Molecular and genetic characterization of MHC deficiency identifies ezh2 as therapeutic target for enhancing immune recognition

Daisuke Ennishi; Katsuyoshi Takata; Wendy Béguelin; Gerben Duns; Anja Mottok; Pedro Farinha; Ali Bashashati; Saeed Saberi; Merrill Boyle; Barbara Meissner; Susana Ben-Neriah; Bruce W. Woolcock; Adèle Telenius; Daniel Lai; Matt Teater; Robert Kridel; Kerry J. Savage; Laurie H. Sehn; Ryan D. Morin; Marco A. Marra; Sohrab P. Shah; Joseph M. Connors; Randy D. Gascoyne; David W. Scott; Ari M. Melnick; Christian Steidl

doi:10.1158/2159-8290.CD-18-1090

Molecular and genetic characterization of MHC deficiency identifies ezh2 as therapeutic target for enhancing immune recognition

Daisuke Ennishi, Katsuyoshi Takata, Wendy Béguelin, Gerben Duns, Anja Mottok, Pedro Farinha, Ali Bashashati, Saeed Saberi, Merrill Boyle, Barbara Meissner, Susana Ben-Neriah, Bruce W. Woolcock, Adèle Telenius, Daniel Lai, Matt Teater, Robert Kridel, Kerry J. Savage, Laurie H. Sehn, Ryan D. Morin, Marco A. MarraSohrab P. Shah, Joseph M. Connors, Randy D. Gascoyne, David W. Scott, Ari M. Melnick, Christian Steidl

研究成果 › 査読

146 被引用数 (Scopus)

抄録

We performed a genomic, transcriptomic, and immunophenotypic study of 347 patients with diffuse large B-cell lymphoma (DLBCL) to uncover the molecular basis underlying acquired deficiency of MHC expression. Low MHC-II expression defines tumors originating from the centroblast-rich dark zone of the germinal center (GC) that was associated with inferior prognosis. MHC-II-deficient tumors were characterized by somatically acquired gene mutations reducing MHC-II expression and a lower amount of tumor-infiltrating lymphocytes. In particular, we demonstrated a strong enrichment of EZH2 mutations in both MHC-I- and MHC-II-negative primary lymphomas, and observed reduced MHC expression and T-cell infiltrates in murine lymphoma models expressing mutant Ezh2 Y641. Of clinical relevance, EZH2 inhibitors significantly restored MHC expression in EZH2 -mutated human DLBCL cell lines. Hence, our findings suggest a tumor progression model of acquired immune escape in GC-derived lymphomas and pave the way for development of complementary therapeutic approaches combining immunotherapy with epigenetic reprogramming.

本文言語	English
ページ（範囲）	546-563
ページ数	18
ジャーナル	Cancer discovery
巻	9
号	4
DOI	https://doi.org/10.1158/2159-8290.CD-18-1090
出版ステータス	Published - 4月 2019
外部発表	はい

ASJC Scopus subject areas

腫瘍学

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10.1158/2159-8290.CD-18-1090

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引用スタイル

Ennishi, D., Takata, K., Béguelin, W., Duns, G., Mottok, A., Farinha, P., Bashashati, A., Saberi, S., Boyle, M., Meissner, B., Ben-Neriah, S., Woolcock, B. W., Telenius, A., Lai, D., Teater, M., Kridel, R., Savage, K. J., Sehn, L. H., Morin, R. D., ... Steidl, C. (2019). Molecular and genetic characterization of MHC deficiency identifies ezh2 as therapeutic target for enhancing immune recognition. Cancer discovery, 9(4), 546-563. https://doi.org/10.1158/2159-8290.CD-18-1090

Ennishi, D, Takata, K, Béguelin, W, Duns, G, Mottok, A, Farinha, P, Bashashati, A, Saberi, S, Boyle, M, Meissner, B, Ben-Neriah, S, Woolcock, BW, Telenius, A, Lai, D, Teater, M, Kridel, R, Savage, KJ, Sehn, LH, Morin, RD, Marra, MA, Shah, SP, Connors, JM, Gascoyne, RD, Scott, DW, Melnick, AM & Steidl, C 2019, 'Molecular and genetic characterization of MHC deficiency identifies ezh2 as therapeutic target for enhancing immune recognition', Cancer discovery, vol. 9, no. 4, pp. 546-563. https://doi.org/10.1158/2159-8290.CD-18-1090

@article{5119ff2f4a3d494ba576412877c24a97,

title = "Molecular and genetic characterization of MHC deficiency identifies ezh2 as therapeutic target for enhancing immune recognition",

abstract = "We performed a genomic, transcriptomic, and immunophenotypic study of 347 patients with diffuse large B-cell lymphoma (DLBCL) to uncover the molecular basis underlying acquired deficiency of MHC expression. Low MHC-II expression defines tumors originating from the centroblast-rich dark zone of the germinal center (GC) that was associated with inferior prognosis. MHC-II-deficient tumors were characterized by somatically acquired gene mutations reducing MHC-II expression and a lower amount of tumor-infiltrating lymphocytes. In particular, we demonstrated a strong enrichment of EZH2 mutations in both MHC-I- and MHC-II-negative primary lymphomas, and observed reduced MHC expression and T-cell infiltrates in murine lymphoma models expressing mutant Ezh2 Y641. Of clinical relevance, EZH2 inhibitors significantly restored MHC expression in EZH2 -mutated human DLBCL cell lines. Hence, our findings suggest a tumor progression model of acquired immune escape in GC-derived lymphomas and pave the way for development of complementary therapeutic approaches combining immunotherapy with epigenetic reprogramming.",

author = "Daisuke Ennishi and Katsuyoshi Takata and Wendy B{\'e}guelin and Gerben Duns and Anja Mottok and Pedro Farinha and Ali Bashashati and Saeed Saberi and Merrill Boyle and Barbara Meissner and Susana Ben-Neriah and Woolcock, {Bruce W.} and Ad{\`e}le Telenius and Daniel Lai and Matt Teater and Robert Kridel and Savage, {Kerry J.} and Sehn, {Laurie H.} and Morin, {Ryan D.} and Marra, {Marco A.} and Shah, {Sohrab P.} and Connors, {Joseph M.} and Gascoyne, {Randy D.} and Scott, {David W.} and Melnick, {Ari M.} and Christian Steidl",

note = "Funding Information: This study was supported by a Program Project Grant from the Terry Fox Research Institute (R.D. Gascoyne, Grant No. 1023; C. Steidl, Grant No. 1061). D. Ennishi was supported by fellowships from the Michael Smith Foundation for Health Research (MSFHR), Canadian Institutes of Health Research (CIHR), and the Japanese Society for The Promotion of Science. K. Takata was supported by fellowships from The Uehara Memorial Foundation. D.W. Scott is supported by the British Columbia Cancer Foundation (BCCF). J.M. Connors and C. Steidl received research funding support from the Terry Fox Research Institute, Genome Canada, Genome British Columbia, CIHR, and the BCCF. A. Mottok was supported by fellowships from the Mildred-Scheel-Cancer-Foundation (German Cancer Aid), the MSFHR, and Lymphoma Canada. R.D. Morin was funded by a CIHR New Investigator Award. M.A. Marra was pleased to acknowledge support from CIHR (FDN-143288) and the Terry Fox Research Institute. S. Shah holds the Canada Research Chair in Computational Cancer Genomics, is an MSFHR scholar, holds a CIHR Foundation grant, and acknowledges support from the BCCF. C. Steidl is supported by a Michael Smith Foundation for Health Research Investigator award. Funding Information: L.H. Sehn reports receiving honoraria from the speakers{\textquoteright} bureaus of Roche/Genentech, Janssen, Celgene, Apobiologix, AstraZeneca, Acerta, Takeda, TG Therapeutics, Teva, Kite, Merck, Amgen, Seattle Genetics, AbbVie, Morphosys, Karyopharm, Lundbeck, and Gilead. S.P. Shah has ownership interest (including stock, patents, etc.) in Contextual Genomics Inc. and is a consultant/advisory board member for the same. D.W. Scott reports receiving commercial research grants from Roche/Genentech, NanoString Technologies, and Jans-sen; and is a consultant/advisory board member for Janssen and Celgene. A.M. Melnick reports receiving commercial research grants from Janssen and GSK; has ownership interest (including stock, patents, etc.) in KDAC; and is a consultant/advisory board member for Janssen. C. Steidl reports receiving a commercial research grant from Bristol-Myers Squibb and is a consultant/advisory board member for Seattle Genetics and Roche. British Columbia Cancer has ownership interest in a patent licensed to NanoString technologies. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: {\textcopyright} 2019 American Association for Cancer Research.",

year = "2019",

month = apr,

doi = "10.1158/2159-8290.CD-18-1090",

language = "English",

volume = "9",

pages = "546--563",

journal = "Cancer Discovery",

issn = "2159-8274",

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

number = "4",

}

TY - JOUR

T1 - Molecular and genetic characterization of MHC deficiency identifies ezh2 as therapeutic target for enhancing immune recognition

AU - Ennishi, Daisuke

AU - Takata, Katsuyoshi

AU - Béguelin, Wendy

AU - Duns, Gerben

AU - Mottok, Anja

AU - Farinha, Pedro

AU - Bashashati, Ali

AU - Saberi, Saeed

AU - Boyle, Merrill

AU - Meissner, Barbara

AU - Ben-Neriah, Susana

AU - Woolcock, Bruce W.

AU - Telenius, Adèle

AU - Lai, Daniel

AU - Teater, Matt

AU - Kridel, Robert

AU - Savage, Kerry J.

AU - Sehn, Laurie H.

AU - Morin, Ryan D.

AU - Marra, Marco A.

AU - Shah, Sohrab P.

AU - Connors, Joseph M.

AU - Gascoyne, Randy D.

AU - Scott, David W.

AU - Melnick, Ari M.

AU - Steidl, Christian

N1 - Funding Information: This study was supported by a Program Project Grant from the Terry Fox Research Institute (R.D. Gascoyne, Grant No. 1023; C. Steidl, Grant No. 1061). D. Ennishi was supported by fellowships from the Michael Smith Foundation for Health Research (MSFHR), Canadian Institutes of Health Research (CIHR), and the Japanese Society for The Promotion of Science. K. Takata was supported by fellowships from The Uehara Memorial Foundation. D.W. Scott is supported by the British Columbia Cancer Foundation (BCCF). J.M. Connors and C. Steidl received research funding support from the Terry Fox Research Institute, Genome Canada, Genome British Columbia, CIHR, and the BCCF. A. Mottok was supported by fellowships from the Mildred-Scheel-Cancer-Foundation (German Cancer Aid), the MSFHR, and Lymphoma Canada. R.D. Morin was funded by a CIHR New Investigator Award. M.A. Marra was pleased to acknowledge support from CIHR (FDN-143288) and the Terry Fox Research Institute. S. Shah holds the Canada Research Chair in Computational Cancer Genomics, is an MSFHR scholar, holds a CIHR Foundation grant, and acknowledges support from the BCCF. C. Steidl is supported by a Michael Smith Foundation for Health Research Investigator award. Funding Information: L.H. Sehn reports receiving honoraria from the speakers’ bureaus of Roche/Genentech, Janssen, Celgene, Apobiologix, AstraZeneca, Acerta, Takeda, TG Therapeutics, Teva, Kite, Merck, Amgen, Seattle Genetics, AbbVie, Morphosys, Karyopharm, Lundbeck, and Gilead. S.P. Shah has ownership interest (including stock, patents, etc.) in Contextual Genomics Inc. and is a consultant/advisory board member for the same. D.W. Scott reports receiving commercial research grants from Roche/Genentech, NanoString Technologies, and Jans-sen; and is a consultant/advisory board member for Janssen and Celgene. A.M. Melnick reports receiving commercial research grants from Janssen and GSK; has ownership interest (including stock, patents, etc.) in KDAC; and is a consultant/advisory board member for Janssen. C. Steidl reports receiving a commercial research grant from Bristol-Myers Squibb and is a consultant/advisory board member for Seattle Genetics and Roche. British Columbia Cancer has ownership interest in a patent licensed to NanoString technologies. No potential conflicts of interest were disclosed by the other authors. Publisher Copyright: © 2019 American Association for Cancer Research.

PY - 2019/4

Y1 - 2019/4

N2 - We performed a genomic, transcriptomic, and immunophenotypic study of 347 patients with diffuse large B-cell lymphoma (DLBCL) to uncover the molecular basis underlying acquired deficiency of MHC expression. Low MHC-II expression defines tumors originating from the centroblast-rich dark zone of the germinal center (GC) that was associated with inferior prognosis. MHC-II-deficient tumors were characterized by somatically acquired gene mutations reducing MHC-II expression and a lower amount of tumor-infiltrating lymphocytes. In particular, we demonstrated a strong enrichment of EZH2 mutations in both MHC-I- and MHC-II-negative primary lymphomas, and observed reduced MHC expression and T-cell infiltrates in murine lymphoma models expressing mutant Ezh2 Y641. Of clinical relevance, EZH2 inhibitors significantly restored MHC expression in EZH2 -mutated human DLBCL cell lines. Hence, our findings suggest a tumor progression model of acquired immune escape in GC-derived lymphomas and pave the way for development of complementary therapeutic approaches combining immunotherapy with epigenetic reprogramming.

AB - We performed a genomic, transcriptomic, and immunophenotypic study of 347 patients with diffuse large B-cell lymphoma (DLBCL) to uncover the molecular basis underlying acquired deficiency of MHC expression. Low MHC-II expression defines tumors originating from the centroblast-rich dark zone of the germinal center (GC) that was associated with inferior prognosis. MHC-II-deficient tumors were characterized by somatically acquired gene mutations reducing MHC-II expression and a lower amount of tumor-infiltrating lymphocytes. In particular, we demonstrated a strong enrichment of EZH2 mutations in both MHC-I- and MHC-II-negative primary lymphomas, and observed reduced MHC expression and T-cell infiltrates in murine lymphoma models expressing mutant Ezh2 Y641. Of clinical relevance, EZH2 inhibitors significantly restored MHC expression in EZH2 -mutated human DLBCL cell lines. Hence, our findings suggest a tumor progression model of acquired immune escape in GC-derived lymphomas and pave the way for development of complementary therapeutic approaches combining immunotherapy with epigenetic reprogramming.

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