NYUHSL Faculty Bibliography

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112

Cancer cell. 2016:30(2):214-228.DOI: 10.1016/j.ccell.2016.06.022

High-throughput Phenotyping of Lung Cancer Somatic Mutations

Berger, Alice H; Brooks, Angela N; Wu, Xiaoyun; Shrestha, Yashaswi; Chouinard, Candace; Piccioni, Federica; Bagul, Mukta; Kamburov, Atanas; Imielinski, Marcin; Hogstrom, Larson; Zhu, Cong; Yang, Xiaoping; Pantel, Sasha; Sakai, Ryo; Watson, Jacqueline; Kaplan, Nathan; Campbell, Joshua D; Singh, Shantanu; Root, David E; Narayan, Rajiv; Natoli, Ted; Lahr, David L; Tirosh, Itay; Tamayo, Pablo; Getz, Gad; Wong, Bang; Doench, John; Subramanian, Aravind; Golub, Todd R; Meyerson, Matthew; Boehm, Jesse S

Recent genome sequencing efforts have identified millions of somatic mutations in cancer. However, the functional impact of most variants is poorly understood. Here we characterize 194 somatic mutations identified in primary lung adenocarcinomas. We present an expression-based variant-impact phenotyping (eVIP) method that uses gene expression changes to distinguish impactful from neutral somatic mutations. eVIP identified 69% of mutations analyzed as impactful and 31% as functionally neutral. A subset of the impactful mutations induces xenograft tumor formation in mice and/or confers resistance to cellular EGFR inhibition. Among these impactful variants are rare somatic, clinically actionable variants including EGFR S645C, ARAF S214C and S214F, ERBB2 S418T, and multiple BRAF variants, demonstrating that rare mutations can be functionally important in cancer.

PMID: 27478040

ISSN: 1878-3686

CID: 5270152

Nature genetics. 2016:48(6):607-16.DOI: 10.1038/ng.3564

Distinct patterns of somatic genome alterations in lung adenocarcinomas and squamous cell carcinomas

Campbell, Joshua D; Alexandrov, Anton; Kim, Jaegil; Wala, Jeremiah; Berger, Alice H; Pedamallu, Chandra Sekhar; Shukla, Sachet A; Guo, Guangwu; Brooks, Angela N; Murray, Bradley A; Imielinski, Marcin; Hu, Xin; Ling, Shiyun; Akbani, Rehan; Rosenberg, Mara; Cibulskis, Carrie; Ramachandran, Aruna; Collisson, Eric A; Kwiatkowski, David J; Lawrence, Michael S; Weinstein, John N; Verhaak, Roel G W; Wu, Catherine J; Hammerman, Peter S; Cherniack, Andrew D; Getz, Gad; Artyomov, Maxim N; Schreiber, Robert; Govindan, Ramaswamy; Meyerson, Matthew

To compare lung adenocarcinoma (ADC) and lung squamous cell carcinoma (SqCC) and to identify new drivers of lung carcinogenesis, we examined the exome sequences and copy number profiles of 660 lung ADC and 484 lung SqCC tumor-normal pairs. Recurrent alterations in lung SqCCs were more similar to those of other squamous carcinomas than to alterations in lung ADCs. New significantly mutated genes included PPP3CA, DOT1L, and FTSJD1 in lung ADC, RASA1 in lung SqCC, and KLF5, EP300, and CREBBP in both tumor types. New amplification peaks encompassed MIR21 in lung ADC, MIR205 in lung SqCC, and MAPK1 in both. Lung ADCs lacking receptor tyrosine kinase-Ras-Raf pathway alterations had mutations in SOS1, VAV1, RASA1, and ARHGAP35. Regarding neoantigens, 47% of the lung ADC and 53% of the lung SqCC tumors had at least five predicted neoepitopes. Although targeted therapies for lung ADC and SqCC are largely distinct, immunotherapies may aid in treatment for both subtypes.

PMID: 27158780

ISSN: 1546-1718

CID: 5270142

Nature genetics. 2016:48(2):176-82.DOI: 10.1038/ng.3470

Identification of focally amplified lineage-specific super-enhancers in human epithelial cancers

Zhang, Xiaoyang; Choi, Peter S; Francis, Joshua M; Imielinski, Marcin; Watanabe, Hideo; Cherniack, Andrew D; Meyerson, Matthew

Whole-genome analysis approaches are identifying recurrent cancer-associated somatic alterations in noncoding DNA regions. We combined somatic copy number analysis of 12 tumor types with tissue-specific epigenetic profiling to identify significant regions of focal amplification harboring super-enhancers. Copy number gains of noncoding regions harboring super-enhancers near KLF5, USP12, PARD6B and MYC are associated with overexpression of these cancer-related genes. We show that two distinct focal amplifications of super-enhancers 3' to MYC in lung adenocarcinoma (MYC-LASE) and endometrial carcinoma (MYC-ECSE) are physically associated with the MYC promoter and correlate with MYC overexpression. CRISPR/Cas9-mediated repression or deletion of a constituent enhancer within the MYC-LASE region led to significant reductions in the expression of MYC and its target genes and to the impairment of anchorage-independent and clonogenic growth, consistent with an oncogenic function. Our results suggest that genomic amplification of super-enhancers represents a common mechanism to activate cancer driver genes in multiple cancer types.

PMCID:4857881

PMID: 26656844

ISSN: 1546-1718

CID: 5270132

Proceedings of the National Academy of Sciences of the United States of America (PNAS). 2014:111(52):18661-6.DOI: 10.1073/pnas.1412228112

Genetic modifiers of EGFR dependence in non-small cell lung cancer

Sharifnia, Tanaz; Rusu, Victor; Piccioni, Federica; Bagul, Mukta; Imielinski, Marcin; Cherniack, Andrew D; Pedamallu, Chandra Sekhar; Wong, Bang; Wilson, Frederick H; Garraway, Levi A; Altshuler, David; Golub, Todd R; Root, David E; Subramanian, Aravind; Meyerson, Matthew

Lung adenocarcinomas harboring activating mutations in the epidermal growth factor receptor (EGFR) represent a common molecular subset of non-small cell lung cancer (NSCLC) cases. EGFR mutations predict sensitivity to EGFR tyrosine kinase inhibitors (TKIs) and thus represent a dependency in NSCLCs harboring these alterations, but the genetic basis of EGFR dependence is not fully understood. Here, we applied an unbiased, ORF-based screen to identify genetic modifiers of EGFR dependence in EGFR-mutant NSCLC cells. This approach identified 18 kinase and kinase-related genes whose overexpression can substitute for EGFR in EGFR-dependent PC9 cells, and these genes include seven of nine Src family kinase genes, FGFR1, FGFR2, ITK, NTRK1, NTRK2, MOS, MST1R, and RAF1. A subset of these genes can complement loss of EGFR activity across multiple EGFR-dependent models. Unbiased gene-expression profiling of cells overexpressing EGFR bypass genes, together with targeted validation studies, reveals EGFR-independent activation of the MEK-ERK and phosphoinositide 3-kinase (PI3K)-AKT pathways. Combined inhibition of PI3K-mTOR and MEK restores EGFR dependence in cells expressing each of the 18 EGFR bypass genes. Together, these data uncover a broad spectrum of kinases capable of overcoming dependence on EGFR and underscore their convergence on the PI3K-AKT and MEK-ERK signaling axes in sustaining EGFR-independent survival.

PMCID:4284598

PMID: 25512530

ISSN: 1091-6490

CID: 5270122

Oncogene. 2014:33(35):4418-23.DOI: 10.1038/onc.2013.581

Oncogenic RIT1 mutations in lung adenocarcinoma

Berger, A H; Imielinski, M; Duke, F; Wala, J; Kaplan, N; Shi, G-X; Andres, D A; Meyerson, M

Lung adenocarcinoma is comprised of distinct mutational subtypes characterized by mutually exclusive oncogenic mutations in RTK/RAS pathway members KRAS, EGFR, BRAF and ERBB2, and translocations involving ALK, RET and ROS1. Identification of these oncogenic events has transformed the treatment of lung adenocarcinoma via application of therapies targeted toward specific genetic lesions in stratified patient populations. However, such mutations have been reported in only ∼55% of lung adenocarcinoma cases in the United States, suggesting other mechanisms of malignancy are involved in the remaining cases. Here we report somatic mutations in the small GTPase gene RIT1 in ∼2% of lung adenocarcinoma cases that cluster in a hotspot near the switch II domain of the protein. RIT1 switch II domain mutations are mutually exclusive with all other known lung adenocarcinoma driver mutations. Ectopic expression of mutated RIT1 induces cellular transformation in vitro and in vivo, which can be reversed by combined PI3K and MEK inhibition. These data identify RIT1 as a driver oncogene in a specific subset of lung adenocarcinomas and suggest PI3K and MEK inhibition as a potential therapeutic strategy in RIT1-mutated tumors.

PMID: 24469055

ISSN: 1476-5594

CID: 5637152

Journal of clinical investigation. 2014:124(4):1582-6.DOI: 10.1172/JCI72763

Oncogenic and sorafenib-sensitive ARAF mutations in lung adenocarcinoma [Case Report]

Imielinski, Marcin; Greulich, Heidi; Kaplan, Bethany; Araujo, Luiz; Amann, Joseph; Horn, Leora; Schiller, Joan; Villalona-Calero, Miguel A; Meyerson, Matthew; Carbone, David P

Targeted cancer therapies often induce "outlier" responses in molecularly defined patient subsets. One patient with advanced-stage lung adenocarcinoma, who was treated with oral sorafenib, demonstrated a near-complete clinical and radiographic remission for 5 years. Whole-genome sequencing and RNA sequencing of primary tumor and normal samples from this patient identified a somatic mutation, ARAF S214C, present in the cancer genome and expressed at high levels. Additional mutations affecting this residue of ARAF and a nearby residue in the related kinase RAF1 were demonstrated across 1% of an independent cohort of lung adenocarcinoma cases. The ARAF mutations were shown to transform immortalized human airway epithelial cells in a sorafenib-sensitive manner. These results suggest that mutant ARAF is an oncogenic driver in lung adenocarcinoma and an indicator of sorafenib response.

PMCID:3973082

PMID: 24569458

ISSN: 1558-8238

CID: 5270112

PLoS one. 2014:9(1).DOI: 10.1371/journal.pone.0087361

A pan-cancer analysis of transcriptome changes associated with somatic mutations in U2AF1 reveals commonly altered splicing events

Brooks, Angela N; Choi, Peter S; de Waal, Luc; Sharifnia, Tanaz; Imielinski, Marcin; Saksena, Gordon; Pedamallu, Chandra Sekhar; Sivachenko, Andrey; Rosenberg, Mara; Chmielecki, Juliann; Lawrence, Michael S; DeLuca, David S; Getz, Gad; Meyerson, Matthew

Although recurrent somatic mutations in the splicing factor U2AF1 (also known as U2AF35) have been identified in multiple cancer types, the effects of these mutations on the cancer transcriptome have yet to be fully elucidated. Here, we identified splicing alterations associated with U2AF1 mutations across distinct cancers using DNA and RNA sequencing data from The Cancer Genome Atlas (TCGA). Using RNA-Seq data from 182 lung adenocarcinomas and 167 acute myeloid leukemias (AML), in which U2AF1 is somatically mutated in 3-4% of cases, we identified 131 and 369 splicing alterations, respectively, that were significantly associated with U2AF1 mutation. Of these, 30 splicing alterations were statistically significant in both lung adenocarcinoma and AML, including three genes in the Cancer Gene Census, CTNNB1, CHCHD7, and PICALM. Cell line experiments expressing U2AF1 S34F in HeLa cells and in 293T cells provide further support that these altered splicing events are caused by U2AF1 mutation. Consistent with the function of U2AF1 in 3' splice site recognition, we found that S34F/Y mutations cause preferences for CAG over UAG 3' splice site sequences. This report demonstrates consistent effects of U2AF1 mutation on splicing in distinct cancer cell types.

PMCID:3909098

PMID: 24498085

ISSN: 1932-6203

CID: 5270102

Nature. 2014:511(7511):543-550.DOI:

Comprehensive molecular profiling of lung adenocarcinoma

Collisson, Eric A.; Campbell, Joshua D.; Brooks, Angela N.; Berger, Alice H.; Lee, William; Chmielecki, Juliann; Beer, David G.; Cope, Leslie; Creighton, Chad J.; Danilova, Ludmila; Ding, Li; Getz, Gad; Hammerman, Peter S.; Hayes, D. Neil; Hernandez, Bryan; Herman, James G.; Heymach, John V.; Jurisica, Igor; Kucherlapati, Raju; Kwiatkowski, David; Ladanyi, Marc; Robertson, Gordon; Schultz, Nikolaus; Shen, Ronglai; Sinha, Rileen; Sougnez, Carrie; Tsao, Ming-Sound; Travis, William D.; Weinstein, John N.; Wigle, Dennis A.; Wilkerson, Matthew D.; Chu, Andy; Cherniack, Andrew D.; Hadjipanayis, Angela; Rosenberg, Mara; Weisenberger, Daniel J.; Laird, Peter W.; Radenbaugh, Amie; Ma, Singer; Stuart, Joshua M.; Byers, Lauren Averett; Baylin, Stephen B.; Govindan, Ramaswamy; Meyerson, Matthew; Rosenberg, Mara; Gabriel, Stacey B.; Cibulskis, Kristian; Sougnez, Carrie; Kim, Jaegil; Stewart, Chip; Lichtenstein, Lee; Lander, Eric S.; Lawrence, Michael S.; Getz; Kandoth, Cyriac; Fulton, Robert; Fulton, Lucinda L.; McLellan, Michael D.; Wilson, Richard K.; Ye, Kai; Fronick, Catrina C.; Maher, Christopher A.; Miller, Christopher A.; Wendl, Michael C.; Cabanski, Christopher; Ding, Li; Mardis, Elaine; Govindan, Ramaswamy; Creighton, Chad J.; Wheeler, David; Balasundaram, Miruna; Butterfield, Yaron S. N.; Carlsen, Rebecca; Chu, Andy; Chuah, Eric; Dhalla, Noreen; Guin, Ranabir; Hirst, Carrie; Lee, Darlene; Li, Haiyan I.; Mayo, Michael; Moore, Richard A.; Mungall, Andrew J.; Schein, Jacqueline E.; Sipahimalani, Payal; Tam, Angela; Varhol, Richard; Robertson, A. Gordon; Wye, Natasja; Thiessen, Nina; Holt, Robert A.; Jones, Steven J. M.; Marra, Marco A.; Campbell, Joshua D.; Brooks, Angela N.; Chmielecki, Juliann; Imielinski, Marcin; Onofrio, Robert C.; Hodis, Eran; Zack, Travis; Sougnez, Carrie; Helman, Elena; Pedamallu, Chandra Sekhar; Mesirov, Jill; Cherniack, Andrew D.; Saksena, Gordon; Schumacher, Steven E.; Carter, Scott L.; Hernandez, Bryan; Garraway, Levi; Beroukhim, Rameen; Gabriel, Stacey B.; Getz, Gad; Meyerson, Matthew; Hadjipanayis, Angela; Lee, Semin; Mahadeshwar, Harshad S.; Pantazi, Angeliki; Protopopov, Alexei; Ren, Xiaojia; Seth, Sahil; Song, Xingzhi; Tang, Jiabin; Yang, Lixing; Zhang, Jianhua; Chen, Peng-Chieh; Parfenov, Michael; Xu, Andrew Wei; Santoso, Netty; Chin, Lynda; Park, Peter J.; Kucherlapati, Raju; Hoadley, Katherine A.; Auman, J. Todd; Meng, Shaowu; Shi, Yan; Buda, Elizabeth; Waring, Scot; Veluvolu, Umadevi; Tan, Donghui; Mieczkowski, Piotr A.; Jones, Corbin D.; Simons, Janae V.; Soloway, Matthew G.; Bodenheimer, Tom; Jefferys, Stuart R.; Roach, Jeffrey; Hoyle, Alan P.; Wu, Junyuan; Balu, Saianand; Singh, Darshan; Prins, Jan F.; Marron, J. S.; Parker, Joel S.; Hayes, D. Neil; Perou, Charles M.; Liu, Jinze; Cope, Leslie; Danilova, Ludmila; Weisenberger, Daniel J.; Maglinte, Dennis T.; Lai, Philip H.; Bootwalla, Moiz S.; Van Den Berg, David J.; Triche, Timothy, Jr.; Baylin, Stephen B.; Laird, Peter W.; Rosenberg, Mara; Chin, Lynda; Zhang, Jianhua; Cho, Juok; DiCara, Daniel; Heiman, David; Lin, Pei; Mallard, William; Voet, Douglas; Zhang, Hailei; Zou, Lihua; Noble, Michael S.; Lawrence, Michael S.; Saksena, Gordon; Gehlenborg, Nils; Thorvaldsdottir, Helga; Mesirov, Jill; Nazaire, Marc-Danie; Robinson, Jim; Getz, Gad; Lee, William; Aksoy, B. Arman; Ciriello, Giovanni; Taylor, Barry S.; Dresdner, Gideon; Gao, Jianjiong; Gross, Benjamin; Seshan, Venkatraman E.; Ladanyi, Marc; Reva, Boris; Sinha, Rileen; Sumer, S. Onur; Weinhold, Nils; Schultz, Nikolaus; Shen, Ronglai; Sander, Chris; Sam Ng; Ma, Singer; Zhu, Jingchun; Radenbaugh, Amie; Stuart, Joshua M.; Benz, Christopher C.; Yau, Christina; Haussler, David; Spellman, Paul T.; Wilkerson, Matthew D.; Parker, Joel S.; Hoadley, Katherine A.; Kimes, Patrick K.; Hayes, D. Neil; Perou, Charles M.; Broom, Bradley M.; Wang, Jing; Lu, Yiling; Patrick Kwok Shing Ng; Diao, Lixia; Byers, Lauren Averett; Liu, Wenbin; Heymach, John V.; Amos, Christopher I.; Weinstein, John N.; Akbani, Rehan; Mills, Gordon B.; Curley, Erin; Paulauskis, Joseph; Lau, Kevin; Morris, Scott; Shelton, Troy; Mallery, David; Gardner, Johanna; Penny, Robert; Saller, Charles; Tarvin, Katherine; Richards, William G.; Cerfolio, Robert; Bryant, Ayesha; Raymond, Daniel P.; Pennell, Nathan A.; Farver, Carol; Czerwinski, Christine; Huelsenbeck-Dill, Lori; Iacocca, Mary; Petrelli, Nicholas; Rabeno, Brenda; Brown, Jennifer; Bauer, Thomas; Dolzhanskiy, Oleg; Potapova, Olga; Rotin, Daniil; Voronina, Olga; Nemirovich-Danchenko, Elena; Fedosenko, Konstantin V.; Gal, Anthony; Behera, Madhusmita; Ramalingam, Suresh S.; Sica, Gabriel; Flieder, Douglas; Boyd, Jeff; Weaver, JoEllen; Kohl, Bernard; Dang Huy Quoc Thinh; Sandusky, George; Juhl, Hartmut; Duhig, Edwina; Illei, Peter; Gabrielson, Edward; Shin, James; Lee, Beverly; Rogers, Kristen; Trusty, Dante; Brock, Malcolm V.; Williamson, Christina; Burks, Eric; Rieger-Christ, Kimberly; Holway, Antonia; Sullivan, Travis; Wigle, Dennis A.; Asiedu, Michael K.; Kosari, Farhad; Travis, William D.; Rekhtman, Natasha; Zakowski, Maureen; Rusch, Valerie W.; Zippile, Paul; Suh, James; Pass, Harvey; Goparaju, Chandra; Owusu-Sarpong, Yvonne; Bartlett, John M. S.; Kodeeswaran, Sugy; Parfitt, Jeremy; Sekhon, Harmanjatinder; Albert, Monique; Eckman, John; Myers, Jerome B.; Cheney, Richard; Morrison, Carl; Gaudioso, Carmelo; Borgia, Jeffrey A.; Bonomi, Philip; Pool, Mark; Liptay, Michael J.; Moiseenko, Fedor; Zaytseva, Irina; Dienemann, Hendrik; Meister, Michael; Schnabel, Philipp A.; Muley, Thomas R.; Peifer, Martin; Gomez-Fernandez, Carmen; Herbert, Lynn; Egea, Sophie; Huang, Mei; Thorne, Leigh B.; Boice, Lori; Salazar, Ashley Hill; Funkhouser, William K.; Rathmell, W. Kimryn; Dhir, Rajiv; Yousem, Samuel A.; Dacic, Sanja; Schneider, Frank; Siegfried, Jill M.; Hajek, Richard; Watson, Mark A.; McDonald, Sandra; Meyers, Bryan; Clarke, Belinda; Yang, Ian A.; Fong, Kwun M.; Hunter, Lindy; Windsor, Morgan; Bowman, Rayleen V.; Peters, Solange; Letovanec, Igor; Khan, Khurram Z.; Jensen, Mark A.; Snyder, Eric E.; Srinivasan, Deepak; Kahn, Ari B.; Baboud, Julien; Pot, David A.; Shaw, Kenna R. Mills; Sheth, Margi; Davidsen, Tanja; Demchok, John A.; Yang, Liming; Wang, Zhining; Tarnuzzer, Roy; Zenklusen, Jean Claude; Ozenberger, Bradley A.; Sofia, Heidi J.; Travis, William D.; Cheney, Richard; Clarke, Belinda; Dacic, Sanja; Duhig, Edwina; Funkhouser, William K.; Illei, Peter; Farver, Carol; Rekhtman, Natasha; Sica, Gabriel; Suh, James; Tsao, Ming-Sound

ISI:000339566300025

ISSN: 0028-0836

CID: 5270632

Somatic Genome Alterations in Human Lung Cancers

Chapter by: Imielinski, Marcin; Hammerman, Peter S.; Thomas, Roman; Meyerson, Matthew

in: Lung cancer by

[S.l.] : Blackwell, 2014

pp. 67-89

ISBN: 978-1-118-46876-0

CID: 5270882

Journal of clinical oncology. 2014:32(15).DOI: 10.1200/jco.2014.32.15_suppl.11034

Oncogenic ARAF as a new driver in lung adenocarcinoma. [Meeting Abstract]

Araujo, Luiz H.; Amann, Joseph; Imielinski, Marcin; Greulich, Heidi; Meyerson, Matthew; Carbone, David Paul

ISI:000358613204767

ISSN: 0732-183x

CID: 5270662