Analysis of Glutamate Receptor Function
University Of Utah, Salt Lake City UT
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Abstract
DESCRIPTION (provided by applicant): Nervous systems are plastic, that is, they can change with experience allowing us to learn, remember and forget. Experience-dependent plasticity occurs in part at synapses - specialized points of contact that mediate signaling between neurons. Experiences, sensations and emotions strengthen or weaken these connections shaping how the nervous system processes and stores information. Our long-term scientific goal is to uncover the molecular machinery that controls synaptic plasticity, as well as to understand how components of this machinery are assembled, and delivered to and regulated at synapses. The AMPA subtypes of ionotropic glutamate receptors (AMPARs) mediate synaptic transmission at most excitatory synapses. We have developed new genetic strategies to uncover the molecular machinery required for synaptic transmission at glutamatergic synapses in C. elegans. In a series of studies, we identified four classes of evolutionarily conserved auxiliary subunits that contribute to AMPAR function, showed that they have dramatic effects on in vivo glutamate-gated currents, and demonstrated that mutations in these genes predictably modify AMPAR-mediated behaviors. We also discovered that the delivery and removal of synaptic AMPARs was dependent on kinesin-1 microtubule-dependent motors. Thus, AMPAR transport along neuronal processes, and glutamate-gated currents, are dramatically reduced in unc-116 mutants (KIF5) and klc-2 mutants (Kinesin light chain 2). These findings led us to search for signaling molecules that regulate the transport of AMPARs. We have now identified two classes of evolutionarily conserved kinases that contribute to the transport of AMPARs to synapses. These same kinases are implicated in cellular models of learning and memory, such as long-term potentiation and long-term depression. We now plan to test the hypothesis that these kinase-signaling pathways contribute to the regulated delivery of synaptic AMPARs and their auxiliary proteins. We predict that what we learn from our proposed studies will have immediate relevance to ongoing studies of synaptic plasticity, learning and memory in vertebrates. Thus, our studies could contribute to new diagnostic or therapeutic modalities for disorders associated with altered neurotransmission in the brain.
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