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A New Vesicular Scaffolding Complex Mediates the G-Protein-Coupled 5-HT1A Receptor Targeting to Neuronal Dendrites.

Authors :
Awabdh, Sana Al
Miserey-Lenkei, Stéphanie
Bouceba, Tahar
Masson, Justine
Kano, Fumi
Marinach-Patrice, Carine
Hamon, Michel
Emerit, Michel Boris
Darmon, Michéle
Source :
Journal of Neuroscience; 10/10/2012, Vol. 32 Issue 41, p14227-14241, 15p
Publication Year :
2012

Abstract

Although essential for their neuronal function, the molecular mechanisms underlying the dendritic targeting of serotonin G-proteincoupled receptors are poorly understood. Here, we characterized a Yif1B-dependent vesicular scaffolding complex mediating the intracellular traffic of the rat 5-HT<subscript>1A</subscript> receptor (5-HT<subscript>1A</subscript>R) toward dendrites. By combining directed mutagenesis, GST-pull down, and surface plasmon resonance, we identified a tribasic motif in the C-tail of the 5-HT<subscript>1A</subscript>R on which Yif1B binds directly with high affinity (KD37 nM). Moreover, we identified Yip1A, Rab6, and Kif5B as new partners of the 5-HT<subscript>1A</subscript>R/Yif1B complex, and showed that their expression in neurons is also crucial for the dendritic targeting of the 5-HT<subscript>1A</subscript>R. Live videomicroscopy revealed that 5-HT<subscript>1A</subscript>R, Yif1B, Yip1A, and Rab6 traffic in vesicles exiting the soma toward the dendritic tree, and also exhibit bidirectional motions, sustaining their role in 5-HT<subscript>1A</subscript>R dendritic targeting. Hence, we propose a new trafficking pathway model in which Yif1B is the scaffold protein recruiting the 5-HT<subscript>1A</subscript>R in a complex including Yip1A and Rab6, with Kif5B and dynein as two opposite molecular motors coordinating the traffic of vesicles along dendritic microtubules. This targeting pathway opens new insights for G-protein-coupled receptors trafficking in neurons. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
02706474
Volume :
32
Issue :
41
Database :
Complementary Index
Journal :
Journal of Neuroscience
Publication Type :
Academic Journal
Accession number :
82562598
Full Text :
https://doi.org/10.1523/JNEUROSCI.6329-11.2012