SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions

Qing Deng; Priya Lakra; Panhong Gou; Haopeng Yang; Cem Meydan; Matthew Teater; Christopher Chin; Wenchao Zhang; Tommy Dinh; Usama Hussein; Xubin Li; Estela Rojas; Weiguang Liu; Patrick K. Reville; Atish Kizhakeyil; Darko Barisic; Sydney Parsons; Ashley Wilson; Jared Henderson; Brooks Scull; Channabasavaiah Gurumurthy; Francisco Vega; Amy Chadburn; Branko Cuglievan; Nader Kim El-Mallawany; Carl Allen; Christopher Mason; Ari Melnick; Michael R. Green

doi:10.1016/j.ccell.2024.02.011

SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions

Qing Deng, Priya Lakra, Panhong Gou, Haopeng Yang, Cem Meydan, Matthew Teater, Christopher Chin, Wenchao Zhang, Tommy Dinh, Usama Hussein, Xubin Li, Estela Rojas, Weiguang Liu, Patrick K. Reville, Atish Kizhakeyil, Darko Barisic, Sydney Parsons, Ashley Wilson, Jared Henderson, Brooks ScullChannabasavaiah Gurumurthy, Francisco Vega, Amy Chadburn, Branko Cuglievan, Nader Kim El-Mallawany, Carl Allen, Christopher Mason, Ari Melnick, Michael R. Green

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

2 Scopus citations

Abstract

SMARCA4 encodes one of two mutually exclusive ATPase subunits in the BRG/BRM associated factor (BAF) complex that is recruited by transcription factors (TFs) to drive chromatin accessibility and transcriptional activation. SMARCA4 is among the most recurrently mutated genes in human cancer, including ∼30% of germinal center (GC)-derived Burkitt lymphomas. In mice, GC-specific Smarca4 haploinsufficiency cooperated with MYC over-expression to drive lymphomagenesis. Furthermore, monoallelic Smarca4 deletion drove GC hyperplasia with centroblast polarization via significantly increased rates of centrocyte recycling to the dark zone. Mechanistically, Smarca4 loss reduced the activity of TFs that are activated in centrocytes to drive GC-exit, including SPI1 (PU.1), IRF family, and NF-κB. Loss of activity for these factors phenocopied aberrant BCL6 activity within murine centrocytes and human Burkitt lymphoma cells. SMARCA4 therefore facilitates chromatin accessibility for TFs that shape centrocyte trajectories, and loss of fine-control of these programs biases toward centroblast cell-fate, GC hyperplasia and lymphoma.

Original language	English (US)
Pages (from-to)	605-622.e11
Journal	Cancer cell
Volume	42
Issue number	4
DOIs	https://doi.org/10.1016/j.ccell.2024.02.011
State	Published - Apr 8 2024

Keywords

B-cell
BAF
epigenetics
germinal center
immunology
lymphoma
SMARCA4
SWI/SNF
transcription

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1016/j.ccell.2024.02.011

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Deng, Q., Lakra, P., Gou, P., Yang, H., Meydan, C., Teater, M., Chin, C., Zhang, W., Dinh, T., Hussein, U., Li, X., Rojas, E., Liu, W., Reville, P. K., Kizhakeyil, A., Barisic, D., Parsons, S., Wilson, A., Henderson, J., ... Green, M. R. (2024). SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions. Cancer cell, 42(4), 605-622.e11. https://doi.org/10.1016/j.ccell.2024.02.011

Deng, Q, Lakra, P, Gou, P, Yang, H, Meydan, C, Teater, M, Chin, C, Zhang, W, Dinh, T, Hussein, U, Li, X, Rojas, E, Liu, W, Reville, PK, Kizhakeyil, A, Barisic, D, Parsons, S, Wilson, A, Henderson, J, Scull, B, Gurumurthy, C, Vega, F, Chadburn, A, Cuglievan, B, El-Mallawany, NK, Allen, C, Mason, C, Melnick, A & Green, MR 2024, 'SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions', Cancer cell, vol. 42, no. 4, pp. 605-622.e11. https://doi.org/10.1016/j.ccell.2024.02.011

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title = "SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions",

abstract = "SMARCA4 encodes one of two mutually exclusive ATPase subunits in the BRG/BRM associated factor (BAF) complex that is recruited by transcription factors (TFs) to drive chromatin accessibility and transcriptional activation. SMARCA4 is among the most recurrently mutated genes in human cancer, including ∼30% of germinal center (GC)-derived Burkitt lymphomas. In mice, GC-specific Smarca4 haploinsufficiency cooperated with MYC over-expression to drive lymphomagenesis. Furthermore, monoallelic Smarca4 deletion drove GC hyperplasia with centroblast polarization via significantly increased rates of centrocyte recycling to the dark zone. Mechanistically, Smarca4 loss reduced the activity of TFs that are activated in centrocytes to drive GC-exit, including SPI1 (PU.1), IRF family, and NF-κB. Loss of activity for these factors phenocopied aberrant BCL6 activity within murine centrocytes and human Burkitt lymphoma cells. SMARCA4 therefore facilitates chromatin accessibility for TFs that shape centrocyte trajectories, and loss of fine-control of these programs biases toward centroblast cell-fate, GC hyperplasia and lymphoma.",

keywords = "B-cell, BAF, epigenetics, germinal center, immunology, lymphoma, SMARCA4, SWI/SNF, transcription",

author = "Qing Deng and Priya Lakra and Panhong Gou and Haopeng Yang and Cem Meydan and Matthew Teater and Christopher Chin and Wenchao Zhang and Tommy Dinh and Usama Hussein and Xubin Li and Estela Rojas and Weiguang Liu and Reville, {Patrick K.} and Atish Kizhakeyil and Darko Barisic and Sydney Parsons and Ashley Wilson and Jared Henderson and Brooks Scull and Channabasavaiah Gurumurthy and Francisco Vega and Amy Chadburn and Branko Cuglievan and El-Mallawany, {Nader Kim} and Carl Allen and Christopher Mason and Ari Melnick and Green, {Michael R.}",

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year = "2024",

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doi = "10.1016/j.ccell.2024.02.011",

language = "English (US)",

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T1 - SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions

AU - Deng, Qing

AU - Lakra, Priya

AU - Gou, Panhong

AU - Yang, Haopeng

AU - Meydan, Cem

AU - Teater, Matthew

AU - Chin, Christopher

AU - Zhang, Wenchao

AU - Dinh, Tommy

AU - Hussein, Usama

AU - Li, Xubin

AU - Rojas, Estela

AU - Liu, Weiguang

AU - Reville, Patrick K.

AU - Kizhakeyil, Atish

AU - Barisic, Darko

AU - Parsons, Sydney

AU - Wilson, Ashley

AU - Henderson, Jared

AU - Scull, Brooks

AU - Gurumurthy, Channabasavaiah

AU - Vega, Francisco

AU - Chadburn, Amy

AU - Cuglievan, Branko

AU - El-Mallawany, Nader Kim

AU - Allen, Carl

AU - Mason, Christopher

AU - Melnick, Ari

AU - Green, Michael R.

PY - 2024/4/8

Y1 - 2024/4/8

N2 - SMARCA4 encodes one of two mutually exclusive ATPase subunits in the BRG/BRM associated factor (BAF) complex that is recruited by transcription factors (TFs) to drive chromatin accessibility and transcriptional activation. SMARCA4 is among the most recurrently mutated genes in human cancer, including ∼30% of germinal center (GC)-derived Burkitt lymphomas. In mice, GC-specific Smarca4 haploinsufficiency cooperated with MYC over-expression to drive lymphomagenesis. Furthermore, monoallelic Smarca4 deletion drove GC hyperplasia with centroblast polarization via significantly increased rates of centrocyte recycling to the dark zone. Mechanistically, Smarca4 loss reduced the activity of TFs that are activated in centrocytes to drive GC-exit, including SPI1 (PU.1), IRF family, and NF-κB. Loss of activity for these factors phenocopied aberrant BCL6 activity within murine centrocytes and human Burkitt lymphoma cells. SMARCA4 therefore facilitates chromatin accessibility for TFs that shape centrocyte trajectories, and loss of fine-control of these programs biases toward centroblast cell-fate, GC hyperplasia and lymphoma.

AB - SMARCA4 encodes one of two mutually exclusive ATPase subunits in the BRG/BRM associated factor (BAF) complex that is recruited by transcription factors (TFs) to drive chromatin accessibility and transcriptional activation. SMARCA4 is among the most recurrently mutated genes in human cancer, including ∼30% of germinal center (GC)-derived Burkitt lymphomas. In mice, GC-specific Smarca4 haploinsufficiency cooperated with MYC over-expression to drive lymphomagenesis. Furthermore, monoallelic Smarca4 deletion drove GC hyperplasia with centroblast polarization via significantly increased rates of centrocyte recycling to the dark zone. Mechanistically, Smarca4 loss reduced the activity of TFs that are activated in centrocytes to drive GC-exit, including SPI1 (PU.1), IRF family, and NF-κB. Loss of activity for these factors phenocopied aberrant BCL6 activity within murine centrocytes and human Burkitt lymphoma cells. SMARCA4 therefore facilitates chromatin accessibility for TFs that shape centrocyte trajectories, and loss of fine-control of these programs biases toward centroblast cell-fate, GC hyperplasia and lymphoma.

KW - B-cell

KW - BAF

KW - epigenetics

KW - germinal center

KW - immunology

KW - lymphoma

KW - SMARCA4

KW - SWI/SNF

KW - transcription

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DO - 10.1016/j.ccell.2024.02.011

M3 - Article

C2 - 38458188

AN - SCOPUS:85188475714

SN - 1535-6108

VL - 42

SP - 605-622.e11

JO - Cancer cell

JF - Cancer cell

IS - 4

ER -

SMARCA4 is a haploinsufficient B cell lymphoma tumor suppressor that fine-tunes centrocyte cell fate decisions

Abstract

Keywords

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