Human DNA-activated protein kinase phosphorylates serines 15 and 37 in the amino-terminal transactivation domain of human p53.

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Mol Cell Biol. 1992 November; 12(11): 5041-5049

Human DNA-activated protein kinase phosphorylates serines 15 and 37 in the amino-terminal transactivation domain of human p53.

S P Lees-Miller, K Sakaguchi, S J Ullrich, E Appella and C W Anderson

Biology Department, Brookhaven National Laboratory, Upton, New York 11973.

ABSTRACT

Human DNA-PK is a nuclear, serine/threonine protein kinase that,when activated by DNA, phosphorylates several DNA-binding substrates,including the tumor suppressor protein p53. To identify whichp53 residues are phosphorylated, we examined DNA-PK's abilityto phosphorylate synthetic peptides corresponding to human p53sequences. Serines 15 and 37 in the amino-terminal transactivationdomain of human p53, and serines 7 and 18 of mouse p53, werephosphorylated by DNA-PK in the context of synthetic peptides.Other serines in these p53 peptides, and serines in other p53peptides, including peptides containing the serine 315 p34cdc2site and the serine 392 casein kinase II site, were not recognizedby DNA-PK or were phosphorylated less efficiently. Phosphorylationof the conserved serine 15 in human p53 peptides depended onthe presence of an adjacent glutamine, and phosphorylation wasinhibited by the presence of a nearby lysine. Phosphorylationof recombinant wild-type mouse p53 was inhibited at high DNAconcentrations, suggesting that DNA-PK may phosphorylate p53only when both are bound to DNA at nearby sites. Our study suggeststhat DNA-PK may have a role in regulating cell growth and indicateshow phosphorylation of serine 15 in DNA-bound p53 could alterp53 function.

Mol Cell Biol. 1992 November; 12(11): 5041-5049

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