| Literature DB >> 26651291 |
Susan van Erp1, Dianne M A van den Heuvel1, Yuki Fujita2, Ross A Robinson3, Anita J C G M Hellemons1, Youri Adolfs1, Eljo Y Van Battum1, Anna M Blokhuis1, Marijn Kuijpers4, Jeroen A A Demmers5, Håkan Hedman6, Casper C Hoogenraad4, Christian Siebold3, Toshihide Yamashita2, R Jeroen Pasterkamp7.
Abstract
Many guidance receptors are proteolytically cleaved by membrane-associated metalloproteases of the ADAM family, leading to the shedding of their ectodomains. Ectodomain shedding is crucial for receptor signaling and function, but how this process is controlled in neurons remains poorly understood. Here, we show that the transmembrane protein Lrig2 negatively regulates ADAM-mediated guidance receptor proteolysis in neurons. Lrig2 binds Neogenin, a receptor for repulsive guidance molecules (RGMs), and prevents premature Neogenin shedding by ADAM17 (TACE). RGMa reduces Lrig2-Neogenin interactions, providing ADAM17 access to Neogenin and allowing this protease to induce ectodomain shedding. Regulation of ADAM17-mediated Neogenin cleavage by Lrig2 is required for neurite growth inhibition by RGMa in vitro and for cortical neuron migration in vivo. Furthermore, knockdown of Lrig2 significantly improves CNS axon regeneration. Together, our data identify a unique ligand-gated mechanism to control receptor shedding by ADAMs and reveal functions for Lrigs in neuron migration and regenerative failure.Entities:
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Year: 2015 PMID: 26651291 DOI: 10.1016/j.devcel.2015.11.008
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270