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Distinct forms of Gq-receptor-dependent plasticity of excitatory transmission in the BNST are differentially affected by stress
Authors:Zoé A. McElligott  Jason R. Klug  William P. Nobis  Sachin Patel  Brad A. Grueter  Thomas L. Kash  Danny G. Winder
Affiliation:aVanderbilt Brain Institute.;bDepartment of Psychiatry.;cDepartment of Molecular Physiology and Biophysics, and;eCenter for Molecular Neuroscience, and Kennedy Center for Human Development, Vanderbilt University Medical Center, Nashville, TN; and ;dDepartment of Pharmacology and Bowles Alcohol Center, University of North Carolina at Chapel Hill, NC
Abstract:Long-term depression (LTD) is an important synaptic mechanism for limiting excitatory influence over circuits subserving cognitive and emotional behavior. A major means of LTD induction is through the recruitment of signaling via Gq-linked receptors activated by norepinephrine (NE), acetylcholine, and glutamate. Receptors from these transmitter families have been proposed to converge on a common postsynaptic LTD maintenance mechanism, such that hetero- and homosynaptic induction produce similar alterations in glutamate synapse efficacy. We report that in the dorsolateral and ventrolateral bed nucleus of the stria terminalis (BNST), recruitment of Gq-linked receptors by glutamate or NE initiates mechanistically distinct forms of postsynaptically maintained LTD and these LTDs are differentially regulated by stress exposure. In particular, we show that although both mGluR5- and α1-adrenergic receptor (AR)-dependent LTDs involve postsynaptic endocytosis, the α1-AR-initiated LTD exclusively involves modulation of signaling through calcium-permeable AMPA receptors. Further, α1-AR- but not mGluR5- dependent LTD is disrupted by restraint stress. α1-AR LTD is also impaired in mice chronically exposed to ethanol. These data thus suggest that in the BNST, NE- and glutamate-activated Gq-linked signaling pathways differentially tune glutamate synapse efficacy in response to stress.
Keywords:addiction   norepinephrine   metabotropic glutamate receptor   calcium-permeable AMPA receptor   ethanol
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