Six Truisms Concerning ACE and the Renin-Angiotensin System Educed From the Genetic Analysis of Mice

doi:10.1161/01.RES.0000169536.73576.66

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Circulation Research. 2005;96:1135-1144
doi: 10.1161/01.RES.0000169536.73576.66

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(Circulation Research. 2005;96:1135.)
© 2005 American Heart Association, Inc.

Review

Six Truisms Concerning ACE and the Renin-Angiotensin System Educed From the Genetic Analysis of Mice

Kenneth E. Bernstein, Hong D. Xiao, Kristen Frenzel, Ping Li, Xiao Z. Shen, Jon W. Adams, Sebastien Fuchs

From the Department of Pathology and Laboratory Medicine, Emory University, Atlanta, Ga.

Correspondence to Dr Ken Bernstein, Rm 7107A WMB, Department of Pathology, 101 Woodruff Cir, Atlanta, GA 30322. E-mail kbernst@emory.edu

This Review is part of a thematic series on Angiotensin Converting Enzyme, which includes the following articles:

Six Truisms Concerning ACE and the Renin-Angiotensin System Educed From the Genetic Analysis of Mice

ACE and Vascular Remodeling ACE II in the Heart and the Kidney

ACE Signaling

ACE Polymorphisms
Rudi Bussi Editors

Key Words: angiotensin • renin-angiotensin system • mouse • cardiovascular disease • angiotensin converting enzyme

An extract of the first 250 words of the full text is provided, because this article has no abstract.

Introduction

The history of the renin-angiotensin system (RAS) is one ofmarvelous discoveries extending from Robert Tigerstedt’snaming renin in 1898 to the present time; biochemists, physiologists,pharmacologists, and practicing clinicians have all combinedto describe the physiologic implications of converting angiotensinogeninto angiotensin II. Indeed, one may argue that the clinicaldevelopment of ACE inhibitors and angiotensin II receptor antagonistshas benefited humankind to a level seen only with the developmentof antibiotics and steroids. As we begin the twenty-first century,it is worthwhile to summarize the state of our knowledge concerningACE and angiotensin II. In doing, we benefit from a whole classof experiments not available to those writing reviews even 10years ago: the revolution in our ability to genetically manipulatethe mouse as an experimental model. This is due to the widespreadapplication of gene targeting by homologous recombination inembryonic stem cells. As is widely appreciated, this technologycan produce a knockout mouse lacking any particular gene. Lessappreciated are the full capabilities of this methodology whichcan be summarized as: if it can be dreamed, it can be done.Gene targeting can be used to create point mutations, duplicatea gene, and modify the expression pattern of a protein almostas easily as creating knockout mice null for a particular protein.We, and others, have used gene targeting in mice to create modificationsin the renin-angiotensin system of a sort not seen in humans.While any single experiment may be assailed as not representing. . . [Full Text of this Article]

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