Mice expressing ACE only in the heart show that increased cardiac angiotensin II is not associated with cardiac hypertrophy

doi:10.1152/ajpheart.01147.2007

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Am J Physiol Heart Circ Physiol 294: H659-H667, 2008. First published November 21, 2007; doi:10.1152/ajpheart.01147.2007
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Mice expressing ACE only in the heart show that increased cardiac angiotensin II is not associated with cardiac hypertrophy

Hong D. Xiao,¹ Sebastien Fuchs,¹ Ellen A. Bernstein,¹ Ping Li,¹ Duncan J. Campbell,² and Kenneth E. Bernstein¹

¹Department of Pathology and Laboratory Medicine, Emory University, Atlanta, Georgia; and ²Saint Vincent's Institute of Medical Research and the Department of Medicine, University of Melbourne, Saint Vincent's Hospital, Fitzroy, Victoria, Australia

Submitted 3 October 2007 ; accepted in final form 14 November 2007

In the heart, angiotensin II has been suggested to regulatecardiac remodeling and promote cardiac hypertrophy. To examinethis, we studied compound heterozygous mice, called angiotensin-convertingenzyme (ACE) 1/8, in which one ACE allele is null, whereas theother ACE allele (the 8 allele) targets expression to the heart.In this model, cardiac ACE levels are about 15 times those ofwild-type mice, and ACE expression is reduced or eliminatedin other tissues. ACE 1/8 mice have 58% the cardiac ACE of aprevious model, called ACE 8/8, but both ACE 1/8 and ACE 8/8mice have ventricular angiotensin II levels about twofold thoseof wild-type controls. Despite equivalent levels of cardiacangiotensin II, ACE 1/8 mice do not develop the marked atrialenlargement or the conduction defects previously reported inthe ACE 8/8 mice. Six-month-old ACE 1/8 mice have normal cardiacfunction, as determined by echocardiography and left ventricularcatheterization, despite the elevated levels of angiotensinII. ACE 1/8 mice also have normal levels of connexin 43. Bothwild-type and ACE 1/8 mice develop similar degrees of cardiachypertrophy after aortic banding. These data suggest that amoderate increase of local angiotensin II production in theheart does not produce cardiac dysfunction, at least under basalconditions, and that, in response to aortic banding, cardiachypertrophy is not augmented by a twofold increase of cardiacangiotensin II.

connexin; gene targeting; blood pressure; genetically modified mice

Address for reprint requests and other correspondence: H. D. Xiao, 101 Woodruff Cir., Rm. 7006, Emory Univ., Dept. of Pathology, Atlanta, GA 30322 (e-mail: hxiao2{at}emory.edu)

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