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Articles, Cellular/Molecular

Transport of the Major Myelin Proteolipid Protein Is Directed by VAMP3 and VAMP7

Anke Feldmann, Jesa Amphornrat, Madeleine Schönherr, Christine Winterstein, Wiebke Möbius, Torben Ruhwedel, Lydia Danglot, Klaus-Armin Nave, Thierry Galli, Dieter Bruns, Jacqueline Trotter and Eva-Maria Krämer-Albers
Journal of Neuroscience 13 April 2011, 31 (15) 5659-5672; https://doi.org/10.1523/JNEUROSCI.6638-10.2011
Anke Feldmann
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Jesa Amphornrat
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Madeleine Schönherr
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Christine Winterstein
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Wiebke Möbius
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Torben Ruhwedel
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Lydia Danglot
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Klaus-Armin Nave
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Thierry Galli
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Dieter Bruns
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Jacqueline Trotter
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Eva-Maria Krämer-Albers
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Abstract

CNS myelination by oligodendrocytes requires directed transport of myelin membrane components and a timely and spatially controlled membrane expansion. In this study, we show the functional involvement of the R-soluble N-ethylmaleimide-sensitive factor attachment protein receptor (R-SNARE) proteins VAMP3/cellubrevin and VAMP7/TI-VAMP in myelin membrane trafficking. VAMP3 and VAMP7 colocalize with the major myelin proteolipid protein (PLP) in recycling endosomes and late endosomes/lysosomes, respectively. Interference with VAMP3 or VAMP7 function using small interfering RNA-mediated silencing and exogenous expression of dominant-negative proteins diminished transport of PLP to the oligodendroglial cell surface. In addition, the association of PLP with myelin-like membranes produced by oligodendrocytes cocultured with cortical neurons was reduced. We furthermore identified Syntaxin-4 and Syntaxin-3 as prime acceptor Q-SNAREs of VAMP3 and VAMP7, respectively. Analysis of VAMP3-deficient mice revealed no myelination defects. Interestingly, AP-3δ-deficient mocha mice, which suffer from impaired secretion of lysosome-related organelles and missorting of VAMP7, exhibit a mild dysmyelination characterized by reduced levels of select myelin proteins, including PLP. We conclude that PLP reaches the cell surface via at least two trafficking pathways with distinct regulations: (1) VAMP3 mediates fusion of recycling endosome-derived vesicles with the oligodendroglial plasma membrane in the course of the secretory pathway; (2) VAMP7 controls exocytosis of PLP from late endosomal/lysosomal organelles as part of a transcytosis pathway. Our in vivo data suggest that exocytosis of lysosome-related organelles controlled by VAMP7 contributes to myelin biogenesis by delivering cargo to the myelin membrane.

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The Journal of Neuroscience: 31 (15)
Journal of Neuroscience
Vol. 31, Issue 15
13 Apr 2011
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Transport of the Major Myelin Proteolipid Protein Is Directed by VAMP3 and VAMP7
Anke Feldmann, Jesa Amphornrat, Madeleine Schönherr, Christine Winterstein, Wiebke Möbius, Torben Ruhwedel, Lydia Danglot, Klaus-Armin Nave, Thierry Galli, Dieter Bruns, Jacqueline Trotter, Eva-Maria Krämer-Albers
Journal of Neuroscience 13 April 2011, 31 (15) 5659-5672; DOI: 10.1523/JNEUROSCI.6638-10.2011

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Transport of the Major Myelin Proteolipid Protein Is Directed by VAMP3 and VAMP7
Anke Feldmann, Jesa Amphornrat, Madeleine Schönherr, Christine Winterstein, Wiebke Möbius, Torben Ruhwedel, Lydia Danglot, Klaus-Armin Nave, Thierry Galli, Dieter Bruns, Jacqueline Trotter, Eva-Maria Krämer-Albers
Journal of Neuroscience 13 April 2011, 31 (15) 5659-5672; DOI: 10.1523/JNEUROSCI.6638-10.2011
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