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1. Transcriptome analysis of rheumatoid arthritis uncovers genes linked to inflammation-induced pain

Author

Bradford E. Hall, Khadijah Mazhar, Emma Macdonald, Margaret Cassidy, Megan Doty, Christian Judkins, Anita Terse, Stephanie Shiers, Saber Tadros, Sijung Yun, Michael D. Burton, Theodore J. Price, and Ashok B. Kulkarni

Subjects
Rheumatoid arthritis, Pain, Transcriptomics, Inflammation, Medicine, Science
Abstract

Abstract Autoimmune diseases such as rheumatoid arthritis (RA) can promote states of chronic inflammation with accompanying tissue destruction and pain. RA can cause inflammatory synovitis in peripheral joints, particularly within the hands and feet, but can also sometimes trigger temporomandibular joint (TMJ) arthralgia. To better understand the effects of ongoing inflammation-induced pain signaling, dorsal root ganglia (DRGs) were acquired from individuals with RA for transcriptomic study. We conducted RNA sequencing from the L5 DRGs because it contains the soma of the sensory neurons that innervate the affected joints in the foot. DRGs from 5 RA patients were compared with 9 non-arthritic controls. RNA-seq of L5 DRGs identified 128 differentially expressed genes (DEGs) that were dysregulated in the RA subjects as compared to the non-arthritic controls. The DRG resides outside the blood brain barrier and, as such, our initial transcriptome analysis detected signs of an autoimmune disorder including the upregulated expression of immunoglobulins and other immunologically related genes within the DRGs of the RA donors. Additionally, we saw the upregulation in genes implicated in neurogenesis that could promote pain hypersensitivity. Overall, our DRG analysis suggests that there are upregulated inflammatory and pain signaling pathways that can contribute to chronic pain in RA.

Published
2024
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2. Subtype-specific and co-occurring genetic alterations in B-cell non-Hodgkin lymphoma

Author

Man Chun John Ma, Saber Tadros, Alyssa Bouska, Tayla Heavican, Haopeng Yang, Qing Deng, Dalia Moore, Ariz Akhter, Keenan Hartert, Neeraj Jain, Jordan Showell, Sreejoyee Ghosh, Lesley Street, Marta Davidson, Christopher Carey, Joshua Tobin, Deepak Perumal, Julie M. Vose, Matthew A. Lunning, Aliyah R. Sohani, Benjamin J. Chen, Shannon Buckley, Loretta J. Nastoupil, R. Eric Davis, Jason R. Westin, Nathan H. Fowler, Samir Parekh, Maher Gandhi, Sattva Neelapu, Douglas Stewart, Kapil Bhalla, Javeed Iqbal, Timothy Greiner, Scott J. Rodig, Adnan Mansoor, and Michael R. Green

Subjects
Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

B-cell non-Hodgkin lymphoma (B-NHL) encompasses multiple clinically and phenotypically distinct subtypes of malignancy with unique molecular etiologies. Common subtypes of B-NHL, such as diffuse large B-cell lymphoma, have been comprehensively interrogated at the genomic level, but rarer subtypes, such as mantle cell lymphoma, remain less extensively characterized. Furthermore, multiple B-NHL subtypes have thus far not been comprehensively compared using the same methodology to identify conserved or subtype-specific patterns of genomic alterations. Here, we employed a large targeted hybrid-capture sequencing approach encompassing 380 genes to interrogate the genomic landscapes of 685 B-NHL tumors at high depth, including diffuse large B-cell lymphoma, mantle cell lymphoma, follicular lymphoma, and Burkitt lymphoma. We identified conserved hallmarks of B-NHL that were deregulated in the majority of tumors from each subtype, including frequent genetic deregulation of the ubiquitin proteasome system. In addition, we identified subtype-specific patterns of genetic alterations, including clusters of co-occurring mutations and DNA copy number alterations. The cumulative burden of mutations within a single cluster were more discriminatory of B-NHL subtypes than individual mutations, implicating likely patterns of genetic cooperation that contribute to disease etiology. We therefore provide the first cross-sectional analysis of mutations and DNA copy number alterations across major B-NHL subtypes and a framework of co-occurring genetic alterations that deregulate genetic hallmarks and likely cooperate in lymphomagenesis.

Published
2021
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3. Polyfunctional Antigen Specific CD4+ T cell Responses in Patients With Human Immunodeficiency Virus/AIDS and Histoplasmosis Immune Reconstitution Inflammatory Syndrome

Author

Maura Manion, Afroditi Boulougoura, Nuha Naqvi, Silvia Lucena Lage, Elizabeth Richards, Christopher Grivas, Elizabeth Laidlaw, Safia Kuriakose, Ana M Ortega-Villa, Saber Tadros, Gregg Roby, Adam Rupert, France Galindo, Megan Anderson, Alice Pau, George Deepe, Virginia Sheikh, and Irini Sereti

Subjects
Microbiology (medical), Infectious Diseases
Abstract

In the combination antiretroviral era, there are limited data regarding the pathogenesis of histoplasmosis immune reconstitution inflammatory syndrome (IRIS) in people with human immunodeficiency virus (HIV). We immunologically characterized 10 cases of histoplasmosis, 4 of whom developed histoplasmosis IRIS. CD4+ T cells in histoplasmosis IRIS demonstrated a significant polyfunctional cytokine response to histoplasma antigen.

Published
2022

4. Data from Selective Inhibition of HDAC3 Targets Synthetic Vulnerabilities and Activates Immune Surveillance in Lymphoma

Author

Michael R. Green, Ari M. Melnick, Robert G. Roeder, David A. Scheinberg, Ahmet Dogan, Cassian Yee, Anas Younes, José Baselga, Giorgio Inghirami, Oliver Weigert, Sattva S. Neelapu, Loretta Nastoupil, Anja Mottok, Sreejoyee Ghosh, Elisa de Stanchina, Matthew Durant, Stefan Alig, Eneda Toska, Man Chun John Ma, Chi-Shuen Chu, Hsia-Yuan Ying, Shailbala Singh, Haopeng Yang, Neeraj Jain, Aaron Y. Chang, Lorena Fontan, Matt Teater, Saber Tadros, and Patrizia Mondello

Abstract

CREBBP mutations are highly recurrent in B-cell lymphomas and either inactivate its histone acetyltransferase (HAT) domain or truncate the protein. Herein, we show that these two classes of mutations yield different degrees of disruption of the epigenome, with HAT mutations being more severe and associated with inferior clinical outcome. Genes perturbed by CREBBP mutation are direct targets of the BCL6–HDAC3 onco-repressor complex. Accordingly, we show that HDAC3-selective inhibitors reverse CREBBP-mutant aberrant epigenetic programming, resulting in: (i) growth inhibition of lymphoma cells through induction of BCL6 target genes such as CDKN1A and (ii) restoration of immune surveillance due to induction of BCL6-repressed IFN pathway and antigen-presenting genes. By reactivating these genes, exposure to HDAC3 inhibitors restored the ability of tumor-infiltrating lymphocytes to kill DLBCL cells in an MHC class I and II–dependent manner, and synergized with PD-L1 blockade in a syngeneic model in vivo. Hence, HDAC3 inhibition represents a novel mechanism-based immune epigenetic therapy for CREBBP-mutant lymphomas.Significance:We have leveraged the molecular characterization of different types of CREBBP mutations to define a rational approach for targeting these mutations through selective inhibition of HDAC3. This represents an attractive therapeutic avenue for targeting synthetic vulnerabilities in CREBBP-mutant cells in tandem with promoting antitumor immunity.This article is highlighted in the In This Issue feature, p. 327

Published
2023

5. Supplementary Figures and Methods from Selective Inhibition of HDAC3 Targets Synthetic Vulnerabilities and Activates Immune Surveillance in Lymphoma

Author

Michael R. Green, Ari M. Melnick, Robert G. Roeder, David A. Scheinberg, Ahmet Dogan, Cassian Yee, Anas Younes, José Baselga, Giorgio Inghirami, Oliver Weigert, Sattva S. Neelapu, Loretta Nastoupil, Anja Mottok, Sreejoyee Ghosh, Elisa de Stanchina, Matthew Durant, Stefan Alig, Eneda Toska, Man Chun John Ma, Chi-Shuen Chu, Hsia-Yuan Ying, Shailbala Singh, Haopeng Yang, Neeraj Jain, Aaron Y. Chang, Lorena Fontan, Matt Teater, Saber Tadros, and Patrizia Mondello

Abstract

Figures S1 - S16 Supplementary Methods

Published
2023

6. Supplementary Tables from Selective Inhibition of HDAC3 Targets Synthetic Vulnerabilities and Activates Immune Surveillance in Lymphoma

Author

Michael R. Green, Ari M. Melnick, Robert G. Roeder, David A. Scheinberg, Ahmet Dogan, Cassian Yee, Anas Younes, José Baselga, Giorgio Inghirami, Oliver Weigert, Sattva S. Neelapu, Loretta Nastoupil, Anja Mottok, Sreejoyee Ghosh, Elisa de Stanchina, Matthew Durant, Stefan Alig, Eneda Toska, Man Chun John Ma, Chi-Shuen Chu, Hsia-Yuan Ying, Shailbala Singh, Haopeng Yang, Neeraj Jain, Aaron Y. Chang, Lorena Fontan, Matt Teater, Saber Tadros, and Patrizia Mondello

Abstract

Tables S1 - S13

Published
2023

7. Supplementary Figures S1-S8; Supplementary Tables S1-S8; Supplementary methods from De Novo Lipid Synthesis Facilitates Gemcitabine Resistance through Endoplasmic Reticulum Stress in Pancreatic Cancer

Author

Pankaj K. Singh, Aaron R. Sasson, Jean Grem, Lyudmyla Berim, Audrey J. Lazenby, Fang Yu, Nina V. Chaika, Jaime Abrego, Enza Vernucci, Venugopal Gunda, Ryan J. King, Surendra K. Shukla, and Saber Tadros

Abstract

Figure S1: FASN inhibition with orlistat shows synergistic activity with gemcitabine in AsPC-1 cells; Figure S2: Effect of orlistat on the lipid content of pancreatic cancer cells; Figure S3: Platensimycin shows synergistic activity with gemcitabine in AsPC-1 cells; Figure S4: Lipid synthesis inhibitor C75 improves the effect of gemcitabine in pancreatic cancer cell lines; Figure S5: Lipid synthesis inhibitor fatostatin improves the effect of gemcitabine in pancreatic cancer cell lines; Figure S6: Albumin-conjugated palmitate does not rescue the anti-proliferative effects of gemcitabine; Figure S7: AdCM does not rescue the antiproliferative effect of gemcitabine on pancreatic cancer cells under the regular and stress conditions; Figure S8: Effect of AdCM on the lipid content of pancreatic cancer cells. Table S1: Metabolic pathway enrichment in pancreatic ductal adenocarcinoma patients treated with gemcitabine (data pooled from TCGA); Table S2: Patient Characteristics for Figure 1D; Table S3: Cell line gemcitabine responsiveness (IC50), FASN expression, and mutation status; Table S4: Orlistat responsiveness in pancreatic cancer cell lines; Table S5: Combination index of gemcitabine and orlistat in pancreatic cancer cell lines PANC-1, AsPC-1, Capan-1, and HPAF-II; Table S6: Combination index of gemcitabine and C75 in pancreatic cancer cell lines PANC-1, and AsPC-1; Table S7: Combination index of gemcitabine and fatostatin in pancreatic cancer cell lines PANC-1, and AsPC-1; Table S8: Combination index of gemcitabine and thapsigargin in pancreatic cancer cell lines PANC-1. SUPPLEMENTARY MATERIALS AND METHODS

Published
2023

8. Data from De Novo Lipid Synthesis Facilitates Gemcitabine Resistance through Endoplasmic Reticulum Stress in Pancreatic Cancer

Author

Pankaj K. Singh, Aaron R. Sasson, Jean Grem, Lyudmyla Berim, Audrey J. Lazenby, Fang Yu, Nina V. Chaika, Jaime Abrego, Enza Vernucci, Venugopal Gunda, Ryan J. King, Surendra K. Shukla, and Saber Tadros

Abstract

Pancreatic adenocarcinoma is moderately responsive to gemcitabine-based chemotherapy, the most widely used single-agent therapy for pancreatic cancer. Although the prognosis in pancreatic cancer remains grim in part due to poor response to therapy, previous attempts at identifying and targeting the resistance mechanisms have not been very successful. By leveraging The Cancer Genome Atlas dataset, we identified lipid metabolism as the metabolic pathway that most significantly correlated with poor gemcitabine response in pancreatic cancer patients. Furthermore, we investigated the relationship between alterations in lipogenesis pathway and gemcitabine resistance by utilizing tissues from the genetically engineered mouse model and human pancreatic cancer patients. We observed a significant increase in fatty acid synthase (FASN) expression with increasing disease progression in spontaneous pancreatic cancer mouse model, and a correlation of high FASN expression with poor survival in patients and poor gemcitabine responsiveness in cell lines. We observed a synergistic effect of FASN inhibitors with gemcitabine in pancreatic cancer cells in culture and orthotopic implantation models. Combination of gemcitabine and the FASN inhibitor orlistat significantly diminished stemness, in part due to induction of endoplasmic reticulum (ER) stress that resulted in apoptosis. Moreover, direct induction of ER stress with thapsigargin caused a similar decrease in stemness and showed synergistic activity with gemcitabine. Our in vivo studies with orthotopic implantation models demonstrated a robust increase in gemcitabine responsiveness upon inhibition of fatty acid biosynthesis with orlistat. Altogether, we demonstrate that fatty acid biosynthesis pathway manipulation can help overcome the gemcitabine resistance in pancreatic cancer by regulating ER stress and stemness. Cancer Res; 77(20); 5503–17. ©2017 AACR.

Published
2023

9. Histopathology and SARS-CoV-2 Cellular Localization in Eye Tissues of COVID-19 Autopsies

Author

H. Nida Sen, Kevin M. Vannella, Yujuan Wang, Joon-Yong Chung, Shilpa Kodati, Sabrina C. Ramelli, Jung Wha Lee, Paola Perez, Sydney R. Stein, Alison Grazioli, James M. Dickey, Kris Ylaya, Manmeet Singh, Kwe Claude Yinda, Andrew Platt, Marcos J. Ramos-Benitez, Christa Zerbe, Vincent J. Munster, Emmie de Wit, Blake M. Warner, Daniel L. Herr, Joseph Rabin, Kapil K. Saharia, David E. Kleiner, Stephen M. Hewitt, Chi-Chao Chan, Daniel S. Chertow, Andrew P. Platt, Shelly J. Curran, Ashley L. Babyak, Luis Perez Valencia, Mary E. Richert, Willie J. Young, Sarah P. Young, Billel Gasmi, Michelly Sampaio De Melo, Sabina Desar, Saber Tadros, Nadia Nasir, Xueting Jin, Sharika Rajan, Esra Dikoglu, Neval Ozkaya, Stefania Pittaluga, Grace Smith, Elizabeth R. Emanuel, Brian Kelsall, Justin A. Olivera, Megan Blawas, Nicole Hays, Madeleine Purcell, Shreya Singireddy, Jocelyn Wu, Katherine Raja, Ryan Curto, Jean Chung, Amy Borth, Kimberly Bowers, Anne Weichold, Paula Minor, Mirahmad Moshref, Emily Kelly, Mohammad M. Sajadi, Thomas M. Scalea, Douglas Tran, Ronson J. Madathil, Siamak Dahi, Kristopher B. Deatrick, Eric M. Krause, Joseph A. Herrold, Ali Tabatabai, Eric Hochberg, Christopher Cornachione, Andrea R. Levine, Justin E. Richards, John Elder, Allen Burke, Michael A. Mazzeffi, Robert Christenson, Zackary Chancer, Mustafa Abdulmahdi, Sabrina Sopha, Tyler Goldberg, Shahabuddin Soherwardi, Yashvir Sangwan, Michael T. McCurdy, Kristen Sudano, Diane Blume, Bethany Radin, Madhat Arnouk, and James W. Eagan

Subjects
Pathology and Forensic Medicine
Published
2023

11. Selective Inhibition of HDAC3 Targets Synthetic Vulnerabilities and Activates Immune Surveillance in Lymphoma

Author

Sattva S. Neelapu, David A. Scheinberg, Saber Tadros, Neeraj Jain, E. De Stanchina, Matthew Durant, Jose Baselga Baselga, Lorena Fontan, Eneda Toska, Oliver Weigert, Cassian Yee, Anas Younes, Ahmet Dogan, Ari Melnick, Aaron Y. Chang, Huan Yang, Anja Mottok, Hsia-Yuan Ying, Loretta J. Nastoupil, Chi-Shuen Chu, Stefan Alig, Robert G. Roeder, Giorgio Inghirami, Patrizia Mondello, Man Chun John Ma, Shailbala Singh, Michael R. Green, Sreejoyee Ghosh, and Matt Teater

Subjects
0301 basic medicine, Lymphoma, Genes, MHC Class I, medicine.disease_cause, B7-H1 Antigen, Epigenome, Mice, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, Immune Checkpoint Inhibitors, Histone Acetyltransferases, Mutation, biology, CREBBP, BCL6, CREB-Binding Protein, Oncology, 030220 oncology & carcinogenesis, Proto-Oncogene Proteins c-bcl-6, Interferon, Growth inhibition, Epigenetic therapy, Signal Transduction, Cyclin-Dependent Kinase Inhibitor p21, Antigen-Presenting Cells, Histone Deacetylases, Article, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, Immune system, Cell Line, Tumor, CREBBP, HDAC3, Interferon, MHC class II, MHC class I, medicine, Animals, Humans, Cell Proliferation, Histocompatibility Antigens Class II, HDAC3, Histone acetyltransferase, Histone Deacetylase Inhibitors, 030104 developmental biology, chemistry, Immune System, MHC class II, Cancer research, biology.protein, Interferons
Abstract

CREBBP mutations are highly recurrent in B-cell lymphomas and either inactivate its histone acetyltransferase (HAT) domain or truncate the protein. Herein, we show that these two classes of mutations yield different degrees of disruption of the epigenome, with HAT mutations being more severe and associated with inferior clinical outcome. Genes perturbed by CREBBP mutation are direct targets of the BCL6–HDAC3 onco-repressor complex. Accordingly, we show that HDAC3-selective inhibitors reverse CREBBP-mutant aberrant epigenetic programming, resulting in: (i) growth inhibition of lymphoma cells through induction of BCL6 target genes such as CDKN1A and (ii) restoration of immune surveillance due to induction of BCL6-repressed IFN pathway and antigen-presenting genes. By reactivating these genes, exposure to HDAC3 inhibitors restored the ability of tumor-infiltrating lymphocytes to kill DLBCL cells in an MHC class I and II–dependent manner, and synergized with PD-L1 blockade in a syngeneic model in vivo. Hence, HDAC3 inhibition represents a novel mechanism-based immune epigenetic therapy for CREBBP-mutant lymphomas. Significance: We have leveraged the molecular characterization of different types of CREBBP mutations to define a rational approach for targeting these mutations through selective inhibition of HDAC3. This represents an attractive therapeutic avenue for targeting synthetic vulnerabilities in CREBBP-mutant cells in tandem with promoting antitumor immunity. This article is highlighted in the In This Issue feature, p. 327

Published
2020

12. Polyfunctional antigen specific CD4± T cell responses in Patients with HIV/AIDS and Histoplasmosis Immune Reconstitution Inflammatory Syndrome

Author

Maura, Manion, Afroditi, Boulougoura, Nuha, Naqvi, Silvia Lucena, Lage, Elizabeth, Richards, Christopher, Grivas, Elizabeth, Laidlaw, Safia, Kuriakose, Ana M, Ortega-Villa, Saber, Tadros, Gregg, Roby, Adam, Rupert, France, Galindo, Megan, Anderson, Alice, Pau, George, Deepe, Virginia, Sheikh, and Irini, Sereti

Subjects
Brief Report
Abstract

In the combination antiretroviral era, there are limited data regarding the pathogenesis of histoplasmosis immune reconstitution inflammatory syndrome (IRIS) in people with human immunodeficiency virus (HIV). We immunologically characterized 10 cases of histoplasmosis, 4 of whom developed histoplasmosis IRIS. CD4+ T cells in histoplasmosis IRIS demonstrated a significant polyfunctional cytokine response to histoplasma antigen.

Published
2022

14. Pathological Features of Tumors of the Nervous System in Hereditary Cancer Predisposition Syndromes: A Review

Author

Ashis Chowdhury, Aleksei Kondrashov, Sriya Namagiri, Abhik Ray-Chaudhury, Yeshavanth Kumar Banasavadi-Siddegowda, and Saber Tadros

Subjects
Neuropathology Review Series, Bioinformatics, Germline, 03 medical and health sciences, Tuberous sclerosis, 0302 clinical medicine, Germline mutation, Neoplastic Syndromes, Hereditary, Peripheral Nervous System Neoplasms, Tuberous Sclerosis, medicine, Humans, MEN1, Genetic Predisposition to Disease, 030304 developmental biology, Genetic testing, 0303 health sciences, medicine.diagnostic_test, business.industry, Cancer, medicine.disease, Precision medicine, 030220 oncology & carcinogenesis, Genetic Phenomena, Mutation, Surgery, Neurology (clinical), business
Abstract

Hereditary cancer predisposition syndromes (HCS) become more recognizable as the knowledge about them expands, and genetic testing becomes more affordable. In this review, we discussed the known HCS that predispose to central and peripheral nervous system tumors. Different genetic phenomena were highlighted, and the important cellular biological alterations were summarized. Genetic mosaicism and germline mutations are features of HCS, and recently, they were described in normal population and as modifiers for the genetic landscape of sporadic tumors. Description of the tumors arising in these conditions was augmented by representative cases explaining the main pathological findings. Clinical spectrum of the syndromes and diagnostic criteria were tabled to outline their role in defining these disorders. Interestingly, precision medicine has found its way to help these groups of patients by offering targeted preventive measures. Understanding the signaling pathway alteration of mammalian target of rapamycin (mTOR) in tuberous sclerosis helped introducing mTOR inhibitors as a prophylactic treatment in these patients. More research to define the germline genetic alterations and resulting cellular signaling perturbations is needed for effective risk-reducing interventions beyond prophylactic surgeries.

Published
2021

15. Genomic Drivers in Follicular Lymphoma

Author

Michael R. Green and Saber Tadros

Subjects
Mutation, Oncogene, EZH2, Cancer research, Follicular lymphoma, medicine, Chromosomal translocation, Biology, medicine.disease, medicine.disease_cause, Enhancer, Somatic evolution in cancer, Chromatin
Abstract

This chapter discusses the genetic mutation landscape in follicular lymphoma (FL) and its role in tumor initiation and progression. The t(14;18)(q32;q21) translocation that places the BCL2 oncogene under control of the immunoglobulin heavy-chain enhancer is a genetic hallmark of FL. However, mutations in chromatin modifying genes (CMGs) such as KMT2D, CREBBP, and EZH2 have emerged as key genetic hits that promote lymphomagenesis. These mutations, and others that are implicated in FL, are discussed in this chapter. We provide insight into their biological function and the mechanisms by which their deregulation contributes to lymphomagenesis, and we discuss their role in disease genesis and progression.

Published
2019

16. Crebbp loss cooperates with Bcl2 overexpression to promote lymphoma in mice

Author

Oscar Blanco, Isidro Sánchez-García, Julie M. Vose, Ash A. Alizadeh, Fernando Rodrigues-Lima, Lucía Ruiz-Roca, David Klinkebiel, Francisco Javier García Criado, María Begoña García Cenador, Alberto Martín-Lorenzo, Kai Fu, Rafael C. Jimenez, Diego Alonso-López, Timothy C. Greiner, Carolina Vicente-Dueñas, Idoia García-Ramírez, Guillermo Rodríguez-Hernández, Keenan Hartert, Saber Tadros, Inés González-Herrero, Martin Bast, Javier De Las Rivas, Michael R. Green, Romain Duval, Matthew A. Lunning, Paul K. Brindle, Dalia Moore, Nebraska Department of Health and Human Services, European Commission, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, National Cancer Institute (US), National Institutes of Health (US), Fundación Inocente Inocente, Instituto de Investigación Biomédica de Salamanca, Josep Carreras Leukemia Foundation, Centre National de la Recherche Scientifique (France), Région Ile-de-France, Université Paris Diderot, Institut National du Cancer (France), Unité de Biologie Fonctionnelle et Adaptative (BFA (UMR_8251 / U1133)), and Université Paris Diderot - Paris 7 (UPD7)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects
0301 basic medicine, genetic structures, [SDV]Life Sciences [q-bio], Immunology, Nonsense mutation, MYC, BINDING PROTEIN, ANALYSES REVEAL, Biochemistry, Frameshift mutation, 03 medical and health sciences, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, Missense mutation, Epigenetics, P300, CREB-binding protein, Gene, GENE-EXPRESSION, Regulation of gene expression, Lymphoid Neoplasia, biology, GENOME-WIDE, B-CELL LYMPHOMA, SOMATIC MUTATIONS, Cell Biology, Hematology, Molecular biology, 3. Good health, 030104 developmental biology, Histone, HISTONE ACETYLATION, 030220 oncology & carcinogenesis, biology.protein, Cancer research, FOLLICULAR LYMPHOMA
Abstract

CREBBP is targeted by inactivating mutations in follicular lymphoma (FL) and diffuse large B-cell lymphoma (DLBCL). Here, we provide evidence from transgenic mouse models that Crebbp deletion results in deficits in B-cell development and can cooperate with Bcl2 overexpression to promote B-cell lymphoma. Through transcriptional and epigenetic profiling of these B cells, we found that Crebbp inactivation was associated with broad transcriptional alterations, but no changes in the patterns of histone acetylation at the proximal regulatory regions of these genes. However, B cells with Crebbp inactivation showed high expression of Myc and patterns of altered histone acetylation that were localized to intragenic regions, enriched for Myc DNA binding motifs, andshowedMycbinding. Through the analysis ofCREBBPmutations from a large cohort of primary human FL and DLBCL, we show a significant difference in the spectrum of CREBBP mutations in these 2 diseases, with higher frequencies of nonsense/ frameshift mutations in DLBCL compared with FL. Together, our data therefore provide important links between Crebbp inactivation and Bcl2 dependence and show a role for Crebbp inactivation in the induction of Myc expression. We suggest this may parallel the role of CREBBP frameshift/nonsense mutations in DLBCL that result in loss of the protein, but may contrast the role of missense mutations in the lysine acetyltransferase domain that are more frequently observed in FL and yield an inactive protein., Research in the M.R.G. group is supported by grants from the Nebraska Department of Health and Human Services (LB506 2016-16) and the National Institutes of Health, National Cancer Institute (1R01CA201380). Research in the I.S.-G. group is partially supported by Fondo Europeo de Desarrollo Regional (FEDER) and by the Ministry of Economy and Competitiveness (SAF2012-32810, SAF2015-64420-R, and Red de Excelencia Consolider OncoBIO SAF2014-57791-REDC), Instituto de Salud Carlos III (PIE14/00066), Instituto de Salud Carlos III Plan de Ayudas Institute of Biomedical Research of Salamanca 2015 Proyectos Integrados (IBY15/00003), by Junta de Castilla y Leon (BIO/SA51/15, CSI001U14, UIC-017, andCSI001U16), Fundacion Inocente Inocente, by the German Carreras Foundation (Organisation der Deutsche Jose Carreras Leukamie-Stiftung eV R13/26), and by the Advanced Research on Interaction Mechanisms of electro Magnetic Exposures with Organisms for Risk Assessment project (European Union’s Seventh Framework Programme [FP7/2007-2013] under grant agreement no. 282891). The Nebraska Lymphoma Study Group tissue bank is supported by the Fred & Pamela Buffett Cancer Center’s National Cancer Institute Cancer Center Support Grant (P30CA036727). The I.S.-G. laboratory is a member of the EuroSyStem and the Developing Evidence to Inform Decisions about Effectiveness Network funded by the European Union under the FP7 program. Research in the C.V.-D. group is partially supported by a “Miguel Servet” Grant (CP14/00082, AES 2013-2016, FEDER) from the Instituto de Salud Carlos III (Ministerio de Economia y Competitividad). I.G.-R. was supported by BES-Ministerio de Economia y Competitividad (BES-2013-063789). G.R.-H. and L.R.-R. were supported by Fondo Social Europeo-Consejeria de Educacion de la Junta de Castilla y Leon. R.D. was supported by a fellowship from Region Ile de France (Appel hors DIM 2013). Research in the F.R.-L. group was supported by grants from Universite Paris Diderot, CNRS, Institut National du Cancer (2012-1-PL-BIO), and the Plan Cancer Environnement 2013. Ultrafast liquid chromatography analyses were done on the platform “Bioprofiler” (Unite de Biologie Fonctionnelle et Adaptative).

Published
2017

17. Targetable genetic alterations of TCF4 (E2-2) drive immunoglobulin expression in diffuse large B-cell lymphoma

Author

Karin E. Smedby, Gunnar Juliusson, Ash A. Alizadeh, Richard Rosenquist, Andrew J. Gentles, Michael R. Green, Saber Tadros, Julie M. Vose, Dhiraj Kumar, Chih Long Liu, Ondrej Havranek, Sattva S. Neelapu, Filippo G. Giancotti, Scott J. Rodig, Qing Deng, Timothy Greiner, Tayla Heavican, Warren Fiskus, Keenan Hartert, Neeraj Jain, Andreas Rosenwald, Alyssa Bouska, Javeed Iqbal, Man Chun John Ma, Matthew A. Lunning, Robert Kridel, Elena Hartmann, R. Eric Davis, Kapil N. Bhalla, Dalia Moore, Christine Pak, Randy D. Gascoyne, and Jason R. Westin

Subjects
0301 basic medicine, Male, Cell Survival, Blotting, Western, Immunoglobulins, Mice, Nude, Biology, Article, Cell Line, 03 medical and health sciences, Mice, 0302 clinical medicine, Transcription Factor 4, immune system diseases, hemic and lymphatic diseases, medicine, Animals, Humans, Enhancer, Gene, B cell, Regulation of gene expression, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, General Medicine, TCF4, medicine.disease, Xenograft Model Antitumor Assays, Lymphoma, Gene expression profiling, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, Lymphoma, Large B-Cell, Diffuse, Diffuse large B-cell lymphoma, Signal Transduction
Abstract

The activated B cell (ABC-like) subtype of diffuse large B cell lymphoma (DLBCL) is characterized by chronic activation of signaling initiated by immunoglobulin μ (IgM). By analyzing the DNA copy number profiles of 1000 DLBCL tumors, we identified gains of 18q21.2 as the most frequent genetic alteration in ABC-like DLBCL. Using integrative analysis of matched gene expression profiling data, we found that the TCF4 (E2-2) transcription factor gene was the target of these alterations. Overexpression of TCF4 in ABC-like DLBCL cell lines led to its occupancy on immunoglobulin (IGHM) and MYC gene enhancers and increased expression of these genes at the transcript and protein levels. Inhibition of TCF4 activity with dominant-negative constructs was synthetically lethal to ABC-like DLBCL cell lines harboring TCF4 DNA copy gains, highlighting these gains as an attractive potential therapeutic target. Furthermore, the TCF4 gene was one of the top BRD4-regulated genes in DLBCL cell lines. BET proteolysis-targeting chimera (PROTAC) ARV771 extinguished TCF4, MYC, and IgM expression and killed ABC-like DLBCL cells in vitro. In DLBCL xenograft models, ARV771 treatment reduced tumor growth and prolonged survival. This work highlights a genetic mechanism for promoting immunoglobulin signaling in ABC-like DLBCL and provides a functional rationale for the use of BET inhibitors in this disease.

Published
2019

18. Subtype-specific and co-occurring genetic alterations in B-cell non-Hodgkin lymphoma

Author

Sattva S. Neelapu, Benjamin J. Chen, Aliyah R. Sohani, Marta Davidson, Dalia Moore, Keenan Hartert, Joshua W.D. Tobin, Douglas A. Stewart, Saber Tadros, Sreejoyee Ghosh, Alyssa Bouska, Matthew A. Lunning, Shannon M. Buckley, Deepak Perumal, Tayla Heavican, Christopher D. Carey, Julie M. Vose, Kapil Bhalla, Loretta J. Nastoupil, Man Chun John Ma, Ariz Akhter, Javeed Iqbal, Samir Parekh, Michael R. Green, Jordan Showell, Maher K. Gandhi, Neeraj Jain, Scott J. Rodig, Haopeng Yang, Lesley Street, Qing Deng, R. Eric Davis, Adnan Mansoor, Timothy Greiner, Nathan Fowler, and Jason R. Westin

Subjects
Adult, Follicular lymphoma, Genomics, Biology, Malignancy, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, immune system diseases, hemic and lymphatic diseases, medicine, Humans, Lymphoma, Follicular, Gene, 030304 developmental biology, Genetics, 0303 health sciences, Hematology, medicine.disease, Burkitt Lymphoma, Lymphoma, Cross-Sectional Studies, Proteasome, chemistry, 030220 oncology & carcinogenesis, Mutation, B-Cell Non-Hodgkin Lymphoma, Cancer research, Mantle cell lymphoma, Lymphoma, Large B-Cell, Diffuse, DNA
Abstract

B-cell non-Hodgkin’s lymphoma (B-NHL) encompasses multiple clinically and phenotypically distinct subtypes of malignancy with unique molecular etiologies. Common subtypes of B-NHL such as diffuse large B-cell lymphoma (DLBCL) have been comprehensively interrogated at the genomic level. But rarer subtypes such as mantle cell lymphoma (MCL) remain sparsely characterized. Furthermore, multiple B-NHL subtypes have thus far not been comprehensively compared using the same methodology to identify conserved or subtype-specific patterns of genomic alterations. Here, we employed a large targeted hybrid-capture sequencing approach encompassing 380 genes to interrogate the genomic landscapes of 685 B-NHL tumors at high depth; including DLBCL, MCL, follicular lymphoma (FL), and Burkitt lymphoma (BL). We identified conserved hallmarks of B-NHL that were deregulated in the majority of tumor from each subtype, including the frequent genetic deregulation of the ubiquitin proteasome system (UPS). In addition, we identified subtype-specific patterns of genetic alterations, including clusters of co-occurring mutations and DNA copy number alterations. The cumulative burden of mutations within a single cluster were more discriminatory of B-NHL subtypes than individual mutations, implicating likely patterns of genetic cooperation that contribute to disease etiology. We therefore provide the first cross-sectional analysis of mutations and DNA copy number alterations across major B-NHL subtypes and a framework of co-occurring genetic alterations that deregulate genetic hallmarks and likely cooperate in lymphomagenesis.

Published
2019

19. Selective inhibition of HDAC3 targets synthetic vulnerabilities and activates immune surveillance in lymphoma

Author

Sattva S. Neelapu, Matt Teater, Michael R. Green, Matthew Durant, David A. Scheinberg, Saber Tadros, Ahmet Dogan, E. De Stanchina, Stefan Alig, Oliver Weigert, Giorgio Inghirami, Patrizia Mondello, Anas Younes, Anja Mottok, Cassian Yee, Aaron Y. Chang, Jose Baselga Baselga, Shailbala Singh, Eneda Toska, Lorena Fontan, Neeraj Jain, Ari Melnick, Huan Yang, Man Chun John Ma, and Loretta J. Nastoupil

Subjects
0303 health sciences, Mutation, biology, Antigen presentation, Mutant, Epigenome, Histone acetyltransferase, BCL6, HDAC3, medicine.disease_cause, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, hemic and lymphatic diseases, MHC class I, biology.protein, medicine, Cancer research, 030304 developmental biology
Abstract

CREBBP mutations are highly recurrent in B-cell lymphomas and either inactivate its histone acetyltransferase (HAT) domain or truncate the protein. Herein, we show that these two classes of mutations yield different degrees of disruption of the epigenome, with HAT mutations being more severe and associated with inferior clinical outcome. Genes perturbed by CREBBP mutation are direct targets of the BCL6/HDAC3 onco-repressor complex. Accordingly, we show that HDAC3 selective inhibitors fully reverse CREBBP mutant aberrant epigenetic programming resulting in: a) growth inhibition of lymphoma cells through induction of BCL6 target genes such as CDKN1A and b) restoration of immune surveillance due to induction of BCL6 repressed IFN pathway and antigen presentation genes. By reactivating these genes, exposure to HDAC3-i restored the ability of tumor infiltrating lymphocytes to kill DLBCL cells in an MHC II and MHC I dependent manner. Hence HDAC3-i represent a novel mechanism-based immune-epigenetic therapy for CREBBP mutant lymphomas.STATEMENT OF SIGNIFICANCEWe have leveraged the molecular characterization of different types of CREBBP mutations to define a rational approach for targeting these mutations through selective inhibition of HDAC3. This represents an attractive therapeutic avenue for targeting synthetic vulnerabilities in CREBBP mutant cells in tandem with promoting anti-tumor immunity.

Published
2019
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20. TET2 Deficiency Causes Germinal Center Hyperplasia, Impairs Plasma Cell Differentiation, and Promotes B-cell Lymphomagenesis

Author

Olivier A. Bernard, Wojciech Rosikiewicz, Rita Shaknovich, Michael R. Green, María Fernández, Iannis Aifantis, Enguerran Mouly, Miguel Torres-Martin, Alan H. Shih, Saber Tadros, Ross L. Levine, Véronique Della-Valle, Ari Melnick, Luisa Cimmino, Matt Durant, Pilar M. Dominguez, Nathalie Droin, Patrycja Pawlikowska, Said Aoufouchi, Parveen Kumar, Matt Teater, Wayne Tam, Wendy Béguelin, Marine Armand, Martín A. Rivas, Hussein Ghamlouch, Giorgio Inghirami, Mark A. Rubin, Lorena Fontan, Olivier Elemento, Ashley S. Doane, Samaneh Motanagh, Maria E. Figueroa, and Sheng Li

Subjects
0301 basic medicine, Somatic cell, Plasma Cells, Mice, Transgenic, Biology, medicine.disease_cause, Dioxygenases, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Proto-Oncogene Proteins, PRDM1, Plasma cell differentiation, medicine, Animals, Humans, Loss function, B cell, Mice, Knockout, Mutation, Hyperplasia, Gene Expression Profiling, Germinal center, Cell Differentiation, Germinal Center, Hematopoietic Stem Cells, CREB-Binding Protein, DNA-Binding Proteins, 030104 developmental biology, medicine.anatomical_structure, Oncology, Cancer research, Lymphoma, Large B-Cell, Diffuse, Positive Regulatory Domain I-Binding Factor 1, 030215 immunology
Abstract

TET2 somatic mutations occur in ∼10% of diffuse large B-cell lymphomas (DLBCL) but are of unknown significance. Herein, we show that TET2 is required for the humoral immune response and is a DLBCL tumor suppressor. TET2 loss of function disrupts transit of B cells through germinal centers (GC), causing GC hyperplasia, impaired class switch recombination, blockade of plasma cell differentiation, and a preneoplastic phenotype. TET2 loss was linked to focal loss of enhancer hydroxymethylation and transcriptional repression of genes that mediate GC exit, such as PRDM1. Notably, these enhancers and genes are also repressed in CREBBP-mutant DLBCLs. Accordingly, TET2 mutation in patients yields a CREBBP-mutant gene-expression signature, CREBBP and TET2 mutations are generally mutually exclusive, and hydroxymethylation loss caused by TET2 deficiency impairs enhancer H3K27 acetylation. Hence, TET2 plays a critical role in the GC reaction, and its loss of function results in lymphomagenesis through failure to activate genes linked to GC exit signals. Significance: We show that TET2 is required for exit of the GC, B-cell differentiation, and is a tumor suppressor for mature B cells. Loss of TET2 phenocopies CREBBP somatic mutation. These results advocate for sequencing TET2 in patients with lymphoma and for the testing of epigenetic therapies to treat these tumors. See related commentary by Shingleton and Dave, p. 1515. This article is highlighted in the In This Issue feature, p. 1494

Published
2018

21. De Novo Lipid Synthesis Facilitates Gemcitabine Resistance Through Endoplasmic Reticulum Stress in Pancreatic Cancer

Author

Jean L. Grem, Lyudmyla Berim, Fang Yu, Jaime Abrego, Surendra K. Shukla, Saber Tadros, Audrey J. Lazenby, Enza Vernucci, Venugopal Gunda, Pankaj K. Singh, Nina V. Chaika, Aaron R. Sasson, and Ryan J. King

Subjects
0301 basic medicine, Cancer Research, medicine.medical_specialty, medicine.medical_treatment, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Pancreatic cancer, medicine, Chemotherapy, medicine.disease, Gemcitabine, Fatty acid synthase, 030104 developmental biology, Endocrinology, Oncology, Apoptosis, 030220 oncology & carcinogenesis, Lipogenesis, Unfolded protein response, biology.protein, Cancer research, Adenocarcinoma, medicine.drug
Abstract

Pancreatic adenocarcinoma is moderately responsive to gemcitabine-based chemotherapy, the most widely used single-agent therapy for pancreatic cancer. Although the prognosis in pancreatic cancer remains grim in part due to poor response to therapy, previous attempts at identifying and targeting the resistance mechanisms have not been very successful. By leveraging The Cancer Genome Atlas dataset, we identified lipid metabolism as the metabolic pathway that most significantly correlated with poor gemcitabine response in pancreatic cancer patients. Furthermore, we investigated the relationship between alterations in lipogenesis pathway and gemcitabine resistance by utilizing tissues from the genetically engineered mouse model and human pancreatic cancer patients. We observed a significant increase in fatty acid synthase (FASN) expression with increasing disease progression in spontaneous pancreatic cancer mouse model, and a correlation of high FASN expression with poor survival in patients and poor gemcitabine responsiveness in cell lines. We observed a synergistic effect of FASN inhibitors with gemcitabine in pancreatic cancer cells in culture and orthotopic implantation models. Combination of gemcitabine and the FASN inhibitor orlistat significantly diminished stemness, in part due to induction of endoplasmic reticulum (ER) stress that resulted in apoptosis. Moreover, direct induction of ER stress with thapsigargin caused a similar decrease in stemness and showed synergistic activity with gemcitabine. Our in vivo studies with orthotopic implantation models demonstrated a robust increase in gemcitabine responsiveness upon inhibition of fatty acid biosynthesis with orlistat. Altogether, we demonstrate that fatty acid biosynthesis pathway manipulation can help overcome the gemcitabine resistance in pancreatic cancer by regulating ER stress and stemness. Cancer Res; 77(20); 5503–17. ©2017 AACR.

Published
2017

22. Targetable genetic alterations of TCF4 (E2-2) drive immunoglobulin expression in the activated B-cell subtype of diffuse large B-cell lymphoma

Author

Sattva S. Neelapu, Randy D. Gascoyne, Andreas Rosenwald, Richard E. Davis, Keenan Hartert, Andrew J. Gentles, Matthew A. Lunning, Elena Hartmann, Saber Tadros, Richard Rosenquist, Robert Kridel, Michael R. Green, Julie M. Vose, Tayla Heavican, Karin Ekstrom-Smedby, Warren Fiskus, Timothy C. Greiner, Javeed Iqbal, Alyssa Bouska, Neeraj Jain, Qing Deng, Dalia Moore, Man-Chun John Ma, Gunnar Juliusson, Dhiraj Kumar, Ondrej Havranek, Christine Pak, Jason R. Westin, Kapil N. Bhalla, Fillippo Giancotti, Liu C, Scott J. Rodig, and Ash A. Alizadeh

Subjects
Immunoglobulin gene, biology, TCF4, medicine.disease, medicine.anatomical_structure, immune system diseases, hemic and lymphatic diseases, Cancer research, medicine, biology.protein, Antibody, Enhancer, Diffuse large B-cell lymphoma, Transcription factor, Gene, B cell
Abstract

The activated B-cell (ABC) subtype of diffuse large B-cell lymphoma (DLBCL) is characterized by the chronic activation of signaling initiated by immunoglobulin-μ (IgM). By analyzing DNA copy profiles of 1,000 DLBCLs, we identified gains of 18q21.2 as the most frequent genetic alteration in ABC-like DLBCL. We show that these alterations target the TCF4 (E2-2) transcription factor, and that over-expression of TCF4 leads to its occupancy on immunoglobulin gene enhancers and increased expression of IgM at the transcript and protein level. The TCF4 gene is one of the top BRD4-regulated genes in DLBCL. Using a BET proteolysis-targeting chimera (PROTAC) we show that TCF4 and IgM expression can be extinguished, and ABC-like DLBCL cells can be killed in vitro and in vivo. This highlights a novel genetic mechanism for promoting immunoglobulin signaling in ABC-like DLBCL and provides a functional rationale for the use of BET inhibitors in this disease.

Published
2017
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23. Loss of KLHL6 promotes diffuse large B-cell lymphoma growth and survival by stabilizing the mRNA decay factor roquin2

Author

Michael R. Green, Anita Saraf, Roberto Bonasio, Kristin Ingvarsdottir, Saber Tadros, Michael P. Washburn, Jaewoo Choi, Luca Busino, Kyutae Lee, and Laurence Florens

Subjects
0301 basic medicine, Cell Survival, RNA Stability, Mutant, Receptors, Antigen, B-Cell, Mice, SCID, TNFAIP3, Gene Expression Regulation, Enzymologic, Article, law.invention, 03 medical and health sciences, law, Mice, Inbred NOD, Cell Line, Tumor, medicine, Animals, Humans, Ligase activity, RNA, Messenger, Tumor Necrosis Factor alpha-Induced Protein 3, Cell Proliferation, Phenocopy, biology, Chemistry, Protein Stability, Tumor Suppressor Proteins, NF-kappa B, Ubiquitination, Cell Biology, medicine.disease, Cell biology, Ubiquitin ligase, Gene Expression Regulation, Neoplastic, Repressor Proteins, 030104 developmental biology, HEK293 Cells, Ubiquitin ligase complex, Mutation, Proteolysis, biology.protein, Suppressor, Tyrosine, Lymphoma, Large B-Cell, Diffuse, Carrier Proteins, Diffuse large B-cell lymphoma, Signal Transduction
Abstract

Kelch-like protein 6 (KLHL6) is an uncharacterized gene mutated in diffuse large B-cell lymphoma (DLBCL). Here we report that KLHL6 assembles with cullin3 to form a functional cullin–RING ubiquitin ligase. Mutations in KLHL6 inhibit its ligase activity by disrupting the interaction with cullin3. Loss of KLHL6 favours DLBCL growth and survival both in vitro and in xenograft models. We further established that the mRNA decay factor roquin2 is a substrate of KLHL6. Degradation of roquin2 is dependent on B-cell receptor activation, and requires the integrity of the Tyr691 residue in roquin2 that is essential for its interaction with KLHL6. A non-degradable roquin2(Y691F) mutant requires its RNA-binding ability to phenocopy the effect of KLHL6 loss. Stabilization of roquin2 promotes mRNA decay of the tumour suppressor and NF-κB pathway inhibitor, tumour necrosis factor-α-inducible gene 3. Collectively, our findings uncover the tumour suppressing mechanism of KLHL6. Choi et al. find that KLHL6, which is mutated in diffuse large B-cell lymphoma, is part of a ubiquitin ligase complex that targets the mRNA decay factor roquin2 for degradation and that loss of KLHL6 enhances cell survival through loss of TNFAIP3.

Published
2017

24. DNA Copy Number Gains of TCF4 (E2-2) Are Associated with Poor Outcome in Diffuse Large B-Cell Lymphoma

Author

Karin E. Smedby, Tayla Heavican, Julie M. Vose, Javeed Iqbal, Chih Long Liu, Ronald Levy, Alyssa Bouska, Saber Tadros, Elena Hartmann, Richard Rosenquist, Randy D. Gascoyne, Ash A. Alizadeh, Gunnar Juliusson, Martin Bast, Keenan Hartert, Andreas Rosenwald, Scott J. Rodig, Timothy C. Greiner, Dalia Moore, Andrew J. Gentles, Matthew A. Lunning, Robert Kridel, Michael R. Green, and Christine Pak

Subjects
Genetics, Mutation, Immunology, Cell Biology, Hematology, TCF4, Biology, SCNA, medicine.disease_cause, Biochemistry, Gene expression profiling, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, Cancer research, Enhancer, Transcription Factor Gene, Transcription factor, 030215 immunology, SNP array
Abstract

The development of B-cells is a complex process that proceeds through multiple stages and is regulated by a hierarchy of transcription factors and other physiologic signals. Each unique B-cell malignancy can be aligned with a 'normal counterpart' at one or more of these discrete developmental stages. However, with the exception of translocations of transcription factor genes, the genetic basis for this is not well defined. We performed an analysis of high-resolution single nucleotide polymorphism (SNP) microarrays from 694 diffuse large B-cell (DLBCL) tumors to identify significant somatic copy number alterations (SCNA). Through integrative analysis of 249 tumors with matched gene expression profiling (GEP) data, we identified the likely targets of these alterations and found that genes that were targeted by DNA copy number gain were significantly enriched for DNA binding activity and transcription factor function. We extended upon this observation by analyzing SNP microarray data of a further 2,716 tumors from 7 additional subtypes of B-cell malignancy. Through this analysis, we identified patterns of transcription factor alterations that aligned with the differentiation state of the 'normal B-cell counterpart' of each malignancy. This provides evidence that SCNA of B-cell transcription factors may underlie the differentiation state of B-cell malignancies. DLBCL can be divided into two subtypes based upon gene expression profiles that align with either the germinal center B-cell differentiation state (GCB-like) or a post-GCB activated B-cell state (ABC-like). Having observed an enrichment for transcription factor SCNAs in DLBCL, and an alignment between transcription factor alterations and differentiation states in other B-cell malignancies, we hypothesized that SCNAs of transcription factors may also underlie the etiology of these molecular subtypes. By testing for associations between SCNAs and cell of origin subtype, we identified three co-segregating DNA copy number gains that were significantly enriched in the ABC-like subtype. These included gains of the BCL6 and SPIB genes that have been previously observed to be associated with the ABC-like subtype. In addition, we found gains of the TCF4 (E2-2) gene to be significantly enriched in ABC-like tumors. In line with this, TCF4 alterations were significantly associated with reduced overall survival in cohorts of patients treated with either CHOP (n=232, P=0.009) or R-CHOP (n=197, P=0.041). B-cell receptor (BCR) signaling is a key survival pathway in ABC-like DLBCL, and the TCF4 gene has a defined role in promoting the expression of immunoglobulin (Ig) genes that encode the B-cell receptor (BCR). The analysis of paired SCNA and GEP data revealed a significantly higher expression of Ig genes in tumors with TCF4 DNA copy number gain compared to those without, suggesting that normal BCR expression may be deregulated by this genetic alteration. In addition, chromatin-immunoprecipitation sequencing (ChIP-seq) for TCF4 in ABC-like DLBCL cell lines also revealed binding of TCF4 to an Ig gene enhancer region. As BCR signaling can be altered by somatic mutations in the CARD11, CD79B and MYD88 genes, we evaluated the relative representation of these mutations and TCF4 DNA copy number gains using targeted deep sequencing of 124 DLBCL tumors. This revealed that TCF4 DNA copy number gains largely mutually excluded CARD11 mutations, but significantly co-segregated with both MYD88 (FDR=0.005) and CD79B (FDR=0.053) mutations. In addition, we observed significant co-segregation between CD79B and MYD88 mutations (FDR Together these data highlight an association between SCNA of B-cell transcription factors and the differentiation state of the 'normal counterpart' of the respective malignant B-cell. In line with this, we show that DNA copy number gains of the TCF4 transcription factor are associated with the ABC-like subtype of DLBCL, significantly worse overall survival, and increased Ig expression. These characteristics, in addition to the co-association between TCF4 DNA copy number gains and somatic mutations of CD79B and MYD88, suggest that TCF4 may be an important modifier of BCR signaling and contribute to the etiology of ABC-like DLBCL. Disclosures Rosenquist: Gilead Sciences: Speakers Bureau. Lunning:TG Therapeutics: Consultancy; AbbVie: Consultancy; Gilead: Consultancy; Bristol-Myer-Squibb: Consultancy; Juno: Consultancy; Genentech: Consultancy; Spectrum: Consultancy; Celgene: Consultancy; Pharmacyclics: Consultancy. Rodig:Bristol-Myers Squibb: Honoraria, Research Funding; Perkin Elmer: Membership on an entity's Board of Directors or advisory committees. Levy:Kite Pharma: Consultancy; Five Prime Therapeutics: Consultancy; Innate Pharma: Consultancy; Beigene: Consultancy; Corvus: Consultancy; Dynavax: Research Funding; Pharmacyclics: Research Funding.

Published
2016

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