Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma

Aditi Qamra; Manjie Xing; Nisha Padmanabhan; Jeffrey Jun Ting Kwok; Shenli Zhang; Chang Xu; Yan Shan Leong; Ai Ping Lee Lim; Qianqao Tang; Wen Fong Ooi; Joyce Suling Lin; Tannistha Nandi; Xiaosai Yao; Xuewen Ong; Minghui Lee; Su Ting Tay; Angie Tan Lay Keng; Erna Gondo Santoso; Cedric Chuan Young Ng; Alvin Ng; Apinya Jusakul; Duane Smoot; Hassan Ashktorab; Sun Young Rha; Khay Guan Yeoh; Wei Peng Yong; Pierce K.H. Chow; Weng Hoong Chan; Hock Soo Ong; Khee Chee Soo; Kyoung Mee Kim; Wai Keong Wong; Steven G. Rozen; Bin Tean Teh; Dennis Kappei; Jeeyun Lee; John Connolly; Patrick Tan

doi:10.1158/2159-8290.CD-16-1022

Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma

Aditi Qamra, Manjie Xing, Nisha Padmanabhan, Jeffrey Jun Ting Kwok, Shenli Zhang, Chang Xu, Yan Shan Leong, Ai Ping Lee Lim, Qianqao Tang, Wen Fong Ooi, Joyce Suling Lin, Tannistha Nandi, Xiaosai Yao, Xuewen Ong, Minghui Lee, Su Ting Tay, Angie Tan Lay Keng, Erna Gondo Santoso, Cedric Chuan Young Ng, Alvin NgApinya Jusakul, Duane Smoot, Hassan Ashktorab, Sun Young Rha, Khay Guan Yeoh, Wei Peng Yong, Pierce K.H. Chow, Weng Hoong Chan, Hock Soo Ong, Khee Chee Soo, Kyoung Mee Kim, Wai Keong Wong, Steven G. Rozen, Bin Tean Teh, Dennis Kappei, Jeeyun Lee, John Connolly, Patrick Tan^*

^*Corresponding author for this work

Research output: Contribution to journal › Journal Article › peer-review

47 Scopus citations

Abstract

Promoter elements play important roles in isoform and cell type-specific expression. We surveyed the epigenomic promoter landscape of gastric adenocarcinoma, analyzing 110 chromatin profiles (H3K4me3, H3K4me1, H3K27ac) of primary gastric cancers, gastric cancer lines, and nonmalignant gastric tissues. We identified nearly 2,000 promoter alterations (somatic promoters), many deregulated in various epithelial malignancies and mapping frequently to alternative promoters within the same gene, generating potential pro-oncogenic isoforms (RASA3). Somatic promoter- associated N-terminal peptides displaying relative depletion in tumors exhibited high-affinity MHC binding predictions and elicited potent T-cell responses in vitro, suggesting a mechanism for reducing tumor antigenicity. In multiple patient cohorts, gastric cancers with high somatic promoter usage also displayed reduced T-cell cytolytic marker expression. Somatic promoters are enriched in PRC2 occupancy, display sensitivity to EZH2 therapeutic inhibition, and are associated with novel cancer-associated transcripts. By generating tumor-specific isoforms and decreasing tumor antigenicity, epigenomic promoter alterations may thus drive intrinsic tumorigenesis and also allow nascent cancers to evade host immunity. SIGNIFICANCE: We apply epigenomic profiling to demarcate the promoter landscape of gastric cancer. Many tumor-specific promoters activate different promoters in the same gene, some generating pro-oncogenic isoforms. Tumor-specific promoters also reduce tumor antigenicity by causing relative depletion of immunogenic peptides, contributing to cancer immunoediting and allowing tumors to evade host immune attack.

Original language	English
Pages (from-to)	630-651
Number of pages	22
Journal	Cancer Discovery
Volume	7
Issue number	6
DOIs	https://doi.org/10.1158/2159-8290.CD-16-1022
State	Published - 2017
Externally published	Yes

Bibliographical note

Publisher Copyright:
© 2017 AACR.

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Qamra, A., Xing, M., Padmanabhan, N., Kwok, J. J. T., Zhang, S., Xu, C., Leong, Y. S., Lim, A. P. L., Tang, Q., Ooi, W. F., Lin, J. S., Nandi, T., Yao, X., Ong, X., Lee, M., Tay, S. T., Keng, A. T. L., Santoso, E. G., Ng, C. C. Y., ... Tan, P. (2017). Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma. Cancer Discovery, 7(6), 630-651. https://doi.org/10.1158/2159-8290.CD-16-1022

@article{388c7ddafe2547e79b717d36af4fe3f6,

title = "Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma",

abstract = "Promoter elements play important roles in isoform and cell type-specific expression. We surveyed the epigenomic promoter landscape of gastric adenocarcinoma, analyzing 110 chromatin profiles (H3K4me3, H3K4me1, H3K27ac) of primary gastric cancers, gastric cancer lines, and nonmalignant gastric tissues. We identified nearly 2,000 promoter alterations (somatic promoters), many deregulated in various epithelial malignancies and mapping frequently to alternative promoters within the same gene, generating potential pro-oncogenic isoforms (RASA3). Somatic promoter- associated N-terminal peptides displaying relative depletion in tumors exhibited high-affinity MHC binding predictions and elicited potent T-cell responses in vitro, suggesting a mechanism for reducing tumor antigenicity. In multiple patient cohorts, gastric cancers with high somatic promoter usage also displayed reduced T-cell cytolytic marker expression. Somatic promoters are enriched in PRC2 occupancy, display sensitivity to EZH2 therapeutic inhibition, and are associated with novel cancer-associated transcripts. By generating tumor-specific isoforms and decreasing tumor antigenicity, epigenomic promoter alterations may thus drive intrinsic tumorigenesis and also allow nascent cancers to evade host immunity. SIGNIFICANCE: We apply epigenomic profiling to demarcate the promoter landscape of gastric cancer. Many tumor-specific promoters activate different promoters in the same gene, some generating pro-oncogenic isoforms. Tumor-specific promoters also reduce tumor antigenicity by causing relative depletion of immunogenic peptides, contributing to cancer immunoediting and allowing tumors to evade host immune attack.",

author = "Aditi Qamra and Manjie Xing and Nisha Padmanabhan and Kwok, {Jeffrey Jun Ting} and Shenli Zhang and Chang Xu and Leong, {Yan Shan} and Lim, {Ai Ping Lee} and Qianqao Tang and Ooi, {Wen Fong} and Lin, {Joyce Suling} and Tannistha Nandi and Xiaosai Yao and Xuewen Ong and Minghui Lee and Tay, {Su Ting} and Keng, {Angie Tan Lay} and Santoso, {Erna Gondo} and Ng, {Cedric Chuan Young} and Alvin Ng and Apinya Jusakul and Duane Smoot and Hassan Ashktorab and Rha, {Sun Young} and Yeoh, {Khay Guan} and Yong, {Wei Peng} and Chow, {Pierce K.H.} and Chan, {Weng Hoong} and Ong, {Hock Soo} and Soo, {Khee Chee} and Kim, {Kyoung Mee} and Wong, {Wai Keong} and Rozen, {Steven G.} and Teh, {Bin Tean} and Dennis Kappei and Jeeyun Lee and John Connolly and Patrick Tan",

note = "Publisher Copyright: {\textcopyright} 2017 AACR.",

year = "2017",

doi = "10.1158/2159-8290.CD-16-1022",

language = "英语",

volume = "7",

pages = "630--651",

journal = "Cancer Discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "6",

}

Qamra, A, Xing, M, Padmanabhan, N, Kwok, JJT, Zhang, S, Xu, C, Leong, YS, Lim, APL, Tang, Q, Ooi, WF, Lin, JS, Nandi, T, Yao, X, Ong, X, Lee, M, Tay, ST, Keng, ATL, Santoso, EG, Ng, CCY, Ng, A, Jusakul, A, Smoot, D, Ashktorab, H, Rha, SY, Yeoh, KG, Yong, WP, Chow, PKH, Chan, WH, Ong, HS, Soo, KC, Kim, KM, Wong, WK, Rozen, SG, Teh, BT, Kappei, D, Lee, J, Connolly, J & Tan, P 2017, 'Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma', Cancer Discovery, vol. 7, no. 6, pp. 630-651. https://doi.org/10.1158/2159-8290.CD-16-1022

TY - JOUR

T1 - Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma

AU - Qamra, Aditi

AU - Xing, Manjie

AU - Padmanabhan, Nisha

AU - Kwok, Jeffrey Jun Ting

AU - Zhang, Shenli

AU - Xu, Chang

AU - Leong, Yan Shan

AU - Lim, Ai Ping Lee

AU - Tang, Qianqao

AU - Ooi, Wen Fong

AU - Lin, Joyce Suling

AU - Nandi, Tannistha

AU - Yao, Xiaosai

AU - Ong, Xuewen

AU - Lee, Minghui

AU - Tay, Su Ting

AU - Keng, Angie Tan Lay

AU - Santoso, Erna Gondo

AU - Ng, Cedric Chuan Young

AU - Ng, Alvin

AU - Jusakul, Apinya

AU - Smoot, Duane

AU - Ashktorab, Hassan

AU - Rha, Sun Young

AU - Yeoh, Khay Guan

AU - Yong, Wei Peng

AU - Chow, Pierce K.H.

AU - Chan, Weng Hoong

AU - Ong, Hock Soo

AU - Soo, Khee Chee

AU - Kim, Kyoung Mee

AU - Wong, Wai Keong

AU - Rozen, Steven G.

AU - Teh, Bin Tean

AU - Kappei, Dennis

AU - Lee, Jeeyun

AU - Connolly, John

AU - Tan, Patrick

PY - 2017

Y1 - 2017

N2 - Promoter elements play important roles in isoform and cell type-specific expression. We surveyed the epigenomic promoter landscape of gastric adenocarcinoma, analyzing 110 chromatin profiles (H3K4me3, H3K4me1, H3K27ac) of primary gastric cancers, gastric cancer lines, and nonmalignant gastric tissues. We identified nearly 2,000 promoter alterations (somatic promoters), many deregulated in various epithelial malignancies and mapping frequently to alternative promoters within the same gene, generating potential pro-oncogenic isoforms (RASA3). Somatic promoter- associated N-terminal peptides displaying relative depletion in tumors exhibited high-affinity MHC binding predictions and elicited potent T-cell responses in vitro, suggesting a mechanism for reducing tumor antigenicity. In multiple patient cohorts, gastric cancers with high somatic promoter usage also displayed reduced T-cell cytolytic marker expression. Somatic promoters are enriched in PRC2 occupancy, display sensitivity to EZH2 therapeutic inhibition, and are associated with novel cancer-associated transcripts. By generating tumor-specific isoforms and decreasing tumor antigenicity, epigenomic promoter alterations may thus drive intrinsic tumorigenesis and also allow nascent cancers to evade host immunity. SIGNIFICANCE: We apply epigenomic profiling to demarcate the promoter landscape of gastric cancer. Many tumor-specific promoters activate different promoters in the same gene, some generating pro-oncogenic isoforms. Tumor-specific promoters also reduce tumor antigenicity by causing relative depletion of immunogenic peptides, contributing to cancer immunoediting and allowing tumors to evade host immune attack.

AB - Promoter elements play important roles in isoform and cell type-specific expression. We surveyed the epigenomic promoter landscape of gastric adenocarcinoma, analyzing 110 chromatin profiles (H3K4me3, H3K4me1, H3K27ac) of primary gastric cancers, gastric cancer lines, and nonmalignant gastric tissues. We identified nearly 2,000 promoter alterations (somatic promoters), many deregulated in various epithelial malignancies and mapping frequently to alternative promoters within the same gene, generating potential pro-oncogenic isoforms (RASA3). Somatic promoter- associated N-terminal peptides displaying relative depletion in tumors exhibited high-affinity MHC binding predictions and elicited potent T-cell responses in vitro, suggesting a mechanism for reducing tumor antigenicity. In multiple patient cohorts, gastric cancers with high somatic promoter usage also displayed reduced T-cell cytolytic marker expression. Somatic promoters are enriched in PRC2 occupancy, display sensitivity to EZH2 therapeutic inhibition, and are associated with novel cancer-associated transcripts. By generating tumor-specific isoforms and decreasing tumor antigenicity, epigenomic promoter alterations may thus drive intrinsic tumorigenesis and also allow nascent cancers to evade host immunity. SIGNIFICANCE: We apply epigenomic profiling to demarcate the promoter landscape of gastric cancer. Many tumor-specific promoters activate different promoters in the same gene, some generating pro-oncogenic isoforms. Tumor-specific promoters also reduce tumor antigenicity by causing relative depletion of immunogenic peptides, contributing to cancer immunoediting and allowing tumors to evade host immune attack.

UR - http://www.scopus.com/inward/record.url?scp=85020420806&partnerID=8YFLogxK

U2 - 10.1158/2159-8290.CD-16-1022

DO - 10.1158/2159-8290.CD-16-1022

M3 - 文章

C2 - 28320776

AN - SCOPUS:85020420806

SN - 2159-8274

VL - 7

SP - 630

EP - 651

JO - Cancer Discovery

JF - Cancer Discovery

IS - 6

ER -

Epigenomic promoter alterations amplify gene isoform and immunogenic diversity in gastric adenocarcinoma

Abstract

Bibliographical note

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