Neuroprotection and Neuronal Differentiation Studies Using Substantia Nigra Dopaminergic Cells Derived from Transgenic Mouse Embryos

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The Journal of Neuroscience, January 1, 1999, 19(1):10-20

Neuroprotection and Neuronal Differentiation Studies Using Substantia Nigra Dopaminergic Cells Derived from Transgenic Mouse Embryos
Jin H. Son, Hong S. Chun, Tong H. Joh, Sunghee Cho, Bruno Conti, and Jong W. Lee
Department of Neurology and Neuroscience, Cornell University Medical College and Laboratory of Molecular Neurobiology, The W. M. Burke Medical Research Institute, White Plains, New York 10605
The major pathological lesion of Parkinson's disease (PD) is the selective cell death of dopaminergic (DA) neurons in substantianigra (SN). Although the initial cause and subsequent molecularsignaling mechanisms leading to DA cell death underlying the PDprocess remain elusive, brain-derived neurotrophic factor (BDNF)is thought to exert neuroprotective as well as neurotrophic rolesfor the survival and differentiation of DA neurons in SN. Addressingmolecular mechanisms of BDNF action in both primary embryonicmesencephalic cultures and in vivo animal models has been technicallydifficult because DA neurons in SN are relatively rare and presentwith many heterogeneous cell populations in midbrain. We havedeveloped and characterized a DA neuronal cell line of embryonicSN origin that is more accessible to molecular analysis and canbe used as an in vitro model system for studying SN DA neurons.A clonal SN DA neuronal progenitor cell line SN4741, arrestedat an early DA developmental stage, was established from transgenicmouse embryos containing the targeted expression of the thermolabileSV40Tag in SN DA neurons. The phenotypic and morphological differentiationof the SN4741 cells could be manipulated by environmental cuesin vitro. Exogenous BDNF treatment produced significant neuroprotectionagainst 1-methyl-4-phenylpyridinium, glutamate, and nitric oxide-inducedneurotoxicity in the SN4741 cells. Simultaneous phosphorylationof receptor tyrosine kinase B accompanied the neuroprotection.This SN DA neuronal cell line provides a unique model system tocircumvent the limitations associated with primary mesencephaliccultures for the elucidation of molecular mechanisms of BDNF actionon DA neurons of theSN.

Key words: neuroprotection; BDNF; substantia nigra; dopaminergic neuron; Parkinson's disease; transgenic mice; neuronal differentiation; conditional immortalization
Copyright © 1999 Society for Neuroscience 0270-6474/99/19110-11$05.00/0

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