Homologous sequences in adenovirus E1A and human papillomavirus E7 proteins mediate interaction with the same set of cellular proteins.

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J Virol. 1992 December; 66(12): 6893-6902

Homologous sequences in adenovirus E1A and human papillomavirus E7 proteins mediate interaction with the same set of cellular proteins.

N Dyson, P Guida, K Münger and E Harlow

Massachusetts General Hospital Cancer Center, Charlestown 02129.

ABSTRACT

Studies of adenovirus E1A oncoprotein mutants suggest that theassociation of E1A with the retinoblastoma protein (pRB) isnecessary for E1A-mediated transformation. Mutational analysisof E1A indicates that two regions of pRB are required for E1Ato form stable complexes with the retinoblastoma protein. Inaddition to pRB binding, these regions are necessary for E1Aassociation with several other cellular proteins, includingp130, p107, cyclin A, and p33cdk2. Here we show that short syntheticpeptides containing the pRB-binding sequences of E1A are sufficientfor interaction with p107, cyclin A, and p130. The E7 proteinof human papillomavirus type 16 contains an element that bindsto pRB and appears to be functionally homologous to the E1Asequences. Peptides containing this region of the E7 proteinwere able to interact with p107, cyclin A, and p130 in additionto pRB. These findings suggest that the common mechanism oftransformation used by these viral oncogenes involves theirassociation with a set of polypeptides.

J Virol. 1992 December; 66(12): 6893-6902

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