Identification of an intracellular protein that specifically interacts with photoaffinity-labeled oncogenic p21 protein

G. Lee, Z. A. Ronai, M. R. Pincus, P. W. Brandt-Rauf, R. B. Murphy, T. M. Delohery, S. Nishimura, Z. Yamaizumi, I. B. Weinstein

Résultat de rechercheexamen par les pairs

16 Citations (Scopus)

Résumé

An oncogenic 21-kDa (p21) protein (Harvey RAS protein with Val12) has been covalently modified with a functional reagent that contains a photoactivatable aromatic azide group. This modified p21 protein has been introduced quantitatively into NIH 3T3 cells using an erythrocyte-mediated fusion technique. The introduced p21 protein was capable of inducing enhanced pinocytosis and DNA synthesis in the recipient cells. To identify the putative intracellular protein(s) that specifically interact with the modified p21 protein, the cells were pulsed with [35S]methionine at selected times after fusion and then UV-irradiated to activate the azide group. The resulting nitrene covalently binds to amino acid residues in adjacent proteins, thus linking the p21 protein to these proteins. The cells were then lysed, and the lysate was immunoprecipitated with the anti-p21 monoclonal antibody Y13-259. The immunoprecipitate was analyzed by SDS/PAGE to identify p21-protein complexes. By using this technique, we found that three protein complexes of 51, 64, and 82 kDa were labeled specifically and reproducibly. The most prominent band is the 64-kDa protein complex that shows a time-dependent rise and fall, peaking within a 5-hr period after introduction of the p21 protein into the cells. These studies provide evidence that in vitro the p21 protein becomes associated with a protein whose mass is about 43 kDa. We suggest that the formation of this complex may play a role in mediating early events involved with cell transformation induced by RAS oncogenes.

Langue d'origineEnglish
Pages (de-à)8678-8682
Nombre de pages5
JournalProceedings of the National Academy of Sciences of the United States of America
Volume86
Numéro de publication22
DOI
Statut de publicationPublished - 1989

Financement

Bailleurs de fondsNuméro du bailleur de fonds
National Cancer InstituteR01CA042500

    ASJC Scopus Subject Areas

    • General

    Empreinte numérique

    Plonger dans les sujets de recherche 'Identification of an intracellular protein that specifically interacts with photoaffinity-labeled oncogenic p21 protein'. Ensemble, ils forment une empreinte numérique unique.

    Citer