Abstract

Intracellular transport by molecular motor proteins is essential for many neuronal and other cellular processes. These processes appear to include positioning organelles and organizing secretion, as well as neuronal signaling, damage responses, and processes that fail in neurodegenerative and other diseases. Our focus is on kinesins, which generate directed movements along microtubules in many cellular contexts including mitosis, vesicle traffic, and axonal transport. Considerable work from our laboratory and others has provided much information about the basic properties of these systems, but has left unanswered several important questions, two of which we will attack in the coming funding period: 1) What is the logic of kinesin motor utilization? 2) How are kinesin motors regulated and attached to intracellular cargoes? To answer these questions, we propose to focus primarily on conventional kinesin, kinesin-I. Tactically, we use both mice and Drosophila because of their unique and complementary features. To achieve our goals, we will attack three specific aims in the next project period. Specifically, we propose: 1) To test the hypothesis that neuron specific forms of kinesin-I carry out neuron-specific functions such as slow and fast axonal transport of neuron-specific cargoes, while ubiquitous forms carry out the same general functions in both neural and non-neural cells. Null and conditional knockout mutants in the three kinesin heavy chain (KIF5A, KIF5B, and KIF5C), and the two major kinesin light chain (KLC1 and KLC2) genes in the mouse will be generated and analyzed using the Iox-cre system. We will focus on a few representative cell types including cultured embryonic fibroblasts, hepatocytes, photoreceptors, motor neurons, sensory neurons, and cultured hippocampal neurons. In addition, we will test the related hypothesis that kinesin-I plays a major role in the slow axonal transport of neurofilaments. 2) To test the hypothesis that kinesin light chain (KLC) is required for both cargo-attachment and regulation of kinesin-I. This hypothesis will be tested by analyzing the biochemical and cellular phenotype of mouse mutants lacking defined KLC subunits. 3) To elucidate the structure and function of two different proposed kinesin-I vesicular attachment complexes. We will determine the composition and role in kinesin-I transport of components of the syd/JIP-3 and the amyloid precursor protein complexes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM035252-22
Application #
6919879
Study Section
Cell Development and Function Integrated Review Group (CDF)
Program Officer
Deatherage, James F
Project Start
1994-01-01
Project End
2007-07-31
Budget Start
2005-08-01
Budget End
2006-07-31
Support Year
22
Fiscal Year
2005
Total Cost
$396,760
Indirect Cost

  Institution

Name
University of California San Diego
Department
Other Basic Sciences
Type
Schools of Medicine
DUNS #
804355790
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Gunawardena, Shermali; Yang, Ge; Goldstein, Lawrence S B (2013) Presenilin controls kinesin-1 and dynein function during APP-vesicle transport in vivo. Hum Mol Genet 22:3828-43
Reis, Gerald F; Yang, Ge; Szpankowski, Lukasz et al. (2012) Molecular motor function in axonal transport in vivo probed by genetic and computational analysis in Drosophila. Mol Biol Cell 23:1700-14
Falzone, Tomás L; Gunawardena, Shermali; McCleary, David et al. (2010) Kinesin-1 transport reductions enhance human tau hyperphosphorylation, aggregation and neurodegeneration in animal models of tauopathies. Hum Mol Genet 19:4399-408
Abe, Namiko; Almenar-Queralt, Angels; Lillo, Concepcion et al. (2009) Sunday driver interacts with two distinct classes of axonal organelles. J Biol Chem 284:34628-39
Shah, Sameer B; Nolan, Rhiannon; Davis, Emily et al. (2009) Examination of potential mechanisms of amyloid-induced defects in neuronal transport. Neurobiol Dis 36:11-25
Falzone, Tomás L; Stokin, Gorazd B; Lillo, Concepción et al. (2009) Axonal stress kinase activation and tau misbehavior induced by kinesin-1 transport defects. J Neurosci 29:5758-67
Stokin, Gorazd B; Almenar-Queralt, Angels; Gunawardena, Shermali et al. (2008) Amyloid precursor protein-induced axonopathies are independent of amyloid-beta peptides. Hum Mol Genet 17:3474-86
Xia, Chun-Hong; Roberts, Elizabeth A; Her, Lu-Shiun et al. (2003) Abnormal neurofilament transport caused by targeted disruption of neuronal kinesin heavy chain KIF5A. J Cell Biol 161:55-66
Gunawardena, Shermali; Her, Lu-Shiun; Brusch, Richard G et al. (2003) Disruption of axonal transport by loss of huntingtin or expression of pathogenic polyQ proteins in Drosophila. Neuron 40:25-40
Ji, Jun-Yuan; Haghnia, Marjan; Trusty, Cory et al. (2002) A genetic screen for suppressors and enhancers of the Drosophila cdk1-cyclin B identifies maternal factors that regulate microtubule and microfilament stability. Genetics 162:1179-95

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