Your search keyword '"Jack F. Shern"' showing total 38 results

1. KDM3B inhibitors disrupt the oncogenic activity of PAX3-FOXO1 in fusion-positive rhabdomyosarcoma

Author

Yong Yean Kim, Berkley E. Gryder, Ranuka Sinniah, Megan L. Peach, Jack F. Shern, Abdalla Abdelmaksoud, Silvia Pomella, Girma M. Woldemichael, Benjamin Z. Stanton, David Milewski, Joseph J. Barchi, John S. Schneekloth, Raj Chari, Joshua T. Kowalczyk, Shilpa R. Shenoy, Jason R. Evans, Young K. Song, Chaoyu Wang, Xinyu Wen, Hsien-Chao Chou, Vineela Gangalapudi, Dominic Esposito, Jane Jones, Lauren Procter, Maura O’Neill, Lisa M. Jenkins, Nadya I. Tarasova, Jun S. Wei, James B. McMahon, Barry R. O’Keefe, Robert G. Hawley, and Javed Khan

Subjects

Science

Abstract

Abstract Fusion-positive rhabdomyosarcoma (FP-RMS) is an aggressive pediatric sarcoma driven primarily by the PAX3-FOXO1 fusion oncogene, for which therapies targeting PAX3-FOXO1 are lacking. Here, we screen 62,643 compounds using an engineered cell line that monitors PAX3-FOXO1 transcriptional activity identifying a hitherto uncharacterized compound, P3FI-63. RNA-seq, ATAC-seq, and docking analyses implicate histone lysine demethylases (KDMs) as its targets. Enzymatic assays confirm the inhibition of multiple KDMs with the highest selectivity for KDM3B. Structural similarity search of P3FI-63 identifies P3FI-90 with improved solubility and potency. Biophysical binding of P3FI-90 to KDM3B is demonstrated using NMR and SPR. P3FI-90 suppresses the growth of FP-RMS in vitro and in vivo through downregulating PAX3-FOXO1 activity, and combined knockdown of KDM3B and KDM1A phenocopies P3FI-90 effects. Thus, we report KDM inhibitors P3FI-63 and P3FI-90 with the highest specificity for KDM3B. Their potent suppression of PAX3-FOXO1 activity indicates a possible therapeutic approach for FP-RMS and other transcriptionally addicted cancers.

Published

2024

2. Urine cell-free DNA multi-omics to detect MRD and predict survival in bladder cancer patients

Author

Pradeep S. Chauhan, Alexander Shiang, Irfan Alahi, R. Taylor Sundby, Wenjia Feng, Bilge Gungoren, Cayce Nawaf, Kevin Chen, Ramandeep K. Babbra, Peter K. Harris, Faridi Qaium, Casey Hatscher, Anna Antiporda, Lindsey Brunt, Lindsey R. Mayer, Jack F. Shern, Brian C. Baumann, Eric H. Kim, Melissa A. Reimers, Zachary L. Smith, and Aadel A. Chaudhuri

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Circulating tumor DNA (ctDNA) sensitivity remains subpar for molecular residual disease (MRD) detection in bladder cancer patients. To remedy this problem, we focused on the biofluid most proximal to the disease, urine, and analyzed urine tumor DNA in 74 localized bladder cancer patients. We integrated ultra-low-pass whole genome sequencing (ULP-WGS) with urine cancer personalized profiling by deep sequencing (uCAPP-Seq) to achieve sensitive MRD detection and predict overall survival. Variant allele frequency, inferred tumor mutational burden, and copy number-derived tumor fraction levels in urine cell-free DNA (cfDNA) significantly predicted pathologic complete response status, far better than plasma ctDNA was able to. A random forest model incorporating these urine cfDNA-derived factors with leave-one-out cross-validation was 87% sensitive for predicting residual disease in reference to gold-standard surgical pathology. Both progression-free survival (HR = 3.00, p = 0.01) and overall survival (HR = 4.81, p = 0.009) were dramatically worse by Kaplan–Meier analysis for patients predicted by the model to have MRD, which was corroborated by Cox regression analysis. Additional survival analyses performed on muscle-invasive, neoadjuvant chemotherapy, and held-out validation subgroups corroborated these findings. In summary, we profiled urine samples from 74 patients with localized bladder cancer and used urine cfDNA multi-omics to detect MRD sensitively and predict survival accurately.

Published

2023

3. Loss of CASZ1 tumor suppressor linked to oncogenic subversion of neuroblastoma core regulatory circuitry

Author

Zhihui Liu, Xiyuan Zhang, Man Xu, Haiyan Lei, Jack F. Shern, and Carol J. Thiele

Subjects

Cytology, QH573-671

Abstract

Abstract The neural crest lineage regulatory transcription factors (TFs) form a core regulatory circuitry (CRC) in neuroblastoma (NB) to specify a noradrenergic tumor phenotype. Oncogenic subversion of CRC TFs is well documented, but the role of loss of tumor suppressors plays remains unclear. Zinc-finger TF CASZ1 is a chromosome 1p36 (chr1p36) tumor suppressor. Single-cell RNA sequencing data analyses indicate that CASZ1 is highly expressed in developing chromaffin cells coincident with an expression of NB CRC TFs. In NB tumor cells, the CASZ1 tumor suppressor is silenced while CRC components are highly expressed. We find the NB CRC component HAND2 directly represses CASZ1 expression. ChIP-seq and transcriptomic analyses reveal that restoration of CASZ1 upregulates noradrenergic neuronal genes and represses expression of CRC components by remodeling enhancer activity. Our study identifies that the restored CASZ1 forms a negative feedback regulatory circuit with the established NB CRC to induce noradrenergic neuronal differentiation of NB.

Published

2022

4. Protocol for using single-cell sequencing to study the heterogeneity of NF1 nerve sheath tumors from clinical biospecimens

Author

Xiyuan Zhang, Vishaka Gopalan, Neeraja Syed, Sridhar Hannenhalli, and Jack F. Shern

Subjects

Bioinformatics, Single Cell, Cancer, Genetics, RNAseq, Science (General), Q1-390

Abstract

Summary: Single-cell sequencing is a powerful technology to understand the heterogeneity of clinical biospecimens. Here, we present a protocol for obtaining single-cell suspension from neurofibromatosis type 1-associated nerve sheath tumors for transcriptomic profiling on the 10x platform. We describe steps for clinical sample collection, generation of single-cell suspension, and cell capture and sequencing. We then detail methods for integrative analysis, developmental Schwann cell trajectory building using bioinformatic tools, and comparative analysis. This protocol can be adapted for single-cell sequencing using mouse nerve tumors.For complete details on the use and execution of this protocol, please refer to Zhang et al. (2022).1 : Publisher’s note: Undertaking any experimental protocol requires adherence to local institutional guidelines for laboratory safety and ethics.

Published

2023

5. Multiple Nf1 Schwann cell populations reprogram the plexiform neurofibroma tumor microenvironment

Author

Leah J. Kershner, Kwangmin Choi, Jianqiang Wu, Xiyuan Zhang, Melissa Perrino, Nathan Salomonis, Jack F. Shern, and Nancy Ratner

Subjects

Cell biology, Oncology, Medicine

Abstract

To define alterations early in tumor formation, we studied nerve tumors in neurofibromatosis 1 (NF1), a tumor predisposition syndrome. Affected individuals develop neurofibromas, benign tumors driven by NF1 loss in Schwann cells (SCs). By comparing normal nerve cells to plexiform neurofibroma (PN) cells using single-cell and bulk RNA sequencing, we identified changes in 5 SC populations, including a de novo SC progenitor–like (SCP-like) population. Long after Nf1 loss, SC populations developed PN-specific expression of Dcn, Postn, and Cd74, with sustained expression of the injury response gene Postn and showed dramatic expansion of immune and stromal cell populations; in corresponding human PNs, the immune and stromal cells comprised 90% of cells. Comparisons between injury-related and tumor monocytes/macrophages support early monocyte recruitment and aberrant macrophage differentiation. Cross-species analysis verified each SC population and unique conserved patterns of predicted cell-cell communication in each SC population. This analysis identified PROS1-AXL, FGF-FGFR, and MIF-CD74 and its effector pathway NF-κB as deregulated in NF1 SC populations, including SCP-like cells predicted to influence other types of SCs, stromal cells, and/or immune cells in mouse and human. These findings highlight remarkable changes in multiple types of SCs and identify therapeutic targets for PN.

Published

2022

6. CASZ1 induces skeletal muscle and rhabdomyosarcoma differentiation through a feed-forward loop with MYOD and MYOG

Author

Zhihui Liu, Xiyuan Zhang, Haiyan Lei, Norris Lam, Sakereh Carter, Oliver Yockey, Max Xu, Arnulfo Mendoza, Edjay R. Hernandez, Jun S. Wei, Javed Khan, Marielle E. Yohe, Jack F. Shern, and Carol J. Thiele

Subjects

Science

Abstract

Embryonal rhabdomyosarcoma (ERMS) is a childhood cancer with impaired myogenic differentiation despite the presence of myogenic transcription factors. Here, the authors show that CASZ1 directly regulates these myogenic factors and the loss of CASZ1 is due to RAS-MEK signaling in ERMS.

Published

2020

7. Chemical genomics reveals histone deacetylases are required for core regulatory transcription

Author

Berkley E. Gryder, Lei Wu, Girma M. Woldemichael, Silvia Pomella, Taylor R. Quinn, Paul M. C. Park, Abigail Cleveland, Benjamin Z. Stanton, Young Song, Rossella Rota, Olaf Wiest, Marielle E. Yohe, Jack F. Shern, Jun Qi, and Javed Khan

Subjects

Science

Abstract

Core regulatory transcription factors are usually regulated by cell-type specific super enhancers (SEs). Here, the authors screen for chemical probes able to distinguish between SE-driven and promoter-driven transcription and find that histone deacetylases are selectively required for core regulatory transcription.

Published

2019

8. Preclinical Development of Bivalent Chimeric Antigen Receptors Targeting Both CD19 and CD22

Author

Haiying Qin, Sneha Ramakrishna, Sang Nguyen, Thomas J. Fountaine, Anusha Ponduri, Maryalice Stetler-Stevenson, Constance M. Yuan, Waleed Haso, Jack F. Shern, Nirali N. Shah, and Terry J. Fry

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Despite high remission rates following CAR-T cell therapy in B-ALL, relapse due to loss of the targeted antigen is increasingly recognized as a mechanism of immune escape. We hypothesized that simultaneous targeting of CD19 and CD22 may reduce the likelihood of antigen loss, thus improving sustained remission rates. A systematic approach to the generation of CAR constructs incorporating two target-binding domains led to several novel CD19/CD22 bivalent CAR constructs. Importantly, we demonstrate the challenges associated with the construction of a bivalent CAR format that preserves bifunctionality against both CD19 and CD22. Using the most active bivalent CAR constructs, we found similar transduction efficiency compared to that of either CD19 or CD22 single CARs alone. When expressed on human T cells, the optimized CD19/CD22 CAR construct induced comparable interferon γ and interleukin-2 in vitro compared to single CARs against dual-antigen-expressing as well as single-antigen-expressing cell lines. Finally, the T cells expressing CD19/CD22 CAR eradicated ALL cell line xenografts and patient-derived xenografts (PDX), including a PDX generated from a patient with CD19− relapse following CD19-directed CAR therapy. The CD19/CD22 bivalent CAR provides an opportunity to test whether simultaneous targeting may reduce risk of antigen loss. Keywords: chimeric antigen receptor, adoptive cell therapy, leukemia

Published

2018

9. Chromosome 8 gain is associated with high-grade transformation in MPNST

Author

Carina Dehner, Chang In Moon, Xiyuan Zhang, Zhaohe Zhou, Chris Miller, Hua Xu, Xiaodan Wan, Kuangying Yang, Jay Mashl, Sara J.C. Gosline, Yuxi Wang, Xiaochun Zhang, Abigail Godec, Paul A. Jones, Sonika Dahiya, Himanshi Bhatia, Tina Primeau, Shunqiang Li, Kai Pollard, Fausto J. Rodriguez, Li Ding, Christine A. Pratilas, Jack F. Shern, and Angela C. Hirbe

Subjects

Genetics, Oncology, Medicine

Abstract

One of the most common malignancies affecting adults with Neurofibromatosis type 1 (NF1) is the malignant peripheral nerve sheath tumor (MPNST), an aggressive and often fatal sarcoma that commonly arises from benign plexiform neurofibromas. Despite advances in our understanding of MPNST pathobiology, there are few effective therapeutic options, and no investigational agents have proven successful in clinical trials. To further understand the genomic heterogeneity of MPNST, and to generate a preclinical platform that encompasses this heterogeneity, we developed a collection of NF1-MPNST patient-derived xenografts (PDX). These PDX were compared with the primary tumors from which they were derived using copy number analysis, whole exome sequencing, and RNA sequencing. We identified chromosome 8 gain as a recurrent genomic event in MPNST and validated its occurrence by FISH in the PDX and parental tumors, in a validation cohort, and by single-cell sequencing in the PDX. Finally, we show that chromosome 8 gain is associated with inferior overall survival in soft-tissue sarcomas. These data suggest that chromosome 8 gain is a critical event in MPNST pathogenesis and may account for the aggressive nature and poor outcomes in this sarcoma subtype.

Published

2021

10. Defining the Extracellular Matrix of Rhabdomyosarcoma

Author

Xiaolei Lian, J. Steffan Bond, Narendra Bharathy, Sergei P. Boudko, Elena Pokidysheva, Jack F. Shern, Melvin Lathara, Takako Sasaki, Teagan Settelmeyer, Megan M. Cleary, Ayeza Bajwa, Ganapati Srinivasa, Christopher P. Hartley, Hans Peter Bächinger, Atiya Mansoor, Sakir H. Gultekin, Noah E. Berlow, and Charles Keller

Subjects

matrix, COL18A1, PLOD1/2, rhabdomyosarcoma, survival, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Rhabdomyosarcoma (RMS) is the most common soft-tissue sarcoma of childhood with a propensity to metastasize. Current treatment for patients with RMS includes conventional systemic chemotherapy, radiation therapy, and surgical resection; nevertheless, little to no improvement in long term survival has been achieved in decades—underlining the need for target discovery and new therapeutic approaches to targeting tumor cells or the tumor microenvironment. To evaluate cross-species sarcoma extracellular matrix production, we have used murine models which feature knowledge of the myogenic cell-of-origin. With focus on the RMS/undifferentiated pleomorphic sarcoma (UPS) continuum, we have constructed tissue microarrays of 48 murine and four human sarcomas to analyze expression of seven different collagens, fibrillins, and collagen-modifying proteins, with cross-correlation to RNA deep sequencing. We have uncovered that RMS produces increased expression of type XVIII collagen alpha 1 (COL18A1), which is clinically associated with decreased long-term survival. We have also identified significantly increased RNA expression of COL4A1, FBN2, PLOD1, and PLOD2 in human RMS relative to normal skeletal muscle. These results complement recent studies investigating whether soft tissue sarcomas utilize collagens, fibrillins, and collagen-modifying enzymes to alter the structural integrity of surrounding host extracellular matrix/collagen quaternary structure resulting in improved ability to improve the ability to invade regionally and metastasize, for which therapeutic targeting is possible.

Published

2021

11. Integrative Bayesian Analysis Identifies Rhabdomyosarcoma Disease Genes

Author

Lin Xu, Yanbin Zheng, Jing Liu, Dinesh Rakheja, Sydney Singleterry, Theodore W. Laetsch, Jack F. Shern, Javed Khan, Timothy J. Triche, Douglas S. Hawkins, James F. Amatruda, and Stephen X. Skapek

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Identifying oncogenic drivers and tumor suppressors remains a challenge in many forms of cancer, including rhabdomyosarcoma. Anticipating gene expression alterations resulting from DNA copy-number variants to be particularly important, we developed a computational and experimental strategy incorporating a Bayesian algorithm and CRISPR/Cas9 “mini-pool” screen that enables both genome-scale assessment of disease genes and functional validation. The algorithm, called iExCN, identified 29 rhabdomyosarcoma drivers and suppressors enriched for cell-cycle and nucleic-acid-binding activities. Functional studies showed that many iExCN genes represent rhabdomyosarcoma line-specific or shared vulnerabilities. Complementary experiments addressed modes of action and demonstrated coordinated repression of multiple iExCN genes during skeletal muscle differentiation. Analysis of two separate cohorts revealed that the number of iExCN genes harboring copy-number alterations correlates with survival. Our findings highlight rhabdomyosarcoma as a cancer in which multiple drivers influence disease biology and demonstrate a generalizable capacity for iExCN to unmask disease genes in cancer. : Xu et al. use an integrative computational pipeline (iExCN) to identify 25 candidate oncogenic driver genes and 4 tumor suppressors in rhabdomyosarcoma, and many are validated in a CRISPR/Cas9 mini-pool screen. Functional assays and correlation with survival indicate that cooperative interactions across iExCN genes contribute to disease biology, including differentiation arrest. Keywords: rhabdomyosarcoma, Bayesian algorithm, CRISPR/Cas9, oncogene, tumor suppressor gene, integrative genomic analysis, childhood cancer

Published

2018

12. CD19 CAR immune pressure induces B-precursor acute lymphoblastic leukaemia lineage switch exposing inherent leukaemic plasticity

Author

Elad Jacoby, Sang M. Nguyen, Thomas J. Fountaine, Kathryn Welp, Berkley Gryder, Haiying Qin, Yinmeng Yang, Christopher D. Chien, Alix E. Seif, Haiyan Lei, Young K. Song, Javed Khan, Daniel W. Lee, Crystal L. Mackall, Rebecca A. Gardner, Michael C. Jensen, Jack F. Shern, and Terry J. Fry

Subjects

Science

Abstract

CAR-T targeting CD19 have been successfully used in a variety of B-cell malignancies but patients may eventually relapse. Here, the authors show that CD19 CAR-T resistance in pre-B cell ALL can be due to the induction of a myeloid lineage switch through an epigenetic alterations in master regulators of B cell development.

Published

2016

13. Sequential loss of tumor surface antigens following chimeric antigen receptor T-cell therapies in diffuse large B-cell lymphoma

Author

Haneen Shalabi, Ira L. Kraft, Hao-Wei Wang, Constance M. Yuan, Bonnie Yates, Cindy Delbrook, Julie D. Zimbelman, Roger Giller, Maryalice Stetler-Stevenson, Elaine S. Jaffe, Daniel W. Lee, Jack F. Shern, Terry J. Fry, and Nirali N. Shah

Subjects

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

Published

2018

14. Liquid biopsies in pediatric oncology: opportunities and obstacles

Author

R. Taylor Sundby, Alex Pan, and Jack F. Shern

Subjects

Adult, medicine.medical_specialty, Neoplasm, Residual, liquid biopsy, business.industry, Biopsy, MEDLINE, biomarkers, Adult care, Disease, circulating DNA, Medical Oncology, Pediatric cancer, cell-free DNA, HEMATOLOGY AND ONCOLOGY: Edited by Brigitte Widemann, Tissue heterogeneity, Pediatrics, Perinatology and Child Health, Pediatric oncology, medicine, Biomarkers, Tumor, Humans, Intensive care medicine, business, Child, Tissue biopsy

Abstract

Purpose of review Liquid biopsies have emerged as a noninvasive alternative to tissue biopsy with potential applications during all stages of pediatric oncology care. The purpose of this review is to provide a survey of pediatric cell-free DNA (cfDNA) studies, illustrate their potential applications in pediatric oncology, and to discuss technological challenges and approaches to overcome these hurdles. Recent findings Recent literature has demonstrated liquid biopsies' ability to inform treatment selection at diagnosis, monitor clonal evolution during treatment, sensitively detect minimum residual disease following local control, and provide sensitive posttherapy surveillance. Advantages include reduced procedural anesthesia, molecular profiling unbiased by tissue heterogeneity, and ability to track clonal evolution. Challenges to wider implementation in pediatric oncology, however, include blood volume restrictions and relatively low mutational burden in childhood cancers. Multiomic approaches address challenges presented by low-mutational burden, and novel bioinformatic analyses allow a single assay to yield increasing amounts of information, reducing blood volume requirements. Summary Liquid biopsies hold tremendous promise in pediatric oncology, enabling noninvasive serial surveillance with adaptive care. Already integrated into adult care, recent advances in technologies and bioinformatics have improved applicability to the pediatric cancer landscape.

Published

2021

15. CASZ1 induces skeletal muscle and rhabdomyosarcoma differentiation through a feed-forward loop with MYOD and MYOG

Author

Xiyuan Zhang, Marielle E. Yohe, Zhihui Liu, Carol J. Thiele, Norris Lam, Haiyan Lei, Jun Wei, Jack F. Shern, Oliver Yockey, Max Xu, Arnulfo Mendoza, Edjay R. Hernandez, Sakereh Carter, and Javed Khan

Subjects

0301 basic medicine, Cell biology, genetic structures, Carcinogenesis, Science, General Physics and Astronomy, Mice, SCID, Biology, Muscle Development, MyoD, Article, General Biochemistry, Genetics and Molecular Biology, Myoblasts, 03 medical and health sciences, 0302 clinical medicine, stomatognathic system, medicine, Animals, Humans, Myocyte, Rhabdomyosarcoma, Embryonal, Epigenetics, Muscle, Skeletal, Rhabdomyosarcoma, lcsh:Science, Transcription factor, MyoD Protein, Zinc finger transcription factor, Multidisciplinary, Skeletal muscle, Sarcoma, General Chemistry, biochemical phenomena, metabolism, and nutrition, medicine.disease, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Female, Myogenin, lcsh:Q, Embryonal rhabdomyosarcoma, Transcription Factors

Abstract

Embryonal rhabdomyosarcoma (ERMS) is a childhood cancer that expresses myogenic master regulatory factor MYOD but fails to differentiate. Here, we show that the zinc finger transcription factor CASZ1 up-regulates MYOD signature genes and induces skeletal muscle differentiation in normal myoblasts and ERMS. The oncogenic activation of the RAS-MEK pathway suppresses CASZ1 expression in ERMS. ChIP-seq, ATAC-seq and RNA-seq experiments reveal that CASZ1 directly up-regulates skeletal muscle genes and represses non-muscle genes through affecting regional epigenetic modifications, chromatin accessibility and super-enhancer establishment. Next generation sequencing of primary RMS tumors identified a single nucleotide variant in the CASZ1 coding region that potentially contributes to ERMS tumorigenesis. Taken together, loss of CASZ1 activity, due to RAS-MEK signaling or genetic alteration, impairs ERMS differentiation, contributing to RMS tumorigenesis., Embryonal rhabdomyosarcoma (ERMS) is a childhood cancer with impaired myogenic differentiation despite the presence of myogenic transcription factors. Here, the authors show that CASZ1 directly regulates these myogenic factors and the loss of CASZ1 is due to RAS-MEK signaling in ERMS.

Published

2020

16. Immuno-transcriptomic profiling of extracranial pediatric solid malignancies

Author

Jack F. Shern, Ching C. Lau, Young K. Song, Beverly A. Teicher, Shintaro Iwata, Paul S. Meltzer, Javed Khan, Uma Mudunuri, Daniel Catchpoole, Yuelin J. Zhu, Udayan Guha, Jay S. Wunder, Marc Ladanyi, Sivasish Sindiri, Marielle E. Yohe, David Milewski, Irene L. Andrulis, John A. Ligon, Nicolas J. Llosa, Xinyu Wen, Rimas J. Orentas, Manoj Tyagi, Igor B. Kuznetsov, Daniel Leino, Yue Qi, Hsien-Chao Chou, Heather Magnan, Jeetendra Kumar, Sushma Nagaraj, Andrew S. Brohl, Vineela Gangalapudi, Jack R. Collins, Jun Wei, Brian Turpin, Katherine E. Masih, Hue V. Reardon, Silvia Regina Caminada de Toledo, Masih, Katherine [0000-0002-0809-668X], and Apollo - University of Cambridge Repository

Subjects

Male, Adolescent, Receptors, Antigen, T-Cell, Immune Targeting, Gene Expression, Biology, Immunotherapy, Adoptive, Article, General Biochemistry, Genetics and Molecular Biology, Whole Exome Sequencing, Immune system, Lymphocytes, Tumor-Infiltrating, Antigens, Neoplasm, PRAME, Cell Line, Tumor, Neoplasms, Exome Sequencing, medicine, Immunogenetics, Tumor Microenvironment, Humans, Child, Tumor-infiltrating lymphocytes, Gene Expression Profiling, T-cell receptor, immunopeptidomics, Cancer, Infant, RNA sequencing, adoptive cell therapy, pediatric oncology, immunogenomics, 0601 Biochemistry and Cell Biology, 1116 Medical Physiology, medicine.disease, Immune Checkpoint Proteins, Pediatric cancer, tumor-infiltrating lymphocytes, Child, Preschool, Cancer research, Female, Sarcoma, T cell receptor, Transcriptome

Abstract

SUMMARY We perform an immunogenomics analysis utilizing whole-transcriptome sequencing of 657 pediatric extra-cranial solid cancer samples representing 14 diagnoses, and additionally utilize transcriptomes of 131 pediatric cancer cell lines and 147 normal tissue samples for comparison. We describe patterns of infiltrating immune cells, T cell receptor (TCR) clonal expansion, and translationally relevant immune checkpoints. We find that tumor-infiltrating lymphocytes and TCR counts vary widely across cancer types and within each diagnosis, and notably are significantly predictive of survival in osteosarcoma patients. We identify potential cancer-specific immunotherapeutic targets for adoptive cell therapies including cell-surface proteins, tumor germline antigens, and lineage-specific transcription factors. Using an orthogonal immunopeptidomics approach, we find several potential immunotherapeutic targets in osteosarcoma and Ewing sarcoma and validated PRAME as a bona fide multi-pediatric cancer target. Importantly, this work provides a critical framework for immune targeting of extracranial solid tumors using parallel immuno-transcriptomic and -peptidomic approaches., Graphical Abstract, In brief Brohl et al. perform immunogenomics analysis of a cohort of 788 pediatric extracranial solid tumors and cell lines, representing 14 diagnoses, utilizing RNA sequencing. They broadly describe prognostically relevant immunophenotypes and provide proof of concept of a transcriptomics-informed adoptive cellular therapy approach, validating PRAME as a multi-pediatric cancer immunotherapy target.

Published

2021

17. Genetic Characterization, Current Model Systems and Prognostic Stratification in PAX Fusion-Negative vs. PAX Fusion-Positive Rhabdomyosarcoma

Author

Carina Dehner, Jack F. Shern, Amy E. Armstrong, Angela C. Hirbe, and Marielle E. Yohe

Subjects

Oncology, medicine.medical_specialty, alveolar rhabdomyosarcoma, fusion-negative RMS, embryonal rhabdomyosarcoma, Review, QH426-470, Models, Biological, Genetic pathways, Prognostic stratification, Epigenesis, Genetic, Mice, Cell Line, Tumor, Internal medicine, Genetics, Animals, Humans, Medicine, Rhabdomyosarcoma, Genetics (clinical), business.industry, Soft tissue sarcoma, Prognosis, medicine.disease, Fusion-Positive Rhabdomyosarcoma, Risk stratification, Alveolar rhabdomyosarcoma, Embryonal rhabdomyosarcoma, rhabdomyosarcoma, Gene Fusion, Paxillin, business, fusion-positive RMS, Signal Transduction

Abstract

Rhabdomyosarcoma (RMS) is the most common soft tissue sarcoma in children and adolescents and accounts for approximately 2% of soft tissue sarcomas in adults. It is subcategorized into distinct subtypes based on histological features and fusion status (PAX-FOXO1/VGLL2/NCOA2). Despite advances in our understanding of the pathobiological and molecular landscape of RMS, the prognosis of these tumors has not significantly improved in recent years. Developing a better understanding of genetic abnormalities and risk stratification beyond the fusion status are crucial to developing better therapeutic strategies. Herein, we aim to highlight the genetic pathways/abnormalities involved, specifically in fusion-negative RMS, assess the currently available model systems to study RMS pathogenesis, and discuss available prognostic factors as well as their importance for risk stratification to achieve optimal therapeutic management.

Published

2021

18. Histone hyperacetylation disrupts core gene regulatory architecture in rhabdomyosarcoma

Author

Hsien-Chao Chou, Anna M. Chiarella, Jiji Chen, Javed Khan, Sukriti Bagchi, Xinyu Wen, Ranu S Sinniah, Ashley Walton, Nathaniel A. Hathaway, Silvia Pomella, Young Min Song, Jack F. Shern, Xiaoli S. Wu, Christopher R. Vakoc, Benjamin Z. Stanton, Berkley E. Gryder, Keji Zhao, Rossella Rota, and Carly M. Sayers

Subjects

BRD4, Chromatin Immunoprecipitation, Pyridines, RNA Stability, RNA polymerase II, Settore MED/05, Article, Histone Deacetylases, Histones, 03 medical and health sciences, 0302 clinical medicine, Transcription (biology), Cell Line, Tumor, Rhabdomyosarcoma, Genetics, Humans, Clustered Regularly Interspaced Short Palindromic Repeats, Gene Regulatory Networks, Transcription factor, 030304 developmental biology, Regulation of gene expression, 0303 health sciences, biology, Forkhead Box Protein O1, SOXE Transcription Factors, Acetylation, Cell biology, Gene Expression Regulation, Neoplastic, Histone, Enhancer Elements, Genetic, Benzamides, biology.protein, Histone deacetylase, RNA Polymerase II, Single-Cell Analysis, Chromatin immunoprecipitation, 030217 neurology & neurosurgery, Transcription Factors

Abstract

Core regulatory transcription factors (CR TFs) orchestrate the placement of super-enhancers (SEs) to activate transcription of cell-identity specifying gene networks, and are critical in promoting cancer. Here, we define the core regulatory circuitry of rhabdomyosarcoma and identify critical CR TF dependencies. These CR TFs build SEs that have the highest levels of histone acetylation, yet paradoxically the same SEs also harbor the greatest amounts of histone deacetylases. We find that hyperacetylation selectively halts CR TF transcription. To investigate the architectural determinants of this phenotype, we used absolute quantification of architecture (AQuA) HiChIP, which revealed erosion of native SE contacts, and aberrant spreading of contacts that involved histone acetylation. Hyperacetylation removes RNA polymerase II (RNA Pol II) from core regulatory genetic elements, and eliminates RNA Pol II but not BRD4 phase condensates. This study identifies an SE-specific requirement for balancing histone modification states to maintain SE architecture and CR TF transcription.

Published

2019

19. Chemical genomics reveals histone deacetylases are required for core regulatory transcription

Author

Abigail Cleveland, Marielle E. Yohe, Jack F. Shern, Lei Wu, Rossella Rota, Paul M.C. Park, Berkley E. Gryder, Olaf Wiest, Jun Qi, Silvia Pomella, Javed Khan, Taylor R. Quinn, Girma M. Woldemichael, Benjamin Z. Stanton, and Young Min Song

Subjects

0301 basic medicine, Oncogene Proteins, Fusion, Transcription, Genetic, General Physics and Astronomy, 02 engineering and technology, Settore MED/05, Gene regulatory networks, Transcription (biology), Rhabdomyosarcoma, Paired Box Transcription Factors, Protein Isoforms, lcsh:Science, Regulation of gene expression, Multidisciplinary, Chemistry, High-Throughput Nucleotide Sequencing, Acetylation, Genomics, 021001 nanoscience & nanotechnology, Chromatin, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, Enhancer Elements, Genetic, 0210 nano-technology, Structural biology, Chemical genetics, Gene isoform, Science, Primary Cell Culture, Molecular Dynamics Simulation, Chromatin structure, General Biochemistry, Genetics and Molecular Biology, Histone Deacetylases, Article, 03 medical and health sciences, Cell Line, Tumor, Humans, Epigenetics, Enhancer, Transcription factor, Sequence Analysis, RNA, General Chemistry, High-Throughput Screening Assays, Gene regulation, Histone Deacetylase Inhibitors, 030104 developmental biology, Molecular Probes, lcsh:Q

Abstract

Identity determining transcription factors (TFs), or core regulatory (CR) TFs, are governed by cell-type specific super enhancers (SEs). Drugs to selectively inhibit CR circuitry are of high interest for cancer treatment. In alveolar rhabdomyosarcoma, PAX3-FOXO1 activates SEs to induce the expression of other CR TFs, providing a model system for studying cancer cell addiction to CR transcription. Using chemical genetics, the systematic screening of chemical matter for a biological outcome, here we report on a screen for epigenetic chemical probes able to distinguish between SE-driven transcription and constitutive transcription. We find that chemical probes along the acetylation-axis, and not the methylation-axis, selectively disrupt CR transcription. Additionally, we find that histone deacetylases (HDACs) are essential for CR TF transcription. We further dissect the contribution of HDAC isoforms using selective inhibitors, including the newly developed selective HDAC3 inhibitor LW3. We show HDAC1/2/3 are the co-essential isoforms that when co-inhibited halt CR transcription, making CR TF sites hyper-accessible and disrupting chromatin looping., Core regulatory transcription factors are usually regulated by cell-type specific super enhancers (SEs). Here, the authors screen for chemical probes able to distinguish between SE-driven and promoter-driven transcription and find that histone deacetylases are selectively required for core regulatory transcription.

Published

2019

20. Preclinical Development of Bivalent Chimeric Antigen Receptors Targeting Both CD19 and CD22

Author

Waleed Haso, Terry J. Fry, Nirali N. Shah, Jack F. Shern, Constance M. Yuan, Sneha Ramakrishna, Thomas J. Fountaine, Sang M. Nguyen, Maryalice Stetler-Stevenson, Anusha Ponduri, and Haiying Qin

Subjects

0301 basic medicine, Cancer Research, lcsh:RC254-282, CD19, Bivalent (genetics), Article, Cell therapy, 03 medical and health sciences, Transduction (genetics), 0302 clinical medicine, Antigen, immune system diseases, hemic and lymphatic diseases, Pharmacology (medical), biology, chimeric antigen receptor, CD22, leukemia, adoptive cell therapy, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chimeric antigen receptor, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Molecular Medicine, human activities

Abstract

Despite high remission rates following CAR-T cell therapy in B-ALL, relapse due to loss of the targeted antigen is increasingly recognized as a mechanism of immune escape. We hypothesized that simultaneous targeting of CD19 and CD22 may reduce the likelihood of antigen loss, thus improving sustained remission rates. A systematic approach to the generation of CAR constructs incorporating two target-binding domains led to several novel CD19/CD22 bivalent CAR constructs. Importantly, we demonstrate the challenges associated with the construction of a bivalent CAR format that preserves bifunctionality against both CD19 and CD22. Using the most active bivalent CAR constructs, we found similar transduction efficiency compared to that of either CD19 or CD22 single CARs alone. When expressed on human T cells, the optimized CD19/CD22 CAR construct induced comparable interferon γ and interleukin-2 in vitro compared to single CARs against dual-antigen-expressing as well as single-antigen-expressing cell lines. Finally, the T cells expressing CD19/CD22 CAR eradicated ALL cell line xenografts and patient-derived xenografts (PDX), including a PDX generated from a patient with CD19− relapse following CD19-directed CAR therapy. The CD19/CD22 bivalent CAR provides an opportunity to test whether simultaneous targeting may reduce risk of antigen loss. Keywords: chimeric antigen receptor, adoptive cell therapy, leukemia

Published

2018

21. Prioritization of Novel Agents for Patients with Rhabdomyosarcoma: A Report from the Children’s Oncology Group (COG) New Agents for Rhabdomyosarcoma Task Force

Author

William H. Meyer, Leo Mascarenhas, Michael D. Deel, Stephen X. Skapek, Brian Turpin, Holly L Pacenta, Peter J. Houghton, Corinne M. Linardic, Douglas J. Harrison, Pooja Hingorani, Douglas S. Hawkins, Wendy Allen-Rhoades, James F. Amatruda, Jack F. Shern, Christine M. Heske, Charles Keller, Javed Khan, David M. Langenau, Elizabeth Stewart, Theodore W. Laetsch, and Eleanor Y. Chen

Subjects

Oncology, Prioritization, medicine.medical_specialty, lcsh:Medicine, new agents, Review, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Cog, Internal medicine, medicine, metastasis, Rhabdomyosarcoma, 030304 developmental biology, relapse, 0303 health sciences, clinical trials, business.industry, Soft tissue sarcoma, lcsh:R, General Medicine, medicine.disease, Clinical trial, Novel agents, 030220 oncology & carcinogenesis, Sarcoma, rhabdomyosarcoma, business

Abstract

Rhabdomyosarcoma is the most common soft tissue sarcoma diagnosed in children and adolescents. Patients that are diagnosed with advanced or relapsed disease have exceptionally poor outcomes. The Children’s Oncology Group (COG) convened a rhabdomyosarcoma new agent task force in 2020 to systematically evaluate novel agents for inclusion in phase 2 or phase 3 clinical trials for patients diagnosed with rhabdomyosarcoma, following a similar effort for Ewing sarcoma. The task force was comprised of clinicians and basic scientists who collectively identified new agents for evaluation and prioritization in clinical trial testing. Here, we report the work of the task force including the framework upon which the decisions were rendered and review the top classes of agents that were discussed. Representative agents include poly-ADP-ribose polymerase (PARP) inhibitors in combination with cytotoxic agents, mitogen-activated protein kinase (MEK) inhibitors in combination with type 1 insulin-like growth factor receptor (IGFR1) inhibitors, histone deacetylase (HDAC) inhibitors, and novel cytotoxic agents.

Published

2021

22. Chromosome 8 gain is associated with high-grade transformation in MPNST

Author

Xiyuan Zhang, Abigail Godec, Jay Mashl, Li Ding, Christopher A. Miller, Sara J. C. Gosline, Christine A. Pratilas, Shunqiang Li, Xiaochun Zhang, Kai Pollard, Paul Jones, Hua Xu, Xiaodan Wan, Angela C. Hirbe, Tina Primeau, Fausto J. Rodriguez, K. Yang, Himanshi Bhatia, Jack F. Shern, Sonika Dahiya, Chang In Moon, Carina Dehner, Zhaohe Zhou, and Yuxi Wang

Subjects

0301 basic medicine, Oncology, Adult, Male, medicine.medical_specialty, Neurofibromatosis 1, Copy number analysis, Malignant peripheral nerve sheath tumor, Nerve Sheath Neoplasms, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Genetics, Humans, Neurofibromatosis, Child, Exome sequencing, Cancer, business.industry, Chromosome, General Medicine, Middle Aged, medicine.disease, Survival Analysis, 030104 developmental biology, 030220 oncology & carcinogenesis, Medicine, Female, Sarcoma, Neoplasm Recurrence, Local, business, Chromosomes, Human, Pair 8, Research Article

Abstract

One of the most common malignancies affecting adults with Neurofibromatosis type 1 (NF1) is the malignant peripheral nerve sheath tumor (MPNST), an aggressive and often fatal sarcoma that commonly arises from benign plexiform neurofibromas. Despite advances in our understanding of MPNST pathobiology, there are few effective therapeutic options, and no investigational agents have proven successful in clinical trials. To further understand the genomic heterogeneity of MPNST, and to generate a preclinical platform that encompasses this heterogeneity, we developed a collection of NF1-MPNST patient-derived xenografts (PDX). These PDX were compared with the primary tumors from which they were derived using copy number analysis, whole exome sequencing, and RNA sequencing. We identified chromosome 8 gain as a recurrent genomic event in MPNST and validated its occurrence by FISH in the PDX and parental tumors, in a validation cohort, and by single-cell sequencing in the PDX. Finally, we show that chromosome 8 gain is associated with inferior overall survival in soft-tissue sarcomas. These data suggest that chromosome 8 gain is a critical event in MPNST pathogenesis and may account for the aggressive nature and poor outcomes in this sarcoma subtype.

Published

2021

23. Defining the Extracellular Matrix of Rhabdomyosarcoma

Author

Ayeza Bajwa, J Steffan Bond, Charles Keller, Sergei P. Boudko, Sakir H. Gultekin, Atiya Mansoor, Megan M. Cleary, Teagan P. Settelmeyer, Christopher P. Hartley, Noah E. Berlow, Melvin Lathara, Hans Peter Bächinger, Elena Pokidysheva, Takako Sasaki, Jack F. Shern, Narendra Bharathy, Xiaolei Lian, and Ganapati Srinivasa

Subjects

Cancer Research, Tumor microenvironment, Tissue microarray, COL18A1, Type XVIII collagen, Fibrillins, Biology, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, survival, lcsh:RC254-282, Undifferentiated Pleomorphic Sarcoma, matrix, Extracellular matrix, Oncology, medicine, Cancer research, PLOD1/2, Sarcoma, rhabdomyosarcoma, Rhabdomyosarcoma, Original Research

Abstract

Rhabdomyosarcoma (RMS) is the most common soft-tissue sarcoma of childhood with a propensity to metastasize. Current treatment for patients with RMS includes conventional systemic chemotherapy, radiation therapy, and surgical resection; nevertheless, little to no improvement in long term survival has been achieved in decades—underlining the need for target discovery and new therapeutic approaches to targeting tumor cells or the tumor microenvironment. To evaluate cross-species sarcoma extracellular matrix production, we have used murine models which feature knowledge of the myogenic cell-of-origin. With focus on the RMS/undifferentiated pleomorphic sarcoma (UPS) continuum, we have constructed tissue microarrays of 48 murine and four human sarcomas to analyze expression of seven different collagens, fibrillins, and collagen-modifying proteins, with cross-correlation to RNA deep sequencing. We have uncovered that RMS produces increased expression of type XVIII collagen alpha 1 (COL18A1), which is clinically associated with decreased long-term survival. We have also identified significantly increased RNA expression of COL4A1, FBN2, PLOD1, and PLOD2 in human RMS relative to normal skeletal muscle. These results complement recent studies investigating whether soft tissue sarcomas utilize collagens, fibrillins, and collagen-modifying enzymes to alter the structural integrity of surrounding host extracellular matrix/collagen quaternary structure resulting in improved ability to improve the ability to invade regionally and metastasize, for which therapeutic targeting is possible.

Published

2021

24. The Role of Polycomb Repressive Complex in Malignant Peripheral Nerve Sheath Tumor

Author

George Mo, Béga Murray, Jack F. Shern, and Xiyuan Zhang

Subjects

0301 basic medicine, mpnst, lcsh:QH426-470, Schwann cell, Malignant peripheral nerve sheath tumor, Review, macromolecular substances, medicine.disease_cause, Nerve Sheath Neoplasms, Neurofibromatosis, 03 medical and health sciences, 0302 clinical medicine, MPNST, Genetics, SUZ12, medicine, Animals, Humans, polycomb repressive complex, Genetics(clinical), malignant peripheral nerve sheath tumor, Polycomb repressive complex, Epigenetics, Genetics (clinical), neurofibromatosis, biology, business.industry, Polycomb Repressive Complex 2, medicine.disease, PRC2, Review article, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mutation, Cancer research, biology.protein, Schwann Cells, Carcinogenesis, business, prc2

Abstract

Malignant peripheral nerve sheath tumors (MPNSTs) are aggressive soft tissue sarcomas that can arise most frequently in patients with neurofibromatosis type 1 (NF1). Despite an increasing understanding of the molecular mechanisms that underlie these tumors, there remains limited therapeutic options for this aggressive disease. One potentially critical finding is that a significant proportion of MPNSTs exhibit recurrent mutations in the genes EED or SUZ12, which are key components of the polycomb repressive complex 2 (PRC2). Tumors harboring these genetic lesions lose the marker of transcriptional repression, trimethylation of lysine residue 27 on histone H3 (H3K27me3) and have dysregulated oncogenic signaling. Given the recurrence of PRC2 alterations, intensive research efforts are now underway with a focus on detailing the epigenetic and transcriptomic consequences of PRC2 loss as well as development of novel therapeutic strategies for targeting these lesions. In this review article, we will summarize the recent findings of PRC2 in MPNST tumorigenesis, including highlighting the functions of PRC2 in normal Schwann cell development and nerve injury repair, as well as provide commentary on the potential therapeutic vulnerabilities of a PRC2 deficient tumor cell.

Published

2020

25. Relationship of DNA methylation to mutational changes and transcriptional organization in fusion-positive and fusion-negative rhabdomyosarcoma

Author

Bishwanath Chatterjee, Peter J. Houghton, Yonghong Wang, Young Min Song, Frederic G. Barr, Javed Khan, Stephen M. Hewitt, Rajesh Patidar, Wenyue Sun, Robert L. Walker, Jack F. Shern, Daniel C. Edelman, Corinne M. Linardic, Bruce R. Pawel, and Paul S. Meltzer

Subjects

Untranslated region, Cancer Research, genetic structures, Oncogene Proteins, Fusion, Datasets as Topic, Biology, Article, Epigenesis, Genetic, 03 medical and health sciences, Fusion-Negative Rhabdomyosarcoma, 0302 clinical medicine, Cell Line, Tumor, Rhabdomyosarcoma, medicine, Animals, Humans, Paired Box Transcription Factors, Point Mutation, Epigenetics, Child, Promoter Regions, Genetic, Gene, Cell Proliferation, Muscle Neoplasms, Methylation, DNA Methylation, medicine.disease, musculoskeletal system, Molecular biology, Fusion protein, Xenograft Model Antitumor Assays, Muscle, Striated, Gene Expression Regulation, Neoplastic, Oncology, Tissue Array Analysis, 030220 oncology & carcinogenesis, DNA methylation, ras Proteins

Abstract

Our previous study of DNA methylation in the pediatric soft tissue tumor rhabdomyosarcoma (RMS) demonstrated that fusion-positive (FP) and fusion-negative (FN) RMS tumors exhibit distinct DNA methylation patterns. To further examine the significance of DNA methylation differences in RMS, we investigated genome-wide DNA methylation profiles in discovery and validation cohorts. Unsupervised analysis of DNA methylation data identified novel distinct subsets associated with the specific fusion subtype in FP RMS and with RAS mutation status in FN RMS. Furthermore, the methylation pattern in normal muscle is most similar to the FN subset with wild-type RAS mutation status. Several biologically relevant genes were identified with methylation and expression differences between the two fusion subtypes of FP RMS or between the RAS wild-type and mutant subsets of FN RMS. Genomic localization studies showed that promoter and intergenic regions were hypomethylated and the 3’ untranslated regions were hypermethylated in FP compared to FN tumors. There was also a significant difference in the distribution of PAX3-FOXO1 binding sites between genes with and without differential methylation. Moreover, genes with PAX3-FOXO1 binding sites and promoter hypomethylation exhibited the highest frequency of overexpression in FP tumors. Finally, a comparison of RMS model systems revealed that patient-derived xenografts most closely recapitulate the DNA methylation patterns found in human RMS tumors compared with cell lines and cell line-derived xenografts. In conclusion, these findings highlight the interaction of epigenetic changes with mutational alterations and transcriptional organization in RMS tumors, and contribute to improved molecular categorization of these tumors.

Published

2019

26. Sequential loss of tumor surface antigens following chimeric antigen receptor T-cell therapies in diffuse large B-cell lymphoma

Author

Jack F. Shern, Elaine S. Jaffe, Ira Lignugaris Kraft, Haneen Shalabi, Constance M. Yuan, Terry J. Fry, Hao-Wei Wang, Julie D. Zimbelman, Daniel W. Lee, Maryalice Stetler-Stevenson, Roger Giller, Cindy Delbrook, Nirali N. Shah, and Bonnie Yates

Subjects

0301 basic medicine, CD20, biology, medicine.medical_treatment, T cell, Hematology, Immunotherapy, medicine.disease, Chimeric antigen receptor, CD19, Lymphoma, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Antigen, immune system diseases, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, biology.protein, medicine, Cancer research, Online Only Articles, neoplasms, Diffuse large B-cell lymphoma

Abstract

Diffuse large B-cell lymphoma (DLBCL) is the predominant subtype of Non-Hodgkin lymphoma (NHL) in adolescents and adults. Originating from a B-cell lineage, the neoplastic cells typically express pan-B- cell antigens including CD19, CD20 and CD22.[1][1] DLBCL can be highly curable, particularly with

Published

2018

27. PAX3-FOXO1 Establishes Myogenic Super Enhancers and Confers BET Bromodomain Vulnerability

Author

Jun Wei, Rajarshi Guha, Xinyu Wen, Sudipto Das, Craig J. Thomas, Young K. Song, Berkley E. Gryder, Madhu Lal-Nag, Joana G. Marques, Nirmalya Sen, Jack F. Shern, Beat W. Schaefer, Keji Zhao, Abigail Cleveland, Marc Ferrer, Alberto Gualtieri, Xiaohu Zhang, Sivasish Sindiri, Marielle E. Yohe, Marco Wachtel, Silvia Pomella, Thorkell Andresson, Rossella Rota, Hsien-Chao Chou, Javed Khan, Frederic G. Barr, University of Zurich, and Khan, Javed

Subjects

0301 basic medicine, Male, endocrine system, BRD4, Oncogene Proteins, Fusion, Cell Cycle Proteins, 610 Medicine & health, Biology, MyoD, digestive system, Settore MED/05, Article, Epigenesis, Genetic, Small Molecule Libraries, 03 medical and health sciences, Mice, Super-enhancer, Protein Domains, Cell Line, Tumor, medicine, Animals, Humans, Paired Box Transcription Factors, Enhancer, Transcription factor, Rhabdomyosarcoma, Alveolar, MyoD Protein, N-Myc Proto-Oncogene Protein, Nuclear Proteins, musculoskeletal system, medicine.disease, Xenograft Model Antitumor Assays, Chromatin, Bromodomain, 030104 developmental biology, Enhancer Elements, Genetic, Oncology, 10036 Medical Clinic, embryonic structures, Cancer research, Alveolar rhabdomyosarcoma, Female, Myogenin, 2730 Oncology, Protein Binding, Transcription Factors

Abstract

Alveolar rhabdomyosarcoma is a life-threatening myogenic cancer of children and adolescent young adults, driven primarily by the chimeric transcription factor PAX3–FOXO1. The mechanisms by which PAX3–FOXO1 dysregulates chromatin are unknown. We find PAX3–FOXO1 reprograms the cis-regulatory landscape by inducing de novo super enhancers. PAX3–FOXO1 uses super enhancers to set up autoregulatory loops in collaboration with the master transcription factors MYOG, MYOD, and MYCN. This myogenic super enhancer circuitry is consistent across cell lines and primary tumors. Cells harboring the fusion gene are selectively sensitive to small-molecule inhibition of protein targets induced by, or bound to, PAX3–FOXO1-occupied super enhancers. Furthermore, PAX3–FOXO1 recruits and requires the BET bromodomain protein BRD4 to function at super enhancers, resulting in a complete dependence on BRD4 and a significant susceptibility to BRD inhibition. These results yield insights into the epigenetic functions of PAX3–FOXO1 and reveal a specific vulnerability that can be exploited for precision therapy. Significance: PAX3–FOXO1 drives pediatric fusion-positive rhabdomyosarcoma, and its chromatin-level functions are critical to understanding its oncogenic activity. We find that PAX3–FOXO1 establishes a myoblastic super enhancer landscape and creates a profound subtype-unique dependence on BET bromodomains, the inhibition of which ablates PAX3–FOXO1 function, providing a mechanistic rationale for exploring BET inhibitors for patients bearing PAX-fusion rhabdomyosarcoma. Cancer Discov; 7(8); 884–99. ©2017 AACR. This article is highlighted in the In This Issue feature, p. 783

Published

2017

28. Genomic Profiling of a Large Set of Diverse Pediatric Cancers Identifies Known and Novel Mutations across Tumor Spectra

Author

Doron Lipson, Trevor J. Pugh, Joana Buxhaku, Jie He, Jack F. Shern, Vinny Faso, Blair Glanville, Alexis Germain, Soheil Meshinchi, James Sun, James Suh, Katherine A. Janeway, Samantha Morley, Julia A. Elvin, John M. Maris, Rachel L. Erlich, Jeffrey S. Ross, Garrett M. Frampton, Siraj M. Ali, Hilary Davies, Jo-Anne Vergilio, Mark Bailey, Daniel Spritz, Juliann Chmielecki, Shakti H. Ramkissoon, Vincent A. Miller, and Philip J. Stephens

Subjects

0301 basic medicine, Male, Cancer Research, Adolescent, PAX3, Biology, Bioinformatics, medicine.disease_cause, Article, Ganglioglioma, 03 medical and health sciences, 0302 clinical medicine, Neuroblastoma, hemic and lymphatic diseases, Neoplasms, medicine, Humans, Rhabdomyosarcoma, Child, neoplasms, Mutation, Gene Expression Profiling, Infant, Newborn, Cancer, Astrocytoma, Infant, medicine.disease, Gene expression profiling, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Child, Preschool, Cancer research, Female, Transcriptome

Abstract

Pediatric cancers are generally characterized by low mutational burden and few recurrently mutated genes. Recent studies suggest that genomic alterations may help guide treatment decisions and clinical trial selection. Here, we describe genomic profiles from 1,215 pediatric tumors representing sarcomas, extracranial embryonal tumors, brain tumors, hematologic malignancies, carcinomas, and gonadal tumors. Comparable published datasets identified similar frequencies of clinically relevant alterations, validating this dataset as biologically relevant. We identified novel ALK fusions in a neuroblastoma (BEND5–ALK) and an astrocytoma (PPP1CB–ALK), novel BRAF fusions in an astrocytoma (BCAS1–BRAF) and a ganglioglioma (TMEM106B–BRAF), and a novel PAX3–GLI2 fusion in a rhabdomyosarcoma. Previously characterized ALK, NTRK1, and PAX3 fusions were observed in unexpected malignancies, challenging the "disease-specific" alterations paradigm. Finally, we identified recurrent variants of unknown significance in MLL3 and PRSS1 predicted to have functional impact. Data from these 1,215 tumors are publicly available for discovery and validation. Cancer Res; 77(2); 509–19. ©2017 AACR.

Published

2017

29. CD19 CAR immune pressure induces B-precursor acute lymphoblastic leukaemia lineage switch exposing inherent leukaemic plasticity

Author

Sang M. Nguyen, Michael C. Jensen, Haiying Qin, Jack F. Shern, Daniel W. Lee, Haiyan Lei, Javed Khan, Kathryn M. Welp, Thomas J. Fountaine, Rebecca Gardner, Elad Jacoby, Berkley E. Gryder, Yinmeng Yang, Young K. Song, Terry J. Fry, Christopher D. Chien, Crystal L. Mackall, and Alix E. Seif

Subjects

0301 basic medicine, Myeloid, Lineage (genetic), Science, Cell Plasticity, Receptors, Antigen, T-Cell, General Physics and Astronomy, Biology, General Biochemistry, Genetics and Molecular Biology, CD19, Article, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Recurrence, hemic and lymphatic diseases, Cell Line, Tumor, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, medicine, Animals, Cell Lineage, Myeloid Cells, Gene Editing, Mice, Knockout, Multidisciplinary, Genome, Lineage markers, General Chemistry, Chimeric antigen receptor, Chromatin, Clone Cells, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Phenotype, 030220 oncology & carcinogenesis, Immunology, Cancer research, biology.protein, Reprogramming, human activities

Abstract

Adoptive immunotherapy using chimeric antigen receptor (CAR) expressing T cells targeting the CD19 B lineage receptor has demonstrated marked success in relapsed pre-B-cell acute lymphoblastic leukaemia (ALL). Persisting CAR-T cells generate sustained pressure against CD19 that may drive unique mechanisms of resistance. Pre-B ALL originates from a committed pre-B cell or an earlier progenitor, with potential to reprogram into other hematopoietic lineages. Here we report changes in lineage markers including myeloid conversion in patients following CD19 CAR therapy. Using murine ALL models we study the long-term effects of CD19 CAR-T cells and demonstrate partial or complete lineage switch as a consistent mechanism of CAR resistance depending on the underlying genetic oncogenic driver. Deletion of Pax5 or Ebf1 recapitulates lineage reprogramming occurring during CD19 CAR pressure. Our findings establish lineage switch as a mechanism of CAR resistance exposing inherent plasticity in genetic subtypes of pre-B-cell ALL., CAR-T targeting CD19 have been successfully used in a variety of B-cell malignancies but patients may eventually relapse. Here, the authors show that CD19 CAR-T resistance in pre-B cell ALL can be due to the induction of a myeloid lineage switch through an epigenetic alterations in master regulators of B cell development.

Published

2016

30. Comprehensive genomic analysis of rhabdomyosarcoma reveals a landscape of alterations affecting a common genetic axis in fusion-positive and fusion-negative tumors

Author

Juliann Chmielecki, Jaume Mora, Jack F. Shern, Young K. Song, Li Chen, Gad Getz, Hongling Liao, Shile Zhang, Stephen X. Skapek, Frederic G. Barr, Lauren Ambrogio, Dominik Bogen, Laura Hurd, Daniel Catchpoole, Sivasish Sindiri, Andrew S. Brohl, Daniel Auclair, Catherine Tolman, Douglas S. Hawkins, Jianjun Wang, Thomas C. Badgett, Jun S. Wei, Mara Rosenberg, James R. Anderson, Javed Khan, Matthew Meyerson, and Rajesh Patidar

Subjects

Neuroblastoma RAS viral oncogene homolog, DNA Copy Number Variations, Genotype, Oncogene Proteins, Fusion, Class I Phosphatidylinositol 3-Kinases, Cell Cycle Proteins, Recurrent Rhabdomyosarcoma, Biology, medicine.disease_cause, Article, Proto-Oncogene Proteins p21(ras), Mice, Phosphatidylinositol 3-Kinases, Rhabdomyosarcoma, medicine, Animals, Cluster Analysis, Humans, Paired Box Transcription Factors, Exome, Gene Regulatory Networks, HRAS, neoplasms, Chromosome Aberrations, Gene Rearrangement, Mutation, Gene rearrangement, Genomics, medicine.disease, musculoskeletal system, Receptors, Fibroblast Growth Factor, Gene Expression Regulation, Neoplastic, Oncology, Cancer research, KRAS, Genome-Wide Association Study, Signal Transduction

Abstract

Despite gains in survival, outcomes for patients with metastatic or recurrent rhabdomyosarcoma remain dismal. In a collaboration between the National Cancer Institute, Children's Oncology Group, and Broad Institute, we performed whole-genome, whole-exome, and transcriptome sequencing to characterize the landscape of somatic alterations in 147 tumor/normal pairs. Two genotypes are evident in rhabdomyosarcoma tumors: those characterized by the PAX3 or PAX7 fusion and those that lack these fusions but harbor mutations in key signaling pathways. The overall burden of somatic mutations in rhabdomyosarcoma is relatively low, especially in tumors that harbor a PAX3/7 gene fusion. In addition to previously reported mutations in NRAS, KRAS, HRAS, FGFR4, PIK3CA, and CTNNB1, we found novel recurrent mutations in FBXW7 and BCOR, providing potential new avenues for therapeutic intervention. Furthermore, alteration of the receptor tyrosine kinase/RAS/PIK3CA axis affects 93% of cases, providing a framework for genomics-directed therapies that might improve outcomes for patients with rhabdomyosarcoma. Significance: This is the most comprehensive genomic analysis of rhabdomyosarcoma to date. Despite a relatively low mutation rate, multiple genes were recurrently altered, including NRAS, KRAS, HRAS, FGFR4, PIK3CA, CTNNB1, FBXW7, and BCOR. In addition, a majority of rhabdomyosarcoma tumors alter the receptor tyrosine kinase/RAS/PIK3CA axis, providing an opportunity for genomics-guided intervention. Cancer Discov; 4(2); 216–31. ©2014 AACR. This article is highlighted in the In This Issue feature, p. 131

Published

2014

31. ARL2 and BART Enter Mitochondria and Bind the Adenine Nucleotide Transporter

Author

Jack F. Shern, Richard A. Kahn, Hillary Van Valkenburgh, J. Daniel Sharer, and Douglas C. Wallace

Subjects

Recombinant Fusion Proteins, Molecular Sequence Data, Mice, Transgenic, GTPase, Mitochondrion, Biology, Kidney, Article, Protein Structure, Secondary, Mice, GTP-binding protein regulators, Adenine nucleotide, GTP-Binding Proteins, Tumor Cells, Cultured, Animals, Amino Acid Sequence, Muscle, Skeletal, Molecular Biology, Peptide sequence, Mitochondrial Import Sequence, Base Sequence, Myocardium, Brain, Membrane Transport Proteins, Transporter, Cell Biology, Peptide Fragments, Mitochondria, Rats, Cytosol, Biochemistry, Microscopy, Fluorescence, Cattle, Carrier Proteins, Mitochondrial ADP, ATP Translocases, Transcription Factors

Abstract

The ADP-ribosylation factor-like 2 (ARL2) GTPase and its binding partner binder of ARL2 (BART) are ubiquitously expressed in rodent and human tissues and are most abundant in brain. Both ARL2 and BART are predominantly cytosolic, but a pool of each was found associated with mitochondria in a protease-resistant form. ARL2 was found to lack covalent N-myristoylation, present on all other members of the ARF family, thereby preserving the N-terminal amphipathic α-helix as a potential mitochondrial import sequence. An overlay assay was developed to identify binding partners for the BART·ARL2·GTP complex and revealed a specific interaction with a protein in bovine brain mitochondria. Purification and partial microsequencing identified the protein as an adenine nucleotide transporter (ANT). The overlay assay was performed on mitochondria isolated from five different tissues from either wild-type or transgenic mice deleted for ANT1. Results confirmed that ANT1 is the predominant binding partner for the BART·ARL2·GTP complex and that the structurally homologous ANT2 protein does not bind the complex. Cardiac and skeletal muscle mitochondria fromant1−/ant1−mice had increased levels of ARL2, relative to that seen in mitochondria from wild-type animals. We conclude that the amount of ARL2 in mitochondria is subject to regulation via an ANT1-sensitive pathway in muscle tissues.

Published

2002

32. MYCN drives oncogenesis by cooperating with the histone methyltransferase G9a and the WDR5 adaptor to orchestrate global gene transcription.

Author

Zhihui Liu, Xiyuan Zhang, Man Xu, Jason J Hong, Amanda Ciardiello, Haiyan Lei, Jack F Shern, and Carol J Thiele

Subjects

Biology (General), QH301-705.5

Abstract

MYCN activates canonical MYC targets involved in ribosome biogenesis, protein synthesis, and represses neuronal differentiation genes to drive oncogenesis in neuroblastoma (NB). How MYCN orchestrates global gene expression remains incompletely understood. Our study finds that MYCN binds promoters to up-regulate canonical MYC targets but binds to both enhancers and promoters to repress differentiation genes. MYCN binding also increases H3K4me3 and H3K27ac on canonical MYC target promoters and decreases H3K27ac on neuronal differentiation gene enhancers and promoters. WDR5 facilitates MYCN promoter binding to activate canonical MYC target genes, whereas MYCN recruits G9a to enhancers to repress neuronal differentiation genes. Targeting both MYCN's active and repressive transcriptional activities using both WDR5 and G9a inhibitors synergistically suppresses NB growth. We demonstrate that MYCN cooperates with WDR5 and G9a to orchestrate global gene transcription. The targeting of both these cofactors is a novel therapeutic strategy to indirectly target the oncogenic activity of MYCN.

Published

2024

33. Cell-free DNA ultra-low-pass whole genome sequencing to distinguish malignant peripheral nerve sheath tumor (MPNST) from its benign precursor lesion: A cross-sectional study.

Author

Jeffrey J Szymanski, R Taylor Sundby, Paul A Jones, Divya Srihari, Noah Earland, Peter K Harris, Wenjia Feng, Faridi Qaium, Haiyan Lei, David Roberts, Michele Landeau, Jamie Bell, Yi Huang, Leah Hoffman, Melissa Spencer, Matthew B Spraker, Li Ding, Brigitte C Widemann, Jack F Shern, Angela C Hirbe, and Aadel A Chaudhuri

Subjects

Medicine

Abstract

BackgroundThe leading cause of mortality for patients with the neurofibromatosis type 1 (NF1) cancer predisposition syndrome is the development of malignant peripheral nerve sheath tumor (MPNST), an aggressive soft tissue sarcoma. In the setting of NF1, this cancer type frequently arises from within its common and benign precursor, plexiform neurofibroma (PN). Transformation from PN to MPNST is challenging to diagnose due to difficulties in distinguishing cross-sectional imaging results and intralesional heterogeneity resulting in biopsy sampling errors.Methods and findingsThis multi-institutional study from the National Cancer Institute and Washington University in St. Louis used fragment size analysis and ultra-low-pass whole genome sequencing (ULP-WGS) of plasma cell-free DNA (cfDNA) to distinguish between MPNST and PN in patients with NF1. Following in silico enrichment for short cfDNA fragments and copy number analysis to estimate the fraction of plasma cfDNA originating from tumor (tumor fraction), we developed a noninvasive classifier that differentiates MPNST from PN with 86% pretreatment accuracy (91% specificity, 75% sensitivity) and 89% accuracy on serial analysis (91% specificity, 83% sensitivity). Healthy controls without NF1 (participants = 16, plasma samples = 16), PN (participants = 23, plasma samples = 23), and MPNST (participants = 14, plasma samples = 46) cohorts showed significant differences in tumor fraction in plasma (P = 0.001) as well as cfDNA fragment length (P < 0.001) with MPNST samples harboring shorter fragments and being enriched for tumor-derived cfDNA relative to PN and healthy controls. No other covariates were significant on multivariate logistic regression. Mutational analysis demonstrated focal NF1 copy number loss in PN and MPNST patient plasma but not in healthy controls. Greater genomic instability including alterations associated with malignant transformation (focal copy number gains in chromosome arms 1q, 7p, 8q, 9q, and 17q; focal copy number losses in SUZ12, SMARCA2, CDKN2A/B, and chromosome arms 6p and 9p) was more prominently observed in MPNST plasma. Furthermore, the sum of longest tumor diameters (SLD) visualized by cross-sectional imaging correlated significantly with paired tumor fractions in plasma from MPNST patients (r = 0.39, P = 0.024). On serial analysis, tumor fraction levels in plasma dynamically correlated with treatment response to therapy and minimal residual disease (MRD) detection before relapse. Study limitations include a modest MPNST sample size despite accrual from 2 major referral centers for this rare malignancy, and lack of uniform treatment and imaging protocols representing a real-world cohort.ConclusionsTumor fraction levels derived from cfDNA fragment size and copy number alteration analysis of plasma cfDNA using ULP-WGS significantly correlated with MPNST tumor burden, accurately distinguished MPNST from its benign PN precursor, and dynamically correlated with treatment response. In the future, our findings could form the basis for improved early cancer detection and monitoring in high-risk cancer-predisposed populations.

Published

2021

34. Diagnostic approach to the evaluation of myeloid malignancies following CAR T-cell therapy in B-cell acute lymphoblastic leukemia

Author

Aimee C Talleur, Brandon M Triplett, Haneen Shalabi, Bonnie Yates, Nirali N Shah, George Mo, Hao-Wei Wang, Shilpa A Shahani, Michael G Douvas, Katherine R Calvo, Jack F Shern, Sridhar Chaganti, Katharine Patrick, Young Song, Terry J Fry, Xiaolin Wu, Javed Khan, and Rebecca A Gardner

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Immunotherapeutic strategies targeting B-cell acute lymphoblastic leukemia (B-ALL) effectively induce remission; however, disease recurrence remains a challenge. Due to the potential for antigen loss, antigen diminution, lineage switch or development of a secondary or treatment-related malignancy, the phenotype and manifestation of subsequent leukemia may be elusive. We report on two patients with multiply relapsed/refractory B-ALL who, following chimeric antigen receptor T-cell therapy, developed myeloid malignancies. In the first case, a myeloid sarcoma developed in a patient with a history of myelodysplastic syndrome. In the second case, two distinct events occurred. The first event represented a donor-derived myelodysplastic syndrome with monosomy 7 in a patient with a prior hematopoietic stem cell transplantation. This patient went on to present with lineage switch of her original B-ALL to ambiguous lineage T/myeloid acute leukemia. With the rapidly evolving field of novel immunotherapeutic strategies, evaluation of relapse and/or subsequent neoplasms is becoming increasingly more complex. By virtue of these uniquely complex cases, we provide a framework for the evaluation of relapse or evolution of a subsequent malignancy following antigen-targeted immunotherapy.

Published

2020

35. Hepatocyte Growth Factor-mediated satellite cells niche perturbation promotes development of distinct sarcoma subtypes

Author

Deborah Morena, Nicola Maestro, Francesca Bersani, Paolo Emanuele Forni, Marcello Francesco Lingua, Valentina Foglizzo, Petar Šćepanović, Silvia Miretti, Alessandro Morotti, Jack F Shern, Javed Khan, Ugo Ala, Paolo Provero, Valentina Sala, Tiziana Crepaldi, Patrizia Gasparini, Michela Casanova, Andrea Ferrari, Gabriella Sozzi, Roberto Chiarle, Carola Ponzetto, and Riccardo Taulli

Subjects

stem cell niche, HGF/met axis, embryonal rhabdomyosarcoma, undifferentiated pleomorphic sarcoma, clonal evolution, combination therapy, Medicine, Science, Biology (General), QH301-705.5

Abstract

Embryonal Rhabdomyosarcoma (ERMS) and Undifferentiated Pleomorphic Sarcoma (UPS) are distinct sarcoma subtypes. Here we investigate the relevance of the satellite cell (SC) niche in sarcoma development by using Hepatocyte Growth Factor (HGF) to perturb the niche microenvironment. In a Pax7 wild type background, HGF stimulation mainly causes ERMS that originate from satellite cells following a process of multistep progression. Conversely, in a Pax7 null genotype ERMS incidence drops, while UPS becomes the most frequent subtype. Murine EfRMS display genetic heterogeneity similar to their human counterpart. Altogether, our data demonstrate that selective perturbation of the SC niche results in distinct sarcoma subtypes in a Pax7 lineage-dependent manner, and define a critical role for the Met axis in sarcoma initiation. Finally, our results provide a rationale for the use of combination therapy, tailored on specific amplifications and activated signaling pathways, to minimize resistance emerging from sarcomas heterogeneity.

Published

2016

36. Clonality and evolutionary history of rhabdomyosarcoma.

Author

Li Chen, Jack F Shern, Jun S Wei, Marielle E Yohe, Young K Song, Laura Hurd, Hongling Liao, Daniel Catchpoole, Stephen X Skapek, Frederic G Barr, Douglas S Hawkins, and Javed Khan

Subjects

Genetics, QH426-470

Abstract

To infer the subclonality of rhabdomyosarcoma (RMS) and predict the temporal order of genetic events for the tumorigenic process, and to identify novel drivers, we applied a systematic method that takes into account germline and somatic alterations in 44 tumor-normal RMS pairs using deep whole-genome sequencing. Intriguingly, we find that loss of heterozygosity of 11p15.5 and mutations in RAS pathway genes occur early in the evolutionary history of the PAX-fusion-negative-RMS (PFN-RMS) subtype. We discover several early mutations in non-RAS mutated samples and predict them to be drivers in PFN-RMS including recurrent mutation of PKN1. In contrast, we find that PAX-fusion-positive (PFP) subtype tumors have undergone whole-genome duplication in the late stage of cancer evolutionary history and have acquired fewer mutations and subclones than PFN-RMS. Moreover we predict that the PAX3-FOXO1 fusion event occurs earlier than the whole genome duplication. Our findings provide information critical to the understanding of tumorigenesis of RMS.

Published

2015

37. The genomic landscape of the Ewing Sarcoma family of tumors reveals recurrent STAG2 mutation.

Author

Andrew S Brohl, David A Solomon, Wendy Chang, Jianjun Wang, Young Song, Sivasish Sindiri, Rajesh Patidar, Laura Hurd, Li Chen, Jack F Shern, Hongling Liao, Xinyu Wen, Julia Gerard, Jung-Sik Kim, Jose Antonio Lopez Guerrero, Isidro Machado, Daniel H Wai, Piero Picci, Timothy Triche, Andrew E Horvai, Markku Miettinen, Jun S Wei, Daniel Catchpool, Antonio Llombart-Bosch, Todd Waldman, and Javed Khan

Subjects

Genetics, QH426-470

Abstract

The Ewing sarcoma family of tumors (EFT) is a group of highly malignant small round blue cell tumors occurring in children and young adults. We report here the largest genomic survey to date of 101 EFT (65 tumors and 36 cell lines). Using a combination of whole genome sequencing and targeted sequencing approaches, we discover that EFT has a very low mutational burden (0.15 mutations/Mb) but frequent deleterious mutations in the cohesin complex subunit STAG2 (21.5% tumors, 44.4% cell lines), homozygous deletion of CDKN2A (13.8% and 50%) and mutations of TP53 (6.2% and 71.9%). We additionally note an increased prevalence of the BRCA2 K3326X polymorphism in EFT patient samples (7.3%) compared to population data (OR 7.1, p = 0.006). Using whole transcriptome sequencing, we find that 11% of tumors pathologically diagnosed as EFT lack a typical EWSR1 fusion oncogene and that these tumors do not have a characteristic Ewing sarcoma gene expression signature. We identify samples harboring novel fusion genes including FUS-NCATc2 and CIC-FOXO4 that may represent distinct small round blue cell tumor variants. In an independent EFT tissue microarray cohort, we show that STAG2 loss as detected by immunohistochemistry may be associated with more advanced disease (p = 0.15) and a modest decrease in overall survival (p = 0.10). These results significantly advance our understanding of the genomic and molecular underpinnings of Ewing sarcoma and provide a foundation towards further efforts to improve diagnosis, prognosis, and precision therapeutics testing.

Published

2014

38. Targeting wild-type and mutationally activated FGFR4 in rhabdomyosarcoma with the inhibitor ponatinib (AP24534).

Author

Samuel Q Li, Adam T Cheuk, Jack F Shern, Young K Song, Laura Hurd, Hongling Liao, Jun S Wei, and Javed Khan

Subjects

Medicine, Science

Abstract

Rhabdomyosarcoma (RMS) is the most common childhood soft tissue sarcoma. Despite advances in modern therapy, patients with relapsed or metastatic disease have a very poor clinical prognosis. Fibroblast Growth Factor Receptor 4 (FGFR4) is a cell surface tyrosine kinase receptor that is involved in normal myogenesis and muscle regeneration, but not commonly expressed in differentiated muscle tissues. Amplification and mutational activation of FGFR4 has been reported in RMS and promotes tumor progression. Therefore, FGFR4 is a tractable therapeutic target for patients with RMS. In this study, we used a chimeric Ba/F3 TEL-FGFR4 construct to test five tyrosine kinase inhibitors reported to specifically inhibit FGFRs in the nanomolar range. We found ponatinib (AP24534) to be the most potent FGFR4 inhibitor with an IC50 in the nanomolar range. Ponatinib inhibited the growth of RMS cells expressing wild-type or mutated FGFR4 through increased apoptosis. Phosphorylation of wild-type and mutated FGFR4 as well as its downstream target STAT3 was also suppressed by ponatinib. Finally, ponatinib treatment inhibited tumor growth in a RMS mouse model expressing mutated FGFR4. Therefore, our data suggests that ponatinib is a potentially effective therapeutic agent for RMS tumors that are driven by a dysregulated FGFR4 signaling pathway.

Published

2013