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Publication : DSCAM regulates delamination of neurons in the developing midbrain.

First Author  Arimura N Year  2020
Journal  Sci Adv Volume  6
Issue  36 PubMed ID  32917586
Mgi Jnum  J:313612 Mgi Id  MGI:6790749
Doi  10.1126/sciadv.aba1693 Citation  Arimura N, et al. (2020) DSCAM regulates delamination of neurons in the developing midbrain. Sci Adv 6(36)
abstractText  For normal neurogenesis and circuit formation, delamination of differentiating neurons from the proliferative zone must be precisely controlled; however, the regulatory mechanisms underlying cell attachment are poorly understood. Here, we show that Down syndrome cell adhesion molecule (DSCAM) controls neuronal delamination by local suppression of the RapGEF2-Rap1-N-cadherin cascade at the apical endfeet in the dorsal midbrain. Dscam transcripts were expressed in differentiating neurons, and DSCAM protein accumulated at the distal part of the apical endfeet. Cre-loxP-based neuronal labeling revealed that Dscam knockdown impaired endfeet detachment from ventricles. DSCAM associated with RapGEF2 to inactivate Rap1, whose activity is required for membrane localization of N-cadherin. Correspondingly, Dscam knockdown increased N-cadherin localization and ventricular attachment area at the endfeet. Furthermore, excessive endfeet attachment by Dscam knockdown was restored by co-knockdown of RapGEF2 or N-cadherin Our findings shed light on the molecular mechanism that regulates a critical step in early neuronal development.
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