PRMT5 interacts with the BCL6 oncoprotein and is required for germinal center formation and lymphoma cell survival

Xiaoqing Lu; Tharu M. Fernando; Chen Lossos; Nevin Yusufova; Fan Liu; Lorena Fontán; Matthew Durant; Huimin Geng; Jacob Melnick; Yuan Luo; Francisco Vega; Vincent Moy; Giorgio Inghirami; Stephen Nimer; Ari M. Melnick; Izidore S. Lossos

doi:10.1182/blood-2018-02-831438

PRMT5 interacts with the BCL6 oncoprotein and is required for germinal center formation and lymphoma cell survival

Xiaoqing Lu, Tharu M. Fernando, Chen Lossos, Nevin Yusufova, Fan Liu, Lorena Fontán, Matthew Durant, Huimin Geng, Jacob Melnick, Yuan Luo, Francisco Vega, Vincent Moy, Giorgio Inghirami, Stephen Nimer, Ari M. Melnick, Izidore S. Lossos

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

49 Scopus citations

Abstract

The germinal center (GC) reaction plays an important role in generating humoral immunity and is believed to give rise to most B-cell lymphomas. GC entry and exit are tightly regulated processes, controlled by the actions of transcription factors such as BCL6. Herein, we demonstrate that protein arginine methyltransferase 5 (PRMT5), a symmetric dimethyl arginine methyltransferase, is also necessary for GC formation and affinity maturation. PRMT5 contributes to GC formation and affinity maturation at least in part through its direct interaction with and methylation of BCL6 at arginine 305 (R305), a modification necessary for the full transcriptional repressive effects of BCL6. Inhibition of PRMT5 in B-cell lymphoma lines led to significant upregulation of BCL6 target genes, and the concomitant inhibition of both BCL6 and PRMT5 exhibited synergistic killing of BCL6- expressing lymphoma cells. Our studies identify PRMT5 as a novel regulator of the GC reaction and highlight the mechanistic rationale of cotargeting PRMT5 and BCL6 in lymphoma.

Original language	English (US)
Pages (from-to)	2026-2039
Number of pages	14
Journal	Blood
Volume	132
Issue number	19
DOIs	https://doi.org/10.1182/blood-2018-02-831438
State	Published - Nov 8 2018
Externally published	Yes

ASJC Scopus subject areas

Biochemistry
Immunology
Hematology
Cell Biology

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Lu, X., Fernando, T. M., Lossos, C., Yusufova, N., Liu, F., Fontán, L., Durant, M., Geng, H., Melnick, J., Luo, Y., Vega, F., Moy, V., Inghirami, G., Nimer, S., Melnick, A. M., & Lossos, I. S. (2018). PRMT5 interacts with the BCL6 oncoprotein and is required for germinal center formation and lymphoma cell survival. Blood, 132(19), 2026-2039. https://doi.org/10.1182/blood-2018-02-831438

Lu, X, Fernando, TM, Lossos, C, Yusufova, N, Liu, F, Fontán, L, Durant, M, Geng, H, Melnick, J, Luo, Y, Vega, F, Moy, V, Inghirami, G, Nimer, S, Melnick, AM & Lossos, IS 2018, 'PRMT5 interacts with the BCL6 oncoprotein and is required for germinal center formation and lymphoma cell survival', Blood, vol. 132, no. 19, pp. 2026-2039. https://doi.org/10.1182/blood-2018-02-831438

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title = "PRMT5 interacts with the BCL6 oncoprotein and is required for germinal center formation and lymphoma cell survival",

abstract = "The germinal center (GC) reaction plays an important role in generating humoral immunity and is believed to give rise to most B-cell lymphomas. GC entry and exit are tightly regulated processes, controlled by the actions of transcription factors such as BCL6. Herein, we demonstrate that protein arginine methyltransferase 5 (PRMT5), a symmetric dimethyl arginine methyltransferase, is also necessary for GC formation and affinity maturation. PRMT5 contributes to GC formation and affinity maturation at least in part through its direct interaction with and methylation of BCL6 at arginine 305 (R305), a modification necessary for the full transcriptional repressive effects of BCL6. Inhibition of PRMT5 in B-cell lymphoma lines led to significant upregulation of BCL6 target genes, and the concomitant inhibition of both BCL6 and PRMT5 exhibited synergistic killing of BCL6- expressing lymphoma cells. Our studies identify PRMT5 as a novel regulator of the GC reaction and highlight the mechanistic rationale of cotargeting PRMT5 and BCL6 in lymphoma.",

author = "Xiaoqing Lu and Fernando, {Tharu M.} and Chen Lossos and Nevin Yusufova and Fan Liu and Lorena Font{\'a}n and Matthew Durant and Huimin Geng and Jacob Melnick and Yuan Luo and Francisco Vega and Vincent Moy and Giorgio Inghirami and Stephen Nimer and Melnick, {Ari M.} and Lossos, {Izidore S.}",

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doi = "10.1182/blood-2018-02-831438",

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AU - Lu, Xiaoqing

AU - Fernando, Tharu M.

AU - Lossos, Chen

AU - Yusufova, Nevin

AU - Liu, Fan

AU - Fontán, Lorena

AU - Durant, Matthew

AU - Geng, Huimin

AU - Melnick, Jacob

AU - Luo, Yuan

AU - Vega, Francisco

AU - Moy, Vincent

AU - Inghirami, Giorgio

AU - Nimer, Stephen

AU - Melnick, Ari M.

AU - Lossos, Izidore S.

PY - 2018/11/8

Y1 - 2018/11/8

N2 - The germinal center (GC) reaction plays an important role in generating humoral immunity and is believed to give rise to most B-cell lymphomas. GC entry and exit are tightly regulated processes, controlled by the actions of transcription factors such as BCL6. Herein, we demonstrate that protein arginine methyltransferase 5 (PRMT5), a symmetric dimethyl arginine methyltransferase, is also necessary for GC formation and affinity maturation. PRMT5 contributes to GC formation and affinity maturation at least in part through its direct interaction with and methylation of BCL6 at arginine 305 (R305), a modification necessary for the full transcriptional repressive effects of BCL6. Inhibition of PRMT5 in B-cell lymphoma lines led to significant upregulation of BCL6 target genes, and the concomitant inhibition of both BCL6 and PRMT5 exhibited synergistic killing of BCL6- expressing lymphoma cells. Our studies identify PRMT5 as a novel regulator of the GC reaction and highlight the mechanistic rationale of cotargeting PRMT5 and BCL6 in lymphoma.

AB - The germinal center (GC) reaction plays an important role in generating humoral immunity and is believed to give rise to most B-cell lymphomas. GC entry and exit are tightly regulated processes, controlled by the actions of transcription factors such as BCL6. Herein, we demonstrate that protein arginine methyltransferase 5 (PRMT5), a symmetric dimethyl arginine methyltransferase, is also necessary for GC formation and affinity maturation. PRMT5 contributes to GC formation and affinity maturation at least in part through its direct interaction with and methylation of BCL6 at arginine 305 (R305), a modification necessary for the full transcriptional repressive effects of BCL6. Inhibition of PRMT5 in B-cell lymphoma lines led to significant upregulation of BCL6 target genes, and the concomitant inhibition of both BCL6 and PRMT5 exhibited synergistic killing of BCL6- expressing lymphoma cells. Our studies identify PRMT5 as a novel regulator of the GC reaction and highlight the mechanistic rationale of cotargeting PRMT5 and BCL6 in lymphoma.

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PRMT5 interacts with the BCL6 oncoprotein and is required for germinal center formation and lymphoma cell survival

Abstract

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