SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex

SPOP, speckle-type POZ protein is a substrate adaptor protein of the Cullin-3/RING ubiquitin E3 complex. The spop gene is the most commonly point mutated in human primary prostate cancers, but the pathological contribution of the SPOP mutations remains unclear. In this study, we investigated several...

Descripción completa

Detalles Bibliográficos
Autores principales: Watanabe, Ryuta, Maekawa, Masashi, Hieda, Miki, Taguchi, Tomohiko, Miura, Noriyoshi, Kikugawa, Tadahiko, Saika, Takashi, Higashiyama, Shigeki
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society for Cell Biology 2020
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7185892/
https://www.ncbi.nlm.nih.gov/pubmed/31967940
http://dx.doi.org/10.1091/mbc.E19-08-0456
_version_ 1783526844619816960
author Watanabe, Ryuta
Maekawa, Masashi
Hieda, Miki
Taguchi, Tomohiko
Miura, Noriyoshi
Kikugawa, Tadahiko
Saika, Takashi
Higashiyama, Shigeki
author_facet Watanabe, Ryuta
Maekawa, Masashi
Hieda, Miki
Taguchi, Tomohiko
Miura, Noriyoshi
Kikugawa, Tadahiko
Saika, Takashi
Higashiyama, Shigeki
author_sort Watanabe, Ryuta
collection PubMed
description SPOP, speckle-type POZ protein is a substrate adaptor protein of the Cullin-3/RING ubiquitin E3 complex. The spop gene is the most commonly point mutated in human primary prostate cancers, but the pathological contribution of the SPOP mutations remains unclear. In this study, we investigated several known factors that are critical in the DNA–­protein cross-link repair process. The depletion of SPOP or overexpression of a prostate cancer–associated SPOP mutant, F133V, in androgen receptor-positive prostate cancer cells increased the amount of topoisomerase 2A (TOP2A) in the nuclei together with the increased amount of γH2AX, an indication of DNA breaks. Tyrosyl–DNA phosphodiesterases (TDPs) and an endo/exonuclease MRE11 are enzymes that liberate TOP2A from the TOP2A–DNA cleavage complex, and thus is essential for the completion of the DNA repair process. We found that the amount of TDP1 and TDP2 was decreased in SPOP-depleted cells, and that of TDP2 and MRE11 was decreased in F133V-overexpressing cells. These results suggest that the F133V mutant exerts dominant-negative and gain-of-function effects in down-regulation of TDP2 and MRE11, respectively. We conclude that SPOP is involved in the DNA–protein cross-link repair process through the elimination of TOP2A from the TOP2A cleavage complex, which may contribute to the genome stability.
format Online
Article
Text
id pubmed-7185892
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher The American Society for Cell Biology
record_format MEDLINE/PubMed
spelling pubmed-71858922020-06-06 SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex Watanabe, Ryuta Maekawa, Masashi Hieda, Miki Taguchi, Tomohiko Miura, Noriyoshi Kikugawa, Tadahiko Saika, Takashi Higashiyama, Shigeki Mol Biol Cell Articles SPOP, speckle-type POZ protein is a substrate adaptor protein of the Cullin-3/RING ubiquitin E3 complex. The spop gene is the most commonly point mutated in human primary prostate cancers, but the pathological contribution of the SPOP mutations remains unclear. In this study, we investigated several known factors that are critical in the DNA–­protein cross-link repair process. The depletion of SPOP or overexpression of a prostate cancer–associated SPOP mutant, F133V, in androgen receptor-positive prostate cancer cells increased the amount of topoisomerase 2A (TOP2A) in the nuclei together with the increased amount of γH2AX, an indication of DNA breaks. Tyrosyl–DNA phosphodiesterases (TDPs) and an endo/exonuclease MRE11 are enzymes that liberate TOP2A from the TOP2A–DNA cleavage complex, and thus is essential for the completion of the DNA repair process. We found that the amount of TDP1 and TDP2 was decreased in SPOP-depleted cells, and that of TDP2 and MRE11 was decreased in F133V-overexpressing cells. These results suggest that the F133V mutant exerts dominant-negative and gain-of-function effects in down-regulation of TDP2 and MRE11, respectively. We conclude that SPOP is involved in the DNA–protein cross-link repair process through the elimination of TOP2A from the TOP2A cleavage complex, which may contribute to the genome stability. The American Society for Cell Biology 2020-03-15 /pmc/articles/PMC7185892/ /pubmed/31967940 http://dx.doi.org/10.1091/mbc.E19-08-0456 Text en © 2020 Watanabe, Maekawa, et al. “ASCB®,” “The American Society for Cell Biology®,” and “Molecular Biology of the Cell®” are registered trademarks of The American Society for Cell Biology. http://creativecommons.org/licenses/by-nc-sa/3.0 This article is distributed by The American Society for Cell Biology under license from the author(s). Two months after publication it is available to the public under an Attribution–Noncommercial–Share Alike 3.0 Unported Creative Commons License.
spellingShingle Articles
Watanabe, Ryuta
Maekawa, Masashi
Hieda, Miki
Taguchi, Tomohiko
Miura, Noriyoshi
Kikugawa, Tadahiko
Saika, Takashi
Higashiyama, Shigeki
SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex
title SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex
title_full SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex
title_fullStr SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex
title_full_unstemmed SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex
title_short SPOP is essential for DNA–protein cross-link repair in prostate cancer cells: SPOP-dependent removal of topoisomerase 2A from the topoisomerase 2A-DNA cleavage complex
title_sort spop is essential for dna–protein cross-link repair in prostate cancer cells: spop-dependent removal of topoisomerase 2a from the topoisomerase 2a-dna cleavage complex
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7185892/
https://www.ncbi.nlm.nih.gov/pubmed/31967940
http://dx.doi.org/10.1091/mbc.E19-08-0456
work_keys_str_mv AT watanaberyuta spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT maekawamasashi spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT hiedamiki spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT taguchitomohiko spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT miuranoriyoshi spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT kikugawatadahiko spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT saikatakashi spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex
AT higashiyamashigeki spopisessentialfordnaproteincrosslinkrepairinprostatecancercellsspopdependentremovaloftopoisomerase2afromthetopoisomerase2adnacleavagecomplex

Ejemplares similares