Abstract

Our goals are to understand the role(s) of neurotrophins in (i) central nervous system (CNS) neuronal survival, (ii) neuronal differentiation, and (iii) protection against neuronal damage. Neurotrophins are a four-member family of structurally related proteins; Nerve Growth Factor (NGF), Brain Derived Neurotrophic Factor (BDNF), Neurotrophin-3 (NT-3) and Neurotrophin-4 (NT-4). BDNF, NT-3 and NT-4 are potent survival factors for many types of CNS neurons. We derived mice carrying null mutations in individual as well as in two or three neurotrophin genes; e.g., NT-4-/- mice, [BDNF-/-, NT-4-/-] mice, [BDNF-/-, NT-3-/-, NT-4-/-] mice, etc. Using these mice, we can ask questions about neuronal survival and differentiation in vivo that could not previously be posed. We will investigate neurotrophin-dependence for CNS neuronal survival, neuronal differentiation in the hippocampus, and neuronal response to ischemia.
Our first aim i s to determine whether neurotrophins are essential for the survival of hippocampal neurons during embryonic and postnatal development. Previous studies and our preliminary results suggest that multiple/alternative neurotrophins can deliver the signal for CNS neurons to survive and CNS neurons may depend on neurotrophins to survive during postnatal development. To test these hypotheses, NT-4-/- and [BDNF-/-, NT-3-/-, NT-4-/-] mice will be examined histologically and immunohistologically to determine (i) whether there is excessive CNS neuronal death during (i) embryogenesis, and (ii) postnatal development.
Our second aim i s to define neurotrophin function in regulating neurite outgrowth in the hippocampus during postnatal development. (i) [BDNF-/-, NT-3-/-, NT-4-/-] mice will be used to determine whether neurotrophins control neurite outgrowth. (ii) mice carrying null mutations in individual neurotrophin genes will be used to determine the specificity of each neurotrophin in neurite outgrowth. (iii) physical exercise will be applied to NT-4-/- and wild type mice to determine whether NT-4 mediate activity-dependent neurite outgrowth. (iv) exogenous NT-4 will be used to rescue the potential abnormal neurite outgrowth.
Our third aim i s to determine whether neurotrophins play a role(s) in protecting the adult nervous system against injury. Our preliminary results showed that NT-4-/- mice have an increased neuronal loss in ischemia. (i) NT-4 and BDNF expression during ischemia will be examined. (ii) exogenous NT-4 and BDNF will be tested for protective effects in our ischemic model. In vitro experiments suggest that neurotrophins modulate CNS neuronal survival and differentiation. Our neurotrophin knockout mice allow us to determine the roles of the various neurotrophins in vivo.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS038489-04
Application #
6694042
Study Section
Special Emphasis Panel (ZRG1-MDCN-6 (01))
Program Officer
Mamounas, Laura
Project Start
2001-01-18
Project End
2005-12-31
Budget Start
2004-01-01
Budget End
2005-12-31
Support Year
4
Fiscal Year
2004
Total Cost
$265,076
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Pathology
Type
Schools of Medicine
DUNS #
092530369
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Matter, Cheryl; Pribadi, Mochtar; Liu, Xin et al. (2009) Delta-catenin is required for the maintenance of neural structure and function in mature cortex in vivo. Neuron 64:320-7
Israely, Inbal; Costa, Rui M; Xie, Cui Wei et al. (2004) Deletion of the neuron-specific protein delta-catenin leads to severe cognitive and synaptic dysfunction. Curr Biol 14:1657-63
Tan, Miao; Groszer, Matthias; Tan, Aiko M et al. (2003) Phosphoinositide 3-kinase cascade facilitates mu-opioid desensitization in sensory neurons by altering G-protein-effector interactions. J Neurosci 23:10292-301
Smith, Desmond J; Leil, Tarek A; Liu, Xin (2003) Neurotrophin-4 is required for tolerance to morphine in the mouse. Neurosci Lett 340:103-6
Lesche, Ralf; Groszer, Matthias; Gao, Jing et al. (2002) Cre/loxP-mediated inactivation of the murine Pten tumor suppressor gene. Genesis 32:148-9
Li, Gang; Robinson, Gertraud W; Lesche, Ralf et al. (2002) Conditional loss of PTEN leads to precocious development and neoplasia in the mammary gland. Development 129:4159-70
Groszer, M; Erickson, R; Scripture-Adams, D D et al. (2001) Negative regulation of neural stem/progenitor cell proliferation by the Pten tumor suppressor gene in vivo. Science 294:2186-9