A Perisynaptic Ménage à Trois between Dlg, DLin-7, and Metro Controls Proper Organization of Drosophila Synaptic Junctions
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2010-04-28Metadata
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Bachmann, André
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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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This work was supported by the Deutsche Forschungsgemeinschaft (DFG-Sonderforschungsbereich 854), the
Leibniz Gemeinschaft (WGL-Pakt f ¨ur Forschung und Innovation), and a Max Planck award from the Alexander von
Humboldt Foundation and the Max Planck Society to E.D.G. R.J.K. is supported by the Deutsche Forschungsgemeinschaft
Emmy-Noether Program.
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URI: https://repositorio.uchile.cl/handle/2250/128555
DOI: DOI:10.1523/JNEUROSCI.0778-10.2010
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The Journal of Neuroscience, April 28, 2010 • 30(17):5811–5824 • 5811
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