Failure of the stem cell niche rather than loss of oocyte stem cells in the aging ovary

نویسندگان

  • Efi Massasa
  • Xavier Santamaria Costa
  • Hugh S. Taylor
چکیده

possibility of postnatal oogenesis in humans and other species has become one of today's most debated topics in the fields of reproductive and developmental biology. Wilhelm Waldeyer concluded in 1870 that oocyte production ceases with birth, and for more than a century scientists have been in consensus that the number of oocytes is gradually reduced throughout adult life [1]. A contemporary understanding of tissue regeneration, together with novel experimental methods, led to a new school of thought that has challenged the model of prenatal "total endowment", by suggesting replenishment of the post-natal oocytes pool by adult Germline Stem Cell (GSC). According to this theory, a small number of GSC remains viable to produce oocytes or oocyte-like cells within the ovary throughout the lifespan of the adult female [2,3]. These cells may originate from within or from outside the ovary. However, in a parabiotic model, or after bone marrow transplantation, the absence of mature donor derived eggs in the recipient suggested that mature eggs are not readily generated by cells from outside of the ovary [4]. Supporters of the GSC model insist that the absence of mature eggs from a donor do not contradict the idea of a progenitor cell that may give rise to a pool of additional oocytes. Last year, Zou et. [5] established a GSC cell line by sorting for ovarian cells that were positive for the mouse vasa homologue (MVH) protein. These cells went through many passages in culture, showed high telomerase activity, and when stably trans-Commentary fected with GFP and transplanted into females, gave rise to offspring that carried the signal. The controversy surrounding the relation between age and the reducing number of eggs produced females only increased. Now, in this issue of Aging, Niikura and colleagues finally clarify what had appeared to be discrepant results. They show that the premeiotic marker Stra8 and Daz1, an exclusive marker of meiosis-committed cells, are highly expressed in the ovary of aged female mice despite their being devoid of oocytes [6]. Further, by grafting an aged ovarian tissue from germ cell-specific Oct4ΔPE::GFP transgenic mice into the ovary of a young wild-type host, the authors show the formation of GFP positive immature follicles along with the co-expression of NOBOX (a primordial oocyte marker). Conversely exposure to the aged environment resulted in a reduced number of immature follicles in the young tissue. Moreover, these finding suggest that the decrease in the …

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عنوان ژورنال:

دوره 2  شماره 

صفحات  -

تاریخ انتشار 2010