Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast

Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast

<p>Abstract</p> <p>Background</p> <p>The ubiquitin(Ub)-proteasome pathway is implicated in the regulation of a variety of cellular functions and plays a major role in stress response in eukaryotic cells, by targeting misfolded and damaged proteins for degradation. In ad...

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Main Authors: Bo Laura, Carenini Nives, Righetti Sabina C, Hayles Jacqueline, Hoe Kwang L, Gatti Laura, Kim Dong U, Park Han O, Perego Paola
Format: Article
Language:English
Published: BMC 2011-01-01
Series:BMC Genomics
Online Access:http://www.biomedcentral.com/1471-2164/12/44
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spelling doaj-ea2fd0428a8c49c6b86f308ae9c5ee032020-11-24T21:17:41ZengBMCBMC Genomics1471-21642011-01-011214410.1186/1471-2164-12-44Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeastBo LauraCarenini NivesRighetti Sabina CHayles JacquelineHoe Kwang LGatti LauraKim Dong UPark Han OPerego Paola<p>Abstract</p> <p>Background</p> <p>The ubiquitin(Ub)-proteasome pathway is implicated in the regulation of a variety of cellular functions and plays a major role in stress response in eukaryotic cells, by targeting misfolded and damaged proteins for degradation. In addition, in the presence of DNA damage, the Ub-proteasome system regulates proteins involved in sensing, repairing, and/or tolerating the damage. Antitumor agents such as cisplatin can activate the pathway, but the role of specific pathway components in cell sensitivity/response to the drug is not known. Since platinum compounds represent clinically relevant antitumor agents and a major limitation to their use is the development of drug resistance, there is an urgent need for identifying targets for improving their efficacy.</p> <p>Results</p> <p>In the present study, we performed a genome-wide screening for sensitivity to cisplatin using non-essential haploid deletion mutants of the fission yeast <it>Schizosaccharomyces pombe</it>, belonging to a collection of haploid strains constructed through homologous recombination. Using this approach, we identified three Ub-proteasome mutants exhibiting hypersensitivity to cisplatin (<it>ubp16</it>, <it>ubc13 </it>and <it>pmt3</it>) and ten mutants (including <it>ufd2</it>, <it>beta7 20S</it>, <it>rpt6/let1</it>) resistant to the drug. In addition, the importance of lub1 gene emerged from the comparison between the present screening and gene expression profile data previously obtained in fission yeast.</p> <p>Conclusions</p> <p>The factors identified in the present study allowed us to highlight most finely the close relationship between the Ub-proteasome system and DNA damage response mechanisms, thus establishing a comprehensive framework of regulators likely relevant also in higher eukaryotes. Our results provide the proof of principle of the involvement of specific genes modulated by cisplatin treatment in cell response to the drug, suggesting their potential role as targets for modulating cisplatin sensitivity. In this regard, the prospective identification of novel targets for modulation of cisplatin sensitivity in an eukaryotic model organism appears particularly intriguing towards the discovery of strategies to overcome cisplatin resistance in human tumors.</p> http://www.biomedcentral.com/1471-2164/12/44
collection DOAJ
language English
format Article
sources DOAJ
author Bo Laura
Carenini Nives
Righetti Sabina C
Hayles Jacqueline
Hoe Kwang L
Gatti Laura
Kim Dong U
Park Han O
Perego Paola
spellingShingle Bo Laura
Carenini Nives
Righetti Sabina C
Hayles Jacqueline
Hoe Kwang L
Gatti Laura
Kim Dong U
Park Han O
Perego Paola
Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
BMC Genomics
author_facet Bo Laura
Carenini Nives
Righetti Sabina C
Hayles Jacqueline
Hoe Kwang L
Gatti Laura
Kim Dong U
Park Han O
Perego Paola
author_sort Bo Laura
title Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
title_short Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
title_full Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
title_fullStr Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
title_full_unstemmed Ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
title_sort ubiquitin-proteasome genes as targets for modulation of cisplatin sensitivity in fission yeast
publisher BMC
series BMC Genomics
issn 1471-2164
publishDate 2011-01-01
description <p>Abstract</p> <p>Background</p> <p>The ubiquitin(Ub)-proteasome pathway is implicated in the regulation of a variety of cellular functions and plays a major role in stress response in eukaryotic cells, by targeting misfolded and damaged proteins for degradation. In addition, in the presence of DNA damage, the Ub-proteasome system regulates proteins involved in sensing, repairing, and/or tolerating the damage. Antitumor agents such as cisplatin can activate the pathway, but the role of specific pathway components in cell sensitivity/response to the drug is not known. Since platinum compounds represent clinically relevant antitumor agents and a major limitation to their use is the development of drug resistance, there is an urgent need for identifying targets for improving their efficacy.</p> <p>Results</p> <p>In the present study, we performed a genome-wide screening for sensitivity to cisplatin using non-essential haploid deletion mutants of the fission yeast <it>Schizosaccharomyces pombe</it>, belonging to a collection of haploid strains constructed through homologous recombination. Using this approach, we identified three Ub-proteasome mutants exhibiting hypersensitivity to cisplatin (<it>ubp16</it>, <it>ubc13 </it>and <it>pmt3</it>) and ten mutants (including <it>ufd2</it>, <it>beta7 20S</it>, <it>rpt6/let1</it>) resistant to the drug. In addition, the importance of lub1 gene emerged from the comparison between the present screening and gene expression profile data previously obtained in fission yeast.</p> <p>Conclusions</p> <p>The factors identified in the present study allowed us to highlight most finely the close relationship between the Ub-proteasome system and DNA damage response mechanisms, thus establishing a comprehensive framework of regulators likely relevant also in higher eukaryotes. Our results provide the proof of principle of the involvement of specific genes modulated by cisplatin treatment in cell response to the drug, suggesting their potential role as targets for modulating cisplatin sensitivity. In this regard, the prospective identification of novel targets for modulation of cisplatin sensitivity in an eukaryotic model organism appears particularly intriguing towards the discovery of strategies to overcome cisplatin resistance in human tumors.</p>
url http://www.biomedcentral.com/1471-2164/12/44
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