Abstract
AbstractThe switch from precursor cell proliferation to onset of differentiation in adult stem cell lineages must be carefully regulated to produce sufficient progeny to maintain and repair tissues, yet prevent overproliferation that may enable oncogenesis. In theDrosophilamale germ cell lineage, spermatogonia produced by germ line stem cells undergo a limited number of transit amplifying mitotic divisions before switching to the spermatocyte program that sets up meiosis and eventual spermatid differentiation. The number of transit amplifying divisions is set by accumulation of thebag-of-marbles(Bam) protein to a critical threshold. Inbammutants, spermatogonia proliferate through several extra rounds of mitosis then die without becoming spermatocytes. Here we show that the key role of Bam for the mitosis to differentiation switch is repressing expression of Held Out Wings (how), homolog of mammalian Quaking. Knock down ofhowin germ cells was sufficient to allow spermatogonia mutant forbamor its partnerbenign gonial cell neoplasm(bgcn) to differentiate, while forced expression of nuclear-targeted How protein in spermatogonia wild-type forbamresulted in continued proliferation at the expense of differentiation. Our findings suggest that Bam targetshowRNA for degradation by acting as an adapter to recruit the CCR4-NOT deadenylation complex via binding its subunit, Caf40. As How is itself an RNA binding protein with roles in RNA processing, our findings reveal that the switch from proliferation to meiosis and differentiation in theDrosophilamale germ line adult stem cell lineage is regulated by a cascade of RNA-binding proteins.
Publisher
Cold Spring Harbor Laboratory