Your search keyword '"Ling-Wen Ding"' showing total 33 results

1. Targeting RNA Exonuclease XRN1 Potentiates Efficacy of Cancer Immunotherapy

Author

Xue-Bin Ran, Ling-Wen Ding, Qiao-Yang Sun, Henry Yang, Jonathan W. Said, Lao Zhentang, Vikas Madan, Pushkar Dakle, Jin-Fen Xiao, Xinyi Loh, Ying Li, Liang Xu, Xiao-Qiang Xiang, Ling-Zhi Wang, Boon Cher Goh, De-Chen Lin, Wee Joo Chng, Soo-Yong Tan, Sudhakar Jha, and H. Phillip Koeffler

Subjects

Cancer Research, Oncology

Abstract

Despite the remarkable clinical responses achieved with immune checkpoint blockade therapy, the response rate is relatively low and only a subset of patients can benefit from the treatment. Aberrant RNA accumulation can mediate IFN signaling and stimulate an immune response, suggesting that targeting RNA decay machinery might sensitize tumor cells to immunotherapy. With this in mind, we identified an RNA exoribonuclease, XRN1, as a potential therapeutic target to suppress RNA decay and stimulate antitumor immunity. Silencing of XRN1 suppressed tumor growth in syngeneic immunocompetent mice and potentiated immunotherapy efficacy, while silencing of XRN1 alone did not affect tumor growth in immunodeficient mice. Mechanistically, XRN1 depletion activated IFN signaling and the viral defense pathway; both pathways play determinant roles in regulating immune evasion. Aberrant RNA-sensing signaling proteins (RIG-I/MAVS) mediated the expression of IFN genes, as depletion of each of them blunted the elevation of antiviral/IFN signaling in XRN1-silenced cells. Analysis of pan-cancer CRISPR-screening data indicated that IFN signaling triggered by XRN1 silencing is a common phenomenon, suggesting that the effect of XRN1 silencing may be extended to multiple types of cancers. Overall, XRN1 depletion triggers aberrant RNA-mediated IFN signaling, highlighting the importance of the aberrant RNA-sensing pathway in regulating immune responses. These findings provide the molecular rationale for developing XRN1 inhibitors and exploring their potential clinical application in combination with cancer immunotherapy.Significance:Targeting XRN1 activates an intracellular innate immune response mediated by RNA-sensing signaling and potentiates cancer immunotherapy efficacy, suggesting inhibition of RNA decay machinery as a novel strategy for cancer treatment.

Published

2023

2. KDM6A Depletion in Breast Epithelial Cells Leads to Reduced Sensitivity to Anticancer Agents and Increased TGFβ Activity

Author

Jin-Fen Xiao, Ley-Fang Kua, Ling-Wen Ding, Qiao-Yang Sun, Khine Nyein Myint, Xiu-Rong Chia, Nachiyappan Venkatachalam, Xinyi Loh, Jason E. Duex, Vanessa Neang, Siqin Zhou, Ying Li, Henry Yang, H. Phillip Koeffler, and Dan Theodorescu

Subjects

Histone Demethylases, Cancer Research, Urinary Bladder Neoplasms, Oncology, Transforming Growth Factor beta, Humans, Antineoplastic Agents, Breast Neoplasms, Epithelial Cells, Female, Molecular Biology, Article

Abstract

KDM6A, an X chromosome-linked histone lysine demethylase, was reported to be frequently mutated in many tumor types including breast and bladder cancer. However, the functional role of KDM6A is not fully understood. Using MCF10A as a model of non-tumorigenic epithelial breast cells, we found that silencing KDM6A promoted cell migration and transformation demonstrated by the formation of tumor-like acini in three-dimensional culture. KDM6A loss reduced the sensitivity of MCF10A cells to therapeutic agents commonly used to treat patients with triple-negative breast cancer and also induced TGFβ extracellular secretion leading to suppressed expression of cytotoxic genes in normal human CD8+ T cells in vitro. Interestingly, when cells were treated with TGFβ, de novo synthesis of KDM6A protein was suppressed while TGFB1 transcription was enhanced, indicating a TGFβ/KDM6A-negative regulatory axis. Furthermore, both KDM6A deficiency and TGFβ treatment promoted disorganized acinar structures in three-dimensional culture, as well as transcriptional profiles associated with epithelial-to-mesenchymal transition and metastasis, suggesting KDM6A depletion and TGFβ drive tumor progression. Implications: Our study provides the preclinical rationale for evaluating KDM6A and TGFβ in breast tumor samples as predictors for response to chemo and immunotherapy, informing personalized therapy based on these findings.

Published

2022

3. Celastrol in cancer therapy: Recent developments, challenges and prospects

Author

Andrea Li Ann Wong, Arul Goel, Gautam Sethi, Lingzhi Wang, Xiaoqiang Xiang, Paul C. Ho, Pei Shi Ong, Ling-Wen Ding, Boon Cher Goh, and Hannah Ying Lim

Subjects

Drug, Cancer Research, business.industry, media_common.quotation_subject, Druggability, Cancer therapy, Cancer, Bioinformatics, medicine.disease, Safety profile, chemistry.chemical_compound, Drug class, Oncology, chemistry, Celastrol, Medicine, Oncology patients, business, media_common

Abstract

Cancer is one of the world's biggest healthcare burdens and despite the current advancements made in treatment plans, the outcomes for oncology patients have yet to reach their full potential. Hence, there is a pressing need to develop novel anti-cancer drugs. A popular drug class for research are natural compounds, due to their multi-targeting potential and enhanced safety profile. One such promising natural bioactive compound derived from a vine, Tripterygium wilfordii is celastrol. Pre-clinical studies revolving around the use of celastrol have revealed positive pharmacological activities in various types of cancers, thus suggesting the chemical's potential anti-cancerous effects. However, despite the numerous preclinical studies carried out over the past few decades, celastrol has not reached human trials for cancer. In this review, we summarize the mechanisms and therapeutic potentials of celastrol in treatment for different types of cancer. Subsequently, we also explore the possible reasons hindering its development for human use as cancer therapy, like its narrow therapeutic window and poor pharmacokinetic properties. Additionally, after critically analysing both in vitro and in vivo evidence, we discuss about the key pathways effected by celastrol and the suitable types of cancer that can be targeted by the natural drug, thus giving insight into future directions that can be taken, such as in-depth analysis and research of the druggability of celastrol derivatives, to aid the clinical translation of this promising anti-cancer lead compound.

Published

2021

4. RNA-Binding Protein ZFP36L1 Suppresses Hypoxia and Cell-Cycle Signaling

Author

Pushkar Dakle, Ruby Yun-Ju Huang, Anand Mayakonda, H. Phillip Koeffler, Qiao-Yang Sun, De-Chen Lin, Xue-Bin Ran, Siqin Zhou, Henry Yang, Ling-Wen Ding, Mei-Shi Yeo, Tiago C. Silva, Soo Yong Tan, Ngan B. Doan, Nachiyappan Venkatachalam, Pavithra Shyamsunder, Angele Pei-Fern Koh, Jin-Fen Xiao, Jonathan W. Said, Xin-Yi Loh, and Benjamin P. Berman

Subjects

0301 basic medicine, Regulation of gene expression, Untranslated region, Cancer Research, Messenger RNA, Chemistry, RNA, RNA-binding protein, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, HIF1A, Oncology, 030220 oncology & carcinogenesis, Gene silencing, E2F1

Abstract

ZFP36L1 is a tandem zinc-finger RNA-binding protein that recognizes conserved adenylate-uridylate–rich elements (ARE) located in 3′untranslated regions (UTR) to mediate mRNA decay. We hypothesized that ZFP36L1 is a negative regulator of a posttranscriptional hub involved in mRNA half-life regulation of cancer-related transcripts. Analysis of in silico data revealed that ZFP36L1 was significantly mutated, epigenetically silenced, and downregulated in a variety of cancers. Forced expression of ZFP36L1 in cancer cells markedly reduced cell proliferation in vitro and in vivo, whereas silencing of ZFP36L1 enhanced tumor cell growth. To identify direct downstream targets of ZFP36L1, systematic screening using RNA pull-down of wild-type and mutant ZFP36L1 as well as whole transcriptome sequencing of bladder cancer cells {plus minus} tet-on ZFP36L1 was performed. A network of 1,410 genes was identified as potential direct targets of ZFP36L1. These targets included a number of key oncogenic transcripts such as HIF1A, CCND1, and E2F1. ZFP36L1 specifically bound to the 3′UTRs of these targets for mRNA degradation, thus suppressing their expression. Dual luciferase reporter assays and RNA electrophoretic mobility shift assays showed that wild-type, but not zinc-finger mutant ZFP36L1, bound to HIF1A 3′UTR and mediated HIF1A mRNA degradation, leading to reduced expression of HIF1A and its downstream targets. Collectively, our findings reveal an indispensable role of ZFP36L1 as a posttranscriptional safeguard against aberrant hypoxic signaling and abnormal cell-cycle progression. Significance: RNA-binding protein ZFP36L1 functions as a tumor suppressor by regulating the mRNA stability of a number of mRNAs involved in hypoxia and cell-cycle signaling.

Published

2020

5. Resveratrol for cancer therapy: Challenges and future perspectives

Author

Boxu Ren, Zhaowu Ma, Ling-Wen Ding, Paul C. Ho, Xiaoqiang Xiang, Marabeth Xin-Yi Kwah, Lingzhi Wang, Muthu K. Shanmugam, Cuiliu Liu, Pei Shi Ong, and Boon Cher Goh

Subjects

0301 basic medicine, Cancer Research, endocrine system diseases, Cancer therapy, Translational research, Antineoplastic Agents, Resveratrol, Bioinformatics, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Neoplasms, medicine, Animals, Humans, skin and connective tissue diseases, business.industry, organic chemicals, food and beverages, Cancer, medicine.disease, Anticancer drug, Bench to bedside, Cancer treatment, Clinical trial, 030104 developmental biology, Oncology, chemistry, 030220 oncology & carcinogenesis, business, hormones, hormone substitutes, and hormone antagonists, Signal Transduction

Abstract

Resveratrol (3,4',5-trihydroxy-trans-stilbene) has been expected to ameliorate cancer and foster breakthroughs in cancer therapy. Despite thousands of preclinical studies on the anticancer activity of resveratrol, little progress has been made in translational research and clinical trials. Most studies have focused on its anticancer effects, cellular mechanisms, and signal transduction pathways in vitro and in vivo. In this review, we aimed to discern the causes that prevent resveratrol from being used in cancer treatment. Among the various limitations, poor pharmacokinetics and low potency seem to be the two main bottlenecks of resveratrol. In addition, resveratrol-induced nephrotoxicity in multiple myeloma patients hinders its further development as an anticancer drug. New insights and strategies have been proposed to accelerate the conversion of resveratrol from bench to bedside. In the interim, the most promising approach is to enhance the bioavailability of resveratrol with new formulations. Alternatively, more potent analogues of resveratrol could be developed to augment its anticancer potency. Given all the gaps mentioned, much work remains to be done. However, if remarkable progress can be made, resveratrol may finally be used for cancer therapy.

Published

2021

6. A Transcriptional Regulatory Loop of Master Regulator Transcription Factors, PPARG, and Fatty Acid Synthesis Promotes Esophageal Adenocarcinoma

Author

De-Chen Lin, Qian Yang, Michael R. Freeman, Joshua J. Breunig, H. Phillip Koeffler, Stephen J. Freedland, Yunzhi Pan, Wei Yang, Bo Zhou, Ling-Wen Ding, Jian Pan, Sai Ma, and Neil A. Bhowmick

Subjects

0301 basic medicine, Male, Cancer Research, Peroxisome proliferator-activated receptor gamma, endocrine system diseases, Esophageal Neoplasms, Cell Survival, Pyridines, Kruppel-Like Transcription Factors, Mice, Nude, Biology, Adenocarcinoma, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Downregulation and upregulation, Cell Line, Tumor, GATA6 Transcription Factor, Animals, Humans, Enhancer, Promoter Regions, Genetic, Transcription factor, Fatty acid synthesis, Regulation of gene expression, GATA6, Proto-Oncogene Proteins c-ets, Fatty Acids, nutritional and metabolic diseases, Xenograft Model Antitumor Assays, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, PPAR gamma, 030104 developmental biology, Enhancer Elements, Genetic, Oncology, Nuclear receptor, chemistry, 030220 oncology & carcinogenesis, Benzamides, Cancer research, Transcription Factors

Abstract

Although obesity is one of the strongest risk factors for esophageal adenocarcinoma, the molecular mechanisms underlying this association remain unclear. We recently identified four esophageal adenocarcinoma–specific master regulator transcription factors (MRTF) ELF3, KLF5, GATA6, and EHF. In this study, gene-set enrichment analysis of both esophageal adenocarcinoma patient samples and cell line models unbiasedly underscores fatty acid synthesis as the central pathway downstream of three MRTFs (ELF3, KLF5, GATA6). Further characterizations unexpectedly identified a transcriptional feedback loop between MRTF and fatty acid synthesis, which mutually activated each other through the nuclear receptor, PPARG. MRTFs cooperatively promoted PPARG transcription by directly regulating its promoter and a distal esophageal adenocarcinoma–specific enhancer, leading to PPARG overexpression in esophageal adenocarcinoma. PPARG was also elevated in Barrett’s esophagus, a recognized precursor to esophageal adenocarcinoma, implying that PPARG might play a role in the intestinal metaplasia of esophageal squamous epithelium. Upregulation of PPARG increased de novo synthesis of fatty acids, phospholipids, and sphingolipids as revealed by mass spectrometry–based lipidomics. Moreover, ChIP-seq, 4C-seq, and a high-fat diet murine model together characterized a novel, noncanonical, and cancer-specific function of PPARG in esophageal adenocarcinoma. PPARG directly regulated the ELF3 super-enhancer, subsequently activating the transcription of other MRTFs through an interconnected regulatory circuitry. Together, elucidation of this novel transcriptional feedback loop of MRTF/PPARG/fatty acid synthesis advances our understanding of the mechanistic foundation for epigenomic dysregulation and metabolic alterations in esophageal adenocarcinoma. More importantly, this work identifies a potential avenue for prevention and early intervention of esophageal adenocarcinoma by blocking this feedback loop. Significance: These findings elucidate a transcriptional feedback loop linking epigenomic dysregulation and metabolic alterations in esophageal adenocarcinoma, indicating that blocking this feedback loop could be a potential therapeutic strategy in high-risk individuals.

Published

2020

7. Lineage-Specific Epigenomic and Genomic Activation of Oncogene HNF4A Promotes Gastrointestinal Adenocarcinomas

Author

Li-Yan Xu, Tiago C. Silva, Yanbing Ding, De-Chen Lin, Qian Yang, Jian Pan, Sigal Gery, Ling-Wen Ding, Benjamin P. Berman, Shao-Yan Hu, Samuel J. Klempner, Simon A. Gayther, Jasmine T. Plummer, Takao Hamakubo, Yan-Yi Jiang, H. Phillip Koeffler, En-Min Li, Stephanie S. Chen, Nicole Gull, and Kenji Daigo

Subjects

0301 basic medicine, Epigenomics, Male, endocrine system, Cancer Research, Gene regulatory network, Mice, Nude, Apoptosis, Computational biology, Biology, Adenocarcinoma, Transcriptome, 03 medical and health sciences, Mice, 0302 clinical medicine, Biomarkers, Tumor, Tumor Cells, Cultured, Animals, Humans, Gene Regulatory Networks, Enhancer, Promoter Regions, Genetic, Transcription factor, Cell Proliferation, Gastrointestinal Neoplasms, Regulation of gene expression, Mice, Inbred BALB C, GATA6, Genomics, Prognosis, Xenograft Model Antitumor Assays, Gene Expression Regulation, Neoplastic, Survival Rate, 030104 developmental biology, Oncology, Hepatocyte Nuclear Factor 4, 030220 oncology & carcinogenesis, DNA methylation, Transcription Factors

Abstract

Gastrointestinal adenocarcinomas (GIAC) of the tubular gastrointestinal (GI) tract including esophagus, stomach, colon, and rectum comprise most GI cancers and share a spectrum of genomic features. However, the unified epigenomic changes specific to GIAC are poorly characterized. Using 907 GIAC samples from The Cancer Genome Atlas, we applied mathematical algorithms to large-scale DNA methylome and transcriptome profiles to reconstruct transcription factor (TF) networks and identify a list of functionally hyperactive master regulator (MR) TF shared across different GIAC. The top candidate HNF4A exhibited prominent genomic and epigenomic activation in a GIAC-specific manner. A complex interplay between the HNF4A promoter and three distal enhancer elements was coordinated by GIAC-specific MRTF including ELF3, GATA4, GATA6, and KLF5. HNF4A also self-regulated its own promoter and enhancers. Functionally, HNF4A promoted cancer proliferation and survival by transcriptional activation of many downstream targets, including HNF1A and factors of interleukin signaling, in a lineage-specific manner. Overall, our study provides new insights into the GIAC-specific gene regulatory networks and identifies potential therapeutic strategies against these common cancers. Significance: These findings show that GIAC-specific master regulatory transcription factors control HNF4A via three distal enhancers to promote GIAC cell proliferation and survival.

Published

2020

8. Super-Enhancers Promote Transcriptional Dysregulation in Nasopharyngeal Carcinoma

Author

Marilynn Chow, Anand Mayakonda, Yanan Lu, Jeffrey W. Tyner, Jiang Yuan, Fenggang Yu, Moli Huang, T. Loh, De-Chen Lin, Yan-Yi Jiang, Ling-Wen Ding, H. Phillip Koeffler, Han Lin, and Samantha L. Savage

Subjects

0301 basic medicine, Cancer Research, Transcription, Genetic, Mice, SCID, Phenylenediamines, Mice, Mice, Inbred NOD, 2.1 Biological and endogenous factors, Aetiology, TEAD1, Cancer, Genetics, Regulation of gene expression, Tumor, Nasopharyngeal Carcinoma, Cyclin-Dependent Kinases, Long non-coding RNA, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Oncology, Long Noncoding, RNA, Long Noncoding, Transcription, Biotechnology, Chromatin Immunoprecipitation, Oncology and Carcinogenesis, Antineoplastic Agents, Biology, SCID, Article, Cell Line, Proto-Oncogene Protein c-ets-2, 03 medical and health sciences, Genetic, Cyclin-dependent kinase, Cell Line, Tumor, medicine, Animals, Humans, Oncology & Carcinogenesis, Epigenetics, Transcription factor, Neoplastic, Human Genome, Carcinoma, Nasopharyngeal Neoplasms, medicine.disease, Xenograft Model Antitumor Assays, HEK293 Cells, Pyrimidines, 030104 developmental biology, Gene Expression Regulation, Nasopharyngeal carcinoma, Cancer research, biology.protein, Inbred NOD, RNA, Chromatin immunoprecipitation, Cyclin-Dependent Kinase-Activating Kinase

Abstract

Nasopharyngeal carcinoma (NPC) is an invasive cancer with particularly high incidence in Southeast Asia and Southern China. The pathogenic mechanisms of NPC, particularly those involving epigenetic dysregulation, remain largely elusive, hampering clinical management of this malignancy. To identify novel druggable targets, we carried out an unbiased high-throughput chemical screening and observed that NPC cells were highly sensitive to inhibitors of cyclin-dependent kinases (CDK), especially THZ1, a covalent inhibitor of CDK7. THZ1 demonstrated pronounced antineoplastic activities both in vitro and in vivo. An integrative analysis using both whole-transcriptome sequencing and chromatin immunoprecipitation sequencing pinpointed oncogenic transcriptional amplification mediated by super-enhancers (SE) as a key mechanism underlying the vulnerability of NPC cells to THZ1 treatment. Further characterization of SE-mediated networks identified many novel SE-associated oncogenic transcripts, such as BCAR1, F3, LDLR, TBC1D2, and the long noncoding RNA TP53TG1. These transcripts were highly and specifically expressed in NPC and functionally promoted NPC malignant phenotypes. Moreover, DNA-binding motif analysis within the SE segments suggest that several transcription factors (including ETS2, MAFK, and TEAD1) may help establish and maintain SE activity across the genome. Taken together, our data establish the landscape of SE-associated oncogenic transcriptional network in NPC, which can be exploited for the development of more effective therapeutic regimens for this disease. Cancer Res; 77(23); 6614–26. ©2017 AACR.

Published

2017

9. Ordering of mutations in acute myeloid leukemia with partial tandem duplication of MLL (MLL-PTD)

Author

Kar Tong Tan, Manoj Garg, Xin-Yi Loh, Satoru Miyano, H P Koeffler, Akitoshi Kinoshita, Yasunobu Nagata, Norimichi Hattori, Wenwen Chien, Qiao-Yang Sun, Y. Y. Jiang, Hagop M. Kantarjian, Michael Lill, Siew Zhuan Tan, De-Chen Lin, Tamara Alpermann, Anand Mayakonda, Li Zhen Liu, T Haferlach, Su Lin Lim, Allen Eng Juh Yeoh, Manja Meggendorfer, Mutsumi Hayashi, Steve Kornblau, Vikas Madan, Hsin-An Hou, Henry Yang, Seishi Ogawa, Ling-Wen Ding, Sumiko Takao, and Jin-Fen Xiao

Subjects

0301 basic medicine, Myeloid, Cancer Research, Mutation rate, NPM1, Time Factors, Cohesin complex, Pediatric Cancer, Childhood Leukemia, Clinical Sciences, Oncology and Carcinogenesis, Immunology, Biology, Acute, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Rare Diseases, Mutation Rate, hemic and lymphatic diseases, medicine, Genetics, 2.1 Biological and endogenous factors, Humans, Exome, Aetiology, neoplasms, Cancer, Cell Proliferation, Pediatric, Mutation, Leukemia, Myeloid leukemia, Hematology, Histone-Lysine N-Methyltransferase, Clone Cells, Leukemia, Myeloid, Acute, 030104 developmental biology, Oncology, Tandem Repeat Sequences, 030220 oncology & carcinogenesis, Myeloid-Lymphoid Leukemia Protein, Original Article, Tandem exon duplication, Nucleophosmin

Abstract

Partial tandem duplication of MLL (MLL-PTD) characterizes acute myeloid leukemia (AML) patients often with a poor prognosis. To understand the order of occurrence of MLL-PTD in relation to other major AML mutations and to identify novel mutations that may be present in this unique AML molecular subtype, exome and targeted sequencing was performed on 85 MLL-PTD AML samples using HiSeq-2000. Genes involved in the cohesin complex (STAG2), a splicing factor (U2AF1) and a poorly studied gene, MGA were recurrently mutated, whereas NPM1, one of the most frequently mutated AML gene, was not mutated in MLL-PTD patients. Interestingly, clonality analysis suggests that IDH2/1, DNMT3A, U2AF1 and TET2 mutations are clonal and occur early, and MLL-PTD likely arises after these initial mutations. Conversely, proliferative mutations (FLT3, RAS), typically appear later, are largely subclonal and tend to be unstable. This study provides important insights for understanding the relative importance of different mutations for defining a targeted therapeutic strategy for MLL-PTD AML patients.

Published

2016

10. Comprehensive mutational analysis of primary and relapse acute promyelocytic leukemia

Author

Michael Heuser, Manoj Garg, T Haferlach, L. Z. Liu, Shih Ly, Yuichi Shiraishi, Takayuki Ikezoe, Michael Lill, Hwei-Fang Tien, Henry Yang, Ling-Wen Ding, Hagop M. Kantarjian, H P Koeffler, T. Ma, Yasunobu Nagata, Wolf-K. Hofmann, Qiao-Yang Sun, Satoru Miyano, Richard A. Larson, Noreen Fulton, Seishi Ogawa, Pavithra Shyamsunder, Masashi Sanada, Kamran Alimoghaddam, W. J. Chng, Norimichi Hattori, Saravanan Ganesan, Wendy Stock, Tamara Alpermann, S. Rostami, Ezhilarasi Chendamarai, Vikram Mathews, Kenichi Yoshida, Anand Mayakonda, Steve Kornblau, M. C. Kuo, Gregory Malnassy, Vikas Madan, Lin Han, A. Ghavamzadeh, Hsin-An Hou, Andrea Biondi, Bayard L. Powell, W. Chien, Jairo Matthews, Janani Sundaresan, Michael Lübbert, Daniel Nowak, Deepika Kanojia, Arnold Ganser, Kar Tong Tan, Maya Koren-Michowitz, Madan, V, Shyamsunder, P, Han, L, Mayakonda, A, Nagata, Y, Sundaresan, J, Kanojia, D, Yoshida, K, Ganesan, S, Hattori, N, Fulton, N, Tan, K, Alpermann, T, Kuo, M, Rostami, S, Matthews, J, Sanada, M, Liu, L, Shiraishi, Y, Miyano, S, Chendamarai, E, Hou, H, Malnassy, G, Ma, T, Garg, M, Ding, L, Sun, Q, Chien, W, Ikezoe, T, Lill, M, Biondi, A, Larson, R, Powell, B, Lubbert, M, Chng, W, Tien, H, Heuser, M, Ganser, A, Koren-Michowitz, M, Kornblau, S, Kantarjian, H, Nowak, D, Hofmann, W, Yang, H, Stock, W, Ghavamzadeh, A, Alimoghaddam, K, Haferlach, T, Ogawa, S, Shih, L, Mathews, V, and Koeffler, H

Subjects

0301 basic medicine, Neuroblastoma RAS viral oncogene homolog, Acute promyelocytic leukemia, Cancer Research, ARID1A, DNA-Binding Protein, DNA Mutational Analysis, Clinical Sciences, Oncology and Carcinogenesis, Immunology, Acute, Biology, DNA Mutational Analysi, Fusion gene, 03 medical and health sciences, 0302 clinical medicine, Leukemia, Promyelocytic, Acute, Recurrence, immune system diseases, medicine, Humans, Exome, neoplasms, Nuclear Protein, Promyelocytic, Genetics, Leukemia, Gene Expression Profiling, Nuclear Proteins, Myeloid leukemia, Cell Differentiation, Hematology, medicine.disease, DNA-Binding Proteins, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Original Article, Human, Transcription Factors

Abstract

Acute promyelocytic leukemia (APL) is a subtype of myeloid leukemia characterized by differentiation block at the promyelocyte stage. Besides the presence of chromosomal rearrangement t(15;17), leading to the formation of PML-RARA (promyelocytic leukemia-retinoic acid receptor alpha) fusion, other genetic alterations have also been implicated in APL. Here, we performed comprehensive mutational analysis of primary and relapse APL to identify somatic alterations, which cooperate with PML-RARA in the pathogenesis of APL. We explored the mutational landscape using whole-exome (n=12) and subsequent targeted sequencing of 398 genes in 153 primary and 69 relapse APL. Both primary and relapse APL harbored an average of eight non-silent somatic mutations per exome. We observed recurrent alterations of FLT3, WT1, NRAS and KRAS in the newly diagnosed APL, whereas mutations in other genes commonly mutated in myeloid leukemia were rarely detected. The molecular signature of APL relapse was characterized by emergence of frequent mutations in PML and RARA genes. Our sequencing data also demonstrates incidence of loss-of-function mutations in previously unidentified genes, ARID1B and ARID1A, both of which encode for key components of the SWI/SNF complex. We show that knockdown of ARID1B in APL cell line, NB4, results in large-scale activation of gene expression and reduced in vitro differentiation potential.

Published

2016

11. Profiling the B/T cell receptor repertoire of lymphocyte derived cell lines

Author

Zhentang Lao, Xin-Yi Loh, H. Phillip Koeffler, Henry Yang, Ling-Wen Ding, Liang Xu, Michael Lill, Wenwen Chien, De-Chen Lin, Anand Mayakonda, Xi Ren, Jin-Fen Xiao, Qiao-Yang Sun, and Kar Tong Tan

Subjects

0301 basic medicine, Cancer Research, Herpesvirus 4, Human, Lymphoma, Lymphocyte, Cancer cell lines, Somatic evolution in cancer, Neoplasms, Receptors, 2.1 Biological and endogenous factors, Lymphocytes, Aetiology, Cancer, education.field_of_study, B-Lymphocytes, Tumor, breakpoint cluster region, Hematology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.anatomical_structure, Oncology, Antigen, Hematologic Neoplasms, Public Health and Health Services, BCR/TCR receptor repertoire, Human, Research Article, T cell, Oncology and Carcinogenesis, Population, Receptors, Antigen, T-Cell, Receptors, Antigen, B-Cell, Biology, lcsh:RC254-282, Cell Line, 03 medical and health sciences, Rare Diseases, EBV lymphocytes, Cell Line, Tumor, Genetics, medicine, Humans, Oncology & Carcinogenesis, education, T-cell receptor, Herpesvirus 4, B-Cell, T lymphocyte, T-Cell, Molecular biology, 030104 developmental biology, Cell culture, RNA

Abstract

Background Clonal VDJ rearrangement of B/T cell receptors (B/TCRs) occurring during B/T lymphocyte development has been used as a marker to track the clonality of B/T cell populations. Methods We systematically profiled the B/T cell receptor repertoire of 936 cancer cell lines across a variety of cancer types as well as 462 Epstein-Barr Virus (EBV) transformed normal B lymphocyte lines using RNA sequencing data. Results Rearranged B/TCRs were readily detected in cell lines derived from lymphocytes, and subclonality or potential biclonality were found in a number of blood cancer cell lines. Clonal BCR/TCR rearrangements were detected in several blast phase CML lines and unexpectedly, one gastric cancer cell line (KE-97), reflecting a lymphoid origin of these cells. Notably, clonality was highly prevalent in EBV transformed B lymphocytes, suggesting either transformation only occurred in a few B cells or those with a growth advantage dominated the transformed population through clonal evolution. Conclusions Our analysis reveals the complexity and heterogeneity of the BCR/TCR rearrangement repertoire and provides a unique insight into the clonality of lymphocyte derived cell lines. Electronic supplementary material The online version of this article (10.1186/s12885-018-4840-5) contains supplementary material, which is available to authorized users.

Published

2018

12. Functional Genome-wide Screening Identifies Targets and Pathways Sensitizing Pancreatic Cancer Cells to Dasatinib

Author

Yun Zheng, Kian Leong Lee, Henry Yang, Peer Wuensche, Ling-Wen Ding, Makoto Sudo, Wenwen Chien, Norimichi Hattori, Manoj Garg, Seiichi Mori, Erkan Baloglu, Sharon Shacham, Qiao-Yang Sun, Sigal Gery, H. Phillip Koeffler, Michael Kauffman, Sarawut Wongphayak, and Liang Xu

Subjects

0301 basic medicine, medicine.drug_class, Dasatinib, Cancer, Synthetic lethality, Biology, XPO, medicine.disease, Tyrosine-kinase inhibitor, Small hairpin RNA, 03 medical and health sciences, Pancreatic Cancer, 030104 developmental biology, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Pancreatic cancer, hemic and lymphatic diseases, medicine, Cancer research, Epigenetics, Signal transduction, medicine.drug, Research Paper

Abstract

This study is an unbiased genomic screen to obtain functional targets for increased effectiveness of dasatinib in pancreatic cancer. Dasatinib, a multi-targeted tyrosine kinase inhibitor, is used in clinical trials for treatment of pancreatic cancer; however, intrinsic and acquired resistance often occurs. We used a dasatinib-resistant pancreatic cancer cell line SU8686 to screen for synthetic lethality that synergizes with dasatinib using a pooled human shRNA library followed by next generation sequencing. Novel genes were identified which when silenced produced a prominent inhibitory effect with dasatinib against the pancreatic cancer cells. Several of these genes are involved in the regulation of epigenetics, as well as signaling pathways of the FOXO and hedgehog families. Small molecule inhibitors of either histone deacetylases or nuclear exporter had marked inhibitory effect with dasatinib in pancreatic cancers, suggesting their potential therapeutic effectiveness in this deadly cancer.

Published

2018

13. Genomic and Functional Analysis of the E3 Ligase PARK2 in Glioma

Author

Henry Yang, De-Chen Lin, Ling-Wen Ding, Ngan B. Doan, Shi-zhu Yu, Dong Yin, Ye Chen, Jonathan W. Said, Haiyan Yan, Michael Kahn, Masaharu Hazawa, H. Phillip Koeffler, Li-Zhen Liu, and Liang Xu

Subjects

Cancer Research, Ubiquitin-Protein Ligases, Down-Regulation, Mice, Nude, Article, Parkin, Cell Line, Mice, Ubiquitin, Cell Line, Tumor, Glioma, medicine, Animals, Humans, beta Catenin, Cell Proliferation, biology, Brain Neoplasms, Cell growth, Tumor Suppressor Proteins, HEK 293 cells, Ubiquitination, Wnt signaling pathway, medicine.disease, Cell biology, Ubiquitin ligase, Gene Expression Regulation, Neoplastic, HEK293 Cells, Oncology, biology.protein, Intracellular

Abstract

PARK2 (PARKIN) is an E3 ubiquitin ligase whose dysfunction has been associated with the progression of Parkinsonism and human malignancies, and its role in cancer remains to be explored. In this study, we report that PARK2 is frequently deleted and underexpressed in human glioma, and low PARK2 expression is associated with poor survival. Restoration of PARK2 significantly inhibited glioma cell growth both in vitro and in vivo, whereas depletion of PARK2 promoted cell proliferation. PARK2 attenuated both Wnt- and EGF-stimulated pathways through downregulating the intracellular level of β-catenin and EGFR. Notably, PARK2 physically interacted with both β-catenin and EGFR. We further found that PARK2 promoted the ubiquitination of these two proteins in an E3 ligase activity-dependent manner. Finally, inspired by these newly identified tumor-suppressive functions of PARK2, we tested and proved that combination of small-molecule inhibitors targeting both Wnt–β-catenin and EGFR–AKT pathways synergistically impaired glioma cell viability. Together, our findings uncover novel cancer-associated functions of PARK2 and provide a potential therapeutic approach to treat glioma. Cancer Res; 75(9); 1815–27. ©2015 AACR.

Published

2015

14. Activation of protein phosphatase 2A tumor suppressor as potential treatment of pancreatic cancer

Author

Seiichi Mori, Itay Tokatly, Wenwen Chien, Henry Yang, Ling-Wen Ding, Qiao-Yang Sun, H. Phillip Koeffler, Jeffrey W. Tyner, Siew Zhuan Tan, Kian Leong Lee, Peer Wuensche, Lorenz Poellinger, Lucia A. Torres-Fernandez, and Norazean Zaiden

Subjects

Cancer Research, Dasatinib, Drug Evaluation, Preclinical, Antineoplastic Agents, Apoptosis, Biology, Penfluridol, Inhibitory Concentration 50, Phenothiazines, Cell Line, Tumor, Pancreatic cancer, Genetics, medicine, Humans, Gene silencing, Computer Simulation, Protein Phosphatase 2, Protein Kinase Inhibitors, Research Articles, Cell Proliferation, Cell growth, Kinase, Tumor Suppressor Proteins, Cell Cycle, General Medicine, Protein phosphatase 2, Cell cycle, medicine.disease, Enzyme Activation, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, Oncology, Biochemistry, Cancer research, Molecular Medicine, medicine.drug

Abstract

We utilized three tiers of screening to identify novel therapeutic agents for pancreatic cancers. First, we analyzed 14 pancreatic cancer cell lines against a panel of 66 small‐molecule kinase inhibitors and dasatinib was the most potent. Second, we performed RNA expression analysis on 3 dasatinib‐resistant and 3 dasatinib–sensitive pancreatic cancer cell lines to profile their gene expression. Third, gene profiling data was integrated with the Connectivity Map database to search for potential drugs. Thioridazine was one of the top ranking small molecules with highly negative enrichment. Thioridazine and its family members of phenothiazine including penfluridol caused pancreatic cancer cell death and affected protein expression levels of molecules involved in cell cycle regulation, apoptosis, and multiple kinase activities. This family of drugs causes activation of protein phosphatase 2 (PP2A). The drug FTY‐720 (activator of PP2A) induced apoptosis of pancreatic cancer cells. Silencing catalytic unit of PP2A rendered pancreatic cancer cells resistant to penfluridol. Our observations suggest potential therapeutic use of penfluridol or similar agent associated with activation of PP2A in pancreatic cancers.

Published

2015

15. Mutational profiling of acute lymphoblastic leukemia with testicular relapse

Author

Anand Mayakonda, Allen Eng Juh Yeoh, Liang Xu, Wenwen Chien, H. Phillip Koeffler, De-Chen Lin, Zhentang Lao, Manoj Garg, Michael Lill, Qiao-Yang Sun, Yan-Yi Jiang, Henry Yang, Ling-Wen Ding, and Kar Tong Tan

Subjects

0301 basic medicine, Oncology, Male, Pathology, Cancer Research, Nucleotidase activity, medicine.medical_treatment, Lymphoblastic Leukemia, DNA Mutational Analysis, Acute lymphoblastic leukemia, Cardiorespiratory Medicine and Haematology, Biochemistry, Somatic evolution in cancer, Recurrence, Missense mutation, Child, Letter to the Editor, Exome sequencing, Cancer, Pediatric, Hematology, Extramedullary relapse, lcsh:Diseases of the blood and blood-forming organs, Precursor Cell Lymphoblastic Leukemia-Lymphoma, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Leukemia, medicine.anatomical_structure, Biotechnology, Urologic Diseases, medicine.medical_specialty, Pediatric Research Initiative, Medullary cavity, Childhood Leukemia, Pediatric Cancer, Testicular relapse, Immunology, Oncology and Carcinogenesis, Biology, lcsh:RC254-282, Clonal Evolution, 03 medical and health sciences, Therapeutic approach, Rare Diseases, Testicular Neoplasms, Clinical Research, Internal medicine, medicine, Genetics, Humans, Preschool, Molecular Biology, Chemotherapy, lcsh:RC633-647.5, business.industry, Human Genome, Infant, Cell Biology, medicine.disease, 030104 developmental biology, Bone marrow, business, ALL, Burkitt's lymphoma, Diffuse large B-cell lymphoma

Abstract

Relapse acute lymphoblastic leukemia (ALL) is the leading cause of childhood cancer deaths. Although relapse usually occurs in the bone marrow (medullary), extramedullary relapse occasionally occurs. Currently, the clonal origin and evolution of extramedullary relapse remain elusive. We selected two pediatric B-ALL patients who experienced testicular ALL relapse and interrogated their leukemic cells (diagnosis, remission, bone marrow relapse and testicular relapse) with whole exome sequencing. Case D483 (5.6 years old at diagnosis of ALL) developed bone marrow and testicular relapse 5 years after diagnosis of B-ALL. At diagnosis he was treated as an intermediate risk with hyperdiploid-ALL with the absence of any well-known ALL fusion-oncogene. Mutations of KRAS (G12D) and CREBBP (S1436C) were found in the founding leukemic clone at diagnosis and persisted in the bone marrow and testis at relapse). Mutation of CREBBP has been frequently found in ALL (particularly in hyperdiploid subtype) and is correlated with increased incidence of relapsed ALL. A MEF2B mutation (R17Q) was found in the bone marrow and testicular relapse sample. Missense mutation of this gene is frequently found in diffuse large B cell lymphoma (DLBCL); this protein regulates the expression of the proto-oncogene BCL6 and contributes to malignant transformation. Second child, case D727 (1.3 years old at diagnosis) harbored a MLL-AF9 fusion and was assigned as a high risk-ALL at diagnosis. Two NT5C2 mutations occurred at relapse, being present at different VAF in bone marrow and testicle: missense mutation R367Q was present with a VAF of 33.5% in bone marrow and 4.5% in testicle; while D407V was present with a VAF of 6.5% in bone marrow and 35.5% in the testicular relapse. NT5C2 encodes a 5'-nucleotidase involved in purine metabolism. The missense mutations (R367Q and D407V) identified here, have been reported as recurrent mutational hotspots of NT5C2 in relapse ALL and have been functionally validated. These mutations increase the 5'-IMP nucleotidase activity of NT5C2 protein leading to resistance to 6-mercaptopurine, a drug that was a component of the treatment regime of this patient. To understand the evolutionary trajectories of these two ALL cases, we analyzed clonal evolution based on their sequencing data. In patient D483, the relapse leukemia was directly evolved from the diagnosis leukemia clone: all of the mutations at diagnosis were persisted at relapse, and four mutated genes (MEF2B, KCNG1, AIM1, OTUD5) were acquired at both bone marrow and testicular relapse with different variant allele frequency (VAF). In patient D727, however, a faction of mutations present at diagnosis were subsequently lost at relapse, suggesting that relapsed leukemia arose from an ancestral subclone that developed before the overt leukemia at diagnosis. The mutational pattern and VAF cluster analysis results suggest that relapse in the patients' testicle represents an independently subclones from the relapse in their bone marrows. Taken together, our sequencing results suggest that relapse of patient D483 was directly evolved from the diagnosis leukemic clone; while the relapse leukemia cells (both bone marrow and testicle) of patient D727 was likely derived from a common ancestral clone, and the testicular relapse arose independently from the bone marrow relapse leukemia. Disclosures Lill: Sanofi: Speakers Bureau; California Cord Blood Services: Consultancy; Kite: Research Funding.

Published

2017

16. Mutational Landscape of Pediatric Acute Lymphoblastic Leukemia

Author

Lucía Fernández, Manoj Garg, H. Phillip Koeffler, Lee Yung Shih, Qiao-Yang Sun, Yan-Yi Jiang, Der Cherng Liang, Masashi Sanada, Yasunobu Nagata, Xin-Yi Loh, Wenwen Chien, Kar Tong Tan, De-Chen Lin, Hema Preethi, Hagop M. Kantarjian, Henry Yang, Li Zhen Liu, Ling-Wen Ding, Su Lin Lim, Steven M. Kornblau, Anand Mayakonda Thippeswamy, Jin Fen Xiao, Vikas Madan, Norihiko Kawamata, Seishi Ogawa, Liang Xu, Allen Eng Juh Yeoh, Michael Lill, and Satoru Miyano

Subjects

0301 basic medicine, Male, Cancer Research, ARID1A, DNA Mutational Analysis, Bioinformatics, Receptor tyrosine kinase, Mice, 2.1 Biological and endogenous factors, Aetiology, Child, Cancer, Pediatric, biology, Blotting, High-Throughput Nucleotide Sequencing, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Oncology, Child, Preschool, Female, Tyrosine kinase, Western, Biotechnology, Pediatric Research Initiative, Adolescent, Pediatric Cancer, Childhood Leukemia, Blotting, Western, Oncology and Carcinogenesis, Article, 03 medical and health sciences, Rare Diseases, Clinical Research, medicine, Genetics, Animals, Humans, Epigenetics, Oncology & Carcinogenesis, Preschool, Transcription factor, Infant, medicine.disease, 030104 developmental biology, Good Health and Well Being, CTCF, Mutation, biology.protein

Abstract

Current standard of care for patients with pediatric acute lymphoblastic leukemia (ALL) is mainly effective, with high remission rates after treatment. However, the genetic perturbations that give rise to this disease remain largely undefined, limiting the ability to address resistant tumors or develop less toxic targeted therapies. Here, we report the use of next-generation sequencing to interrogate the genetic and pathogenic mechanisms of 240 pediatric ALL cases with their matched remission samples. Commonly mutated genes fell into several categories, including RAS/receptor tyrosine kinases, epigenetic regulators, transcription factors involved in lineage commitment, and the p53/cell-cycle pathway. Unique recurrent mutational hotspots were observed in epigenetic regulators CREBBP (R1446C/H), WHSC1 (E1099K), and the tyrosine kinase FLT3 (K663R, N676K). The mutant WHSC1 was established as a gain-of-function oncogene, while the epigenetic regulator ARID1A and transcription factor CTCF were functionally identified as potential tumor suppressors. Analysis of 28 diagnosis/relapse trio patients plus 10 relapse cases revealed four evolutionary paths and uncovered the ordering of acquisition of mutations in these patients. This study provides a detailed mutational portrait of pediatric ALL and gives insights into the molecular pathogenesis of this disease. Cancer Res; 77(2); 390–400. ©2016 AACR.

Published

2017

17. Genomic and Epigenomic Heterogeneity of Hepatocellular Carcinoma

Author

Anand Mayakonda, Xiaoping Liu, De-Chen Lin, Dong Yin, Lehang Lin, Ling-Wen Ding, Erwei Song, Huy Q. Dinh, Jie Wang, H. Phillip Koeffler, Benjamin P. Berman, and Pinbo Huang

Subjects

0301 basic medicine, Adult, Male, Cancer Research, Carcinoma, Hepatocellular, DNA Copy Number Variations, DNA Mutational Analysis, Genomics, Biology, Malignancy, Article, 03 medical and health sciences, Genetic Heterogeneity, 0302 clinical medicine, medicine, Carcinoma, Humans, Exome, Epigenetics, neoplasms, Epigenomics, Aged, Genetics, Genetic heterogeneity, Liver Neoplasms, Cancer, High-Throughput Nucleotide Sequencing, Middle Aged, medicine.disease, digestive system diseases, Neoplasm Proteins, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Mutation, Cancer research, Female

Abstract

Understanding the intratumoral heterogeneity of hepatocellular carcinoma is instructive for developing personalized therapy and identifying molecular biomarkers. Here we applied whole-exome sequencing to 69 samples from 11 patients to resolve the genetic architecture of subclonal diversification. Spatial genomic diversity was found in all 11 hepatocellular carcinoma cases, with 29% of driver mutations being heterogeneous, including TERT, ARID1A, NOTCH2, and STAG2. Similar with other cancer types, TP53 mutations were always shared between all tumor regions, that is, located on the “trunk” of the evolutionary tree. In addition, we found that variants within several drug targets such as KIT, SYK, and PIK3CA were mutated in a fully clonal manner, indicating their therapeutic potentials for hepatocellular carcinoma. Temporal dissection of mutational signatures suggested that mutagenic processes associated with exposure to aristolochic acid and aflatoxin might play a more important role in early, as opposed to late, stages of hepatocellular carcinoma development. Moreover, we observed extensive intratumoral epigenetic heterogeneity in hepatocellular carcinoma based on multiple independent analytical methods and showed that intratumoral methylation heterogeneity might play important roles in the biology of hepatocellular carcinoma cells. Our results also demonstrated prominent heterogeneity of intratumoral methylation even in a stable hepatocellular carcinoma genome. Together, these findings highlight widespread intratumoral heterogeneity at both the genomic and epigenomic levels in hepatocellular carcinoma and provide an important molecular foundation for better understanding the pathogenesis of this malignancy. Cancer Res; 77(9); 2255–65. ©2017 AACR.

Published

2016

18. Mutational profiling of a MonoMAC syndrome family with GATA2 deficiency

Author

Mori M, Michael Lill, Henry Yang, Anand Mayakonda, Kar Tong Tan, Ling-Wen Ding, H P Koeffler, Y. Y. Jiang, Takayuki Ikezoe, Wenwen Chien, Qiao-Yang Sun, and De-Chen Lin

Subjects

Male, Cancer Research, Adolescent, DNA Mutational Analysis, Biology, Article, Monocytes, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, medicine, Profiling (information science), Humans, Germ-Line Mutation, Genetics, GATA2 Deficiency, Extramural, Hematology, medicine.disease, MonoMAC, Pedigree, GATA2 Transcription Factor, Oncology, 030220 oncology & carcinogenesis, Myelodysplastic Syndromes, Female, 030215 immunology

Published

2016

19. Abstract 2569: BCL6 promotes glioma and serves as a novel therapeutic target

Author

Steve E. Savinoff, De-Chen Lin, Jean-Paul Kovalik, Ngan B. Doan, Liang Xu, Jonathan W. Said, Anand Mayakonda, Marina Dutra-Clarke, Yan-Yi Jiang, Jeffrey W. Tyner, Joshua J. Breunig, Jianhong Ching, Yi Chen, William H. Yong, Henry Yang, Ling-Wen Ding, Phillip Koeffler, Masaharu Hazawa, and Markus Müschen

Subjects

Cancer Research, Oncology, business.industry, Glioma, Cancer research, Medicine, business, BCL6, medicine.disease

Abstract

ZBTB transcription factors orchestrate gene transcription during tissue development. However, their roles in glioblastoma multiforme (GBM) remain unexplored. Here, through a functional screening of ZBTB genes, we identify that BCL6 is required for GBM cell proliferation and is overexpressed in GBM samples. Using a somatic transgenic mouse model, Bcl6 confers the proliferative and invasive stimuli to glioma cells in vivo. Moreover, we discover AXL as a novel downstream target of BCL6. Through AXL, BCL6 enhances both MEK-ERK and S6K-RPS6 axes. Pharmacological inhibition of BCL6 activity effectively blocks GBM growth and inhibits AXL expression. Together, these findings uncover a novel glioma-promoting role of BCL6, and provide the rationale of targeting BCL6 as a potential therapeutic approach. Citation Format: Liang Xu, Ye CHEN, Marina Dutra-Clarke, Anand Mayakonda, Masaharu Hazawa, Steve E. Savinoff, Ngan Doan, Jonathan W. Said, William H. Yong, Henry Yang, Ling-Wen Ding, Yan-Yi Jiang, Jeffrey W. Tyner, Jianhong Ching, Jean-Paul Kovalik, Markus Müschen, Joshua J. Breunig, De-Chen Lin, Phillip Koeffler. BCL6 promotes glioma and serves as a novel therapeutic target [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 2569. doi:10.1158/1538-7445.AM2017-2569

Published

2017

20. Abstract 806: MGA is a potential tumor suppressor in acute myeloid leukemia

Author

Xin-Yi Loh, Wenwen Chien, Qiao-Yang Sun, Yan-Yi Jiang, De-Chen Lin, Jin-Fen Xiao, Kar Tong Tan, Anand Mayakonda, H. Phillip Koeffler, Henry Yang, Ling-Wen Ding, and Sigal Gery

Subjects

Cancer Research, Myeloid, Myeloid leukemia, Transfection, Biology, Molecular biology, Small hairpin RNA, Cyclin E1, Promyelocytic leukemia protein, medicine.anatomical_structure, Oncology, biology.protein, medicine, Gene silencing, Luciferase

Abstract

MGA is an incompletely studied gene with a high mutation frequency in MLL-PTD AML (9%) and in core bind factor AML (8%). This gene encodes a MAX-interacting protein and is believed to act as a transcription factor that suppresses MYC binding to its target. By in silico analysis, we found that MGA is expressed in normal myeloid hematopoietic cells and AML, and the expression level is comparable with TET2 or DNMT3A. Further data mining of TCGA revealed a high frequency of inactivating mutations of the MGA gene in a variety of cancers such as various adenocarcinomas. To interrogate functionally its role in leukemogenesis, lentiviral constructs containing either shRNA or CRISPR-sgRNA targeted to different regions of the MGA gene were generated. MGA expressing AML cell line EOL-1 was silenced by shRNA or CRISPER system. Silencing was confirmed by western blot (shRNA) and Sanger Sequencing (sgRNA). An increase of methylcellulose colony number (~30%) was observed in MGA silenced cell lines. Control EOL-1 cells or EOL-1 cells silenced with MGA CRISPR sgRNAs were injected into both flanks of NSG mice, and tumor masses were harvested 21 days after injection. Silencing of MGA by CRISPR-sgRNA consistently enhanced in vivo xenograft cell growth. In addition, western blot analyses revealed silencing of MGA in EOL-1 cells increased protein levels of Cyclin E1 and phos-RB (S807 phosphorylation inhibits the ability of RB to target protein allowing cell cycle progression), indicative of a proliferative advantage conferred by the silencing of MGA. MGA may be a potential regulator of the MYC pathway. We, therefore, examined whether silencing of MGA alters MYC transcriptional activity. Luciferase reporter assay was carried out in 293FT cells stabilized with either scramble or shRNA- targeting MGA. Luciferase activities were measured 48 h after transfection of cells with MYC activity reporter pMyc4ElbLuc and normalized to the corresponding co-transfected Renilla luciferase activity. A fourfold increase in luciferase activity was observed in MGA silenced cells when compared with non- targeting shRNA controls. Furthermore, Kaplan–Meier survival analysis was performed in the TCGA-AML patients by comparison of cases with highest versus lowest expression of MGA. P-values were calculated by log-rank test. MGA expression data and patient survival data were retrieved from TCGA-AML patients RNA seq, or microarray (70 AML patients). The MGA expression ‘high’ and ‘low’ groups were defined by 15% higher than the median or 15% lower than the median, respectively. AML patients with lower levels of MGA in their leukemic samples had a worse outcome compared with those whose leukemic cells expressed higher levels of MGA. Collectively, our results suggest that MGA may function as a potential tumor-suppressor in AML. Citation Format: Qiaoyang Sun, Lingwen Ding, Kar-Tong Tan, Wenwen Chien, Xinyi Loh, Jinfen Xiao, Anand Mayakonda, Dechen Lin, Yanyi Jiang, Henry Yang, Sigal Gery, H. Phillip Koeffler. MGA is a potential tumor suppressor in acute myeloid leukemia [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 806. doi:10.1158/1538-7445.AM2017-806

Published

2017

21. Abstract 4494: Tumor suppressive role of ZFP36L1 by suppressing HIF1α and Cyclin D1 in bladder and breast cancer

Author

Ling-Wen Ding, Xin-Yi Loh, and H. Phillip Koeffler

Subjects

Zinc finger, Cancer Research, Messenger RNA, Immunoprecipitation, Wild type, Cancer, Biology, Cell cycle, medicine.disease, medicine.disease_cause, Cyclin D1, Oncology, Cancer research, medicine, Carcinogenesis

Abstract

AU-rich mRNAs are a class of mRNAs that contains AU-rich elements (AREs) motifs in their 3’UTR. The half-life and turnover of AU-rich mRNAs are tightly regulated by AREs-binding proteins, such as Zinc finger protein 36 C3H type-like 1 (ZFP36L1). ZFP36L1 is one of the RNA-binding proteins (RBPs), which consists of two tandemly repeated zinc finger motifs that specifically recognize AREs motifs and mediate mRNAs decay. However, our knowledge on role of ZFP36L1 in breast and bladder cancers and its downstream targets remains poorly elucidated. Here, we hypothesized that ZFP36L1 might degrade oncogenic mRNAs transcripts, thus leading to suppression of tumorigenesis. Our analysis of in silico data revealed that ZFP36L1 is significantly mutated or downregulated in a variety of cancers. The high proportion of inactivation mutation pattern as well as the Mutsig result suggest that it may act as an unappreciated tumor suppressor. Lower ZFP36L1 expression correlated with reduced survival in patients. Forced expression of ZFP36L1 markedly reduced cellular proliferation, invasiveness and migration in vitro, as well as tumor growth in vivo. In addition, microarray and RNA-seq data analysis showed that several important cancer-related candidates such as IL8 and HIF1α were significantly downregulated. Overexpression of ZFP36L1 reduced HIF1α mRNA and protein expression. Similarly, HIF1α forced expression also inhibited ZFP36L1 mRNA and protein, suggesting a feedback loop of HIF1α and ZFP36L1. Dual luciferase reporter assays and RNA Electro-mobility Shift Assay (REMSA) showed that only wild type ZFP36L1, but not different mutants of ZFP36L1, was able to bind directly and to degrade a HIF1α 3’UTR construct that contains AU-rich regions. Meanwhile, mRNA pull down assay demonstrated that ZFP36L1 protein recognized cell-cycle related transcripts. Overexpression of ZFP36L1 led to reduction of Cyclin D1 and phospho-Rb in protein expression. Furthermore, SILAC data unveiled interesting binding partners of ZFP36L1. Collectively, our findings propose that ZFP36L1 might have a critical tumor suppressive role in breast and bladder cancer by negatively regulating mRNA whose protein products cooperatively promote hypoxia and transition into S phase of cell cycle. Augmenting ZFP36L1 function might disable the cell cycle and proliferation of aggressive bladder tumors. Citation Format: Xin Yi Loh, Ling Wen Ding, H. Phillip Koeffler. Tumor suppressive role of ZFP36L1 by suppressing HIF1α and Cyclin D1 in bladder and breast cancer [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 4494. doi:10.1158/1538-7445.AM2017-4494

Published

2017

22. KPT-330 has antitumour activity against non-small cell lung cancer

Author

Su Lin Lim, Makoto Sudo, Norimichi Hattori, Wenwen Chien, Haibo Sun, M. Kauffman, Ling-Wen Ding, Qiao-Yang Sun, H P Koeffler, Tsuyoshi Nakamaki, Sharon Shacham, and G L E-Ling

Subjects

Male, p53, Cancer Research, Cell cycle checkpoint, Lung Neoplasms, Cytoplasmic and Nuclear, Receptors, Cytoplasmic and Nuclear, Apoptosis, Mice, SCID, medicine.disease_cause, NSCLC, CRM1, Mice, 0302 clinical medicine, Mice, Inbred NOD, Carcinoma, Non-Small-Cell Lung, Receptors, Antineoplastic Combined Chemotherapy Protocols, Tensin, Non-Small-Cell Lung, Lung, Cancer, 0303 health sciences, Mutation, Tumor, Lung Cancer, 3. Good health, Hydrazines, Oncology, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Public Health and Health Services, Development of treatments and therapeutic interventions, medicine.drug, Oncology and Carcinogenesis, p73, Antineoplastic Agents, Cell Growth Processes, Biology, Karyopherins, SCID, Cell Line, 03 medical and health sciences, In vivo, Cell Line, Tumor, medicine, Genetics, Animals, Humans, Oncology & Carcinogenesis, Lung cancer, neoplasms, 030304 developmental biology, Cisplatin, Carcinoma, G1 Phase, Triazoles, medicine.disease, Genes, p53, Xenograft Model Antitumor Assays, In vitro, SINE, respiratory tract diseases, Genes, Immunology, Cancer research, Inbred NOD, Translational Therapeutics

Abstract

Background: We investigated the biologic and pharmacologic activities of a chromosome region maintenance 1 (CRM1) inhibitor against human non-small cell lung cancer (NSCLC) cells both in vitro and in vivo. Methods: The in vitro and in vivo effects of a novel CRM1 inhibitor (KPT-330) for a large number of anticancer parameters were evaluated using a large panel of 11 NSCLC cell lines containing different key driver mutations. Mice bearing human NSCLC xenografts were treated with KPT-330, and tumour growth was assessed. Results: KPT-330 inhibited proliferation and induced cell cycle arrest and apoptosis-related proteins in 11 NSCLC cells lines. Moreover, the combination of KPT-330 with cisplatin synergistically enhanced the cell kill of the NSCLC cells in vitro. Human NSCLC tumours growing in immunodeficient mice were markedly inhibited by KPT-330. Also, KPT-330 was effective even against NSCLC cells with a transforming mutation of either exon 20 of EGFR, TP53, phosphatase and tensin homologue, RAS or PIK3CA, suggesting the drug might be effective against a variety of lung cancers irrespective of their driver mutation. Conclusions: Our results support clinical testing of KPT-330 as a novel therapeutic strategy for NSCLC.

Published

2014

23. PIAS4 is an activator of hypoxia signalling via VHL suppression during growth of pancreatic cancer cells

Author

Peer Wuensche, Wenwen Chien, Jonathan W. Said, H P Koeffler, Kian Leong Lee, Ngan B. Doan, Ling-Wen Ding, H Kato, and Lorenz Poellinger

Subjects

Vascular Endothelial Growth Factor A, Cancer Research, Jumonji Domain-Containing Histone Demethylases, Pancreatic disease, endocrine system diseases, pancreatic cancer, urologic and male genital diseases, RNA, Small Interfering, Poly-ADP-Ribose Binding Proteins, Tumor, Protein Inhibitors of Activated STAT, female genital diseases and pregnancy complications, Cell Hypoxia, Gene Expression Regulation, Neoplastic, Vascular endothelial growth factor A, Oncology, Von Hippel-Lindau Tumor Suppressor Protein, PIAS4, Public Health and Health Services, RNA Interference, Hypoxia-Inducible Factor 1, medicine.symptom, Signal Transduction, STAT3 Transcription Factor, medicine.medical_specialty, Oncology and Carcinogenesis, Biology, Adenocarcinoma, Small Interfering, alpha Subunit, Cell Line, Internal medicine, Pancreatic cancer, Cell Line, Tumor, medicine, Humans, Oncology & Carcinogenesis, neoplasms, Molecular Diagnostics, Cell Proliferation, Neoplastic, Cell growth, Activator (genetics), hypoxia, Cancer, Sumoylation, Hypoxia (medical), medicine.disease, Hypoxia-Inducible Factor 1, alpha Subunit, Pancreatic Neoplasms, Endocrinology, Gene Expression Regulation, Cancer research, RNA

Abstract

Background: The PIAS4 protein belongs to the family of protein inhibitors of activated STAT, but has since been implicated in various biological activities including the post-translational modification known as sumoylation. In this study, we explored the roles of PIAS4 in pancreatic tumourigenesis. Methods: The expression levels of PIAS4 in pancreatic cancer cells were examined. Cell proliferation and invasion was studied after overexpression and gene silencing of PIAS4. The effect of PIAS4 on hypoxia signalling was investigated. Results: The protein was overexpressed in pancreatic cancer cells compared with the normal pancreas. Gene silencing by PIAS4 small interfering RNA (siRNA) suppressed pancreatic cancer cell growth and overexpression of PIAS4 induced expression of genes related to cell growth. The overexpression of PIAS4 is essential for the regulation of the hypoxia signalling pathway. PIAS4 interacts with the tumour suppressor von Hippel-Lindau (VHL) and leads to VHL sumoylation, oligomerization, and impaired function. Pancreatic cancer cells (Panc0327, MiaPaCa2) treated with PIAS4 siRNA suppressed expression of the hypoxia-inducible factor hypoxia-inducible factor 1 alpha and its target genes JMJD1A, VEGF, and STAT3. Conclusion: Our study elucidates the role of PIAS4 in the regulation of pancreatic cancer cell growth, where the suppression of its activity represents a novel therapeutic target for pancreatic cancers.

Published

2013

24. Erratum: Comprehensive mutational analysis of primary and relapse acute promyelocytic leukemia

Author

Hsin-An Hou, Kamran Alimoghaddam, Bayard L. Powell, Andrea Biondi, Henry Yang, Ling-Wen Ding, Satoru Miyano, W. J. Chng, Janani Sundaresan, Masashi Sanada, Norimichi Hattori, Yuichi Shiraishi, Daniel Nowak, Lin Han, Saravanan Ganesan, Deepika Kanojia, Yasunobu Nagata, Wendy Stock, Steve Kornblau, Jairo Matthews, T Haferlach, T. Ma, Kenichi Yoshida, Ezhilarasi Chendamarai, Madan, M. C. Kuo, Anand Mayakonda, Gregory Malnassy, H P Koeffler, A. Ghavamzadeh, Michael Heuser, Richard A. Larson, Hagop M. Kantarjian, W. Chien, Takayuki Ikezoe, Tamara Alpermann, Manoj Garg, Seishi Ogawa, Wolf-K. Hofmann, Qiao-Yang Sun, S. Rostami, Michael Lübbert, Noreen Fulton, Pavithra Shyamsunder, Shih Ly, Mathews, L. Z. Liu, Michael Lill, Hwei-Fang Tien, Maya Koren-Michowitz, Arnold Ganser, and Kar Tong Tan

Subjects

Acute promyelocytic leukemia, Oncology, Cancer Research, medicine.medical_specialty, DNA Mutational Analysis, Acute myeloid leukaemia, 03 medical and health sciences, 0302 clinical medicine, Leukemia, Promyelocytic, Acute, Recurrence, Internal medicine, medicine, Humans, Exome, Cancer genetics, Hematology, business.industry, Gene Expression Profiling, Nuclear Proteins, Cell Differentiation, medicine.disease, DNA-Binding Proteins, Mutational analysis, Leukemia, 030220 oncology & carcinogenesis, Immunology, Erratum, business, Transcription Factors, 030215 immunology

Abstract

Acute promyelocytic leukemia (APL) is a subtype of myeloid leukemia characterized by differentiation block at the promyelocyte stage. Besides the presence of chromosomal rearrangement t(15;17), leading to the formation of PML-RARA (promyelocytic leukemia-retinoic acid receptor alpha) fusion, other genetic alterations have also been implicated in APL. Here, we performed comprehensive mutational analysis of primary and relapse APL to identify somatic alterations, which cooperate with PML-RARA in the pathogenesis of APL. We explored the mutational landscape using whole-exome (n=12) and subsequent targeted sequencing of 398 genes in 153 primary and 69 relapse APL. Both primary and relapse APL harbored an average of eight non-silent somatic mutations per exome. We observed recurrent alterations of FLT3, WT1, NRAS and KRAS in the newly diagnosed APL, whereas mutations in other genes commonly mutated in myeloid leukemia were rarely detected. The molecular signature of APL relapse was characterized by emergence of frequent mutations in PML and RARA genes. Our sequencing data also demonstrates incidence of loss-of-function mutations in previously unidentified genes, ARID1B and ARID1A, both of which encode for key components of the SWI/SNF complex. We show that knockdown of ARID1B in APL cell line, NB4, results in large-scale activation of gene expression and reduced in vitro differentiation potential.

Published

2016

25. Abstract 2868: SETDB1 accelerates non-small cell lung cancer (NSCLC) tumorigenesis through WNT signalling pathway

Author

David Chia, H. Phillip Koeffler, Qiao-Yang Sun, Lee Goodglick, Jin-Fen Xiao, Ngan B. Doan, Vei Mah, Jonathan W. Said, Mohammad Alavi, Henry Yang, and Ling-Wen Ding

Subjects

FZD1, Cancer Research, Wnt signaling pathway, non-small cell lung cancer (NSCLC), Biology, medicine.disease, medicine.disease_cause, Histone H3, Cyclin D1, Oncology, Immunology, Histone methylation, medicine, Cancer research, Ectopic expression, Carcinogenesis

Abstract

Histone methylation deregulation leads to disruption of chromatin structure and gene expression pattern in many human cancers. Histone H3 lysine K9 methyltransferase, SETDB1 (SET domain, bifurcated 1) is initially reported to control heterochromatin structure, repress gene expression and be essential in early embryogenesis. Studies have recently shown its involvement in boosting tumorigenesis in different kinds of human cancers, including lung cancer. However, the mechanism underlying its ability to promote tumorigenesis remains largely unknown. In our study, we sought to investigate the oncogenic role of SETDB1 in NSCLC. Our immunohistochemistry found that 72% out of 387-lung cancer cases stained positively for SETDB1, compared to 46% samples of normal bronchial epithelium (p Ectopic expression of SETDB1 in NSCLC cell lines enhanced clonogenic growth in vitro and significantly enlarges tumor size in vivo; while depleting endogenous SETDB1 expression with shRNAs suppressed NSCLC cells proliferation and tumor formation. Analyzing the expression pattern of cells with forced expression of SETDB1 combined with TOP/FOP luciferase assay and western blotting showed that WNT/β-catenin signaling was activated upon overexpression of SETDB1, as well as upregulation of its downstream targets, c-Myc and Cyclin D1. ChIP assay showed that SETDB1 binds to WNT relevant genes, such as APOE, IGFBP4, FZD1 and LRP8 and upregulates their transcription, which is very distinct from its canonical suppressing function of H3K9 trimethylation. Interestingly, we also noted that SETDB1 was able to repress P53 expression, while diminishing P53 expression reciprocally enhanced SETDB1 expression. In summary, our study demonstrates that SETDB1 enhances NSCLC tumorigenesis through activating WNT/β-catenin signaling and repressing tumor suppressor P53. Our novel findings provide new insight into a non-canonical function of SETDB1 in activating gene expression, and suggest therapeutic benefit of targeting SETDB1 in NSCLC having high expression level of this protein. Citation Format: Qiaoyang Sun, Lingwen Ding, Jinfen Xiao, Lee Goodglick, David Chia, Vei Mah, Mohammad Alavi, Ngan Doan, Jonathan W. Said, Henry Yang, H.Phillip Koeffler. SETDB1 accelerates non-small cell lung cancer (NSCLC) tumorigenesis through WNT signalling pathway. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 2868. doi:10.1158/1538-7445.AM2015-2868

Published

2015

26. Abstract 122: PARK2 is a negative regulator of Wnt and EGFR pathways in glioma

Author

Henry Yang, Ling-Wen Ding, Ngan B. Doan, De-Chen Lin, Shi-zhu Yu, Michael Kahn, Dong Yin, Jonathan W. Said, Masaharu Hazawa, Phillip Koeffler, Haiyan Yan, Li-Zhen Liu, Ye Chen, and Liang Xu

Subjects

Cancer Research, biology, Microarray analysis techniques, Cell growth, business.industry, Wnt signaling pathway, Cancer, medicine.disease, Ubiquitin ligase, Cyclin D1, Oncology, Glioma, Immunology, medicine, biology.protein, Cancer research, Ectopic expression, business

Abstract

PARK2 is an E3 ubiquitin ligase whose dysfunction has been associated with the progression of autosomal recessive juvenile Parkinson's disease and human malignancies. However, its role in cancer remains to be explored. In this study, we report that PARK2 is frequently deleted and underexpressed in human glioma, and low PARK2 expression is associated with poor survival in cohorts of both low-grade glioma and glioblastoma multiforme (GBM). Functional studies revealed a tumor-suppressive role of PARK2 in GBM cells. Restoration of PARK2 significantly inhibited glioma cell growth both in vitro and in vivo, while depletion of endogenous PARK2 promoted cell proliferation. cDNA microarray analysis showed that PARK2 expression strongly altered the activity of both the Wnt and EGFR pathways. Immunoblot analysis confirmed that ectopic expression of PARK2 suppressed the intracellular levels of β-catenin, EGFR, as well as their down-stream targets including Cyclin D1, TCF4, c-Myc, p-AKT and p-S6K, etc. Notably, PARK2 physically interacted with both β-catenin and EGFR, and promoted their ubiquitination in an E3-ligase dependent manner. Similar to the ligase-dead PARK2 mutant (C431S), three PARK2 mutants harboring cancer-derived somatic mutations (T173A, T240M and P294S) showed decreased ability to ubiquitinate either β-catenin or EGFR proteins. We further found that PARK2 attenuated the cellular response to both Wnt3a and EGF stimulation, suggesting PARK2 is a negative regulator of both the Wnt and EGFR pathways. Lastly, inspired by these newly identified functions of PARK2, we tested and proved that the combination of small-molecule inhibitors targeting both Wnt-β-catenin and EGFR-AKT pathways synergistically impaired glioma cell viability. In aggregate, our findings uncover novel, cancer-associated functions of PARK2 and provide a potential therapeutic approach to treat glioma. Citation Format: Liang Xu, De-Chen Lin, Ye Chen, Haiyan Yan, Masaharu Hazawa, Ngan Doan, Jonathan W. Said, Ling-Wen Ding, Li-Zhen Liu, Henry Yang, Shi-zhu Yu, Michael Kahn, Dong Yin, Phillip Koeffler. PARK2 is a negative regulator of Wnt and EGFR pathways in glioma. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 122. doi:10.1158/1538-7445.AM2015-122

Published

2015

27. Abstract 138: Novel PAK4 allosteric modulators (PAMs) provide potential therapeutic options in human gastric cancer

Author

Sharon Shacham, Sigal Gery, H. Phillip Koeffler, William Senapedis, Qiao-Yang Sun, Ling-Wen Ding, Wenwen Chien, Erkan Baloglu, Muhammad Ikhsan B. Muzakar, and Jin-Fen Xiao

Subjects

Cancer Research, Cell growth, Cancer, Biology, medicine.disease, medicine.disease_cause, Metastasis, Oncology, Apoptosis, Immunology, Cancer cell, medicine, Cancer research, Viability assay, Carcinogenesis, PI3K/AKT/mTOR pathway

Abstract

Expression of PAK4 (p21-activated serine/threonine kinase 4) is associated with gastric tumorigenesis. Overexpression of PAK4 is correlated with metastasis of gastric cancer and in part confers cisplatin resistance in gastric cancer patients. We transduced the human gastric cancer cell line AGS with CRISPR/cas9 targeting PAK4, and observed reduced cell proliferation and motility. Novel PAK4 allosteric modulators (PAMs) were evaluated for their potential therapeutic use for gastric cancer. A panel of human gastric cancer cell lines was screened with four PAMs (KPT-7189, -7349, -7657, -8752). MTS assay showed inhibition of cell viability by PAMs in 6 of 10 gastric cancer cell lines (IC50 ranged from 50 to 5000 nM). Cell cycle analysis and annexin V assay indicated a combination of cell growth arrest at G1 phase and cell apoptosis after treatment with PAMs. Furthermore, PAMs diminished expression levels of PAK4, induced apoptosis-related molecule caspase-3, and suppressed PI3K/Akt and MEK/Erk signaling. Wound assay showed inhibition of cell migration and soft agar assay demonstrated suppression of colony formation for gastric cancer cells treated with PAMs. Mouse xenograft models are currently under investigation. Remarkably, PAMs in combination with cisplatin induced cell death in cisplatin-resistant gastric cancer cells in a synergistic manner. This study demonstrates PAMs have anti-tumor activity against gastric cancer cells and suggests their potential use for the treatment of gastric cancer. Citation Format: Wenwen Chien, Jinfen Xiao, Ling-Wen Ding, Muhammad Ikhsan B. Muzakar, Qiao-Yang Sun, Sigal Gery, William Senapedis, Sharon Shacham, Erkan Baloglu, H. Phillip Koeffler. Novel PAK4 allosteric modulators (PAMs) provide potential therapeutic options in human gastric cancer. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 138. doi:10.1158/1538-7445.AM2015-138

Published

2015

28. Abstract 3939: The genomic landscape of nasopharyngeal carcinoma

Author

Yasunobu Nagata, Soo-Chin Lee, De-Chen Lin, Arjun Sharma, Henry Yang, Ling-Wen Ding, Feng Gang Yu, Ana Maria Varela, Soh Ha Chan, H. Phillip Koeffler, Masaharu Hazawa, Li-Zhen Liu, Xuan Meng, Seishi Ogawa, Yusuke Sato, Liang Xu, Boon Cher Goh, Min Zin Oo, Bengt Fredrik Petersson, and Paul A. MacAry

Subjects

Cancer Research, Oncology, Nasopharyngeal carcinoma, medicine, Cancer research, Biology, medicine.disease

Abstract

Background Nasopharyngeal carcinoma (NPC) arises from the epithelial tissue of the nasopharynx. This cancer has remarkable ethnic and geographic distributions, with a particularly high prevalence in Southern China and Southeast Asia. Genetic susceptibility and Epstein-Barr virus infections have been implicated in the pathogenesis of NPC. However, genomic abnormalities of this neoplasm remain largely obscure, and no effective targeted therapy has been established. Therefore, a strong need exists to characterize the genetic alterations of this type of tumour for guiding the development of more effective and innovative therapeutic regimens. Methods Whole exomes sequencing (WES) was performed on 56 NPC germline/tumor pairs and 5 NPC cell lines. Transcriptome sequencing (RNA-seq) was conducted on 4 tumors from this cohort. An additional 61 NPC germline/tumor pairs and 5 non-paired primary tumors were further subjected to targeted regional deep-sequencing (TS). The somatic copy number variations (SCNV) of 52 primary tumors were profiled by SNP-array hybridization (50 of them also had WES data). Finally, both in vitro and in vivo biological and biochemical experiments were performed to evaluate the newly-identified mutations in NPC cell lines. Results We identified a total of 1,577 non-silent somatic mutations affecting 1,413 genes from WES, revealing a relatively low mutational rate and wide mutational diversity. Integration of the results from WES, TS and RNA-seq revealed a distinct mutational signature and a number of significantly mutated genes (such as TP53, ARID1A, MLL2, BAP1, PIK3CA, etc.) in NPC. Pathway enrichment analysis of genetic lesions identified several important cellular processes and pathways in NPC including chromatin modification, ERBB-PI3K signaling and autophagy machinery. We further characterized the biological functions of both ARID1A and BAP1 proteins in NPC cell lines. Depletion of wild-type endogenous ARID1A expression with shRNAs resulted in increased anchorage-independent colony formation, cell migration and xenograft growth in vivo, whereas ectopically expressed ARID1A suppressed both cell proliferation and migration. Similarly, ectopic expression of wild-type BAP1 suppressed anchorage-independent colony formation of NPC cells. Conclusion We characterized the genomic landscape of 128 NPC cases, and identified a number of novel driver genes with statistical and biological evidence. Integrated analysis showed enrichment of genetic lesions affecting chromatin modification, ERBB-PI3K signaling and autophagy machinery, offering opportunities for developing novel treatments. These results in aggregate provide an important genetic foundation for further study of the molecular pathology and etiology of this fatal disease. Citation Format: DECHEN LIN, Xuan Meng, Masaharu Hazawa, Yasunobu Nagata, Ana Maria Varela, Liang Xu, Yusuke Sato, Li-Zhen Liu, Ling-Wen Ding, Arjun Sharma, Boon Cher Goh, Soo Chin Lee, Bengt Fredrik Petersson, Feng Gang Yu, Paul Macary, Min Zin Oo, Soh Ha Chan, Henry Yang, Seishi Ogawa, H. Phillip Koeffler. The genomic landscape of nasopharyngeal carcinoma. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 3939. doi:10.1158/1538-7445.AM2015-3939

Published

2015

29. Abstract 5570: Laminin-5 gamma-2 (LAMC2) is highly expressed in anaplastic thyroid carcinoma and is associated with tumor progression, migration and invasion by modulating signaling of EGFR

Author

Vikas Madan, H. Phillip Koeffler, Meng Xuan, Deepika Kanojia, Jonathan W. Said, Henry Yang, Ngan B. Doan, Ling-Wen Ding, Manoj Garg, Wenwen Chien, Sigal Gery, Abhishek Sampath, Ryoko Okamoto, Gleen D Braunstein, and Li-Zhen Liu

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Cell cycle checkpoint, business.industry, Cell growth, Cell cycle, medicine.disease_cause, Small hairpin RNA, Oncology, Cell culture, Tumor progression, Cancer research, Gene silencing, Medicine, business, Carcinogenesis

Abstract

Context: Anaplastic thyroid carcinoma (ATC) is an aggressive malignancy having no effective treatment. Laminin subunit gamma-2 (LAMC2) is an epithelial basement membrane protein involved in cell migration and tumour invasion and might represent an ideal target for the development of novel therapeutic approaches for ATC. Objective: Study the role of LAMC2 in ATC tumorigenesis. Design: LAMC2 expression was evaluated by RT-PCR, western blotting and immunohistochemistry in tumor specimens, adjacent non-cancerous tissues and cell lines. shRNA approach was used to investigate the effect of LAMC2 knockdown on tumorigenesis of ATC. Results: LAMC2 was highly expressed in ATC samples and cell lines compared to normal thyroid tissues. Silencing LAMC2 by shRNA in ATC cells moderately inhibited cell growth in liquid culture and dramatically decreased growth in soft agar and in xenografts growing in immunodeficient mice. Silencing LAMC2 caused cell cycle arrest and significantly suppressed migration, invasion and wound healing of ATC cells. Rescue experiments by overexpressing LAMC2 in LAMC2 knockdown cells, reversed the inhibitory effects as shown by increased cell proliferation and colony formation. Microarray data demonstrated that LAMC2 shRNA significantly altered expression of genes associated with migration, invasion, proliferation and survival. Immunoprecipitation and co-localization experiments showed that LAMC2 bound to EGFR in ATC cells. Silencing LAMC2 partially blocked EGF-mediated activation of EGFR and its downstream pathway. Interestingly, cetuximab (EGFR blocking antibody) or EGFR siRNA additively enhanced the anti-proliferative activity of the LAMC2 knockdown ATC cells compared to control cells. Conclusions: To our knowledge, this is the first report investigating the effect of LAMC2 on cell growth, cell cycle, migration, invasion and EGFR signaling in ATC cells, suggesting that LAMC2 may be a potential therapeutic target for treatment of ATC. Citation Format: Manoj Garg, Deepika Kanojia, Ryoko Okamoto, Vikas Madan, Wenwen Chien, Abhishek Sampath, Ling-Wen Ding, Meng Xuan, Jonathan W Said, Ngan Doan, Li-Zhen Liu, Henry Yang, Sigal Gery, Gleen D Braunstein, H.Phillip Koeffler. Laminin-5 gamma-2 (LAMC2) is highly expressed in anaplastic thyroid carcinoma and is associated with tumor progression, migration and invasion by modulating signaling of EGFR. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 5570. doi:10.1158/1538-7445.AM2014-5570

Published

2014

30. Abstract 2225: Comprehensive molecular characterization of esophageal squamous cell carcinoma

Author

Manoj Garg, Yasunobu Nagata, Yusuke Okuno, Xuan Meng, De-Chen Lin, Ming-Rong Wang, Yusuke Sato, Henry Yang, Liang Xu, Ling-Wen Ding, Li-Zhen Liu, Phillip Koeffler, Seishi Ogawa, and Jia-Jie Hao

Subjects

Genetics, Cancer Research, Somatic cell, Cancer, Cell cycle, Biology, medicine.disease, Germline mutation, Oncology, medicine, Cancer research, Ectopic expression, Epigenetics, Copy-number variation, EP300

Abstract

Background Esophageal squamous cell carcinoma (ESCC) is a world-wide prevalent cancer, which is particularly common in certain regions of Asia. However, the genetic alterations of this disease have not been fully described. Methods We determined the mutational landscape of ESCC through whole-exome or targeted deep sequencing of 139 tumor/germline pairs. The somatic copy number variations (SCNV) of over 180 ESCC tumors were analyzed by SNP-array or array-CGH. Candidate driver mutations were mathematically calculated by the most updated algorithm MutSigCV, and the protein expression of which were thoroughly evaluated by immunohistochemistry. Finally, biological effects of candidate drivers were examined through functional studies in vitro and in vivo. Results Deep sequencing and computational analysis identified frequent and novel driver mutations affecting genes such as FAT1 (11.5%), ZNF750 (7.2%), EP300 (7.9%) and MLL2 (18.0%). FAT1 and ZNF750 genes were homozygouly deleted in 3.5% and 3.4% ESCCs, respectively, and their RNA transcripts and proteins were expressed at much lower levels in primary tumors compared to adjacent normal esophageal epithelial. Importantly, silencing of wild-type FAT1 or ZNF750 expression with siRNA/shRNAs significantly promoted cell proliferation and decreased cell differentiation, whereas ectopic expression of these genes resulted in opposite biological consequences. These genetic alterations and biological evidence strongly suggest that FAT1 and ZNF750 likely encode tumor suppressors which are frequently disrupted in ESCC. Furthermore, by integrating the landscape of somatic mutation, SCNV and protein dysregulation, we proposed that RTK-PI3K-MAPK pathways, cell cycle and epigenetic regulation are frequently altered by multiple molecular mechanisms in esophageal tumors. Finally, our systematic approaches uncovered many novel druggable candidates in this disease, such as FGFR1, ALK and XPO1. Conclusions By demonstrating the genomic landscape of over 180 ESCC cases, our integrated study unmasks a number of novel genetic lesions in ESCC and provides an important molecular foundation for understanding esophageal tumors and developing therapeutic targets. Citation Format: Dechen Lin, Xuan Meng, Liang Xu, Lingwen Ding, Manoj Garg, Henry Yang, Lizhen Liu, Jiajie Hao, Mingrong Wang, Yasunobu Nagata, Yusuke Sato, Yusuke Okuno, Seishi Ogawa, Phillip Koeffler. Comprehensive molecular characterization of esophageal squamous cell carcinoma. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 2225. doi:10.1158/1538-7445.AM2014-2225

Published

2014

31. Abstract 586: Genomic and functional characterizations of phosphodiesterase 4Din human cancers

Author

Jenny Lester, Martin J. Walsh, De-Chen Lin, Michèl Schummer, Nicole Urban, Patrick Tan, Danny Chan, Jonathan W. Said, Ngan B. Doan, Arjun Sharma, Liang Xu, Phillip Koeffler, Henry Yang, Craig J. Thomas, Jay Vadgama, Ling-Wen Ding, Li-Zhen Liu, Paresma R. Patel, and Beth Y. Karlan

Subjects

Gene isoform, Cancer Research, Melanoma, Phosphodiesterase, Cancer, Biology, medicine.disease, Molecular biology, chemistry.chemical_compound, PDE4D Gene, Oncology, chemistry, Cancer cell, medicine, Ectopic expression, Growth inhibition

Abstract

Background Phosphodiesterase 4D (PDE4D) degrades the secondary messenger adenosine 3’, 5’-cyclic monophosphate (cAMP). PDE4D recently was implicated in cancer cell proliferation, but alterations in its genome and function in tumors are unclear. Methods PDE4D gene copy number determined by SNP-CHIP was comprehensively analyzed in a large number of solid tumor specimens from diverse origins (n=5,569). Expression of PDE4D gene transcripts were examined in 971 primary tumors, as well as established cancer cell lines. PDE4D protein expression in 11 different types of cancers were evaluated by immunohistochemistry (n=165). Endogenous PDE4D in multiple types of tumor cell lines was suppressed by both shRNAs and compound 26B, a novel inhibitor of PDE4D, and the effects on apoptosis and proliferation were examined. We further investigated the molecular mechanisms involved. Effect of ectopic expression of PDE4D on tumor growth was assessed both in vitro and in vivo. Results Homozygous deletion of PDE4D occurred in 198 cases out of 5,569 primary solid tumors (3.56%), with most of them being internal microdeletions. Unexpectedly, these internal microdeletions did not result in loss of its gene products, as the expression of PDE4D mRNA and protein was not compromised in the PDE4D-microdeleted samples. Immunohistochemistry staining revealed that PDE4D protein levels were up-regulated in several types of tumors. Importantly, genetic and pharmacological suppression of endogenous PDE4D caused apoptosis and growth inhibition preferentially in a variety of cancer cells but not in non-malignant epithelial cells. We further showed that anti-tumor events triggered by PDE4D-suppression were lineage-dependently associated with induction of BIM and down-regulation of MITF. Moreover, ectopic expression of the PDE4D short isoform (PDE4D2) enhanced the proliferation of melanoma both in vitro and in vivo. Conclusions We show for the first time that although targeted by genomic homozygous microdeletions, alternatively spliced PDE4D can function as a tumor-promoting factor. PDE4D represents a novel, targetable enzyme of cancer cells. Citation Format: Dechen Lin, Liang Xu, Ling-Wen Ding, Arjun Sharma, Li-Zhen Liu, Henry Yang, Patrick Tan, Jay Vadgama, Beth Karlan, Jenny Lester, Nicole Urban, Michèl Schummer, Ngan Doan, Jonathan Said, Martin Walsh, Paresma Patel, Craig Thomas, Daniel Chan, Phillip Koeffler. Genomic and functional characterizations of phosphodiesterase 4Din human cancers. [abstract]. In: Proceedings of the 104th Annual Meeting of the American Association for Cancer Research; 2013 Apr 6-10; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2013;73(8 Suppl):Abstract nr 586. doi:10.1158/1538-7445.AM2013-586

Published

2013

32. Selective inhibition of unfolded protein response induces apoptosis in pancreatic cancer cells

Author

Phillip Koeffler, Su Lin Lim, Manoj Garg, Jin-Fen Xiao, Lorenz Poellinger, Shojiro Kitajima, Wenwen Chien, Itay Tokatly, Kian Leong Lee, Haibo Sun, Qiao-Yang Sun, Wei Zhong Leong, Sumiko Takao, Siew Zhuan Tan, Lucia A. Torres-Fernandez, Sigal Gery, and Ling-Wen Ding

Subjects

X-Box Binding Protein 1, pancreatic cancer, Apoptosis, UPR, Mice, SCID, Deoxycytidine, Bortezomib, chemistry.chemical_compound, 0302 clinical medicine, Mice, Inbred NOD, Pancreatic tumor, Enzyme Inhibitors, Toyocamycin, Sulfonamides, 0303 health sciences, Reverse Transcriptase Polymerase Chain Reaction, Cell Cycle, Drug Synergism, Cell cycle, Boronic Acids, 3. Good health, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Oncology, Pyrazines, 030220 oncology & carcinogenesis, RNA Interference, Growth inhibition, Research Paper, RNA Splicing, Blotting, Western, Regulatory Factor X Transcription Factors, Thiophenes, Naphthalenes, Protein Serine-Threonine Kinases, Biology, 03 medical and health sciences, Cell Line, Tumor, Pancreatic cancer, Endoribonucleases, medicine, Animals, Humans, Clonogenic assay, Cell Proliferation, 030304 developmental biology, Cell growth, Endoplasmic reticulum, IRE1α, medicine.disease, Xenograft Model Antitumor Assays, Gemcitabine, Molecular biology, Pancreatic Neoplasms, chemistry, Unfolded Protein Response, Cancer research, Unfolded protein response, Transcription Factors

Abstract

Endoplasmic reticulum stress from unfolded proteins is associated with the proliferation of pancreatic tumor cells, making the many regulatory molecules of this pathway appealing targets for therapy. The objective of our study was to assess potential therapeutic efficacy of inhibitors of unfolded protein response (UPR) in pancreatic cancers focusing on IRE1α inhibitors. IRE1α-mediated XBP-1 mRNA splicing encodes a transcription factor that enhances transcription of chaperone proteins in order to reverse UPR. Proliferation assays using a panel of 14 pancreatic cancer cell lines showed a dose- and time-dependent growth inhibition by IRE1α-specific inhibitors (STF-083010, 2-Hydroxy-1-naphthaldehyde, 3-Ethoxy-5,6-dibromosalicylaldehyde, toyocamycin). Growth inhibition was also noted using a clonogenic growth assay in soft agar, as well as a xenograft in vivo model of pancreatic cancer. Cell cycle analysis showed that these IRE1α inhibitors caused growth arrest at either the G1 or G2/M phases (SU8686, MiaPaCa2) and induced apoptosis (Panc0327, Panc0403). Western blot analysis showed cleavage of caspase 3 and PARP, and prominent induction of the apoptotic molecule BIM. In addition, synergistic effects were found between either STF-083010, 2-Hydroxy-1-naphthaldehyde, 3-Ethoxy-5,6-dibromosalicylaldehyde, or toyocamycin and either gemcitabine or bortezomib. Our data suggest that use of an IRE1α inhibitor is a novel therapeutic approach for treatment of pancreatic cancers.

33. SOX7 is down-regulated in lung cancer

Author

Wenwen Chien, Makoto Sudo, Takahide Hayano, Dong Xie, H. Phillip Koeffler, Dong Yin, Ling-Wen Ding, Seiichi Mori, Manoj Garg, Geraldine Leong, Norihiko Kawamata, Shuo Shi, and Patrick Tan

Subjects

Cancer Research, Lung Neoplasms, Apoptosis, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, SOXF Transcription Factors, 2.1 Biological and endogenous factors, Epidermal growth factor receptor, Aetiology, Non-Small-Cell Lung, Lung, Cancer, 0303 health sciences, Tumor, Smoking, Cell Cycle, Single Nucleotide, CNAG, Gene Expression Regulation, Neoplastic, ErbB Receptors, Oncology, 030220 oncology & carcinogenesis, Lung cancer, SOX7, Receptor, Tumor suppressor gene, DNA Copy Number Variations, Oncology and Carcinogenesis, Copy number analysis, Down-Regulation, Biology, Polymorphism, Single Nucleotide, Cell Line, 03 medical and health sciences, Clinical Research, Cell Line, Tumor, Genetics, medicine, Humans, Oncology & Carcinogenesis, Polymorphism, SNP-Chip, Gene, neoplasms, 030304 developmental biology, Neoplastic, Epidermal Growth Factor, Cell growth, Research, Human Genome, Carcinoma, DNA Methylation, medicine.disease, Promoter methylation, Molecular biology, respiratory tract diseases, Gene Expression Regulation, Cell culture, Mutation, Cancer research, biology.protein, Genome-Wide Association Study

Abstract

Background SOX7 is a transcription factor belonging to the SOX family. Its role in lung cancer is unknown. Methods In this study, whole genomic copy number analysis was performed on a series of non-small cell lung cancer (NSCLC) cell lines and samples from individuals with epidermal growth factor receptor (EGFR) mutations using a SNP-Chip platform. SOX7 was measured in NSCLC samples and cell lines, and forced expressed in one of these lines. Results A notable surprise was that the numerous copy number (CN) changes observed in samples of Asian, non-smoking EGFR mutant NSCLC were nearly the same as those CN alterations seen in a large collection of NSCLC from The Cancer Genome Atlas which is presumably composed of predominantly Caucasians who often smoked. However, four regions had CN changes fairly unique to the Asian EGFR mutant group. We also examined CN changes in NSCLC lines. The SOX7 gene was homozygously deleted in one (HCC2935) of 10 NSCLC cell lines and heterozygously deleted in two other NSCLC lines. Expression of SOX7 was significantly downregulated in NSCLC cell lines (8/10, 80%) and a large collection of NSCLC samples compared to matched normal lung (57/62, 92%, p= 0.0006). Forced-expression of SOX7 in NSCLC cell lines markedly reduced their cell growth and enhanced their apoptosis. Conclusion These data suggest that SOX7 is a novel tumor suppressor gene silenced in the majority of NSCLC samples.