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Publication : A multistate stem cell dynamics maintains homeostasis in mouse spermatogenesis.

First Author  Nakagawa T Year  2021
Journal  Cell Rep Volume  37
Issue  3 Pages  109875
PubMed ID  34686326 Mgi Jnum  J:328290
Mgi Id  MGI:6881866 Doi  10.1016/j.celrep.2021.109875
Citation  Nakagawa T, et al. (2021) A multistate stem cell dynamics maintains homeostasis in mouse spermatogenesis. Cell Rep 37(3):109875
abstractText  In mouse testis, a heterogeneous population of undifferentiated spermatogonia (Aundiff) harbors spermatogenic stem cell (SSC) potential. Although GFRalpha1(+) Aundiff maintains the self-renewing pool in homeostasis, the functional basis of heterogeneity and the implications for their dynamics remain unresolved. Here, through quantitative lineage tracing of SSC subpopulations, we show that an ensemble of heterogeneous states of SSCs supports homeostatic, persistent spermatogenesis. Such heterogeneity is maintained robustly through stochastic interconversion of SSCs between a renewal-biased Plvap(+)/GFRalpha1(+) state and a differentiation-primed Sox3(+)/GFRalpha1(+) state. In this framework, stem cell commitment occurs not directly but gradually through entry into licensed but uncommitted states. Further, Plvap(+)/GFRalpha1(+) cells divide slowly, in synchrony with the seminiferous epithelial cycle, while Sox3(+)/GFRalpha1(+) cells divide much faster. Such differential cell-cycle dynamics reduces mitotic load, and thereby the potential to acquire harmful de novo mutations of the self-renewing pool, while keeping the SSC density high over the testicular open niche.
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