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1. Clinical genomic profiling in the management of patients with soft tissue and bone sarcoma

Author

Gounder, Mrinal M, Agaram, Narasimhan P, Trabucco, Sally E, Robinson, Victoria, Ferraro, Richard A, Millis, Sherri Z, Krishnan, Anita, Lee, Jessica, Attia, Steven, Abida, Wassim, Drilon, Alexander, Chi, Ping, Angelo, Sandra P D’, Dickson, Mark A, Keohan, Mary Lou, Kelly, Ciara M, Agulnik, Mark, Chawla, Sant P, Choy, Edwin, Chugh, Rashmi, Meyer, Christian F, Myer, Parvathi A, Moore, Jessica L, Okimoto, Ross A, Pollock, Raphael E, Ravi, Vinod, Singh, Arun S, Somaiah, Neeta, Wagner, Andrew J, Healey, John H, Frampton, Garrett M, Venstrom, Jeffrey M, Ross, Jeffrey S, Ladanyi, Marc, Singer, Samuel, Brennan, Murray F, Schwartz, Gary K, Lazar, Alexander J, Thomas, David M, Maki, Robert G, Tap, William D, Ali, Siraj M, and Jin, Dexter X

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Clinical Sciences, Oncology and Carcinogenesis, Cancer, Biotechnology, Clinical Research, Human Genome, Genetic Testing, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Biomarkers, Tumor, Bone Neoplasms, Genomics, Humans, Mutation, Osteosarcoma, Prospective Studies, Sarcoma
Abstract

There are more than 70 distinct sarcomas, and this diversity complicates the development of precision-based therapeutics for these cancers. Prospective comprehensive genomic profiling could overcome this challenge by providing insight into sarcomas' molecular drivers. Through targeted panel sequencing of 7494 sarcomas representing 44 histologies, we identify highly recurrent and type-specific alterations that aid in diagnosis and treatment decisions. Sequencing could lead to refinement or reassignment of 10.5% of diagnoses. Nearly one-third of patients (31.7%) harbor potentially actionable alterations, including a significant proportion (2.6%) with kinase gene rearrangements; 3.9% have a tumor mutational burden ≥10 mut/Mb. We describe low frequencies of microsatellite instability (

Published
2022

2. Landscape of Cyclin Pathway Genomic Alterations Across 5,356 Prostate Cancers: Implications for Targeted Therapeutics.

Author

Jardim, Denis L, Millis, Sherri Z, Ross, Jeffrey S, Woo, Michelle Sue-Ann, Ali, Siraj M, and Kurzrock, Razelle

Subjects
Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

The cyclin pathway may confer resistance to standard treatments but also offer novel therapeutic opportunities in prostate cancer. Herein, we analyzed prostate cancer samples (majority metastatic) using comprehensive genomic profiling performed by next-generation sequencing (315 genes, >500× coverage) for alterations in activating and sensitizing cyclin genes (CDK4 amplification, CDK6 amplification, CCND1, CCND2, CCND3, CDKN2B [loss], CDKN2A [loss], SMARCB1), androgen receptor (AR) gene, and coalterations in genes leading to cyclin inhibitor therapeutic resistance (RB1 and CCNE1). Overall, cyclin sensitizing pathway genomic abnormalities were found in 9.7% of the 5,356 tumors. Frequent alterations included CCND1 amplification (4.2%) and CDKN2A and B loss (2.4% each). Alterations in possible resistance genes, RB1 and CCNE1, were detected in 9.7% (up to 54.6% in neuroendocrine) and 1.2% of cases, respectively, whereas AR alterations were seen in 20.9% of tumors (~27.3% in anaplastic). Cyclin sensitizing alterations were also more frequently associated with concomitant AR alterations.

Published
2021

4. Recurrent secondary genomic alterations in desmoplastic small round cell tumors

Author

Chow, Warren A, Yee, Jiing-Kuan, Tsark, Walter, Wu, Xiwei, Qin, Hanjun, Guan, Min, Ross, Jeffrey S, Ali, Siraj M, and Millis, Sherri Z

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Rare Diseases, Cancer, Pediatric, Pediatric Cancer, Biotechnology, Human Genome, Cancer Genomics, Orphan Drug, Clinical Research, 2.1 Biological and endogenous factors, Adolescent, Adult, Aged, Biomarkers, Tumor, Child, Chromosome Aberrations, DNA-Binding Proteins, Desmoplastic Small Round Cell Tumor, Female, Genome, Human, Humans, Male, Middle Aged, MutS Homolog 3 Protein, Neoplasm Recurrence, Local, Oncogene Proteins, Fusion, Prognosis, RNA-Binding Protein EWS, Receptor, Fibroblast Growth Factor, Type 4, Transcription Factors, Translocation, Genetic, Tumor Suppressor Protein p53, WT1 Proteins, Young Adult, Desmoplastic small round cell tumor, Sarcoma, Genomic profiling, FGFR4, Medical Biochemistry and Metabolomics, Genetics & Heredity, Medical biochemistry and metabolomics
Abstract

BackgroundDesmoplastic small round cell tumor (DSRCT) is a rare, highly aggressive, translocation-associated soft-tissue sarcoma that primarily affects children, adolescents, and young adults, with a striking male predominance. It is characterized by t(11;22) generating a novel EWSR1-WT1 fusion gene. Secondary genomic alterations are rarely described.MethodsTumor tissue from 83 DSRCT patients was assayed by hybrid-capture based comprehensive genomic profiling, FoundationOne® Heme next generation sequencing analysis of 406 genes and RNA sequencing of 265 genes. Tumor mutation burden was calculated from a minimum of 1.4 Mb sequenced DNA. Microsatellite instability status was determined by a novel algorithm analyzing 114 specific loci.ResultsComprehensive genomic profiling identified several genomically-defined DSRCT subgroups. Recurrent genomic alterations were most frequently detected in FGFR4, ARID1A, TP53, MSH3, and MLL3 genes. With the exception of FGFR4, where the genomic alterations predicted activation, most of the alterations in the remaining genes predicted gene inactivation. No DSRCT were TMB or MSI high.ConclusionsIn summary, recurrent secondary somatic alterations in FGFR4, ARID1A, TP53, MSH3, and MLL3 were detected in 82% of DSRCT, which is significantly greater than previously reported. These alterations may have both prognostic and therapeutic implications.

Published
2020

5. The Pan‐Cancer Landscape of Coamplification of the Tyrosine Kinases KIT, KDR, and PDGFRA

Author

Disel, Umut, Madison, Russell, Abhishek, Kumar, Chung, Jon H, Trabucco, Sally E, Matos, Asli O, Frampton, Garrett M, Albacker, Lee A, Reddy, Venkataprasanth, Karadurmus, Nuri, Benson, Adam, Webster, Jennifer, Paydas, Semra, Cabanillas, Ruben, Nangia, Chaitali, Ozturk, MA, Millis, Sherri Z, Pal, Sumanta K, Wilky, Breelyn, Sokol, Ethan S, Gay, Laurie M, Soman, Salil, Ganesan, Shridar, Janeway, Katherine, Stephens, Phil J, Zhu, Viola W, Ou, Sai‐Hong Ignatius, Lovly, Christine M, Gounder, Mrinal, Schrock, Alexa B, Ross, Jeffrey S, Miller, Vincent A, Klempner, Samuel J, and Ali, Siraj M

Subjects
Cancer, Rare Diseases, Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Gene Amplification, Humans, Middle Aged, Neoplasms, Receptor Protein-Tyrosine Kinases, Receptor, Platelet-Derived Growth Factor alpha, Vascular Endothelial Growth Factor Receptor-2, Young Adult, amplification, tyrosine kinase inhibitor, KIT, PDGFRA, genomic profiling, sarcoma, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeAmplifications of receptor tyrosine kinases (RTKS) are therapeutic targets in multiple tumor types (e.g. HER2 in breast cancer), and amplification of the chromosome 4 segment harboring the three RTKs KIT, PDGFRA, and KDR (4q12amp) may be similarly targetable. The presence of 4q12amp has been sporadically reported in small tumor specific series but a large-scale analysis is lacking. We assess the pan-cancer landscape of 4q12amp and provide early clinical support for the feasibility of targeting this amplicon.Experimental designTumor specimens from 132,872 patients with advanced cancer were assayed with hybrid capture based comprehensive genomic profiling which assays 186-315 genes for all classes of genomic alterations, including amplifications. Baseline demographic data were abstracted, and presence of 4q12amp was defined as 6 or more copies of KIT/KDR/PDGFRA. Concurrent alterations and treatment outcomes with matched therapies were explored in a subset of cases.ResultsOverall 0.65% of cases harbored 4q12amp at a median copy number of 10 (range 6-344). Among cancers with >100 cases in this series, glioblastomas, angiosarcomas, and osteosarcomas were enriched for 4q12amp at 4.7%, 4.8%, and 6.4%, respectively (all p < 0.001), giving an overall sarcoma (n = 6,885) incidence of 1.9%. Among 99 pulmonary adenocarcinoma cases harboring 4q12amp, 50 (50%) lacked any other known driver of NSLCC. Four index cases plus a previously reported case on treatment with empirical TKIs monotherapy had stable disease on average exceeding 20 months.ConclusionWe define 4q12amp as a significant event across the pan-cancer landscape, comparable to known pan-cancer targets such as NTRK and microsatellite instability, with notable enrichment in several cancers such as osteosarcoma where standard treatment is limited. The responses to available TKIs observed in index cases strongly suggest 4q12amp is a druggable oncogenic target across cancers that warrants a focused drug development strategy.Implications for practiceCoamplification of the receptor tyrosine kinases (rtks) KIT/KDR/PDGFRA (4q12amp) is present broadly across cancers (0.65%), with enrichment in osteosarcoma and gliomas. Evidence for this amplicon having an oncogenic role is the mutual exclusivity of 4q12amp to other known drivers in 50% of pulmonary adenocarcinoma cases. Furthermore, preliminary clinical evidence for driver status comes from four index cases of patients empirically treated with commercially available tyrosine kinase inhibitors with activity against KIT/KDR/PDGFRA who had stable disease for 20 months on average. The sum of these lines of evidence suggests further clinical and preclinical investigation of 4q12amp is warranted as the possible basis for a pan-cancer drug development strategy.

Published
2020

6. Prevalence of established and emerging biomarkers of immune checkpoint inhibitor response in advanced hepatocellular carcinoma.

Author

Ang, Celina, Klempner, Samuel J, Ali, Siraj M, Madison, Russell, Ross, Jeffrey S, Severson, Eric A, Fabrizio, David, Goodman, Aaron, Kurzrock, Razelle, Suh, James, and Millis, Sherri Z

Subjects
biomarkers, hepatocellular carcinoma, immunotherapy, tumor mutation burden, Oncology and Carcinogenesis
Abstract

The clinical deployment of immune checkpoint inhibitors (ICIs) has created a tandem drive for the identification of biomarkers linked to benefit. Comprehensive genomic profiling was performed to evaluate the frequency of genomic biomarkers of ICI response in 755 patients with advanced hepatocellular carcinoma (HCC). Median age was 62 years' old, 73% were male, 46% had extrahepatic disease, 107 had documented hepatitis C, 96 had hepatitis B and 4 patients were coinfected. Median tumor mutation burden (TMB) was 4 mutations/Mb and only 6 tumors (0.8%) were TMB-high. Out of 542 cases assessed for microsatellite instability (MSI), one (0.2%) was MSI-high and TMB-high. Twenty-seven (4%) patients had POLE/D alterations. One patient had a pathogenic POLE R762W mutation but TMB was 4 mutations/Mb. Forty percent had DNA damage response gene alterations. In a small case series (N=17) exploring the relationship between biomarkers and ICI response, one patient (TMB 15 mutations/Mb, MSI-low) had a sustained complete response to nivolumab lasting > 2 years. Otherwise there were no significant genomic or TMB differences between responders, progressors, and those with stable disease. Overall, markers of genomic instability were infrequent in this cohort. Larger clinically annotated datasets are needed to explore genomic and non-genomic determinants of ICI response in HCC.

Published
2019

7. Phosphatidylinositol 3‐kinase pathway genomic alterations in 60,991 diverse solid tumors informs targeted therapy opportunities

Author

Millis, Sherri Z, Jardim, Denis L, Albacker, Lee, Ross, Jeffrey S, Miller, Vincent A, Ali, Siraj M, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Cancer Genomics, Cancer, Urologic Diseases, Digestive Diseases, Genetics, Biotechnology, Women's Health, Human Genome, Colo-Rectal Cancer, Rare Diseases, 2.1 Biological and endogenous factors, AMP-Activated Protein Kinase Kinases, Class I Phosphatidylinositol 3-Kinases, Estrogen Receptor alpha, F-Box-WD Repeat-Containing Protein 7, Female, Genes, erbB, Humans, Male, Mitogen-Activated Protein Kinase Kinases, Molecular Targeted Therapy, Neoplasms, Odds Ratio, PTEN Phosphohydrolase, Phosphatidylinositol 3-Kinases, Protein Serine-Threonine Kinases, Proto-Oncogene Mas, Proto-Oncogene Proteins c-met, Receptors, Androgen, Signal Transduction, Tumor Suppressor Protein p53, ras Proteins, cancer genome, molecular profile, phosphoinositide 3-kinase catalytic subunit alpha, precision oncology, targeted therapy, phosphoinositide 3-kinase catalytic subunit α, Public Health and Health Services, Oncology & Carcinogenesis, Oncology and carcinogenesis, Public health
Abstract

BackgroundThe phosphatidylinositol 3-kinase (PI3K) pathway is frequently altered in cancer. This report describes the landscape of PI3K alterations in solid tumors as well as co-alterations serving as potential resistance/attenuation mechanisms.MethodsConsecutive samples were analyzed in a commercial Clinical Laboratory Improvement Amendment-certified laboratory using comprehensive genomic profiling performed by next-generation sequencing (315 genes). The co-alterations evaluated included the Erb-B2 receptor tyrosine kinase 2 (ERBB2), ERBB3, ERBB4, RAS, MET proto-oncogene tyrosine kinase (MET), and mitogen-activated protein kinase kinase (MAP2K) genes as well as tumor protein 53 (TP53), estrogen receptor 1 (ESR1), and androgen receptor (AR).ResultsAlterations in any of 18 PI3K-pathway associated genes were identified in 44% of 60,991 tumors. Although single base and insertions/deletions (indels) were the most frequent alterations, copy number changes and rearrangements were identified in 11% and 0.9% of patients, respectively. Overall, the most frequently altered genes were PIK3 catalytic subunit α (PIK3CA) (13%), phosphatase and tensin homolog (PTEN) (9%), and serine/threonine kinase 11 (STK11) (5%). Tumor types that frequently harbored at least 1 PI3K alteration were uterine (77%), cervical (62%), anal (59%), and breast (58%) cancers. Alterations also were discerned frequently in tumors with carcinosarcoma (89%) and squamous cell carcinoma (62%) histologies. Tumors with a greater likelihood of co-occurring PI3K pathway and MAPK pathway alterations included colorectal cancers (odds ratio [OR], 1.64; P

Published
2019

8. BRAF in Lung Cancers: Analysis of Patient Cases Reveals Recurrent BRAF Mutations, Fusions, Kinase Duplications, and Concurrent Alterations.

Author

Sheikine, Yuri, Pavlick, Dean, Klempner, Samuel J, Trabucco, Sally E, Chung, Jon H, Rosenzweig, Mark, Wang, Kai, Velcheti, Vamsidhar, Frampton, Garrett M, Peled, Nir, Murray, Molly, Chae, Young Kwang, Albacker, Lee A, Gay, Laurie, Husain, Hatim, Suh, James H, Millis, Sherri Z, Reddy, Venkataprasanth P, Elvin, Julia A, Hartmaier, Ryan J, Dowlati, Afshin, Stephens, Phil, Ross, Jeffrey S, Bivona, Trever G, Miller, Vincent A, Ganesan, Shridar, Schrock, Alexa B, Ou, Sai-Hong Ignatius, and Ali, Siraj M

Subjects
Cancer, Lung Cancer, Genetics, Human Genome, Lung, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Good Health and Well Being
Abstract

Dabrafenib and trametinib are approved for the management of advanced non-small-cell lung cancers (NSCLCs) that harbor BRAF V600E mutations. Small series and pan-cancer analyses have identified non-V600 alterations as therapeutic targets. We sought to examine a large genomic data set to comprehensively characterize non-V600 BRAF alterations in lung cancer. A total of 23,396 patients with lung cancer provided data to assay with comprehensive genomic profiling. Data were reviewed for predicted pathogenic BRAF base substitutions, short insertions and deletions, copy number changes, and rearrangements. Adenocarcinomas represented 65% of the occurrences; NSCLC not otherwise specified (NOS), 15%; squamous cell carcinoma, 12%; and small-cell lung carcinoma, 5%. BRAF was altered in 4.5% (1,048 of 23,396) of all tumors; 37.4% (n = 397) were BRAF V600E, 38% were BRAF non-V600E activating mutations, and 18% were BRAF inactivating. Rearrangements were observed at a frequency of 4.3% and consisted of N-terminal deletions (NTDs; 0.75%), kinase domain duplications (KDDs; 0.75%), and BRAF fusions (2.8%). The fusions involved three recurrent fusion partners: ARMC10, DOCK4, and TRIM24. BRAF V600E was associated with co-occurrence of SETD2 alterations, but other BRAF alterations were not and were instead associated with CDKN2A, TP53, and STK11 alterations (P < .05). Potential mechanisms of acquired resistance to BRAF V600E inhibition are demonstrated. This series characterized the frequent occurrence (4.4%) of BRAF alterations in lung cancers. Recurrent BRAF alterations in NSCLC adenocarcinoma are comparable to the frequency of other NSCLC oncogenic drivers, such as ALK, and exceed that of ROS1 or RET. This work supports a broad profiling approach in lung cancers and suggests that non-V600E BRAF alterations represent a subgroup of lung cancers in which targeted therapy should be considered.

Published
2018

10. Prevalence of Homologous Recombination Pathway Gene Mutations in Melanoma: Rationale for a New Targeted Therapeutic Approach

Author

Kim, Kevin B., Soroceanu, Liliana, de Semir, David, Millis, Sherri Z., Ross, Jeffrey, Vosoughi, Elham, Dar, Altaf A., Nosrati, Mehdi, Desprez, Pierre-Yves, Ice, Ryan, Chen, Michelle, Chetal, Kashish, Bhattacharjee, Anukana, Moretto, John, Leong, Stanley P., Singer, Mark I., Parrett, Brian M., Minor, David R., McAllister, Sean, Miller, James R., III, Salomonis, Nathan, and Kashani-Sabet, Mohammed

Published
2021
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11. Next-generation sequencing in the clinical setting clarifies patient characteristics and potential actionability

Author

Bieg-Bourne, Cheyennedra C, Millis, Sherri Z, Piccioni, David E, Fanta, Paul T, Goldberg, Michael E, Chmielecki, Juliann, Parker, Barbara A, and Kurzrock, Razelle

Subjects
Clinical Research, Cancer, Biotechnology, Genetics, Good Health and Well Being, Biomarkers, Tumor, DNA Mutational Analysis, Genetic Predisposition to Disease, High-Throughput Nucleotide Sequencing, Humans, Mutation, Neoplasms, Precision Medicine, Reproducibility of Results, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Enhancements in clinical-grade next-generation sequencing (NGS) have fueled the advancement of precision medicine in the clinical oncology field. Here, we survey the molecular profiles of 1,113 patients with diverse malignancies who successfully underwent clinical-grade NGS (236-404 genes) in an academic tertiary cancer center. Among the individual tumors examined, the majority showed at least one detectable alteration (97.2%). Among 2,045 molecular aberrations was the involvement of 302 distinct genes. The most commonly altered genes were TP53 (47.0%), CDKN2A (18.0%), TERT (17.0%), and KRAS (16.0%), and the majority of patients had tumors that harbored multiple alterations. Tumors displayed a median of four alterations (range, 0-29). Most individuals had at least one potentially actionable alteration (94.7%), with the median number of potentially actionable alterations per patient being 2 (range, 0-13). A total of 1,048 (94.2%) patients exhibited a unique molecular profile, with either genes altered or loci within the gene(s) altered being distinct. Approximately 13% of patients displayed a genomic profile identical to at least one other patient; although genes altered were the same, the affected loci may have differed. Overall, our results underscore the complex heterogeneity of malignancies and argue that customized combination therapies will be essential to optimize cancer treatment regimens. Cancer Res; 77(22); 6313-20. ©2017 AACR.

Published
2017

12. HER2 expression status in diverse cancers: review of results from 37,992 patients

Author

Yan, Min, Schwaederle, Maria, Arguello, David, Millis, Sherri Z, Gatalica, Zoran, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Biotechnology, Breast Cancer, Gene Expression Regulation, Neoplastic, Humans, Immunohistochemistry, In Situ Hybridization, In Situ Hybridization, Fluorescence, Neoplasms, Receptor, ErbB-2, HER2 overexpression, IHC, FISH, HER2 amplification, Receptor, erbB-2, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

Human epidermal growth factor receptor 2 (HER2) amplification/overexpression is an effective therapeutic target in breast and gastric cancer. Although HER2 positivity has been reported in other malignancies, previous studies generally focused on one cancer type, making it challenging to compare HER2 positivity across studies/malignancies. Herein, we examined 37,992 patient samples for HER2 expression (+/- amplification) in a single laboratory. All 37,992 patients were tested by immunohistochemistry (IHC); 21,642 of them were also examined for HER2 amplification with either fluorescent in situ hybridization (FISH) (11,670 patients) or chromogenic in situ hybridization (CISH) (9,972 patients); 18,262 patients had tumors other than breast or gastric cancer. All tissues were analyzed in a Clinical Laboratory Improvement Amendments (CLIA) laboratory (Caris Life Sciences) at the request of referring physicians. HER2 protein overexpression was found in 2.7 % of samples. Over-expressed HER2 was detected predominantly in malignancies of epithelial origin; for cancers derived from mesenchyme, neuroendocrine tissue, central nervous system, and kidney, HER2 expression and amplification were remarkably rare or non-existent. Bladder carcinomas, gallbladder, extrahepatic cholangiocarcinomas, cervical, uterine, and testicular cancers showed HER2 positivity rates of 12.4, 9.8, 6.3, 3.9, 3.0, and 2.4 %, respectively. HER2 overexpression and/or amplification is frequently found across tumor types. These observations may have significant therapeutic implications in cancers not traditionally thought to benefit from anti-HER2 therapies.

Published
2015

19. POU2AF3 ‐rearranged Sarcomas: A Novel Tumor Defined by Fusions of EWSR1 or FUS to a Gene Formerly Designated COLCA2

Author

Hiemenz, Matthew C., primary, Kaur, Jaspreet, additional, Kuang, Zheng, additional, Huang, Richard S. P., additional, Harries, Lukas, additional, Metzger, Dana, additional, Schiavone, Kelsie, additional, Millis, Sherri Z., additional, Lin, Douglas I., additional, Lechpammer, Mirna, additional, Decker, Brennan, additional, Mata, Douglas A., additional, Reddy, Abhinav, additional, Parke, Matthew, additional, Lee, Eun Y., additional, Cui, Xiaoyan, additional, Iwenofu, O. Hans, additional, Buehler, Darya, additional, Henderson, Les, additional, Baldwin, Erin, additional, Boikos, Sosipatros A., additional, Ramkissoon, Shakti H., additional, and Smith, Steven C., additional

Published
2023
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26. Comprehensive Landscape of Cyclin Pathway Gene Alterations and Co-occurrence with FGF/FGFR Aberrations Across Urinary Tract Tumors.

Author

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

Subjects
CANCER chemotherapy, THERAPEUTIC use of antineoplastic agents, FIBROBLAST growth factors, GENETIC mutation, CELL cycle proteins, INDIVIDUALIZED medicine, CELLULAR signal transduction, URINARY organs, TREATMENT effectiveness, CELL cycle, MOLECULAR biology, CHROMOSOME abnormalities, COMORBIDITY, GENETIC profile
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. Cyclin gene alterations are common in urinary tract tumors and often co-occur with FGF/FGFR aberrations. This article analyzes molecular alterations affecting the cyclin signals and potential co-drivers in key pathways. Rare subtypes of urinary tract cancers are included to identify unique alteration patterns and potential therapeutic opportunities. [ABSTRACT FROM AUTHOR]

Published
2023
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34. Genomic Characterization of Testicular Germ Cell Tumors Relapsing After Chemotherapy

Author

Necchi, Andrea, primary, Bratslavsky, Gennady, additional, Corona, Robert J., additional, Chung, Jon H., additional, Millis, Sherri Z., additional, Elvin, Julia A., additional, Vergilio, Jo-Anne, additional, Suh, James, additional, Ramkissoon, Shakti, additional, Severson, Eric, additional, Daniel, Sugganth, additional, Killian, Jonathan K., additional, Ali, Siraj M., additional, Schrock, Alexa B., additional, Reddy, Prasanth, additional, Miller, Vincent A., additional, Welsh, Allison, additional, Gay, Laurie M., additional, and Ross, Jeffrey S., additional

Published
2020
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39. Prospective Comprehensive Genomic Profiling of Primary and Metastatic Prostate Tumors

Author

Chung, Jon H., primary, Dewal, Ninad, additional, Sokol, Ethan, additional, Mathew, Paul, additional, Whitehead, Robert, additional, Millis, Sherri Z., additional, Frampton, Garrett M., additional, Bratslavsky, Gennady, additional, Pal, Sumanta K., additional, Lee, Richard J., additional, Necchi, Andrea, additional, Gregg, Jeffrey P., additional, Lara, Primo, additional, Antonarakis, Emmanuel S., additional, Miller, Vincent A., additional, Ross, Jeffrey S., additional, Ali, Siraj M., additional, and Agarwal, Neeraj, additional

Published
2019
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40. The Pan-Cancer Landscape of Coamplification of the Tyrosine Kinases KIT, KDR, and PDGFRA

Author

Disel, Umut, primary, Madison, Russell, additional, Abhishek, Kumar, additional, Chung, Jon H., additional, Trabucco, Sally E., additional, Matos, Asli O., additional, Frampton, Garrett M., additional, Albacker, Lee A., additional, Reddy, Venkataprasanth, additional, Karadurmus, Nuri, additional, Benson, Adam, additional, Webster, Jennifer, additional, Paydas, Semra, additional, Cabanillas, Ruben, additional, Nangia, Chaitali, additional, Ozturk, M.A., additional, Millis, Sherri Z., additional, Pal, Sumanta K., additional, Wilky, Breelyn, additional, Sokol, Ethan S., additional, Gay, Laurie M., additional, Soman, Salil, additional, Ganesan, Shridar, additional, Janeway, Katherine, additional, Stephens, Phil J., additional, Zhu, Viola W., additional, Ou, Sai-Hong Ignatius, additional, Lovly, Christine M., additional, Gounder, Mrinal, additional, Schrock, Alexa B., additional, Ross, Jeffrey S., additional, Miller, Vincent A., additional, Klempner, Samuel J., additional, and Ali, Siraj M., additional

Published
2019
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43. Ductal (PDC), acinar (PAC) and neuroendocrine (PNC) carcinomas of the prostate: A comparative comprehensive genomic profiling (CGP) study.

Author

Bratslavsky, Gennady, primary, Jacob, Joseph, additional, Shapiro, Oleg, additional, Liu, Nick, additional, Ferry, Elizabeth Kate, additional, Elvin, Julia Andrea, additional, Vergilio, Jo-Anne, additional, Killian, Jonathan Keith, additional, Ngo, Nhu, additional, Ramkissoon, Shakti, additional, Severson, Eric Allan, additional, Hemmerich, Amanda, additional, Ali, Siraj Mahamed, additional, Chung, Jon, additional, Schrock, Alexa Betzig, additional, Reddy, Prasanth, additional, Millis, Sherri Z., additional, Alexander, Brian, additional, Necchi, Andrea, additional, and Ross, Jeffrey S., additional

Published
2019
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46. Degree of MDM2 Amplification Affects Clinical Outcomes in Dedifferentiated Liposarcoma

Author

Bill, Kate Lynn J., primary, Seligson, Nathan D., additional, Hays, John L., additional, Awasthi, Achal, additional, Demoret, Bryce, additional, Stets, Colin W., additional, Duggan, Megan C., additional, Bupathi, Manojkumar, additional, Brock, Guy N., additional, Millis, Sherri Z., additional, Shakya, Reena, additional, Timmers, Cynthia D., additional, Wakely, Paul E., additional, Pollock, Raphael E., additional, and Chen, James L., additional

Published
2019
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47. Ductal and acinar carcinomas of the prostate: A comparative comprehensive genomic profiling study.

Author

Liu, Nick, primary, Kotula, Leszek, additional, Byler, Timothy, additional, Jacob, Joseph, additional, Alexander, Brian Michael, additional, Gay, Laurie M., additional, Shapiro, Oleg, additional, Millis, Sherri Z., additional, Elvin, Julia Andrea, additional, Chung, Jon, additional, Vergilio, Jo-Anne, additional, Ramkissoon, Shakti, additional, Severson, Eric Allan, additional, Killian, Jonathan Keith, additional, Ali, Siraj Mahamed, additional, Schrock, Alexa Betzig, additional, Miller, Vincent A., additional, Necchi, Andrea, additional, de La Roza, Gustavo, additional, and Ross, Jeffrey S., additional

Published
2019
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48. Genomic findings in adenocarcinoma of the urinary bladder.

Author

Shapiro, Oleg, primary, Kotula, Leszek, additional, Byler, Timothy, additional, Jacob, Joseph, additional, Alexander, Brian Michael, additional, Gay, Laurie M., additional, Millis, Sherri Z., additional, Elvin, Julia Andrea, additional, Chung, Jon, additional, Vergilio, Jo-Anne, additional, Ramkissoon, Shakti, additional, Severson, Eric Allan, additional, Killian, Jonathan Keith, additional, Ali, Siraj Mahamed, additional, Schrock, Alexa Betzig, additional, Miller, Vincent A., additional, de La Roza, Gustavo, additional, Ross, Jeffrey S., additional, Bratslavsky, Gennady, additional, and Liu, Nick, additional

Published
2019
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49. Cyclin Pathway Genomic Alterations Across 190,247 Solid Tumors: Leveraging Large‐Scale Data to Inform Therapeutic Directions.

Author

Jardim, Denis L., Millis, Sherri Z., Ross, Jeffrey S., Woo, Michelle Sue‐Ann, Ali, Siraj M., and Kurzrock, Razelle

Subjects
TUMOR treatment, GENOMICS
Abstract

Background: We describe the landscape of cyclin and interactive gene pathway alterations in 190,247 solid tumors. Methods: Using comprehensive genomic profiling (315 genes, >500× coverage), samples were analyzed for alterations in activating/sensitizing cyclin genes (CDK4 amplification, CDK6 amplification, CCND1, CCND2, CCND3, CDKN2B [loss], CDKN2A [loss], SMARCB1), hormone genes (estrogen receptor 1 [ESR1], androgen receptor [AR]), and co‐alterations in genes leading to cyclin inhibitor therapeutic resistance (RB1 and CCNE1). Results: Alterations in at least one cyclin activating/sensitizing gene occurred in 24% of malignancies. Tumors that frequently harbored at least one cyclin alteration were brain gliomas (47.1%), esophageal (40.3%) and bladder cancer (37.9%), and mesotheliomas (37.9%). The most frequent alterations included CDKN2A (13.9%) and CDKN2B loss (12.5%). Examples of unique patterns of alterations included CCND1 amplification in breast cancer (17.3%); CDK4 alterations in sarcomas (12%); CCND2 in testicular cancer (23.4%), and SMARCB1 mutations in kidney cancer (3% overall, 90% in malignant rhabdoid tumors). Alterations in resistance genes RB1 and CCNE1 affected 7.2% and 3.6% of samples. Co‐occurrence analysis demonstrated a lower likelihood of concomitant versus isolated alterations in cyclin activating/sensitizing and resistance genes (odds ratio [OR], 0.35; p <.001), except in colorectal, cervical, and small intestine cancers. AR and cyclin activating/sensitizing alterations in prostate cancer co‐occurred more frequently (vs. AR alterations and wild‐type cyclin activating/sensitizing alterations) (OR, 1.79; p <.001) as did ESR1 and cyclin activating/sensitizing alterations in breast (OR, 1.62; p <.001) and cervical cancer (OR, 4.08; p =.04) (vs. ESR1 and cyclin wild‐type activating/sensitizing alterations). Conclusion: Cyclin pathway alterations vary according to tumor type/histology, informing opportunities for targeted therapy, including for rare cancers. Implications for Practice: Cyclin pathway genomic abnormalities are frequent in human solid tumors, with substantial variation according to tumor site and histology. Opportunities for targeted therapy emerge with comprehensive profiling of this pathway. This article identifies molecular alterations in genes involved in the cyclin activation/sensitizing pathways and reports coexisting resistance and hormone pathway alterations in 190,247 diverse solid tumors that underwent next‐generation sequencing. [ABSTRACT FROM AUTHOR]

Published
2021
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50. Genomic analysis reveals low tumor mutation burden which may be associated with GNAQ/11 alteration in a series of primary leptomeningeal melanomas.

Author

Fortin Ensign, Shannon, Bollin, Kathryn, Millis, Sherri Z., Hinds, Brian R., Kosty, Michael, and Uchiyama, Christopher

Subjects
BRAF genes, MELANOMA, CENTRAL nervous system, CYCLIN-dependent kinase inhibitor-2A, TUMORS
Abstract

Primary central nervous system melanoma is rare and characterized by a variable prognosis, and no current treatment guidelines exist. We describe the clinical course of a 70‐year‐old female patient diagnosed with primary leptomeningeal melanoma (LMN) whose case represents the diagnostic and management challenges of this tumor. Targeted genomic sequencing of 315 genes from this tumor revealed GNAQ Q209L mutation and low (4 mutations/Megabase) tumor mutation burden (TMB). Wild‐type NRAS, KIT, and BRAF were also observed. A cohort of 4,787 melanomas was subsequently analyzed to identify additional primary central nervous system melanomas, of which 10 additional tumors met pathologic criteria (0.21% of total melanoma cohort). These tumors were genomically assessed according to the same targeted sequencing panel, and 6 of the tumors were also found to harbor a GNAQ mutation. All 10 tumors had low (less than or equal to 2 mutations/Megabase) TMB indicating a potential trend between G‐protein‐coupled receptor (GPCR) alterations and low TMB in LMNs. GPCR alterations were found to significantly correlate with TMB across the cohort of 4,787 melanomas, supporting this potential finding in the limited LMN subset. [ABSTRACT FROM AUTHOR]

Published
2020
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