Seminars in Nephrology
Volume 29, Issue 6 , Pages 569-578, November 2009

Sexual Dimorphism, the Aging Kidney, and Involvement of Nitric Oxide Deficiency

  • Chris Baylis, PhD

      Affiliations

    • Corresponding Author InformationAddress reprint requests to Dr. Chris Baylis, 1600 SW Archer Rd, Room M544, University of Florida, PO Box 100274, Gainesville, FL 32667

Departments of Physiology and Medicine (Nephrology), University of Florida, Gainesville, FL

Summary 

Females develop less age-dependent loss of renal function, in part because of cardiorenal protective effects of estrogens. The low androgen level in women also may be protective, although the animal and clinical data are controversial. Both estrogen and androgens act through multiple mechanisms, sometimes beneficial, sometimes damaging, which makes it difficult to predict the impact of hormone replacement therapy in an aging population. Nitric oxide (NO) deficiency contributes to age-dependent cardiovascular risk and kidney damage in animal models. The increased oxidative stress of aging impacts at multiple sites in the NO biosynthetic pathway to decrease NO production/action. Endothelial dysfunction develops with aging and is delayed in women, in association with a delayed increase in asymmetric dimethylarginine. Animal data suggest that the aging kidney develops NO deficiency because of changes in the neuronal NO synthase. Relative preservation of NO production in females contributes to the better cardiovascular and renal responses to aging.

Keywords: Estrogen, androgen, asymmetric dimethylarginine, cardiovascular events, dimethylarginine dimethylaminohydrolase

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PII: S0270-9295(09)00145-4

doi:10.1016/j.semnephrol.2009.07.003

Seminars in Nephrology
Volume 29, Issue 6 , Pages 569-578, November 2009