Your search keyword '"Jeffrey S. Ross"' showing total 1,609 results

151. Supplementary Figure 5 from BRAF Fusions Define a Distinct Molecular Subset of Melanomas with Potential Sensitivity to MEK Inhibition

Author

William Pao, Vincent A. Miller, Igor Puzanov, Jeffrey A. Sosman, Jennifer A. Pietenpol, Jeffrey S. Ross, Cindy L. Vnencak-Jones, Pamela L. Lyle, Brian D. Lehmann, Geoff Otto, Philip J. Stephens, Doron Lipson, and Katherine E. Hutchinson

Abstract

PDF file - 89K, Supplementary Figure S5. Comparison of reverse phase protein array (RPPA) data in TCGA skin cutaneous melanoma dataset.

Published

2023

152. Supplementary Patient Data from Emergence of Constitutively Active Estrogen Receptor-α Mutations in Pretreated Advanced Estrogen Receptor–Positive Breast Cancer

Author

Vincent A. Miller, Myles Brown, Philip Stephens, Lajos Pusztai, Steven E. Come, Stuart Schnitt, Lauren Gilmore, Tamar Rubinek, Ido Wolf, Lior Soussan-Gutman, Addie Dvir, Jeffrey S. Ross, Geoff Otto, Doron Lipson, Matthew Hawryluk, James Sun, Mirna Jarosz, Maureen T. Cronin, Justin M. Balko, Jennifer Giltnane, Carlos L. Arteaga, Henry Gómez, Massimo Cristofanilli, Jose A. Perez-Fidalgo, Jaime Ferrer-Lozano, Ana Maria Gonzalez-Angulo, Funda Meric-Bernstam, Garrett Frampton, Gilles Buchwalter, Roman Yelensky, and Rinath Jeselsohn

Abstract

XLSX file - 122K

Published

2023

153. Supplementary Figure 2 from Genetic Analysis of 779 Advanced Differentiated and Anaplastic Thyroid Cancers

Author

Daniel W. Bowles, Bryan R. Haugen, Jeffrey S. Ross, Lauren Fishbein, Rebecca E. Schweppe, Aik-Choon Tan, Daniel V. LaBarbera, Pierre Vanden Borre, Jena D. French, Stephanie Davis, Kelsi E. Deaver, Ryan Hartmaier, Ethan S. Sokol, Laurie M. Gay, and Nikita Pozdeyev

Abstract

Genetic alterations in papillary thyroid cancer

Published

2023

154. Supplementary Movie 2 from On-target Resistance to the Mutant-Selective EGFR Inhibitor Osimertinib Can Develop in an Allele-Specific Manner Dependent on the Original EGFR-Activating Mutation

Author

Christine M. Lovly, Jens Meiler, Alexa B. Schrock, Lyudmila Bazhenova, Siraj Ali, Vincent A. Miller, Jeffrey S. Ross, Jarrod A. Smith, Zhenfang Du, Vincent Huang, Huan Qiao, Yingjun Yan, David Westover, Yun-Kai Zhang, and Benjamin P. Brown

Abstract

Supplementary Movie 2

Published

2023

155. Data from Hybrid Capture–Based Genomic Profiling of Circulating Tumor DNA from Patients with Advanced Cancers of the Gastrointestinal Tract or Anus

Author

Vincent A. Miller, Siraj M. Ali, Fadi Braiteh, Craig Devoe, Philip J. Stephens, Jeffrey S. Ross, Jason K. Sicklick, Razelle Kurzrock, Joseph Chao, Richard D. Carvajal, Rodolfo Bordoni, Bryan Leyland-Jones, Lauren Young, Allison Welsh, Brady Forcier, Jon H. Chung, Samuel J. Klempner, Dean Pavlick, and Alexa B. Schrock

Abstract

Purpose: Genomic profiling of tumor biopsies from advanced gastrointestinal and anal cancers is increasingly used to inform treatment. In some cases, tissue biopsy can be prohibitive, and we sought to investigate whether analysis of blood-derived circulating tumor DNA (ctDNA) may provide a minimally invasive alternative.Experimental Design: Hybrid capture–based genomic profiling of 62 genes was performed on blood-based ctDNA from 417 patients with gastrointestinal carcinomas to assess the presence of genomic alterations (GA) and compare with matched tissue samples.Results: Evidence of ctDNA was detected in 344 of 417 samples (82%), and of these, ≥1 reportable GA was detected in 89% (306/344) of samples. Frequently altered genes were TP53 (72%), KRAS (35%), PIK3CA (14%), BRAF (8%), and EGFR (7%). In temporally matched ctDNA and tissue samples available from 25 patients, 86% of alterations detected in tissue were also detected in ctDNA, including 95% of short variants, but only 50% of amplifications. Conversely, 63% of alterations detected in ctDNA were also detected in matched tissue. Examples demonstrating clinical utility are presented.Conclusions: Genomic profiling of ctDNA detected potentially clinically relevant GAs in a significant subset of patients with gastrointestinal carcinomas. In these tumor types, most alterations detected in matched tissue were also detected in ctDNA, and with the exception of amplifications, ctDNA sequencing routinely detected additional alterations not found in matched tissue, consistent with tumor heterogeneity. These results suggest feasibility and utility of ctDNA testing in advanced gastrointestinal cancers as a complementary approach to tissue testing, and further investigation is warranted. Clin Cancer Res; 24(8); 1881–90. ©2018 AACR.

Published

2023

156. Circulating and urinary tumour DNA in urothelial carcinoma — upper tract, lower tract and metastatic disease

Author

Kyle M. Rose, Heather L. Huelster, Joshua J. Meeks, Bishoy M. Faltas, Guru P. Sonpavde, Seth P. Lerner, Jeffrey S. Ross, Philippe E. Spiess, G. Daniel Grass, Rohit K. Jain, Ashish M. Kamat, Aram Vosoughi, Liang Wang, Xuefeng Wang, and Roger Li

Subjects

Urology

Published

2023

157. Liquid Biopsy-Based Next-Generation Sequencing Is an Alternative to Tissue Molecular Profiling of Lymphoid, Plasma-Cell, and Myeloid Neoplasms

Author

Douglas A Mata, Jessica K Lee, Brennan Decker, Vignesh Shanmugam, Chelsea B Marcus, Hanna Tukachinsky, Alexa B Schrock, Nimesh R Patel, Jeffrey S Ross, Geoffrey R Oxnard, Jo-Anne Vergilio, Kamran M Mirza, Mina L Xu, and Jamal K Benhamida

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

158. Clinicopathologic and Genomic Landscape of Non-Small Cell Lung Cancer Brain Metastases

Author

Richard S P Huang, Lukas Harries, Brennan Decker, Matthew C Hiemenz, Karthikeyan Murugesan, James Creeden, Khaled Tolba, Laura P Stabile, Shakti H Ramkissoon, Timothy F Burns, and Jeffrey S Ross

Subjects

Cancer Research, Kelch-Like ECH-Associated Protein 1, Lung Neoplasms, Brain Neoplasms, NF-E2-Related Factor 2, Receptor Protein-Tyrosine Kinases, Genomics, B7-H1 Antigen, ErbB Receptors, Proto-Oncogene Proteins p21(ras), Oncology, Carcinoma, Non-Small-Cell Lung, Mutation, Humans, Retrospective Studies

Abstract

Background In patients with non-small cell lung cancer (NSCLC), 10%-40% will eventually develop brain metastases. We present the clinicopathologic, genomic, and biomarker landscape of a large cohort of NSCLC brain metastases (NSCLC-BM) samples. Materials and Methods We retrospectively analyzed 3035 NSCLC-BM tested with comprehensive genomic profiling (CGP) during routine clinical care. In addition, we compared the NSCLC-BM to a separate cohort of 7277 primary NSCLC (pNSCLC) specimens. Finally, we present data on 67 paired patients with NSCLC-BM and pNSCLC. Results Comprehensive genomic profiling analysis of the 3035 NSCLC-BMs found that the most frequent genomic alterations (GAs) were in the TP53, KRAS, CDKN2A, STK11, CDKN2B, EGFR, NKX2-1, RB1, MYC, and KEAP1 genes. In the NSCLC-BM cohort, there were significantly higher rates of several targetable GAs compared with pNSCLC, including ALK fusions, KRAS G12C mutations, and MET amplifications; and decreased frequency of MET exon14 skipping mutations (all P < .05). In the subset of NSCLC-BM (n = 1063) where concurrent PD-L1 immunohistochemistry (IHC) was performed, 54.7% of the patients with NSCLC-BM were eligible for pembrolizumab based on PD-L1 IHC (TPS ≥ 1), and 56.9% were eligible for pembrolizumab based on TMB-High status. In addition, in a series 67 paired pNSCLC and NSCLC-BM samples, 85.1% (57/67) had at least one additional GA discovered in the NSCLC-BM sample when compared with the pNSCLC sample. Conclusions Herein, we defined the clinicopathologic, genomic, and biomarker landscape of a large cohort of patients with NSCLC-BM which can help inform study design of future clinical studies for patients with NSCLC with BM. In certain clinical situations, metastatic NSCLC brain tissue or cerebral spinal fluid specimens may be needed to fully optimize personalized treatment.

Published

2022

159. Variable Genomic Landscapes of Advanced Melanomas with Heavy Pigmentation

Author

Richard S P Huang, Julie Y Tse, Lukas Harries, Ryon P Graf, Douglas I Lin, Karthikeyan Murugesan, Matthew C Hiemenz, Vamsi Parimi, Tyler Janovitz, Brennan Decker, Eric Severson, Mia A Levy, Shakti H Ramkissoon, Julia A Elvin, Jeffrey S Ross, and Erik A Williams

Subjects

Cancer Research, Oncology, Pigmentation, Mutation, Biomarkers, Tumor, Humans, Genomics, Melanoma, B7-H1 Antigen

Abstract

Background In the current study, we examined the real-world prevalence of highly pigmented advanced melanomas (HPMel) and the clinicopathologic, genomic, and ICPI biomarker signatures of this class of tumors. Materials and Methods Our case archive of clinical melanoma samples for which the ordering physician requested testing for both PD-L1 immunohistochemistry (IHC) and comprehensive genomic profiling (CGP) was screened for HPMel cases, as well as for non-pigmented or lightly pigmented advanced melanoma cases (LPMel). Results Of the 1268 consecutive melanoma biopsies in our archive that had been submitted for PD-L1 IHC, 13.0% (165/1268) were HPMel and 87.0% (1103/1268) were LPMel. In the HPMel cohort, we saw a significantly lower tumor mutational burden (TMB, median 8.8 mutations/Mb) than in the LPMel group (11.4 mut/Mb), although there was substantial overlap. In examining characteristic secondary genomic alterations (GA), we found that the frequencies of GA in TERTp, CDKN2A, TP53, and PTEN were significantly lower in the HPMel cases than in LPMel. A higher rate of GA in CTNNB1, APC, PRKAR1A, and KIT was identified in the HPMel cohort compared with LPMel. Conclusions In this study, we quantified the failure rates of melanoma samples for PD-L1 testing due to high melanin pigmentation and showed that CGP can be used in these patients to identify biomarkers that can guide treatment decisions for HPMel patients. Using this practical clinical definition for tumor pigmentation, our results indicate that HPMel are frequent at 13% of melanoma samples, and in general appear molecularly less developed, with a lower TMB and less frequent secondary GA of melanoma progression.

Published

2022

160. Spinales Lipom

Author

Kevin R. Moore, Jeffrey S. Ross, and Christopher Güttler

Published

2023

161. Spinale Dermoidzyste

Author

Kevin R. Moore, Jeffrey S. Ross, and Justus F. Kleine

Published

2023

162. Autoren

Author

Jeffrey S. Anderson, A. James Barkovich, Susan I. Blaser, Bryson Borg, Philip R. Chapman, H. Christian Davidson, P. Ellen Grant, Bronwyn E. Hamilton, H. Ric Harnsberger, Gary L. Hedlund, Chang Yueh Ho, Anna Illner, Miral D. Jhaveri, Gregory L. Katzman, Nicholas A. Koontz, Laurie A. Loevner, Daniel E. Meltzer, A. Carlson Merrow, Sara M. O’Hara, Anne G. Osborn, James M. Provenzale, Charles Raybaud, John H. Rees, Caroline D. Robson, Jeffrey S. Ross, Karen L. Salzman, Lubdha M. Shah, Hilda E. Stambuk, and Gilbert Vézina

Published

2023

163. Ewing-Sarkom

Author

Kevin R. Moore, Jeffrey S. Ross, and Stefan Felix Thieme

Published

2023

164. Spinales Astrozytom

Author

Kevin R. Moore, Jeffrey S. Ross, and Michael Scheel

Published

2023

165. Osteogenesis imperfecta

Author

Kevin R. Moore, Jeffrey S. Ross, and Christoph Csapo-Schmidt

Published

2023

166. Kaudales Regressionssyndrom

Author

Kevin R. Moore, Jeffrey S. Ross, and Anna Tietze

Published

2023

167. Achondroplasie

Author

Kevin R. Moore, Jeffrey S. Ross, and Christoph Csapo-Schmidt

Published

2023

168. Neuromyelitis-optica-Spektrum- Erkrankungen

Author

Kevin R. Moore, Jeffrey S. Ross, and Justus F. Kleine

Published

2023

169. Segmentale spinale Dysgenesie

Author

Kevin R. Moore, Jeffrey S. Ross, and Anna Tietze

Published

2023

170. Chiari-3-Malformation

Author

Kevin R. Moore, Jeffrey S. Ross, and Juliane Stöckel

Published

2023

171. Can Patients with Muscle-invasive Bladder Cancer and Fibroblast Growth Factor Receptor-3 Alterations Still Be Considered for Neoadjuvant Pembrolizumab? A Comprehensive Assessment from the Updated Results of the PURE-01 Study

Author

Jeffrey S. Ross, Filippo Pederzoli, Andrea Salonia, Ewan A. Gibb, Ryan Dittamore, Maurizio Colecchia, Joep J. de Jong, Giorgio Gandaglia, Nicola Fossati, Marco Bandini, Patrizia Giannatempo, Roberta Lucianò, Laura Marandino, Andrea Gallina, Daniele Raggi, Yang Liu, Alberto Briganti, Elai Davicioni, Andrea Necchi, Francesco Montorsi, Elena Farè, Urology, Necchi, Andrea, Raggi, Daniele, Giannatempo, Patrizia, Marandino, Laura, Farè, Elena, Gallina, Andrea, Colecchia, Maurizio, Lucianò, Roberta, Salonia, Andrea, Gandaglia, Giorgio, Fossati, Nicola, Bandini, Marco, Pederzoli, Filippo, Dittamore, Ryan, Liu, Yang, Davicioni, Elai, Ross, Jeffrey S, de Jong, Joep J, Briganti, Alberto, Montorsi, Francesco, and Gibb, Ewan A

Subjects

musculoskeletal diseases, Oncology, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Urology, medicine.medical_treatment, 030232 urology & nephrology, Pembrolizumab, Antibodies, Monoclonal, Humanized, Cystectomy, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, Internal medicine, medicine, Clinical endpoint, Humans, Hedgehog Proteins, Radiology, Nuclear Medicine and imaging, Fibroblast growth factor receptor-3 activity, Fibroblast growth factor receptor-3 mutations/fusions, Bladder cancer, business.industry, Muscles, Immunotherapy, Fibroblast growth factor receptor 3, Neoadjuvant pembrolizumab, musculoskeletal system, medicine.disease, Neoadjuvant Therapy, Fibroblast growth factor receptor-3 expression, Gene expression profiling, stomatognathic diseases, Exact test, Urinary Bladder Neoplasms, 030220 oncology & carcinogenesis, Surgery, business, Muscle-invasive bladder cancer

Abstract

In the PURE-01 study, patients with muscle-invasive bladder cancer (MIBC) who achieved a pathological complete response (CR; ypT0N0) had tumor features suggesting that pre-existing immunity may promote response. We focused on fibroblast growth factor receptor-3 (FGFR3) genomic alterations (GAs) as potential tumor resistance features. The primary endpoint of our study was CR. FGFR3 GAs were assessed via comprehensive genomic profiling of sequenced DNA (N = 112), a transcriptome-based FGFR3 activity signature, an FGFR3 subtyping model based on long noncoding RNA (lncRNA), and gene expression profiling (N = 84 for all three). We used Wilcoxon rank-sum tests, Fisher's exact test, and logistic regression analyses to analyze the associations between the various FGFR3 alterations and CR. High FGFR3 activity was defined as a signature score that was higher than the median value. Cases that were positive for lncRNA-FGFR3 subtype (lncRNA-FGFR3 active, N = 11) had consistent biology with published data: low epithelial-mesenchymal transition and immune-signature scores, high p53 activity, FGFR3 activity, and sonic hedgehog activity. In total, 17 (15.2%), 42 (50%), and 11 patients (13%) showed FGFR3 GAs or high FGFR3 signature scores, or had lncRNA-FGFR3–active tumors. Despite an association of high FGFR3 gene expression with a lower CR rate (p = 0.01), we did not find a correlation between FGFR3 activity or mutation/fusion and CR (p = 0.2 and p = 0.8). We conclude that the association of FGFR3 expression with pathological response is balanced by multiple factors. Overall, FGFR3-altered tumors should not be excluded from neoadjuvant immunotherapy studies at this time. Patient summary In patients with muscle-invasive bladder cancer treated within the PURE-01 trial, we analyzed the role of fibroblast growth factor receptor-3 (FGFR3) alterations, at the DNA and RNA levels, in association with the pathological response. We did not find any robust association, mainly when analyzing the landscape of alterations defining tumors with higher biological FGFR activity. Overall, FGFR3 activity and gene alterations did not provide sufficiently robust data to exclude patients whose tumors harbor these alterations from neoadjuvant immunotherapy trials.

Published

2021

172. Clinicopathological and genomic characterization of BCORL1-driven high-grade endometrial stromal sarcomas

Author

Brennan Decker, Richard S.P. Huang, Julia A. Elvin, Jeffrey S. Ross, Douglas I. Lin, Douglas A. Mata, Shakti H. Ramkissoon, Matthew Hiemenz, Mirna Lechpammer, and Natalie Danziger

Subjects

Leiomyosarcoma, Pathology, medicine.medical_specialty, Stromal cell, Endometrial stromal sarcoma, Histology, Biology, medicine.disease, Pathology and Forensic Medicine, Gross examination, medicine, Atypia, Nuclear atypia, Myxoid Leiomyosarcoma

Abstract

BCORL1 is a transcriptional corepressor homologous to BCOR. We describe 12 BCORL1-altered uterine sarcomas with striking resemblance to BCOR-altered endometrial stromal sarcoma (BCOR-ESS), including 5 with BCORL1 rearrangements (JAZF1-BCORL1, EP300-BCORL1, or internal BCORL1 rearrangement), 5 with inactivating BCORL1 mutations (T513fs*22, P600fs*1, R945*, R1196*, or R1265fs*4) and 2 with homozygous BCORL1 deletion. The median patient age was 57.5 years (range 33-79). An association with aggressive clinical behavior was identified. Diagnoses assigned prior to genomic testing varied: 7 tumors were previously diagnosed as ESS, 2 as high-grade uterine sarcomas, 2 as myxoid uterine leiomyosarcomas, and 1 as a uterine spindle cell neoplasm consistent with leiomyosarcoma. Tumors harbored frequent gelatinous, mucomyxoid-like appearance by gross examination and unique histology with morphological overlap with BCOR-ESS. Key microscopic features included (1) a spindle cell appearance, most often with at least focal myxoid stroma, (2) variable amounts of hypocellular fibromyxoid spindle areas with lower grade atypia and/or (3) variable amounts of epithelioid areas with higher grade atypia. Specifically, spindle and epithelioid components were present in 100 and 75% of sarcomas, respectively; myxoid stroma was identified in 83%, collagen plaques or fibrosis in 50%, and high-grade nuclear atypia was present in 42%. Like BCOR-ESS, 50% of BCORL1-altered sarcomas exhibited CDK4 amplification or CDKN2A loss. In contrast, 33% harbored NF1 alterations, while 25% had other alterations in the NF2-mTOR pathway, expanding potential therapeutic targets. In conclusion, inactivating BCORL1 genomic alterations may define a distinct subset of high-grade endometrial stromal sarcomas with biological overlap with BCOR-ESS, both of which may mimic myxoid leiomyosarcomas.

Published

2021

173. Emerging targets in upper tract urothelial carcinomas: the TERT gene

Author

Andrés, Ortíz Restrepo, Jeffrey S, Ross, Philippe E, Spiess, Andrea, Necchi, Roger, Li, and Herney Andrés, García-Perdomo

Abstract

Urothelial carcinoma (UC) is the fourth most prevalent malignancy in adults, accounting for 2.1% of cancer-related deaths. We aimed to describe the most frequent telomerase reverse transcriptase (TERT) gene mutations in this type of cancer and their relationship with the prognosis and treatment of this disease.We performed a search strategy in Medline and Embase with the following keywords: telomerase reverse transcriptase (TERT) gene and upper tract UC. We included reviews and observational studies to support the statements throughout the manuscript.The transcriptional activation of the TERT gene and subsequent telomerase activity is a prerequisite step in malignant transformation and progression. In advanced upper tract UC, TERT mutations are the most common genomic alterations in the Foundation Medicine database. C228T mutations predict distant metastasis in 60% of patients with renal pelvis cancer and 11% with ureteral cancer. Also, C228T and C250T mutations in urine DNA had a sensitivity of 87% and specificity of 94.7%. All TERT genomic alterations are inactivating short variant sequence mutations. There are no copy number gains or losses in TERT and no TERT gene rearrangements or fusions.Multiple markers, and mutations regarding the TERT gene and its promoter have been found in upper tract UC. The C250T and C228T mutations have shown promising results as diagnostic markers detected with urine tests.

Published

2022

174. The Paradoxical Role of Body Mass Index in Patients with Muscle-invasive Bladder Cancer Receiving Neoadjuvant Immunotherapy

Author

Alberto Martini, Daniele Raggi, Laura Marandino, Francesco Montorsi, Jeffrey S. Ross, Ewan A. Gibb, and Andrea Necchi

Subjects

Urinary Bladder Neoplasms, Oncology, Muscles, Urology, Humans, Radiology, Nuclear Medicine and imaging, Surgery, Immunotherapy, Neoadjuvant Therapy, Body Mass Index

Published

2022

175. Circulating Cell-Free DNA Yield and Circulating-Tumor DNA Quantity from Liquid Biopsies of 12 139 Cancer Patients

Author

Eric Allan Severson, Ole Gjoerup, Jeffrey M. Venstrom, Lucas Dennis, Douglas I. Lin, Daniel Duncan, Lei Yang, Jonathan Keith Killian, Jeffrey S. Ross, Shakti H. Ramkissoon, Dean Pavlick, Geoff Oxnard, Richard S.P. Huang, Julia A. Elvin, Jinpeng Xiao, Bernard Fendler, Matthew Hiemenz, Cui Guo, Aparna Aiyer, and Dexter X. Jin

Subjects

medicine.medical_specialty, business.industry, Biochemistry (medical), Clinical Biochemistry, Liquid Biopsy, Urology, Cancer, medicine.disease, Peripheral blood, Circulating Cell-Free DNA, Circulating Tumor DNA, Patient age, Circulating tumor DNA, Neoplasms, Mutation, Biomarkers, Tumor, Humans, Medicine, Tumor type, Stage (cooking), Liquid biopsy, business, Cell-Free Nucleic Acids, Retrospective Studies

Abstract

Background The amounts of circulating cell-free DNA (cfDNA) and circulating-tumor DNA (ctDNA) present in peripheral blood liquid biopsies can vary due to preanalytic/analytic variables. In this study, we examined the impact of patient age, sex, stage, and tumor type on cfDNA yield, ctDNA fraction, and estimated ctDNA quantity from a large cohort of clinical liquid biopsy samples. Methods We performed a retrospective analysis of 12 139 consecutive samples received for liquid biopsy (FoundationOne® Liquid) clinical testing. Results Significant differences in both cfDNA yield and estimated ctDNA quantity were observed based on the underlying tumor type that initiated the liquid biopsy analysis and the stage of the patient (P Conclusions In this study, we show that ctDNA quantity varied significantly based on patient age, sex, stage, and tumor type, which could offer an explanation as to why certain liquid biopsy specimens are more likely to fail sequencing or provide clinically meaningful results. In addition, this could affect future clinical decisions on the blood sample volumes required to allow successful liquid biopsy testing.

Published

2021

176. Comparison of PD-L1 tumor cell expression with 22C3, 28-8, and SP142 IHC assays across multiple tumor types

Author

Jake G Maule, Lani K Clinton, Ryon P Graf, Jinpeng Xiao, Geoffrey R Oxnard, Jeffrey S Ross, and Richard S P Huang

Subjects

Pharmacology, Cancer Research, Lung Neoplasms, Oncology, Carcinoma, Non-Small-Cell Lung, Immunology, Molecular Medicine, Immunology and Allergy, Humans, Immunohistochemistry, B7-H1 Antigen

Abstract

BackgroundMultiple PD-L1 immunohistochemistry (IHC) assays, including DAKO 22C3, DAKO 28-8, and Ventana SP142 PD-L1 IHC assays, have been approved by the Food and Drug Administration as a companion diagnostic (CDx) for various antiprogrammed death-1 and antiprogrammed death ligand 1 (PD-L1) based cancer immunotherapies. Here we present 22C3, 28-8, and SP142 analysis of 418 tumor specimens encountered in routine clinical practice.MethodsAll specimens were tested with 22C3, 28-8, and SP142 assays following the manufacturer’s established staining protocols.ResultsThe same PD-L1 status (defined as tumor cell expression (TC) scores with all three assays ≥1% or all ConclusionsOur data suggest that 22C3 is the most sensitive PD-L1 IHC assay for tumor cell expression, followed by 28-8 and in turn by SP-142. These findings represent an additional factor for clinical teams to consider when deciding which PD-L1 IHC assay (and in turn which CDx-associated PD-L1 based immunotherapy) is most appropriate for each individual patient.

Published

2022

177. Primary Adult Retroperitoneal Sarcoma: A Comprehensive Genomic Profiling Study

Author

Eric Allan Severson, Filippo Pederzoli, Dexter X. Jin, Marco Bandini, Jeffrey M. Venstrom, Shakti Ramkissoon, Gennady Bratslavsky, Dean V. Pavlick, Erik A. Williams, Alexa B. Schrock, Petros Grivas, Jeffrey S. Ross, Natalie Danzinger, J. Keith Killian, Sally E. Trabucco, Prasanth Reddy, Brian M. Alexander, Giuseppe Basile, Douglas I. Lin, Kimberley McGregor, Andrea Necchi, Philippe E. Spiess, and Julia A. Elvin

Subjects

0301 basic medicine, Genomic profiling, Follicular dendritic cells, medicine.medical_treatment, Liposarcoma, Biology, medicine.disease, Targeted therapy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Cancer research, medicine, biology.protein, General Earth and Planetary Sciences, Retroperitoneal sarcoma, Mdm2, Gene, Immunostaining, General Environmental Science

Abstract

Background: Adult primary retroperitoneal sarcomas (RPSs) are a group of heterogeneous tumors with different histological subtypes. Comprehensive genomic profiling (CGP) analyses have recently provided significant insights into the biology of sarcomas by identifying genomic alterations (GAs) which could benefit from targeted therapies. Methods: RPS were evaluated by CGP using next-generation sequencing of up to 406 cancer-related genes. Tumor mutational burden (TMB) was determined on 0.83 to 1.14 mut/Mb of sequenced DNA. Finally, PD-L1 expression was determined. Results: Overall, 296 cases of primary RPS were analyzed. Liposarcoma (LPS) subtype had more GA/tumor than leiomyosarcoma (LMS) subtypes, with follicular dendritic cell sarcomas harboring the highest and synovial sarcomas the lowest. TP53 and Rb1 alterations were the highest in LMS, and CDK4/6 and MDM2 in LPS. However, both the TMB and targetable GA rates were low across subtypes. PD-L1 immunostaining was low positive in 21% and high positive in 5% of patients, respectively. Conclusions: CGP analysis revealed that potentially actionable genomic targets were rare in our cohort of RPS. Moreover, RPSs seem less likely to respond to immune checkpoint inhibitors based on putative biomarkers status. Nevertheless, genomic stratification according to histological subtypes led to description of GAs that can inform future clinical trials design.

Published

2021

178. Clinicopathologic and genomic characterization of PD-L1-positive uterine cervical carcinoma

Author

Matthew Hiemenz, Richard S.P. Huang, Jeffrey S. Ross, James Haberberger, Julia A. Elvin, Daniel L. Duncan, Karthikeyan Murugesan, Douglas I. Lin, Shakti H. Ramkissoon, Natalie Danziger, and Eric Allan Severson

Subjects

0301 basic medicine, APOBEC, Oncology, Cervical cancer, medicine.medical_specialty, Pathology, business.industry, Microsatellite instability, Pembrolizumab, medicine.disease, PD-L1 Positive, Pathology and Forensic Medicine, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Internal medicine, medicine, Adenocarcinoma, Immunohistochemistry, business, Cervix

Abstract

Positive program death-ligand 1 (PD-L1) immunohistochemistry (IHC) is an approved companion diagnostic guiding the use of immune checkpoint inhibitors in uterine cervical carcinoma (CXC). The clinical and genomic features of PD-L1-positive (PD-L1positive) CXC have not been previously described. We reviewed the clinicopathologic and molecular features of 647 CXC cases that were tested using DAKO 22C3 PD-L1 IHC and comprehensive genomic profiling during the course of clinical care. PD-L1positive cases were defined via a combined positive score of ≥ 1. No differences were found in age, genetic ancestry, and HPV status of the PD-L1positive (n = 548) and PD-L1negative disease subset. The PD-L1 positivity rate varied by histologic subtype of CXC with squamous cell carcinoma (SCC) having a PD-L1 positivity rate of 91% (397/437) and usual-type adenocarcinoma’s PD-L1 positivity rate being 60% (35/58). In addition, the PD-L1 positivity rate varied depending on site of the specimen with 89.1% (261/293) positivity rate observed in cervix specimens compared to 25% (2/8) in brain metastases specimens. No significant difference in tumor mutational burden (TMB), microsatellite instability, and CD274 (encoding PD-L1) amplification was observed between PD-L1positive and PD-L1negative CXC subsets. By combining TMB with PD-L1, an additional 17 patients are eligible for pembrolizumab when compared to PD-L1 testing alone. TERT promoter alterations and APOBEC mutational signature were enriched in the PD-L1positive CXC SCC (p = 0.011, and p = 0.004, respectively). Our study reveals important prevalence data on PD-L1 positivity in CXC non-SCC and suggests that further studies in these histologic subtypes are warranted. In addition, we also provide a key framework to guide both specimen selection and future investigations of predictors of immunotherapy response in cervical cancer patients. Lastly, TERT promoter alterations and APOBEC mutational signature may be a biologically unique subset of PD-L1positive CXC SCC.

Published

2021

179. Comparative Genomic Analysis of Intrahepatic Cholangiocarcinoma: Biopsy Type, Ancestry, and Testing Patterns

Author

Jason K. Sicklick, Hanna Tukachinsky, Kimberly McGregor, Shumei Kato, Mason A. Israel, Halla Nimeiri, Geoffrey R. Oxnard, Jeffrey S. Ross, Karthikeyan Murugesan, Ethan Sokol, Razelle Kurzrock, Ole Gjoerup, and Natalie Danziger

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, IDH1, Biopsy, Cholangiocarcinoma, 03 medical and health sciences, 0302 clinical medicine, Text mining, Internal medicine, medicine, Humans, Liquid biopsy, Intrahepatic Cholangiocarcinoma, medicine.diagnostic_test, business.industry, Genomics, medicine.disease, Primary tumor, Clinical trial, Bile Ducts, Intrahepatic, 030104 developmental biology, Bile Duct Neoplasms, 030220 oncology & carcinogenesis, Biomarker (medicine), Hepatobiliary, business

Abstract

BackgroundAt diagnosis, the majority of patients with intrahepatic cholangiocarcinoma (IHCC) present with advanced disease and a poor prognosis. Comprehensive genomic profiling (CGP) early in the disease course may increase access to targeted therapies and clinical trials; however, unresolved issues remain surrounding the optimal biopsy type to submit for CGP.Patients and MethodsMutational frequencies between primary tumor biopsies (Pbx), metastatic biopsies (Mbx), and liquid biopsies (Lbx) in 1,632 patients with IHCC were compared.ResultsPotentially actionable alterations were found in 52%, 34%, and 35% of patients in the Pbx, Mbx, and Lbx cohorts, respectively. In Pbx, Mbx, and Lbx, FGFR2 rearrangements were found in 9%, 6%, and 4%, and IDH1 mutations were identified in 16%, 5%, and 9% patients, respectively. Moreover, alterations in FGFR2 and IDH1 were significantly associated with distinct ancestries, including 2.1-fold enrichment for FGFR2 rearrangements in patients with African ancestry and 1.5-fold enrichment for IDH1 mutations in patients with admixed American (Hispanic) ancestry. Finally, the publication of biomarker-driven clinical trials in IHCC correlated with changing CGP testing patterns. Significant correlations between patient characteristics and IHCC trial disclosures were observed, including a significant decrease from time between biopsy and CGP testing, and more frequent testing of primary versus metastatic samples.ConclusionOverall, because of the high likelihood of identifying actionable genomic alterations, CGP should be considered for the majority of patients with inoperable IHCC, and Lbx and Mbx can be considered as part of the diagnostic suite.Implications for PracticeComprehensive genomic profiling (CGP) should be considered for all patients with intrahepatic cholangiocarcinoma (IHCC) or suspected IHCC, as actionable alterations were commonly found in multiple genes and a wide variety of FGFR2 fusion partners were identified. The disclosure of IHCC trial data correlated with increased use of CGP, an encouraging trend that moves new therapeutic options forward for rare cancers with a rare biomarker. Although tissue from the primary lesion may identify actionable alterations at higher rates, CGP of a liquid biopsy or metastatic site can be considered, particularly if the primary tissue block is exhausted.

Published

2021

180. Supporting Patients with Cancer after Dobbs v. Jackson Women's Health Organization

Author

Andrew G Shuman, Matti S Aapro, Benjamin Anderson, Katherine Arbour, Pedro C Barata, Aditya Bardia, Eduardo Bruera, Bruce A Chabner, Herbert Chen, Edwin Choy, Pierfranco Conte, Giuseppe Curigliano, Don Dizon, Eileen O’Reilly, Antonio Tito Fojo, Hans Gelderblom, Timothy A Graubert, Jayne S Gurtler, Evan Hall, Fred R Hirsch, Ahmed Idbaih, David H Ilson, Michael Kelley, Carlo La Vecchia, Heinz Ludwig, Beverly Moy, Hyman Muss, Frans Opdam, Rebecca D Pentz, Marshall R Posner, Jeffrey S Ross, Adrian Sacher, Suresh Senan, Enrique Soto-Perez-de-Celis, Kenneth K Tanabe, Jan B Vermorken, Eric Wehrenberg-Klee, Susan E Bates, Radiation Oncology, CCA - Cancer Treatment and quality of life, and CCA - Cancer biology and immunology

Subjects

Cancer Research, Oncology, Human medicine

Abstract

In the context of cancer, whether or not to choose pregnancy termination represents a difficult and multifaceted decision. In this editorial, members of The Oncologist editorial team attempt to contextualize the potential implications of the recent Supreme Court decision in Dobbs v. Jackson Women’s Health Organizationfor patients with cancer.

Published

2022

181. Molecular Characterization of Mesothelioma: Impact of Histologic Type and Site of Origin on Molecular Landscape

Author

Ibiayi Dagogo-Jack, Russell W. Madison, Jochen K. Lennerz, Kuei-Ting Chen, Julia F. Hopkins, Alexa B. Schrock, Lauren L. Ritterhouse, Ashley Lester, Keith A. Wharton Jr, Mari Mino-Kenudson, Natalie Danziger, Yin P. Hung, Douglas A. Mata, and Jeffrey S. Ross

Subjects

Mesothelioma, Cancer Research, Lung Neoplasms, Pleural Neoplasms, Tumor Suppressor Proteins, Mesothelioma, Malignant, Immunohistochemistry, B7-H1 Antigen, Oncology, Biomarkers, Tumor, Humans, Neoplasm Recurrence, Local, Ubiquitin Thiolesterase, In Situ Hybridization, Fluorescence

Abstract

PURPOSE Mesothelioma is an aggressive malignancy with heterogeneous outcomes that are partly driven by the differential efficacy of existing therapies across histologic types and sites of origin. Large-scale molecular analysis of mesothelioma and its subtypes has the potential to inform future therapeutic strategies. MATERIALS AND METHODS We analyzed 1,294 mesotheliomas {980 pleural (malignant pleural mesothelioma [MPM]) and 314 peritoneal (malignant peritoneal mesothelioma [MPeM])} using next-generation sequencing, determined programmed death ligand-1 (PD-L1) expression and histology in a subset of cases, and assessed MTAP /CDKN2A copy-number status by fluorescence in situ hybridization and T-cell infiltration in an independent cohort. RESULTS The molecular landscape of MPM was characterized by inactivating alterations in CDKN2A (49%), BAP1 (44%), CDKN2B (42%), MTAP (34%), and NF2 (33%). Compared with epithelioid MPM, nonepithelioid (ie, biphasic and sarcomatoid) MPM had identical tumor mutational burden (median 1.25 mut/Mb, P = .63), more commonly expressed PD-L1 (74% v 51%, P = .02), and was more likely to harbor MTAP, CDKN2A, and CDKN2B copy loss ( P < .05). Fluorescence in situ hybridization confirmed that homozygous MTAP loss was enriched in nonepithelioid MPM. Relative to MPM, MPeM had comparable tumor mutational burden and PD-L1 expression. The molecular profile of MPeM was similar to MPM, with the distinction that PBRM1 alterations occurred at higher frequency (16% v 7%, P < .01). ALK rearrangements were only observed in MPeM. CONCLUSION Regardless of histology and location, the molecular landscape of mesothelioma primarily consists of inactivating alterations in tumor suppressor genes, with enrichment of certain alterations in distinct subsets (eg, MTAP loss in nonepithelioid tumors). Given the limited efficacy of current therapies for this disease, novel approaches targeting recurring alterations should be explored.

Published

2022

182. SPOP Mutations as a Predictive Biomarker for Androgen Receptor Axis-Targeted Therapy in De Novo Metastatic Castration-Sensitive Prostate Cancer

Author

Umang Swami, Ryon P. Graf, Roberto H. Nussenzveig, Virginia Fisher, Hanna Tukachinsky, Alexa B. Schrock, Gerald Li, Jeffrey S. Ross, Nicolas Sayegh, Nishita Tripathi, Vinay Mathew Thomas, Geoffrey R. Oxnard, Emmanuel S. Antonarakis, and Neeraj Agarwal

Subjects

Male, Cancer Research, Prostatic Neoplasms, Androgen Antagonists, Docetaxel, Disease-Free Survival, Prostatic Neoplasms, Castration-Resistant, Treatment Outcome, Oncology, Receptors, Androgen, Mutation, Humans, Castration, Biomarkers

Abstract

Purpose: Intensification of androgen deprivation therapy (ADT) with either docetaxel or androgen receptor axis–targeted therapies (ARAT) are the current standard of care for patients with metastatic castration-sensitive prostate cancer (mCSPC). However, biomarkers guiding treatment selection are lacking. We hypothesized that ADT intensification with ARAT, but not with docetaxel, would be associated with improved outcomes in patients with de novo (dn)-mCSPC harboring SPOP mutations. Experimental Design: Patient-level data from a deidentified nationwide (U.S.-based) prostate cancer clinico-genomic database between January 2011 and December 2021 were extracted. Eligibility criteria: diagnosis of metastatic disease within 30 days of original prostate cancer diagnosis, genomic profiling of a tissue biopsy collected within 90 days of original diagnosis, and initiation of ARAT or docetaxel within 120 days of initial diagnosis. The log-rank test and Cox proportional hazards models were used to compare time to castration-resistant prostate cancer (TTCRPC) and overall survival (OS) for patients with and without SPOP mutations undergoing ADT intensification with ARAT or docetaxel. Results: In the ARAT cohort, presence of SPOP mutation compared with wild-type was associated with more favorable TTCRPC [not reached (NR) vs. 16.7 months; adjusted HR (aHR), 0.20; 95% confidence interval (CI), 0.06–0.63; P = 0.006] and OS (NR vs. 27.2 months; aHR, 0.19; 95% CI, 0.05–0.79; P = 0.022). In contrast, SPOP mutation status was not associated with TTCRPC or OS in docetaxel-treated cohort. Conclusions: In real-world settings, SPOP mutations were associated with improved outcomes to ADT plus ARAT (but not ADT plus docetaxel) in patients with dn-mCSPC. This may serve as a predictive biomarker to guide treatment selection for patients with mCSPC.

Published

2022

183. Genomic Biomarkers and Genome-Wide Loss-of-Heterozygosity Scores in Metastatic Prostate Cancer Following Progression on Androgen-Targeting Therapies

Author

Amado J. Zurita, Ryon P. Graf, Guillermo Villacampa, Kira Raskina, Ethan Sokol, Dexter Jin, Emmanuel S. Antonarakis, Gerald Li, Richard S. P. Huang, Irene Casanova-Salas, Ana Vivancos, Joan Carles, Jeffrey S. Ross, Alexa B. Schrock, Geoffrey R. Oxnard, Joaquin Mateo, Institut Català de la Salut, [Zurita AJ] The University of Texas MD Anderson Cancer Center, Houston, TX. [Graf RP, Raskina K, Sokol E, Jin D] Foundation Medicine Inc, Cambridge, MA. [Villacampa G, Casanova-Salas I, Vivancos A, Carles J, Mateo J] Vall d'Hebron Institute of Oncology (VHIO), Barcelona, Spain. Vall d'Hebron Hospital Universitari, Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

Male, Cancer Research, Chemical Actions and Uses::Pharmacologic Actions::Physiological Effects of Drugs::Hormones, Hormone Substitutes, and Hormone Antagonists::Hormones::Androgens [CHEMICALS AND DRUGS], Otros calificadores::/uso terapéutico [Otros calificadores], Marcadors tumorals, Otros calificadores::Otros calificadores::/farmacoterapia [Otros calificadores], factores biológicos::biomarcadores::marcadores tumorales [COMPUESTOS QUÍMICOS Y DROGAS], Androgen Antagonists, Genomics, Pròstata - Càncer - Tractament, Other subheadings::Other subheadings::/drug therapy [Other subheadings], Neoplasms::Neoplasms by Site::Urogenital Neoplasms::Genital Neoplasms, Male::Prostatic Neoplasms::Prostatic Neoplasms, Castration-Resistant [DISEASES], Prostatic Neoplasms, Castration-Resistant, Oncology, neoplasias::neoplasias por localización::neoplasias urogenitales::neoplasias de los genitales masculinos::neoplasias de la próstata::neoplasias prostáticas resistentes a la castración [ENFERMEDADES], Androgens, Biomarkers, Tumor, Humans, acciones y usos químicos::acciones farmacológicas::efectos fisiológicos de los fármacos::hormonas, sustitutos de hormonas y antagonistas de hormonas::hormonas::andrógenos [COMPUESTOS QUÍMICOS Y DROGAS], Andrògens - Ús terapèutic, Other subheadings::/therapeutic use [Other subheadings], Biological Factors::Biomarkers::Biomarkers, Tumor [CHEMICALS AND DRUGS]

Abstract

PURPOSE To study the impact of standard-of-care hormonal therapies on metastatic prostate cancer (mPC) clinical genomic profiles in real-world practice, with a focus on homologous recombination-repair (HRR) genes. PATIENTS AND METHODS Targeted next-generation sequencing of 1,302 patients with mPC was pursued using the FoundationOne or FoundationOne CDx assays. Longitudinal clinical data for correlative analysis were curated via technology-enabled abstraction of electronic health records. Genomic biomarkers, including individual gene aberrations and genome-wide loss-of-heterozygosity (gLOH) scores, were compared according to biopsy location and time of sample acquisition (androgen deprivation therapy [ADT]-naïve, ADT-progression and post-ADT, and novel hormonal therapies [NHT]-progression), using chi-square and Wilcoxon rank-sum tests. Multivariable analysis used linear regression. False-discovery rate of 0.05 was applied to account for multiple comparisons. RESULTS Eight hundred forty (65%), 132 (10%), and 330 (25%) biopsies were ADT-naïve, ADT-progression, and NHT-progression, respectively. Later-stage samples were enriched for AR, MYC, TP53, PTEN, and RB1 aberrations (all adjusted P values < .05), but prevalence of HRR-related BRCA2, ATM, and CDK12 aberrations remained stable. Primary and metastatic ADT-naïve biopsies presented similar prevalence of TP53 (36% v 31%) and BRCA2 (8% v 7%) aberrations; 81% of ADT-naïve BRCA2-mutated samples presented BRCA2 biallelic loss. Higher gLOH scores were independently associated with HRR genes ( BRCA2, PALB2, and FANCA), TP53, and RB1 aberrations, and with prior exposure to hormonal therapies in multivariable analysis. CONCLUSION Prevalence of HRR-gene aberrations remains stable along mPC progression, supporting the use of diagnostic biopsies to guide poly (ADP-ribose) polymerase inhibitor treatment in metastatic castration-resistant prostate cancer. gLOH scores increase with emerging resistance to hormonal therapies, independently of individual HRR gene mutations.

Published

2022

184. Histiocytic and Dendritic Cell Sarcomas of Hematopoietic Origin Share Targetable Genomic Alterations Distinct from Follicular Dendritic Cell Sarcoma

Author

Jonathan Keith Killian, Sam Sadigh, Alison M. Friedmann, Chelsea Marcus, Valentina Nardi, Wesley R Samore, Erik A. Williams, Joseph Giessinger, Kathleen Foley-Peres, Shakti H. Ramkissoon, Riza R. Milante, Abner Louissaint, Eric Allan Severson, Daniel Duncan, Yin P Hung, Lucas R. Massoth, Lawrence R. Zukerberg, G. Petur Nielsen, Smruthy Sivakumar, Robert P. Hasserjian, Martin K. Selig, Jo-Anne Vergilio, Vinayak Venkataraman, Vikram Desphande, Judith A. Ferry, and Jeffrey S. Ross

Subjects

Cancer Research, Malignant histiocytosis, Dendritic Cell Sarcoma, Follicular, Histiocytic sarcoma, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Langerhans cell histiocytosis, medicine, Humans, Child, Histiocyte, Follicular dendritic cells, business.industry, Sarcomas, Hematopoietic Stem Cell Transplantation, Sarcoma, Dendritic Cells, Genomics, Interdigitating dendritic cell sarcoma, medicine.disease, Oncology, 030220 oncology & carcinogenesis, Follicular dendritic cell sarcoma, Histiocytoses, Mutation, Cancer research, Neoplasm Recurrence, Local, business, 030215 immunology

Abstract

Background Histiocytic and dendritic cell neoplasms are a diverse group of tumors arising from monocytic or dendritic cell lineage. Whereas the genomic features for Langerhans cell histiocytosis and Erdheim‐Chester disease have been well described, other less common and often aggressive tumors in this broad category remain poorly characterized, and comparison studies across the World Health Organization diagnostic categories are lacking. Methods Tumor samples from a total of 102 patient cases within four major subtypes of malignant histiocytic and dendritic cell neoplasms, including 44 follicular dendritic cell sarcomas (FDCSs), 41 histiocytic sarcomas (HSs), 7 interdigitating dendritic cell sarcomas (IDCSs), and 10 Langerhans cell sarcomas (LCSs), underwent hybridization capture with analysis of up to 406 cancer‐related genes. Results Among the entire cohort of 102 patients, CDKN2A mutations were most frequent across subtypes and made up 32% of cases, followed by TP53 mutations (22%). Mitogen‐activated protein kinase (MAPK) pathway mutations were present and enriched among the malignant histiocytosis (M) group (HS, IDCS, and LCS) but absent in FDCS (72% vs. 0%; p, Histiocytic and dendritic cell neoplasms are a diverse group of tumors arising from the monocytic or dendritic cell lineage. This article presents the molecular characteristics of the four major subtypes of malignant histiocytic and dendritic cell neoplasms, focusing on genomic alterations that could represent therapeutic targets.

Published

2021

185. Recurrent urothelial carcinoma-like FGFR3 genomic alterations in malignant Brenner tumors of the ovary

Author

Jeffrey S. Ross, Jeffrey M. Venstrom, Jonathan Keith Killian, Julia A. Elvin, Shakti H. Ramkissoon, and Douglas I. Lin

Subjects

Adult, 0301 basic medicine, Pathology, medicine.medical_specialty, endocrine system diseases, Serous carcinoma, Brenner Tumor, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, Ovarian carcinoma, Biomarkers, Tumor, medicine, Carcinoma, Humans, Receptor, Fibroblast Growth Factor, Type 3, Aged, Ovarian Neoplasms, business.industry, Gene Expression Profiling, Ovary, Middle Aged, medicine.disease, female genital diseases and pregnancy complications, Cystadenocarcinoma, Serous, stomatognathic diseases, Serous fluid, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Clear cell carcinoma, Female, business, Ovarian cancer, Carcinoma, Endometrioid, Clear cell

Abstract

Malignant Brenner tumor is a rare primary ovarian carcinoma subtype that may present diagnostic and therapeutic conundrums. Here, we characterize the genomics of 11 malignant Brenner tumors, which represented 0.1% of 14,153 clinically advanced ovarian carcinomas submitted for genomic profiling during the course of clinical care. At the time of molecular profiling, there was no evidence of a primary urothelial carcinoma of the urinary tract in any case. Cases with transitional-like morphologic features in the setting of variant ovarian serous or endometrioid carcinoma morphology were excluded from the final cohort. Malignant Brenner tumors exhibited CDKN2A/2B loss and oncogenic FGFR1/3 genomic alterations in 55% of cases, respectively; including recurrent FGFR3 S249C or FGFR3-TACC3 fusion in 45% of cases. FGFR3-mutated cases had an associated benign or borderline Brenner tumor pre-cursor components, further confirming the diagnosis and the ovarian site of origin. Malignant Brenner tumors were microsatellite stable, had low tumor mutational burden and exhibited no evidence of homologous recombination deficiency. PIK3CA mutations were enriched with FGFR3 alterations, while FGFR3 wild-type cases featured MDM2 amplification or TP53 mutations. The FGFR3 S249C short variant mutation was absent in 14,142 non-Brenner, ovarian carcinomas subtypes. In contrast to malignant Brenner tumors, FGFR1/2/3 alterations were present in ~5% of non-Brenner, ovarian serous, clear cell and endometrioid carcinoma subtypes, most often as FGFR1 amplification in serous carcinoma or FGFR2 short variant alterations in clear cell or endometrioid carcinomas, respectively. Finally, malignant Brenner tumors had overall distinct genomic signatures compared to FGFR-mutated ovarian serous, endometrioid, and clear cell carcinoma subtypes. This study provides insights into the molecular pathogenesis of malignant Brenner tumors, contrasts the extent of FGFR1/2/3 alterations in ovarian serous, clear cell and endometrioid carcinomas and emphasizes the potential value of novel and FDA-approved, anti-FGFR inhibitors, such as erdafitinib and pemigatinib, in refractory, FGFR3-mutated malignant Brenner tumors.

Published

2021

186. Comprehensive Genomic Profiling of Adult Renal Sarcomas Provides Insight into Disease Biology and Opportunities for Targeted Therapies

Author

Eduard Fridman, Benedito A. Carneiro, Shaolei Lu, Jennifer Webster, Russell Madison, Gennady Bratslavsky, Jeffrey S. Ross, Siraj M. Ali, Evgeny Yakirevich, Matthew Cooke, and Shamlal Mangray

Subjects

Adult, Urology, 030232 urology & nephrology, PDGFRA, 03 medical and health sciences, 0302 clinical medicine, CDKN2A, medicine, Humans, Radiology, Nuclear Medicine and imaging, Carcinoma, Renal Cell, Gene, Kidney, business.industry, Microsatellite instability, Sarcoma, Genomics, Amplicon, medicine.disease, Kidney Neoplasms, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Mutation, Cancer research, Surgery, business, KDR Gene Amplification

Abstract

Background Primary adult renal sarcomas (RSs) are rare aggressive neoplasms. Clinical outcomes are extremely poor, and optimal treatment remains challenging. Objective To identify genomic alterations (GAs) in patients with RSs. Design, setting, and participants Comprehensive genomic profiling (CGP) was conducted on DNA/RNA extracted from formalin-fixed paraffin-embedded tissue using the FoundationOne Heme/Sarcoma assay in 13 adult, locally advanced or metastatic RSs of various histologic types. Outcome measurements and statistical analysis All classes of GAs, including base substitutions, small indels, rearrangements, copy number alterations, tumor mutational burden (TMB), and microsatellite instability (MSI), were analyzed. Results and limitations CGP revealed 55 GAs (4.2 per tumor), 29 of which were clinically relevant genomic alterations (CRGAs; 2.2 per tumor). At least one CRGA was detected in nine (69%) cases. High-level amplifications (more than six copies) involving 4q12 amplicon of the KIT and PDGFRA genes were identified in four (31%) cases (two undifferentiated pleomorphic sarcomas [UPSs], one sarcomatoid renal cell carcinoma, and one myxofibrosarcoma). Both UPSs also had KDR gene amplification in addition to KIT and PDGFRA. Additional CRGAs were found in CDKN2A/B (23%), NF1 (23%), and MET (8%). All RSs were MSI stable, the mean TMB was 3.5 mutations/megabase (Mb), and none (0%) featured TMB >10 mutations/Mb. Limitations include the small sample size. Conclusions RSs are characterized by diverse histology and genomic profiles including 31% of cases with 4q12 amplification harboring the KIT/PDGFRA/KDR genes. Of the tumors, 69% carry CRGAs, which could lead to potential benefit from targeted therapies; however, a low TMB also suggests that these cases are unlikely to respond to checkpoint inhibitors. Patient summary This study provides insights into molecular biology of renal sarcoma, a rare aggressive subtype of kidney tumors. We demonstrated that renal sarcomas harbor unique, recurrent, clinically relevant molecular abnormalities that provide new opportunities for targeted therapies.

Published

2021

187. Urothelial Cancers with Small Cell Variant Histology Have Confirmed High Tumor Mutational Burden, Frequent TP53 and RB Mutations, and a Unique Gene Expression Profile

Author

Woonyoung Choi, O. Cussenot, Jean H. Hoffman-Censits, Eva Compérat, Siraj M. Ali, William Kevin Kelly, Geraldine Cancel-Tassin, Andres Matoso, Edouard J. Trabulsi, David J. McConkey, Russell Madison, Megan Hoi Yan Fong, Sumanta K. Pal, Noah M. Hahn, and Jeffrey S. Ross

Subjects

Urology, Cell, 030232 urology & nephrology, 03 medical and health sciences, 0302 clinical medicine, Biomarkers, Tumor, Humans, Medicine, Urothelial cancer, Radiology, Nuclear Medicine and imaging, Gene, Bladder cancer, business.industry, Unique gene, Genomics, medicine.disease, Phenotype, medicine.anatomical_structure, Urinary Bladder Neoplasms, Oncology, 030220 oncology & carcinogenesis, Mutation, Cancer research, Immunohistochemistry, Surgery, Tumor Suppressor Protein p53, Transcriptome, business, Variant histology

Abstract

Although predominantly urothelial, some bladder cancer and upper tract urothelial cancer (BC/UTUC) harbor histologic variants. Small cell BC (SCBC) variants comprised ˜5% of The Cancer Genome Atlas BC cohort, with a poor prognosis. We describe genomic profiles of BC/UTUC with small cell/neuroendocrine features identified in the Foundation Medicine database from June 2012 to September 2018. Of 3368 BC/UTUC samples, 3.92% (132) harbored small cell/neuroendocrine features by immunohistochemistry. Mutations were noted in: TP53 (92%), RB1 (75%), combined TP53/RB1 (72%), and TERT promoter (68%). Of the samples, 6.5% had TMB ≥ 10 mutations/Mb. RNA expression profiling of 24 pure SCBC and 51 urothelial BC (UBC) muscle-invasive samples evaluated from a separate cohort revealed a large number of differentially expressed genes with suppression of several inflammatory pathways in SCBC compared with UBC. This largest reported SCBC dataset to date confirms enrichment of signatures in SCBC similar to small cell lung cancer and describes unique gene expression compared with UBC. These findings may explain aggressive SCBC phenotype. Patient summary Small cell bladder cancer (SCBC) is an aggressive subtype that microscopically resembles aggressive small cell lung cancer (SCLC). This study confirms that SCBC shares DNA changes similar to SCLC and that SCBC expresses many genes that urothelial bladder cancer does not, possibly explaining aggressive SCBC activity.

Published

2021

188. Perspectives

Author

Jeffrey S. Ross

Subjects

Radiology, Nuclear Medicine and imaging, Neurology (clinical)

Published

2023

189. Abstract PS5-08: Comparison of PD-L1 protein expression between primary tumors and metastatic lesions in triple negative breast cancers

Author

Shakti H. Ramkissoon, Lajos Pusztai, Richard S.P. Huang, David L. Rimm, Brian M. Alexander, Kim Blenman, Jeffrey S. Ross, Mariya Rozenblit, and Natalie Danziger

Subjects

Oncology, Cancer Research, medicine.medical_specialty, biology, Tumor-infiltrating lymphocytes, business.industry, Cancer, medicine.disease, Metastasis, Immune system, Breast cancer, Internal medicine, PD-L1, medicine, biology.protein, Immunohistochemistry, business, Triple-negative breast cancer

Abstract

Background: Several recent studies that compared small cohorts of metastatic and primary lesions, suggested substantial heterogeneity in tumor infiltrating lymphocyte count, immune gene expression and PD-L1 protein expression across different metastatic sites and between primary breast cancers and metastasis. Understanding the frequency of PD-L1 positivity rates across different tissue sites can indicate differences in the immune microenvironment and may also guide biopsy site selection. We compared PD-L1 positivity on immune cells and tumor cells in primary and metastatic triple negative breast cancer tumors (TNBC).Methods: A retrospective data analysis of the Foundation Medicine PD-L1 IHC database was conducted on 340 cases of TNBC. PD-L1 positivity was determined by IHC using SP142CDx. Results are reported as percent of PD-L1 stained immune cells (IC) in the tumor area. A tumor was considered PD-L1 positive if ≥ 1% IC stained positive with PD-L1. As an exploratory analysis, PD-L1 positivity of tumor cells (TC) was also assessed. PD-L1 percent positive staining results are reported as means with 95% CI. The proportion of PD-L1 positive and negative IC and TC in primary tumors vs metastatic sites was compared using Chi-Square test. Prism 8 was used for all data analysis.Results: All patients were female, with median age 56 years (range 26-89); 179 samples were from primary tumors and 161 from metastatic lesions, representing 15 different tissue sites. Overall, PD-L1 expression on immune cells was statistically significantly more frequent in primary tumors compared to metastatic sites (63.7% [n=114] vs 42.9% [n=69]), p Table 1: Sample Characteristics and % PD-L1 positivity on immune cellsSample typeTotal N (%)N PD-L1 positive (%, 95% CI)Primary Tumor179 (52.6)114 (63.7%, 56.2% - 70.7%)Metastatic Lesion161 (47.4)69 (42.9%, 35.1% - 50.9%)Sites of MetastasesN (% of metastatic samples)N PD-L1 positive (%, 95% CI)Lung16 (10.0)11 (68.8%, 41.3% - 90.0%)Soft Tissues23 (14.3)15 (65.2%, 42.7% - 83.6%)Lymph Nodes45 (28.0)23 (51.1%, 35.8% - 66.3%)Skin21 (13.0)5 (23.8%, 8.22% - 47.2%)Liver23 (14.3)4 (17.4%, 5.00% - 38.8%)Bone12 (7.5)2 (16.7%, 2.10% - 48.4%)Brain9 (5.6)5Mediastinum4 (2.5)1Pleura2 (1.2)0Muscle1 ( Table 2: Comparison of PD-L1 positivity in primary versus metastatic sitesTissuePDL1+ Immune CellPDL1- Immune CellP valuePDL1+ Tumor CellPDL- Tumor CellP valuePrimary114650.0001151640.1313Metastasis69927154 Citation Format: Mariya Rozenblit, Richard Huang, Natalie Danziger, Brian Alexander, Shakti Ramkissoon, Kim Blenman, Jeffrey Ross, David Rimm, Lajos Pusztai. Comparison of PD-L1 protein expression between primary tumors and metastatic lesions in triple negative breast cancers [abstract]. In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr PS5-08.

Published

2021

190. Genomic Analysis of Circulating Tumor DNA in 3,334 Patients with Advanced Prostate Cancer Identifies Targetable BRCA Alterations and AR Resistance Mechanisms

Author

Andrew Simmons, Charles J. Ryan, Simon Chowdhury, Bernard Fendler, Jon Chung, Wassim Abida, Ryon Graf, Hanna Tukachinsky, Jeffrey S. Ross, Andrea Loehr, Tony Golsorkhi, Karim Fizazi, Jeffrey M. Venstrom, Russell Madison, Lucas Dennis, Samantha Morley, Ole Gjoerup, Geoffrey R. Oxnard, Brian M. Alexander, Lei Zhong, Eric Allan Severson, and Simon Paul Watkins

Subjects

0301 basic medicine, Cancer Research, biology, business.industry, Concordance, medicine.disease, Germline, Androgen receptor, 03 medical and health sciences, Exon, Prostate cancer, 030104 developmental biology, 0302 clinical medicine, Oncology, Circulating tumor DNA, Polyclonal antibodies, 030220 oncology & carcinogenesis, Cancer research, biology.protein, medicine, business, CHEK2

Abstract

Purpose: Comprehensive genomic profiling (CGP) is of increasing value for patients with metastatic castration-resistant prostate cancer (mCRPC). mCRPC tends to metastasize to bone, making tissue biopsies challenging to obtain. We hypothesized CGP of cell-free circulating tumor DNA (ctDNA) could offer a minimally invasive alternative to detect targetable genomic alterations (GA) that inform clinical care. Experimental Design: Using plasma from 3,334 patients with mCRPC (including 1,674 screening samples from TRITON2/3), we evaluated the landscape of GAs detected in ctDNA and assessed concordance with tissue-based CGP. Results: A total of 3,129 patients (94%) had detectable ctDNA with a median ctDNA fraction of 7.5%; BRCA1/2 was mutated in 295 (8.8%). In concordance analysis, 72 of 837 patients had BRCA1/2 mutations detected in tissue, 67 (93%) of which were also identified using ctDNA, including 100% of predicted germline variants. ctDNA harbored some BRCA1/2 alterations not identified by tissue testing, and ctDNA was enriched in therapy resistance alterations, as well as possible clonal hematopoiesis mutations (e.g., in ATM and CHEK2). Potential androgen receptor resistance alterations were detected in 940 of 2,213 patients (42%), including amplifications, polyclonal and compound mutations, rearrangements, and novel deletions in exon 8. Conclusions: Genomic analysis of ctDNA from patients with mCRPC recapitulates the genomic landscape detected in tissue biopsies, with a high level of agreement in detection of BRCA1/2 mutations, but more acquired resistance alterations detected in ctDNA. CGP of ctDNA is a compelling clinical complement to tissue CGP, with reflex to tissue CGP if negative for actionable variants. See related commentary by Hawkey and Armstrong, p. 2961

Published

2021

191. Optimized EGFR Blockade Strategies in EGFR Addicted Gastroesophageal Adenocarcinomas

Author

Salvatore Siena, Daniel Moya-Rull, Andrea Sartore-Bianchi, Emanuele Rausa, Annalisa Petrelli, Annunziata Gloghini, Brian M. Alexander, Daniela Conticelli, Asa Dahle-Smith, Sara Erika Bellomo, Filippo Pietrantonio, J. Lee, Siraj M. Ali, Giovanni Sgroi, Vincent A. Miller, Federica Morano, Salvatore Corallo, Uberto Fumagalli, Silvia Giordano, Maria Di Bartolomeo, Caterina Marchiò, Giovanni de Manzoni, Anna Sapino, Antonino Sottile, Stefano De Pascale, Gian Luca Baiocchi, Laura D'Errico, Silvia Marsoni, Rossella Reddavid, Simona Corso, Michele Prisciandaro, Stefania Durando, Zosia Miedzybrodzka, Cristina Migliore, Alexa B. Schrock, Russell D. Petty, Maria Apicella, Jeffrey S. Ross, Maurizio Degiuli, Sarah Molfino, Maria Bencivenga, and Stefano Ughetto

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Esophageal Neoplasms, medicine.medical_treatment, Adenocarcinoma, medicine.disease_cause, Antibodies, Targeted therapy, Cohort Studies, Mice, 03 medical and health sciences, 0302 clinical medicine, Stomach Neoplasms, Trastuzumab, Internal medicine, Monoclonal, Tumor Cells, Cultured, medicine, Animals, Humans, Molecular Targeted Therapy, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, EGFR inhibitors, Cultured, Everolimus, Cetuximab, business.industry, TOR Serine-Threonine Kinases, Antibodies, Monoclonal, Cancer, Protein-Tyrosine Kinases, medicine.disease, Tumor Cells, ErbB Receptors, HEK293 Cells, 030104 developmental biology, 030220 oncology & carcinogenesis, KRAS, business, Signal Transduction, medicine.drug

Abstract

Purpose: Gastric and gastroesophageal adenocarcinomas represent the third leading cause of cancer mortality worldwide. Despite significant therapeutic improvement, the outcome of patients with advanced gastroesophageal adenocarcinoma is poor. Randomized clinical trials failed to show a significant survival benefit in molecularly unselected patients with advanced gastroesophageal adenocarcinoma treated with anti-EGFR agents. Experimental Design: We performed analyses on four cohorts: IRCC (570 patients), Foundation Medicine, Inc. (9,397 patients), COG (214 patients), and the Fondazione IRCCS Istituto Nazionale dei Tumori (206 patients). Preclinical trials were conducted in patient-derived xenografts (PDX). Results: The analysis of different gastroesophageal adenocarcinoma patient cohorts suggests that EGFR amplification drives aggressive behavior and poor prognosis. We also observed that EGFR inhibitors are active in patients with EGFR copy-number gain and that coamplification of other receptor tyrosine kinases or KRAS is associated with worse response. Preclinical trials performed on EGFR-amplified gastroesophageal adenocarcinoma PDX models revealed that the combination of an EGFR mAb and an EGFR tyrosine kinase inhibitor (TKI) was more effective than each monotherapy and resulted in a deeper and durable response. In a highly EGFR-amplified nonresponding PDX, where resistance to EGFR drugs was due to inactivation of the TSC2 tumor suppressor, cotreatment with the mTOR inhibitor everolimus restored sensitivity to EGFR inhibition. Conclusions: This study underscores EGFR as a potential therapeutic target in gastric cancer and identifies the combination of an EGFR TKI and a mAb as an effective therapeutic approach. Finally, it recognizes mTOR pathway activation as a novel mechanism of primary resistance that can be overcome by the combination of EGFR and mTOR inhibitors. See related commentary by Openshaw et al., p. 2964

Published

2021

192. CYLD mutation characterizes a subset of HPV-positive head and neck squamous cell carcinomas with distinctive genomics and frequent cylindroma-like histologic features

Author

Brian M. Alexander, Kevin Jon Williams, Jacob R. Bledsoe, Meagan Montesion, Erik A. Williams, Julie Y. Tse, Mark C. Mochel, Krzysztof Glomski, Jeffrey S. Ross, Julia A. Elvin, and Shakti H. Ramkissoon

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Pathology, Cell, medicine.disease_cause, Article, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Cylindroma, Biomarkers, Tumor, medicine, Humans, PTEN, Missense mutation, Tumour virus infections, Aged, Aged, 80 and over, Basement membrane, Mutation, biology, Squamous Cell Carcinoma of Head and Neck, business.industry, Oral cancer, Papillomavirus Infections, Middle Aged, medicine.disease, Carcinoma, Adenoid Cystic, Deubiquitinating Enzyme CYLD, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cohort, biology.protein, Female, Histopathology, business

Abstract

Mutations in the tumor suppressor CYLD, known to be causative of cylindromas, were recently described in a subset of high-risk (hr) HPV-positive head and neck squamous cell carcinomas (HNSCC). Pathologic and genetic characterization of these CYLD-mutant carcinomas, however, remains limited. Here, we investigated whether CYLD mutations characterize a histopathologically and genomically distinct subset of hrHPV-positive HNSCC. Comprehensive genomic profiling via hybrid capture-based DNA sequencing was performed on 703 consecutive head and neck carcinomas with hrHPV sequences, identifying 148 unique cases (21%) harboring CYLD mutations. Clinical data, pathology reports, and histopathology were reviewed. CYLD mutations included homozygous deletions (n = 61/148; 41%), truncations (n = 52; 35%), missense (n = 26; 18%) and splice-site (n = 9; 6%) mutations, and in-frame deletion (n = 1; 1%). Among hrHPV-positive HNSCC, the CYLD-mutant cohort showed substantially lower tumor mutational burden than CYLD-wildtype cases (n = 555) (median 2.6 vs. 4.4 mut/Mb, p

Published

2021

193. A pan-cancer analysis of PD-L1 immunohistochemistry and gene amplification, tumor mutation burden and microsatellite instability in 48,782 cases

Author

Jonathan Keith Killian, Julie Y. Tse, Shakti H. Ramkissoon, Julia A. Elvin, James Haberberger, Richard S.P. Huang, Priti Hegde, Naomi L Ferguson, Matthew Hiemenz, Clarence Owens, Amanda Hemmerich, Jeffrey S. Ross, Brian M. Alexander, Erik A. Williams, Eric Allan Severson, Claire Edgerly, Jeffrey M. Venstrom, Jo-Anne Vergilio, Daniel L. Duncan, Douglas I. Lin, and Natalie Danziger

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Pathology, medicine.medical_treatment, Cell, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Immune system, Internal medicine, PD-L1, Gene duplication, medicine, biology, business.industry, Microsatellite instability, Immunotherapy, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Immunohistochemistry, business, Companion diagnostic

Abstract

PD-L1 immunohistochemistry (IHC) currently has the most Food and Drug Administration (FDA) approvals as a companion diagnostic (CDx) for immunotherapies in specific tumor types; however, multiple other immunotherapy biomarkers exist. We performed this study to examine and report the prevalence of PD-L1 expression in a wide variety of tumor types and examine its relationship to microsatellite instability (MSI), tumor mutational burden (TMB), and CD274 (PD-L1) gene amplification. We performed a retrospective analysis of all cases in which both PD-L1 IHC (using the DAKO 22C3 IHC assay with either tumor proportion score (TPS) or combined positive score (CPS); or the VENTANA SP142 assay with infiltrating immune cell score (IC)) and comprehensive genomic profiling (CGP) were tested at Foundation Medicine between January 2016 and November 2019. Of note, PD-L1 positivity is defined per the CDx indication and tumor proportion score (TPS ≥ 1) for indications without a CDx claim; and TMB positivity is defined as ≥10 mutations/Mb. A total of 48,782 cases were tested for PD-L1 IHC and CGP. Immune cell expression of PD-L1 was more frequently identified than tumor cell expression of PD-L1. We saw a high correlation between PD-L1 expression and CD274 gene amplification (p

Published

2021

194. Early-onset metastatic and clinically advanced prostate cancer is a distinct clinical and molecular entity characterized by increased TMPRSS2–ERG fusions

Author

Ericka M. Ebot, Sarki A. Abdulkadir, Michael C. Burns, Garrett M. Frampton, Maha Hussain, Jeffrey S. Ross, and Zachary R. Chalmers

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Oncogene Proteins, Fusion, Urology, 030232 urology & nephrology, Disease, SPOP, TMPRSS2, Article, 03 medical and health sciences, Prostate cancer, 0302 clinical medicine, Internal medicine, Biopsy, Biomarkers, Tumor, medicine, Humans, PTEN, Age of Onset, Neoplasm Metastasis, Lymph node, Aged, Retrospective Studies, Aged, 80 and over, medicine.diagnostic_test, biology, business.industry, High-Throughput Nucleotide Sequencing, Prostatic Neoplasms, Middle Aged, Prognosis, medicine.disease, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, business, Erg, Follow-Up Studies

Abstract

BACKGROUND: Men with early-onset prostate cancer are at increased risk for cancer-related mortality, yet the prevalence and spectrum of molecular alterations in this patient population is unknown. Here, we analyze comprehensive genomic profiling data to characterize the molecular drivers of early-onset prostate cancer in patients with clinically advanced and metastatic disease. METHODS: Next-generation sequencing was ordered as a part of routine clinical care for 10,189 patients with prostate cancer between 02/2013 and 03/2020 using commercially available comprehensive genomic profiling. RESULTS: Deidentified genomic data for 10,189 unique patients with prostate cancer were obtained (median age = 66 y, range = 34–90 y). 439 patients were ≤50 y (4.3%), 1928 patients were between ages of 51 and 59 y (18.9%), and 7822 patients were ≥60 y (76.8%). Of metastatic biopsy sites, lymph node, liver, and bone were the most common in all groups, accounting for 60.2% of all specimens. Overall, 97.4% of patients harbored pathologic genomic alterations. The most commonly altered genes were TP53, TMPRSS2–ERG, PTEN, AR, MYC, MLL2, RAD21, BRCA2, APC, SPOP, PIK3CA, RB1, MLL3, CDK12, ATM, and CTNNB1. Patients ≤50 y harbored significantly more TMPRSS2–ERG fusions than patients ≥60 y, while AR copy number alterations as well as SPOP and ASXL1 mutations were significantly less frequent. CONCLUSIONS: Clinically advanced and metastatic early-onset prostate cancer is a distinct clinical subgroup with characteristic genomic alterations including increased frequency of TMPRSS2–ERG fusions and fewer AR, SPOP, and ASXL1 alterations.

Published

2021

195. Predictive Biomarkers for Immune Checkpoint Inhibitors in Metastatic Breast Cancer

Author

Prashanth Ashok Kumar, Ethan Sokol, Richard S.P. Huang, Shakti H. Ramkissoon, Eric Allan Severson, Jeffrey S. Ross, Abirami Sivapiragasam, Natalie Danziger, Lee A. Albacker, Jonathan Keith Killian, Kimberly McGregor, and Charlotte Brown

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_treatment, B7-H1 Antigen, 0302 clinical medicine, Neoplasm Metastasis, Precision Medicine, skin and connective tissue diseases, Immune Checkpoint Inhibitors, Original Research, Aged, 80 and over, biology, comprehensive genomic profiling, Middle Aged, Metastatic breast cancer, 030220 oncology & carcinogenesis, Immunohistochemistry, Mdm2, Female, immunotherapy, metastatic breast cancer, Databases, Nucleic Acid, Adult, medicine.medical_specialty, tumor mutational burden, Clinical Decision-Making, STK11, Breast Neoplasms, Young Adult, 03 medical and health sciences, Breast cancer, Predictive Value of Tests, PD-L1, Internal medicine, Biomarkers, Tumor, medicine, Humans, Radiology, Nuclear Medicine and imaging, Aged, business.industry, Gene Expression Profiling, Clinical Cancer Research, biomarkers, Microsatellite instability, Immunotherapy, medicine.disease, 030104 developmental biology, Drug Resistance, Neoplasm, PD‐L1, Mutation, biology.protein, microsatellite instability, Transcriptome, business

Abstract

We examined a large dataset of female metastatic breast cancers (MBCs) profiled with comprehensive genomic profiling (CGP) to identify the prevalence and distribution of immunotherapy responsiveness‐associated biomarkers. DNA was extracted from 3831 consecutive MBCs: 1237 (ERpos/HER2 neg), 1953 ERneg/HER2 amp, and 641 triple‐negative breast cancer (TNBC). CGP was performed using the FoundationOne® or FoundationOne®CDx NGS assay. Tumor mutational burden (TMB) and microsatellite instability (MSI) were determined in a subset of cases. PD‐L1 expression in immunocytes in a subset of cases was determined by immunohistochemistry using the companion diagnostic VENTANA PD‐L1 SP142 Assay. The median age of the cohort was 54 years (range 20–89). Genomic alterations (GAs)/tumor were similar (range: 5.9–7.3). Markers of potential immune checkpoint inhibitor (ICPI) benefit included: CD274 (PD‐L1) amplification (1%–3%), BRAF GA (1%–4%), TMB of ≥10 mutations/Mb (8%–12%), MSI‐high (0.1%–0.4%), PBRM1 GA (1%), and positive PD‐L1 staining of immunocytes ranging from 13% in ERpos/HER2 neg and 33% in ERneg/HER2 amp to 47% in the TNBC group. Potential markers of ICPI resistance included inactivating STK11 GA (1%–2%) and MDM2 amplification (3%–6%). MTOR pathway targets were common with lowest frequency in TNBC. ERBB2 short variant mutations were most frequent ERpos/HER2 neg and absent in TNBC. BRCA1/2 GA were least frequent in ERneg/HER2 amp. The demonstrations of clinical benefit of immunotherapy in MBC support the need for development and utilization of biomarkers to guide the use of ICPIs for these patients. In addition to guiding therapy selection, CGP shows potential to identify GA linked to response and resistance to ICPI in MBC., Both our results and published literature suggest that in addition to guiding targeted therapy selection, comprehensive genomic profiling shows potential to identify genomic alterations linked to response and resistance to immune checkpoint inhibitor (ICPI) therapy in metastatic breast cancer (MBC). The demonstration of clinical benefit of immune checkpoint blockade in MBC supports the need for the development of biomarkers used to guide the use of ICPI drugs for these patients.

Published

2020

196. ERBB2 Pathway in Biliary Tract Carcinoma: Clinical Implications of a Targetable Pathway

Author

Assaf Moore, Jeffrey S. Ross, Baruch Brenner, Riad Haddad, Aaron Sulkes, Irit Ben-Aharon, Oded Jacobi, and Tal Goshen-Lago

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Receptor, ErbB-2, medicine.medical_treatment, Clone (cell biology), Disease, Targeted therapy, Cholangiocarcinoma, ErbB, Internal medicine, medicine, Humans, Clinical significance, Liquid biopsy, Gastrointestinal Neoplasms, Chemotherapy, business.industry, Hematology, Trastuzumab, Bile Ducts, Intrahepatic, Bile Duct Neoplasms, Mutation, Neratinib, business, Signal Transduction, medicine.drug

Abstract

Background/Aims: Current chemotherapy regimens for cholangiocarcinoma (CCA) yield poor outcomes, with a median overall survival of Methods: Tissue samples of intrahepatic CCA (IHCC) and extrahepatic CCA (EHCC) underwent NGS for somatic aberrations. The clinical outcomes for patients treated with anti-HER2 agents were evaluated. Results: A total of 1,863 CCA cases (1,615 IHCCs and 248 EHCCs) underwent NGS, and they revealed a high prevalence of ERBB alterations (IHCC, 4.2%; EHCC, 9.7%). Among these, 23.8% of the IHCCs and 53.6% of the EHCCs had a point mutation in ERBB2, and 66.6% of the IHCCs and 41.2% of the EHCCs had ERBB copy number amplification. Three EHCC patients were diagnosed at our institute with ERBB/EGFR aberrations; 2 patients were treated with neratinib and 1 patient with a chemotherapy-trastuzumab combination. All 3 achieved disease stabilization and a clinical benefit. One patient underwent a liquid biopsy before and after 3 months of treatment, demonstrating disappearance of the ERBB2 clone and emergence of a Myc-mutated clone after treatment. Conclusions: The genomic landscape of CCAs may harbor targetable alterations, especially in the ERBB/EGFR pathway. These alterations may have clinical significance in everyday practice.

Published

2020

197. Comprehensive Genomic Profiling of Carcinoma of Unknown Primary Origin: Retrospective Molecular Classification Considering the CUPISCO Study Design

Author

Holger Moch, Marlene Thomas, Andreas Beringer, Ethan Sokol, Alwin Krämer, Jeffrey S. Ross, Ferran Losa, Giulia Baciarello, Julia A. Elvin, Dexter X. Jin, Linda Mileshkin, Nhu Ngo, and University of Zurich

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Cancer Diagnostics and Molecular Pathology, Lung Neoplasms, medicine.medical_treatment, 610 Medicine & health, Targeted therapy, law.invention, Loss of heterozygosity, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, law, Internal medicine, 10049 Institute of Pathology and Molecular Pathology, Proto-Oncogene Proteins, ROS1, Carcinoma, Biomarkers, Tumor, Medicine, Unknown primary tumors, Genetic profiling, Humans, Molecular targeted therapy, Retrospective Studies, business.industry, Gene Expression Profiling, Microsatellite instability, Genomics, Protein-Tyrosine Kinases, medicine.disease, Clinical trial, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Adenocarcinoma, Neoplasms, Unknown Primary, business

Abstract

Background Carcinoma of unknown primary origin (CUP) accounts for 2%–5% of newly diagnosed advanced malignancies, with chemotherapy as the standard of care. CUPISCO (NCT03498521) is an ongoing randomized trial using comprehensive genomic profiling (CGP) to assign patients with CUP to targeted or immunotherapy treatment arms based on genomic profiling. We performed a retrospective analysis of CUP cases referred for CGP to determine how many were potentially eligible for enrollment into an experimental CUPISCO arm. Materials and Methods Centrally reviewed adenocarcinoma and undifferentiated CUP specimens in the FoundationCore database were analyzed using the hybrid capture‐based FoundationOne CDx assay (mean coverage, >600×). Presence of genomic alterations, microsatellite instability (MSI), tumor mutational burden (TMB), genomic loss of heterozygosity (gLOH), and programmed death‐ligand 1 (PD‐L1) positivity were determined. Results A total of 96 of 303 patients (31.7%) could be matched to an experimental CUPISCO arm. Key genomic alterations included ERBB2 (7.3%), PIK3CA (6.3%), NF1 (5.6%), NF2 (4.6%), BRAF (4.3%), IDH1 (3.3%), PTEN, FGFR2, EGFR (3.6% each), MET (4.3%), CDK6 (3.0%), FBXW7, CDK4 (2.3% each), IDH2, RET, ROS1, NTRK (1.0% each), and ALK (0.7%). Median TMB was 3.75 mutations per megabase of DNA; 34 patients (11.6%) had a TMB ≥16 mutations per megabase. Three patients (1%) had high MSI, and 42 (14%) displayed high PD‐L1 expression (tumor proportion score ≥50%). gLOH could be assessed in 199 of 303 specimens; 19.6% had a score of >16%. Conclusions Thirty‐two percent of patients would have been eligible for targeted therapy in CUPISCO. Future studies, including additional biomarkers such as PD‐L1 positivity and gLOH, may identify a greater proportion potentially benefiting from CGP‐informed treatment. Clinical trial identification number. NCT03498521 Implications for Practice The findings of this retrospective analysis of carcinoma of unknown primary origin (CUP) cases validate the experimental treatment arms being used in the CUPISCO study (NCT03498521), an ongoing randomized trial using comprehensive genomic profiling to assign patients with CUP to targeted or immunotherapy treatment arms based on the presence of pathogenic genomic alterations. The findings also suggest that future studies including additional biomarkers and treatment arms, such as programmed death‐ligand 1 positivity and genomic loss of heterozygosity, may identify a greater proportion of patients with CUP potentially benefiting from comprehensive genomic profiling‐informed treatment., This article focuses on the ability of comprehensive genomic profiling to identify potentially targetable genetic alterations in cancers of unknown primary, based on the inclusion criteria for the CUPISCO clinical trial and aiming for more effective therapeutic options for patients.

Published

2020

198. CYLD-mutant cylindroma-like basaloid carcinoma of the anus: a genetically and morphologically distinct class of HPV-related anal carcinoma

Author

Amanda Hemmerich, Mark C. Mochel, Shakti H. Ramkissoon, Jeffrey S. Ross, Radwa Sharaf, Brendan J. Gillespie, Julia A. Elvin, Brian M. Alexander, Ethan Sokol, Meagan Montesion, Erik A. Williams, Parth J. Patel, Kevin Jon Williams, Julie Y. Tse, James Corines, and Dean Pavlick

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Pathology, Anal Carcinoma, DNA Mutational Analysis, Mutation, Missense, Alphapapillomavirus, medicine.disease_cause, Article, Pathology and Forensic Medicine, 03 medical and health sciences, 0302 clinical medicine, Cylindroma, Cancer genomics, Biomarkers, Tumor, medicine, Humans, Missense mutation, Tumour virus infections, Genetic Predisposition to Disease, Hyaline, Aged, Retrospective Studies, Sequence Deletion, Aged, 80 and over, Mutation, business.industry, Papillomavirus Infections, Histology, Middle Aged, Anus Neoplasms, Cell Transformation, Viral, Anus, medicine.disease, Carcinoma, Adenoid Cystic, Deubiquitinating Enzyme CYLD, Phenotype, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Female, Histopathology, RNA Splice Sites, business

Abstract

Rare reports of anal carcinoma (AC) describe histologic resemblance to cutaneous cylindroma, but mutations in the tumor suppressor CYLD, the gene responsible for familial and sporadic cylindromas, have not been systematically investigated in AC. Here, we investigate CYLD-mutant AC, focusing on molecular correlates of distinct histopathology. Comprehensive genomic profiling (hybrid-capture-based DNA sequencing) was performed on 574 ACs, of which 75 unique cases (13%) harbored a CYLD mutation. Clinical data, pathology reports, and histopathology were reviewed for each CYLD-mutant case. The spectrum of CYLD mutations included truncating (n = 50; 67%), homozygous deletion (n = 10; 13%), missense (n = 16; 21%), and splice-site (n = 3; 4%) events. Compared with CYLD-wildtype AC (n = 499), CYLD-mutant ACs were significantly enriched for females (88% vs. 67%, p = 0.0001), slightly younger (median age 59 vs. 61 years, p = 0.047), and included near-universal detection of high-risk HPV sequences (97% vs. 88%, p = 0.014), predominantly HPV16 (96%). The CYLD-mutant cohort also showed significantly lower tumor mutational burden (TMB; median 2.6 vs. 5.2 mut/Mb, p

Published

2020

199. Real-World Comprehensive Genomic Profiling Success Rates in Tissue and Liquid Prostate Carcinoma Specimens

Author

Matthew C Hiemenz, Ryon P Graf, Kelsie Schiavone, Lukas Harries, Geoffrey R Oxnard, Jeffrey S Ross, and Richard S P Huang

Subjects

Cancer Research, Oncology

Abstract

Challenges with sequencing tissue samples from patients with prostate cancer have been reported in clinical trials. To assess the success rate of comprehensive genomic profiling (CGP) for prostate cancer patients, we analyzed a real-world cohort who underwent sequencing of their prostate tissue sample as well as a subset of patients with a reflex liquid biopsy. Overall, a significant majority (82%) of tissue prostate carcinoma samples yielded reportable CGP results. Of those samples that were unsuccessful, most (75%) were inadequate samples that did not meet pre-established criteria to advance into sequencing. For cases where liquid CGP was performed if tissue CGP was unsuccessful, mutations that were likely attributable to prostate carcinoma were observed in most cases and all cases were successful in generating a report. These results suggest that, for CGP testing, prostate cancer tissue is a reasonable matrix type and that liquid samples can be effectively used as an alternative to tissue.

Published

2022

200. Comprehensive Landscape of Cyclin Pathway Gene Alterations and Co-occurrence with FGF/FGFR Aberrations Across Urinary Tract Tumors

Author

Denis L F Jardim, Sherri Z Millis, Jeffrey S Ross, Scott Lippman, Siraj M Ali, and Razelle Kurzrock

Subjects

Cancer Research, Oncology

Abstract

Background Cyclin pathway gene alterations are frequent in urothelial tumors and may co-exist with other important aberrations, leading to therapeutic opportunities. We characterized the landscape of cyclin gene alterations in urothelial and non-urothelial urinary tract (UT) malignancies. Patients and Methods Overall, 6842 urothelial and 897 non-urothelial UT cancers were analyzed (hybrid-capture-based comprehensive genomic profile (Foundation Medicine)). Alteration frequency in cyclin-sensitizing and -resistance genes, and co-occurrence with fibroblast growth factor receptor (FGFR) gene abnormalities were evaluated. Results Cyclin-activating gene alterations were detected in 47.3% of urothelial and 37.9% of non-urothelial UT cancers. Frequency varied by histology and tumor site. CDKN2A and CDKN2B loss were the most frequent alterations in urothelial tumors (present in 38.5% and 30.4% of patients, respectively). Both genes were less frequently altered in adenocarcinomas (15.2% and 8.9%), but commonly altered in squamous cell carcinomas (74.4% and 39%). Tumors of neuroendocrine origin were relatively silent in activating cyclin alterations, but frequently displayed Rb1 alterations (86% and 83.7% of neuroendocrines and small cell carcinomas). Urachal tumors (n = 79) presented a distinct landscape of cyclin alterations relative to other UT cancers, with less frequent alterations overall. FGF/FGFR genes were altered in 34.9% of urothelial (22.1% in FGFR3), and 19.4% of non-urothelial urinary tract tumors (6.8% FGFR3). Cyclin-activating alterations frequently co-occurred with FGF/FGFR alterations but were in general mutually exclusively with cyclin resistance alterations (RB1/CCNE1). Conclusions Cyclin pathway activating alterations are common in urinary tract tumors, but frequency varies with histology and tumors sites. Co-occurrence of cyclin and FGFR pathway alterations may inform therapeutic opportunities.

Published

2022