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1. Genetic Heterogeneity of BRAF Fusion Kinases in Melanoma Affects Drug Responses

Author

Botton, Thomas, Talevich, Eric, Mishra, Vivek Kumar, Zhang, Tongwu, Shain, A Hunter, Berquet, Céline, Gagnon, Alexander, Judson, Robert L, Ballotti, Robert, Ribas, Antoni, Herlyn, Meenhard, Rocchi, Stéphane, Brown, Kevin M, Hayward, Nicholas K, Yeh, Iwei, and Bastian, Boris C

Subjects
Biological Sciences, Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Animals, Dimerization, Drug Resistance, Neoplasm, Female, Gene Expression Regulation, Neoplastic, Humans, Intracellular Signaling Peptides and Proteins, Melanoma, Mice, Mice, Nude, Mitogen-Activated Protein Kinases, Oncogene Proteins, Fusion, Protein Isoforms, Protein Kinase Inhibitors, Proto-Oncogene Proteins B-raf, RNA Interference, RNA, Small Interfering, Signal Transduction, Vemurafenib, ras Proteins, BRAF fusion, MEK inhibitor, RAF inhibitor, kinase, melanoma, paradoxical activation, pre-clinical, rearrangement, sequencing, translocation, Biochemistry and Cell Biology, Medical Physiology, Biological sciences
Abstract

BRAF fusions are detected in numerous neoplasms, but their clinical management remains unresolved. We identified six melanoma lines harboring BRAF fusions representative of the clinical cases reported in the literature. Their unexpected heterogeneous responses to RAF and MEK inhibitors could be categorized upon specific features of the fusion kinases. Higher expression level correlated with resistance, and fusion partners containing a dimerization domain promoted paradoxical activation of the mitogen-activated protein kinase (MAPK) pathway and hyperproliferation in response to first- and second-generation RAF inhibitors. By contrast, next-generation αC-IN/DFG-OUT RAF inhibitors blunted paradoxical activation across all lines and had their therapeutic efficacy further increased in vitro and in vivo by combination with MEK inhibitors, opening perspectives in the clinical management of tumors harboring BRAF fusions.

Published
2019

2. Hybrid Capture‐Based Tumor Sequencing and Copy Number Analysis to Confirm Origin of Metachronous Metastases in BRCA1‐Mutant Cholangiocarcinoma Harboring a Novel YWHAZ‐BRAF Fusion

Author

Lim, Huat C, Montesion, Meagan, Botton, Thomas, Collisson, Eric A, Umetsu, Sarah E, Behr, Spencer C, Gordan, John D, Stephens, Phil J, and Kelley, Robin K

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Liver Disease, Human Genome, Biotechnology, Clinical Research, Cancer, Digestive Diseases, Digestive Diseases - (Gallbladder), Genetics, Rare Diseases, Liver Cancer, 2.1 Biological and endogenous factors, Detection, screening and diagnosis, Aetiology, 4.1 Discovery and preclinical testing of markers and technologies, Good Health and Well Being, BRCA1 Protein, Cholangiocarcinoma, DNA Copy Number Variations, Humans, Neoplasm Metastasis, Proto-Oncogene Proteins B-raf, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

Biliary tract cancers such as cholangiocarcinoma represent a heterogeneous group of cancers that can be difficult to diagnose. Recent comprehensive genomic analyses in large cholangiocarcinoma cohorts have defined important molecular subgroups within cholangiocarcinoma that may relate to anatomic location and etiology [1], [2], [3], [4] and may predict responsiveness to targeted therapies in development [5], [6], [7]. These emerging data highlight the potential for tumor genomics to inform diagnosis and treatment options in this challenging tumor type. We report the case of a patient with a germline BRCA1 mutation who presented with a cholangiocarcinoma driven by the novel YWHAZ-BRAF fusion. Hybrid capture-based DNA sequencing and copy number analysis performed as part of clinical care demonstrated that two later-occurring tumors were clonally derived from the primary cholangiocarcinoma rather than distinct new primaries, revealing an unusual pattern of late metachronous metastasis. We discuss the clinical significance of these genetic alterations and their relevance to therapeutic strategies.Key pointsHybrid capture-based next-generation DNA sequencing assays can provide diagnostic clarity in patients with unusual patterns of metastasis and recurrence in which the pathologic diagnosis is ambiguous.To our knowledge, this is the first reported case of a YWHAZ-BRAF fusion in pancreaticobiliary cancer, and a very rare case of cholangiocarcinoma in the setting of a germline BRCA1 mutation.The patient's BRCA1 mutation and YWHAZ-BRAF fusion constitute potential targets for future therapy.

Published
2018

3. Bi-allelic Loss of CDKN2A Initiates Melanoma Invasion via BRN2 Activation

Author

Zeng, Hanlin, Jorapur, Aparna, Shain, A Hunter, Lang, Ursula E, Torres, Rodrigo, Zhang, Yuntian, McNeal, Andrew S, Botton, Thomas, Lin, Jue, Donne, Matthew, Bastian, Ingmar N, Yu, Richard, North, Jeffrey P, Pincus, Laura, Ruben, Beth S, Joseph, Nancy M, Yeh, Iwei, Bastian, Boris C, and Judson, Robert L

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, Cell Line, Tumor, Cell Movement, Cyclin-Dependent Kinase Inhibitor p16, E2F1 Transcription Factor, Female, Gene Expression Regulation, Neoplastic, Homeodomain Proteins, Humans, Loss of Heterozygosity, Lung Neoplasms, Male, Melanocytes, Melanoma, Mice, Inbred NOD, Neoplasm Invasiveness, POU Domain Factors, Point Mutation, Proto-Oncogene Proteins B-raf, Signal Transduction, Skin Neoplasms, Transcriptional Activation, BRN2, CDKN2A, CRISPR engineering, E2F1, invasion, melanocytes, melanoma, Neurosciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

Loss of the CDKN2A tumor suppressor is associated with melanoma metastasis, but the mechanisms connecting the phenomena are unknown. Using CRISPR-Cas9 to engineer a cellular model of melanoma initiation from primary human melanocytes, we discovered that a lineage-restricted transcription factor, BRN2, is downstream of CDKN2A and directly regulated by E2F1. In a cohort of melanocytic tumors that capture distinct progression stages, we observed that CDKN2A loss coincides with both the onset of invasive behavior and increased BRN2 expression. Loss of the CDKN2A protein product p16INK4A permitted metastatic dissemination of human melanoma lines in mice, a phenotype rescued by inhibition of BRN2. These results demonstrate a mechanism by which CDKN2A suppresses the initiation of melanoma invasion through inhibition of BRN2.

Published
2018

4. Vitiligo auto‐immune response upon oxidative stress‐related mitochondrial DNA release opens up new therapeutic strategies.

Author

Sant'Anna‐Silva, Ana C. B., Botton, Thomas, Rossi, Andrea, Dobner, Jochen, Bzioueche, Hanene, Thach, Nguyen, Blot, Lauriane, Pagnotta, Sophie, Kleszczynski, Konrad, Steinbrink, Kerstin, Mazure, Nathalie M., Rocchi, Stéphane, Krutmann, Jean, Passeron, Thierry, and Tulic, Meri K.

Subjects
*MELAS syndrome, *NUCLEAR factor E2 related factor, *MONONUCLEAR leukocytes, *INTERFERON regulatory factors, *MEDICAL ethics, *TYPE I interferons
Abstract

This article explores the connection between mitochondrial DNA (mtDNA) and vitiligo, an autoimmune disease that causes skin and hair depigmentation. The study reveals that vitiligo patients have an increased number of mtDNA variants, which leads to the release of mtDNA into the cytoplasm. This triggers an inflammatory response and promotes an autoimmune reaction against melanocytes. The findings suggest that targeting mtDNA release and oxidative stress could be potential therapeutic approaches for vitiligo. Additionally, the study suggests that vitiligo can be considered a mitochondrial disease, opening up the possibility of mitochondrial-specific treatments for managing the condition. [Extracted from the article]

Published
2024
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5. NTRK3 kinase fusions in Spitz tumours

Author

Yeh, Iwei, Tee, Meng Kian, Botton, Thomas, Shain, A Hunter, Sparatta, Alyssa J, Gagnon, Alexander, Vemula, Swapna S, Garrido, Maria C, Nakamaru, Kenji, Isoyama, Takeshi, McCalmont, Timothy H, LeBoit, Philip E, and Bastian, Boris C

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, 2.1 Biological and endogenous factors, Good Health and Well Being, Adolescent, Adult, Aged, Child, Child, Preschool, Comparative Genomic Hybridization, Discoidin Domain Receptor 2, Female, Humans, Male, Melanoma, Mitogen-Activated Protein Kinases, Molecular Motor Proteins, Myosin Heavy Chains, Myosin Type V, Nevus, Epithelioid and Spindle Cell, Oncogene Fusion, Phosphatidylinositol 3-Kinases, Proto-Oncogene Proteins c-ets, Repressor Proteins, Sequence Analysis, DNA, Sequence Analysis, RNA, Skin Neoplasms, ETS Translocation Variant 6 Protein, NTRK3 fusion, Spitz tumour, melanoma, kinase inhibitor, Spitz naevus, atypical Spitz tumour, spitzoid melanoma, oncogene, genetics, Clinical Sciences, Pathology, Clinical sciences, Oncology and carcinogenesis
Abstract

Oncogenic fusions in TRK family receptor tyrosine kinases have been identified in several cancers and can serve as therapeutic targets. We identified ETV6-NTRK3, MYO5A-NTRK3 and MYH9-NTRK3 fusions in Spitz tumours, and demonstrated that NTRK3 fusions constitutively activate the mitogen-activated protein kinase, phosphoinositide 3-kinase and phospholipase Cγ1 pathways in melanocytes. This signalling was inhibited by DS-6051a, a small-molecule inhibitor of NTRK1/2/3 and ROS1. NTRK3 fusions expand the range of oncogenic kinase fusions in melanocytic neoplasms and offer targets for a small subset of melanomas for which no targeted options currently exist. Copyright © 2016 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

Published
2016

6. CNVkit: Genome-Wide Copy Number Detection and Visualization from Targeted DNA Sequencing.

Author

Talevich, Eric, Shain, A Hunter, Botton, Thomas, and Bastian, Boris C

Subjects
Humans, In Situ Hybridization, Fluorescence, Sequence Analysis, DNA, Computational Biology, Genome, Human, Software, Comparative Genomic Hybridization, Genome-Wide Association Study, DNA Copy Number Variations, High-Throughput Nucleotide Sequencing, In Situ Hybridization, Fluorescence, Sequence Analysis, DNA, Genome, Human, Bioinformatics, Biological Sciences, Information and Computing Sciences, Mathematical Sciences
Abstract

Germline copy number variants (CNVs) and somatic copy number alterations (SCNAs) are of significant importance in syndromic conditions and cancer. Massively parallel sequencing is increasingly used to infer copy number information from variations in the read depth in sequencing data. However, this approach has limitations in the case of targeted re-sequencing, which leaves gaps in coverage between the regions chosen for enrichment and introduces biases related to the efficiency of target capture and library preparation. We present a method for copy number detection, implemented in the software package CNVkit, that uses both the targeted reads and the nonspecifically captured off-target reads to infer copy number evenly across the genome. This combination achieves both exon-level resolution in targeted regions and sufficient resolution in the larger intronic and intergenic regions to identify copy number changes. In particular, we successfully inferred copy number at equivalent to 100-kilobase resolution genome-wide from a platform targeting as few as 293 genes. After normalizing read counts to a pooled reference, we evaluated and corrected for three sources of bias that explain most of the extraneous variability in the sequencing read depth: GC content, target footprint size and spacing, and repetitive sequences. We compared the performance of CNVkit to copy number changes identified by array comparative genomic hybridization. We packaged the components of CNVkit so that it is straightforward to use and provides visualizations, detailed reporting of significant features, and export options for integration into existing analysis pipelines. CNVkit is freely available from https://github.com/etal/cnvkit.

Published
2016

7. Kinase fusions are frequent in Spitz tumours and spitzoid melanomas

Author

Wiesner, Thomas, He, Jie, Yelensky, Roman, Esteve-Puig, Rosaura, Botton, Thomas, Yeh, Iwei, Lipson, Doron, Otto, Geoff, Brennan, Kristina, Murali, Rajmohan, Garrido, Maria, Miller, Vincent A, Ross, Jeffrey S, Berger, Michael F, Sparatta, Alyssa, Palmedo, Gabriele, Cerroni, Lorenzo, Busam, Klaus J, Kutzner, Heinz, Cronin, Maureen T, Stephens, Philip J, and Bastian, Boris C

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Clinical Research, Cancer, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Base Sequence, DNA Mutational Analysis, Genome, Human, Humans, Melanoma, Molecular Sequence Data, Nevus, Epithelioid and Spindle Cell, Oncogene Proteins, Fusion, Protein Kinases, Reproducibility of Results, Skin Neoplasms, Xenograft Model Antitumor Assays
Abstract

Spitzoid neoplasms are a group of melanocytic tumours with distinctive histopathological features. They include benign tumours (Spitz naevi), malignant tumours (spitzoid melanomas) and tumours with borderline histopathological features and uncertain clinical outcome (atypical Spitz tumours). Their genetic underpinnings are poorly understood, and alterations in common melanoma-associated oncogenes are typically absent. Here we show that spitzoid neoplasms harbour kinase fusions of ROS1 (17%), NTRK1 (16%), ALK (10%), BRAF (5%) and RET (3%) in a mutually exclusive pattern. The chimeric proteins are constitutively active, stimulate oncogenic signalling pathways, are tumourigenic and are found in the entire biologic spectrum of spitzoid neoplasms, including 55% of Spitz naevi, 56% of atypical Spitz tumours and 39% of spitzoid melanomas. Kinase inhibitors suppress the oncogenic signalling of the fusion proteins in vitro. In summary, kinase fusions account for the majority of oncogenic aberrations in spitzoid neoplasms and may serve as therapeutic targets for metastatic spitzoid melanomas.

Published
2014

9. Recurrent BRAF kinase fusions in melanocytic tumors offer an opportunity for targeted therapy

Author

Botton, Thomas, Yeh, Iwei, Nelson, Tyrrell, Vemula, Swapna S, Sparatta, Alyssa, Garrido, Maria C, Allegra, Maryline, Rocchi, Stephane, Bahadoran, Philippe, McCalmont, Timothy H, LeBoit, Philip E, Burton, Elizabeth A, Bollag, Gideon, Ballotti, Robert, and Bastian, Boris C

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Rare Diseases, Cancer, Orphan Drug, Biotechnology, Human Genome, Genetics, Aetiology, 2.1 Biological and endogenous factors, Adolescent, Adult, Child, Preschool, Enzyme Activation, Female, Gene Rearrangement, Humans, Indoles, MAP Kinase Signaling System, Male, Melanocytes, Melanoma, Middle Aged, Molecular Targeted Therapy, Nevus, Epithelioid and Spindle Cell, Niacinamide, Oncogene Proteins, Fusion, Phenylurea Compounds, Proto-Oncogene Proteins B-raf, Skin Neoplasms, Sorafenib, Sulfonamides, Vemurafenib, Young Adult, melanoma, oncogenes, BRAF, kinase, translocation, Medical and Health Sciences, Dermatology & Venereal Diseases, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

BRAF is the most prevalent oncogene and an important therapeutic target in melanoma. In some cancers, BRAF is activated by rearrangements that fuse its kinase domain to 5' partner genes. We examined 848 comparative genomic hybridization profiles of melanocytic tumors and found copy number transitions within BRAF in 10 tumors, of which six could be further characterized by sequencing. In all, the BRAF kinase domain was fused in-frame to six N-terminal partners. No other mutations were identified in melanoma oncogenes. One of the seven melanoma cell lines without known oncogenic mutations harbored a similar BRAF fusion, which constitutively activated the MAP kinase pathway. Sorafenib, but not vemurafenib, could block MAP kinase pathway activation and proliferation of the cell line at clinically relevant concentrations, whereas BRAF(V) (600E) mutant melanoma cell lines were significantly more sensitive to vemurafenib. The patient from whom the cell line was derived showed a durable clinical response to sorafenib.

Published
2013

12. Compounds Triggering ER Stress Exert Anti-Melanoma Effects and Overcome BRAF Inhibitor Resistance

Author

Cerezo, Michaël, Lehraiki, Abdelali, Millet, Antoine, Rouaud, Florian, Plaisant, Magali, Jaune, Emilie, Botton, Thomas, Ronco, Cyril, Abbe, Patricia, Amdouni, Hella, Passeron, Thierry, Hofman, Veronique, Mograbi, Baharia, Dabert-Gay, Anne-Sophie, Debayle, Delphine, Alcor, Damien, Rabhi, Nabil, Annicotte, Jean-Sébastien, Héliot, Laurent, Gonzalez-Pisfil, Mariano, Robert, Caroline, Moréra, Solange, Vigouroux, Armelle, Gual, Philippe, Ali, Maruf M.U., Bertolotto, Corine, Hofman, Paul, Ballotti, Robert, Benhida, Rachid, and Rocchi, Stéphane

Published
2016
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16. Abstract 5518: Bi-allelic loss of CDKN2A initiates melanoma invasion and metastasis via E2F1-BRN2 axis

Author

Zeng, Hanlin, primary, Jorapur, Aparna, additional, Shain, A. Hunter, additional, Lang, Ursula E., additional, Torres, Rodrigo, additional, Zhang, Yuntian, additional, Botton, Thomas, additional, Lin, Jue, additional, Mcneal, Andrew S., additional, Donne, Matthew, additional, Bastian, Ingmar N., additional, North, Jeffrey, additional, Pincus, Laura, additional, Yu, Richard, additional, Ruben, Beth S., additional, Joseph, Nancy, additional, Ye, Iwei, additional, Bastian, Boris C., additional, and Judson, Robert L., additional

Published
2018
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17. Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway

Author

Shain, A Hunter, primary, Garrido, Maria, additional, Botton, Thomas, additional, Talevich, Eric, additional, Yeh, Iwei, additional, Sanborn, J Zachary, additional, Chung, Jongsuk, additional, Wang, Nicholas J, additional, Kakavand, Hojabr, additional, Mann, Graham J, additional, Thompson, John F, additional, Wiesner, Thomas, additional, Roy, Ritu, additional, Olshen, Adam B, additional, Gagnon, Alexander, additional, Gray, Joe W, additional, Huh, Nam, additional, Hur, Joe S, additional, Busam, Klaus J, additional, Scolyer, Richard A, additional, Cho, Raymond J, additional, Murali, Rajmohan, additional, and Bastian, Boris C, additional

Published
2015
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18. Abstract 2968: Exome sequencing of desmoplastic melanoma reveals recurrent NFKBIE promoter mutations and diverse MAPK/PI3K pathway activating mutations

Author

Shain, Alan H., primary, Garrido, Maria, additional, Botton, Thomas, additional, Talevich, Eric, additional, Yeh, Iweh, additional, Sanborn, Zack, additional, Chung, Jongsuk, additional, Wang, Nicholas, additional, Kakavand, Hojabr, additional, Mann, Graham, additional, Thompson, John, additional, Wiesner, Thomas, additional, Roy, Ritu, additional, Olshen, Adam, additional, Gagnon, Alexander, additional, Gray, Joe, additional, Huh, Nam, additional, Hur, Joe, additional, Busam, Klaus, additional, Scolyer, Richard, additional, Cho, Raymond, additional, Murali, Rajmohan, additional, and Bastian, Boris, additional

Published
2015
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19. Ciglitazone negatively regulates CXCL1 signaling through MITF to suppress melanoma growth

Author

Botton, Thomas, Puissant, Alexandre, Cheli, Yann, Tomic, Tijana, Giuliano, Sandy, Fajas, Lluis, Deckert, Marcel, Ortonne, Jean-Paul, Bertololotto, Corine, Tartare-Deckert, Sophie, Ballotti, Robert, Rocchi, Stéphane, Centre méditérannéen de médecine moléculaire ( C3M ), Université Nice Sophia Antipolis ( UNS ), Université Côte d'Azur ( UCA ) -Université Côte d'Azur ( UCA ) -Institut National de la Santé et de la Recherche Médicale ( INSERM ), Institut de Génétique Moléculaire de Montpellier ( IGMM ), Université de Montpellier ( UM ) -Centre National de la Recherche Scientifique ( CNRS ), Régulations des réactions immunitaires et inflammatoires, Université Côte d'Azur ( UCA ) -Université Côte d'Azur ( UCA ) -IFR50-Institut National de la Santé et de la Recherche Médicale ( INSERM ), Service de dermatologie, CHU Nice, Centre méditérannéen de médecine moléculaire (C3M), Université Nice Sophia Antipolis (... - 2019) (UNS), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut de Génétique Moléculaire de Montpellier (IGMM), Centre National de la Recherche Scientifique (CNRS)-Université de Montpellier (UM), COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-COMUE Université Côte d'Azur (2015-2019) (COMUE UCA)-IFR50-Institut National de la Santé et de la Recherche Médicale (INSERM), and Centre Hospitalier Universitaire de Nice (CHU Nice)

Subjects
MITF, Chemokine, animal diseases, Thiazolidinedione, apoptosis, respiratory system, Melanoma
Abstract

International audience; We have previously demonstrated that the thiazolidinedione ciglitazone inhibited, independently of PPAR activation, melanoma cell growth. Further investigations now show that ciglitazone effects are mediated through the regulation of secreted factors. Q-PCR screening of several genes involved in melanoma biology reveals that ciglitazone inhibits expression of the CXCL1 chemokine gene. CXCL1 is overexpressed in melanoma and contributes to tumorigenicity. We show that ciglitazone induces a diminution of CXCL1 level in different human melanoma cell lines. This effect is mediated by the down regulation of microphthalmia-associated transcription factor, MITF, the master gene in melanocyte differentiation and involved in melanoma development. Further, recombinant CXCL1 protein is sufficient to abrogate thiazolidinedione effects such as apoptosis induction, while extinction of the CXCL1 pathway mimics phenotypic changes observed in response to ciglitazone. Finally, inhibition of human melanoma tumor development in nude mice treated with ciglitazone is associated with a strong decrease in MITF and CXCL1 levels. Our results demonstrate that anti-melanoma effects of thiazolidinediones involve an inhibition of the MITF/CXCL1 axis and highlight the key role of this specific pathway in melanoma malignancy.

Published
2010
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20. Activating MET kinase rearrangements in melanoma and Spitz tumours

Author

Yeh, Iwei, primary, Botton, Thomas, additional, Talevich, Eric, additional, Shain, A. Hunter, additional, Sparatta, Alyssa J., additional, de la Fouchardiere, Arnaud, additional, Mully, Thaddeus W., additional, North, Jeffrey P., additional, Garrido, Maria C., additional, Gagnon, Alexander, additional, Vemula, Swapna S., additional, McCalmont, Timothy H., additional, LeBoit, Philip E., additional, and Bastian, Boris C., additional

Published
2015
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21. Kinase fusions are frequent in Spitz tumours and spitzoid melanomas.

Author

Lipson, Doron, Lipson, Doron, Otto, Geoff, Brennan, Kristina, Murali, Rajmohan, Garrido, Maria, Miller, Vincent, Ross, Jeffrey, Berger, Michael, Sparatta, Alyssa, Palmedo, Gabriele, Cerroni, Lorenzo, Busam, Klaus, Kutzner, Heinz, Cronin, Maureen, Stephens, Philip, Wiesner, Thomas, He, Jie, Yelensky, Roman, Esteve-Puig, Rosaura, Botton, Thomas, Bastian, Boris, Yeh, Iwei, Lipson, Doron, Lipson, Doron, Otto, Geoff, Brennan, Kristina, Murali, Rajmohan, Garrido, Maria, Miller, Vincent, Ross, Jeffrey, Berger, Michael, Sparatta, Alyssa, Palmedo, Gabriele, Cerroni, Lorenzo, Busam, Klaus, Kutzner, Heinz, Cronin, Maureen, Stephens, Philip, Wiesner, Thomas, He, Jie, Yelensky, Roman, Esteve-Puig, Rosaura, Botton, Thomas, Bastian, Boris, and Yeh, Iwei

Abstract

Spitzoid neoplasms are a group of melanocytic tumours with distinctive histopathological features. They include benign tumours (Spitz naevi), malignant tumours (spitzoid melanomas) and tumours with borderline histopathological features and uncertain clinical outcome (atypical Spitz tumours). Their genetic underpinnings are poorly understood, and alterations in common melanoma-associated oncogenes are typically absent. Here we show that spitzoid neoplasms harbour kinase fusions of ROS1 (17%), NTRK1 (16%), ALK (10%), BRAF (5%) and RET (3%) in a mutually exclusive pattern. The chimeric proteins are constitutively active, stimulate oncogenic signalling pathways, are tumourigenic and are found in the entire biologic spectrum of spitzoid neoplasms, including 55% of Spitz naevi, 56% of atypical Spitz tumours and 39% of spitzoid melanomas. Kinase inhibitors suppress the oncogenic signalling of the fusion proteins in vitro. In summary, kinase fusions account for the majority of oncogenic aberrations in spitzoid neoplasms and may serve as therapeutic targets for metastatic spitzoid melanomas.

Published
2014

25. Exome sequencing of desmoplastic melanoma identifies recurrent NFKBIE promoter mutations and diverse activating mutations in the MAPK pathway.

Author

Garrido, Maria, Botton, Thomas, Talevich, Eric, Yeh, Iwei, Wang, Nicholas J, Kakavand, Hojabr, Mann, Graham J, Thompson, John F, Olshen, Adam B, Gagnon, Alexander, Gray, Joe W, Scolyer, Richard A, Murali, Rajmohan, Bastian, Boris C, Sanborn, J Zachary, Chung, Jongsuk, Huh, Nam, Wiesner, Thomas, Shain, A Hunter, and Roy, Ritu

Subjects
*DESMOPLASTIC small round cell tumor, *MELANOMA, *MITOGEN-activated protein kinase phosphatases, *GENETIC mutation, *PHYSIOLOGICAL effects of ultraviolet radiation, *COHORT analysis
Abstract

Desmoplastic melanoma is an uncommon variant of melanoma with sarcomatous histology, distinct clinical behavior and unknown pathogenesis. We performed low-coverage genome and high-coverage exome sequencing of 20 desmoplastic melanomas, followed by targeted sequencing of 293 genes in a validation cohort of 42 cases. A high mutation burden (median of 62 mutations/Mb) ranked desmoplastic melanoma among the most highly mutated cancers. Mutation patterns strongly implicate ultraviolet radiation as the dominant mutagen, indicating a superficially located cell of origin. Newly identified alterations included recurrent promoter mutations of NFKBIE, encoding NF-κB inhibitor ɛ (IκBɛ), in 14.5% of samples. Common oncogenic mutations in melanomas, in particular in BRAF (encoding p.Val600Glu) and NRAS (encoding p.Gln61Lys or p.Gln61Arg), were absent. Instead, other genetic alterations known to activate the MAPK and PI3K signaling cascades were identified in 73% of samples, affecting NF1, CBL, ERBB2, MAP2K1, MAP3K1, BRAF, EGFR, PTPN11, MET, RAC1, SOS2, NRAS and PIK3CA, some of which are candidates for targeted therapies. [ABSTRACT FROM AUTHOR]

Published
2015
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