Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations

Yunyun Jiang; Gabriel G. Malouf; Jianping Zhang; Xiaofeng Zheng; Yunxin Chen; Erika J. Thompson; John N. Weinstein; Ying Yuan; Jean Philippe Spano; Russell Broaddus; Nizar M. Tannir; David Khayat; Karen H. Lu; Xiaoping Su

doi:10.18632/oncotarget.5399

Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations

Yunyun Jiang, Gabriel G. Malouf, Jianping Zhang, Xiaofeng Zheng, Yunxin Chen, Erika J. Thompson, John N. Weinstein, Ying Yuan, Jean Philippe Spano, Russell Broaddus, Nizar M. Tannir, David Khayat, Karen H. Lu, Xiaoping Su

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22 Scopus citations

Abstract

Background: Integrative analysis of endometrioid endometrial carcinoma (EEC) using multiple platforms has distinguished four molecular subgroups. However, the landscape of expressed long non-coding RNAs (lncRNA) and their role in charting EEC subgroups and determining clinical aggressiveness remain largely unknown. Materials and Methods: We performed integrative analysis of lncRNAs in EEC using The Cancer Genome Atlas (TCGA) molecular RNAseq profiles of 191 primary tumors for which genomic data were also available. We established lncRNA subgroup classification, correlated it with chromatin modifying gene expression, and described correlations between our lncRNA classification and clinico-genomic tumor features. Results: Using stringent criteria, we identified 1,931 expressed lncRNAs and predicted potential drivers through integrative analysis. Unsupervised clustering of lncRNA expression revealed three robust categories: basal-like, luminal-like and CTNNB1-enriched subgroups. Basal-like subgroup was enriched for aggressive tumors with higher pathological grade (p < 0.0001), TNM stage (p = 0.01), and somatic mutations in trithorax-group genes (MLL, MLL2 and MLL3); and it overexpressed polycomb genes EZH2 and CBX2. In contrast to the luminal-like subgroup, progesterone (PGR) and estrogen receptor (ESR1) genes were highly down-regulated in the EEC basal-like subgroup. Consistent with its enrichment for CTNNB1 mutations (69%), lncRNA profile of the CTNNB1-enriched EEC subgroup was highly similar to that of the CTNNB1-enriched liver cancer subgroup. Conclusions: Our results reveal the utility of systematic characterization of clinically annotated EEC in three clinically relevant subgroups. They also highlight the convergence of aberrations in polycomb- and trithorax-group genes in aggressive basal EEC subtypes, providing a rationale for further investigation of epigenetic therapy in this setting.

Original language	English (US)
Pages (from-to)	39865-39876
Number of pages	12
Journal	Oncotarget
Volume	6
Issue number	37
DOIs	https://doi.org/10.18632/oncotarget.5399
State	Published - 2015

Keywords

Endometrioid endometrial carcinoma
Expression profiling
Long non-coding RNA
Polycomb complex
RNA-Seq

ASJC Scopus subject areas

Oncology

MD Anderson CCSG core facilities

Bioinformatics Shared Resource
Biostatistics Resource Group

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10.18632/oncotarget.5399

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Jiang, Y., Malouf, G. G., Zhang, J., Zheng, X., Chen, Y., Thompson, E. J., Weinstein, J. N., Yuan, Y., Spano, J. P., Broaddus, R., Tannir, N. M., Khayat, D., Lu, K. H., & Su, X. (2015). Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations. Oncotarget, 6(37), 39865-39876. https://doi.org/10.18632/oncotarget.5399

Jiang, Y, Malouf, GG, Zhang, J, Zheng, X , Chen, Y, Thompson, EJ, Weinstein, JN , Yuan, Y, Spano, JP, Broaddus, R, Tannir, NM, Khayat, D, Lu, KH & Su, X 2015, 'Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations', Oncotarget, vol. 6, no. 37, pp. 39865-39876. https://doi.org/10.18632/oncotarget.5399

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title = "Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations",

abstract = "Background: Integrative analysis of endometrioid endometrial carcinoma (EEC) using multiple platforms has distinguished four molecular subgroups. However, the landscape of expressed long non-coding RNAs (lncRNA) and their role in charting EEC subgroups and determining clinical aggressiveness remain largely unknown. Materials and Methods: We performed integrative analysis of lncRNAs in EEC using The Cancer Genome Atlas (TCGA) molecular RNAseq profiles of 191 primary tumors for which genomic data were also available. We established lncRNA subgroup classification, correlated it with chromatin modifying gene expression, and described correlations between our lncRNA classification and clinico-genomic tumor features. Results: Using stringent criteria, we identified 1,931 expressed lncRNAs and predicted potential drivers through integrative analysis. Unsupervised clustering of lncRNA expression revealed three robust categories: basal-like, luminal-like and CTNNB1-enriched subgroups. Basal-like subgroup was enriched for aggressive tumors with higher pathological grade (p < 0.0001), TNM stage (p = 0.01), and somatic mutations in trithorax-group genes (MLL, MLL2 and MLL3); and it overexpressed polycomb genes EZH2 and CBX2. In contrast to the luminal-like subgroup, progesterone (PGR) and estrogen receptor (ESR1) genes were highly down-regulated in the EEC basal-like subgroup. Consistent with its enrichment for CTNNB1 mutations (69%), lncRNA profile of the CTNNB1-enriched EEC subgroup was highly similar to that of the CTNNB1-enriched liver cancer subgroup. Conclusions: Our results reveal the utility of systematic characterization of clinically annotated EEC in three clinically relevant subgroups. They also highlight the convergence of aberrations in polycomb- and trithorax-group genes in aggressive basal EEC subtypes, providing a rationale for further investigation of epigenetic therapy in this setting.",

keywords = "Endometrioid endometrial carcinoma, Expression profiling, Long non-coding RNA, Polycomb complex, RNA-Seq",

author = "Yunyun Jiang and Malouf, {Gabriel G.} and Jianping Zhang and Xiaofeng Zheng and Yunxin Chen and Thompson, {Erika J.} and Weinstein, {John N.} and Ying Yuan and Spano, {Jean Philippe} and Russell Broaddus and Tannir, {Nizar M.} and David Khayat and Lu, {Karen H.} and Xiaoping Su",

year = "2015",

doi = "10.18632/oncotarget.5399",

language = "English (US)",

volume = "6",

pages = "39865--39876",

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T1 - Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations

AU - Jiang, Yunyun

AU - Malouf, Gabriel G.

AU - Zhang, Jianping

AU - Zheng, Xiaofeng

AU - Chen, Yunxin

AU - Thompson, Erika J.

AU - Weinstein, John N.

AU - Yuan, Ying

AU - Spano, Jean Philippe

AU - Broaddus, Russell

AU - Tannir, Nizar M.

AU - Khayat, David

AU - Lu, Karen H.

AU - Su, Xiaoping

PY - 2015

Y1 - 2015

N2 - Background: Integrative analysis of endometrioid endometrial carcinoma (EEC) using multiple platforms has distinguished four molecular subgroups. However, the landscape of expressed long non-coding RNAs (lncRNA) and their role in charting EEC subgroups and determining clinical aggressiveness remain largely unknown. Materials and Methods: We performed integrative analysis of lncRNAs in EEC using The Cancer Genome Atlas (TCGA) molecular RNAseq profiles of 191 primary tumors for which genomic data were also available. We established lncRNA subgroup classification, correlated it with chromatin modifying gene expression, and described correlations between our lncRNA classification and clinico-genomic tumor features. Results: Using stringent criteria, we identified 1,931 expressed lncRNAs and predicted potential drivers through integrative analysis. Unsupervised clustering of lncRNA expression revealed three robust categories: basal-like, luminal-like and CTNNB1-enriched subgroups. Basal-like subgroup was enriched for aggressive tumors with higher pathological grade (p < 0.0001), TNM stage (p = 0.01), and somatic mutations in trithorax-group genes (MLL, MLL2 and MLL3); and it overexpressed polycomb genes EZH2 and CBX2. In contrast to the luminal-like subgroup, progesterone (PGR) and estrogen receptor (ESR1) genes were highly down-regulated in the EEC basal-like subgroup. Consistent with its enrichment for CTNNB1 mutations (69%), lncRNA profile of the CTNNB1-enriched EEC subgroup was highly similar to that of the CTNNB1-enriched liver cancer subgroup. Conclusions: Our results reveal the utility of systematic characterization of clinically annotated EEC in three clinically relevant subgroups. They also highlight the convergence of aberrations in polycomb- and trithorax-group genes in aggressive basal EEC subtypes, providing a rationale for further investigation of epigenetic therapy in this setting.

AB - Background: Integrative analysis of endometrioid endometrial carcinoma (EEC) using multiple platforms has distinguished four molecular subgroups. However, the landscape of expressed long non-coding RNAs (lncRNA) and their role in charting EEC subgroups and determining clinical aggressiveness remain largely unknown. Materials and Methods: We performed integrative analysis of lncRNAs in EEC using The Cancer Genome Atlas (TCGA) molecular RNAseq profiles of 191 primary tumors for which genomic data were also available. We established lncRNA subgroup classification, correlated it with chromatin modifying gene expression, and described correlations between our lncRNA classification and clinico-genomic tumor features. Results: Using stringent criteria, we identified 1,931 expressed lncRNAs and predicted potential drivers through integrative analysis. Unsupervised clustering of lncRNA expression revealed three robust categories: basal-like, luminal-like and CTNNB1-enriched subgroups. Basal-like subgroup was enriched for aggressive tumors with higher pathological grade (p < 0.0001), TNM stage (p = 0.01), and somatic mutations in trithorax-group genes (MLL, MLL2 and MLL3); and it overexpressed polycomb genes EZH2 and CBX2. In contrast to the luminal-like subgroup, progesterone (PGR) and estrogen receptor (ESR1) genes were highly down-regulated in the EEC basal-like subgroup. Consistent with its enrichment for CTNNB1 mutations (69%), lncRNA profile of the CTNNB1-enriched EEC subgroup was highly similar to that of the CTNNB1-enriched liver cancer subgroup. Conclusions: Our results reveal the utility of systematic characterization of clinically annotated EEC in three clinically relevant subgroups. They also highlight the convergence of aberrations in polycomb- and trithorax-group genes in aggressive basal EEC subtypes, providing a rationale for further investigation of epigenetic therapy in this setting.

KW - Endometrioid endometrial carcinoma

KW - Expression profiling

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KW - Polycomb complex

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Long non-coding RNA profiling links subgroup classification of endometrioid endometrial carcinomas with trithorax and polycomb complex aberrations

Abstract

Keywords

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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