PUMA regulates germ cell loss and primordial follicle endowment in mice.

Reproduction

MIMR-PHI Institute of Medical Research27-31 Wright Street, Clayton, Victoria 3168, AustraliaDepartment of Anatomy and Developmental BiologyMonash University, Clayton, Victoria, AustraliaThe Walter and Eliza Hall Institute of Medical ResearchMelbourne, Victoria, AustraliaDepartment of Medical BiologyThe University of Melbourne, Melbourne, Victoria, AustraliaMIMR-PHI Institute of Medical Research27-31 Wright Street, Clayton, Victoria 3168, AustraliaDepartment of Anatomy and Developmental BiologyMonash University, Clayton, Victoria, AustraliaThe Walter and Eliza Hall Institute of Medical ResearchMelbourne, Victoria, AustraliaDepartment of Medical BiologyThe University of Melbourne, Melbourne, Victoria, Australia

Published: August 2014

AI Article Synopsis

  • The study identifies BBC3 (PUMA) as a crucial protein that regulates germ cell death during ovarian development, impacting the number of primordial follicles formed.
  • Disruption of the Bbc3 gene led to a significant increase in germ cell counts in female mice, resulting in a nearly doubled number of primordial follicles by postnatal day 10.
  • BBC3 is essential for controlling germ cell death early in development but does not influence germ cell proliferation or the subsequent loss of germ cells during later stages.

Article Abstract

The number of primordial follicles initially established within the ovary is influenced by the extent of germ cell death during foetal ovarian development, but the mechanisms that mediate this death have not been fully uncovered. In this study, we identified BBC3 (PUMA) (p53 upregulated modulator of apoptosis, also known as BCL2-binding component 3), a pro-apoptotic BH3-only protein belonging to the BCL2 family, as a critical determinant of the number of germ cells during ovarian development. Targeted disruption of the Bbc3 gene revealed a significant increase in the number of germ cells as early as embryonic day 13.5. The number of germ cells remained elevated in Bbc3(-/-) female mice compared with WT female mice throughout the remainder of embryonic and early postnatal life, resulting in a 1.9-fold increase in the number of primordial follicles in the ovary on postnatal day 10. The increase in the number of germ cells observed in the ovaries of Bbc3(-/-) mice could not be attributed to the altered proliferative activity of germ cells within the ovaries. Furthermore, BBC3 was found to be not required for the massive germ cell loss that occurs during germ cell nest breakdown. Our data indicate that BBC3 is a critical regulator of germ cell death that acts during the migratory phase of oogenesis or very soon after the arrival of germ cells in the gonad and that BBC3-mediated cell death limits the number of primordial follicles established in the initial ovarian reserve.

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Source
http://dx.doi.org/10.1530/REP-13-0666DOI Listing

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