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- W2036288082 endingPage "e1001494" @default.
- W2036288082 startingPage "e1001494" @default.
- W2036288082 abstract "In Drosophila postembryonic neuroblasts, transition in gene expression programs of a cascade of transcription factors (also known as the temporal series) acts together with the asymmetric division machinery to generate diverse neurons with distinct identities and regulate the end of neuroblast proliferation. However, the underlying mechanism of how this temporal series acts during development remains unclear. Here, we show that Hh signaling in the postembryonic brain is temporally regulated; excess (earlier onset of) Hh signaling causes premature neuroblast cell cycle exit and under-proliferation, whereas loss of Hh signaling causes delayed cell cycle exit and excess proliferation. Moreover, the Hh pathway functions downstream of Castor but upstream of Grainyhead, two components of the temporal series, to schedule neuroblast cell cycle exit. Interestingly, hh is likely a target of Castor. Hence, Hh signaling provides a link between the temporal series and the asymmetric division machinery in scheduling the end of neurogenesis." @default.
- W2036288082 created "2016-06-24" @default.
- W2036288082 creator A5010748765 @default.
- W2036288082 creator A5025993965 @default.
- W2036288082 creator A5044138798 @default.
- W2036288082 creator A5071363714 @default.
- W2036288082 date "2013-02-26" @default.
- W2036288082 modified "2023-10-16" @default.
- W2036288082 title "Hedgehog Signaling Acts with the Temporal Cascade to Promote Neuroblast Cell Cycle Exit" @default.
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