Your search keyword '"John E Pimanda"' showing total 67 results

1. Targeting an Inducible SALL4-Mediated Cancer Vulnerability with Sequential Therapy

Author

Jianzhong Xi, Miao Liu, Yue Wu, Hannan Wong, Shenyi Yin, Hongbo R. Luo, Xi Tian, Alicia Stein, Julie A. I. Thoms, Yanjing V. Liu, Zhiyuan Chen, John E. Pimanda, Leslie E. Silberstein, Daniel G. Tenen, Kalpana Kumari, Nikki R. Kong, Jun Qi, Junyu Yang, Chong Gao, Yao-Chung Liu, Junsu Kwon, Li Chai, and Ashwin Unnikrishnan

Subjects

Cancer Research, Pyridines, Apoptosis, Mice, SCID, Decitabine, Article, Mice, chemistry.chemical_compound, Downregulation and upregulation, Mice, Inbred NOD, SALL4, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, microRNA, Tumor Cells, Cultured, Animals, Humans, Medicine, Cell Proliferation, business.industry, Entinostat, Cancer, DNA Methylation, medicine.disease, Xenograft Model Antitumor Assays, eye diseases, Gene Expression Regulation, Neoplastic, Oncology, chemistry, Hypomethylating agent, Benzamides, Cancer cell, Cancer research, Deoxycytidine, business, Transcription Factors

Abstract

Oncofetal protein SALL4 is critical for cancer cell survival. Targeting SALL4, however, is only applicable in a fraction of cancer patients who are positive for this gene. To overcome this limitation, we propose to induce a cancer vulnerability by engineering a partial dependency upon SALL4. Following exogenous expression of SALL4, SALL4-negative cancer cells became partially dependent on SALL4. Treatment of SALL4-negative cells with the FDA-approved hypomethylating agent 5-aza-2′-deoxycytidine (DAC) resulted in transient upregulation of SALL4. DAC pretreatment sensitized SALL4-negative cancer cells to entinostat, which negatively affected SALL4 expression through a microRNA, miRNA-205, both in culture and in vivo. Moreover, SALL4 was essential for the efficiency of sequential treatment of DAC and entinostat. Overall, this proof-of-concept study provides a framework whereby the targeting pathways such as SALL4-centered therapy can be expanded, sensitizing cancer cells to treatment by transient target induction and engineering a dependency. Significance: These findings provide a therapeutic approach for patients harboring no suitable target by induction of a SALL4-mediated vulnerability.

Published

2021

2. Induction of a SALL4-dependency for targeted cancer therapy

Author

Li Chai, Yue Wu, Daniel G. Tenen, Hongbo R. Luo, Shenyi Yin, Jianzhong Xi, Leslie E. Silberstein, Xi Tian, Miao Liu, Julie A. I. Thoms, Jun Qi, Alicia Stein, John E. Pimanda, Yanjing Liu, Junyu Yang, Yao-Chung Liu, Chong Gao, Ashwin Unnikrishnan, Nikki R. Kong, Junsu Kwon, and Zhiyuan Chen

Subjects

business.industry, Entinostat, medicine.drug_class, medicine.medical_treatment, Histone deacetylase inhibitor, Cancer, medicine.disease, eye diseases, Targeted therapy, chemistry.chemical_compound, Downregulation and upregulation, chemistry, Apoptosis, SALL4, Cancer cell, medicine, Cancer research, business

Abstract

Oncofetal protein SALL4 is critical for tumor cell survival, making it a promising target in cancer therapy. However, it is detectable only in a subset of cancer patients, which limits the therapeutic impact of a SALL4 targeted therapy. Here we report that SALL4 can be activated and/or upregulated pharmacologically by hypomethylating agents, such as 5-Aza-2’-deoxycytidine (DAC), which are used clinically, and that SALL4 negative cancer cells become SALL4 dependent following exogenous expression of SALL4. In addition, the histone deacetylase inhibitor Entinostat (ENT) negatively regulates SALL4 expression by upregulating miR-205. Both ENT and miR-205 treatment induced cell apoptosis, rescuable by SALL4 expression or miR-205 inhibition. Finally, DAC pre-treatment sensitizes SALL4 negative cancer cell lines to ENT both in culture and in vivo by upregulating SALL4. Overall, we propose a framework whereby the scope of targeted therapy can be expanded by sensitizing cancer cells to treatment by target induction and engineered dependency.SignificanceThis proof of concept study demonstrates that targeted cancer therapy can be achieved by inducing a targetable gene establishing a survival-dependency for cancer cells. For SALL4, sequential treatment of DAC and ENT could expand the scope of SALL4 targeted cancer therapy.

Published

2020

3. RNA splicing alterations induce a cellular stress response associated with poor prognosis in AML

Author

Tobias Herold, Govardhan Anande, Henry R. Hampton, Ashwin Unnikrishnan, John E. Pimanda, Nandan P. Deshpande, Aarif M. N. Batcha, Sylvain Mareschal, Jason W. H. Wong, Marc R. Wilkins, and Sören Lehmann

Subjects

0303 health sciences, Poor prognosis, Somatic cell, Myeloid leukemia, Biology, 3. Good health, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, 030220 oncology & carcinogenesis, Cellular stress response, Protein diversity, RNA splicing, Cancer research, Gene, 030304 developmental biology

Abstract

RNA splicing is a fundamental biological process that generates protein diversity from a finite set of genes. Recurrent somatic mutations of splicing factor genes are relatively uncommon in Acute Myeloid Leukemia (AML, < 20%). We examined whether RNA splicing differences exist in AML even in the absence of splicing factor mutations. Analyzing RNA-seq data from two independent cohorts of AML patients, we identified recurrent differential alternative splicing between patients with poor and good prognosis. These alternative splicing events occurred even in patients without any discernible splicing factor mutations. The alternative splicing events recurrently occurred in genes involved in specific molecular functions, primarily related to protein translation. Developing informatics tools to predict the functional impact of alternative splicing on the translated protein, we discovered that ~45% of the splicing events directly affected highly conserved protein domains. Several splicing factors were themselves misspliced in patients, and the splicing of their target transcripts were also altered. By studying differential gene expression in the same patients, we identified that alternative splicing of protein translation genes in ELNAdv patients resulted in the induction of an integrated stress response and up- regulation of inflammation-related genes. Lastly, using machine learning techniques, we identified a set of four genes whose alternative splicing can refine the accuracy of existing risk prognosis schemes and validated it in a completely independent cohort. Our discoveries therefore identify aberrant alternative splicing as a molecular feature of adverse AML with clinical relevance.

Published

2020

4. Human endogenous retroviruses form a reservoir of T cell targets in hematological cancers

Author

John E. Pimanda, Anne-Mette Bjerregaard, Andrea Marion Marquard, Kirsten Grønbæk, Aron Charles Eklund, Sine Reker Hadrup, Kathrine Valentini Jensen, Staffan Holmberg-Thydén, Anne Ortved Gang, Inge Høgh Dufva, Zoltan Szallasi, Ashwin Unnikrishnan, Amalie Kai Bentzen, Nicola Ternette, Tripti Tamhane, Annie Borch, Andreas Due Ørskov, Govardhan Anande, Marianne Bach Treppendahl, Sunil Kumar Saini, and Anders Gorm Pedersen

Subjects

0301 basic medicine, T cell, Science, viruses, T-Lymphocytes, General Physics and Astronomy, Epitopes, T-Lymphocyte, Cancer immunotherapy, Human leukocyte antigen, Biology, CD8-Positive T-Lymphocytes, Major histocompatibility complex, General Biochemistry, Genetics and Molecular Biology, Article, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, Monitoring, Immunologic, Neoplasms, MHC class I, medicine, Humans, Myeloid Cells, Epigenetics, lcsh:Science, Gene, Multidisciplinary, Gene Expression Profiling, Endogenous Retroviruses, Immunosurveillance, General Chemistry, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Hematologic Neoplasms, embryonic structures, biology.protein, Cancer research, Human genome, lcsh:Q, Immunotherapy, CD8

Abstract

Human endogenous retroviruses (HERV) form a substantial part of the human genome, but mostly remain transcriptionally silent under strict epigenetic regulation, yet can potentially be reactivated by malignant transformation or epigenetic therapies. Here, we evaluate the potential for T cell recognition of HERV elements in myeloid malignancies by mapping transcribed HERV genes and generating a library of 1169 potential antigenic HERV-derived peptides predicted for presentation by 4 HLA class I molecules. Using DNA barcode-labeled MHC-I multimers, we find CD8+ T cell populations recognizing 29 HERV-derived peptides representing 18 different HERV loci, of which HERVH-5, HERVW-1, and HERVE-3 have more profound responses; such HERV-specific T cells are present in 17 of the 34 patients, but less frequently in healthy donors. Transcriptomic analyses reveal enhanced transcription of the HERVs in patients; meanwhile DNA-demethylating therapy causes a small and heterogeneous enhancement in HERV transcription without altering T cell recognition. Our study thus uncovers T cell recognition of HERVs in myeloid malignancies, thereby implicating HERVs as potential targets for immunotherapeutic therapies., Human endogenous retroviruses (HERV) normally remain quiescent, but can be reactivated by malignant transformation. Here the authors find, via HERV peptide library testing and tetramer validation, more profound HERV transcription and associated T cell recognition in myeloid cancer patients to implicate HERVs as potential therapeutic targets.

Published

2020

5. RNA splicing alterations induce a cellular stress response associated with poor prognosis inAcute Myeloid Leukemia

Author

John E. Pimanda, Tobias Herold, Henry R. Hampton, Sylvain Mareschal, Sören Lehmann, Marc R. Wilkins, Nandan P. Deshpande, Jason W. H. Wong, Ashwin Unnikrishnan, Govardhan Anande, and Aarif M. N. Batcha

Subjects

0301 basic medicine, Cancer Research, Myeloid, RNA Splicing, Biology, medicine.disease_cause, Article, 03 medical and health sciences, Splicing factor, 0302 clinical medicine, hemic and lymphatic diseases, medicine, Humans, Gene, Biological Phenomena, Mutation, Alternative splicing, Myeloid leukemia, medicine.disease, Prognosis, Leukemia, Alternative Splicing, Leukemia, Myeloid, Acute, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, RNA splicing, Cancer research, RNA Splicing Factors

Abstract

Purpose: RNA splicing is a fundamental biological process that generates protein diversity from a finite set of genes. Recurrent somatic mutations of splicing factor genes are common in some hematologic cancers but are relatively uncommon in acute myeloid leukemia (AML, < 20% of patients). We examined whether RNA splicing differences exist in AML, even in the absence of splicing factor mutations. Experimental Design: We developed a bioinformatics pipeline to study alternative RNA splicing in RNA-sequencing data from large cohorts of patients with AML. Results: We have identified recurrent differential alternative splicing between patients with poor and good prognosis. These splicing events occurred even in patients without any discernible splicing factor mutations. Alternative splicing recurrently occurred in genes with specific molecular functions, primarily related to protein translation. Developing tools to predict the functional impact of alternative splicing on the translated protein, we discovered that approximately 45% of the splicing events directly affected highly conserved protein domains. Several splicing factors were themselves misspliced and the splicing of their target transcripts were altered. Studying differential gene expression in the same patients, we identified that alternative splicing of protein translation genes in ELNAdv patients resulted in the induction of an integrated stress response and upregulation of inflammation-related genes. Finally, using machine learning techniques, we identified a splicing signature of four genes which refine the accuracy of existing risk prognosis schemes and validated it in a completely independent cohort. Conclusions: Our discoveries therefore identify aberrant alternative splicing as a molecular feature of adverse AML with clinical relevance. See related commentary by Bowman, p. 3503

Published

2020

6. Disruption of a −35 kb Enhancer Impairs CTCF Binding and MLH1 Expression in Colorectal Cells

Author

John E. Pimanda, Rebecca C. Poulos, Deborah Packham, Rachel Williams, Qing Liu, Mathew A. Sloane, Luke B. Hesson, Jason W. H. Wong, Dominik Beck, Julie A. I. Thoms, Robyn L. Ward, Andrea Nuñez, Yizhou Huang, Nicholas J. Hawkins, and Kathy Knezevic

Subjects

0301 basic medicine, Regulation of gene expression, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, nutritional and metabolic diseases, Biology, medicine.disease, MLH1, digestive system diseases, Germline, Lynch syndrome, Chromosome conformation capture, 03 medical and health sciences, 030104 developmental biology, Oncology, CTCF, Cancer research, medicine, Enhancer, neoplasms, Chromatin immunoprecipitation

Abstract

Purpose: MLH1 is a major tumor suppressor gene involved in the pathogenesis of Lynch syndrome and various sporadic cancers. Despite their potential pathogenic importance, genomic regions capable of regulating MLH1 expression over long distances have yet to be identified. Experimental Design: Here, we use chromosome conformation capture (3C) to screen a 650-kb region flanking the MLH1 locus to identify interactions between the MLH1 promoter and distal regions in MLH1-expressing and nonexpressing cells. Putative enhancers were functionally validated using luciferase reporter assays, chromatin immunoprecipitation, and CRISPR-Cas9–mediated deletion of endogenous regions. To evaluate whether germline variants in the enhancer might contribute to impaired MLH1 expression in patients with suspected Lynch syndrome, we also screened germline DNA from a cohort of 74 patients with no known coding mutations or epimutations at the MLH1 promoter. Results: A 1.8-kb DNA fragment, 35 kb upstream of the MLH1 transcription start site enhances MLH1 gene expression in colorectal cells. The enhancer was bound by CTCF and CRISPR-Cas9–mediated deletion of a core binding region impairs endogenous MLH1 expression. A total of 5.4% of suspected Lynch syndrome patients have a rare single-nucleotide variant (G > A; rs143969848; 2.5% in gnomAD European, non-Finnish) within a highly conserved CTCF-binding motif, which disrupts enhancer activity in SW620 colorectal carcinoma cells. Conclusions: A CTCF-bound region within the MLH1-35 enhancer regulates MLH1 expression in colorectal cells and is worthy of scrutiny in future genetic screening strategies for suspected Lynch syndrome associated with loss of MLH1 expression. Clin Cancer Res; 24(18); 4602–11. ©2018 AACR.

Published

2018

7. AML-079: The PNT Domain of ERG Regulates Hematopoietic Stemness and is Required for the Maintenance of ERG-Induced Leukemia

Author

Yehudit Birger, Julie A. I. Thoms, Gilbert G. Privé, Eitan Kugler, John E. Pimanda, Shreyas Madiwale, Shai Izraeli, Avigail Rein, and Darren Yong

Subjects

Cancer Research, Myeloid, genetic structures, business.industry, ETS transcription factor family, Hematopoietic stem cell, Myeloid leukemia, Hematology, Cell cycle, medicine.disease, eye diseases, Cell biology, Leukemia, Haematopoiesis, medicine.anatomical_structure, Oncology, Medicine, sense organs, Progenitor cell, business

Abstract

The ETS transcription factor ERG has a crucial role in hematopoiesis. It is essential for hematopoietic stem cell maintenance and megakaryopoiesis. Increased expression of ERG is associated with poor prognosis in acute myeloid leukemia. Previous studies by us and others established ERG as an oncogene in human leukemia. The PNT domain of ERG is a conserved domain that, in some other ETS factors, is required for protein-protein interactions, but its function for ERG is unknown. To examine whether the PNT domain of ERG is essential for hematopoietic stem and progenitor cells (HSPC) transformation, murine fetal liver-derived-HSPC were transduced with human WT and deleted PNT (DelPNT) domain ERG and cultured in methylcellulose. In re-plating assays, the PNT domain was not essential for HSPC self-renewal yet, DelPNT-ERG-transduced cells demonstrated increased proliferation capacity. Flow cytometry analysis showed decreased expression of hematopoietic stem markers for DelPNT-ERG-transduced cells. Consistent with these findings, RNA sequencing revealed enrichment of genes associated with myeloid differentiation and loss of hematopoietic stem cell signature in HSPC transduced with DelPNT-ERG. Transduction-transplantation assays in C57B6 mice suggested that the PNT domain is not essential for leukemia development. Nevertheless, time to leukemia development was significantly delayed for delPNT-ERG-transduced mice. Gene expression analysis showed enrichment for cell cycle and Myc target genes in leukemia induced by WT-ERG as compared to DelPNT-ERG. The proximity map of ERG-interacting protein suggested that the PNT domain is essential for ERG association with the SWI-SNF complex, which was previously shown to mediate the viability and proliferation of leukemia cells, at least in part by the maintenance of Myc expression. To further validate this finding, we conducted ChIP-sequencing on myeloid progenitor cell line and revealed decreased intensities of histone modifications associated with an active enhancer at the Myc locus in cells transduced with DelPNT-ERG as compared to WT-ERG. These results suggest that in pre-leukemic conditions, the PNT domain has a role in preserving the stem cell phenotype associated with ERG, thereby preventing premature differentiation. Furthermore, ERG interaction with the SWI-SNF complex was significantly dependent on the PNT domain and may be essential for leukemia maintenance.

Published

2020

8. A Menin-MLL Inhibitor Induces Specific Chromatin Changes and Eradicates Disease in Models of MLL-Rearranged Leukemia

Author

Andrei V. Krivtsov, Richard B. Lock, Kenneth N. Ross, Florian Perner, Sarah Naomi Olsen, Tara Pritchard, David A. Claremon, Charlie Hatton, Connor D. Jones, Eric J. Earley, Lisa McDermott, Dominik Beck, Gerard McGeehan, Duohui Jing, Diego Chacon, Jayant Y. Gadrey, Andrew J. Gifford, Ali Braytee, Malcolm A. Smith, Kathryn Evans, Brian M. McKeever, Hannah Uckelmann, Heather J. Lee, Scott A. Armstrong, Benjamin K. Eschle, John E. Pimanda, Beverly A. Teicher, and Jennifer A. Perry

Subjects

0301 basic medicine, Cancer Research, Apoptosis, Chromatin remodeling, 03 medical and health sciences, Mice, 0302 clinical medicine, Proto-Oncogene Proteins, hemic and lymphatic diseases, medicine, Animals, Humans, MEN1, Oncology & Carcinogenesis, neoplasms, Cell Proliferation, Gene Rearrangement, biology, Gene Expression Regulation, Leukemic, Myeloid leukemia, Cell Differentiation, DOT1L, medicine.disease, Chromatin, Leukemia, Leukemia, Myeloid, Acute, 030104 developmental biology, KMT2A, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Transcription Factors

Abstract

© 2019 Elsevier Inc. Inhibition of the Menin (MEN1) and MLL (MLL1, KMT2A) interaction is a potential therapeutic strategy for MLL-rearranged (MLL-r) leukemia. Structure-based design yielded the potent, highly selective, and orally bioavailable small-molecule inhibitor VTP50469. Cell lines carrying MLL rearrangements were selectively responsive to VTP50469. VTP50469 displaced Menin from protein complexes and inhibited chromatin occupancy of MLL at select genes. Loss of MLL binding led to changes in gene expression, differentiation, and apoptosis. Patient-derived xenograft (PDX) models derived from patients with either MLL-r acute myeloid leukemia or MLL-r acute lymphoblastic leukemia (ALL) showed dramatic reductions of leukemia burden when treated with VTP50469. Multiple mice engrafted with MLL-r ALL remained disease free for more than 1 year after treatment. These data support rapid translation of this approach to clinical trials.

Published

2019

9. Constitutive CHK1 Expression Drives a pSTAT3-CIP2A Circuit that Promotes Glioblastoma Cell Survival and Growth

Author

Shruthi Subramanian, Zeenat Jahan, Toni Rose Jue, Anchit Khanna, Kerrie L. McDonald, Han Shen, Ashwin Unnikrishnan, Brett W. Stringer, Sylvia A. Chung, John E. Pimanda, Govardhan Anande, Bryan W. Day, Kathleen S. Ensbey, and Julie A. I. Thoms

Subjects

0301 basic medicine, STAT3 Transcription Factor, Cancer Research, Cell, Mice, Nude, Apoptosis, Mice, SCID, Biology, medicine.disease_cause, Autoantigens, 03 medical and health sciences, Mice, 0302 clinical medicine, Cell Movement, Mice, Inbred NOD, Glioma, Gene expression, medicine, Biomarkers, Tumor, Tumor Cells, Cultured, Animals, Humans, CHEK1, Phosphorylation, Molecular Biology, Cell Proliferation, Mice, Inbred BALB C, Oncogene, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Protein phosphatase 2, medicine.disease, Prognosis, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, Survival Rate, 030104 developmental biology, medicine.anatomical_structure, Oncology, Cell culture, 030220 oncology & carcinogenesis, Checkpoint Kinase 1, Cancer research, Female, Carcinogenesis, Glioblastoma

Abstract

High-constitutive activity of the DNA damage response protein checkpoint kinase 1 (CHK1) has been shown in glioblastoma (GBM) cell lines and in tissue sections. However, whether constitutive activation and overexpression of CHK1 in GBM plays a functional role in tumorigenesis or has prognostic significance is not known. We interrogated multiple glioma patient cohorts for expression levels of CHK1 and the oncogene cancerous inhibitor of protein phosphatase 2A (CIP2A), a known target of high-CHK1 activity, and examined the relationship between these two proteins in GBM. Expression levels of CHK1 and CIP2A were independent predictors for reduced overall survival across multiple glioma patient cohorts. Using siRNA and pharmacologic inhibitors we evaluated the impact of their depletion using both in vitro and in vivo models and sought a mechanistic explanation for high CIP2A in the presence of high-CHK1 levels in GBM and show that; (i) CHK1 and pSTAT3 positively regulate CIP2A gene expression; (ii) pSTAT3 and CIP2A form a recursively wired transcriptional circuit; and (iii) perturbing CIP2A expression induces GBM cell senescence and retards tumor growth in vitro and in vivo. Taken together, we have identified an oncogenic transcriptional circuit in GBM that can be destabilized by targeting CIP2A. Implications: High expression of CIP2A in gliomas is maintained by a CHK1-dependent pSTAT3–CIP2A recursive loop; interrupting CIP2A induces cell senescence and slows GBM growth adding impetus to the development of CIP2A as an anticancer drug target.

Published

2019

10. The EMT modulator SNAI1 contributes to AML pathogenesis via its interaction with LSD1

Author

Pieter Van Vlierberghe, John E. Pimanda, Jueqiong Wang, Emma Toulmin, Catherine Carmichael, Benjamin J. Shields, Steven Goossens, Nicholas C. Wong, Sona Samuel, David J. Curtis, Kathy Knezevic, Thao Nguyen, Charlotte De Maziere, Melissa J. Davis, Andrew C. Perkins, Katharina Haigh, Yizhou Huang, William R L McInnes, Béatrice Lintermans, Ross A. Dickins, Johannes Zuber, Julie A. I. Thoms, Soroor Hediyeh-Zadeh, Matthew E. Ritchie, Jody J. Haigh, Benjamin T. Kile, Anna Milne, Helen Mitchell, Dominik Beck, Geert Berx, Tim Lammens, Matthew P. McCormack, Kevin R. Gillinder, Oluseyi Kolawole, Ethan P. Oxley, Aissa Benyoucef, and Anh Vo

Subjects

0301 basic medicine, Myeloid, Epithelial-Mesenchymal Transition, Immunology, HL-60 Cells, Mice, Transgenic, Biology, Biochemistry, 03 medical and health sciences, Mice, 0302 clinical medicine, hemic and lymphatic diseases, Cell Line, Tumor, medicine, Animals, Humans, Epithelial–mesenchymal transition, 1102 Cardiorespiratory Medicine and Haematology, 1103 Clinical Sciences, 1114 Paediatrics and Reproductive Medicine, Histone Demethylases, Myeloid leukemia, KDM1A, Cell Biology, Hematology, medicine.disease, Leukemia, Haematopoiesis, Leukemia, Myeloid, Acute, 030104 developmental biology, medicine.anatomical_structure, Cell Transformation, Neoplastic, HEK293 Cells, 030220 oncology & carcinogenesis, Cancer research, Ectopic expression, Myelopoiesis, Snail Family Transcription Factors, Protein Binding

Abstract

Modulators of epithelial-to-mesenchymal transition (EMT) have recently emerged as novel players in the field of leukemia biology. The mechanisms by which EMT modulators contribute to leukemia pathogenesis, however, remain to be elucidated. Here we show that overexpression of SNAI1, a key modulator of EMT, is a pathologically relevant event in human acute myeloid leukemia (AML) that contributes to impaired differentiation, enhanced self-renewal, and proliferation of immature myeloid cells. We demonstrate that ectopic expression of Snai1 in hematopoietic cells predisposes mice to AML development. This effect is mediated by interaction with the histone demethylase KDM1A/LSD1. Our data shed new light on the role of SNAI1 in leukemia development and identify a novel mechanism of LSD1 corruption in cancer. This is particularly pertinent given the current interest surrounding the use of LSD1 inhibitors in the treatment of multiple different malignancies, including AML.

Published

2019

11. Scarcity of Recurrent Regulatory Driver Mutations in Colorectal Cancer Revealed by Targeted Deep Sequencing

Author

Deborah Packham, Jason W. H. Wong, Luke B. Hesson, Anushi Shah, Caroline Janitz, John E. Pimanda, Rebecca C. Poulos, Robyn L. Ward, Dilmi Perera, and Nicholas J. Hawkins

Subjects

Genetics, 0303 health sciences, Cancer Research, Mutation, medicine.diagnostic_test, business.industry, Cancer, Promoter, Base excision repair, medicine.disease_cause, medicine.disease, Noncoding DNA, Article, Deep sequencing, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, medicine, business, Gene, 030304 developmental biology, Genetic testing

Abstract

Background Genetic testing of cancer samples primarily focuses on protein-coding regions, despite most mutations arising in noncoding DNA. Noncoding mutations can be pathogenic if they disrupt gene regulation, but the benefits of assessing promoter mutations in driver genes by panel testing has not yet been established. This is especially the case in colorectal cancer, for which few putative driver variants at regulatory elements have been reported. Methods We designed a unique target capture sequencing panel of 39 colorectal cancer driver genes and their promoters, together with more than 35 megabases of regulatory elements focusing on gene promoters. Using this panel, we sequenced 95 colorectal cancer and matched normal samples at high depth, averaging 170× and 82× coverage, respectively. Results Our target capture sequencing design enabled improved coverage and variant detection across captured regions. We found cases with hereditary defects in mismatch and base excision repair due to deleterious germline coding variants, and we identified mutational spectra consistent with these repair deficiencies. Focusing on gene promoters and other regulatory regions, we found little evidence for base or region-specific recurrence of functional somatic mutations. Promoter elements, including TERT, harbored few mutations, with none showing strong functional evidence. Recurrent regulatory mutations were rare in our sequenced regions in colorectal cancer, though we highlight some candidate mutations for future functional studies. Conclusions Our study supports recent findings that regulatory driver mutations are rare in many cancer types and suggests that the inclusion of promoter regions into cancer panel testing is currently likely to have limited clinical utility in colorectal cancer.

Published

2019

12. A quantitative proteomics approach identifies ETV6 and IKZF1 as new regulators of an ERG-driven transcriptional network

Author

Yizhou Huang, Karen L. MacKenzie, Mark J. Raftery, Kathy Knezevic, Zara Ali, Tom Taghon, Shiyong Ma, Julie A. I. Thoms, Ineke de Jong, Dominik Beck, Ling Zhong, Yi Fang Guan, Ashwin Unnikrishnan, Jonas Larsson, Sofie Peirs, Jason W. H. Wong, Pieter Van Vlierberghe, Inge Van de Walle, and John E. Pimanda

Subjects

HIGH EXPRESSION, 0301 basic medicine, Proteomics, Proteome, Transcription, Genetic, HISTONE METHYLATION, ACUTE MYELOID-LEUKEMIA, Kaplan-Meier Estimate, Biology, DEFINITIVE HEMATOPOIESIS, 03 medical and health sciences, Ikaros Transcription Factor, Transcriptional Regulator ERG, Cell Line, Tumor, Consensus Sequence, Genetics, Transcriptional regulation, Humans, Gene Regulatory Networks, GENOME-WIDE ANALYSIS, Progenitor cell, Enhancer, ACUTE LYMPHOBLASTIC-LEUKEMIA, Proportional Hazards Models, Regulation of gene expression, Binding Sites, Base Sequence, Proto-Oncogene Proteins c-ets, Gene Expression Regulation, Leukemic, Gene regulation, Chromatin and Epigenetics, Biology and Life Sciences, MASS-SPECTROMETRY, GATA FACTORS, Prognosis, STEM-CELL, Repressor Proteins, Haematopoiesis, Leukemia, Myeloid, Acute, 030104 developmental biology, Enhancer Elements, Genetic, FACTOR-BINDING PROFILES, Cancer research, Stem cell, Erg, Developmental Biology, Protein Binding

Abstract

© The Author(s) 2016. Aberrant stem cell-like gene regulatory networks are a feature of leukaemogenesis. The ETS-related gene (ERG), an important regulator of normal haematopoiesis, is also highly expressed in T-ALL and acute myeloid leukaemia (AML). However, the transcriptional regulation of ERG in leukaemic cells remains poorly understood. In order to discover transcriptional regulators of ERG, we employed a quantitative mass spectrometry-based method to identify factors binding the 321 bp ERG +85 stem cell enhancer region in MOLT-4 T-ALL and KG-1 AML cells. Using this approach, we identified a number of known binders of the +85 enhancer in leukaemic cells along with previously unknown binders, including ETV6 and IKZF1. We confirmed that ETV6 and IKZF1 were also bound at the +85 enhancer in both leukaemic cells and in healthy human CD34+ haematopoietic stem and progenitor cells. Knockdown experiments confirmed that ETV6 and IKZF1 are transcriptional regulators not just of ERG, but also of a number of genes regulated by a densely interconnected network of seven transcription factors. At last, we show that ETV6 and IKZF1 expression levels are positively correlated with expression of a number of heptad genes in AML and high expression of all nine genes confers poorer overall prognosis.

Published

2016

13. Acute Sensitivity of Ph-like Acute Lymphoblastic Leukemia to the SMAC-Mimetic Birinapant

Author

Richard B. Lock, Hernan Carol, Jennifer Richmond, Kathryn Evans, Raushan T. Kurmasheva, John E. Pimanda, Alissa Robbins, Rosemary Sutton, Peter J. Houghton, Glenn M. Marshall, Susan L. Heatley, Deborah L. White, Malcolm A. Smith, Catherine A. Billups, and Dominik Beck

Subjects

0301 basic medicine, Cancer Research, Vincristine, Indoles, Combination therapy, Gene Expression, Apoptosis, Mice, SCID, Pharmacology, Biology, Article, Mice, 03 medical and health sciences, Mice, Inbred NOD, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Cytotoxicity, Dipeptides, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Haematopoiesis, 030104 developmental biology, Oncology, Female, Tumor necrosis factor alpha, Ex vivo, medicine.drug

Abstract

Ph-like acute lymphoblastic leukemia (ALL) is a genetically defined high-risk ALL subtype with a generally poor prognosis. In this study, we evaluated the efficacy of birinapant, a small-molecule mimetic of the apoptotic regulator SMAC, against a diverse set of ALL subtypes. Birinapant exhibited potent and selective cytotoxicity against B-cell precursor ALL (BCP-ALL) cells that were cultured ex vivo or in vivo as patient-derived tumor xenografts (PDX). Cytotoxicity was consistently most acute in Ph-like BCP-ALL. Unbiased gene expression analysis of BCP-ALL PDX specimens identified a 68-gene signature associated with birinapant sensitivity, including an enrichment for genes involved in inflammatory response, hematopoiesis, and cell death pathways. All Ph-like PDXs analyzed clustered within this 68-gene classifier. Mechanistically, birinapant sensitivity was associated with expression of TNF receptor TNFR1 and was abrogated by interfering with the TNFα/TNFR1 interaction. In combination therapy, birinapant enhanced the in vivo efficacy of an induction-type regimen of vincristine, dexamethasone, and L-asparaginase against Ph-like ALL xenografts, offering a preclinical rationale to further evaluate this SMAC mimetic for BCP-ALL treatment. Cancer Res; 76(15); 4579–91. ©2016 AACR.

Published

2016

14. MAPK/ERK2 phosphorylates ERG at serine 283 in leukemic cells and promotes stem cell signatures and cell proliferation

Author

Yizhou Huang, Karen L. MacKenzie, Dominik Beck, Santi Suryani, John E. Pimanda, Vashe Chandrakanthan, Jake Olivier, Adam Boulton, Elias N. Glaros, Richard B. Lock, John H. Bushweller, Julie A. I. Thoms, Shane R. Thomas, Kathy Knezevic, Melinda L. Tursky, and Jason W. H. Wong

Subjects

0301 basic medicine, Cancer Research, genetic structures, MAP Kinase Signaling System, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Article, Fusion gene, 03 medical and health sciences, Transcriptional Regulator ERG, Cell Line, Tumor, Serine, Humans, Protein phosphorylation, Phosphorylation, Progenitor cell, Cell Proliferation, Binding Sites, Leukemia, Myeloid leukemia, Hematology, Hematopoietic Stem Cells, eye diseases, Leukemia, Myeloid, Acute, Haematopoiesis, 030104 developmental biology, Oncology, Cancer research, sense organs, Stem cell, Transcriptome, Protein Processing, Post-Translational, Erg

Abstract

Aberrant ERG (v-ets avian erythroblastosis virus E26 oncogene homolog) expression drives leukemic transformation in mice and high expression is associated with poor patient outcomes in acute myeloid leukemia (AML) and T-acute lymphoblastic leukemia (T-ALL). Protein phosphorylation regulates the activity of many ETS factors but little is known about ERG in leukemic cells. To characterize ERG phosphorylation in leukemic cells, we applied liquid chromatography coupled tandem mass spectrometry and identified five phosphorylated serines on endogenous ERG in T-ALL and AML cells. S283 was distinct as it was abundantly phosphorylated in leukemic cells but not in healthy hematopoietic stem and progenitor cells (HSPCs). Overexpression of a phosphoactive mutant (S283D) increased expansion and clonogenicity of primary HSPCs over and above wild-type ERG. Using a custom antibody, we screened a panel of primary leukemic xenografts and showed that ERG S283 phosphorylation was mediated by mitogen-activated protein kinase/extracellular signal-regulated kinase (MAPK/ERK) signaling and in turn regulated expression of components of this pathway. S283 phosphorylation facilitates ERG enrichment and transactivation at the ERG +85 HSPC enhancer that is active in AML and T-ALL with poor prognosis. Taken together, we have identified a specific post-translational modification in leukemic cells that promotes progenitor proliferation and is a potential target to modulate ERG-driven transcriptional programs in leukemia.

Published

2016

15. Jak2V617F and Dnmt3a loss cooperate to induce myelofibrosis through activated enhancer-driven inflammation

Author

Rebecca Austin, Brad Wackrow, Joanne Green, Victoria Ling, Jasmin Straube, Leanne Cooper, Therese Vu, Axia Song, Konstanze Döhner, Luke B. Hesson, Matthew Heidecker, Eva Baxter, John E. Pimanda, Dirk Heckl, Megan Bywater, Stephen H. Kazakoff, Nicola Waddell, Sebastien Jacquelin, Raajit K. Rampal, Geoffrey R. Hill, Steven W. Lane, Frank Stegelmann, Amy H. Porter, and Lars Bullinger

Subjects

0301 basic medicine, Immunology, Mutation, Missense, Inflammation, Biology, Biochemistry, DNA Methyltransferase 3A, 03 medical and health sciences, Mice, Polycythemia vera, medicine, Animals, Humans, DNA (Cytosine-5-)-Methyltransferases, Progenitor cell, Enhancer, Myelofibrosis, Cell Biology, Hematology, Janus Kinase 2, medicine.disease, Hematopoietic Stem Cells, Mice, Mutant Strains, Chromatin, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Amino Acid Substitution, Primary Myelofibrosis, Hematologic Neoplasms, embryonic structures, Cancer research, Bone marrow, medicine.symptom, Signal Transduction

Abstract

Myeloproliferative neoplasms (MPNs) are a group of blood cancers that arise following the sequential acquisition of genetic lesions in hematopoietic stem and progenitor cells (HSPCs). We identify mutational cooperation between Jak2V617F expression and Dnmt3a loss that drives progression from early-stage polycythemia vera to advanced myelofibrosis. Using in vivo, clustered regularly interspaced short palindromic repeats (CRISPR) with CRISPR-associated protein 9 (Cas9) disruption of Dnmt3a in Jak2V617F knockin HSPC, we show that Dnmt3a loss blocks the accumulation of erythroid elements and causes fibrotic infiltration within the bone marrow and spleen. Transcriptional analysis and integration with human data sets identified a core DNMT3A-driven gene-expression program shared across multiple models and contexts of Dnmt3a loss. Aberrant self-renewal and inflammatory signaling were seen in Dnmt3a−/− Jak2V617F HSPC, driven by increased chromatin accessibility at enhancer elements. These findings identify oncogenic cooperativity between Jak2V617F-driven MPN and Dnmt3a loss, leading to activation of HSPC enhancer–driven inflammatory signaling.

Published

2018

16. Srsf2P95H initiates myeloid bias and myelodysplastic/myeloproliferative syndrome from hemopoietic stem cells

Author

Meaghan Wall, John E. Pimanda, Govardhan Anande, Scott Taylor, Jane Jialu Xu, Louise E. Purton, Alistair M. Chalk, Shuh Ying Tan, Ashwin Unnikrishnan, Carl R. Walkley, and Monique Smeets

Subjects

0301 basic medicine, Myeloid, Myelodysplastic syndromes, Immunology, Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, Transplantation, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, Myeloproliferative Disorders, medicine.anatomical_structure, medicine, Cancer research, Erythropoiesis, Myelopoiesis, Exome

Abstract

Mutations in SRSF2 occur in myelodysplastic syndromes (MDS) and MDS/myeloproliferative neoplasms (MPN). SRSF2 mutations cluster at proline 95, with the most frequent mutation being a histidine (P95H) substitution. They undergo positive selection, arise early in the course of disease, and have been identified in age-related clonal hemopoiesis. It is not clear how mutation of SRSF2 modifies hemopoiesis or contributes to the development of myeloid bias or MDS/MPN. Two prior mouse models of Srsf2P95H mutation have been reported; however, these models do not recapitulate many of the clinical features of SRSF2-mutant disease and relied on bone marrow (BM) transplantation stress to elicit the reported phenotypes. We describe a new conditional murine Srsf2P95H mutation model, where the P95H mutation is expressed physiologically and heterozygously from its endogenous locus after Cre activation. Using multiple Cre lines, we demonstrate that during native hemopoiesis (ie, no BM transplantation), the Srsf2P95H mutation needs to occur within the hemopoietic stem-cell-containing populations to promote myelomonocytic bias and expansion with corresponding transcriptional and RNA splicing changes. With age, nontransplanted Srsf2P95H animals developed a progressive, transplantable disease characterized by myeloid bias, morphological dysplasia, and monocytosis, hallmarks of MDS/MPN in humans. Analysis of cooccurring mutations within the BM demonstrated the acquisition of additional mutations that are recurrent in humans with SRSF2 mutations. The tractable Srsf2P95H/+ knock-in model we have generated is highly relevant to human disease and will serve to elucidate the effect of SRSF2 mutations on initiation and maintenance of MDS/MPN.

Published

2018

17. Systematic Screening of Promoter Regions Pinpoints Functional Cis-Regulatory Mutations in a Cutaneous Melanoma Genome

Author

Anushi Shah, John E. Pimanda, Jason W. H. Wong, Rebecca C. Poulos, Dominik Beck, and Julie A. I. Thoms

Subjects

Cancer Research, Skin Neoplasms, Transcription, Genetic, Sp1 Transcription Factor, Mutant, Biology, medicine.disease_cause, Genome, Germline mutation, Genes, Reporter, Cell Line, Tumor, medicine, Humans, Regulatory Elements, Transcriptional, Promoter Regions, Genetic, Melanoma, Molecular Biology, Gene, Transcription factor, Genetics, Models, Genetic, Genome, Human, NADH Dehydrogenase, Promoter, Molecular biology, NDUFB9, Chromatin, Genetic Techniques, Oncology, Mutation, Carcinogenesis

Abstract

With the recent discovery of recurrent mutations in the TERT promoter in melanoma, identification of other somatic causal promoter mutations is of considerable interest. Yet, the impact of sequence variation on the regulatory potential of gene promoters has not been systematically evaluated. This study assesses the impact of promoter mutations on promoter activity in the whole-genome sequenced malignant melanoma cell line COLO-829. Combining somatic mutation calls from COLO-829 with genome-wide chromatin accessibility and histone modification data revealed mutations within promoter elements. Interestingly, a high number of potential promoter mutations ( n = 23) were found, a result mirrored in subsequent analysis of TCGA whole-melanoma genomes. The impact of wild-type and mutant promoter sequences were evaluated by subcloning into luciferase reporter vectors and testing their transcriptional activity in COLO-829 cells. Of the 23 promoter regions tested, four mutations significantly altered reporter activity relative to wild-type sequences. These data were then subjected to multiple computational algorithms that score the cis -regulatory altering potential of mutations. These analyses identified one mutation, located within the promoter region of NDUFB9 , which encodes the mitochondrial NADH dehydrogenase (ubiquinone) 1 beta subcomplex 9, to be recurrent in 4.4% (19 of 432) of TCGA whole-melanoma exomes. The mutation is predicted to disrupt a highly conserved SP1/KLF transcription factor binding motif and its frequent co-occurrence with mutations in the coding sequence of NF1 supports a pathologic role for this mutation in melanoma. Taken together, these data show the relatively high prevalence of promoter mutations in the COLO-829 melanoma genome, and indicate that a proportion of these significantly alter the regulatory potential of gene promoters. Implications: Genomic-based screening within gene promoter regions suggests that functional cis -regulatory mutations may be common in melanoma genomes, highlighting the need to examine their role in tumorigenesis. Mol Cancer Res; 13(8); 1218–26. ©2015 AACR . This article is featured in Highlights of This Issue, [p. 1161][1] [1]: /lookup/volpage/13/1161?iss=8

Published

2015

18. Clinical significance of cancerous inhibitor of protein phosphatase 2A in human cancers

Author

Anchit Khanna and John E. Pimanda

Subjects

0301 basic medicine, Cancer Research, Oncogene, Bortezomib, Drug resistance, Protein phosphatase 2, Biology, Bioinformatics, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, medicine, Cancer research, Biomarker (medicine), Clinical significance, CHEK1, Erlotinib, medicine.drug

Abstract

Cancerous Inhibitor of Protein Phosphatase 2A (CIP2A), a recently identified oncogene, has emerged as a potential drug target for a range of different tumor types. High CIP2A expression has been reported in almost all solid organ cancers and in some hematological tumors and is associated with high grade and poor prognosis. Notably, high CIP2A expression is determined in over 70% of tumor patient samples in the majority of human cancers. High expression of CIP2A has also been proposed as a useful biomarker that predicts therapeutic response to chemotherapeutics such as Bortezomib, Erlotinib, Checkpoint Kinase 1 inhibitors and pro-senescence based therapies. In this review, we highlight, critically evaluate and discuss the ambiguity in CIP2A's prognostic role in different human cancers and its role in modulating response and resistance to chemotherapeutics.

Published

2015

19. Granulomonocytic progenitors are key target cells of azacytidine in higher risk myelodysplastic syndromes and acute myeloid leukemia

Author

Emmanuelle Clappier, Ashfaq Ali, Raphael Itzykson, Aline Massé, Aline Renneville, Jean Soulier, Hervé Dombret, Reinaldo Dal Bello, John E. Pimanda, Justine Penneroux, Emmanuel Raffoux, Raouf Ben Abdelali, Pierre Fenaux, Lucie Hernandez, Lionel Adès, Claude Preudhomme, Alexandre Puissant, Ashwin Unnikrishnan, and Samuel Quentin

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, Antimetabolites, Antineoplastic, Myeloid, Pilot Projects, 03 medical and health sciences, Internal medicine, medicine, Biomarkers, Tumor, Humans, Prospective Studies, Progenitor cell, Regulation of gene expression, Hematology, business.industry, Myelodysplastic syndromes, Multipotent Stem Cells, Myeloid leukemia, High-Throughput Nucleotide Sequencing, medicine.disease, Hematopoietic Stem Cells, Prognosis, Gene Expression Regulation, Neoplastic, Leukemia, Leukemia, Myeloid, Acute, 030104 developmental biology, medicine.anatomical_structure, Oncology, Myelodysplastic Syndromes, Cancer research, Azacitidine, business, Granulocytes

Published

2017

20. AZA-MS: A novel multiparameter mass spectrometry method to determine the intracellular dynamics of azacitidine therapy in vivo

Author

Mark J. Raftery, Russell Pickford, Ashwin Unnikrishnan, John E. Pimanda, Arjun Verma, Luke B. Hesson, A N Q Vo, and Andrea Nuñez

Subjects

0301 basic medicine, Cancer Research, Cytoplasm, RNA methylation, Azacitidine, Immunology, Mass Spectrometry, 03 medical and health sciences, chemistry.chemical_compound, In vivo, Bone Marrow, Cell Line, Tumor, medicine, Humans, heterocyclic compounds, neoplasms, RNA, Cytidine, Hematology, DNA Methylation, Deoxyribonucleoside, stomatognathic diseases, 030104 developmental biology, DNA demethylation, Oncology, chemistry, Drug Resistance, Neoplasm, Myelodysplastic Syndromes, Cancer research, Original Article, DNA, medicine.drug

Abstract

© 2018 Macmillan Publishers Limited, part of Springer Nature. All rights reserved. The cytidine analogue, 5-azacytidine (AZA; 5-AZA-cR), is the primary treatment for myelodysplastic syndrome and chronic myelomonocytic leukaemia. However, only ∼50% of treated patients will respond to AZA and the drivers of AZA resistance in vivo are poorly understood. To better understand the intracellular dynamics of AZA upon therapy and decipher the molecular basis for AZA resistance, we have developed a novel, multiparameter, quantitative mass spectrometry method (AZA-MS). Using AZA-MS, we have accurately quantified the abundance of the ribonucleoside (5-AZA-cR) and deoxyribonucleoside (5-AZA-CdR) forms of AZA in RNA, DNA and the cytoplasm within the same sample using nanogram quantities of input material. We report that although AZA induces DNA demethylation in a dose-dependent manner, it has no corresponding effect on RNA methylation. By applying AZA-MS to primary bone marrow samples from patients undergoing AZA therapy, we have identified that responders accumulate more 5-AZA-CdR in their DNA compared with nonresponders. AZA resistance was not a result of impaired AZA metabolism or intracellular accumulation. Furthermore, AZA-MS has helped to uncover different modes of AZA resistance. Whereas some nonresponders fail to incorporate sufficient 5-AZA-CdR into DNA, others incorporate 5-AZA-CdR and effect DNA demethylation like AZA responders, but show no clinical benefit.

Published

2017

21. Overexpression of ERG in cord blood progenitors promotes expansion and recapitulates molecular signatures of high ERG leukemias

Author

Yizhou Huang, Laura A. Richards, Karen L. MacKenzie, A Kumari, Shai Izraeli, Melinda L. Tursky, Liat Goldberg, Eun Kyung Lee, Kathy Knezevic, Kathryn Evans, Jason W. H. Wong, Julie A. I. Thoms, John E. Pimanda, Jake Olivier, Richard B. Lock, Dominik Beck, Ashwin Unnikrishnan, and Jonathan M. Morris

Subjects

Cancer Research, genetic structures, Genetic Vectors, CD34, Antigens, CD34, Biology, Transcriptional Regulator ERG, Transduction, Genetic, hemic and lymphatic diseases, Gene expression, medicine, Humans, Progenitor cell, Cells, Cultured, Cell Proliferation, Stem Cells, High-Throughput Nucleotide Sequencing, Myeloid leukemia, Hematology, Fetal Blood, medicine.disease, eye diseases, Leukemia, Myeloid, Acute, Leukemia, Haematopoiesis, Cell Transformation, Neoplastic, Retroviridae, Gene Expression Regulation, Oncology, Mutation, Immunology, Trans-Activators, Cancer research, sense organs, Stem cell, Transcriptome, Erg

Abstract

High expression of the ETS family transcription factor ERG is associated with poor clinical outcome in acute myeloid leukemia (AML) and acute T-cell lymphoblastic leukemia (T-ALL). In murine models, high ERG expression induces both T-ALL and AML. However, no study to date has defined the effect of high ERG expression on primary human hematopoietic cells. In the present study, human CD34+ cells were transduced with retroviral vectors to elevate ERG gene expression to levels detected in high ERG AML. RNA sequencing was performed on purified populations of transduced cells to define the effects of high ERG on gene expression in human CD34+ cells. Integration of the genome-wide expression data with other data sets revealed that high ERG drives an expression signature that shares features of normal hematopoietic stem cells, high ERG AMLs, early T-cell precursor-ALLs and leukemic stem cell signatures associated with poor clinical outcome. Functional assays linked this gene expression profile to enhanced progenitor cell expansion. These results support a model whereby a stem cell gene expression network driven by high ERG in human cells enhances the expansion of the progenitor pool, providing opportunity for the acquisition and propagation of mutations and the development of leukemia.

Published

2014

22. 2008 - ALTERED EXPRESSION OF EPITHELIAL TO MESENCHYMAL TRANSITION MODULATORS IN ACUTE MYELOID LEUKAEMIA - A MODEL OF LSD1 CORRUPTION

Author

Thao Nguyen, Matthew E. Ritchie, Charlotte De Maziere, Kathy Knezevic, Melissa J. Davis, Anh Vo, Matthew P. McCormack, Jueqiong Wang, Jody J. Haigh, Soroor Hediyeh Zadeh, Anna Milne, Julie A. I. Thoms, Benjamin J. Shields, Steven Goossens, Geert Berx, Katharina Haigh, Benjamin T. Kile, Yizhou Huang, Catherine Carmichael, and John E. Pimanda

Subjects

Cancer Research, Myeloid, biology, Cell Biology, Hematology, Haematopoiesis, medicine.anatomical_structure, Histone, hemic and lymphatic diseases, SNAI1, Genetics, biology.protein, medicine, Cancer research, Demethylase, Epithelial–mesenchymal transition, Epigenetics, Stem cell, Molecular Biology

Abstract

Aberrant expression of the SNAIL & ZEB families of Epithelial to Mesenchymal Transition (EMT) modulators is an emerging theme in acute leukemia biology. EMT regulation has long been implicated in epithelial tumor pathogenesis, however a role in hematopoietic malignancy has only recently been explored. In this study, we describe a novel mechanism of AML pathogenesis involving SNAI1 induced epigenetic dysregulation via corruption of the histone demethylase LSD1. SNAI1 is expressed ∼10-fold higher in AML blasts compared to normal hematopoietic cells, suggesting a functional role for SNAI1 in AML. Indeed, SNAI1 knockdown induces differentiation in human AML cells, while Snai1 deletion delays tumour onset in mouse AML models. Furthermore, transgenic Snai1 expression perturbs myeloid development, resulting in accumulation of immature myeloid cells with enhanced self-renewal capacity - ultimately predisposing mice to AML. Intriguingly, impaired myeloid development by Snai1 absolutely requires its interaction with Lsd1, a H3K4 histone demethylase that has emerged as a novel therapeutic target in AML. Mechanistically, this interaction results in corruption of Lsd1 function via aberrant recruitment to Snai1 gene targets, and sequestration away from its own targets. Ultimately, this leads to changes in H3K4me1/2 methylation at specific promoters and enhancers, and subsequently altered gene expression. This model provides insight into the mechanisms by which LSD1 can be perturbed in AML, and offers a possible explanation for why LSD1 inhibition/loss has somewhat dichotomous effects on normal and malignant hematopoietic stem cells. Furthermore, as other members of the SNAIL and ZEB families are known to interact with LSD1, it is likely that this model will be more broadly applicable to other EMT modulators in AML, representing a possible new focus for future therapeutic studies.

Published

2019

23. Cancerous Inhibitor of Protein Phosphatase 2A, an Emerging Human Oncoprotein and a Potential Cancer Therapy Target

Author

John E. Pimanda, Jukka Westermarck, and Anchit Khanna

Subjects

Oncogene Proteins, Regulation of gene expression, Cancer Research, Effector, Chemistry, Phosphatase, Intracellular Signaling Peptides and Proteins, Membrane Proteins, macromolecular substances, Protein phosphatase 2, Autoantigens, Gene Expression Regulation, Neoplastic, Mice, Cell Transformation, Neoplastic, Oncology, Neoplasms, Cancer cell, Cancer research, Animals, Humans, Phosphorylation, E2F1, Molecular Targeted Therapy, Protein Phosphatase 2, Protein kinase B

Abstract

Protein phosphatase 2A (PP2A) complexes function as tumor suppressors by inhibiting the activity of several critical oncogenic signaling pathways. Consequently, inhibition of the PP2A phosphatase activity is one of many prerequisites for the transformation of normal human cells into cancerous cells. However, mechanisms for PP2A inactivation in human cancers are poorly understood. The aberrant expression of cancerous inhibitor of protein phosphatase 2A (CIP2A), a recently identified endogenous PP2A inhibitor in malignant cells, is one such mechanism. Various independent studies have validated CIP2A's role in promoting tumor growth and resistance to apoptosis and senescence-inducing therapies. Notably, high CIP2A expression predicts poor patient prognosis in several human cancer types. Among the oncogenic proteins dephosphorylated by PP2A, the MYC oncoprotein, which is phosphorylated at serine 62, has surfaced as a marker for the oncogenic activity of CIP2A. The positive-feedback loop between CIP2A and MYC augments the activity of MYC in cancer cells. In addition, CIP2A promotes the phosphorylation and activity of additional oncoproteins, including E2F1 and AKT. However, CIP2A is not essential for normal mouse growth and development. These findings indicate that CIP2A is a novel anticancer target based on PP2A reactivation and inhibition of the oncogenic activity of its downstream effectors. The potential approaches and feasibility of targeting CIP2A are discussed here. Cancer Res; 73(22); 6548–53. ©2013 AACR.

Published

2013

24. Chk1 Targeting Reactivates PP2A Tumor Suppressor Activity in Cancer Cells

Author

Jukka Westermarck, Merja A. Helenius, Caj Haglund, Agnieszka Szwajda, Anni Laine, Yuba Raj Pokharel, Mike R. Russel, Carsten Weiss, John E. Pimanda, Camilla Böckelman, Tapio Visakorpi, Anchit Khanna, Juha Klefström, Johanna I. Partanen, Ilona Schreck, Ari Ristimäki, Tero Aittokallio, Otto Kauko, Kristina A. Cole, Turker Bilgen, and Stefanie Bormann

Subjects

Cancer Research, animal structures, Cell Survival, medicine.medical_treatment, Biology, medicine.disease_cause, Autoantigens, environment and public health, Article, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Neuroblastoma, Tumor Cells, Cultured, medicine, Humans, Molecular Targeted Therapy, Protein Phosphatase 2, CHEK1, Protein Kinase Inhibitors, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Kinase, Effector, Cell growth, Tumor Suppressor Proteins, Intracellular Signaling Peptides and Proteins, Membrane Proteins, medicine.disease, 3. Good health, Cell biology, Enzyme Activation, Gene Expression Regulation, Neoplastic, enzymes and coenzymes (carbohydrates), Oncology, 030220 oncology & carcinogenesis, Checkpoint Kinase 1, embryonic structures, Cancer cell, biological phenomena, cell phenomena, and immunity, Carcinogenesis, Protein Kinases

Abstract

Checkpoint kinase Chk1 is constitutively active in many cancer cell types and new generation Chk1 inhibitors show marked antitumor activity as single agents. Here we present a hitherto unrecognized mechanism that contributes to the response of cancer cells to Chk1-targeted therapy. Inhibiting chronic Chk1 activity in cancer cells induced the tumor suppressor activity of protein phosphatase protein phosphatase 2A (PP2A), which by dephosphorylating MYC serine 62, inhibited MYC activity and impaired cancer cell survival. Mechanistic investigations revealed that Chk1 inhibition activated PP2A by decreasing the transcription of cancerous inhibitor of PP2A (CIP2A), a chief inhibitor of PP2A activity. Inhibition of cancer cell clonogenicity by Chk1 inhibition could be rescued in vitro either by exogenous expression of CIP2A or by blocking the CIP2A-regulated PP2A complex. Chk1-mediated CIP2A regulation was extended in tumor models dependent on either Chk1 or CIP2A. The clinical relevance of CIP2A as a Chk1 effector protein was validated in several human cancer types, including neuroblastoma, where CIP2A was identified as an NMYC-independent prognostic factor. Because the Chk1–CIP2A–PP2A pathway is driven by DNA-PK activity, functioning regardless of p53 or ATM/ATR status, our results offer explanative power for understanding how Chk1 inhibitors mediate single-agent anticancer efficacy. Furthermore, they define CIP2A-PP2A status in cancer cells as a pharmacodynamic marker for their response to Chk1-targeted therapy. Cancer Res; 73(22); 6757–69. ©2013 AACR.

Published

2013

25. Bivalent promoter marks and a latent enhancer may prime the leukaemia oncogene LMO1 for ectopic expression in T-cell leukaemia

Author

Kathy Knezevic, S H Oram, Jonathan Sive, Julie A. I. Thoms, Judith Schütte, Sarah Kinston, Richard B. Lock, Fernando J Calero-Nieto, John E. Pimanda, and Berthold Göttgens

Subjects

Chromatin Immunoprecipitation, Cancer Research, Mice, Transgenic, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Mice, 03 medical and health sciences, 0302 clinical medicine, Transcriptional regulation, Animals, Humans, transcriptional regulation, Promoter Regions, Genetic, Enhancer, 030304 developmental biology, 0303 health sciences, Reporter gene, Oncogene, bivalent chromatin, Promoter, Oncogenes, Hematology, LIM Domain Proteins, Molecular biology, DNA-Binding Proteins, Haematopoiesis, Enhancer Elements, Genetic, Oncology, 030220 oncology & carcinogenesis, Original Article, LMO1, Ectopic expression, T-ALL, Chromatin immunoprecipitation, Transcription Factors

Abstract

LMO1 is a transcriptional regulator and a T-acute lymphoblastic leukaemia (T-ALL) oncogene. Although first identified in association with a chromosomal translocation in T-ALL, the ectopic expression of LMO1 occurs far more frequently in the absence of any known mutation involving its locus. Given that LMO1 is barely expressed in any haematopoietic lineage, and activation of transcriptional drivers in leukaemic cells is not well described, we investigated the regulation of this gene in normal haematopoietic and leukaemic cells. We show that LMO1 has two promoters that drive reporter gene expression in transgenic mice to neural tissues known to express endogenous LMO1. The LMO1 promoters display bivalent histone marks in multiple blood lineages including T-cells, and a 3' flanking region at LMO1 +57 contains a transcriptional enhancer that is active in developing blood cells in transgenic mouse embryos. The LMO1 promoters become activated in T-ALL together with the 3' enhancer, which is bound in primary T-ALL cells by SCL/TAL1 and GATA3. Taken together, our results show that LMO1 is poised for expression in normal progenitors, where activation of SCL/TAL1 together with a breakdown of epigenetic repression of LMO1 regulatory elements induces ectopic LMO1 expression that contributes to the development and maintenance of T-ALL.

Published

2013

26. Myelodysplastic syndromes are propagated by rare and distinct human cancer stem cells in vivo

Author

Peter Hokland, Luca Malcovati, Teresa Mortera-Blanco, Paresh Vyas, Mohsen Karimi, Magnus Tobiasson, Lennart Nilsson, Stefan N. Constantinescu, Rikard Erlandsson, John E. Pimanda, Helen Doolittle, Stephen Taylor, Mtakai Ngara, Laura Stenson, Supat Thongjuea, Pierre Fenaux, Onima Chowdhury, Claus Nerlov, David C. Wedge, Peter J. Campbell, Elli Papaemmanuil, Sten Linnarsson, Christian Scharenberg, Dag Josefsen, Andrea Pellagatti, Eva Hellström-Lindberg, Gudrun Göhring, Eleni Giannoulatou, Sten Eirik W. Jacobsen, Qiaolin Deng, Brigitte Schlegelberger, Kristina Anderson, David G. Bowen, Mario Cazzola, Sally Ann Clark, Iain C. Macaulay, Gunnar Kvalheim, Sara Duarte, Adam J. Mead, Sudhir Tauro, Jacqueline Boultwood, Alice Giustacchini, Ingunn Dybedal, Una Kjällquist, Petter S. Woll, Ashwin Unnikrishnan, Mette Holm, and Rickard Sandberg

Subjects

Cancer Research, Biology, medicine.disease_cause, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Antigens, CD, Mice, Inbred NOD, In vivo, Cancer stem cell, hemic and lymphatic diseases, medicine, Animals, Humans, Genetic Predisposition to Disease, Progenitor cell, 030304 developmental biology, Genetics, Mutation, 0303 health sciences, business.industry, Gene Expression Profiling, Myelodysplastic syndromes, Cell Biology, Flow Cytometry, Prognosis, medicine.disease, 3. Good health, Gene expression profiling, Oncology, Myelodysplastic Syndromes, 030220 oncology & carcinogenesis, Cancer cell, Immunology, Neoplastic Stem Cells, Cancer research, Chromosomes, Human, Pair 5, Heterografts, Chromosome Deletion, Stem cell, business, Human cancer, 030215 immunology

Abstract

Evidence for distinct human cancer stem cells (CSCs) remains contentious and the degree to which differentcancer cells contribute to propagating malignancies in patients remains unexplored. In low- to intermediate-risk myelodysplastic syndromes (MDS), we establish the existence of rare multipotent MDS stem cells (MDS-SCs), and their hierarchical relationship to lineage-restricted MDS progenitors. All identified somatically acquired genetic lesions were backtracked to distinct MDS-SCs, establishing their distinct MDS-propagating function invivo. In isolated del(5q)-MDS, acquisition of del(5q) preceded diverse recurrent driver mutations. Sequential analysis in del(5q)-MDS revealed genetic evolution in MDS-SCs and MDS-progenitors prior to leukemic transformation. These findings provide definitive evidence for rare human MDS-SCs invivo, with extensive implications for the targeting of the cells required and sufficient for MDS-propagation. © 2014 Elsevier Inc.

Published

2016

27. Integrated Genetic, Epigenetic, and Transcriptional Profiling Identifies Molecular Pathways in the Development of Laterally Spreading Tumors

Author

Caroline E. Ford, Regina Ryan, John E. Pimanda, Michael J. Bourke, Ashraf Dower, Luke B. Hesson, Chau To Kwok, Dominik Beck, Andrea Nuñez, Nicholas J. Hawkins, Sameer Srivastava, Benedict Ng, Deborah Packham, Peter Zarzour, Jason W. H. Wong, Robyn L. Ward, and Mathew A. Sloane

Subjects

0301 basic medicine, Adenoma, Cancer Research, Gene Dosage, Biology, Malignant transformation, Epigenesis, Genetic, Transcriptome, 03 medical and health sciences, Humans, Gene Regulatory Networks, Epigenetics, Molecular Biology, Sequence Analysis, RNA, Gene Expression Profiling, Wnt signaling pathway, Computational Biology, Epigenome, Genomics, DNA Methylation, Actin cytoskeleton, SLITRK1, 3. Good health, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, DNA methylation, Mutation, Cancer research, Female, Colorectal Neoplasms, Genome-Wide Association Study

Abstract

Laterally spreading tumors (LST) are colorectal adenomas that develop into extremely large lesions with predominantly slow progression to cancer, depending on lesion subtype. Comparing and contrasting the molecular profiles of LSTs and colorectal cancers offers an opportunity to delineate key molecular alterations that drive malignant transformation in the colorectum. In a discovery cohort of 11 LSTs and paired normal mucosa, we performed a comprehensive and unbiased screen of the genome, epigenome, and transcriptome followed by bioinformatics integration of these data and validation in an additional 84 large, benign colorectal lesions. Mutation rates in LSTs were comparable with microsatellite-stable colorectal cancers (2.4 vs. 2.6 mutations per megabase); however, copy number alterations were infrequent (averaging only 1.5 per LST). Frequent genetic, epigenetic, and transcriptional alterations were identified in genes not previously implicated in colorectal neoplasia (ANO5, MED12L, EPB41L4A, RGMB, SLITRK1, SLITRK5, NRXN1, ANK2). Alterations to pathways commonly mutated in colorectal cancers, namely, the p53, PI3K, and TGFβ pathways, were rare. Instead, LST-altered genes converged on axonal guidance, Wnt, and actin cytoskeleton signaling. These integrated omics data identify molecular features associated with noncancerous LSTs and highlight that mutation load, which is relatively high in LSTs, is a poor predictor of invasive potential. Implications: The novel genetic, epigenetic, and transcriptional changes associated with LST development reveal important insights into why some adenomas do not progress to cancer. The finding that LSTs exhibit a mutational load similar to colorectal carcinomas has implications for the validity of molecular biomarkers for assessing cancer risk. Mol Cancer Res; 14(12); 1217–28. ©2016 AACR.

Published

2016

28. Declined presentation mesenchymal stem cell-like cell mediated hematopoietic stem cell generation from non-hemogenic endothelial cells

Author

Yizhou Huang, John E. Pimanda, Vashe Chandrakanthan, Samir Taoudi, Brendan Lee, Kathy Knezevic, Young Chan Kang, Carl Power, Ashwin Unnikrishnan, Qiao Qiao, William R. Walsh, Dominik Beck, Rema A. Oliver, and Chris Lee

Subjects

Cancer Research, Hematopoietic stem cell, Stem cell factor, Amniotic stem cells, Cell Biology, Hematology, Biology, Cell biology, Endothelial stem cell, medicine.anatomical_structure, Cancer stem cell, Genetics, medicine, Stem cell, Molecular Biology, Stem cell transplantation for articular cartilage repair, Adult stem cell

Published

2017

29. A Runx1-Smad6 Rheostat Controls Runx1 Activity during Embryonic Hematopoiesis

Author

Katrin Ottersbach, Sarah Kinston, Berthold Göttgens, Stéphanie G. I. Polderdijk, Anja Kolb-Kokocinski, Mary E. Janes, Marella F. T. R. de Bruijn, Nicola K. Wilson, Niv Pencovich, Kathy Knezevic, Thomas Bee, John E. Pimanda, and Yoram Groner

Subjects

Smad6 Protein, Molecular Sequence Data, Mice, Transgenic, SMAD, Regulatory Sequences, Nucleic Acid, Biology, Mice, chemistry.chemical_compound, hemic and lymphatic diseases, Chlorocebus aethiops, Animals, Humans, Molecular Biology, Transcription factor, Base Sequence, GATA2, Gene Expression Regulation, Developmental, Articles, Cell Biology, Embryo, Mammalian, Hematopoietic Stem Cells, Hematopoiesis, Haematopoiesis, RUNX1, chemistry, Proteasome, FLI1, COS Cells, Core Binding Factor Alpha 2 Subunit, embryonic structures, Cancer research, Stem cell, K562 Cells

Abstract

The oncogenic transcription factor Runx1 is required for the specification of definitive hematopoietic stem cells (HSC) in the developing embryo. The activity of this master regulator is tightly controlled during development. The transcription factors that upregulate the expression of Runx1 also upregulate the expression of Smad6, the inhibitory Smad, which controls Runx1 activity by targeting it to the proteasome. Here we show that Runx1, in conjunction with Fli1, Gata2, and Scl, directly regulates the expression of Smad6 in the aorta-gonad-mesonephros (AGM) region in the developing embryo, where HSCs originate. Runx1 regulates Smad6 activity via a novel upstream enhancer, and Runx1 null embryos show reduced Smad6 transcripts in the yolk-sac and c-Kit-positive fetal liver cells. By directly regulating the expression of Smad6, Runx1 sets up a functional rheostat to control its own activity. The perturbation of this rheostat, using a proteasomal inhibitor, results in an increase in Runx1 and Smad6 levels that can be directly attributed to increased Runx1 binding to tissue-specific regulatory elements of these genes. Taken together, we describe a scenario in which a key hematopoietic transcription factor controls its own expression levels by transcriptionally controlling its controller.

Published

2011

30. Lymphocyte-Specific Chromatin Accessibility Pre-determines Glucocorticoid Resistance in Acute Lymphoblastic Leukemia

Author

Duohui Jing, Jian-Qing Mi, Kathryn Evans, John E. Pimanda, Yizhou Huang, Chelsea Mayoh, Chao Zhang, Keith C.S. Sia, Miriam Span, Meng Wang, Jason W. H. Wong, Richard B. Lock, Cara E. Toscan, Xiaoyun Liu, Hannah McCalmont, Xiaolu Tai, Dominik Beck, Rebecca C. Poulos, and Julia C. Zhang

Subjects

0301 basic medicine, Cancer Research, Apoptosis, Mice, SCID, Biology, Dexamethasone, 03 medical and health sciences, Glucocorticoid Sensitivity, Glucocorticoid receptor, Mice, Inbred NOD, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Humans, Lymphocytes, Epigenetics, Enhancer, Glucocorticoids, Mice, Knockout, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Xenograft Model Antitumor Assays, Chromatin, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, CTCF, DNA methylation, Azacitidine, Cancer research, hormones, hormone substitutes, and hormone antagonists, Glucocorticoid, medicine.drug

Abstract

Summary Glucocorticoids play a critical role in the treatment of lymphoid malignancies. While glucocorticoid efficacy can be largely attributed to lymphocyte-specific apoptosis, its molecular basis remains elusive. Here, we studied genome-wide lymphocyte-specific open chromatin domains (LSOs), and integrated LSOs with glucocorticoid-induced RNA transcription and chromatin modulation using an in vivo patient-derived xenograft model of acute lymphoblastic leukemia (ALL). This led to the identification of LSOs critical for glucocorticoid-induced apoptosis. Glucocorticoid receptor cooperated with CTCF at these LSOs to mediate DNA looping, which was inhibited by increased DNA methylation in glucocorticoid-resistant ALL and non-lymphoid cell types. Our study demonstrates that lymphocyte-specific epigenetic modifications pre-determine glucocorticoid resistance in ALL and may account for the lack of glucocorticoid sensitivity in other cell types.

Published

2018

31. Epigenetic silencing of BIM in glucocorticoid poor-responsive pediatric acute lymphoblastic leukemia, and its reversal by histone deacetylase inhibition

Author

Andrea Biondi, Barbara Szymanska, Petra S. Bachmann, Glenn M. Marshall, Vera Magistroni, Greta Geninson, Angela Mogavero, Berthold Göttgens, Richard Saffery, Rocco Piazza, Richard B. Lock, Nicholas C. Wong, Mary E. Janes, Vivek A Bhadri, Diego Miranda-Saavedra, John E. Pimanda, Giovanni Cazzaniga, Carlo Gambacorti-Passerini, Carwyn Davies, Jeffrey M. Craig, Bachmann, P, Piazza, R, Janes, M, Wong, N, Davies, C, Mogavero, A, Bhadri, V, Szymanska, B, Geninson, G, Magistroni, V, Cazzaniga, G, Biondi, A, Miranda Saavedra, D, Göttgens, B, Saffery, R, Craig, J, Marshall, G, GAMBACORTI PASSERINI, C, Pimanda, J, and Lock, R

Subjects

Antineoplastic Agents, Hormonal, medicine.drug_class, Immunology, Antineoplastic Agents, Mice, SCID, Biology, Hydroxamic Acids, Biochemistry, Dexamethasone, Histone Deacetylases, Mice, Histone H3, Glucocorticoid receptor, Proto-Oncogene Proteins, medicine, Animals, Humans, Gene silencing, Gene Silencing, Child, Histone H3 acetylation, Glucocorticoids, Vorinostat, Bcl-2-Like Protein 11, Histone deacetylase inhibitor, Membrane Proteins, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Histone Deacetylase Inhibitors, Drug Resistance, Neoplasm, Genetic Loci, BIM, ALL, Cancer research, Histone deacetylase, Apoptosis Regulatory Proteins, Glucocorticoid, medicine.drug

Abstract

Glucocorticoids play a critical role in the therapy of lymphoid malignancies, including pediatric acute lymphoblastic leukemia (ALL), although the mechanisms underlying cellular resistance remain unclear. We report glucocorticoid resistance attributable to epigenetic silencing of the BIM gene in pediatric ALL biopsies and xenografts established in immune-deficient mice from direct patient explants as well as a therapeutic approach to reverse resistance in vivo. Glucocorticoid resistance in ALL xenografts was consistently associated with failure to up-regulate BIM expression after dexamethasone exposure despite confirmation of a functional glucocorticoid receptor. Although a comprehensive assessment of BIM CpG island methylation revealed no consistent changes, glucocorticoid resistance in xenografts and patient biopsies significantly correlated with decreased histone H3 acetylation. Moreover, the histone deacetylase inhibitor vorinostat relieved BIM repression and exerted synergistic antileukemic efficacy with dexamethasone in vitro and in vivo. These findings provide a novel therapeutic strategy to reverse glucocorticoid resistance and improve outcome for high-risk pediatric ALL.

Published

2010

32. Generating Multipotent Stem Cells From Primary Human Adipocytes for Tissue Repair

Author

John E. Pimanda

Subjects

Cancer Research, Primary (chemistry), Multipotent Stem Cell, Genetics, Cell Biology, Hematology, Biology, Tissue repair, Molecular Biology, Cell biology

Published

2018

33. Mesoderm-Derived PDGFRA+ Cells Regulate Emergence of Hematopoietic Stem Cells in the Dorsal Aorta

Author

John E. Pimanda

Subjects

Cancer Research, Mesoderm, Cell Biology, Hematology, PDGFRA, Biology, Cell biology, Haematopoiesis, Dorsal aorta, medicine.anatomical_structure, Genetics, medicine, Stem cell, Molecular Biology

Published

2018

34. A previously unrecognized promoter of LMO2 forms part of a transcriptional regulatory circuit mediating LMO2 expression in a subset of T-acute lymphoblastic leukaemia patients

Author

S H Oram, Bjp Huntly, Berthold Göttgens, Julie A. I. Thoms, Clare Pridans, Mary E. Janes, JR Landry, S Anand, John E. Pimanda, Padma-Sheela Jayaraman, Sarah Kinston, and Richard B. Lock

Subjects

LMO2, Chromatin Immunoprecipitation, Cancer Research, Transcription, Genetic, Transgene, Gene Expression, Mice, Transgenic, chromatin immunoprecipitation, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Mice, Transcriptional Regulator ERG, Proto-Oncogene Proteins, hemic and lymphatic diseases, Metalloproteins, Genetics, Animals, Humans, transcriptional regulation, human, Promoter Regions, Genetic, Enhancer, Molecular Biology, Adaptor Proteins, Signal Transducing, Oligonucleotide Array Sequence Analysis, Homeodomain Proteins, Regulation of gene expression, Proto-Oncogene Protein c-fli-1, Reverse Transcriptase Polymerase Chain Reaction, LIM Domain Proteins, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, ChIP-on-chip, Haematopoiesis, FLI1, leukaemia, Trans-Activators, Cancer research, Ectopic expression, Transcription Factors

Abstract

The T-cell oncogene Lim-only 2 (LMO2) critically influences both normal and malignant haematopoiesis. LMO2 is not normally expressed in T cells, yet ectopic expression is seen in the majority of T-acute lymphoblastic leukaemia (T-ALL) patients with specific translocations involving LMO2 in only a subset of these patients. Ectopic lmo2 expression in thymocytes of transgenic mice causes T-ALL, and retroviral vector integration into the LMO2 locus was implicated in the development of clonal T-cell disease in patients undergoing gene therapy. Using array-based chromatin immunoprecipitation, we now demonstrate that in contrast to B-acute lymphoblastic leukaemia, human T-ALL samples largely use promoter elements with little influence from distal enhancers. Active LMO2 promoter elements in T-ALL included a previously unrecognized third promoter, which we demonstrate to be active in cell lines, primary T-ALL patients and transgenic mice. The ETS factors ERG and FLI1 previously implicated in lmo2-dependent mouse models of T-ALL bind to the novel LMO2 promoter in human T-ALL samples, while in return LMO2 binds to blood stem/progenitor enhancers in the FLI1 and ERG gene loci. Moreover, LMO2, ERG and FLI1 all regulate the +1 enhancer of HHEX/PRH, which was recently implicated as a key mediator of early progenitor expansion in LMO2-driven T-ALL. Our data therefore suggest that a self-sustaining triad of LMO2/ERG/FLI1 stabilizes the expression of important mediators of the leukaemic phenotype such as HHEX/PRH.

Published

2010

35. Abstract 3173: Lymphocyte-specific chromatin accessibility predetermines glucocorticoid resistance in acute lymphoblastic leukemia

Author

Jian-Qing Mi, Rebecca C. Poulos, Richard B. Lock, Yizhou Huang, Jason W. H. Wong, Xiaoyun Liu, Keith C.S. Sia, Duohui Jing, Miriam Span, Dominik Beck, John E. Pimanda, and Chao Zhang

Subjects

Cancer Research, Biology, Chromatin, Glucocorticoid receptor, Glucocorticoid Sensitivity, Oncology, CTCF, DNA methylation, Cancer research, medicine, Epigenetics, Chromatin immunoprecipitation, Glucocorticoid, medicine.drug

Abstract

Glucocorticoids are well known for their immunosuppressive activity, and play a critical role in the treatment of lymphoid malignancies. However, the development of resistance remains a significant barrier to cure and the mechanisms are poorly defined. Moreover, glucocorticoids are rarely efficacious in treating myeloid and other non-lymphoid malignancies, and the mechanisms of lymphocyte-specific efficacy are unclear. To address these issues, we first carried out a global analysis of DNase I hypersensitive sites in 18 lymphoid and 64 non-lymphoid cell types to map lymphocyte-specific open chromatin domains (LSOs). We then integrated these domains with genome-wide glucocorticoid-induced gene transcription and epigenetic modulation in an in vivo patient-derived xenograft (PDX) model of acute lymphoblastic leukemia (ALL). Performing chromatin immunoprecipitation and assays for transposase-accessible chromatin (ATAC), we determined a strong correlation between glucocorticoid receptor (GR) binding and chromatin accessibility, acetylated histone marks and binding of a DNA structural protein (CTCF), and identified 1,536 GR bound LSOs. We next analyzed RNA-seq data in glucocorticoid sensitive and resistant ALL PDXs for expression changes in genes located within 100 kb of the LSOs after glucocorticoid treatment in vivo, and identified four groups comprising 389 genes that were significantly differentially expressed. Of the 198 up-regulated genes, 143 showed increased H3K27Ac enrichments at 177 LSOs. Forty-two LSOs showed the increase only in glucocorticoid sensitive but not resistant ALLs. Applying this to an extended panel of ALL PDXs, basal DNA methylation at the 42 LSOs was significantly higher in resistant ALLs despite no difference within the gene bodies, whereas the basal chromatin accessibility indicated by ATAC abundance was diminished. Pathway analysis indicated that the LSO regulated genes were involved in repressing B- and T- cell receptor signaling pathways and activating the apoptotic pathway. One such LSO was at the pro-apoptotic BIM gene locus, where CTCF binding was found only in lymphocytes but not in other cell types. The GR cooperated with CTCF to mediate interactions between the promoter and the BIM LSO to direct DNA looping, thus triggering BIM transcription. Importantly, this LSO was heavily methylated in resistant ALLs as well as non-lymphoid cells. Azacitidine, a DNA demethylating drug that is routinely used in the clinic, could partially reverse these changes and restore glucocorticoid sensitivity. Taken together, this study demonstrated for the first time that lymphocyte-specific epigenetic modifications pre-determine glucocorticoid resistance in ALL and may account for the lack of glucocorticoid sensitivity in other cell type. Reversal of these epigenetic changes may lead to improvements in the use of glucocorticoids in the clinic. Citation Format: Duohui Jing, Yizhou Huang, Xiaoyun Liu, Keith Sia, Rebecca C. Poulos, Miriam Span, Chao Zhang, Jianqing Mi, Jason WH Wong, Dominik Beck, John E. Pimanda, Richard B. Lock. Lymphocyte-specific chromatin accessibility predetermines glucocorticoid resistance in acute lymphoblastic leukemia [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 3173.

Published

2018

36. The SCL transcriptional network and BMP signaling pathway interact to regulate RUNX1 activity

Author

David Tannahill, Ian J. Donaldson, Sandie Piltz, John E. Pimanda, Anthony R. Green, Berthold Göttgens, Sarah Kinston, Liz Huckle, Josette Renée Landry, Kathy Knezevic, and Marella F. T. R. de Bruijn

Subjects

animal structures, Smad6 Protein, Molecular Sequence Data, Mice, Transgenic, Bone Morphogenetic Protein 4, SMAD, Biology, Mice, Mediator, Proto-Oncogene Proteins, hemic and lymphatic diseases, Basic Helix-Loop-Helix Transcription Factors, Animals, Humans, Gene Regulatory Networks, Regulatory Elements, Transcriptional, Enhancer, BMP signaling pathway, Transcription factor, Conserved Sequence, Regulation of gene expression, Multidisciplinary, Base Sequence, Computational Biology, Endothelial Cells, Gene Expression Regulation, Developmental, Biological Sciences, Embryo, Mammalian, Multigene Family, Bone Morphogenetic Proteins, Core Binding Factor Alpha 2 Subunit, embryonic structures, NIH 3T3 Cells, Cancer research, Signal transduction, Sequence Alignment, Protein Binding, Signal Transduction, TAL1

Abstract

Hematopoietic stem cell (HSC) development is regulated by several signaling pathways and a number of key transcription factors, which include Scl/Tal1, Runx1, and members of the Smad family. However, it remains unclear how these various determinants interact. Using a genome-wide computational screen based on the well characterized Scl +19 HSC enhancer, we have identified a related Smad6 enhancer that also targets expression to blood and endothelial cells in transgenic mice. Smad6, Bmp4, and Runx1 transcripts are concentrated along the ventral aspect of the E10.5 dorsal aorta in the aorta–gonad–mesonephros region from which HSCs originate. Moreover, Smad6, an inhibitor of Bmp4 signaling, binds and inhibits Runx1 activity, whereas Smad1, a positive mediator of Bmp4 signaling, transactivates the Runx1 promoter. Taken together, our results integrate three key determinants of HSC development; the Scl transcriptional network, Runx1 activity, and the Bmp4/Smad signaling pathway.

Published

2007

37. 72 personalized treatment approach for GFI 136N heterozygous or homozygous MDS patients

Author

J. Hoenes, Anne Helness, B.A. van der Reijden, Tobias Schroeder, Cyrus Khandanpour, John E. Pimanda, Hideki Makishima, U. Germing, B. Lacramioara, Elli Papaemmanuil, Charles Vadnais, T. Radiovoyevich, Jaroslaw P. Maciejewski, Uwe Platzbecker, Ashwin Unnikrishnan, Ulrich Dührsen, Rainer Haas, Gerhard Ehninger, Lars Michel, Jurjen Jansen, A. Marneth, and Tarik Möröy

Subjects

Oncology, Cancer Research, medicine.medical_specialty, business.industry, Internal medicine, Personalized treatment, medicine, Medizin, Hematology, business

Published

2015

38. A novel mouse model identifies cooperating mutations and therapeutic targets critical for chronic myeloid leukemia progression

Author

Hikari Osaki, Daniel G. Tenen, John E. Pimanda, David J. Adams, Eshwar Meduri, Louise van der Weyden, Donna Foster, Sarah J. Horton, George Giotopoulos, Rab K. Prinjha, Alistair G. Rust, Paolo Gallipoli, Brian J. P. Huntly, Wai-In Chan, George S. Vassiliou, Steffen Koschmieder, Giotopoulos, George [0000-0003-1390-6592], Gallipoli, Paolo [0000-0001-7254-2253], Vassiliou, George [0000-0003-4337-8022], Huntly, Brian [0000-0003-0312-161X], and Apollo - University of Cambridge Repository

Subjects

Candidate gene, Genes, myb, Immunology, Vascular Endothelial Growth Factor C, Fusion Proteins, bcr-abl, Mice, Transgenic, Disease, Biology, News, medicine.disease_cause, Insights, Article, Insertional mutagenesis, hemic and lymphatic diseases, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, medicine, Tumor Cells, Cultured, Immunology and Allergy, Animals, Humans, Molecular Targeted Therapy, neoplasms, Mutation, Leukemia, Experimental, Gene Expression Regulation, Leukemic, Myeloid leukemia, medicine.disease, Hematopoietic Stem Cells, Phenotype, 3. Good health, Leukemia, Mutagenesis, Insertional, Cancer research, DNA Transposable Elements, Experimental pathology

Abstract

Giotopoulos et al. report a novel mouse model that closely mimics the natural progression of human chronic myeloid leukemia to blast crisis, and use this model to identify novel candidate genes and pathways that, in combination with BCR-ABL, drive disease progression., The introduction of highly selective ABL-tyrosine kinase inhibitors (TKIs) has revolutionized therapy for chronic myeloid leukemia (CML). However, TKIs are only efficacious in the chronic phase of the disease and effective therapies for TKI-refractory CML, or after progression to blast crisis (BC), are lacking. Whereas the chronic phase of CML is dependent on BCR-ABL, additional mutations are required for progression to BC. However, the identity of these mutations and the pathways they affect are poorly understood, hampering our ability to identify therapeutic targets and improve outcomes. Here, we describe a novel mouse model that allows identification of mechanisms of BC progression in an unbiased and tractable manner, using transposon-based insertional mutagenesis on the background of chronic phase CML. Our BC model is the first to faithfully recapitulate the phenotype, cellular and molecular biology of human CML progression. We report a heterogeneous and unique pattern of insertions identifying known and novel candidate genes and demonstrate that these pathways drive disease progression and provide potential targets for novel therapeutic strategies. Our model greatly informs the biology of CML progression and provides a potent resource for the development of candidate therapies to improve the dismal outcomes in this highly aggressive disease.

Published

2015

39. The paralogous hematopoietic regulators Lyl1 and Scl are coregulated by Ets and GATA factors, but Lyl1 cannot rescue the early Scl–/– phenotype

Author

Josette Renée Landry, Fred Sablitzky, Kathy Knezevic, Laure Gambardella, Berthold Göttgens, Sarah Kinston, Valerie Kouskoff, George A. Follows, John E. Pimanda, Georges Lacaud, Wan Y I Chan, Ian J. Donaldson, Sandie Piltz, and Anthony R. Green

Subjects

Time Factors, animal structures, Cellular differentiation, Molecular Sequence Data, Immunology, Gene Expression, Biology, behavioral disciplines and activities, Biochemistry, Cell Line, Proto-Oncogene Protein c-ets-1, Mice, Proto-Oncogene Proteins, hemic and lymphatic diseases, Basic Helix-Loop-Helix Transcription Factors, Animals, Humans, Amino Acid Sequence, Promoter Regions, Genetic, Transcription factor, Conserved Sequence, T-Cell Acute Lymphocytic Leukemia Protein 1, Mice, Knockout, Base Sequence, fungi, Endothelial Cells, Promoter, Cell Biology, Hematology, Embryo, Mammalian, Embryonic stem cell, Hematopoiesis, Neoplasm Proteins, GATA2 Transcription Factor, Haematopoiesis, Phenotype, FLI1, Cancer research, Ectopic expression, Stem cell, Sequence Alignment

Abstract

Transcription factors are key regulators of hematopoietic stem cells (HSCs), yet the molecular mechanisms that control their expression are largely unknown. Previously, we demonstrated that expression of Scl/Tal1, a transcription factor required for the specification of HSCs, is controlled by Ets and GATA factors. Here we characterize the molecular mechanisms controlling expression of Lyl1, a paralog of Scl also required for HSC function. Two closely spaced promoters directed expression to hematopoietic progenitor, megakaryocytic, and endothelial cells in transgenic mice. Conserved binding sites required for promoter activity were bound in vivo by GATA-2 and the Ets factors Fli1, Elf1, Erg, and PU.1. However, despite coregulation of Scl and Lyl1 by the same Ets and GATA factors, Scl expression was initiated prior to Lyl1 in embryonic stem (ES) cell differentiation assays. Moreover, ectopic expression of Scl but not Lyl1 rescued hematopoietic differentiation in Scl−/− ES cells, thus providing a molecular explanation for the vastly different phenotypes of Scl−/− and Lyl1−/− mouse embryos. Furthermore, coregulation of Scl and Lyl1 later during development may explain the mild phenotype of Scl−/− adult HSCs.

Published

2006

40. The Proto-Oncogene ERG in Megakaryoblastic Leukemias

Author

John E. Pimanda, Sabine Strehl, Liat Rainis, Shai Izraeli, Ester Rosenthal, Tsutomu Toki, Berthold Göttgens, Etsuro Ito, and Keren Machol

Subjects

Cancer Research, Chromosomes, Human, Pair 21, Molecular Sequence Data, Biology, Proto-Oncogene Mas, chemistry.chemical_compound, Transcriptional Regulator ERG, Leukemia, Megakaryoblastic, Acute, Proto-Oncogene Proteins, hemic and lymphatic diseases, Basic Helix-Loop-Helix Transcription Factors, medicine, Humans, Cell Lineage, GATA1 Transcription Factor, Promoter Regions, Genetic, T-Cell Acute Lymphocytic Leukemia Protein 1, X chromosome, Oncogene Proteins, Base Sequence, Hematopoietic stem cell, GATA1, Hematopoietic Stem Cells, medicine.disease, DNA-Binding Proteins, medicine.anatomical_structure, Oncology, RUNX1, chemistry, Trans-Activators, Cancer research, Erythroid-Specific DNA-Binding Factors, Leukemia, Erythroblastic, Acute, K562 Cells, Chromosome 21, Trisomy, Erg, HeLa Cells, Transcription Factors

Abstract

Aneuploidy is one of the hallmarks of cancer. Acquired additions of chromosome 21 are a common finding in leukemias, suggesting a contributory role to leukemogenesis. About 10% of patients with a germ line trisomy 21 (Down syndrome) are born with transient megakaryoblastic leukemia. We and others have shown acquired mutations in the X chromosome gene GATA1 in all these cases. The gene or genes on chromosome 21 whose overexpression promote the megakaryoblastic phenotype are presently unknown. We propose that ERG, an Ets transcription factor situated on chromosome 21, is one such candidate. We show that ERG is expressed in hematopoietic stem cells, megakaryoblastic cell lines, and in primary leukemic cells from Down syndrome patients. ERG expression is induced upon megakaryocytic differentiation of the erythroleukemia cell lines K562 and UT-7, and forced expression of ERG in K562 cells induces erythroid to megakaryoblastic phenotypic switch. We also show that ERG activates the gpIb megakaryocytic promoter and binds the gpIIb promoter in vivo. Furthermore, both ERG and ETS2 bind in vivo the hematopoietic enhancer of SCL/TAL1, a key regulator of hematopoietic stem cell and megakaryocytic development. We propose that trisomy 21 facilitates the occurrence of megakaryoblastic leukemias through a shift toward the megakaryoblastic lineage caused by the excess expression of ERG, and possibly by other chromosome 21 genes, such as RUNX1 and ETS2, in hematopoietic progenitor cells, coupled with a differentiation arrest caused by the acquisition of mutations in GATA1.

Published

2005

41. Maintenance of primitive haematopoiesis is shared by SCL and LYL1

Author

Yizhou Huang, Cedric S. Tremblay, David R. Powell, Jesslyn Saw, David J. Curtis, Dominic Beck, Sung Kai Chiu, and John E. Pimanda

Subjects

Cancer Research, LYL1, Genetics, Cell Biology, Hematology, Biology, Molecular Biology, Neuroscience, Primitive haematopoiesis

Published

2017

42. Declined presentation characterisation of stromal cell populations in the foetal liver and their contributions to embryonic haematopoietic and vascular development

Author

John E. Pimanda, Rema A. Oliver, Vashe Chandrakanthan, Christine Loo, Kathy Knezevic, Young Chan Kang, Willam Walsh, Jason W. H. Wong, Brendan Lee, Govardhan Anande, Carl Power, and Qiao Qiao

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Stromal cell, Cell Biology, Hematology, Biology, Foetal liver, Embryonic stem cell, Haematopoiesis, Genetics, medicine, Presentation (obstetrics), Molecular Biology

Published

2017

43. In vivo CRISPR editing of DNMT3A in JAK2V617F hematopoietic stem cells induces myelofibrosis

Author

Steven W. Lane, Matthew Heidecker, John E. Pimanda, Luke B. Hesson, Sebastien Jacquelin, Jasmin Straube, Axia Song, Therese Vu, Nicole Cloonan, Geff Hill, Leanne Cooper, and Dirk Heckl

Subjects

Cancer Research, Cell Biology, Hematology, Biology, medicine.disease, Virology, Haematopoiesis, In vivo, Genetics, Cancer research, medicine, CRISPR, Stem cell, Myelofibrosis, Molecular Biology

Published

2017

44. Opposing regulation of BIM and BCL2 controls glucocorticoid-induced apoptosis of pediatric acute lymphoblastic leukemia cells

Author

Jason W. H. Wong, John E. Pimanda, Julie A. I. Thoms, Kathy Knezevic, Duohui Jing, Dominik Beck, Vivek A Bhadri, Nurul A. Yakob, and Richard B. Lock

Subjects

Chromatin Immunoprecipitation, Antineoplastic Agents, Hormonal, Immunology, Blotting, Western, Apoptosis, Enzyme-Linked Immunosorbent Assay, Mice, SCID, Biology, Real-Time Polymerase Chain Reaction, Biochemistry, Dexamethasone, Mice, Glucocorticoid receptor, Receptors, Glucocorticoid, Mice, Inbred NOD, hemic and lymphatic diseases, Proto-Oncogene Proteins, Gene silencing, Animals, Humans, MYB, neoplasms, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Bcl-2-Like Protein 11, Reverse Transcriptase Polymerase Chain Reaction, Membrane Proteins, Combination chemotherapy, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Xenograft Model Antitumor Assays, ChIP-sequencing, Gene Expression Regulation, Neoplastic, Proto-Oncogene Proteins c-bcl-2, Drug Resistance, Neoplasm, Cancer research, biological phenomena, cell phenomena, and immunity, Signal transduction, Apoptosis Regulatory Proteins, Chromatin immunoprecipitation, Signal Transduction

Abstract

Glucocorticoids are critical components of combination chemotherapy regimens in pediatric acute lymphoblastic leukemia (ALL). The proapoptotic BIM protein is an important mediator of glucocorticoid-induced apoptosis in normal and malignant lymphocytes, whereas the antiapoptotic BCL2 confers resistance. The signaling pathways regulating BIM and BCL2 expression in glucocorticoid-treated lymphoid cells remain unclear. In this study, pediatric ALL patient-derived xenografts (PDXs) inherently sensitive or resistant to glucocorticoids were exposed to dexamethasone in vivo. Microarray analysis showed that KLF13 and MYB gene expression changes were significantly greater in dexamethasone-sensitive than -resistant PDXs. Chromatin immunoprecipitation (ChIP) analysis detected glucocorticoid receptor (GR) binding at the KLF13 promoter to trigger KLF13 expression only in sensitive PDXs. Next, KLF13 bound to the MYB promoter, deactivating MYB expression only in sensitive PDXs. Sustained MYB expression in resistant PDXs resulted in maintenance of BCL2 expression and inhibition of apoptosis. ChIP sequencing analysis revealed a novel GR binding site in a BIM intronic region (IGR) that was engaged only in dexamethasone-sensitive PDXs. The absence of GR binding at the BIM IGR was associated with BIM silencing and dexamethasone resistance. This study has identified novel mechanisms of opposing BCL2 and BIM gene regulation that control glucocorticoid-induced apoptosis in pediatric ALL cells in vivo.

Published

2014

45. Epigenetic inactivation of the candidate tumor suppressor USP44 is a frequent and early event in colorectal neoplasia: Epigenetic inactivation of the candidate tumor suppressor USP44 is a frequent and early event in colorectal neoplasia

Author

Robyn L. Ward, Dilmi Perera, Michael J. Bourke, John E. Pimanda, Mathew A. Sloane, Jason W. H. Wong, Nicholas J. Hawkins, Oliver M. Sieber, Luke B. Hesson, and Andrea Nuñez

Subjects

Adenoma, Adult, Male, Cancer Research, Antimetabolites, Antineoplastic, Adolescent, Colorectal cancer, Colon, Bisulfite sequencing, Gene Expression, Biology, Decitabine, Polymorphism, Single Nucleotide, Epigenesis, Genetic, Young Adult, Intestinal mucosa, Combined bisulfite restriction analysis, Cell Line, Tumor, medicine, Humans, Genes, Tumor Suppressor, Intestinal Mucosa, Molecular Biology, Aged, Oligonucleotide Array Sequence Analysis, Aged, 80 and over, Rectum, Cancer, Middle Aged, medicine.disease, Aneuploidy, Candidate Tumor Suppressor Gene, Molecular biology, digestive system diseases, DNA methylation, Cancer research, Azacitidine, CpG Islands, Ubiquitin-Specific Proteases, Colorectal Neoplasms, Ubiquitin Thiolesterase, Research Paper

Abstract

In mouse models, loss of the candidate tumor suppressor gene Ubiquitin Specific Protease 44 (USP44) is associated with aneuploidy and cancer. USP44 is also transcriptionally silenced in human cancers. Here we investigated the molecular mechanism of USP44 silencing and whether this correlated with aneuploidy in colorectal adenomas. DNA methylation at the USP44 CpG island (CGI) promoter was measured using combined bisulfite restriction analysis (COBRA) in colorectal cancer (CRC) cell lines (n = 18), and with COBRA and bisulfite sequencing in colorectal adenomas (n = 89) and matched normal colonic mucosa (n = 51). The USP44 CGI was hypermethylated in all CRC cell lines, in most colorectal adenomas (79 of 89, 89%) but rarely in normal mucosa samples (3 of 51, 6%). USP44 expression was also compared between normal mucosa and paired hypermethylated adenomas in six patients using qRT-PCR. Hypermethylation of the USP44 CGI in adenomas was associated with a 1.8 to 5.5-fold reduction in expression compared with paired normal mucosa. Treatment of CRC cell lines with the DNA hypomethylating agent decitabine resulted in a 14 to 270-fold increase in USP44 expression. Whole genome SNP array data showed that gain or loss of individual chromosomes occurred in adenomas, but hypermethylation did not correlate with more aneuploidy. In summary, our data shows that USP44 is epigenetically inactivated in colorectal adenomas, but this alone is not sufficient to cause aneuploidy in colorectal neoplasia.

Published

2014

46. Diffner E, Beck D, Gudgin E, et al. Activity of a heptad of transcription factors is associated with stem cell programs and clinical outcome in acute myeloid leukemia. Blood. 2013;121(12):2289-2300

Author

Stefan K. Bohlander, Kathy Knezevic, George S. Vassiliou, Lies Boelen, Jason W. H. Wong, Alan Kenneth Burnett, Berthold Goettgens, Klaus H. Metzeler, Weng Khong Lim, Jake Olivier, Brian J. P. Huntly, John E. Pimanda, Clare Pridans, Sam Foster, Christian Buske, Debbie K. Goode, Katrin Ottersbach, Eva Diffner, Gos Micklem, Julie A. I. Thoms, Emma Gudgin, and Dominik Beck

Subjects

Errata, business.industry, Immunology, Cancer research, Myeloid leukemia, Medicine, Cell Biology, Hematology, Stem cell, business, Biochemistry, Transcription factor

Published

2014

47. Genome-scale expression and transcription factor binding profiles reveal therapeutic targets in transgenic ERG myeloid leukemia

Author

Rebecca Hannah, Anat Biran, Peter D. Aplan, John E. Pimanda, Yoel Kloog, Judith Schütte, Ginette Schiby, Kathy Knezevic, Jasmine Jacob-Hirsch, Sarah Kinston, Berthold Göttgens, Clara D. Bloomfield, Guido Marcucci, Yehudit Birger, Dominik Beck, Liat Goldberg, Marloes R. Tijssen, and Shai Izraeli

Subjects

Myeloid, genetic structures, Transcription, Genetic, Immunology, PIM1, Antineoplastic Agents, Mice, Transgenic, Mice, SCID, Biology, Biochemistry, Mice, Proto-Oncogene Proteins c-pim-1, Transcriptional Regulator ERG, Mice, Inbred NOD, hemic and lymphatic diseases, medicine, Animals, Humans, Progenitor cell, Myeloid Progenitor Cells, Myeloid Neoplasia, Gene Expression Regulation, Leukemic, Myeloid leukemia, Cell Biology, Hematology, Genomics, medicine.disease, eye diseases, Leukemia, Haematopoiesis, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Enhancer Elements, Genetic, Cancer research, Trans-Activators, sense organs, Erg, Neoplasm Transplantation, Transcription Factors

Abstract

The ETS transcription factor ERG plays a central role in definitive hematopoiesis, and its overexpression in acute myeloid leukemia (AML) is associated with a stem cell signature and poor prognosis. Yet how ERG causes leukemia is unclear. Here we show that pan-hematopoietic ERG expression induces an early progenitor myeloid leukemia in transgenic mice. Integrated genome-scale analysis of gene expression and ERG binding profiles revealed that ERG activates a transcriptional program similar to human AML stem/progenitor cells and to human AML with high ERG expression. This transcriptional program was associated with activation of RAS that was required for leukemia cells growth in vitro and in vivo. We further show that ERG induces expression of the Pim1 kinase oncogene through a novel hematopoietic enhancer validated in transgenic mice and human CD34(+) normal and leukemic cells. Pim1 inhibition disrupts growth and induces apoptosis of ERG-expressing leukemic cells. The importance of the ERG/PIM1 axis is further underscored by the poorer prognosis of AML highly expressing ERG and PIM1. Thus, integrative genomic analysis demonstrates that ERG causes myeloid progenitor leukemia characterized by an induction of leukemia stem cell transcriptional programs. Pim1 and the RAS pathway are potential therapeutic targets of these high-risk leukemias.

Published

2013

48. Relative distribution of folate species is associated with global DNA methylation in human colorectal mucosa

Author

Keith N. Rand, John E. Pimanda, Nicholas J. Hawkins, Peter L. Molloy, Michael J. Bourke, Jia Liu, Alan P. Meagher, Luke B. Hesson, and Robyn L. Ward

Subjects

Male, Cancer Research, Pathology, medicine.medical_specialty, Colorectal cancer, Colon, Biology, Folic Acid, Alu Elements, Tandem Mass Spectrometry, medicine, Distribution (pharmacology), Humans, Prospective Studies, Prospective cohort study, Methylenetetrahydrofolate Reductase (NADPH2), Aged, Case-control study, Rectum, Cancer, Methylation, DNA Methylation, Middle Aged, medicine.disease, Long Interspersed Nucleotide Elements, Oncology, Case-Control Studies, DNA methylation, Cancer research, Female, Colorectal Neoplasms, DNA hypomethylation, Chromatography, Liquid

Abstract

Folate exists as functionally diverse species within cells. Although folate deficiency may contribute to DNA hypomethylation in colorectal cancer, findings on the association between total folate concentration and global DNA methylation have been inconsistent. This study determined global, LINE-1, and Alu DNA methylation in blood and colon of healthy and colorectal cancer patients and their relationship to folate distribution. Blood and normal mucosa from 112 colorectal cancer patients and 114 healthy people were analyzed for global DNA methylation and folate species distribution using liquid chromatography tandem mass spectrometry. Repeat element methylation was determined using end-specific PCR. Colorectal mucosa had lower global and repeat element DNA methylation compared with peripheral blood (P < 0.0001). After adjusting for age, sex and smoking history, global but not repeat element methylation was marginally higher in normal mucosa from colorectal cancer patients compared with healthy individuals. Colorectal mucosa from colorectal cancer subjects had lower 5-methyltetrahydrofolate and higher tetrahydrofolate and formyltetrahydrofolate levels than blood from the same individual. Blood folate levels should not be used as a surrogate for the levels in colorectal mucosa because there are marked differences in folate species distribution between the two tissues. Similarly, repeat element methylation is not a good surrogate measure of global DNA methylation in both blood and colonic mucosa. There was no evidence that mucosal global DNA methylation or folate distribution was related to the presence of cancer per se, suggesting that if abnormalities exist, they are confined to individual cells rather than the entire colon. Cancer Prev Res; 5(7); 921–9. ©2012 AACR.

Published

2012

49. ERG promotes T-acute lymphoblastic leukemia and is transcriptionally regulated in leukemic cells by a stem cell enhancer

Author

Shai Izraeli, Karen L. MacKenzie, Sarah Kinston, Kathy Knezevic, Richard B. Lock, Berthold Göttgens, Yoram Groner, Georg von Jonquieres, Dominik Spensberger, Sam Foster, Yael Kirschenbaum, Vashe Chandrakanthan, Julie A. I. Thoms, John E. Pimanda, Yehudit Birger, Jason W. H. Wong, and S. Helen Oram

Subjects

genetic structures, T-Lymphocytes, Immunology, Molecular Sequence Data, Mice, Transgenic, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Biochemistry, T Acute Lymphoblastic Leukemia, Mice, Transcriptional Regulator ERG, Cell Line, Tumor, Proto-Oncogene Proteins, Metalloproteins, medicine, Basic Helix-Loop-Helix Transcription Factors, Animals, Humans, RNA, Messenger, Progenitor cell, Promoter Regions, Genetic, Proto-Oncogene Proteins c-vav, Cells, Cultured, T-Cell Acute Lymphocytic Leukemia Protein 1, Adaptor Proteins, Signal Transducing, Cell Proliferation, Base Sequence, Gene Expression Regulation, Leukemic, GATA3, Cell Biology, Hematology, LIM Domain Proteins, medicine.disease, Survival Analysis, eye diseases, Neoplasm Proteins, DNA-Binding Proteins, Leukemia, Gene Knockdown Techniques, Cancer research, Trans-Activators, sense organs, Stem cell, Erg, Sequence Alignment, Neoplasm Transplantation, TAL1

Abstract

The Ets-related gene (ERG) is an Ets-transcription factor required for normal blood stem cell development. ERG expression is down-regulated during early T-lymphopoiesis but maintained in T-acute lymphoblastic leukemia (T-ALL), where it is recognized as an independent risk factor for adverse outcome. However, it is unclear whether ERG is directly involved in the pathogenesis of T-ALL and how its expression is regulated. Here we demonstrate that transgenic expression of ERG causes T-ALL in mice and that its knockdown reduces the proliferation of human MOLT4 T-ALL cells. We further demonstrate that ERG expression in primary human T-ALL cells is mediated by the binding of other T-cell oncogenes SCL/TAL1, LMO2, and LYL1 in concert with ERG, FLI1, and GATA3 to the ERG +85 enhancer. This enhancer is not active in normal T cells but in transgenic mice targets expression to fetal liver c-kit+ cells, adult bone marrow stem/progenitors and early CD4−CD8− double-negative thymic progenitors. Taken together, these data illustrate that ERG promotes T-ALL and that failure to extinguish activity of stem cell enhancers associated with regulatory transcription factors such as ERG can contribute to the development of leukemia.

Published

2011

50. Genome-wide computational screen for bloon stem cell enhancers integrates RUNX1 and the BMP signaling pathway into the SCL transcriptional network

Author

Kathy Knezevic, Berthold Göttgens, Sandie Piltz, Ian J. Donaldson, Anthony R. Green, David Tannahill, Josette-Renee Landry, Liz Huckle, Sarah Kinston, Marella F. Bruijn, and John E. Pimanda

Subjects

animal structures, Immunology, SMAD, Biology, Biochemistry, Genome, chemistry.chemical_compound, hemic and lymphatic diseases, medicine, Enhancer, BMP signaling pathway, Transcription factor, Molecular Biology, Hematopoietic stem cell, Cell Biology, Hematology, Cell biology, medicine.anatomical_structure, RUNX1, chemistry, embryonic structures, Cancer research, Molecular Medicine, Signal transduction, Stem cell, TAL1

Abstract

Hematopoietic stem cell (HSC) development is regulated by several signaling pathways and a number of key transcription factors, which include Scl/Tal1, Runx1 and members of the Smad family. However, it remains unclear how these various determinants interact. Using a genome-wide computational screen based on the well-characterized Scl +19 HSC enhancer, we have identified a related Smad6 enhancer that also targets expression to blood and endothelial cells in transgenic mice. We show that at E10.5, Smad6 and Bmp4 transcripts are concentrated along the ventral pole of the dorsal aorta and resemble Runx1 expression in the aorta-gonad-mesonephros (AGM) region where HSCs originate. Moreover, Smad6 binds and inhibits Runx1 activity whereas Smad1, a mediator of Bmp4 signaling, transactivates the Runx1 promoter. Taken together, our results integrate three key determinants of HSC development; the Scl network, Runx1 activity and the Bmp4/Smad signaling pathway.

Published

2007