Literature DB >> 17272668

Effects of dietary protein restriction on nephron number in the mouse.

Chantal C Hoppe1, Roger G Evans, John F Bertram, Karen M Moritz.   

Abstract

In rats, maternal protein restriction reduces nephron endowment and often leads to adult hypertension. Sex differences in these responses have been identified. The molecular and genetic bases of these phenomena can best be identified in a mouse model, but effects of maternal protein restriction on kidney development have not been examined in mice. Therefore, we determined how combined prenatal and postnatal protein restriction in mice affects organ weight, glomerular number and dimensions, and renal expression of angiotensin receptor mRNA, in both male and female offspring. C57/BL6/129sv mice received either a normal (20% wt/wt; NP) or low (9% wt/wt; LP) protein diet during gestation and postnatal life. Offspring were examined at postnatal day 30. Protein restriction retarded growth of the kidney, liver, spleen, heart, and brain. All organs except the brain weighed less in female than male offspring. Protein restriction increased normalized (to body weight) brain weight, with females having relatively heavier brains than males. The effects of protein restriction were not sex dependent, except that normalized liver weight was reduced in males but increased in females. Glomerular volume, but not number, was greater in female than in male mice. Maternal protein restriction reduced nephron endowment similarly in male and female mice. Renal expression of AT(1A) receptor mRNA was approximately sixfold greater in female than male NP mice, but similar in male LP and female LP mice. We conclude that maternal protein restriction reduces nephron endowment in mice. This effect provides a basis for future studies of developmental programming in the mouse.

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Year:  2007        PMID: 17272668     DOI: 10.1152/ajpregu.00442.2006

Source DB:  PubMed          Journal:  Am J Physiol Regul Integr Comp Physiol        ISSN: 0363-6119            Impact factor:   3.619


  36 in total

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Review 2.  Epigenetics and developmental programming of adult onset diseases.

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Review 3.  Genetic, environmental, and epigenetic factors involved in CAKUT.

Authors:  Nayia Nicolaou; Kirsten Y Renkema; Ernie M H F Bongers; Rachel H Giles; Nine V A M Knoers
Journal:  Nat Rev Nephrol       Date:  2015-08-18       Impact factor: 28.314

Review 4.  Why and how we determine nephron number.

Authors:  John F Bertram; Luise A Cullen-McEwen; Gary F Egan; Norbert Gretz; Edwin Baldelomar; Scott C Beeman; Kevin M Bennett
Journal:  Pediatr Nephrol       Date:  2014-04       Impact factor: 3.714

5.  Renal blood flow and dynamic autoregulation in conscious mice.

Authors:  Radu Iliescu; Radu Cazan; Gerald R McLemore; Marcia Venegas-Pont; Michael J Ryan
Journal:  Am J Physiol Renal Physiol       Date:  2008-06-25

Review 6.  Defining and redefining the nephron progenitor population.

Authors:  Caroline Hendry; Bree Rumballe; Karen Moritz; Melissa H Little
Journal:  Pediatr Nephrol       Date:  2011-01-14       Impact factor: 3.714

Review 7.  Sexual dimorphism: the aging kidney, involvement of nitric oxide deficiency, and angiotensin II overactivity.

Authors:  Chris Baylis
Journal:  J Gerontol A Biol Sci Med Sci       Date:  2012-09-07       Impact factor: 6.053

Review 8.  Understanding developmental pharmacodynamics: importance for drug development and clinical practice.

Authors:  Hussain Mulla
Journal:  Paediatr Drugs       Date:  2010-08-01       Impact factor: 3.022

Review 9.  Epigenetics: a new way to look at kidney diseases.

Authors:  Pazit Beckerman; Yi-An Ko; Katalin Susztak
Journal:  Nephrol Dial Transplant       Date:  2014-03-27       Impact factor: 5.992

10.  Prematurity in mice leads to reduction in nephron number, hypertension, and proteinuria.

Authors:  Cary Stelloh; Kenneth P Allen; David L Mattson; Alexandra Lerch-Gaggl; Sreenivas Reddy; Asraf El-Meanawy
Journal:  Transl Res       Date:  2011-11-08       Impact factor: 7.012

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