| Literature DB >> 30905618 |
Nereo Kalebic1, Carlotta Gilardi1, Barbara Stepien1, Michaela Wilsch-Bräuninger1, Katherine R Long1, Takashi Namba1, Marta Florio1, Barbara Langen1, Benoit Lombardot1, Anna Shevchenko1, Manfred W Kilimann2, Hiroshi Kawasaki3, Pauline Wimberger4, Wieland B Huttner5.
Abstract
The evolutionary expansion of the mammalian neocortex (Ncx) is thought to be linked to increased proliferative capacity of basal progenitors (BPs) and their neurogenic capacity. Here, by quantifying BP morphology in the developing Ncx of mouse, ferret, and human, we show that increased BP proliferative capacity is linked to an increase in BP process number. We identify human membrane-bound PALMDELPHIN (PALMD-Caax) as an underlying factor, and we show that it drives BP process growth and proliferation when expressed in developing mouse and ferret Ncx. Conversely, CRISPR/Cas9-mediated disruption of PALMD or its binding partner ADDUCIN-γ in fetal human Ncx reduces BP process numbers and proliferation. We further show that PALMD-induced processes enable BPs to receive pro-proliferative integrin-dependent signals. These findings provide a link between BP morphology and proliferation, suggesting that changes in BP morphology may have contributed to the evolutionary expansion of the Ncx.Entities:
Keywords: Neurogenesis; Palmd; neocortical development; neocortical expansion; neural progenitor cells; neural progenitor morphology
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Year: 2019 PMID: 30905618 DOI: 10.1016/j.stem.2019.02.017
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633