CREBBP inactivation promotes the development of HDAC3-dependent lymphomas

Yanwen Jiang; Ana Ortega-Molina; Huimin Geng; Hsia Yuan Ying; Katerina Hatzi; Sara Parsa; Dylan McNally; Ling Wang; Ashley S. Doane; Xabier Agirre; Matt Teater; Cem Meydan; Zhuoning Li; David Poloway; Shenqiu Wang; Daisuke Ennishi; David W. Scott; Kristy R. Stengel; Janice E. Kranz; Edward Holson; Sneh Sharma; James W. Young; Chi Shuen Chu; Robert G. Roeder; Rita Shaknovich; Scott W. Hiebert; Randy D. Gascoyne; Wayne Tam; Olivier Elemento; Hans Guido Wendel; Ari M. Melnick

doi:10.1158/2159-8290.CD-16-0975

CREBBP inactivation promotes the development of HDAC3-dependent lymphomas

Yanwen Jiang, Ana Ortega-Molina, Huimin Geng, Hsia Yuan Ying, Katerina Hatzi, Sara Parsa, Dylan McNally, Ling Wang, Ashley S. Doane, Xabier Agirre, Matt Teater, Cem Meydan, Zhuoning Li, David Poloway, Shenqiu Wang, Daisuke Ennishi, David W. Scott, Kristy R. Stengel, Janice E. Kranz, Edward HolsonSneh Sharma, James W. Young, Chi Shuen Chu, Robert G. Roeder, Rita Shaknovich, Scott W. Hiebert, Randy D. Gascoyne, Wayne Tam, Olivier Elemento, Hans Guido Wendel, Ari M. Melnick

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

189 Scopus citations

Abstract

Somatic mutations in CREBBP occur frequently in B-cell lymphoma. Here, we show that loss of CREBBP facilitates the development of germinal center (GC)–derived lymphomas in mice. In both human and murine lymphomas, CREBBP loss-of-function resulted in focal depletion of enhancer H3K27 acetylation and aberrant transcriptional silencing of genes that regulate B-cell signaling and immune responses, including class II MHC. Mechanistically, CREBBP-regulated enhancers are counter-regulated by the BCL6 transcriptional repressor in a complex with SMRT and HDAC3, which we found to bind extensively to MHC class II loci. HDAC3 loss-of-function rescued repression of these enhancers and corresponding genes, including MHC class II, and more profoundly suppressed CREBBP -mutant lymphomas in vitro and in vivo. Hence, CREBBP loss-of-function contributes to lymphomagenesis by enabling unopposed suppression of enhancers by BCL6/SMRT/HDAC3 complexes, suggesting HDAC3-targeted therapy as a precision approach for CREBBP -mutant lymphomas. SIGNIFICANCE: Our fi ndings establish the tumor suppressor function of CREBBP in GC lymphomas in which CREBBP mutations disable acetylation and result in unopposed deacetylation by BCL6/SMRT/ HDAC3 complexes at enhancers of B-cell signaling and immune response genes. Hence, inhibition of HDAC3 can restore the enhancer histone acetylation and may serve as a targeted therapy for CREBBP - mutant lymphomas.

Original language	English (US)
Pages (from-to)	38-53
Number of pages	16
Journal	Cancer discovery
Volume	7
Issue number	1
DOIs	https://doi.org/10.1158/2159-8290.CD-16-0975
State	Published - Jan 2017
Externally published	Yes

ASJC Scopus subject areas

Oncology

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10.1158/2159-8290.CD-16-0975

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Jiang, Y., Ortega-Molina, A., Geng, H., Ying, H. Y., Hatzi, K., Parsa, S., McNally, D., Wang, L., Doane, A. S., Agirre, X., Teater, M., Meydan, C., Li, Z., Poloway, D., Wang, S., Ennishi, D., Scott, D. W., Stengel, K. R., Kranz, J. E., ... Melnick, A. M. (2017). CREBBP inactivation promotes the development of HDAC3-dependent lymphomas. Cancer discovery, 7(1), 38-53. https://doi.org/10.1158/2159-8290.CD-16-0975

Jiang, Y, Ortega-Molina, A, Geng, H, Ying, HY, Hatzi, K, Parsa, S, McNally, D, Wang, L, Doane, AS, Agirre, X, Teater, M, Meydan, C, Li, Z, Poloway, D, Wang, S, Ennishi, D, Scott, DW, Stengel, KR, Kranz, JE, Holson, E, Sharma, S, Young, JW, Chu, CS, Roeder, RG, Shaknovich, R, Hiebert, SW, Gascoyne, RD, Tam, W, Elemento, O, Wendel, HG & Melnick, AM 2017, 'CREBBP inactivation promotes the development of HDAC3-dependent lymphomas', Cancer discovery, vol. 7, no. 1, pp. 38-53. https://doi.org/10.1158/2159-8290.CD-16-0975

@article{39bc2be3eaf34327ae65ded9815de03d,

title = "CREBBP inactivation promotes the development of HDAC3-dependent lymphomas",

abstract = "Somatic mutations in CREBBP occur frequently in B-cell lymphoma. Here, we show that loss of CREBBP facilitates the development of germinal center (GC)–derived lymphomas in mice. In both human and murine lymphomas, CREBBP loss-of-function resulted in focal depletion of enhancer H3K27 acetylation and aberrant transcriptional silencing of genes that regulate B-cell signaling and immune responses, including class II MHC. Mechanistically, CREBBP-regulated enhancers are counter-regulated by the BCL6 transcriptional repressor in a complex with SMRT and HDAC3, which we found to bind extensively to MHC class II loci. HDAC3 loss-of-function rescued repression of these enhancers and corresponding genes, including MHC class II, and more profoundly suppressed CREBBP -mutant lymphomas in vitro and in vivo. Hence, CREBBP loss-of-function contributes to lymphomagenesis by enabling unopposed suppression of enhancers by BCL6/SMRT/HDAC3 complexes, suggesting HDAC3-targeted therapy as a precision approach for CREBBP -mutant lymphomas. SIGNIFICANCE: Our fi ndings establish the tumor suppressor function of CREBBP in GC lymphomas in which CREBBP mutations disable acetylation and result in unopposed deacetylation by BCL6/SMRT/ HDAC3 complexes at enhancers of B-cell signaling and immune response genes. Hence, inhibition of HDAC3 can restore the enhancer histone acetylation and may serve as a targeted therapy for CREBBP - mutant lymphomas.",

author = "Yanwen Jiang and Ana Ortega-Molina and Huimin Geng and Ying, {Hsia Yuan} and Katerina Hatzi and Sara Parsa and Dylan McNally and Ling Wang and Doane, {Ashley S.} and Xabier Agirre and Matt Teater and Cem Meydan and Zhuoning Li and David Poloway and Shenqiu Wang and Daisuke Ennishi and Scott, {David W.} and Stengel, {Kristy R.} and Kranz, {Janice E.} and Edward Holson and Sneh Sharma and Young, {James W.} and Chu, {Chi Shuen} and Roeder, {Robert G.} and Rita Shaknovich and Hiebert, {Scott W.} and Gascoyne, {Randy D.} and Wayne Tam and Olivier Elemento and Wendel, {Hans Guido} and Melnick, {Ari M.}",

note = "Funding Information: Y. Jiang was a Scholar of the American Society of Hematology. A. Ortega-Molina is supported by funding from The Leukemia & Lymphoma Society. H. Geng is supported by a Junior Investigator award from the UCSF Academic Senate. H.-Y. Ying is supported by the 2016 AACR-Takeda Oncology Fellowship in Lymphoma Research (grant number 16-40-38 -YING), and was supported by the Ministry of Science and Technology, Republic of China. S. Wang is supported by a postdoctoral fellowship from the Swedish Research Council (VR) and by the 2015 AACR-Millennium Fellowship in Lymphoma Research (grant number 15-40-38 -WANG). D. Ennishi, D.W. Scott, and R.D. Gascoyne are supported by a Terry Fox Program Project grant (grant number 1023). D.W. Scott is also funded by the BC Cancer Foundation. S. Sharma and J.W. Young are supported by P01 CA23766 from the National Cancer Institute, NIH and Swim Across America. C.-S. Chu was supported by a fellowship from the Ministry of Science and Technology, Republic of China. R.G. Roeder was supported by NIH grant R01CA178765. O. Elemento is supported by NSF CAREER and R01 CA194547. S.W. Hiebert is supported by NCI R01-CA164605. H.G. Wendel is supported by the American Cancer Society grant RSG-13- 048-01-LIB, the Lymphoma Research Foundation, Cycle for Survival, Functional Genomics Initiative, W.H. Goodwin and A. Goodwin and the Commonwealth Foundation for Cancer Research, Steven Greenberg, the Center for Experimental Therapeutics at Memorial Sloan Kettering Cancer Center, NIH grants RO1CA183876-01 and 1R01CA19038-01 and Core Grant P30 CA008748 and P50 CA192937-01A1. H.G. Wendel is a Scholar of the Leukemia and Lymphoma Society and is supported by an LLS SCOR. A.M. Melnick is supported by NIH R01 CA187109, LLS TRP 6457-15, LLS SCOR#7012-16, and the Chemotherapy Foundation. Publisher Copyright: {\textcopyright} 2017 American Association for Cancer Research.",

year = "2017",

month = jan,

doi = "10.1158/2159-8290.CD-16-0975",

language = "English (US)",

volume = "7",

pages = "38--53",

journal = "Cancer discovery",

issn = "2159-8274",

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

number = "1",

}

TY - JOUR

T1 - CREBBP inactivation promotes the development of HDAC3-dependent lymphomas

AU - Jiang, Yanwen

AU - Ortega-Molina, Ana

AU - Geng, Huimin

AU - Ying, Hsia Yuan

AU - Hatzi, Katerina

AU - Parsa, Sara

AU - McNally, Dylan

AU - Wang, Ling

AU - Doane, Ashley S.

AU - Agirre, Xabier

AU - Teater, Matt

AU - Meydan, Cem

AU - Li, Zhuoning

AU - Poloway, David

AU - Wang, Shenqiu

AU - Ennishi, Daisuke

AU - Scott, David W.

AU - Stengel, Kristy R.

AU - Kranz, Janice E.

AU - Holson, Edward

AU - Sharma, Sneh

AU - Young, James W.

AU - Chu, Chi Shuen

AU - Roeder, Robert G.

AU - Shaknovich, Rita

AU - Hiebert, Scott W.

AU - Gascoyne, Randy D.

AU - Tam, Wayne

AU - Elemento, Olivier

AU - Wendel, Hans Guido

AU - Melnick, Ari M.

N1 - Funding Information: Y. Jiang was a Scholar of the American Society of Hematology. A. Ortega-Molina is supported by funding from The Leukemia & Lymphoma Society. H. Geng is supported by a Junior Investigator award from the UCSF Academic Senate. H.-Y. Ying is supported by the 2016 AACR-Takeda Oncology Fellowship in Lymphoma Research (grant number 16-40-38 -YING), and was supported by the Ministry of Science and Technology, Republic of China. S. Wang is supported by a postdoctoral fellowship from the Swedish Research Council (VR) and by the 2015 AACR-Millennium Fellowship in Lymphoma Research (grant number 15-40-38 -WANG). D. Ennishi, D.W. Scott, and R.D. Gascoyne are supported by a Terry Fox Program Project grant (grant number 1023). D.W. Scott is also funded by the BC Cancer Foundation. S. Sharma and J.W. Young are supported by P01 CA23766 from the National Cancer Institute, NIH and Swim Across America. C.-S. Chu was supported by a fellowship from the Ministry of Science and Technology, Republic of China. R.G. Roeder was supported by NIH grant R01CA178765. O. Elemento is supported by NSF CAREER and R01 CA194547. S.W. Hiebert is supported by NCI R01-CA164605. H.G. Wendel is supported by the American Cancer Society grant RSG-13- 048-01-LIB, the Lymphoma Research Foundation, Cycle for Survival, Functional Genomics Initiative, W.H. Goodwin and A. Goodwin and the Commonwealth Foundation for Cancer Research, Steven Greenberg, the Center for Experimental Therapeutics at Memorial Sloan Kettering Cancer Center, NIH grants RO1CA183876-01 and 1R01CA19038-01 and Core Grant P30 CA008748 and P50 CA192937-01A1. H.G. Wendel is a Scholar of the Leukemia and Lymphoma Society and is supported by an LLS SCOR. A.M. Melnick is supported by NIH R01 CA187109, LLS TRP 6457-15, LLS SCOR#7012-16, and the Chemotherapy Foundation. Publisher Copyright: © 2017 American Association for Cancer Research.

PY - 2017/1

Y1 - 2017/1

N2 - Somatic mutations in CREBBP occur frequently in B-cell lymphoma. Here, we show that loss of CREBBP facilitates the development of germinal center (GC)–derived lymphomas in mice. In both human and murine lymphomas, CREBBP loss-of-function resulted in focal depletion of enhancer H3K27 acetylation and aberrant transcriptional silencing of genes that regulate B-cell signaling and immune responses, including class II MHC. Mechanistically, CREBBP-regulated enhancers are counter-regulated by the BCL6 transcriptional repressor in a complex with SMRT and HDAC3, which we found to bind extensively to MHC class II loci. HDAC3 loss-of-function rescued repression of these enhancers and corresponding genes, including MHC class II, and more profoundly suppressed CREBBP -mutant lymphomas in vitro and in vivo. Hence, CREBBP loss-of-function contributes to lymphomagenesis by enabling unopposed suppression of enhancers by BCL6/SMRT/HDAC3 complexes, suggesting HDAC3-targeted therapy as a precision approach for CREBBP -mutant lymphomas. SIGNIFICANCE: Our fi ndings establish the tumor suppressor function of CREBBP in GC lymphomas in which CREBBP mutations disable acetylation and result in unopposed deacetylation by BCL6/SMRT/ HDAC3 complexes at enhancers of B-cell signaling and immune response genes. Hence, inhibition of HDAC3 can restore the enhancer histone acetylation and may serve as a targeted therapy for CREBBP - mutant lymphomas.

AB - Somatic mutations in CREBBP occur frequently in B-cell lymphoma. Here, we show that loss of CREBBP facilitates the development of germinal center (GC)–derived lymphomas in mice. In both human and murine lymphomas, CREBBP loss-of-function resulted in focal depletion of enhancer H3K27 acetylation and aberrant transcriptional silencing of genes that regulate B-cell signaling and immune responses, including class II MHC. Mechanistically, CREBBP-regulated enhancers are counter-regulated by the BCL6 transcriptional repressor in a complex with SMRT and HDAC3, which we found to bind extensively to MHC class II loci. HDAC3 loss-of-function rescued repression of these enhancers and corresponding genes, including MHC class II, and more profoundly suppressed CREBBP -mutant lymphomas in vitro and in vivo. Hence, CREBBP loss-of-function contributes to lymphomagenesis by enabling unopposed suppression of enhancers by BCL6/SMRT/HDAC3 complexes, suggesting HDAC3-targeted therapy as a precision approach for CREBBP -mutant lymphomas. SIGNIFICANCE: Our fi ndings establish the tumor suppressor function of CREBBP in GC lymphomas in which CREBBP mutations disable acetylation and result in unopposed deacetylation by BCL6/SMRT/ HDAC3 complexes at enhancers of B-cell signaling and immune response genes. Hence, inhibition of HDAC3 can restore the enhancer histone acetylation and may serve as a targeted therapy for CREBBP - mutant lymphomas.

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JO - Cancer discovery

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CREBBP inactivation promotes the development of HDAC3-dependent lymphomas

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