Awardee OrganizationUNIVERSITY OF CALIFORNIA BERKELEY
Description
Abstract Text
Membrane trafficking contributes to the intracellular organization of all
eukaryotic cells, and to the specialized functions of many cell types.
The membranous compartments of the secretory and endocytic pathways
exhibit distinct biochemical properties related to the specific functions
that they perform. This intracellular organization is maintained, in
part, by transport vesicles that shuttle membrane and soluble cargo from
one intracellular compartment of another. In specialized cell types, such
as epithelial cells, vesicular trafficking plays and important role in
the maintenance of cell surface polarity that is essential for vectorial
transport and secretory functions. Furthermore, the regulation of certain
membrane trafficking events, for example those underlying the regulated
secretion of neurotransmitter at the synapse, play important roles in
intercellular communication. The long-term objective of the proposed
research is an understanding of the molecular mechanisms responsible for
these intracellular membrane trafficking events. Such an understanding
will ultimately provide insight into a wide variety of cellular
processes. The strategy to be employed in approaching this objective is
the biochemical and functional characterization of a family of proteins,
the syntaxins, that have been proposed to act as receptors for
intracellular membrane transport vesicles. Particular emphasis will be
focused on the role of syntaxin 1 in synaptic vesicle docking and fusion.
The proposed research will address the following specific aims:
1. Biochemical characterization of the interaction between membrane of
the syntaxin family and other specific components of the intracellular
membrane trafficking machinery.
2. Identification of the signal(s) within the syntaxins responsible for
localization to different intracellular membrane compartments.
3. Functional characterization of the role of syntaxins in constitutive
and regulated secretion from PC12 cells.
No Sub Projects information available for 5R01GM051313-04
Publications
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