Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome

To clarify genome-wide DNA methylation profiles during multistage renal carcinogenesis, bacterial artificial chromosome array-based methylated CpG island amplification (BAMCA) was performed. Non-cancerous renal cortex tissue obtained from patients with clear cell renal cell carcinomas (RCCs) (N) was...

Descripción completa

Detalles Bibliográficos
Autores principales: Arai, Eri, Ushijima, Saori, Fujimoto, Hiroyuki, Hosoda, Fumie, Shibata, Tatsuhiro, Kondo, Tadashi, Yokoi, Sana, Imoto, Issei, Inazawa, Johji, Hirohashi, Setsuo, Kanai, Yae
Formato: Texto
Lenguaje:English
Publicado: Oxford University Press 2009
Materias:
Cancer Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2639047/
https://www.ncbi.nlm.nih.gov/pubmed/19037089
http://dx.doi.org/10.1093/carcin/bgn268
_version_ 1782164439500324864
author Arai, Eri
Ushijima, Saori
Fujimoto, Hiroyuki
Hosoda, Fumie
Shibata, Tatsuhiro
Kondo, Tadashi
Yokoi, Sana
Imoto, Issei
Inazawa, Johji
Hirohashi, Setsuo
Kanai, Yae
author_facet Arai, Eri
Ushijima, Saori
Fujimoto, Hiroyuki
Hosoda, Fumie
Shibata, Tatsuhiro
Kondo, Tadashi
Yokoi, Sana
Imoto, Issei
Inazawa, Johji
Hirohashi, Setsuo
Kanai, Yae
author_sort Arai, Eri
collection PubMed
description To clarify genome-wide DNA methylation profiles during multistage renal carcinogenesis, bacterial artificial chromosome array-based methylated CpG island amplification (BAMCA) was performed. Non-cancerous renal cortex tissue obtained from patients with clear cell renal cell carcinomas (RCCs) (N) was at the precancerous stage where DNA hypomethylation and DNA hypermethylation on multiple bacterial artificial chromosome (BAC) clones were observed. By unsupervised hierarchical clustering analysis based on BAMCA data for their N, 51 patients with clear cell RCCs were clustered into two subclasses, Clusters A(N) (n = 46) and B(N) (n = 5). Clinicopathologically aggressive clear cell RCCs were accumulated in Cluster B(N), and the overall survival rate of patients in Cluster B(N) was significantly lower than that of patients in Cluster A(N). By unsupervised hierarchical clustering analysis based on BAMCA data for their RCCs, 51 patients were clustered into two subclasses, Clusters A(T) (n = 43) and B(T) (n = 8). Clinicopathologically aggressive clear cell RCCs were accumulated in Cluster B(T), and the overall survival rate of patients in Cluster B(T) was significantly lower than that of patients in Cluster A(T). Multivariate analysis revealed that belonging to Cluster B(T) was an independent predictor of recurrence. Cluster B(N) was completely included in Cluster B(T), and the majority of the BAC clones that significantly discriminated Cluster B(N) from Cluster A(N) also discriminated Cluster B(T) from Cluster A(T). In individual patients, DNA methylation status in N was basically inherited by the corresponding clear cell RCC. DNA methylation alterations in the precancerous stage may generate more malignant clear cell RCCs and determine patient outcome.
format Text
id pubmed-2639047
institution National Center for Biotechnology Information
language English
publishDate 2009
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-26390472009-02-25 Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome Arai, Eri Ushijima, Saori Fujimoto, Hiroyuki Hosoda, Fumie Shibata, Tatsuhiro Kondo, Tadashi Yokoi, Sana Imoto, Issei Inazawa, Johji Hirohashi, Setsuo Kanai, Yae Carcinogenesis Cancer Biology To clarify genome-wide DNA methylation profiles during multistage renal carcinogenesis, bacterial artificial chromosome array-based methylated CpG island amplification (BAMCA) was performed. Non-cancerous renal cortex tissue obtained from patients with clear cell renal cell carcinomas (RCCs) (N) was at the precancerous stage where DNA hypomethylation and DNA hypermethylation on multiple bacterial artificial chromosome (BAC) clones were observed. By unsupervised hierarchical clustering analysis based on BAMCA data for their N, 51 patients with clear cell RCCs were clustered into two subclasses, Clusters A(N) (n = 46) and B(N) (n = 5). Clinicopathologically aggressive clear cell RCCs were accumulated in Cluster B(N), and the overall survival rate of patients in Cluster B(N) was significantly lower than that of patients in Cluster A(N). By unsupervised hierarchical clustering analysis based on BAMCA data for their RCCs, 51 patients were clustered into two subclasses, Clusters A(T) (n = 43) and B(T) (n = 8). Clinicopathologically aggressive clear cell RCCs were accumulated in Cluster B(T), and the overall survival rate of patients in Cluster B(T) was significantly lower than that of patients in Cluster A(T). Multivariate analysis revealed that belonging to Cluster B(T) was an independent predictor of recurrence. Cluster B(N) was completely included in Cluster B(T), and the majority of the BAC clones that significantly discriminated Cluster B(N) from Cluster A(N) also discriminated Cluster B(T) from Cluster A(T). In individual patients, DNA methylation status in N was basically inherited by the corresponding clear cell RCC. DNA methylation alterations in the precancerous stage may generate more malignant clear cell RCCs and determine patient outcome. Oxford University Press 2009-02 2008-11-26 /pmc/articles/PMC2639047/ /pubmed/19037089 http://dx.doi.org/10.1093/carcin/bgn268 Text en © The Author 2008. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org The online version of this article has been published under an open access model. Users are entitled to use, reproduce, disseminate, or display the open access version of this article for non-commercial purposes provided that: the original authorship is properly and fully attributed; the Journal and Oxford University Press are attributed as the original place of publication with the correct citation details given; if an article is subsequently reproduced or disseminated not in its entirety but only in part or as a derivative work this must be clearly indicated. For commercial re-use, please contact journals.permissions@oxfordjournals.org
spellingShingle Cancer Biology
Arai, Eri
Ushijima, Saori
Fujimoto, Hiroyuki
Hosoda, Fumie
Shibata, Tatsuhiro
Kondo, Tadashi
Yokoi, Sana
Imoto, Issei
Inazawa, Johji
Hirohashi, Setsuo
Kanai, Yae
Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
title Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
title_full Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
title_fullStr Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
title_full_unstemmed Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
title_short Genome-wide DNA methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
title_sort genome-wide dna methylation profiles in both precancerous conditions and clear cell renal cell carcinomas are correlated with malignant potential and patient outcome
topic Cancer Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2639047/
https://www.ncbi.nlm.nih.gov/pubmed/19037089
http://dx.doi.org/10.1093/carcin/bgn268
work_keys_str_mv AT araieri genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT ushijimasaori genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT fujimotohiroyuki genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT hosodafumie genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT shibatatatsuhiro genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT kondotadashi genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT yokoisana genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT imotoissei genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT inazawajohji genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT hirohashisetsuo genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome
AT kanaiyae genomewidednamethylationprofilesinbothprecancerousconditionsandclearcellrenalcellcarcinomasarecorrelatedwithmalignantpotentialandpatientoutcome

Ejemplares similares