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Article

Regulation of p53 Localization and Activity by Ubc13

, , , , &
Pages 8901-8913 | Received 27 Jun 2006, Accepted 15 Sep 2006, Published online: 27 Mar 2023
 

Abstract

The abundance and activity of p53 are regulated largely by ubiquitin ligases. Here we demonstrate a previously undisclosed regulation of p53 localization and activity by Ubc13, an E2 ubiquitin-conjugating enzyme. While increasing p53 stability, Ubc13 decreases p53 transcriptional activity and increases its localization to the cytoplasm, changes that require its ubiquitin-conjugating activity. Ubc13 elicits K63-dependent ubiquitination of p53, which attenuates Hdm2-induced polyubiquitination of p53. Ubc13 association with p53 requires an intact C-terminal domain of p53 and is markedly stronger with a p53 mutant that cannot tetramerize. Expression of Ubc13 in vivo increases the pool of monomeric p53, indicating that Ubc13 affects tetramerization of p53. Significantly, wild-type but not mutant Ubc13 is associated with polysomes and enriches p53 within this fraction. In response to DNA damage, Ubc13 is no longer capable of facilitating p53 monomerization, in part due to a decrease in its own levels which is p53 dependent. Our findings point to a newly discerned mechanism important in the regulation of p53 organization, localization, and activity by Ubc13.

Supplemental material for this article may be found at http://mcb.asm.org/.

We thank S. N. Jones, C. Pickart, J. Manfredi, B. Vogelstein, and Z. J. Chen for providing plasmids and cell lines and J. Manfredi, Z. Q. Pan, M. O'Connell, H. Habelhah, A. Bhoumik, Kate Welsh, and the other members of the Ronai lab for their assistance and constructive comments. A. Laine is part of the M.D./Ph.D. Program at Mount Sinai School of Medicine, New York.

This work was supported by NIH grants CA78419 (to Z.R.) and CA69381 (to J.C.R.).

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