AB088. Genomic study on the cancers in urological system

OBJECTIVE: Bladder cancer and renal cancer are common malignancies in the urological system. The aims of the present study are to detect the genomic changes in the cancer tissues by massively parallel DNA sequence technology. METHODS: The cancer tissues with matched morphologically normal tissues an...

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Autores principales: Gui, Yaoting, Huang, Yi, Guo, Guangwu, Tang, Aifa, Li, Zesong, Wu, Song, Li, Xianxin, Cai, Zhiming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: AME Publishing Company 2015
Materias:
Podium Lecture
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4708858/
http://dx.doi.org/10.3978/j.issn.2223-4683.2015.s088
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author Gui, Yaoting
Huang, Yi
Guo, Guangwu
Tang, Aifa
Li, Zesong
Wu, Song
Li, Xianxin
Cai, Zhiming
author_facet Gui, Yaoting
Huang, Yi
Guo, Guangwu
Tang, Aifa
Li, Zesong
Wu, Song
Li, Xianxin
Cai, Zhiming
author_sort Gui, Yaoting
collection PubMed
description OBJECTIVE: Bladder cancer and renal cancer are common malignancies in the urological system. The aims of the present study are to detect the genomic changes in the cancer tissues by massively parallel DNA sequence technology. METHODS: The cancer tissues with matched morphologically normal tissues and peripheral blood samples were collected from the patients with urothelial bladder carcinoma (UBC) and clear cell renal cell carcinoma (ccRCC). Whole genome, exome or transcriptome of the samples were sequenced by massively parallel DNA sequencing technology. The somatic mutations, copy number variations and mRNA variations were identified by different bioinformatic methods and validated by Sanger DNA sequencing. RESULTS: We sequenced the exomes of nine individuals with UBC and screened all the somatically mutated genes in a prevalence set of 88 additional individuals with UBC with different tumor stages and grades, and identified genetic aberrations of the chromatin remodeling genes (UTX, MLL-MLL3, CREBBP-EP300, NCOR1, ARID1A and CHD6) in 59% of our 97 subjects with UBC. Of these genes, we showed UTX to be altered substantially more frequently in tumors of low stages and grades, highlighting its potential role in the classification and diagnosis of bladder cancer. We sequenced whole exomes of 10 ccRCC samples and performed a screen of 1,100 genes in 88 additional ccRCCs, from which we discovered 12 previously unidentified genes mutated at elevated frequencies in ccRCC. Notably, we detected frequent mutations in the ubiquitin-mediated proteolysis pathway (UMPP), and alterations in the UMPP were significantly associated with overexpression of HIF1α and HIF2α in the tumors. CONCLUSIONS: Our results provide an overview of the genetic basis of UBC and suggest that aberration of chromatin regulation might be a hallmark of bladder cancer. Our findings highlight the potential contribution of UMPP to ccRCC tumorigenesis through the activation of the hypoxia regulatory network.
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spelling pubmed-47088582016-01-26 AB088. Genomic study on the cancers in urological system Gui, Yaoting Huang, Yi Guo, Guangwu Tang, Aifa Li, Zesong Wu, Song Li, Xianxin Cai, Zhiming Transl Androl Urol Podium Lecture OBJECTIVE: Bladder cancer and renal cancer are common malignancies in the urological system. The aims of the present study are to detect the genomic changes in the cancer tissues by massively parallel DNA sequence technology. METHODS: The cancer tissues with matched morphologically normal tissues and peripheral blood samples were collected from the patients with urothelial bladder carcinoma (UBC) and clear cell renal cell carcinoma (ccRCC). Whole genome, exome or transcriptome of the samples were sequenced by massively parallel DNA sequencing technology. The somatic mutations, copy number variations and mRNA variations were identified by different bioinformatic methods and validated by Sanger DNA sequencing. RESULTS: We sequenced the exomes of nine individuals with UBC and screened all the somatically mutated genes in a prevalence set of 88 additional individuals with UBC with different tumor stages and grades, and identified genetic aberrations of the chromatin remodeling genes (UTX, MLL-MLL3, CREBBP-EP300, NCOR1, ARID1A and CHD6) in 59% of our 97 subjects with UBC. Of these genes, we showed UTX to be altered substantially more frequently in tumors of low stages and grades, highlighting its potential role in the classification and diagnosis of bladder cancer. We sequenced whole exomes of 10 ccRCC samples and performed a screen of 1,100 genes in 88 additional ccRCCs, from which we discovered 12 previously unidentified genes mutated at elevated frequencies in ccRCC. Notably, we detected frequent mutations in the ubiquitin-mediated proteolysis pathway (UMPP), and alterations in the UMPP were significantly associated with overexpression of HIF1α and HIF2α in the tumors. CONCLUSIONS: Our results provide an overview of the genetic basis of UBC and suggest that aberration of chromatin regulation might be a hallmark of bladder cancer. Our findings highlight the potential contribution of UMPP to ccRCC tumorigenesis through the activation of the hypoxia regulatory network. AME Publishing Company 2015-08 /pmc/articles/PMC4708858/ http://dx.doi.org/10.3978/j.issn.2223-4683.2015.s088 Text en 2015 Translational Andrology and Urology. All rights reserved.
spellingShingle Podium Lecture
Gui, Yaoting
Huang, Yi
Guo, Guangwu
Tang, Aifa
Li, Zesong
Wu, Song
Li, Xianxin
Cai, Zhiming
AB088. Genomic study on the cancers in urological system
title AB088. Genomic study on the cancers in urological system
title_full AB088. Genomic study on the cancers in urological system
title_fullStr AB088. Genomic study on the cancers in urological system
title_full_unstemmed AB088. Genomic study on the cancers in urological system
title_short AB088. Genomic study on the cancers in urological system
title_sort ab088. genomic study on the cancers in urological system
topic Podium Lecture
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4708858/
http://dx.doi.org/10.3978/j.issn.2223-4683.2015.s088
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