Extension of Longevity and Reduction of Inflammation is Ovarian-Dependent, but Germ Cell-Independent in Post-Reproductive Female Mice

Authors

Tracy L. Habermehl, Utah State UniversityFollow
Kate C. Parkinson, Utah State UniversityFollow
Gene B. Hubbard, University of Texas Health Science Center at San Antonio
Yuji Ikeno, University of Texas Health Science Center at San Antonio
Jennifer I. Engelmeyer, University of Cologne
Björn Schumacher, University of Cologne
Jeffrey B. Mason, Utah State UniversityFollow

Document Type

Article

Journal/Book Title/Conference

GeroScience

Volume

41

Issue

1

Publisher

Springer International Publishing

Publication Date

12-13-2018

First Page

1

Last Page

36

Abstract

Cardiovascular disease, rare in premenopausal women, increases sharply at menopause and is typically accompanied by chronic inflammation. Previous work in our laboratory demonstrated that replacing senescent ovaries in post-reproductive mice with young, actively cycling ovaries restored many health benefits, including decreased cardiomyopathy and restoration of immune function. Our objective here was to determine if depletion of germ cells from young transplanted ovaries would alter the ovarian-dependent extension of life and health span. Sixty-day-old germ cell-depleted and germ cell-containing ovaries were transplanted to post-reproductive, 17-month-old mice. Mean life span for female CBA/J mice is approximately 644 days. Mice that received germ cell-containing ovaries lived 798 days (maximum = 815 days). Mice that received germ cell-depleted ovaries lived 880 days (maximum = 1046 days), 29% further past the time of surgery than mice that received germ cell-containing ovaries. The severity of inflammation was reduced in all mice that received young ovaries, whether germ cell-containing or germ cell-depleted. Aging-associated inflammatory cytokine changes were reversed in post-reproductive mice by 4 months of new-ovary exposure. In summary, germ cell depletion enhanced the longevity-extending effects of the young, transplanted ovaries and, as with germ cell-containing ovaries, decreased the severity of inflammation, but did so independent of germ cells. Based on these observations, we propose that gonadal somatic cells are programed to preserve the somatic health of the organism with the intent of facilitating future germline transmission. As reproductive potential decreases or is lost, the incentive to preserve the somatic health of the organism is lost as well.

Comments

This is a post-peer-review, pre-copyedit version of an article published in GeroScience. The final authenticated version is available online at: http://dx.doi.org/10.1007/s11357-018-0049-4

Recommended Citation

Habermehl, T.L., Parkinson, K.C., Hubbard, G.B. et al. GeroScience (2018). https://doi.org/10.1007/s11357-018-0049-4