Your search keyword '"Stephen J. Murphy"' showing total 32 results

1. Tumor Junction Burden and Antigen Presentation as Predictors of Survival in Mesothelioma Treated With Immune Checkpoint Inhibitors

Author

George Vasmatzis, Jun Yin, Tobias Peikert, Janet Schaefer-Klein, Maria J. Disselhorst, Mitesh J. Borad, Paul Baas, Giannoula Karagouga, Stephen J. Murphy, James B. Smadbeck, Sarah H. Johnson, Julia B. Udell, Aakash Desai, John C. Cheville, Farhad Kosari, Alexa McCune, and Aaron S. Mansfield

Subjects

Mesothelioma, Pulmonary and Respiratory Medicine, Oncology, medicine.medical_specialty, Lung Neoplasms, Chromosomal rearrangements, medicine.medical_treatment, Antigen presentation, Ipilimumab, medicine.disease_cause, Article, Immune checkpoint inhibitors, Internal medicine, medicine, Humans, Antigen Presentation, Mutation, Antigen processing, business.industry, Proportional hazards model, Mesothelioma, Malignant, Immunotherapy, medicine.disease, Nivolumab, Structural variants, business, medicine.drug

Abstract

Introduction: The favorable outcomes with immunotherapy for mesothelioma were somewhat unexpected because this tumor has a low tumor mutation burden which has been associated with benefit in other cancers. Because chromosomal rearrangements are common in mesothelioma and have neoantigenic potential, we sought to determine whether they are associated with survival in patients treated with immunotherapy.Methods: Pleural biopsies of mesothelioma after at least one line of therapy were obtained from patients (n = 44) before treatment with nivolumab alone (NCT29908324) or in combination with ipilimumab (NCT30660511). RNA and whole-genome sequencing were performed to identify the junctions resulting from chromosomal rearrangements and antigen processing and presentation gene set expression. Associations with overall survival (OS) were estimated using Cox models. An OS cutoff of 1.5 years was used to distinguish patients with and without durable benefit for use in receiving operating characteristic curves.Results: Although tumor junction burdens were not predictive of OS, we identified significant interactions between the junction burdens and multiple antigen processing and presentation gene sets. The "regulation of antigen processing and presentation of peptide antigen" gene set revealed an interaction with tumor junction burden and was predictive of OS. This interaction also predicted 1.5-year or greater survival with an area under the receiving operating characteristic curve of 0.83. This interaction was not predictive of survival in a separate cohort of patients with mesothelioma who did not receive immune checkpoint inhibitors.Conclusions: Analysis of structural variants and antigen presentation gene set expression may facilitate patient selection for immune checkpoint inhibitors. (C) 2021 International Association for the Study of Lung Cancer. Published by Elsevier Inc.

Published

2022

2. Immune Cell Infiltration May Be a Key Determinant of Long-Term Survival in Small Cell Lung Cancer

Author

Michael K. Asiedu, Ping Yang, Eunhee S. Yi, Farhad Kosari, Marie Christine Aubry, Dennis A. Wigle, Nafiseh Janaki, Tobias Peikert, George Vasmatzis, Kaustubh N. Bhinge, Simone Terra, Mariza de Andrade, Aaron S. Mansfield, Stephen J. Murphy, Aqsa Nasir, Virginia P. Van Keulen, Prasuna Muppa, and Anurag Sharma

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Tumor microenvironment, Antitumor immunity, business.industry, humanities, respiratory tract diseases, Gene expression profiling, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immune system, Oncology, 030220 oncology & carcinogenesis, Survivorship curve, Cancer research, Immunohistochemistry, Medicine, business, Immune cell infiltration, Immunostaining

Abstract

Introduction Although most patients with SCLC die within a few months of diagnosis, a subgroup of patients survive for many years. Factors determining long-term survivorship remain largely unknown. We present the first comprehensive comparative genomic and tumor microenvironment analyses of SCLC between patients with long-term survivorship and patients with the expected survivorship. Methods We compared surgically resected tumors of 23 long-term SCLC survivors (survival >4 years) and 18 SCLC survivors with the expected survival time (survival ≤2 years). There were no significant differences in clinical variables, including TNM staging and curative- versus non–curative-intent surgery between the groups. Gene expression profiling was performed by using microarrays, and tumor microenvironment analyses were performed by immunohistochemistry of prominent immune-related markers. Results Immune-related genes and pathways represented the majority of the differentially overexpressed genes in long-term survivorship compared with in expected survivorship. The differences in the immunological tumor microenvironment were confirmed by quantitative immunostaining. Increased numbers of tumor-infiltrating and associated lymphocytes were present throughout tumors of long-term survivors of SCLC. Several differentiating patterns of enhanced antitumor immunity were identified. Although some areas of the tumors of long-term survivors of SCLC also harbored higher numbers of suppressive immune cells (monocytes, regulatory lymphocytes, and macrophages), the ratios of these suppressive cells to CD3-positive lymphocytes were generally lower in the tumors of long-term survivors of SCLC, indicating a less tumor-suppressive microenvironment. Conclusions Our data demonstrate that long-term survivorship of patients with SCLC is strongly influenced by the presence of the immune cells in the tumor microenvironment. Characterization of the antitumor immune responses may identify opportunities for individualized immunotherapies for SCLC.

Published

2019

3. Large Chromosomal Rearrangements Yield Biomarkers to Distinguish Low-Risk From Intermediate- and High-Risk Prostate Cancer

Author

R. Jeffrey Karnes, William R. Sukov, Faye R. Harris, Athanasios Gaitatzes, Sarah H. Johnson, James B. Smadbeck, Irina V. Kovtun, Stephen J. Murphy, John C. Cheville, Farhad Kosari, George Vasmatzis, Laureano J. Rangel, Sara M. Kloft-Nelson, Simone Terra, Shabnam Zarei, Patricia T. Greipp, Ryan A. Knudson, Darlene L. Knutson, and Terry M. Therneau

Subjects

Male, Oncology, medicine.medical_specialty, DNA Copy Number Variations, Chromosomal rearrangement, urologic and male genital diseases, Gleason Score 6, Prostate cancer, Risk Factors, Internal medicine, Biomarkers, Tumor, Humans, Medicine, PTEN, Copy-number variation, In Situ Hybridization, Fluorescence, Aged, Neoplasm Staging, Retrospective Studies, Receiver operating characteristic, medicine.diagnostic_test, biology, business.industry, Biopsy, Needle, Prostate, Prostatic Neoplasms, Cancer, DNA, Neoplasm, General Medicine, Middle Aged, medicine.disease, ROC Curve, Disease Progression, biology.protein, business, Follow-Up Studies, Fluorescence in situ hybridization

Abstract

Objective To test the hypothesis that chromosomal rearrangements (CRs) can distinguish low risk of progression (LRP) from intermediate and high risk of progression (IHRP) to prostate cancer (PCa) and if these CRs have the potential to identify men with LRP on needle biopsy that harbor IHRP PCa in the prostate gland. Patients and Methods Mate pair sequencing of amplified DNA from pure populations of Gleason patterns in 154 frozen specimens from 126 patients obtained between August 14, 2001, and July 15, 2011, was used to detect CRs including abnormal junctions and copy number variations. Potential CR biomarkers with higher incidence in IHRP than in LRP to cancer and having significance in PCa biology were identified. Independent validation was performed by fluorescence in situ hybridization in 152 specimens from 124 patients obtained between February 12, 2002, and July 12, 2008. Results The number of abnormal junctions did not distinguish LRP from IHRP. Loci corresponding to genes implicated in PCa were more frequently altered in IHRP. Integrated analysis of copy number variations and microarray data yielded 6 potential markers that were more frequently detected in Gleason pattern 3 of a Gleason score 7 of PCa than in Gleason pattern 3 of a Gleason score 6 PCa. Five of those were cross-validated in an independent sample set with statistically significant areas under the receiver operating characteristic curves (AUCs) (P≤.01). Probes detecting deletions in PTEN and CHD1 had AUCs of 0.87 (95% CI, 0.77-0.97) and 0.73 (95% CI, 0.60-0.86), respectively, and probes detecting gains in ASAP1, MYC, and HDAC9 had AUCs of 0.71 (95% CI, 0.59-0.84), 0.82 (95% CI, 0.71-0.93), and 0.77 (95% CI, 0.66-0.89), respectively (for expansion of gene symbols, use search tool at www.genenames.org). Conclusion Copy number variations in regions encompassing important PCa genes were predictive of cancer significance and have the potential to identify men with LRP PCa by needle biopsy who have IHRP PCa in their prostate gland.

Published

2019

4. Personalized tumor-specific DNA junctions to detect circulating tumor in patients with endometrial cancer

Author

Matthew S. Block, Piyan Zhang, Tommaso Grassi, George Vasmatzis, Marla Kay S. Sommerfield, Stephen J. Murphy, John C. Cheville, Janet L. Schaefer Klein, Faye R. Harris, Alyssa Larish, Giannoula Karagouga, Serena Cappuccio, Minetta C. Liu, Andrea Mariani, Francesco Multinu, James B. Smadbeck, and Maureen A. Lemens

Subjects

Oncology, Physiology, Artificial Gene Amplification and Extension, Disease, Biochemistry, Polymerase Chain Reaction, law.invention, Circulating Tumor DNA, law, Basic Cancer Research, Medicine and Health Sciences, Precision Medicine, Polymerase chain reaction, Multidisciplinary, Obstetrics and Gynecology, Genomics, Body Fluids, Serous fluid, Real-time polymerase chain reaction, Blood, Medicine, Female, Anatomy, Research Article, medicine.medical_specialty, Science, Research and Analysis Methods, Blood Plasma, Uterine Cancer, Cancer Genomics, Malignant Tumors, Genomic Medicine, Uterine cancer, Cancer detection and diagnosis, Internal medicine, medicine, Genetics, Humans, Molecular Biology Techniques, Molecular Biology, Biology and life sciences, business.industry, Endometrial cancer, Gynecologic Cancers, Cancers and Neoplasms, Histology, Precision medicine, medicine.disease, Diagnostic medicine, Endometrial Neoplasms, Women's Health, business, Gynecological Tumors, Biomarkers

Abstract

Introduction There are no reliable blood biomarkers for monitoring endometrial cancer patients in the current clinical practice. Circulating tumor DNA (ctDNA) is emerging as a promising non-invasive method to measure tumor burden, define prognosis and monitor disease status in many solid cancers. In this pilot study, we investigated if unique tumor-specific DNA junctions can be used to detect ctDNA levels in patients with endometrial cancer. Methods Chromosomal rearrangements in primary tumors of eleven patients with high-grade or advanced stage endometrial cancer were determined by whole-genome Mate-Pair sequencing. Identified unique tumor-specific junctions were evaluated in pre- and six-week post-surgery patient plasma using individualized quantitative polymerase chain reaction (qPCR) assays. The relationship between clinicopathological features and detection of ctDNA was investigated. Results CtDNA was detected in 60% (6/10) of cases pre-surgery and in 27% (3/11) post-surgery. The detection of ctDNA pre-surgery was consistent with clinical indicators of aggressive disease such as advanced stage (80% - 4/5), lymphatic spread of disease (100% - 3/3), serous histology (80% - 4/5), deep myometrial invasion (100% - 3/3), lympho-vascular space invasion (75% - 3/4). All patients in which ctDNA was detected post-surgically had type II endometrial cancer. Discussion This pilot study demonstrates the feasibility of using personalized tumor-specific junction panels for detecting ctDNA in the plasma of endometrial cancer patients. Larger studies and longer follow-up are needed to validate the potential association between pre-surgical ctDNA detection and the presence of cancers with aggressive pathologic tumor characteristics or advanced stage observed in this study.

Published

2021

5. OA13.04 Chromosomal Rearrangements and Antigen Presentation as Predictors of Survival in Mesothelioma Treated With Immune Checkpoint Inhibitors

Author

Stephen J. Murphy, Mitesh J. Borad, Paul Baas, J. Schaefer Klein, Alexa McCune, Giannoula Karagouga, Julia B. Udell, John C. Cheville, Farhad Kosari, Aakash Desai, Sarah H. Johnson, Aaron S. Mansfield, James B. Smadbeck, George Vasmatzis, Tobias Peikert, Maria J. Disselhorst, and Jun Yin

Subjects

Pulmonary and Respiratory Medicine, Oncology, business.industry, Immune checkpoint inhibitors, Antigen presentation, Cancer research, medicine, Mesothelioma, medicine.disease, business

Published

2021

6. Combination targeted treatment may enhance antitumor activity in ERBB3 amplified high-grade serous endometrial cancer cells resistant to single agent targeted therapy

Author

Andrea Mariani, Janet L. Schaefer Klein, Jamie Lynch, Aaron S. Mansfield, S. John Weroha, Leila A. Jones, Michael T. Barrett, James B. Smadbeck, Alyssa Larish, Panos Z. Anastasiadis, George Vasmatzis, Mitesh J. Borad, Stephen J. Murphy, Faye R. Harris, Dorsay Sadeghian, Wan-Hsin Lin, Maureen A. Lemens, Angela Emanuel, and Ryan W. Feathers

Subjects

Cobimetinib, business.industry, medicine.medical_treatment, Cmax, Obstetrics and Gynecology, medicine.disease, Primary tumor, Targeted therapy, chemistry.chemical_compound, Serous fluid, Oncology, chemistry, ErbB, Cancer research, Medicine, Viability assay, business, PI3K/AKT/mTOR pathway

Abstract

Objectives: Up-regulation of ERBB pathways represent targetable alterations in many high grade endometrial cancers (EC); ERBB3 amplifications in particular may contribute to ineffective pathway targeting due to persistent co-activation of other ERBB binding partners, leading to tumor growth and survival. The efficacy of downstream dual-inhibition of MEK+AKT or MEK+PI3K in an ERBB3 amplified EC primary tumor was studied using a microcancer 3D ex-vivo tumor cell viability assay. Methods: Tumor was prospectively collected from a patient with stage II, FIGO grade 3, serous EC and genomic characterization was performed using multiple sequencing methods: whole exome, RNA, and MatePair analysis. Somatic mutations, structural variance, with transcriptomic profiling was used to identify potential driver pathways for subsequent pharmacologic inhibition. Primary tumor cells were grown in a three-dimensional environment and the formed microcancers were subjected to drug treatment. Cell viability was determined by the CellTiter-Glow Luminescent Assay. Data transformation and dose-response curves were generated using GraphPad PRISM using four parameter logistic regression. CompuSyn software with the Chou-Talalay method was used to analyze drug interactions and synergy. The Fractional response-Combination index (Fa-CI) plot was generated with Microsoft Excel. Capivasertib, GDC-0084, and cobimetinib were used to inhibit AKT, PI3K/mTOR, and MEK, respectively. Inhibitory effect was defined as percent reduction in ATP at clinically-defined predicted plasma maximum concentration (Cmax) values. Results: Genomic sequencing revealed overexpression of a mutated ERBB3 (c.889G>T; p.Asp297Tyr) transcript within a 6N focal amplification. Additional pertinent alterations included a MYC mid-level gain, and TP53 double hit (loss and exonic splicing silencer (ESS)). Inhibition of cell viability was moderate by single agents: capivasertib, cobimetanib, or GDC-0084, as shown by inhibitory effect values of 33.9%, 35.9% and 49.9%, respectively. Two combinations with cobimetinib demonstrated increasing inhibitory effect values of 76.2% for cobimetanib/capivasertib at the Cmax of capivasertib and 79.7% for cobimetanib/GDC-0084 at the Cmax of cobimetanib. Synergy was evidenced by a combination index 0.8 (Figure 1). Download : Download high-res image (185KB) Download : Download full-size image Conclusions: Combined inhibition of MEK and PI3K-AKT-mTOR pathways synergistically suppress viability in a patient-derived high-grade serous EC harboring a ERBB3 amplification. Further ex-vivo testing should be performed in endometrial tumors with other ERBB3 aberrations to allow generalization of results.

Published

2021

7. Chromoanasynthesis is a common mechanism that leads to ERBB2 amplifications in a cohort of early stage HER2+ breast cancer samples

Author

Athanasios Gaitatzes, Stephen J. Murphy, Farhad Kosari, Jennifer M. Kachergus, Daniel J. Serie, George Vasmatzis, Yan W. Asmann, Brian M. Necela, Mitesh J. Borad, James B. Smadbeck, E. Aubrey Thompson, Sarah A. McLaughlin, Sarah H. Johnson, Xue Wang, and Katherine B. Geiersbach

Subjects

0301 basic medicine, Cancer Research, Amplification, Replication, Biology, Chromoanagenesis, Genome, Chromoplexy, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Surgical oncology, Gene duplication, Genetics, medicine, skin and connective tissue diseases, Chromothripsis, Chromosome, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chromosome 17 (human), 030104 developmental biology, Oncology, Chromoanasynthesis, 030220 oncology & carcinogenesis, Cancer research

Abstract

Background HER2 positive (HER2+) breast cancers involve chromosomal structural alterations that act as oncogenic driver events. Methods We interrogated the genomic structure of 18 clinically-defined HER2+ breast tumors through integrated analysis of whole genome and transcriptome sequencing, coupled with clinical information. Results ERBB2 overexpression in 15 of these tumors was associated with ERBB2 amplification due to chromoanasynthesis with six of them containing single events and the other nine exhibiting multiple events. Two of the more complex cases had adverse clinical outcomes. Chromosomes 8 was commonly involved in the same chromoanasynthesis with 17. In ten cases where chromosome 8 was involved we observed NRG1 fusions (two cases), NRG1 amplification (one case), FGFR1 amplification and ADAM32 or ADAM5 fusions. ERBB3 over-expression was associated with NRG1 fusions and EGFR and ERBB3 expressions were anti-correlated. Of the remaining three cases, one had a small duplication fully encompassing ERBB2 and was accompanied with a pathogenic mutation. Conclusion Chromoanasynthesis involving chromosome 17 can lead to ERBB2 amplifications in HER2+ breast cancer. However, additional large genomic alterations contribute to a high level of genomic complexity, generating the hypothesis that worse outcome could be associated with multiple chromoanasynthetic events.

Published

2018

8. EGFR mediates activation of RET in lung adenocarcinoma with neuroendocrine differentiation characterized by ASCL1 expression

Author

Prasuna Muppa, Geoffrey C. Halling, Mariza de Andrade, Nafiseh Janaki, Stephen J. Murphy, Kaustubh N. Bhinge, Farhad Kosari, Irina V. Kovtun, Simone Terra, Tobias Peikert, Aqsa Nasir, Hamed Rahi, Marie Christine Aubry, Lin Yang, Aaron S. Mansfield, George Vasmatzis, Ping Yang, and Joanne Yi

Subjects

0301 basic medicine, Pathology, Lung Neoplasms, endocrine system diseases, Neuroendocrine differentiation, Receptor tyrosine kinase, 0302 clinical medicine, Cell Movement, Basic Helix-Loop-Helix Transcription Factors, Epidermal growth factor receptor, Phosphorylation, RNA, Small Interfering, EGFR inhibitors, biology, ASCL1, Cell Cycle, Prognosis, ErbB Receptors, Gene Expression Regulation, Neoplastic, Oncology, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Adenocarcinoma, Protein Binding, Research Paper, medicine.drug, medicine.medical_specialty, EGFR, Adenocarcinoma of Lung, 03 medical and health sciences, Gefitinib, Cell Line, Tumor, medicine, Humans, neuroendocrine, Gene Silencing, RNA, Messenger, Lung cancer, Protein Kinase Inhibitors, Cell Proliferation, business.industry, Proto-Oncogene Proteins c-ret, medicine.disease, Molecular medicine, Carcinoma, Neuroendocrine, Alternative Splicing, lung cancer, 030104 developmental biology, Cancer research, biology.protein, Neoplasm Grading, RET, business

Abstract

// Kaustubh Bhinge 1 , Lin Yang 2 , Simone Terra 6 , Aqsa Nasir 2 , Prasuna Muppa 6 , Marie Christine Aubry 6 , Joanne Yi 6 , Nafiseh Janaki 2 , Irina V. Kovtun 3 , Stephen J. Murphy 1 , Geoffrey Halling 1 , Hamed Rahi 1 , Aaron Mansfield 5 , Mariza de Andrade 4 , Ping Yang 4 , George Vasmatzis 1 , Tobias Peikert 7 , Farhad Kosari 1 1 Department of Molecular Medicine, Mayo Clinic, Rochester, MN, USA 2 Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, MN, USA 3 Department of Molecular Pharmacology and Experimental Therapeutics, Mayo Clinic, Rochester, MN, USA 4 Department of Health Sciences Research, Mayo Clinic, Rochester, MN, USA 5 Department of Medical Oncology, Mayo Clinic, Rochester, MN, USA 6 Department of Anatomic Pathology, Mayo Clinic, Rochester, MN, USA 7 Department of Pulmonary and Critical Care Medicine, Mayo Clinic, Rochester, MN, USA Correspondence to: Farhad Kosari, email: kosari.farhad@mayo.edu Keywords: ASCL1, RET, EGFR, lung cancer, neuroendocrine Received: April 10, 2016 Accepted: February 06, 2017 Published: February 24, 2017 ABSTRACT Achaete-scute homolog 1 (ASCL1) is a neuroendocrine transcription factor specifically expressed in 10-20% of lung adenocarcinomas (AD) with neuroendocrine (NE) differentiation (NED). ASCL1 functions as an upstream regulator of the RET oncogene in AD with high ASCL1 expression (A + AD). RET is a receptor tyrosine kinase with two main human isoforms; RET9 (short) and RET51 (long). We found that elevated expression of RET51 associated mRNA was highly predictive of poor survival in stage-1 A + AD (p=0.0057). Functional studies highlighted the role of RET in promoting invasive properties of A + AD cells. Further, A + AD cells demonstrated close to 10 fold more sensitivity to epidermal growth factor receptor (EGFR) inhibitors, including gefitinib, than AD cells with low ASCL1 expression. Treatment with EGF robustly induced phosphorylation of RET at Tyr-905 in A + AD cells with wild type EGFR. This phosphorylation was blocked by gefitinib and by siRNA-EGFR. Immunoprecipitation experiments found EGFR in a complex with RET in the presence of EGF and suggested that RET51 was the predominant RET isoform in the complex. In the microarray datasets of stage-1 and all stages of A + AD, high levels of EGFR and RET RNA were significantly associated with poor overall survival (p < 0.01 in both analyses). These results implicate EGFR as a key regulator of RET activation in A + AD and suggest that EGFR inhibitors may be therapeutic in patients with A + AD tumors even in the absence of an EGFR or RET mutation.

Published

2017

9. Integrated Genomic Analysis of Pancreatic Ductal Adenocarcinomas Reveals Genomic Rearrangement Events as Significant Drivers of Disease

Author

Stephen J. Murphy, Travis M. Drucker, Joema Felipe Lima, Robert R. McWilliams, Fariborz Rakhshan Rohakhtar, Timothy D. Wiltshire, Fergus J. Couch, Benjamin R. Kipp, Steven N. Hart, Faye R. Harris, Geoffrey C. Halling, James B. Smadbeck, Sarah H. Johnson, George Vasmatzis, Farhad Kosari, Gloria M. Petersen, Mark J. Truty, and Subbaya Subramanian

Subjects

0301 basic medicine, Cancer Research, endocrine system diseases, Genomics, Mice, SCID, Biology, Article, Transcriptome, Mice, 03 medical and health sciences, 0302 clinical medicine, Mice, Inbred NOD, FHIT, Cell Line, Tumor, Animals, Humans, Exome sequencing, Gene Rearrangement, Genetics, Point mutation, Wnt signaling pathway, Gene rearrangement, digestive system diseases, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, genomic DNA, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Disease Progression, Carcinoma, Pancreatic Ductal, Signal Transduction

Abstract

Many somatic mutations have been detected in pancreatic ductal adenocarcinoma (PDAC), leading to the identification of some key drivers of disease progression, but the involvement of large genomic rearrangements has often been overlooked. In this study, we performed mate pair sequencing (MPseq) on genomic DNA from 24 PDAC tumors, including 15 laser-captured microdissected PDAC and 9 patient-derived xenografts, to identify genome-wide rearrangements. Large genomic rearrangements with intragenic breakpoints altering key regulatory genes involved in PDAC progression were detected in all tumors. SMAD4, ZNF521, and FHIT were among the most frequently hit genes. Conversely, commonly reported genes with copy number gains, including MYC and GATA6, were frequently observed in the absence of direct intragenic breakpoints, suggesting a requirement for sustaining oncogenic function during PDAC progression. Integration of data from MPseq, exome sequencing, and transcriptome analysis of primary PDAC cases identified limited overlap in genes affected by both rearrangements and point mutations. However, significant overlap was observed in major PDAC-associated signaling pathways, with all PDAC exhibiting reduced SMAD4 expression, reduced SMAD-dependent TGFβ signaling, and increased WNT and Hedgehog signaling. The frequent loss of SMAD4 and FHIT due to genomic rearrangements strongly implicates these genes as key drivers of PDAC, thus highlighting the strengths of an integrated genomic and transcriptomic approach for identifying mechanisms underlying disease initiation and progression. Cancer Res; 76(3); 749–61. ©2015 AACR.

Published

2016

10. Sa1466 EUS HAS THE POTENTIAL TO EVALUATE MEMBERS OF THE TUMOR NECROSIS FACTOR (TNF) SUPERFAMILY AND IDENTIFY DRUG TARGETS ON AN INDIVIDUAL PDAC PATIENT BASIS TO GUIDE PRECISION IMMUNE-ONCOLOGY ELIGIBILITY

Author

Ferga C. Gleeson, Benjamin R. Kipp, Rory A. Jackson, Kevin C. Halling, Michael J. Levy, Rondell P. Graham, Stephen J. Murphy, and Lizhi Zhang

Subjects

Oncology, Drug, medicine.medical_specialty, business.industry, media_common.quotation_subject, Tnf superfamily, Gastroenterology, Immune system, Internal medicine, medicine, Radiology, Nuclear Medicine and imaging, Tumor necrosis factor alpha, business, media_common

Published

2020

11. Biliary tract cancer patient-derived xenografts: Surgeon impact on individualized medicine

Author

Rondell P. Graham, Michael Torbenson, Isaac Lynch, Lewis R. Roberts, Gregory J. Gores, Rory L. Smoot, Sean P. Cleary, Mark J. Truty, John R. Bergquist, David M. Nagorney, Matthew C. Hernandez, Tommy Ivanics, James B. Smadbeck, Amro M. Abdelrahman, Stephen J. Murphy, Jennifer L. Leiting, and Lin Yang

Subjects

Oncology, medicine.medical_specialty, CCA, cholangiocarcinoma, MatePair sequencing, OS, overall survival, Loss of heterozygosity, CDKN2A, TTH, time to tumor harvest, Internal medicine, Biopsy, Internal Medicine, medicine, Immunology and Allergy, iCCA, intrahepatic cholangiocarcinoma, lcsh:RC799-869, LOH, loss of heterozygosity, OPTR, overall patient take rate, PDX, patient-derived xenograft, Intrahepatic Cholangiocarcinoma, Hepatology, medicine.diagnostic_test, business.industry, Incidence (epidemiology), TTF, time to tumor formation, Hazard ratio, Gastroenterology, HRs, hazard ratios, GBCA, gallbladder carcinoma, ECM, extracellular matrix, Patient-derived xenografts, pCCA, perihilar cholangiocarcinoma, Biliary tract, biliary tract, lcsh:Diseases of the digestive system. Gastroenterology, Personalized medicine, gallbladder carcinoma, cholangiocarcinoma, business, dCCA, distal cholangiocarcinoma, Research Article

Abstract

Background & Aims Biliary tract tumors are uncommon but highly aggressive malignancies with poor survival outcomes. Due to their low incidence, research into effective therapeutics has been limited. Novel research platforms for pre-clinical studies are desperately needed. We sought to develop a patient-derived biliary tract cancer xenograft catalog. Methods With appropriate consent and approval, surplus malignant tissues were obtained from surgical resection or radiographic biopsy and implanted into immunocompromised mice. Mice were monitored for xenograft growth. Established xenografts were verified by a hepatobiliary pathologist. Xenograft characteristics were correlated with original patient/tumor characteristics and oncologic outcomes. A subset of xenografts were then genomically characterized using Mate Pair sequencing (MPseq). Results Between October 2013 and January 2018, 87 patients with histologically confirmed biliary tract carcinomas were enrolled. Of the 87 patients, 47 validated PDX models were successfully generated. The majority of the PDX models were created from surgical resection specimens (n = 44, 94%), which were more likely to successfully engraft when compared to radiologic biopsies (p = 0.03). Histologic recapitulation of original patient tumor morphology was observed in all xenografts. Successful engraftment was an independent predictor for worse recurrence-free survival. MPseq showed genetically diverse tumors with frequent alterations of CDKN2A, SMAD4, NRG1, TP53. Sequencing also identified worse survival in patients with tumors containing tetraploid genomes. Conclusions This is the largest series of biliary tract cancer xenografts reported to date. Histologic and genomic analysis of patient-derived xenografts demonstrates accurate recapitulation of original tumor morphology with direct correlations to patient outcomes. Successful development of biliary cancer tumografts is feasible and may be used to direct subsequent therapy in high recurrence risk patients. Lay summary Patient biliary tract tumors grown in immunocompromised mice are an invaluable resource in the treatment of biliary tract cancers. They can be used to guide individualized cancer treatment in high-risk patients., Graphical abstract, Highlights • Biliary tract tumors are uncommon but highly aggressive malignancies with poor survival outcomes. • Patient-derived xenografts preserve the unique histology and genetic characteristics of the original patient tumor. • Successful engraftment is an independent predictor for worse recurrence-free patient survival. • Patients with tumors containing tetraploid genomes had worse overall survival.

Published

2020

12. Neoantigenic Potential of Complex Chromosomal Rearrangements in Mesothelioma

Author

Svetomir N. Markovic, Eric S. Edell, Virginia P. Van Keulen, Enrique Garcia-Rivera, Giannoula Karagouga, Aaron O. Bungum, Vishnu Serla, Tobias Peikert, Marie Christine Aubry, Wendy K. Nevala, Janet L. Schaefer Klein, Hongzheng Ren, Stephen J. Murphy, Faye R. Harris, Sarah H. Johnson, Aaron S. Mansfield, Jin Jen, George Vasmatzis, Laura R. Elsbernd, John C. Cheville, Farhad Kosari, Courtney L. Erskine, Carlos P. Sosa, James B. Smadbeck, Haidong Dong, and Julia Udell

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Mesothelioma, In silico, T cell, Pleural Neoplasms, T-Lymphocytes, Gene Dosage, Receptors, Antigen, T-Cell, Major histocompatibility complex, Article, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Lymphocytes, Tumor-Infiltrating, Medicine, Humans, Computer Simulation, Antigens, Clonal Selection, Antigen-Mediated, Gene Rearrangement, Chromothripsis, biology, HLA-A Antigens, business.industry, Sequence Analysis, RNA, T-cell receptor, Chromoplexy, DNA, Neoplasm, Genomics, Sequence Analysis, DNA, medicine.disease, Survival Rate, 030104 developmental biology, medicine.anatomical_structure, Oncology, HLA-B Antigens, 030220 oncology & carcinogenesis, Cancer research, biology.protein, business, Peptides

Abstract

Introduction Malignant pleural mesothelioma is a disease primarily associated with exposure to the carcinogen asbestos. Whereas other carcinogen-related tumors are associated with a high tumor mutation burden, mesothelioma is not. We sought to resolve this discrepancy. Methods We used mate-pair (n = 22), RNA (n = 28), and T cell receptor sequencing along with in silico predictions and immunologic assays to understand how structural variants of chromosomes affect the transcriptome. Results We observed that inter- or intrachromosomal rearrangements were present in every specimen and were frequently in a pattern of chromoanagenesis such as chromoplexy or chromothripsis. Transcription of rearrangement-related junctions was predicted to result in many potential neoantigens, some of which were proven to bind patient-specific major histocompatibility complex molecules and to expand intratumoral T cell clones. T cells responsive to these predicted neoantigens were also present in a patient's circulating T cell repertoire. Analysis of genomic array data from the mesothelioma cohort in The Cancer Genome Atlas suggested that multiple chromothriptic-like events negatively impact survival. Conclusions Our findings represent the discovery of potential neoantigen expression driven by structural chromosomal rearrangements. These results may have implications for the development of novel immunotherapeutic strategies and the selection of patients to receive immunotherapies.

Published

2018

13. Using Genomics to Differentiate Multiple Primaries From Metastatic Lung Cancer

Author

Aaron S. Mansfield, Simone Terra, Giannoula Karagouga, Tobias Peikert, Konstantinos Leventakos, Marie Christine Aubry, Stephen J. Murphy, Benjamin R. Kipp, William R. Sukov, Faye R. Harris, Eunhee S. Yi, Sarah H. Johnson, Farhad Kosari, Geoffrey C. Halling, Aqsa Nasir, Ping Yang, Dennis A. Wigle, James B. Smadbeck, George Vasmatzis, and Vishnu Serla

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Adult, Male, Lineage (genetic), Lung Neoplasms, Somatic cell, Genomics, Disease, Chromosomal rearrangement, Germline, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Neoplasm Metastasis, Lung cancer, Lung, business.industry, Cell Differentiation, medicine.disease, Editorial Commentary, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, business

Abstract

Introduction Genomic technologies present a promising mechanism of resolving the clinical dilemma of distinguishing independent primary tumors from intrapulmonary metastases in NSCLC. We evaluated the utility of discordant mapping somatic junctions from chromosomal rearrangements in diagnosing metastatic disease compared to the current standard histologic review. Material and Methods Mate-pair sequencing was performed on DNA extracted from 76 distinct tumors from 37 cases of multiple lung cancers. Discordant mapping junctions and chromosomal copy levels were assessed for each tumor. Blood-derived DNA was available on 22 of these cases for germline assessments. A lung cancer next-generation sequencing panel was additionally performed on tumor pairs from 17 patients. Results Whereas mate-pair sequencing was able to classify lineage in all tumor pairs, histologic review appeared to misclassify lineage in 9 of 33 (27%) same-histology tumor pair comparisons. Based on disagreement between the reviewing pathologists, histopathologic lineage was classified as indeterminate in seven cases. In two cases where pathologists agreed on a metastatic call, no shared junctions were found suggesting independent primaries. Although germline junctions passing algorithmic filters were common, on average less than three were present and all had predictable structures of small focal rearrangements or transposons. Evaluation of shared chromosomal copy changes and driver mutations through a lung cancer next-generation sequencing panel, while informative, were nondefinitive in calling lineage in all cases. Conclusions The highly unique nature and prevalence of chromosomal rearrangement in lung cancers provide a useful and definitive technique for calling lineage in multifocal lung cancer.

Published

2018

14. Heterogeneity of PD-L1 expression between invasive and lepidic components of lung adenocarcinomas

Author

Aaron S. Mansfield, Stephen J. Murphy, Marie Christine Aubry, and Neil Majithia

Subjects

Cancer Research, Radiation, Lung, medicine.anatomical_structure, Oncology, business.industry, Cancer research, Medicine, Radiology, Nuclear Medicine and imaging, Pd l1 expression, business

Published

2019

15. Chromosomal catastrophe is a frequent event in clinically insignificant prostate cancer

Author

Stephen J. Murphy, John C. Cheville, Irina V. Kovtun, George Vasmatzis, and Sarah H. Johnson

Subjects

Male, Oncology, medicine.medical_specialty, Pathology, DNA Copy Number Variations, Biology, genomic rearrangements, Gleason Score 6, Prostate cancer, Transcriptional Regulator ERG, catastrophe, Internal medicine, Biomarkers, Tumor, medicine, Chromosomes, Human, Humans, gleason score, Genetic Predisposition to Disease, High-grade prostatic intraepithelial neoplasia, Chromosome Aberrations, Gene Rearrangement, Chromothripsis, Chromosome Fragile Sites, Chromosomal fragile site, Prostatic Neoplasms, Cancer, Gene rearrangement, prostate cancer, medicine.disease, Gene Expression Regulation, Neoplastic, Phenotype, Tumor progression, Disease Progression, Trans-Activators, chromothripsis, Neoplasm Grading, Research Paper

Abstract

Massive genomic rearrangements, a result of single catastrophic event termed chromothrispsis or chromosomal catastrophe, have been identified in a variety of human cancers. In a few cancer types, chromothripsis was found to be associated with poor prognosis. We performed mate-pair sequencing and analysis of structural rearrangements in 132 prostate cancer cases which included clinically insignificant Gleason score 6 tumors, clinically significant tumors of higher grade (7+) and high grade prostatic intraepithelial neoplasia. Chromothripsis was observed at least 30 per cent of the samples across different grades. Surprisingly, it was frequently observed in clinically insignificant Gleason score 6 tumors, indicating that chromothripsis does not define more aggressive phenotype. The degree of chromothripsis did not increase significantly in tumors of advanced grades and did not appear to contribute to tumor progression. Our data showed that distribution of chromothriptic rearrangements differed from that of fragile sites but correlated with the size of chromosomes. We also provided evidence that rearrangements resulting from chromothripsis were present in the cells of neighboring Gleason patterns of the same tumor. Our data suggest that that chromothripsis plays role in prostate cancer initiation.

Published

2015

16. Management of Multifocal Lung Cancer: Results of a Survey

Author

K. Robert Shen, John J. Mullon, Ping Yang, George Vasmatzis, Christopher L. Hallemeier, Stephen D. Cassivi, Alex A. Adjei, Aaron S. Mansfield, Charles F. Thomas, Dennis A. Wigle, Francis C. Nichols, Tobias Peikert, Randolph S. Marks, Shanda H. Blackmon, Mark S. Allen, Stephen J. Murphy, Marie Christine Aubry, Sarah L. Kratz, Konstantinos Leventakos, David E. Midthun, Julian R. Molina, William P. Holland, Eric S. Edell, and Yolanda I. Garces

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Male, medicine.medical_specialty, Lung Neoplasms, medicine.medical_treatment, Specialty, Article, Mediastinoscopy, 03 medical and health sciences, 0302 clinical medicine, Surveys and Questionnaires, medicine, Humans, Stage (cooking), Lung cancer, Neoplasm Staging, Response rate (survey), medicine.diagnostic_test, business.industry, Standard treatment, Mediastinum, Middle Aged, medicine.disease, Radiation therapy, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Radiology, business

Abstract

Introduction Multifocal lung cancer is an increasingly common clinical scenario, but there is lack of high-level evidence for its optimal treatment. Thus, we surveyed members of the interdisciplinary International Association for the Study of Lung Cancer on their therapeutic approaches and analyzed the resultant practice patterns. Methods We described the clinical scenario of an otherwise healthy 60-year-old man with bilateral pulmonary nodules and asked the 6373 members of the International Association for the Study of Lung Cancer whether they would recommend surgery, and if so, the extent of surgery. We also asked what other measures would be recommended to complete the staging and whether radiation therapy or chemotherapy would be suggested. Results We received 221 responses (response rate 3.5%) from multiple specialists. Most respondents (140 [63%]) recommended surgery for this scenario. Surgeons were significantly more likely to recommend surgery than were those in other specialties. Of those who recommended surgery, most would obtain a PET/CT scan to rule out distant metastases and a magnetic resonance imaging scan to rule out brain metastases; but in the absence of radiographic lymph node involvement, most would not stage the mediastinum by bronchoscopy or mediastinoscopy before resection. When surgery was not recommended or declined, respondents commonly recommended radiation. Conclusions This survey suggests that therapeutic recommendations for multifocal lung cancer are influenced to a large extent by physicians' specialty training, probably because of the lack of high-level evidence for its standard treatment. Ongoing systematic and multidisciplinary approaches with robust short-term and long-term patient outcomes may improve the quality of evidence for the optimal management of this clinical entity.

Published

2017

17. Identification of Independent Primary Tumors and Intrapulmonary Metastases Using DNA Rearrangements in Non–Small-Cell Lung Cancer

Author

Tobias Peikert, Benjamin R. Kipp, Simone Terra, George Vasmatzis, Marie Christine Aubry, Geoffrey C. Halling, Ping Yang, Michael K. Asiedu, Travis M. Drucker, Stephen J. Murphy, Faye R. Harris, Sarah H. Johnson, Dennis A. Wigle, and Eunhee S. Yi

Subjects

Gene Rearrangement, Cancer Research, Pathology, medicine.medical_specialty, Lung Neoplasms, Gene Dosage, Laser Capture Microdissection, ORIGINAL REPORTS, Sequence Analysis, DNA, Gene rearrangement, Biology, medicine.disease, DNA sequencing, law.invention, Metastasis, genomic DNA, Oncology, law, Carcinoma, Non-Small-Cell Lung, Carcinoma, medicine, Humans, Lung cancer, Polymerase chain reaction, Laser capture microdissection

Abstract

Purpose Distinguishing independent primary tumors from intrapulmonary metastases in non–small-cell carcinoma remains a clinical dilemma with significant clinical implications. Using next-generation DNA sequencing, we developed a chromosomal rearrangement–based approach to differentiate multiple primary tumors from metastasis. Methods Tumor specimens from patients with known independent primary tumors and metastatic lesions were used for lineage test development, which was then applied to multifocal tumors. Laser capture microdissection was performed separately for each tumor. Genomic DNA was isolated using direct in situ whole-genome amplification methodology, and next-generation sequencing was performed using an Illumina mate-pair library protocol. Sequence reads were mapped to the human genome, and primers spanning the fusion junctions were used for validation polymerase chain reaction. Results A total of 41 tumor samples were sequenced (33 adenocarcinomas [ADs] and eight squamous cell carcinomas [SQCCs]), with a range of three to 276 breakpoints per tumor identified. Lung tumors predicted to be independent primary tumors based on different histologic subtype did not share any genomic rearrangements. In patients with lung primary tumors and paired distant metastases, shared rearrangements were identified in all tumor pairs, emphasizing the patient specificity of identified breakpoints. Multifocal AD and SQCC samples were reviewed independently by two pulmonary pathologists. Concordance between histology and genomic data occurred in the majority of samples. Discrepant tumor samples were resolved by genome sequencing. Conclusion A diagnostic lineage test based on genomic rearrangements from mate-pair sequencing demonstrates promise for distinguishing independent primary from metastatic disease in lung cancer.

Published

2014

18. Genomic Rearrangements Define Lineage Relationships between Adjacent Lepidic and Invasive Components in Lung Adenocarcinoma

Author

Simone Terra, Dennis A. Wigle, Tobias Peikert, Charlie T. Seto, Faye R. Harris, Sarah H. Johnson, Joema Felipe Lima, Stephen J. Murphy, Marie Christine Aubry, George Vasmatzis, Michael K. Asiedu, Ping Yang, Geoffrey C. Halling, and Farhad Kosari

Subjects

Gene Rearrangement, Cancer Research, Pathology, medicine.medical_specialty, Lung Neoplasms, Lung, Lineage (genetic), Adenocarcinoma of Lung, Gene rearrangement, Adenocarcinoma, Biology, medicine.disease, Article, DNA sequencing, Germline, Pathogenesis, medicine.anatomical_structure, Oncology, medicine, Adenocarcinoma of the lung, Humans, Cell Lineage

Abstract

The development of adenocarcinoma of the lung is believed to proceed from in situ disease (adenocarcinoma in situ, AIS) to minimally invasive disease with prominent lepidic growth (minimally invasive adenocarcinoma, MIA), then to fully invasive adenocarcinoma (AD), but direct evidence for this model has been lacking. Because some lung adenocarcinomas show prominent lepidic growth (AD-L), we designed a study to address the lineage relationship between the lepidic (noninvasive) component (L) and the adjacent nonlepidic growth component representing invasive disease within individual tumors. Lineage relationships were evaluated by next-generation DNA sequencing to define large genomic rearrangements in microdissected tissue specimens collected by laser capture. We found a strong lineage relationship between the majority of adjacent lepidic and invasive components, supporting a putative AIS–AD transition. Notably, many rearrangements were detected in the less aggressive lepidic component, although the invasive component exhibited an overall higher rate of genomic rearrangement. Furthermore, a significant number of genomic rearrangements were present in histologically normal lung adjacent to tumor, but not in host germline DNA, suggesting field defects restricted to zonal regions near a tumor. Our results offer a perspective on the genetic pathogenesis underlying adenocarcinoma development and its clinical management. Cancer Res; 74(11); 3157–67. ©2014 AACR.

Published

2014

19. Lineage Relationship of Gleason Patterns in Gleason Score 7 Prostate Cancer

Author

R. Jeffrey Karnes, George Vasmatzis, John C. Cheville, Farhad Kosari, Shabnam Zarei, William R. Sukov, Stephen J. Murphy, Irina V. Kovtun, and Sarah H. Johnson

Subjects

Male, Cancer Research, Pathology, medicine.medical_specialty, Chromosome Breakpoints, Laser Capture Microdissection, Gleason Score 6, Prostate cancer, medicine, Humans, PTEN, Cell Lineage, In Situ Hybridization, Fluorescence, Laser capture microdissection, Gene Rearrangement, biology, Breakpoint, Prostatic Neoplasms, DNA, Neoplasm, Gene rearrangement, medicine.disease, Oncology, Tumor progression, Disease Progression, biology.protein, Cancer research, Neoplasm Grading, Genome-Wide Association Study

Abstract

Gleason score 7 (GS7) prostate cancer [tumors with both Gleason patterns 3 (GP3) and 4 (GP4)] portends a significantly more aggressive tumor than Gleason score 6 (GS6). It is, therefore, critical to understand the molecular relationship of adjacent GP3 and GP4 tumor cell populations and relate molecular abnormalities to disease progression. To decipher molecular relatedness, we used laser capture microdissection (LCM) and whole-genome amplification (WGA) to separately collect and amplify DNA from adjacent GP3 and GP4 cell populations from 14 cases of GS7 prostate cancer. We then carried out massively parallel mate-pair next generation sequencing (NGS) to examine the landscape of large chromosomal alterations. We identified four to 115 DNA breakpoints in GP3 and 17 to 480 in GP4. Our findings indicate that while GP3 and GP4 from the same tumor each possess unique breakpoints, they also share identical ones, indicating a common origin. Approximately 300 chromosomal breakpoints were localized to the regions affected in at least two tumors, whereas more than 3,000 were unique within the set of 14 tumors. TMPRSS2–ERG was the most recurrent rearrangement present in eight cases, in both GP3 and GP4. PTEN rearrangements were found in five of eight TMPRSS2–ERG fusion–positive cases in both GP3 and GP4. Hierarchical clustering analysis revealed that GP3 has greater breakpoint similarity to its partner GP4 compared with GP3 from different patients. We show evidence that LCM, WGA, and NGS of adjacent tumor regions provide an important tool in deciphering lineage relationships and discovering chromosomal alterations associated with tumor progression. Cancer Res; 73(11); 3275–84. ©2013 AACR.

Published

2013

20. Chromoplectic TPM3-ALK rearrangement in a patient with inflammatory myofibroblastic tumor who responded to ceritinib after progression on crizotinib

Author

Geoffrey C. Halling, Dennis A. Wigle, Steven I. Robinson, Stephen J. Murphy, Aaron S. Mansfield, Faye R. Harris, Jin Jen, Sarah H. Johnson, E. S. Yi, George Vasmatzis, Randolph S. Marks, and James B. Smadbeck

Subjects

0301 basic medicine, Male, Oncogene Proteins, Fusion, Pyridines, medicine.medical_treatment, Tropomyosin, Targeted therapy, 0302 clinical medicine, Anaplastic Lymphoma Kinase, Sulfones, chromoplexy, Myofibroblasts, IMT, Sarcoma, Standard of Care, Hematology, Chromoplexy, Protein-Tyrosine Kinases, musculoskeletal system, 3. Good health, Oncology, 030220 oncology & carcinogenesis, cardiovascular system, tissues, medicine.drug, Adult, Thoracic Tumors, medicine.drug_class, Receptor, Platelet-Derived Growth Factor beta, resistance, 03 medical and health sciences, Crizotinib, Proto-Oncogene Proteins, medicine, ROS1, Humans, ceritinib, cardiovascular diseases, Ceritinib, business.industry, Receptor Protein-Tyrosine Kinases, Original Articles, medicine.disease, ALK inhibitor, 030104 developmental biology, Pyrimidines, ALK, Drug Resistance, Neoplasm, Localized disease, Cancer research, Pyrazoles, Neoplasm Recurrence, Local, business

Abstract

Ceritinib resulted in a significant, durable response of a metastatic inflammatory myofibroblastic tumor (IMT) after failure of crizotinib. A chromoplectic TPM3–ALK rearrangement involving many known oncogenes was found in the residual IMT. Ceritinib may be useful for patients with IMT after failure of crizotinib, and chromoplexy may have a role in the oncogenesis or treatment resistance of IMTs., Background Inflammatory myofibroblastic tumors (IMTs) are rare sarcomas that can occur at any age. Surgical resection is the primary treatment for patients with localized disease; however, these tumors frequently recur. Less commonly, patients with IMTs develop or present with metastatic disease. There is no standard of care for these patients and traditional cytotoxic therapy is largely ineffective. Most IMTs are associated with oncogenic ALK, ROS1 or PDGFRβ fusions and may benefit from targeted therapy. Patient and methods We sought to understand the genomic abnormalities of a patient who presented for management of metastatic IMT after progression of disease on crizotinib and a significant and durable partial response to the more potent ALK inhibitor ceritinib. Results The residual IMT was resected based on the recommendations of a multidisciplinary tumor sarcoma tumor board and analyzed by whole-genome mate pair sequencing. Analysis of the residual, resected tumor identified a chromoplectic TPM3–ALK rearrangement that involved many other known oncogenes and was confirmed by rtPCR. Conclusions In our analysis of the treatment-resistant, residual IMT, we identified a complex pattern of genetic rearrangements consistent with chromoplexy. Although it is difficult to know for certain if these chromoplectic rearrangements preceded treatment, their presence suggests that chromoplexy has a role in the oncogenesis of IMTs. Furthermore, this patient's remarkable response suggests that ceritinib should be considered as an option after progression on crizotinib for patients with metastatic or unresectable IMT and ALK mutations.

Published

2016

21. P1.13-12 EGFR Therapy in ASCL1 Positive Lung Adenocarcinoma

Author

Tobias Peikert, Irina V. Kovtun, George Vasmatzis, Prasuna Muppa, Kaustubh N. Bhinge, Marie-Christine Aubry, Stephen J. Murphy, Farhad Kosari, Lin Yang, and Aaron S. Mansfield

Subjects

Pulmonary and Respiratory Medicine, ASCL1, Lung, medicine.anatomical_structure, Oncology, business.industry, Cancer research, Medicine, Adenocarcinoma, business, medicine.disease

Published

2018

22. Abstract 5726: Rearrangement-related peptides with neoantigenic potential in malignant pleural mesothelioma

Author

Tobias Peikert, George Vasmatzis, Svetomir N. Markovic, Julia Udell, John C. Cheville, Farhad Kosari, Carlos P. Sosa, Eric S. Edell, Aaron S. Mansfield, Jin Jen, Aaron O. Bungum, Vishnu Serla, Faye R. Harris, Sarah H. Johnson, Haidong Dong, Marie Christine Aubry, Stephen J. Murphy, Wendy K. Nevala, James B. Smadbeck, Giannoula Karagouga, Hongzheng Ren, and Janet L. Schaefer Klein

Subjects

Cancer Research, Chromothripsis, Point mutation, In silico, Chromoplexy, Biology, medicine.disease, DNA sequencing, Transcriptome, Oncology, medicine, Cancer research, Mesothelioma, Gene

Abstract

Malignant pleural mesothelioma is a disease primarily associated with exposure to the carcinogen asbestos. Consistent with this carcinogenic exposure, cytogenetic analyses have identified multiple recurrent structural chromosomal abnormalities in this malignancy, but more recent high-throughput sequencing evaluations of point mutations suggest that there is a low mutational burden in mesothelioma. Since tumor mutational burden has been correlated with responses to treatment with immune checkpoint inhibitors such as nivolumab, it was not consistent that patients with mesothelioma and low mutation burdens would have similar response rates in clinical trials with immune checkpoint inhibitors as patients with non-small cell lung cancer which is associated with a high mutation burden. In order to reconcile these differences, and given the potential for an improved understanding of the molecular pathogenesis of mesothelioma to improve therapeutic options, we used mate-pair sequencing (MPseq) and RNA sequencing (RNAseq) to understand how structural variants affect the transcriptome. MPseq differs from standard next generation sequencing approaches by tiling the whole genome with larger fragments (2-5kb) to reliably detect structural variants such as insertions, deletions and rearrangements. Amongst 22 mesothelioma specimens there were 1535 chromosomal rearrangements (median 41, range 3-298 per specimen), that resulted in junctions or novel fusions of non-coding DNA or genes. Six-hundred thirty-seven of these rearrangements (median 22, range 5-103 range per specimen) resulted in novel fusions of genes. Many of these inter- or intra-chromosomal rearrangements were consistent with a pattern of chromoanagesis such as chromoplexy or chromothripsis. Chromosomal rearrangements detected by MPseq were used to guide analysis of RNAseq data and revealed that these chromosomal junctions resulted in the expression of 179 novel amino acid sequences (median 5, 0-51 range per specimen). To determine whether transcription of chromosomal rearrangement-related junctions have neoantigenic potential, we used in silico tools to determine whether any of the expressed junctions contained peptides that could be presented by patient-specific HLA molecules. The top candidate rearrangement-related peptides with neoantigenic potential bound patient-specific HLA molecules nearly as well or as well as a positive control in competitive binding assays. Our findings represent the discovery of potential neoantigen expression driven by structural chromosomal rearrangements. These results may have implications for the development of novel therapeutic strategies, the selection of patients to receive immunotherapy, and blood-based treatment monitoring strategies. Citation Format: Aaron S. Mansfield, Tobias Peikert, James B. Smadbeck, Julia B. Udell, Farhad Kosari, Stephen J. Murphy, Hongzheng Ren, Vishnu V. Serla, Janet L. Schaefer Klein, Giannoula Karagouga, Faye R. Harris, Carlos Sosa, Sarah H. Johnson, Wendy Nevala, Svetomir N. Markovic, Aaron O. Bungum, Eric S. Edell, Haidong Dong, John C. Cheville, Marie Christine Aubry, Jin Jen, George Vasmatzis. Rearrangement-related peptides with neoantigenic potential in malignant pleural mesothelioma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 5726.

Published

2018

23. Heterogeneity of programmed cell death-ligand 1 expression in lung cancer

Author

Marie Christine Aubry, George Vasmatzis, Stephen J. Murphy, Dennis A. Wigle, Aaron S. Mansfield, Joanne Yi, and Tobias Peikert

Subjects

Pulmonary and Respiratory Medicine, business.industry, Inflammation, medicine.disease, Metastasis, Programmed cell death ligand 1, Oncology, Gene expression, microRNA, medicine, Cancer research, Epigenetics, medicine.symptom, Lung cancer, business

Abstract

sequenced the miRNA in these cells and found that cells with EMT memory have distinct miRNA profile compared to cells with transient EMT, suggesting that the epigenetic switch upon chronic IL-1b exposure leads to selective gene expression. These findings, for the first time, demonstrate a unique feature in chronic inflammation that allows cells to metastasize and eventually grow in distant organs, suggesting that these cells may serve as a reservoir for tumor metastasis and relapse. The intent of this study is to ultimately identify targets to intervene in preventing and treating metastatic behavior in lung cancer.

Published

2016

24. 70 Heterogeneity of programmed death-ligand 1 expression in multifocal lung cancer

Author

Tobias Peikert, J. Yi, Marie Christine Aubry, George Vasmatzis, Dennis A. Wigle, Aaron S. Mansfield, and Stephen J. Murphy

Subjects

Pulmonary and Respiratory Medicine, Cancer Research, Oncology, business.industry, medicine, Cancer research, Lung cancer, medicine.disease, Ligand (biochemistry), business, Programmed death

Published

2016

25. P1.02-060 EGFR Mediates Activation of RET in Lung Adenocarcinoma with Neuroendocrine Differentiation Characterized by ASCL1 Expression

Author

George Vasmatzis, Prasuna Muppa, Ping Yang, Tobias Peikert, Kaustubh N. Bhinge, Farhad Kosari, Hamed Rahi, Marie Christine Aubry, Joanne Yi, Aaron S. Mansfield, Stephen J. Murphy, Lin Yang, Mariza de Andrade, Nafiseh Janaki, Aqsa Nasir, Simone Terra, and Irina V. Kovtun

Subjects

Pulmonary and Respiratory Medicine, Oncology, medicine.medical_specialty, Lung, business.industry, medicine.disease, Neuroendocrine differentiation, ASCL1, medicine.anatomical_structure, Internal medicine, medicine, Adenocarcinoma, business, Gene

Published

2017

26. Abstract 440: Quantification of somatic chromosomal rearrangements in circulating cell-free DNA from ovarian cancers

Author

George Vasmatzis, Stephen J. Murphy, James B. Smadbeck, Aminah Jatoi, Andrea Mariani, Farhad Kosari, Irina V. Kovtun, Kimberly R. Kalli, Francesco Multinu, Geoffrey C. Halling, Faye R. Harris, and Sarah H. Johnson

Subjects

Cancer Research, Oncology, Somatic cell, Biology, Molecular biology, Circulating Cell-Free DNA

Abstract

Circulating tumor DNA (ctDNA) provides great potential for the non-invasive clinical assessment of tumor burden. We developed a monitoring protocol using next generation mate-pair sequencing to identify chromosomal rearrangement signatures in primary tumors to follow ctDNA in blood. Primary tumors of 10 patients with ovarian cancer were sequenced, and individualized tumor-specific panels were designed to detect the junctions in ctDNA. A novel algorithm was developed and applied to data generated by quantitative PCR to calculate the percent of ctDNA. Selected junctions, some with potential as therapeutic targets, were detected in pre-surgically drawn blood in eight out of ten patients. Of these eight, three demonstrated the continued presence of circulating tumor DNA post-surgery, and five had undetectable levels, consistent with their documented presence or absence of disease. The detection of somatic junctions derived from ctDNA could be an effective way to monitor ovarian cancer patients for relapse and therapy response. Citation Format: Faye R. Harris, Irina Kovtun, James Smadbeck, Francesco Multinu, Aminah Jatoi, Kimberly R. Kalli, Stephen J. Murphy, Geoffrey C. Halling, Farhad Kosari, Sarah H. Johnson, Andrea Mariani, George Vasmatzis. Quantification of somatic chromosomal rearrangements in circulating cell-free DNA from ovarian cancers. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 440.

Published

2016

27. Abstract 4513: A prognostic model for pulmonary carcinoid tumors based on large chromosomal alterations

Author

Sarah E. Kerr, Marie Christine Aubry, George Vasmatzis, Sarah H. Johnson, Julian R. Molina, Aaron S. Mansfield, Stephen J. Murphy, and Konstantinos Leventakos

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Carcinoid tumors, Cancer, Aneuploidy, Chromosomal translocation, medicine.disease, law.invention, 03 medical and health sciences, genomic DNA, 030104 developmental biology, 0302 clinical medicine, law, 030220 oncology & carcinogenesis, Internal medicine, Medicine, Macrodissection, Human genome, business, Polymerase chain reaction

Abstract

PURPOSE: Previous mutational analyses have failed to identify a predictive or prognostic marker for pulmonary carcinoid tumors (PCT). The heterogeneity of PCTs coupled with a lack of detailed information about the tumor biology, impedes patient stratification into groups based on tumor phenotypes or treatment response. We sought to use high-throughput next-generation sequencing to improve prognostication. METHODS: We stratified 37 patients with resected PCTs as low risk (n = 17) and high risk (n = 20) based on a 5 year long follow up for recurrence. Patients with no recurrence within 5 years from initial treatment were deemed low risk. Macrodissection was followed by genomic DNA isolation and next-generation sequencing was performed using an Illumina Mate Pair library protocol. Sequence reads were mapped to the human genome, and primers spanning the fusion junctions were used for validation polymerase chain reaction. RESULTS: Carcinoids commonly harbor rearrangements (median 3.5, range 1-167). Large chromosomal gains or losses were found in 24 of the cases (64.8%). We developed a prognostic score that included the total amount of genetic alterations (deletions and translocations). ROC analysis revealed an AUC of 0.76. High risk patients had a mean score of 20 and low risk patients had a mean score of 5.45 (p value = 0.03, Welch Two Sample t-test). Further analysis of the specific genetic alterations harbored by high and low risk PCTs and correlation with the pathologic and immunohistochemical information is currently underway. CONCLUSION: Large chromosomal rearrangements and aneuploidy portend a poor prognosis for patients with PCTs. Mate Pair sequencing of PCTs provides valuable prognostic information for this highly heterogeneous group of cancers. Citation Format: Konstantinos Leventakos, Aaron S. Mansfield, Stephen J. Murphy, Sarah H. Johnson, Sarah E. Kerr, Marie Christine Aubry, George Vasmatzis, Julian R. Molina. A prognostic model for pulmonary carcinoid tumors based on large chromosomal alterations. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 4513.

Published

2016

28. Abstract 1129: EGFR-mediated activation of RET in ASCL1+ lung adenocarcinoma

Author

Hamed Rahi, Julian R. Molina, Aaron S. Mansfield, Yang Lin, George Vasmatzis, Ping Yang, Dennis A. Wigle, Joanne Yi, Marie Christine Aubry, Aqsa Nasir, Farhad Kosari, Stephen J. Murphy, Simone Terra, Kaustubh N. Bhinge, and Irina V. Kovtun

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, biology, business.industry, Large cell, Population, Cancer, medicine.disease, Receptor tyrosine kinase, Gefitinib, Internal medicine, biology.protein, Cancer research, Medicine, Adenocarcinoma, business, education, Lung cancer, EGFR inhibitors, medicine.drug

Abstract

Lung cancer accounts for about 27% of the cancer related deaths in the USA annually. Pathologically, it is a very complex disease broadly classified into small cell lung cancer (SCLC) and non-small cell lung cancer (NSCLC). NSCLCs are further classified into squamous cell carcinoma, large cell carcinoma and adenocarcinoma. Achaete-scute homolog 1 (ASCL1), an important transcription factor essential in the development of neuroendocrine cells (NE) in lungs is shown to be specifically expressed in lung NE cancers and 10-20% of adenocarcinomas (AD) with NE differentiation (NED), thus suggesting a role in the pathogenesis of these tumors. Our previous study showed that ASCL1 is a regulator of the RET oncogene in AD with NED. RET is a receptor tyrosine kinase with two isoforms in humans: RET9 (short) and RET51 (long). We performed survival analysis to study implications of RET isoforms in ASCL1+ tumors and found that elevated expression of the long RET mRNA was associated with poor survival. Subsequent in vitro experiments demonstrated that treatment with EGF robustly induced phosphorylation of RET in HCC1833 and H1755 cell lines which have high endogenous levels of ASCL1 and RET but not in VMRC-LCD cell line which has high level of ASCL1 but low level of RET. EGF induced phosphorylation of RET was diminished by gefitinib and by EGFR siRNA. Immunoprecipitation results indicated direct binding between EGFR and RET in presence of EGF. Furthermore, a high throughput drug screening found 8 EGFR inhibitors that were 10 - 250 fold more cytotoxic in ASCL1+ compared with ASCL1- AD cells. These results implicate EGFR as a key regulator of RET activation in ASCL1+ AD and suggest that EGFR inhibitors may be therapeutic for this population of patients. Citation Format: Kaustubh N. Bhinge, Yang Lin, Hamed Rahi, Marie Christine Aubry, Aaron Mansfield, Irina Kovtun, Stephen Murphy, Ping Yang, Dennis Wigle, Joanne (Eunhee) Yi, Aqsa Nasir, Simone Terra, Julian Molina, George Vasmatzis, Farhad Kosari. EGFR-mediated activation of RET in ASCL1+ lung adenocarcinoma. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 1129.

Published

2016

29. Abstract 5251: ASCL1 and RET expression define a clinically relevant subgroup of lung adenocarcinoma characterized by neuroendocrine differentiation

Author

Dennis A. Wigle, Farhad Kosari, Marie Christine Aubry, Cristiane M. Ida, Ping Yang, Janet L. Schaefer Klein, George Vasmatzis, Irina V. Kovtun, Lin Yang, Stephen J. Murphy, and Sandra C. Tomaszek

Subjects

Cancer Research, Pathology, medicine.medical_specialty, biology, Cancer, Chromogranin A, Context (language use), medicine.disease, Neuroendocrine differentiation, Oncology, Cancer research, medicine, Synaptophysin, biology.protein, Biomarker (medicine), Adenocarcinoma, Lung cancer

Abstract

ASCL1 is an important regulatory transcription factor in pulmonary neuroendocrine cell development, but its value as a biomarker of neuroendocrine differentiation in lung adenocarcinoma (AD) and as a potential prognostic biomarker remains unclear. We examined ASCL1expression in lung cancer samples of varied histologic subtype, clinical outcome, and smoking status and compared to expression of traditional neuroendocrine markers. ASCL1 mRNA expression was found almost exclusively in smokers with AD, in contrast to non-smokers. ASCL1 protein expression by immunohistochemistry (IHC) correlated best with synaptophysin compared to chromogranin and CD56/NCAM. Analysis of a compendium of 367 microarray-based gene expression profiles in stage I lung adenocarcinomas identified significantly higher expression levels of the RET oncogene in ASCL1 positive tumors (ASCL1+) compared to ASCL1- tumors (q-value < 10 - 9). High levels of RET expression in ASCL1+ but not in ASCL1- tumors was associated with significantly shorter overall survival in stage 1 (p = 0.007) and in all AD (p = 0.037). RET protein expression by IHC had an association with overall survival in the context of ASCL1 expression. In silico gene set analysis and in vitro experiments by ASCL1 shRNA in AD cells with high endogenous expression of ASCL1 and RET implicated ASCL1 as a potential upstream regulator of the RET oncogene. Also, silencing ASCL1 in AD cells markedly reduced cell growth and motility. These results suggest that ASCL1 and RET expression define a clinically relevant subgroup of approximately 10% of AD characterized by neuroendocrine differentiation. Citation Format: Farhad Kosari, Cristiane M. Ida, Marie Christine Aubry, Lin Yang, Irina V. Kovtun, Janet L. Schaefer Klein, Sandra C. Tomaszek, Stephen J. Murphy, Ping Yang, Dennis Wigle, George Vasmatzis. ASCL1 and RET expression define a clinically relevant subgroup of lung adenocarcinoma characterized by neuroendocrine differentiation. [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 5251. doi:10.1158/1538-7445.AM2014-5251

Published

2014

30. Genomic rearrangements in lung adenocarcinoma: Lineage relationships between the in situ and invasive components

Author

Ping Yang, Dennis A. Wigle, Faye R. Harris, Stephen J. Murphy, Bruce W. Eckloff, Sarah H. Johnson, Marie-Christine Aubry, Joema Felipe Lima, Tobias Peikert, Charlie T. Seto, George Vasmatzis, and Michael K. Asiedu

Subjects

In situ, Cancer Research, Lung, medicine.anatomical_structure, Lineage (genetic), Oncology, business.industry, medicine, Cancer research, Adenocarcinoma, medicine.disease, business

Abstract

7568 Background: The molecular events in the initiation and progression of invasive lung adenocarcinoma remain poorly characterized. These tumors are thought to develop through an adenocarcinoma in situ (AIS), minimally invasive adenocarcinoma (MIA), invasive adenocarcinoma (AD) sequence. The goal of our study was to assess lineage relationships between in situ and invasive components within adenocarcinomas with prominent lepidic growth patterns. Methods: Frozen tissue from fourteen lung adenocarcinomas with mixtures of AD together with an adjacent in situ component (AIS), varying in ratio between 40 to 80%, were selected from our Lung Specimen Registry. Laser capture microdissection (LCM) of each component was performed separately for each tumor. Genomic DNA was isolated using a direct in situ whole genome amplification (WGA) methodology, and Next Generation Sequencing performed using an Illumina Mate Pair (MP) library protocol. MP sequence reads were mapped to the human genome and primers spanning the fusion junctions were used in validation PCRs. Results: Genomic break points identical and unique to a specific patient were identified between the AIS and AD components in 13 (of 14) cases. The total number of events per case ranged from 4-215, and the number of identical events shared between the AIS and AD components ranged from 30 to 90%. Recurrent genomic breakpoints between cases were also observed, with the 2 most common involving 8q24.3 in 5 cases and FAM19A2 on chromosome 12 in 4 cases. PCR validation of selected genomic alterations confirmed the genomic break points identified from sequencing in both the AIS and AD in all cases. Interestingly, we also observed a limited number of genomic alterations present in a zonal distribution of surrounding normal lung around the tumor mass. Conclusions: Our study demonstrates unique chromosomal alterations present in both the AIS and AD components of individual lung tumors with features of lepidic growth. These data provide evidence for lineage relationship and clonal relatedness between the two components, and provide genomic evidence for a model of stepwise progression from AIS to invasive AD in this subset of lung adenocarcinomas.

Published

2013

31. Abstract 3008: Shared gene expression alterations in prostate cancer and histologically benign prostate from patients with prostate cancer

Author

Sibel Erdogan, Stephen J. Murphy, Thomas J. Sebo, John C. Cheville, Farhad Kosari, George Vasmatzis, R. Jeffrey Karnes, Alexey A. Leontovich, and Cristiane M. Ida

Subjects

PCA3, Cancer Research, Pathology, medicine.medical_specialty, Cancer prevention, business.industry, medicine.disease, Gene expression profiling, Transcriptome, Prostate cancer, medicine.anatomical_structure, Oncology, Stroma, Prostate, medicine, Cancer research, business, Microdissection

Abstract

The frequent observations of heterogeneous tumor foci in prostate cancers indicate that the molecular changes induced by carcinogenic insult take place over wide areas within the diseased prostate. These ‘field effect’ alterations provide important clues regarding the initiation of prostate cancer (PCa) and suggest targets for cancer prevention or biomarkers for early detection. However, PCa field effect biomarkers that have passed independent validation are lacking largely because these alterations are subtle and difficult to distinguish from unrelated small changes in gene expression in the benign prostate. We postulated that shared expression alterations in PCa and in benign prostate tissue in prostate glands that contain prostate cancer (BPC) would have a higher potential for independent validation than alterations identified in BPC alone. Expression analyses was performed on PCa (n = 37) and unmatched BPC (n = 36) and contrasted with benign prostate glands (BP) from patients free of prostate cancer (n =28). These analyses identified gene alterations that were concomitantly present in both PCa and BPC. The majority of the selected markers were validated by quantitative RT-PCR in an independent set of BPC (n = 33) and BP (n =18). Validated markers included genes and non-exonic sequences not previously associated with PCa field effect. A statistical model based on CCNB1 and non-exonic NACA locus discriminated between BPC and BP in the RT-PCR set and in an external microarray dataset with accuracies of 0.84 and 0.90, respectively. Genes with predominant expression in prostate stroma were identified by expression profiling of stroma and epithelial cells collected by laser captured microdissection. Pathway analysis identified enriched GO categories in BPC stroma including PDGFR signaling. These results validate our approach for finding PCa field effect alterations and demonstrate a prostate cancer transcriptome fingerprint in the adjacent non-neoplastic cells. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr 3008. doi:1538-7445.AM2012-3008

Published

2012

32. Global gene expression profiling in normal endometrium and endometrial cancer in the same patient using laser capture microdissection can be used for data reduction

Author

J. Felipe Lima, Bobbie S. Gostout, Shabnam Zarei, George Vasmatzis, Stephen J. Murphy, J. Munz, Alexandra Meuter, and Boris Winterhoff

Subjects

Gynecology, Gene expression profiling, medicine.medical_specialty, Oncology, business.industry, Endometrial cancer, medicine, Cancer research, Obstetrics and Gynecology, Normal endometrium, medicine.disease, business, Laser capture microdissection

Published

2012