SMO-M2 mutation does not support cell-autonomous Hedgehog activity in cerebellar granule cell precursors

01 Pubblicazione su rivista
Petroni Marialaura, Sahùn Roncero Maria, Ramponi Valentina, Fabretti Francesca, Nicolis Di Robilant Vittoria, Moretti Marta, Alfano Vincenzo, Corsi Alessandro, De Panfilis Simone, Giubettini Maria, Di Giulio Stefano, Capalbo Carlo, Belardinilli Francesca, Coppa Anna, Sardina Francesca, Colicchia Valeria, Pedretti Flaminia, Infante Paola, Cardinali Beatrice, Tessitore Alessandra, Canettieri Gianluca, De Smaele Enrico, Giannini Giuseppe
ISSN: 2045-2322

Growth and patterning of the cerebellum is compromised if granule cell precursors do not properly expand and migrate. During embryonic and postnatal cerebellar development, the Hedgehog pathway tightly regulates granule cell progenitors to coordinate appropriate foliation and lobule formation. Indeed, granule cells impairment or defects in the Hedgehog signaling are associated with developmental, neurodegenerative and neoplastic disorders. So far, scant and inefficient cellular models have been available to study granule cell progenitors, in vitro. Here, we validated a new culture method to grow postnatal granule cell progenitors as hedgehog-dependent neurospheres with prolonged self-renewal and ability to differentiate into granule cells, under appropriate conditions. Taking advantage of this cellular model, we provide evidence that Ptch1-KO, but not the SMO-M2 mutation, supports constitutive and cell-autonomous activity of the hedgehog pathway.

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