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Drosophila perlecan modulates FGF and hedgehog signals to activate neural stem cell division
Authors:Park Youngji  Rangel Carolina  Reynolds M Megan  Caldwell M Craig  Johns Misty  Nayak Mamatha  Welsh C Jane R  McDermott Sean  Datta Sumana
Affiliation:Department of Biochemistry and Biophysics, Texas A&M University, TAMU 2128, College Station, TX 77843-2128, USA.
Abstract:Mutations in the Drosophila trol gene cause cell cycle arrest of neuroblasts in the larval brain. Here, we show that trol encodes the Drosophila homolog of Perlecan and regulates neuroblast division by modulating both FGF and Hh signaling. Addition of human FGF-2 to trol mutant brains in culture rescues the trol proliferation phenotype, while addition of a MAPK inhibitor causes cell cycle arrest of the regulated neuroblasts in wildtype brains. Like FGF, Hh activates stem cell division in the larval brain in a Trol-dependent fashion. Coimmunoprecipitation studies are consistent with interactions between Trol and Hh and between mammalian Perlecan and Shh that are not competed with heparin sulfate. Finally, analyses of mutations in trol, hh, and ttv suggest that Trol affects Hh movement. These results indicate that Trol can mediate signaling through both of the FGF and Hedgehog pathways to control the onset of stem cell proliferation in the developing nervous system.
Keywords:Drosophila   Perlecan   Stem cell proliferation   FGF   Hedgehog   trol
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