Sex-Specific Effects of Prenatal Low-Protein and Carbenoxolone Exposure on Renal Angiotensin Receptor Expression in Rats

doi:10.1161/01.HYP.0000188702.96256.46

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Hypertension. 2005;46:1374-1380
Published online before print October 17, 2005, doi: 10.1161/01.HYP.0000188702.96256.46

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(Hypertension. 2005;46:1374.)
© 2005 American Heart Association, Inc.

Original Articles

Sex-Specific Effects of Prenatal Low-Protein and Carbenoxolone Exposure on Renal Angiotensin Receptor Expression in Rats

Sarah McMullen; Simon C. Langley-Evans

From the Division of Nutritional Sciences, University of Nottingham, Loughborough, United Kingdom.

Correspondence to Simon C. Langley-Evans, Division of Nutritional Sciences, University of Nottingham, Sutton Bonington Campus, Loughborough, LE12 5RD, United Kingdom. E-mail simon.langley-evans{at}nottingham.ac.uk

Experimental models have shown the developing cardiovascularand renal systems to be sensitive to mild shifts in maternalnutrition, leading to altered function and risk of disease inadult life. The offspring of Wistar rats fed a low-protein dietduring pregnancy exhibit a reduced nephron number and hypertensionin postnatal life, providing a useful tool to examine the mechanisticbasis of programming. Evidence indicates that upregulation ofthe renin-angiotensin system plays an important role, in particularthrough receptor-mediated changes in angiotensin II activity.However, although programmed hypertension has proven dependenton maternal glucocorticoids, there appear to be conflictingeffects of prenatal low-protein and glucocorticoid exposureon postnatal angiotensin receptor expression. This study aimedto resolve this issue by comparing the effects of low-proteinand glucocorticoid exposures on postnatal nephron number andangiotensin receptor expression. In addition, this study examinedthe modulation of prenatal treatment effects by postnatal inhibitionof type 1 angiotensin receptor. The data demonstrates that whereasprenatal low-protein and glucocorticoid exposure have a similareffect in reducing nephron number, there are age- and gender-relateddifferences in their effects on postnatal angiotensin receptorexpression. In addition, this study provides novel evidenceof a substantial upregulation of type 2 angiotensin receptorexpression in low-protein- and glucocorticoid-exposed femaleoffspring at 20 weeks of age, with implications for subsequentrenal remodeling and function. Despite being targeted to thepostnephrogenic period, inhibition of type 1 angiotensin receptorhad an inhibitory effect on renal and somatic growth, additionallyindicating its unsuitability during early life.

Key Words: hypertension • programming • gender • angiotensin receptor • nephron • rat

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