2010
Revised: October 23, 2010
Accepted: October 30, 2010
Published online: December 26, 2010

Abstract

The myocardium adapts to ischemic insults in a variety of ways. One adaptation is the phenomenon of acute preconditioning, which can greatly ameliorate ischemic damage. However, this effect wanes within a few hours and does not confer chronic protection. A more chronic adaptation is the so-called second window of preconditioning, which enables protection for a few days. The most potent adaptation invoked by the myocardium to minimize the effects of ischemia is the growth of blood vessels in the heart, angiogenesis and arteriogenesis (collateral growth), which prevent the development of ischemia by enabling flow to a jeopardized region of the heart. This brief review examines the mechanisms underlying angiogenesis and arteriogenesis in the heart. The concept of a redox window, which is an optimal redox state for vascular growth, is discussed along with signaling mechanisms invoked by reactive oxygen species that are stimulated during ischemia-reperfusion. Finally, the review discusses of some of the pathologies, especially the metabolic syndrome, that negatively affect collateral growth through the corruption of redox signaling processes.

Keywords: Angiogenesis, Arteriogenesis, Redox-dependent signaling, Mitochondria