Abstract

Learning and memory are likely to involve changes in the efficacy of synaptic transmission. In many cases, these changes are thought to involve modulation of the mechanism by which transmitter is released from the nerve terminal. This proposal attempts to illuminate some of the fundamental cellular mechanisms by which synapses release transmitter, on the presumption that understanding these mechanisms is a precondition to fully understanding how release is altered by learning or by disease states. The approach of this proposal is to use Drosophila genetics to explore two proteins appear to be central to this process: synaptotagmin and synaprobrevin. Both proteins are on synaptic vesicles and Drosophila mutations have been isolated in both genes. Mutations will be characterized by a combination of electrophysiology, electron microscopy, and the use of a fluorescent dye to monitor membrane trafficking. To probe the actions of these proteins more closely, engineered alteration in these proteins will be reintroduced into the mutant files. Drosophila will also be used to screen for novel mutations that may reveal previously unknown components of the synaptic machinery. Specifically, this project will: 1. Create alterations in particular domains of synaptotagmin for biochemical and genetic experiments. 2. By examining the phenotype of these altered synaptotagmins to test the hypotheses that synaptotagmin is the Ca2+ -sensor for triggering vesicle fusion, a regulator of vesicle docking, and involved in vesicle recycling. 3. Use Drosophila that lack synaprobrevin and use cloned genes encoding additional members of the v-SNARE family to identify sequences essential for targeting synaptobrevin to vesicles and targeting vesicles to their appropriate release sites. 4. Use altered synaptobrevins to determining which regions are essential for vesicle fusion with the plasma membrane. 5. Screen for enhancers and suppressors of known synaptic mutations and characterize those mutations. 6. Screen physiologically for mutations in synaptic transmission and characterize those mutations.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Specialized Center (P50)
Project #
5P50MH048108-10
Application #
6347622
Study Section
Project Start
2000-09-01
Project End
2001-08-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
10
Fiscal Year
2000
Total Cost
$154,408
Indirect Cost

  Institution

Name
Stanford University
Department
Type
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Murthy, Mala; Garza, Dan; Scheller, Richard H et al. (2003) Mutations in the exocyst component Sec5 disrupt neuronal membrane traffic, but neurotransmitter release persists. Neuron 37:433-47
Gorska-Andrzejak, J; Stowers, R S; Borycz, J et al. (2003) Mitochondria are redistributed in Drosophila photoreceptors lacking milton, a kinesin-associated protein. J Comp Neurol 463:372-88
Finley, Michael F A; Scheller, Richard H; Madison, Daniel V (2003) SNAP-25 Ser187 does not mediate phorbol ester enhancement of hippocampal synaptic transmission. Neuropharmacology 45:857-62
Deisseroth, Karl; Mermelstein, Paul G; Xia, Houhui et al. (2003) Signaling from synapse to nucleus: the logic behind the mechanisms. Curr Opin Neurobiol 13:354-65
Waters, Jack; Smith, Stephen J (2002) Vesicle pool partitioning influences presynaptic diversity and weighting in rat hippocampal synapses. J Physiol 541:811-23
Horrigan, Frank T; Aldrich, Richard W (2002) Coupling between voltage sensor activation, Ca2+ binding and channel opening in large conductance (BK) potassium channels. J Gen Physiol 120:267-305
Stowers, R Steven; Megeath, Laura J; Gorska-Andrzejak, Jolanta et al. (2002) Axonal transport of mitochondria to synapses depends on milton, a novel Drosophila protein. Neuron 36:1063-77
Hopf, F Woodward; Waters, Jack; Mehta, Samar et al. (2002) Stability and plasticity of developing synapses in hippocampal neuronal cultures. J Neurosci 22:775-81
Montgomery, Johanna M; Madison, Daniel V (2002) State-dependent heterogeneity in synaptic depression between pyramidal cell pairs. Neuron 33:765-77
Finley, Michael F A; Patel, Sejal M; Madison, Daniel V et al. (2002) The core membrane fusion complex governs the probability of synaptic vesicle fusion but not transmitter release kinetics. J Neurosci 22:1266-72

Showing the most recent 10 out of 81 publications