Cardiovascular roles of nitric oxide: A review of insights from nitric oxide synthase gene disrupted mice

doi:10.1016/j.cardiores.2007.06.024

Cardiovascular Research 2008 77(1):19-29; doi:10.1016/j.cardiores.2007.06.024

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Cardiovascular roles of nitric oxide: A review of insights from nitric oxide synthase gene disrupted mice

Victor W.T. Liu and Paul L. Huang^*

Cardiovascular Research Center, Massachusetts General Hospital and Harvard Medical School, Boston,MA 02114, United States

^* Corresponding author. Cardiovascular Research Center, Massachusetts General Hospital East, 149 Thirteenth Street, Charlestown, MA 02129. Tel: +1 617 724 9849; fax: +1 617 726 5806. E-mail address: phuang1{at}partners.org (P.L. Huang).

Nitric oxide (NO) is a gaseous molecule that plays many keyroles in the cardiovascular system. Each of the enzymes thatgenerate NO—neuronal, inducible and endothelial NO synthase—hasbeen genetically disrupted in mice. This review discusses thecardiovascular phenotypes of each of the NO synthase (NOS) geneknockout mice, and the insights gained into the roles of NOin the cardiovascular system. Mice lacking the endothelial isoformare hypertensive, have endothelial dysfunction and show a moresevere outcome in response to vascular injury, to stroke andcerebral ischaemia, and to diet-induced atherosclerosis. Micelacking the neuronal isoform show a less severe outcome in responseto stroke and cerebral ischaemia but have increased diet-inducedatherosclerosis. Mice lacking the inducible isoform show reducedhypotension to septic shock. Together, NOS gene knockout micehave been useful tools that complement our other approachesto studying the multiple roles of NO in the cardiovascular system.

KEYWORDS Nitric oxide; Gene knockout; Targeted disruption; Animal models; Pathophysiology; Atherosclerosis; Vascular dysfunction; Cerebral ischaemia; Mouse models

Time for primary review: 20 days

This article was published online by Elsevier on 30 June, 2007.

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