Pirh2, a p53-induced ubiquitin-protein ligase, promotes p53 degradation

Roger P. Leng; Yunping Lin; Weili Ma; Hong Wu; Benedicte Lemmers; Stephen Chung; John M. Parant; Guillermina Lozano; Razqallah Hakem; Samuel Benchimol

doi:10.1016/S0092-8674(03)00193-4

Pirh2, a p53-induced ubiquitin-protein ligase, promotes p53 degradation

Roger P. Leng, Yunping Lin, Weili Ma, Hong Wu, Benedicte Lemmers, Stephen Chung, John M. Parant, Guillermina Lozano, Razqallah Hakem, Samuel Benchimol

Genetics

Research output: Contribution to journal › Article › peer-review

619 Scopus citations

Abstract

The p53 tumor suppressor exerts anti-proliferative effects in response to various types of stress including DNA damage and abnormal proliferative signals. Tight regulation of p53 is essential for maintaining normal cell growth and this occurs primarily through posttranslational modifications of p53. Here, we describe Pirh2, a gene regulated by p53 that encodes a RING-H2 domain-containing protein with intrinsic ubiquitin-protein ligase activity. Pirh2 physically interacts with p53 and promotes ubiquitination of p53 independently of Mdm2. Expression of Pirh2 decreases the level of p53 protein and abrogation of endogenous Pirh2 expression increases the level of p53. Furthermore, Pirh2 represses p53 functions including p53-dependent transactivation and growth inhibition. We propose that Pirh2 is involved in the negative regulation of p53 function through physical interaction and ubiquitin-mediated proteolysis. Hence, Pirh2, like Mdm2, participates in an autoregulatory feedback loop that controls p53 function.

Original language	English (US)
Pages (from-to)	779-791
Number of pages	13
Journal	Cell
Volume	112
Issue number	6
DOIs	https://doi.org/10.1016/S0092-8674(03)00193-4
State	Published - Mar 21 2003

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/S0092-8674(03)00193-4

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title = "Pirh2, a p53-induced ubiquitin-protein ligase, promotes p53 degradation",

abstract = "The p53 tumor suppressor exerts anti-proliferative effects in response to various types of stress including DNA damage and abnormal proliferative signals. Tight regulation of p53 is essential for maintaining normal cell growth and this occurs primarily through posttranslational modifications of p53. Here, we describe Pirh2, a gene regulated by p53 that encodes a RING-H2 domain-containing protein with intrinsic ubiquitin-protein ligase activity. Pirh2 physically interacts with p53 and promotes ubiquitination of p53 independently of Mdm2. Expression of Pirh2 decreases the level of p53 protein and abrogation of endogenous Pirh2 expression increases the level of p53. Furthermore, Pirh2 represses p53 functions including p53-dependent transactivation and growth inhibition. We propose that Pirh2 is involved in the negative regulation of p53 function through physical interaction and ubiquitin-mediated proteolysis. Hence, Pirh2, like Mdm2, participates in an autoregulatory feedback loop that controls p53 function.",

author = "Leng, {Roger P.} and Yunping Lin and Weili Ma and Hong Wu and Benedicte Lemmers and Stephen Chung and Parant, {John M.} and Guillermina Lozano and Razqallah Hakem and Samuel Benchimol",

note = "Funding Information: We thank C. Arrowsmith and A. Ayed for providing us with bacterial expression vectors encoding truncated p53 mutants; J. Manfredi for the p21-luciferase reporter construct; M. Oren for the p53DD plasmid; H. Vaziri for the BJT/DD cells; and M. Tyers for advice in setting up the in vitro ubiquitination assay. We thank our colleagues in the Benchimol laboratory for useful and critical discussions. This work was supported by the National Cancer Institute of Canada with funds from the Canadian Cancer Society and by the Canadian Institutes of Health Research. R.P.L. was supported initially by an Amgen Fellowship Award and is currently supported by a Fellowship Award from the Canadian Institutes of Health Research. ",

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AU - Leng, Roger P.

AU - Lin, Yunping

AU - Ma, Weili

AU - Wu, Hong

AU - Lemmers, Benedicte

AU - Chung, Stephen

AU - Parant, John M.

AU - Lozano, Guillermina

AU - Hakem, Razqallah

AU - Benchimol, Samuel

N1 - Funding Information: We thank C. Arrowsmith and A. Ayed for providing us with bacterial expression vectors encoding truncated p53 mutants; J. Manfredi for the p21-luciferase reporter construct; M. Oren for the p53DD plasmid; H. Vaziri for the BJT/DD cells; and M. Tyers for advice in setting up the in vitro ubiquitination assay. We thank our colleagues in the Benchimol laboratory for useful and critical discussions. This work was supported by the National Cancer Institute of Canada with funds from the Canadian Cancer Society and by the Canadian Institutes of Health Research. R.P.L. was supported initially by an Amgen Fellowship Award and is currently supported by a Fellowship Award from the Canadian Institutes of Health Research.

PY - 2003/3/21

Y1 - 2003/3/21

N2 - The p53 tumor suppressor exerts anti-proliferative effects in response to various types of stress including DNA damage and abnormal proliferative signals. Tight regulation of p53 is essential for maintaining normal cell growth and this occurs primarily through posttranslational modifications of p53. Here, we describe Pirh2, a gene regulated by p53 that encodes a RING-H2 domain-containing protein with intrinsic ubiquitin-protein ligase activity. Pirh2 physically interacts with p53 and promotes ubiquitination of p53 independently of Mdm2. Expression of Pirh2 decreases the level of p53 protein and abrogation of endogenous Pirh2 expression increases the level of p53. Furthermore, Pirh2 represses p53 functions including p53-dependent transactivation and growth inhibition. We propose that Pirh2 is involved in the negative regulation of p53 function through physical interaction and ubiquitin-mediated proteolysis. Hence, Pirh2, like Mdm2, participates in an autoregulatory feedback loop that controls p53 function.

AB - The p53 tumor suppressor exerts anti-proliferative effects in response to various types of stress including DNA damage and abnormal proliferative signals. Tight regulation of p53 is essential for maintaining normal cell growth and this occurs primarily through posttranslational modifications of p53. Here, we describe Pirh2, a gene regulated by p53 that encodes a RING-H2 domain-containing protein with intrinsic ubiquitin-protein ligase activity. Pirh2 physically interacts with p53 and promotes ubiquitination of p53 independently of Mdm2. Expression of Pirh2 decreases the level of p53 protein and abrogation of endogenous Pirh2 expression increases the level of p53. Furthermore, Pirh2 represses p53 functions including p53-dependent transactivation and growth inhibition. We propose that Pirh2 is involved in the negative regulation of p53 function through physical interaction and ubiquitin-mediated proteolysis. Hence, Pirh2, like Mdm2, participates in an autoregulatory feedback loop that controls p53 function.

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Pirh2, a p53-induced ubiquitin-protein ligase, promotes p53 degradation

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