Prepubertal castration eliminates sex differences in lifespan and growth trajectories in genetically heterogeneous mice

Author:

Jiang Nisi12ORCID,Cheng Catherine J.12,Gelfond Jonathan13,Strong Randy145ORCID,Diaz Vivian1,Nelson James F.12

Affiliation:

1. The Sam and Ann Barshop Institute for Longevity and Aging Studies, UT Health San Antonio San Antonio Texas USA

2. Department of Cellular and Integrative Physiology UT Health San Antonio San Antonio Texas USA

3. Department of Population Health Sciences UT Health San Antonio San Antonio Texas USA

4. Department of Pharmacology UT Health San Antonio San Antonio Texas USA

5. Research Service of the South Texas Veterans Health Care System San Antonio Texas USA

Abstract

AbstractSex differences in aging and longevity have been widely observed, with females consistently outliving males across human populations. However, the mechanisms driving these disparities remain poorly understood. In this study, we explored the influence of post‐pubertal testicular effects on sex differences in aging by prepubertally castrating genetically heterogeneous (UM‐HET3) mice, a unique mouse model that emulates human sex differences in age‐related mortality. Prepubertal castration eliminated the longevity disparity between sexes by reducing the elevated early‐ to mid‐life mortality rate observed in males and extending their median lifespan to match that of females. Additionally, castration extended the duration of body weight growth and attenuated the inverse correlation between early‐age body weight and lifespan in males, aligning their growth trajectories with those of females. Our findings suggest that post‐pubertal testicular actions in genetically diverse mice are primarily responsible for sex differences in longevity as well as growth trajectories. These findings offer a foundation for further investigation into the fundamental mechanisms driving sex‐specific aging patterns and the development of potential pro‐longevity interventions.

Funder

National Institute on Aging

Publisher

Wiley

Subject

Cell Biology,Aging

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