Transformation-specific interaction of the bovine papillomavirus E5 oncoprotein with the platelet-derived growth factor receptor transmembrane domain and the epidermal growth factor receptor cytoplasmic domain.

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J Virol. 1993 September; 67(9): 5303-5311

Transformation-specific interaction of the bovine papillomavirus E5 oncoprotein with the platelet-derived growth factor receptor transmembrane domain and the epidermal growth factor receptor cytoplasmic domain.

B D Cohen, D J Goldstein, L Rutledge, W C Vass, D R Lowy, R Schlegel and J T Schiller

Laboratory of Cellular Oncology, National Cancer Institute, Bethesda, Maryland 20892.

ABSTRACT

The bovine papillomavirus E5 transforming protein appears toactivate both the epidermal growth factor receptor (EGF-R) andthe platelet-derived growth factor receptor (PDGF-R) by a ligand-independentmechanism. To further investigate the ability of E5 to activatereceptors of different classes and to determine whether thisstimulation occurs through the extracellular domain requiredfor ligand activation, we constructed chimeric genes encodingPDGF-R and EGF-R by interchanging the extracellular, membrane,and cytoplasmic coding domains. Chimeras were transfected intoNIH 3T3 and CHO(LR73) cells. All chimeras expressed stable proteinwhich, upon addition of the appropriate ligand, could be activatedas assayed by tyrosine autophosphorylation and biological transformation.Cotransfection of E5 with the wild-type and chimeric receptorsresulted in the ligand-independent activation of receptors,provided that a receptor contained either the transmembranedomain of the PDGF-R or the cytoplasmic domain of the EGF-R.Chimeric receptors that contained both of these domains exhibitedthe highest level of E5-induced biochemical and biological stimulation.These results imply that E5 activates the PDGF-R and EGR-R bytwo distinct mechanisms, neither of which specifically involvesthe extracellular domain of the receptor. Consistent with thebiochemical and biological activation data, coimmunoprecipitationstudies demonstrated that E5 formed a complex with any chimerathat contained a PDGF-R transmembrane domain or an EGF-R cytoplasmicdomain, with those chimeras containing both domains demonstratingthe greatest efficiency of complex formation. These resultssuggest that although different domains of the PDGF-R and EGF-Rare required for E5 activation, both receptors are activateddirectly by formation of an E5-containing complex.

J Virol. 1993 September; 67(9): 5303-5311

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