GΑ Subunit Coordinates with Ephrin-B to Balance Self-Renewal and Differentiation in Neural Progenitor Cells

Abstract

Proper development of the mammalian brain requires that neural progenitor cells balance self-renewal and differentiation under precise temporal and spatial regulation, but the underlying mechanisms are not well understood. In this study, we identify GΑ subunit as a positive regulator of mammalian neurogenesis, working with the regulator of G protein signaling (RGS)-mediated ephrin-B signaling pathway as two opposing forces to maintain a balance between self-renewal and differentiation in the developing mouse cerebral cortex. Multiple GΑ i subunits are expressed by cortical neural progenitor cells during the course of cortical neurogenesis. Activation of GΑ i signaling, through in utero electroporation-mediated expression of wild-type and constitutively active GΑ i subunits, counteracts the function of ephrin-B in cortical neural progenitors to induce differentiation. Genetic knock-in of an RGS-insensitive G184SGΑ i2 causes early cell cycle exit and a reduction of cortical neural progenitor cells and leads to a defect in the production of late born cortical neurons, similar to what is observed in mutant mice with deficiency in ephrin-B reverse signaling pathway. This study reveals a role of GΑ subunit in mammalian neurogenesis and uncovers a developmental mechanism, coordinated by the GΑ and ephrin-B signaling pathways, for control of the balance between self-renewal and differentiation in neural progenitor cells. S TEM C ELLS 2010; 28:1581–1589.