Publication | Open Access
Ephrin-A2 reverse signaling negatively regulates neural progenitor proliferation and neurogenesis
206
Citations
39
References
2005
Year
Cell DeathCellular NeurobiologySocial SciencesNeuroregenerationEpendymaAutophagyCell NumberCell SignalingMolecular NeuroscienceNeuroprotectionOlfactory BulbCell BiologyDevelopmental BiologyStem Cell ResearchNeuroscienceMolecular NeurobiologyShorter Cell CycleMedicineNeural Stem CellEphrin-a2 Reverse
The number of cells in an organ is regulated by mitogens and trophic factors that impinge on intrinsic determinants of proliferation and apoptosis. We here report the identification of an additional mechanism to control cell number in the brain: EphA7 induces ephrin-A2 reverse signaling, which negatively regulates neural progenitor cell proliferation. Cells in the neural stem cell niche in the adult brain proliferate more and have a shorter cell cycle in mice lacking ephrin-A2. The increased progenitor proliferation is accompanied by a higher number of cells in the olfactory bulb. Disrupting the interaction between ephrin-A2 and EphA7 in the adult brain of wild-type mice disinhibits proliferation and results in increased neurogenesis. The identification of ephrin-A2 and EphA7 as negative regulators of progenitor cell proliferation reveals a novel mechanism to control cell numbers in the brain.
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