SNT, a differentiation-specific target of neurotrophic factor-induced tyrosine kinase activity in neurons and PC12 cells.

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Mol Cell Biol. 1993 April; 13(4): 2203-2213

SNT, a differentiation-specific target of neurotrophic factor-induced tyrosine kinase activity in neurons and PC12 cells.

S J Rabin, V Cleghon and D R Kaplan

Eukaryotic Signal Transduction Group, National Cancer Institute-Frederick Cancer Research and Development Center, Maryland 21702-1201.

ABSTRACT

To elucidate the signal transduction mechanisms used by ligandsthat induce differentiation and the cessation of cell division,we utilized p13suc1-agarose, a reagent that binds p34cdc2/cdk2.By using this reagent, we identified a 78- to 90-kDa speciesin PC12 pheochromocytoma cells that is rapidly phosphorylatedon tyrosine following treatment with the differentiation factorsnerve growth factor (NGF) and fibroblast growth factor but notby the mitogens epidermal growth factor or insulin. This species,called SNT (suc-associated neurotrophic factor-induced tyrosine-phosphorylatedtarget), was also phosphorylated on tyrosine in primary ratcortical neurons treated with the neurotrophic factors neurotrophin-3,brain-derived neurotrophic factor, and fibroblast growth factorbut not in those treated with epidermal growth factor. In neuronaland fibroblast cells, where NGF can also act as a mitogen, SNTwas tyrosine phosphorylated to a much greater extent duringNGF-induced differentiation than during NGF-induced proliferation.SNT was phosphorylated in vitro on serine, threonine, and tyrosinein p13suc1-agarose precipitates from NGF-treated PC12 cells,indicating that this protein may be a substrate of kinase activitiesassociated with p13suc1-p34cdc2/cdk2 complexes. In addition,SNT was associated predominantly with nuclear fractions followingsubcellular fractionation of NGF-treated PC12 cells. Finally,in PC12 cells, NGF-stimulated tyrosine phosphorylation of SNTwas dependent on the levels of Trk tyrosine kinase activityand was constitutively induced by expression of pp60v-src. However,Ras was not required for constitutive SNT tyrosine phosphorylation,suggesting that this protein functions distally to Trk and pp60v-srcbut in a pathway parallel to that of Ras. SNT is the first identifiedspecific target of differentiation factor-induced tyrosine kinaseactivity in neuronal cells.

Mol Cell Biol. 1993 April; 13(4): 2203-2213

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