Physiological Impact of Increased Expression of the AT1 Angiotensin Receptor

doi:10.1161/01.HYP.0000092000.07559.57

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Hypertension. 2003;42:507-514
Published online before print September 8, 2003, doi: 10.1161/01.HYP.0000092000.07559.57

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(Hypertension. 2003;42:507.)
© 2003 American Heart Association, Inc.

Scientific Contributions

Physiological Impact of Increased Expression of the AT₁ Angiotensin Receptor

Thu H. Le; Hyung-Suk Kim; Andrew M. Allen; Robert F. Spurney; Oliver Smithies; Thomas M. Coffman

From the Department of Medicine, Duke University and Durham VA Medical Centers (T.H.L., R.F.S., T.M.C.), Durham, NC; the Department of Pathology, University of North Carolina (H.-S.K., O.S.), Chapel Hill, NC; and The Howard Florey Institute, University of Melbourne (A.M.A.), Australia.

Correspondence to Thomas Coffman, MD, Division of Nephrology, Department of Medicine, Duke University and Durham VA Medical Centers, 508 Fulton St, Bldg 6, Room 1100, Durham, NC 27705. E-mail tcoffman{at}duke.edu

To test the effect of increased AT₁ receptor expression on bloodpressure, we used gene targeting to generate mouse lines witha tandem duplication of the AT_1A receptor gene locus (Agtr1a)along with >10 kb of 5' flanking DNA. By successive breeding,we generated mice with 3 and 4 copies of the Agtr1a gene locuson an inbred 129/Sv background. AT_1A mRNA expression and AT₁-specificbinding of ¹²⁵I-angiotensin II were increased in proportionto Agtr1a gene copy number. These animals survived in expectednumbers, and their body, heart, and kidney weights were similarto wild-type, 2-copy control mice. Pressor responses to angiotensinII were blunted in the 4-copy mice compared with control mice.In male mice, there was no correlation between resting bloodpressure and Agtr1a gene copy number or AT_1A mRNA levels. However,in female mice, there was a highly significant positive correlationbetween blood pressure and AT_1A receptor expression, paralleledby significant increases in aldosterone synthase expressionwith increase in gene copy number. Furthermore, in female butnot male mice, there was a positive correlation between kallikreinand AT_1A receptor mRNA levels and an inverse correlation betweenrenin mRNA and Agtr1a copy number. Thus, in female but not malemice, genetic variants that increase expression of AT₁ receptorsaffect blood pressure and gene expression programs. The impactof enhanced AT₁ receptor expression on blood pressure may beblunted by systemic compensatory responses and altered signal-effectorcoupling in the vasculature.

Key Words: hypertension, renal • renin • aldosterone • mice • gender

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