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1. Phase II Study of Enzalutamide for Patients With Androgen Receptor–Positive Salivary Gland Cancers (Alliance A091404)

Author

Alan L. Ho, Nathan R. Foster, Alex J. Zoroufy, Jordan D. Campbell, Francis Worden, Katharine Price, Douglas Adkins, Daniel W. Bowles, Hyunseok Kang, Barbara Burtness, Eric Sherman, Roscoe Morton, Luc G.T. Morris, Zaineb Nadeem, Nora Katabi, Pamela Munster, and Gary K. Schwartz

Subjects
Male, Cancer Research, Oncology, Receptors, Androgen, Nitriles, Phenylthiohydantoin, Humans, Female, Androgen Antagonists, Salivary Gland Neoplasms
Abstract

PURPOSE The androgen receptor (AR) is expressed (+) in a subset of salivary gland cancers (SGCs). This phase II trial evaluated the efficacy of the antiandrogen enzalutamide in AR+ SGC. METHODS Patients with locally advanced/unresectable or metastatic AR+ SGCs were enrolled. Enzalutamide (160 mg) was given orally once daily. The primary end point was the best overall response rate per RECIST v1.1 within eight cycles. Confirmed responses in ≥ 5 of 41 patients would be considered promising. Secondary end points were progression-free survival, overall survival, and safety. RESULTS Forty-six patients were enrolled; 30 (65.2%) received prior systemic therapy, including 13 (28.3%) with AR-targeted drugs. Of seven (15.2%) partial responses (PRs), only two (4.3%) were confirmed per protocol and counted toward the primary end point. Twenty-four patients (52.2%) had stable disease; 15 (32.6%) had progression of disease as best response. Twenty-six patients (56.5%) experienced tumor regression in target lesions; 18 (39.1%) had partial response/stable disease ≥ 6 months. Tumor regressions were observed in female patients (5 of 6 [83.3%]) and those who received prior AR– (6 of 13 [46.2%]) or human epidermal growth factor receptor 2–targeted therapies (5 of 8 [62.5%]). Three patients remained on treatment at data cutoff (duration, 32.2-49.8 months). The median progression-free survival was 5.6 months (95% CI, 3.7 to 7.5); the median overall survival was 17.0 months (95% CI, 11.8 to 30.0). The most common adverse events were fatigue, hypertension, hot flashes, and weight loss. Total and free testosterone levels increased by a mean of 61.2% and 48.8%, respectively, after enzalutamide. CONCLUSION Enzalutamide demonstrated limited activity in AR+ SGC, failing to meet protocol-defined success in part because of a lack of response durability. Strategies to enhance the efficacy of antiandrogen therapy are needed.

Published
2022
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2. Data from Genomic and Transcriptomic Correlates of Thyroid Carcinoma Evolution after BRAF Inhibitor Therapy

Author

Luc G.T. Morris, James A. Fagin, Timothy A. Chan, Alan L. Ho, Eric J. Sherman, Richard J. Wong, Snjezana Dogan, Vladimir Makarov, Neal Patel, Zaineb Nadeem, Cristina Valero, Fengshen Kuo, Catherine Han, Ronald Ghossein, Bin Xu, Brian R. Untch, and Mark Lee

Abstract

Targeted inhibition of BRAF V600E achieves tumor control in a subset of advanced thyroid tumors. Nearly all tumors develop resistance, and some have been observed to subsequently undergo dedifferentiation. The molecular alterations associated with thyroid cancer dedifferentiation in the setting of BRAF inhibition are unknown. We analyzed targeted next-generation sequencing data from 639 advanced, recurrent and/or metastatic thyroid carcinomas, including 15 tumors that were treated with BRAF inhibitor drugs and had tissue sampled during or posttreatment, 8 of which had matched pretherapy samples. Pre- and posttherapy tissues from one additional patient were profiled with whole-exome sequencing and RNA expression profiling. Mutations in genes comprising the SWI/SNF chromatin remodeling complex and the PI3K–AKT–mTOR, MAPK, and JAK–STAT pathways all increased in prevalence across more dedifferentiated thyroid cancer histologies. Of 7 thyroid cancers that dedifferentiated after BRAF inhibition, 6 had mutations in these pathways. These mutations were mostly absent from matched pretreatment samples and were rarely detected in tumors that did not dedifferentiate. Additional analyses in one of the vemurafenib-treated tumors before and after anaplastic transformation revealed the emergence of an oncogenic PIK3CA mutation, activation of ERK signaling, dedifferentiation, and development of an immunosuppressive tumor microenvironment. These findings validate earlier preclinical data implicating these genetic pathways in resistance to BRAF inhibitors, and suggest that genetic alterations mediating acquired drug resistance may also promote thyroid tumor dedifferentiation.Implications:The possibility that thyroid cancer dedifferentiation may be attributed to selective pressure applied by BRAF inhibitor–targeted therapy should be investigated further.

Published
2023
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3. Supplemental Figures 1-6 from Genomic and Transcriptomic Correlates of Thyroid Carcinoma Evolution after BRAF Inhibitor Therapy

Author

Luc G.T. Morris, James A. Fagin, Timothy A. Chan, Alan L. Ho, Eric J. Sherman, Richard J. Wong, Snjezana Dogan, Vladimir Makarov, Neal Patel, Zaineb Nadeem, Cristina Valero, Fengshen Kuo, Catherine Han, Ronald Ghossein, Bin Xu, Brian R. Untch, and Mark Lee

Abstract

Supplemental Figure 1. Increased clonal heterogeneity in anaplastic metastases (ATC Met 1, 5 clones Supplemental Figure 2. Copy-number alterations for the pre-vemurafenib papillary thyroid carcinoma sample Supplemental Figure 3. Differentially expressed gene analyses comparing pre-treatment PTC sample and ATC metastases in MSK-THY1. Supplemental Figure 4. Prevalence of genetic alterations linked to BRAF inhibitor resistance and/or ATC pathogenesis in primary TCGA PTCs and metastatic/recurrent PTCs, PDTCs, and ATCs sequenced by MSK-IMPACT. Supplemental Figure 5. Histology and immunohistochemical studies for MSK-THY6. Supplemental Figure 6. Mutational landscape of tumors that underwent dedifferentiation subsequent to BRAF inhibitor targeted therapy with vemurafenib or dabrafenib.

Published
2023
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4. Supplemental Tables 1-5 from Genomic and Transcriptomic Correlates of Thyroid Carcinoma Evolution after BRAF Inhibitor Therapy

Author

Luc G.T. Morris, James A. Fagin, Timothy A. Chan, Alan L. Ho, Eric J. Sherman, Richard J. Wong, Snjezana Dogan, Vladimir Makarov, Neal Patel, Zaineb Nadeem, Cristina Valero, Fengshen Kuo, Catherine Han, Ronald Ghossein, Bin Xu, Brian R. Untch, and Mark Lee

Abstract

Supplemental Table 1. Genomic alterations observed in MSK-THY1 Supplemental Table 2. Cellular prevalence of single nucleotide variants in MSK-THY Supplemental Table 3. Normalized gene expression data from patient MSK-THY1 Supplemental Table 4. Mutational data for 639 thyroid tumors sequenced by MSK-IMPACT Supplemental Table 5. Mutational data for BRAFi treated thyroid cancers with post-treatment sequencing

Published
2023
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5. Genomic and Transcriptomic Correlates of Thyroid Carcinoma Evolution after BRAF Inhibitor Therapy

Author

Timothy A. Chan, Eric J. Sherman, Catherine Han, Zaineb Nadeem, Vladimir Makarov, Alan L. Ho, James A. Fagin, Mark Lee, Bin Xu, Richard J. Wong, Snjezana Dogan, Neal Patel, Cristina Valero, Ronald Ghossein, Luc G. T. Morris, Fengshen Kuo, and Brian R. Untch

Subjects
Male, Proto-Oncogene Proteins B-raf, Cancer Research, endocrine system diseases, medicine.medical_treatment, Article, Targeted therapy, Thyroid carcinoma, Transcriptome, Tumor Microenvironment, Humans, Medicine, Thyroid Neoplasms, Protein Kinase Inhibitors, Molecular Biology, Thyroid cancer, Exome sequencing, PI3K/AKT/mTOR pathway, Tumor microenvironment, business.industry, Thyroid, Genomics, medicine.disease, medicine.anatomical_structure, Oncology, Cancer research, Female, business
Abstract

Targeted inhibition of BRAF V600E achieves tumor control in a subset of advanced thyroid tumors. Nearly all tumors develop resistance, and some have been observed to subsequently undergo dedifferentiation. The molecular alterations associated with thyroid cancer dedifferentiation in the setting of BRAF inhibition are unknown. We analyzed targeted next-generation sequencing data from 639 advanced, recurrent and/or metastatic thyroid carcinomas, including 15 tumors that were treated with BRAF inhibitor drugs and had tissue sampled during or posttreatment, 8 of which had matched pretherapy samples. Pre- and posttherapy tissues from one additional patient were profiled with whole-exome sequencing and RNA expression profiling. Mutations in genes comprising the SWI/SNF chromatin remodeling complex and the PI3K–AKT–mTOR, MAPK, and JAK–STAT pathways all increased in prevalence across more dedifferentiated thyroid cancer histologies. Of 7 thyroid cancers that dedifferentiated after BRAF inhibition, 6 had mutations in these pathways. These mutations were mostly absent from matched pretreatment samples and were rarely detected in tumors that did not dedifferentiate. Additional analyses in one of the vemurafenib-treated tumors before and after anaplastic transformation revealed the emergence of an oncogenic PIK3CA mutation, activation of ERK signaling, dedifferentiation, and development of an immunosuppressive tumor microenvironment. These findings validate earlier preclinical data implicating these genetic pathways in resistance to BRAF inhibitors, and suggest that genetic alterations mediating acquired drug resistance may also promote thyroid tumor dedifferentiation. Implications: The possibility that thyroid cancer dedifferentiation may be attributed to selective pressure applied by BRAF inhibitor–targeted therapy should be investigated further.

Published
2022
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13. Supplementary figure and table legends from The Immune Microenvironment and Neoantigen Landscape of Aggressive Salivary Gland Carcinomas Differ by Subtype

Author

Luc G.T. Morris, Timothy A. Chan, Alan L. Ho, Nadeem Riaz, Richard J. Wong, A. Ari Hakimi, Ian Ganly, Snjezana Dogan, Diego Chowell, Vladimir Makarov, Martin G. Dalin, Zaineb Nadeem, Mark Lee, Nora Katabi, Fengshen Kuo, and Maximilian Linxweiler

Abstract

Supplementary figure and table legends

Published
2023
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17. Data from The Immune Microenvironment and Neoantigen Landscape of Aggressive Salivary Gland Carcinomas Differ by Subtype

Author

Luc G.T. Morris, Timothy A. Chan, Alan L. Ho, Nadeem Riaz, Richard J. Wong, A. Ari Hakimi, Ian Ganly, Snjezana Dogan, Diego Chowell, Vladimir Makarov, Martin G. Dalin, Zaineb Nadeem, Mark Lee, Nora Katabi, Fengshen Kuo, and Maximilian Linxweiler

Abstract

Purpose:Salivary gland carcinomas (SGC) are rare, aggressive cancers with high rates of recurrence and distant metastasis. These factors, and a lack of active systemic therapies, contribute to poor clinical outcome. Response rates with immune checkpoint blockade have been low, although clinical data remain sparse. To improve the efficacy of therapies, a more comprehensive understanding of relevant molecular alterations and immunologic processes is needed.Experimental Design:To characterize the immune microenvironment and neoantigen landscape of SGCs, we performed RNA sequencing (RNA-seq) in 76 tumors representing the three most lethal histologies: adenoid cystic carcinoma (ACC), myoepithelial carcinoma (MECA), and salivary duct carcinoma (SDC). We analyzed transcriptomic profiles, tumor-infiltrating immune cell populations, and measures of T-cell activation/dysfunction. In 37 cases also undergoing exome sequencing, we analyzed somatic mutations and neoantigens.Results:SDCs exhibited high levels of immune infiltration, with corresponding higher levels of T-cell dysfunction, and higher mutational load. In contrast, ACCs were characterized by an immune-excluded microenvironment, the presence of M2-polarized macrophages and myeloid-derived suppressor cells, and very low mutational load. MECAs were more heterogeneous, with both immune-low and immune-high phenotypes represented. Across all SGCs, levels of immune infiltration were associated with mutation- and fusion-derived neoantigens, and with aggressive clinical behavior.Conclusions:These findings provide new insights into the immune microenvironment and neoantigen landscape of SGCs, showing that mechanisms of immune escape appear to differ by histology. These data nominate potential immunologic vulnerabilities and may help guide the next steps of investigation in precision immunotherapy for these difficult-to-treat cancers.

Published
2023
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29. Immunogenic neoantigens derived from gene fusions stimulate T cell responses

Author

Justin Tepe, Alan L. Ho, Robert M. Samstein, Nora Katabi, Fengshen Kuo, Raghvendra M. Srivastava, Marc Cohen, Nadeem Riaz, Kety Huberman, Zaineb Nadeem, S. Ken Tian, Timothy A. Chan, Chirag Krishna, Richard J. Wong, Phaedra Agius, Kanika Arora, Douglas R. Hoen, Katelynd Vanness, Nancy Bouvier, Ronald Ghossein, Rajarsi Mandal, Wei Yang, Martin G. Dalin, Ken-Wing Lee, Vladimir Makarov, Jonathan J. Havel, Diego Chowell, Heather Geiger, Luc G. T. Morris, Leonard H. Wexler, Nicolas Robine, Jennifer S. Sims, Neerav Shukla, and Ian Ganly

Subjects
0301 basic medicine, Chromosomal Proteins, Non-Histone, T-Lymphocytes, medicine.medical_treatment, Programmed Cell Death 1 Receptor, medicine.disease_cause, Fusion gene, 0302 clinical medicine, Cancer immunotherapy, Neoplasms, Cytotoxic T cell, Poly-ADP-Ribose Binding Proteins, Complete response, Oncogene Proteins, Mutation, Applied Mathematics, Nuclear Proteins, General Medicine, 3. Good health, medicine.anatomical_structure, Head and Neck Neoplasms, 030220 oncology & carcinogenesis, Immunotherapy, Gene Fusion, General Mathematics, Recombinant Fusion Proteins, T cell, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Proto-Oncogene Proteins c-myb, 03 medical and health sciences, Antigen, Antigens, Neoplasm, medicine, Humans, Gene, Whole Genome Sequencing, business.industry, Squamous Cell Carcinoma of Head and Neck, Head and neck cancer, Cancer, medicine.disease, Head and neck squamous-cell carcinoma, Fusion protein, NFI Transcription Factors, 030104 developmental biology, Cancer research, business, T-Lymphocytes, Cytotoxic
Abstract

Anti-tumor immunity is driven by self versus non-self discrimination. Many immunotherapeutic approaches to cancer have taken advantage of tumor neoantigens derived from somatic mutations. Here, we demonstrate that gene fusions are a source of immunogenic neoantigens that can mediate responses to immunotherapy. We identified an exceptional responder with metastatic head and neck cancer who experienced a complete response to immune checkpoint inhibitor therapy, despite a low mutational load and minimal pre-treatment immune infiltration in the tumor. Using whole-genome sequencing and RNA sequencing, we identified a novel gene fusion and demonstrated that it produces a neoantigen that can specifically elicit a host cytotoxic T cell response. In a cohort of head and neck tumors with low mutation burden, minimal immune infiltration and prevalent gene fusions, we also identified gene fusion-derived neoantigens that generate cytotoxic T cell responses. Finally, analyzing additional datasets of fusion-positive cancers, including checkpoint-inhibitor-treated tumors, we found evidence of immune surveillance resulting in negative selective pressure against gene fusion-derived neoantigens. These findings highlight an important class of tumor-specific antigens and have implications for targeting gene fusion events in cancers that would otherwise be less poised for response to immunotherapy, including cancers with low mutational load and minimal immune infiltration. Fusion proteins in cancers with low mutational burden represent functional neoantigens that elicit T cell activation and mediate responses to immunotherapy.

Published
2019
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30. The Immune Microenvironment and Neoantigen Landscape of Aggressive Salivary Gland Carcinomas Differ by Subtype

Author

Martin G. Dalin, Vladimir Makarov, Richard J. Wong, Nora Katabi, Mark Lee, Luc G. T. Morris, Alan L. Ho, Snjezana Dogan, Nadeem Riaz, Zaineb Nadeem, Timothy A. Chan, A. Ari Hakimi, Maximilian Linxweiler, Diego Chowell, Fengshen Kuo, and Ian Ganly

Subjects
0301 basic medicine, Adult, Male, Cancer Research, Adenoid cystic carcinoma, medicine.medical_treatment, Biology, Article, Salivary duct carcinoma, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Immune system, Lymphocytes, Tumor-Infiltrating, Antigen, Antigens, Neoplasm, Antineoplastic Combined Chemotherapy Protocols, Exome Sequencing, medicine, Biomarkers, Tumor, Tumor Microenvironment, Humans, Exome sequencing, Aged, Aged, 80 and over, Sequence Analysis, RNA, Immunotherapy, biochemical phenomena, metabolism, and nutrition, Middle Aged, medicine.disease, Prognosis, Salivary Gland Neoplasms, Immunohistochemistry, Immune checkpoint, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Mutation, Cancer research, Female, Follow-Up Studies
Abstract

Purpose: Salivary gland carcinomas (SGC) are rare, aggressive cancers with high rates of recurrence and distant metastasis. These factors, and a lack of active systemic therapies, contribute to poor clinical outcome. Response rates with immune checkpoint blockade have been low, although clinical data remain sparse. To improve the efficacy of therapies, a more comprehensive understanding of relevant molecular alterations and immunologic processes is needed. Experimental Design: To characterize the immune microenvironment and neoantigen landscape of SGCs, we performed RNA sequencing (RNA-seq) in 76 tumors representing the three most lethal histologies: adenoid cystic carcinoma (ACC), myoepithelial carcinoma (MECA), and salivary duct carcinoma (SDC). We analyzed transcriptomic profiles, tumor-infiltrating immune cell populations, and measures of T-cell activation/dysfunction. In 37 cases also undergoing exome sequencing, we analyzed somatic mutations and neoantigens. Results: SDCs exhibited high levels of immune infiltration, with corresponding higher levels of T-cell dysfunction, and higher mutational load. In contrast, ACCs were characterized by an immune-excluded microenvironment, the presence of M2-polarized macrophages and myeloid-derived suppressor cells, and very low mutational load. MECAs were more heterogeneous, with both immune-low and immune-high phenotypes represented. Across all SGCs, levels of immune infiltration were associated with mutation- and fusion-derived neoantigens, and with aggressive clinical behavior. Conclusions: These findings provide new insights into the immune microenvironment and neoantigen landscape of SGCs, showing that mechanisms of immune escape appear to differ by histology. These data nominate potential immunologic vulnerabilities and may help guide the next steps of investigation in precision immunotherapy for these difficult-to-treat cancers.

Published
2019

31. Nucleolin phosphorylation regulates PARN deadenylase activity during cellular stress response

Author

Shu Xiao, Emral Devany, Kenneth Ng, Rachele Dolce Rameau, Anjana Saxena, Xiaokan Zhang, Frida E. Kleiman, Zaineb Nadeem, and Elif Caglar

Subjects
0301 basic medicine, Ultraviolet Rays, Biology, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Stress, Physiological, Cellular stress response, Gene expression, microRNA, Humans, Phosphorylation, Casein Kinase II, Molecular Biology, RNA-Binding Proteins, Translation (biology), Cell Biology, Phosphoproteins, Research Papers, Cell biology, Enzyme Activation, 030104 developmental biology, Gene Expression Regulation, Proto-Oncogene Proteins c-bcl-2, 030220 oncology & carcinogenesis, Phosphoprotein, Exoribonucleases, Tumor Suppressor Protein p53, Nucleolin
Abstract

Nucleolin (NCL) is an abundant stress-responsive, RNA-binding phosphoprotein that controls gene expression by regulating either mRNA stability and/or translation. NCL binds to the AU-rich element (ARE) in the 3'UTR of target mRNAs, mediates miRNA functions in the nearby target sequences, and regulates mRNA deadenylation. However, the mechanism by which NCL phosphorylation affects these functions and the identity of the deadenylase involved, remain largely unexplored. Earlier we demonstrated that NCL phosphorylation is vital for cell cycle progression and proliferation, whereas phosphorylation-deficient NCL at six consensus CK2 sites confers dominant-negative effect on proliferation by increasing p53 expression, possibly mimicking cellular DNA damage conditions. In this study, we show that NCL phosphorylation at those CK2 consensus sites in the N-terminus is necessary to induce deadenylation upon oncogenic stimuli and UV stress. NCL-WT, but not hypophosphorylated NCL-6/S*A, activates poly (A)-specific ribonuclease (PARN) deadenylase activity. We further demonstrate that NCL interacts directly with PARN, and under non-stress conditions also forms (a) complex (es) with factors that regulate deadenylation, such as p53 and the ARE-binding protein HuR. Upon UV stress, the interaction of hypophosphorylated NCL-6/S*A with these proteins is favored. As an RNA-binding protein, NCL interacts with PARN deadenylase substrates such as TP53 and BCL2 mRNAs, playing a role in their downregulation under non-stress conditions. For the first time, we show that NCL phosphorylation offers specificity to its protein-protein, protein-RNA interactions, resulting in the PARN deadenylase regulation, and hence gene expression, during cellular stress responses.

Published
2017

32. Multi-dimensional genomic analysis of myoepithelial carcinoma identifies prevalent oncogenic gene fusions

Author

Marta Persson, Ian Ganly, Vladimir Makarov, Kalyani Chadalavada, Timothy A. Chan, Alexis Desrichard, Nora Katabi, Luc G. T. Morris, Logan A. Walsh, Alan L. Ho, Cristina R. Antonescu, Ronald Ghossein, Ken-Wing Lee, Zaineb Nadeem, Lyndsay West, Martin G. Dalin, Deepa Ramaswami, Fengshen Kuo, Göran Stenman, Jonathan J. Havel, Nadeem Riaz, and Gouri Nanjangud

Subjects
Male, 0301 basic medicine, Oncogene Proteins, Fusion, Oncogene Proteins, General Physics and Astronomy, medicine.disease_cause, physiological processes, Myoepithelioma, 0302 clinical medicine, polycyclic compounds, lcsh:Science, In Situ Hybridization, Fluorescence, Aged, 80 and over, Mutation, Multidisciplinary, Genomics, Middle Aged, Salivary Gland Neoplasms, Phenotype, 3. Good health, Nuclear DNA, DNA-Binding Proteins, 030220 oncology & carcinogenesis, Female, Adult, Adolescent, Science, Biology, Article, General Biochemistry, Genetics and Molecular Biology, Young Adult, 03 medical and health sciences, Cell Line, Tumor, medicine, Humans, Oncogene Fusion, Receptor, Fibroblast Growth Factor, Type 1, Gene, Aged, Oncogene, Cancer, Sequence Analysis, DNA, General Chemistry, biochemical phenomena, metabolism, and nutrition, bacterial infections and mycoses, medicine.disease, HEK293 Cells, 030104 developmental biology, Salivary gland cancer, Cancer research, bacteria, lcsh:Q
Abstract

Myoepithelial carcinoma (MECA) is an aggressive salivary gland cancer with largely unknown genetic features. Here we comprehensively analyze molecular alterations in 40 MECAs using integrated genomic analyses. We identify a low mutational load, and high prevalence (70%) of oncogenic gene fusions. Most fusions involve the PLAG1 oncogene, which is associated with PLAG1 overexpression. We find FGFR1-PLAG1 in seven (18%) cases, and the novel TGFBR3-PLAG1 fusion in six (15%) cases. TGFBR3-PLAG1 promotes a tumorigenic phenotype in vitro, and is absent in 723 other salivary gland tumors. Other novel PLAG1 fusions include ND4-PLAG1; a fusion between mitochondrial and nuclear DNA. We also identify higher number of copy number alterations as a risk factor for recurrence, independent of tumor stage at diagnosis. Our findings indicate that MECA is a fusion-driven disease, nominate TGFBR3-PLAG1 as a hallmark of MECA, and provide a framework for future diagnostic and therapeutic research in this lethal cancer., Myoepithelial carcinoma (MECA) is a rare aggressive salivary gland cancer. Here, the authors analyze the genomic landscape of MECA and identify a high prevalence of oncogenic gene fusions, primarily PLAG1 fusions, highlighting TGFBR3-PLAG1 as a potential hallmark of MECA.

Published
2017
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33. Multi-dimensional genomic analysis of myoepithelial carcinoma identifies prevalent oncogenic gene fusions

Author

Luc G. T. Morris, Gouri Nanjangud, Ken-Wing Lee, Göran Stenman, Kalyani Chadalavada, Jonathan J. Havel, Deepa Ramaswami, Martin G. Dalin, Cristina R. Antonescu, Marta Persson, Fengshen Kuo, Nadeem Riaz, Logan A. Walsh, Zaineb Nadeem, Lyndsay West, Alan L. Ho, Nora Katabi, Ronald Ghossein, Alexis Desrichard, Timothy A. Chan, and Vladimir Makarov

Subjects
Genetics, 0303 health sciences, Salivary gland, Oncogene, Cancer, Biology, biochemical phenomena, metabolism, and nutrition, medicine.disease, Major histocompatibility complex, Phenotype, 3. Good health, Nuclear DNA, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Salivary gland cancer, 030220 oncology & carcinogenesis, medicine, biology.protein, Gene, 030304 developmental biology
Abstract

Myoepithelial carcinoma (MECA) is an aggressive type of salivary gland cancer with largely unknown molecular features. MECA may arise de novo or result from oncogenic transformation of a pre-existing pleomorphic adenoma (MECA ex-PA). We comprehensively analyzed the molecular alterations in MECA with integrated genomic analyses. We identified a low mutational load (0.5/MB), but a high prevalence of fusion oncogenes (28/40 tumors; 70%). We foundFGFR1-PLAG1in 7 (18%) cases, and the novelTGFBR3-PLAG1fusion in 6 (15%) cases.TGFBR3-PLAG1was specific for MECA de novo tumors or the malignant component of MECA ex-PA, was absent in 723 other salivary gland tumors, and promoted a tumorigenic phenotype in vitro. We discovered other novelPLAG1fusions, includingND4-PLAG1,which is an oncogenic fusion between mitochondrial and nuclear DNA. One tumor harbored anMSN-ALKfusion, which was tumorigenic in vitro, and targetable with ALK inhibitors. Certain gene fusions were predicted to result in neoantigens with high MHC binding affinity. A high number of copy number alterations was associated with poorer prognosis. Our findings indicate that MECA is a fusion-driven disease, nominateTGFBR3-PLAG1as a hallmark of MECA, and provide a framework for future steps of diagnostic and therapeutic research in this lethal cancer.

Published
2017
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34. Induced Expression of Nucleolin Phosphorylation-Deficient Mutant Confers Dominant-Negative Effect on Cell Proliferation

Author

Benjamin Trinité, Zaineb Nadeem, Anjana Saxena, Shu Xiao, Dibash K. Das, Xin Li, Angela Chi, Priscilla Maldonado, and Elif Caglar

Subjects
Gene Expression, lcsh:Medicine, Apoptosis, Biochemistry, Suppressor Genes, 0302 clinical medicine, Cell Cycle and Cell Division, Phosphorylation, Post-Translational Modification, Casein Kinase II, lcsh:Science, Genes, Dominant, Cellular Stress Responses, 0303 health sciences, Multidisciplinary, Cell Death, biology, Protein Stability, Kinase, RNA-Binding Proteins, 3. Good health, Cell biology, Ubiquitin ligase, Subcellular Localization, Cell Processes, 030220 oncology & carcinogenesis, Cellular Structures and Organelles, Casein kinase 2, Half-Life, Research Article, Transcriptional Activation, Tumor Suppressor Genes, 03 medical and health sciences, Gene Types, Cell Line, Tumor, Genetics, Humans, Mitosis, Cell Proliferation, 030304 developmental biology, Cyclin-dependent kinase 1, Cell growth, lcsh:R, Biology and Life Sciences, Proteins, Nucleolus, Cell Biology, Phosphoproteins, Molecular biology, Amino Acid Substitution, biology.protein, lcsh:Q, Tumor Suppressor Protein p53, Apoptosis Regulatory Proteins, Protein Processing, Post-Translational, Nucleolin
Abstract

Nucleolin (NCL) is a major nucleolar phosphoprotein that has pleiotropic effects on cell proliferation and is elevated in a variety of tumors. NCL is highly phosphorylated at the N-terminus by two major kinases: interphase casein kinase 2 (CK2) and mitotic cyclin-dependent kinase 1 (CDK1). Earlier we demonstrated that a NCL-mutant that is partly defective in undergoing phosphorylation by CK2 inhibits chromosomal replication through its interactions with Replication Protein A, mimicking the cellular response to DNA damage. We further delineated that the N-terminus of NCL associates with Hdm2, the most common E3 ubiquitin ligase of p53. We reported that NCL antagonizes Hdm2 to stabilize p53 and stimulates p53 transcriptional activity. Although NCL-phosphorylation by CK2 and ribosomal DNA transcription are closely coordinated during interphase, the role of NCL phosphorylation in regulating cell proliferation remains unexplored. We have therefore engineered unique human cells that specifically induce expression of NCL-wild type (WT) or a phosphorylation-deficient NCL-mutant, 6/S*A where all the six CK2 consensus serine sites residing in the N-terminus NCL were mutated to alanine. Here we show that this NCL-mutant is defective in undergoing phosphorylation by CK2. We also demonstrate that NCL-phosphorylation by CK2 is required through the S-phase progression in cell cycle and hence proliferation. Induced expression of NCL with mutated CK2 phosphorylation sites stabilizes p53, results in higher expression of Bcl2 (B-cell lymphoma 2) homology 3 (BH3)-only apoptotic markers and causes a dominant-negative effect on cell viability. Our unique cellular system thus provides the first evidential support to delineate phospho-specific functions of NCL on cell proliferation.

Published
2014
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35. The clinical and biologic impact of PPP6C mutations in melanoma

Author

Zaineb Nadeem, Nathaniel H. Fleming, Jiaying Tian, Heidi L. Gold, Eleazar Vega-Saenz de Miera, Lawrence B. Gardner, Eva Hernando-Monge, Richard L. Shapiro, Jordan Wengrod, and Iman Osman

Subjects
Cancer Research, Oncology, DNA repair, Cell growth, business.industry, Melanoma, Cancer research, Medicine, Affect (psychology), business, medicine.disease
Abstract

9067 Background: PP6C binds to regulatory units to affect a number of important pathways including cell proliferation and DNA repair. Recently two independent groups reported for the first time the presence of somatic mutations in the PPP6C gene in ~10% of short term cultures and limited number of human melanoma tissues. However, the clinical or biological relevance of PPP6C mutations in melanoma patients is unknown. Our objectives were to examine the clinical relevance of PPP6C mutations in a well characterized cohort of melanoma specimens linked to extensive, prospectively-collected clinical information and to explore the functional consequence of different categories of mutations. Methods: Sanger dideoxy sequencing was performed on PCR-amplified DNA from macro-dissected FFPE tumors. Associations between PPP6C mutations and baseline characteristics, recurrence, survival, and BRAF/ NRAS mutational status were examined. The impact of mutations on binding PP6C regulatory units was assessed as well as the effect on additional downstream pathways. Results: 308 primary melanoma patients (118 Stage I, 92 Stage II, and 98 Stage III) were examined (median follow up: 5.3 years). 50 PPP6C mutations in 33 patients (10.7%) were identified with 11 tumors harboring more than one mutation. One mutation (R301C) was identified in 6 patients. PPP6C mutations occurred with similar frequencies across stages and showed no association with BRAF or NRAS mutations. Mutations were categorized into 3 groups: Mutations resulting in premature stop codon (n=9), those occurring in the active site (n=16) and others (n=8). 8/9 (89%) patients with stop mutations recurred and developed visceral metastases. Functional studies revealed that PPP6C mutants also behaved differently; some PPP6C mutations led to decreased binding to regulatory subunits, others, including the R301C mutation did not. Conclusions: Our data suggest that PPP6C mutation is an early event in melanoma progression and independent of BRAF or NRAS mutations. Data also suggest different biologic and clinical impact of PPP6C mutations, with stop mutations showing association with development of visceral metastases that requires further clinical and functional study.

Published
2013
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36. Abstract 3188: Nucleolin phosphorylation mediated regulation of gene expression in determining cellular fate during the DNA damage response (DDR)

Author

Frida E. Kleiman, Anjana Saxena, Elif Caglar ýþýn, Zaineb Nadeem, Shu Xiao, Xiaokan Zhang, and Emral Devany

Subjects
Regulation of gene expression, Cancer Research, Oncology, DNA damage, Cancer research, Phosphorylation, Biology, Nucleolin
Abstract

The phosphoprotein nucleolin integrates several critical cellular processes, such as cell growth, proliferation, cell cycle arrest, apoptosis as well as DDR. Elevated levels of nucleolin are found in highly proliferative cells including a variety of tumors. Nucleolin is highly phosphorylated at the N-terminus by two major kinases: interphase casein kinase 2 (CK2) and mitotic cyclin-dependent kinase (Cdk). Earlier we have demonstrated that the N-terminus of nucleolin associates with Hdm2 to stabilize p53 protein and causes p53-mediated apoptosis. Additionally, nucleolin via its RNA-binding properties has been demonstrated to regulate the stability of several mRNAs and enhance translation. Besides, nucleolin post-translational modifications are linked to its role as an RNA-binding stress-responsive protein. Based on these studies, we hypothesize a role for nucleolin phosphorylation in regulating mRNA stability of different target genes during DDR. To test this we have engineered a novel system with tet-off promoter in human osteosarcoma cells to express 3xFlag-tagged nucleolin-wt or phospho-mutant [6/S*A, defective in undergoing phosphorylation at six consensus CK2 sites] that allow us to control expression of nucleolin using doxycycline. Cell proliferation assays with these inducible cells indicated that although nucleolin phosphorylation by CK2 was required for cell proliferation in unstressed cells, a hypo-phosphorylated nucleolin mutant caused higher cell viability upon genotoxic stress. Further, nucleolin phospho-variants differentially elevated p53 protein levels and hypo-phosphorylated nucleolin associated with p53 even under non-stressed conditions. Our co-immunoprecipitation (co-IP) assays also showed that nucleolin associated with poly(A)-specific ribonuclease (PARN), an mRNA decay enzyme that controls mRNA stability of different genes during DDR. Importantly, hypo-phosphorylated nucleolin mutant decreased PARN deadenylase activity in vitro. Interestingly, nucleolin also interacted with cellular p53-mRNA as detected by RNA immunoprecipitation assays with nucleolin antibodies followed by qRT-PCR. Our data for the first time provides evidential support that nucleolin phosphorylation can play a regulatory role in driving the cell cycle and controlling gene expression during DDR. Direct associations of nucleolin with p53 and PARN probably affect p53-signaling as well as PARN-deadenylase activity. Understanding the control of gene expression that is regulated by nucleolin phosphorylation during DDR, will provide valuable insights into the mechanism(s) behind the cellular decisions of cell survival or death upon DNA damage. Citation Format: Xiaokan Zhang, Shu Xiao, Emral Devany, Zaineb Nadeem, Elif Caglar ýþýn, Frida Kleiman, Anjana D. Saxena. Nucleolin phosphorylation mediated regulation of gene expression in determining cellular fate during the DNA damage response (DDR). [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 3188. doi:10.1158/1538-7445.AM2013-3188

Published
2013
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