Homeostatic regulation of the proteasome via an Rpn4-dependent feedback circuit

Donghong Ju; Li Wang; Xicheng Mao; Youming Xie

doi:10.1016/j.bbrc.2004.06.105

Homeostatic regulation of the proteasome via an Rpn4-dependent feedback circuit

Donghong Ju, Li Wang, Xicheng Mao, Youming Xie

Internal Medicine

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

67 Scopus citations

Abstract

The 26S proteasome is a complex protease consisting of at least 32 different subunits. Early studies showed that Rpn4 (also named Son1 and Ufd5) is a transcriptional activator of the Saccharomyces cerevisiae proteasome genes, and that Rpn4 is rapidly degraded by the 26S proteasome. These observations suggested that in vivo proteasome abundance may be regulated by an Rpn4-dependent feedback circuit. Here, we present direct evidence to support the Rpn4-proteasome feedback model. We show that proteasome expression is increased when proteasome activity is impaired, and that this increase is Rpn4-dependent. Moreover, we demonstrate that expression of a stable form of Rpn4 leads to elevation of proteasome expression. Our data also reveal that the Rpn4-proteasome feedback circuit is critical for cell growth when proteasome activity is compromised, and plays an important role in response to DNA damage. This study provides important insights into the mechanism underlying proteasome homeostasis.

Original language	English (US)
Pages (from-to)	51-57
Number of pages	7
Journal	Biochemical and Biophysical Research Communications
Volume	321
Issue number	1
DOIs	https://doi.org/10.1016/j.bbrc.2004.06.105
State	Published - Aug 13 2004

Keywords

DNA damage
Feedback regulation
Gene transcription
Proteasome
Proteolysis
Rpn4
Ubiquitin

ASJC Scopus subject areas

Biophysics
Biochemistry
Molecular Biology
Cell Biology

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10.1016/j.bbrc.2004.06.105

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title = "Homeostatic regulation of the proteasome via an Rpn4-dependent feedback circuit",

abstract = "The 26S proteasome is a complex protease consisting of at least 32 different subunits. Early studies showed that Rpn4 (also named Son1 and Ufd5) is a transcriptional activator of the Saccharomyces cerevisiae proteasome genes, and that Rpn4 is rapidly degraded by the 26S proteasome. These observations suggested that in vivo proteasome abundance may be regulated by an Rpn4-dependent feedback circuit. Here, we present direct evidence to support the Rpn4-proteasome feedback model. We show that proteasome expression is increased when proteasome activity is impaired, and that this increase is Rpn4-dependent. Moreover, we demonstrate that expression of a stable form of Rpn4 leads to elevation of proteasome expression. Our data also reveal that the Rpn4-proteasome feedback circuit is critical for cell growth when proteasome activity is compromised, and plays an important role in response to DNA damage. This study provides important insights into the mechanism underlying proteasome homeostasis.",

keywords = "DNA damage, Feedback regulation, Gene transcription, Proteasome, Proteolysis, Rpn4, Ubiquitin",

author = "Donghong Ju and Li Wang and Xicheng Mao and Youming Xie",

note = "Funding Information: We are grateful to J{\"u}rgen Dohmen, Erica Johnson, Alex Varshavsky, and George Brush for strains and anti-tubulin antibody. We thank George Brush, Michael Tainsky, and Robert Pauley for comments on the manuscript. This study was supported by a grant to Y.X. from Barbara Ann Karmanos Cancer Institute, Wayne State University. Li Wang is a visiting scholar from East China Normal University and a grant from NIEHS (ES06639). Copyright: Copyright 2012 Elsevier B.V., All rights reserved.",

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AU - Ju, Donghong

AU - Wang, Li

AU - Mao, Xicheng

AU - Xie, Youming

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PY - 2004/8/13

Y1 - 2004/8/13

N2 - The 26S proteasome is a complex protease consisting of at least 32 different subunits. Early studies showed that Rpn4 (also named Son1 and Ufd5) is a transcriptional activator of the Saccharomyces cerevisiae proteasome genes, and that Rpn4 is rapidly degraded by the 26S proteasome. These observations suggested that in vivo proteasome abundance may be regulated by an Rpn4-dependent feedback circuit. Here, we present direct evidence to support the Rpn4-proteasome feedback model. We show that proteasome expression is increased when proteasome activity is impaired, and that this increase is Rpn4-dependent. Moreover, we demonstrate that expression of a stable form of Rpn4 leads to elevation of proteasome expression. Our data also reveal that the Rpn4-proteasome feedback circuit is critical for cell growth when proteasome activity is compromised, and plays an important role in response to DNA damage. This study provides important insights into the mechanism underlying proteasome homeostasis.

AB - The 26S proteasome is a complex protease consisting of at least 32 different subunits. Early studies showed that Rpn4 (also named Son1 and Ufd5) is a transcriptional activator of the Saccharomyces cerevisiae proteasome genes, and that Rpn4 is rapidly degraded by the 26S proteasome. These observations suggested that in vivo proteasome abundance may be regulated by an Rpn4-dependent feedback circuit. Here, we present direct evidence to support the Rpn4-proteasome feedback model. We show that proteasome expression is increased when proteasome activity is impaired, and that this increase is Rpn4-dependent. Moreover, we demonstrate that expression of a stable form of Rpn4 leads to elevation of proteasome expression. Our data also reveal that the Rpn4-proteasome feedback circuit is critical for cell growth when proteasome activity is compromised, and plays an important role in response to DNA damage. This study provides important insights into the mechanism underlying proteasome homeostasis.

KW - DNA damage

KW - Feedback regulation

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KW - Proteasome

KW - Proteolysis

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KW - Ubiquitin

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Homeostatic regulation of the proteasome via an Rpn4-dependent feedback circuit

Abstract

Keywords

ASJC Scopus subject areas

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