Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers

BACKGROUND: The most common B-cell cancers, chronic lymphocytic leukemia/lymphoma (CLL), follicular and diffuse large B-cell (FL, DLBCL) lymphomas, have distinct clinical courses, yet overlapping “cell-of-origin”. Dynamic changes to the epigenome are essential regulators of B-cell differentiation. T...

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Autores principales: Andrews, Jared M., Pyfrom, Sarah C., Schmidt, Jennifer A., Koues, Olivia I., Kowalewski, Rodney A., Grams, Nicholas R., Sun, Jessica J., Berman, Leigh R., Duncavage, Eric J., Lee, Yi-Shan, Cashen, Amanda F., Oltz, Eugene M., Payton, Jacqueline E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8403728/
https://www.ncbi.nlm.nih.gov/pubmed/34461601
http://dx.doi.org/10.1016/j.ebiom.2021.103559
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author Andrews, Jared M.
Pyfrom, Sarah C.
Schmidt, Jennifer A.
Koues, Olivia I.
Kowalewski, Rodney A.
Grams, Nicholas R.
Sun, Jessica J.
Berman, Leigh R.
Duncavage, Eric J.
Lee, Yi-Shan
Cashen, Amanda F.
Oltz, Eugene M.
Payton, Jacqueline E.
author_facet Andrews, Jared M.
Pyfrom, Sarah C.
Schmidt, Jennifer A.
Koues, Olivia I.
Kowalewski, Rodney A.
Grams, Nicholas R.
Sun, Jessica J.
Berman, Leigh R.
Duncavage, Eric J.
Lee, Yi-Shan
Cashen, Amanda F.
Oltz, Eugene M.
Payton, Jacqueline E.
author_sort Andrews, Jared M.
collection PubMed
description BACKGROUND: The most common B-cell cancers, chronic lymphocytic leukemia/lymphoma (CLL), follicular and diffuse large B-cell (FL, DLBCL) lymphomas, have distinct clinical courses, yet overlapping “cell-of-origin”. Dynamic changes to the epigenome are essential regulators of B-cell differentiation. Therefore, we reasoned that these distinct cancers may be driven by shared mechanisms of disruption in transcriptional circuitry. METHODS: We compared purified malignant B-cells from 52 patients with normal B-cell subsets (germinal center centrocytes and centroblasts, naïve and memory B-cells) from 36 donor tonsils using >325 high-resolution molecular profiling assays for histone modifications, open chromatin (ChIP-, FAIRE-seq), transcriptome (RNA-seq), transcription factor (TF) binding, and genome copy number (microarrays). FINDINGS: From the resulting data, we identified gains in active chromatin in enhancers/super-enhancers that likely promote unchecked B-cell receptor signaling, including one we validated near the immunoglobulin superfamily receptors FCMR and PIGR. More striking and pervasive was the profound loss of key B-cell identity TFs, tumor suppressors and their super-enhancers, including EBF1, OCT2(POU2F2), and RUNX3. Using a novel approach to identify transcriptional feedback, we showed that these core transcriptional circuitries are self-regulating. Their selective gain and loss form a complex, iterative, and interactive process that likely curbs B-cell maturation and spurs proliferation. INTERPRETATION: Our study is the first to map the transcriptional circuitry of the most common blood cancers. We demonstrate that a critical subset of B-cell TFs and their cognate enhancers form self-regulatory transcriptional feedback loops whose disruption is a shared mechanism underlying these diverse subtypes of B-cell lymphoma. FUNDING: National Institute of Health, Siteman Cancer Center, Barnes-Jewish Hospital Foundation, Doris Duke Foundation.
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spelling pubmed-84037282021-09-02 Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers Andrews, Jared M. Pyfrom, Sarah C. Schmidt, Jennifer A. Koues, Olivia I. Kowalewski, Rodney A. Grams, Nicholas R. Sun, Jessica J. Berman, Leigh R. Duncavage, Eric J. Lee, Yi-Shan Cashen, Amanda F. Oltz, Eugene M. Payton, Jacqueline E. EBioMedicine Research Paper BACKGROUND: The most common B-cell cancers, chronic lymphocytic leukemia/lymphoma (CLL), follicular and diffuse large B-cell (FL, DLBCL) lymphomas, have distinct clinical courses, yet overlapping “cell-of-origin”. Dynamic changes to the epigenome are essential regulators of B-cell differentiation. Therefore, we reasoned that these distinct cancers may be driven by shared mechanisms of disruption in transcriptional circuitry. METHODS: We compared purified malignant B-cells from 52 patients with normal B-cell subsets (germinal center centrocytes and centroblasts, naïve and memory B-cells) from 36 donor tonsils using >325 high-resolution molecular profiling assays for histone modifications, open chromatin (ChIP-, FAIRE-seq), transcriptome (RNA-seq), transcription factor (TF) binding, and genome copy number (microarrays). FINDINGS: From the resulting data, we identified gains in active chromatin in enhancers/super-enhancers that likely promote unchecked B-cell receptor signaling, including one we validated near the immunoglobulin superfamily receptors FCMR and PIGR. More striking and pervasive was the profound loss of key B-cell identity TFs, tumor suppressors and their super-enhancers, including EBF1, OCT2(POU2F2), and RUNX3. Using a novel approach to identify transcriptional feedback, we showed that these core transcriptional circuitries are self-regulating. Their selective gain and loss form a complex, iterative, and interactive process that likely curbs B-cell maturation and spurs proliferation. INTERPRETATION: Our study is the first to map the transcriptional circuitry of the most common blood cancers. We demonstrate that a critical subset of B-cell TFs and their cognate enhancers form self-regulatory transcriptional feedback loops whose disruption is a shared mechanism underlying these diverse subtypes of B-cell lymphoma. FUNDING: National Institute of Health, Siteman Cancer Center, Barnes-Jewish Hospital Foundation, Doris Duke Foundation. Elsevier 2021-08-27 /pmc/articles/PMC8403728/ /pubmed/34461601 http://dx.doi.org/10.1016/j.ebiom.2021.103559 Text en © 2021 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research Paper
Andrews, Jared M.
Pyfrom, Sarah C.
Schmidt, Jennifer A.
Koues, Olivia I.
Kowalewski, Rodney A.
Grams, Nicholas R.
Sun, Jessica J.
Berman, Leigh R.
Duncavage, Eric J.
Lee, Yi-Shan
Cashen, Amanda F.
Oltz, Eugene M.
Payton, Jacqueline E.
Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers
title Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers
title_full Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers
title_fullStr Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers
title_full_unstemmed Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers
title_short Loss of synergistic transcriptional feedback loops drives diverse B-cell cancers
title_sort loss of synergistic transcriptional feedback loops drives diverse b-cell cancers
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8403728/
https://www.ncbi.nlm.nih.gov/pubmed/34461601
http://dx.doi.org/10.1016/j.ebiom.2021.103559
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