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      A Perisynaptic Ménage à Trois between Dlg, DLin-7, and Metro Controls Proper Organization of Drosophila Synaptic Junctions

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          Abstract

          Structural plasticity of synaptic junctions is a prerequisite to achieve and modulate connectivity within nervous systems, e.g., during learning and memory formation. It demands adequate backup systems that allow remodeling while retaining sufficient stability to prevent unwanted synaptic disintegration. The strength of submembranous scaffold complexes, which are fundamental to the architecture of synaptic junctions, likely constitutes a crucial determinant of synaptic stability. Postsynaptic density protein-95 (PSD-95)/ Discs-large (Dlg)-like membrane-associated guanylate kinases (DLG-MAGUKs) are principal scaffold proteins at both vertebrate and invertebrate synapses. At Drosophila larval glutamatergic neuromuscular junctions (NMJs) DlgA and DlgS97 exert pleiotropic functions, probably reflecting a few known and a number of yet-unknown binding partners. In this study we have identified Metro, a novel p55/MPP-like Drosophila MAGUK as a major binding partner of perisynaptic DlgS97 at larval NMJs. Based on homotypic LIN-2,-7 (L27) domain interactions, Metro stabilizes junctional DlgS97 in a complex with the highly conserved adaptor protein DLin-7. In a remarkably interdependent manner, Metro and DLin-7 act downstream of DlgS97 to control NMJ expansion and proper establishment of synaptic boutons. Using quantitative 3D-imaging we further demonstrate that the complex controls the size of postsynaptic glutamate receptor fields. Our findings accentuate the importance of perisynaptic scaffold complexes for synaptic stabilization and organization.

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          Author and article information

          Journal
          J Neurosci
          J. Neurosci
          jneuro
          jneurosci
          J. Neurosci
          The Journal of Neuroscience
          Society for Neuroscience
          0270-6474
          1529-2401
          28 April 2010
          : 30
          : 17
          : 5811-5824
          Affiliations
          [1] 1Institut für Genetik, Heinrich-Heine-Universität Düsseldorf, D-40225 Düsseldorf, Germany,
          [2] 2Leibniz Institute for Neurobiology, Department of Neurochemistry, D-39118 Magdeburg, Germany,
          [3] 3Institut für Physiologie, Universität Würzburg, D-97070 Würzburg, Germany,
          [4] 4Rudolf Virchow Deutsche Forschungsgemeinschaft Research Center for Experimental Medicine, D-97078 Würzburg, Germany,
          [5] 5European Neuroscience Institute, D-37077 Göttingen, Germany,
          [6] 6Institut für Biologie, Freie Universität Berlin, 14195 Berlin, Germany,
          [7] 7Instituto de Ciencias Biomédicas, Facultad de Medicina, Universidad de Chile, Santiago 6530499, Chile, and
          [8] 8Max Planck Institute of Cell Biology and Genetics, D-01307 Dresden, Germany
          Author notes
          Correspondence should be addressed to Ulrich Thomas, Department of Neurochemistry, Leibniz Institute for Neurobiology, Brenneckestrasse 6, D-39118 Magdeburg, Germany. thomas@ 123456ifn-magdeburg.de

          *A.B. and O.K. contributed equally to this work.

          Article
          PMC6632599 PMC6632599 6632599 3589377
          10.1523/JNEUROSCI.0778-10.2010
          6632599
          20427642
          3abc962f-935d-4be7-b03b-9669e4c7e92b
          Copyright © 2010 the authors 0270-6474/10/305811-14$15.00/0
          History
          : 12 February 2010
          : 1 March 2010
          Categories
          Articles
          Cellular/Molecular

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