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Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development

Rpn13 is a novel mammalian proteasomal receptor that has recently been identified as an amplification target in ovarian cancer. It can interact with ubiquitin and activate the deubiquitinating enzyme Uch37 at the 26S proteasome. Since neither Rpn13 nor Uch37 is an integral proteasomal subunit, we ex...

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Autores principales: Al-Shami, Amin, Jhaver, Kanchan G., Vogel, Peter, Wilkins, Carrie, Humphries, Juliane, Davis, John J., Xu, Nianhua, Potter, David G., Gerhardt, Brenda, Mullinax, Robert, Shirley, Cynthia R., Anderson, Stephen J., Oravecz, Tamas
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2965108/
https://www.ncbi.nlm.nih.gov/pubmed/21048919
http://dx.doi.org/10.1371/journal.pone.0013654
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author Al-Shami, Amin
Jhaver, Kanchan G.
Vogel, Peter
Wilkins, Carrie
Humphries, Juliane
Davis, John J.
Xu, Nianhua
Potter, David G.
Gerhardt, Brenda
Mullinax, Robert
Shirley, Cynthia R.
Anderson, Stephen J.
Oravecz, Tamas
author_facet Al-Shami, Amin
Jhaver, Kanchan G.
Vogel, Peter
Wilkins, Carrie
Humphries, Juliane
Davis, John J.
Xu, Nianhua
Potter, David G.
Gerhardt, Brenda
Mullinax, Robert
Shirley, Cynthia R.
Anderson, Stephen J.
Oravecz, Tamas
author_sort Al-Shami, Amin
collection PubMed
description Rpn13 is a novel mammalian proteasomal receptor that has recently been identified as an amplification target in ovarian cancer. It can interact with ubiquitin and activate the deubiquitinating enzyme Uch37 at the 26S proteasome. Since neither Rpn13 nor Uch37 is an integral proteasomal subunit, we explored whether either protein is essential for mammalian development and survival. Deletion of Uch37 resulted in prenatal lethality in mice associated with severe defect in embryonic brain development. In contrast, the majority of Rpn13-deficient mice survived to adulthood, although they were smaller at birth and fewer in number than wild-type littermates. Absence of Rpn13 produced tissue-specific effects on proteasomal function: increased proteasome activity in adrenal gland and lymphoid organs, and decreased activity in testes and brain. Adult Rpn13(−/−) mice reached normal body weight but had increased body fat content and were infertile due to defective gametogenesis. Additionally, Rpn13(−/−) mice showed increased T-cell numbers, resembling growth hormone-mediated effects. Indeed, serum growth hormone and follicular stimulating hormone levels were significantly increased in Rpn13(−/−) mice, while growth hormone receptor expression was reduced in the testes. In conclusion, this is the first report characterizing the physiological roles of Uch37 and Rpn13 in murine development and implicating a non-ATPase proteasomal protein, Rpn13, in the process of gametogenesis.
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spelling pubmed-29651082010-11-03 Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development Al-Shami, Amin Jhaver, Kanchan G. Vogel, Peter Wilkins, Carrie Humphries, Juliane Davis, John J. Xu, Nianhua Potter, David G. Gerhardt, Brenda Mullinax, Robert Shirley, Cynthia R. Anderson, Stephen J. Oravecz, Tamas PLoS One Research Article Rpn13 is a novel mammalian proteasomal receptor that has recently been identified as an amplification target in ovarian cancer. It can interact with ubiquitin and activate the deubiquitinating enzyme Uch37 at the 26S proteasome. Since neither Rpn13 nor Uch37 is an integral proteasomal subunit, we explored whether either protein is essential for mammalian development and survival. Deletion of Uch37 resulted in prenatal lethality in mice associated with severe defect in embryonic brain development. In contrast, the majority of Rpn13-deficient mice survived to adulthood, although they were smaller at birth and fewer in number than wild-type littermates. Absence of Rpn13 produced tissue-specific effects on proteasomal function: increased proteasome activity in adrenal gland and lymphoid organs, and decreased activity in testes and brain. Adult Rpn13(−/−) mice reached normal body weight but had increased body fat content and were infertile due to defective gametogenesis. Additionally, Rpn13(−/−) mice showed increased T-cell numbers, resembling growth hormone-mediated effects. Indeed, serum growth hormone and follicular stimulating hormone levels were significantly increased in Rpn13(−/−) mice, while growth hormone receptor expression was reduced in the testes. In conclusion, this is the first report characterizing the physiological roles of Uch37 and Rpn13 in murine development and implicating a non-ATPase proteasomal protein, Rpn13, in the process of gametogenesis. Public Library of Science 2010-10-27 /pmc/articles/PMC2965108/ /pubmed/21048919 http://dx.doi.org/10.1371/journal.pone.0013654 Text en Al-Shami et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Al-Shami, Amin
Jhaver, Kanchan G.
Vogel, Peter
Wilkins, Carrie
Humphries, Juliane
Davis, John J.
Xu, Nianhua
Potter, David G.
Gerhardt, Brenda
Mullinax, Robert
Shirley, Cynthia R.
Anderson, Stephen J.
Oravecz, Tamas
Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development
title Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development
title_full Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development
title_fullStr Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development
title_full_unstemmed Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development
title_short Regulators of the Proteasome Pathway, Uch37 and Rpn13, Play Distinct Roles in Mouse Development
title_sort regulators of the proteasome pathway, uch37 and rpn13, play distinct roles in mouse development
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2965108/
https://www.ncbi.nlm.nih.gov/pubmed/21048919
http://dx.doi.org/10.1371/journal.pone.0013654
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