Reg-1α Promotes Differentiation of Cortical Progenitors via Its N-Terminal Active Domain. Front

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Varilh, Marjorie | van Ba, Acquatella-Tran | Silhol, Michelle | Nieto-Lopez, Francisco | Moussaed, Mireille | Lebart, Marie-Christine | Bovolenta, Paola | Verdier, Jean-Michel | Rossel, Mireille | Marcilhac, Anne | Trousse, Françoise

Edité par CCSD ; Frontiers media -

International audience. Reg-1α belongs to the Reg family of small, secreted proteins expressed in both pancreas and nervous system. Reg-1α is composed of two domains, an insoluble C-type lectin domain and a short soluble N-terminal peptide, which is released from the molecule upon proteolytic N-terminal processing, although the biological significance of this proteolysis remains unclear. We have previously shown that binding of Reg-1α to its receptor Extl3 stimulates axonal outgrowth. Reg-1α and Extl3 genes are expressed in the developing cortex but their expression decreases in adulthood, pointing to a possible function of this signaling system at the early developmental stages. Here, we demonstrate that recombinant Reg-1α increases migration and differentiation of cultured embryonic rat telencephalic progenitors via the activation of GSK-3β activity. In vivo overexpression of Reg-1α by in utero electroporation, has a similar effect, favoring premature differentiation of cortical progenitors. Notably, the N-terminal soluble domain, but not the C-type lectin domain, is largely responsible for Reg-1α effects on cortical neuronal differentiation. We thus conclude that Reg-1α via its proteolytically generated N-terminal domain is required for basic development processes.

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