PRE & POSTSYNAPTIC NICOTINIC ACHRS--STRUCTURE & FUNCTION
Project Number5R01MH054251-02
Contact PI/Project LeaderSARGENT, PETER B.
Awardee OrganizationUNIVERSITY OF CALIFORNIA, SAN FRANCISCO
Description
Abstract Text
DESCRIPTION (Adapted from applicant's abstract): The long-term goal of our
research is to understand the nature and the consequences of diversity in
the expression of neuronal acetylcholine receptors (nAChRs). Recent
molecular biological studies have identified a family of putative nAChR
genes in the nervous system. However, there is little evidence that nAChRs
generally serve the same function in the central nervous system that they do
in the peripheral nervous system, where they underlie fast, excitatory
synaptic transmission. We propose to use both structural and functional
approaches to examine nAChRs in two preparations from the embryonic chicken,
where monoclonal antibodies specific for each of the nicotinic receptor gene
products are available: the lateral spiriform nucleus (SpL), located in the
mesencephalon, and the ciliary ganglion, located in the orbit. We will use
subunit-specific antibodies to chick nAChRs and immunocytochemical
techniques to examine the distribution of nAChR subunits among and within
neurons. At the cellular level, we will examine whether all cells within
the neuronal population (SpL, or ciliary ganglion) express the same subset
of subunits. At the subcellular level, we will examine the distribution of
receptor subunits at the neuronal surface in order to determine which
subunits are located at synaptic sites, which subunits are located
extrasynaptically, and which may be transported to axon terminals. Finally,
at the molecular level, we will use fluorophore-tagged antibodies and
fluorescence resonance energy transfer (FRET) to examine the proximity of
subunits to each other. This technique should allow us to learn which
subunits are assembled into receptor oligomers. We will pay particular
attention to presynaptic nicotinic receptors, which, although virtually
uncharacterized to date, may represent the predominant form of nAChR in the
central nervous system. We will examine by immunocytochemical techniques
whether presynaptic nicotinic receptors are found on the surface of SpL axon
terminals that project to the optic tectum and whether they are present on
the terminals of preganglionic neurons that project to the ciliary ganglion.
Should presynaptic receptors be found in the ciliary ganglion, we will
attempt to characterize these receptors functionally by patch clamp
recordings. The studies should enhance our understanding of the structure
and function of neuronal nicotinic receptors by (1) identifying which
subunits associate to form receptor oligomers likely to serve both
postsynaptic and presynaptic functions and (2) examining the structure and
function of nicotinic presynaptic receptors. It is likely that a fuller
understanding of the structure and function of both postsynaptic and
presynaptic nicotinic receptors will be essential for understanding
nicotine's effects on the nervous system and of the basis of nicotine
tolerance and dependence.
No Sub Projects information available for 5R01MH054251-02
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