Your search keyword '"Siraj M, Ali"' showing total 630 results

1. Augmented interpretation of HER2, ER, and PR in breast cancer by artificial intelligence analyzer: enhancing interobserver agreement through a reader study of 201 cases

Author

Minsun Jung, Seung Geun Song, Soo Ick Cho, Sangwon Shin, Taebum Lee, Wonkyung Jung, Hajin Lee, Jiyoung Park, Sanghoon Song, Gahee Park, Heon Song, Seonwook Park, Jinhee Lee, Mingu Kang, Jongchan Park, Sergio Pereira, Donggeun Yoo, Keunhyung Chung, Siraj M. Ali, and So-Woon Kim

Subjects

Artificial intelligence (AI), Breast cancer, Concordance, Digital pathology, Estrogen receptor (ER), Human epidermal growth factor receptor 2 (HER2), Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Accurate classification of breast cancer molecular subtypes is crucial in determining treatment strategies and predicting clinical outcomes. This classification largely depends on the assessment of human epidermal growth factor receptor 2 (HER2), estrogen receptor (ER), and progesterone receptor (PR) status. However, variability in interpretation among pathologists pose challenges to the accuracy of this classification. This study evaluates the role of artificial intelligence (AI) in enhancing the consistency of these evaluations. Methods AI-powered HER2 and ER/PR analyzers, consisting of cell and tissue models, were developed using 1,259 HER2, 744 ER, and 466 PR-stained immunohistochemistry (IHC) whole-slide images of breast cancer. External validation cohort comprising HER2, ER, and PR IHCs of 201 breast cancer cases were analyzed with these AI-powered analyzers. Three board-certified pathologists independently assessed these cases without AI annotation. Then, cases with differing interpretations between pathologists and the AI analyzer were revisited with AI assistance, focusing on evaluating the influence of AI assistance on the concordance among pathologists during the revised evaluation compared to the initial assessment. Results Reevaluation was required in 61 (30.3%), 42 (20.9%), and 80 (39.8%) of HER2, in 15 (7.5%), 17 (8.5%), and 11 (5.5%) of ER, and in 26 (12.9%), 24 (11.9%), and 28 (13.9%) of PR evaluations by the pathologists, respectively. Compared to initial interpretations, the assistance of AI led to a notable increase in the agreement among three pathologists on the status of HER2 (from 49.3 to 74.1%, p

Published

2024

2. Generalizing AI-driven Assessment of Immunohistochemistry across Immunostains and Cancer Types: A Universal Immunohistochemistry Analyzer.

Author

Biagio Brattoli, Mohammad Mostafavi, Taebum Lee, Wonkyung Jung, Jeongun Ryu, Seonwook Park, Jongchan Park, Sérgio Pereira, Seunghwan Shin, Sangjoon Choi, Hyojin Kim, Donggeun Yoo, Siraj M. Ali, Kyunghyun Paeng, Chan-Young Ock, Soo Ick Cho, and Seokhwi Kim

Published

2024

3. Inflamed immune phenotype predicts favorable clinical outcomes of immune checkpoint inhibitor therapy across multiple cancer types

Author

Jeanne Shen, Sergio Pereira, Chan-Young Ock, Yung-Jue Bang, Seulki Kim, Sehhoon Park, Se-Hoon Lee, George A Fisher, Young Kwang Chae, Yoon-La Choi, Jin-Haeng Chung, Tony S K Mok, Leeseul Kim, Jun-Eul Hwang, Gahee Park, Sanghoon Song, Seunghwan Shin, Yoojoo Lim, Wonkyung Jung, Heon Song, Hyojin Kim, Taebum Lee, Sukjun Kim, Chang Ho Ahn, Seokhwi Kim, Ben W Dulken, Stephanie Bogdan, Maggie Huang, Chiyoon Oum, and Siraj M. Ali

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background The inflamed immune phenotype (IIP), defined by enrichment of tumor-infiltrating lymphocytes (TILs) within intratumoral areas, is a promising tumor-agnostic biomarker of response to immune checkpoint inhibitor (ICI) therapy. However, it is challenging to define the IIP in an objective and reproducible manner during manual histopathologic examination. Here, we investigate artificial intelligence (AI)-based immune phenotypes capable of predicting ICI clinical outcomes in multiple solid tumor types.Methods Lunit SCOPE IO is a deep learning model which determines the immune phenotype of the tumor microenvironment based on TIL analysis. We evaluated the correlation between the IIP and ICI treatment outcomes in terms of objective response rates (ORR), progression-free survival (PFS), and overall survival (OS) in a cohort of 1,806 ICI-treated patients representing over 27 solid tumor types retrospectively collected from multiple institutions.Results We observed an overall IIP prevalence of 35.2% and significantly more favorable ORRs (26.3% vs 15.8%), PFS (median 5.3 vs 3.1 months, HR 0.68, 95% CI 0.61 to 0.76), and OS (median 25.3 vs 13.6 months, HR 0.66, 95% CI 0.57 to 0.75) after ICI therapy in IIP compared with non-IIP patients, respectively (p

Published

2024

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

Author

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

Subjects

Science

Abstract

Comprehensive molecular profiles are required to understand and treat sarcomas, which comprise more than 70 different subtypes. Here, the authors profile the genomic landscape of 7494 sarcomas across 44 histologies using targeted panel sequencing and identify potential therapeutic targets.

Published

2022

5. Deficiency of the splicing factor RBM10 limits EGFR inhibitor response in EGFR-mutant lung cancer

Author

Shigeki Nanjo, Wei Wu, Niki Karachaliou, Collin M. Blakely, Junji Suzuki, Yu-Ting Chou, Siraj M. Ali, D. Lucas Kerr, Victor R. Olivas, Jonathan Shue, Julia Rotow, Manasi K. Mayekar, Franziska Haderk, Nilanjana Chatterjee, Anatoly Urisman, Jia Chi Yeo, Anders J. Skanderup, Aaron C. Tan, Wai Leong Tam, Oscar Arrieta, Kazuyoshi Hosomichi, Akihiro Nishiyama, Seiji Yano, Yuriy Kirichok, Daniel S.W. Tan, Rafael Rosell, Ross A Okimoto, and Trever G. Bivona

Subjects

Oncology, Therapeutics, Medicine

Abstract

Molecularly targeted cancer therapy has improved outcomes for patients with cancer with targetable oncoproteins, such as mutant EGFR in lung cancer. Yet, the long-term survival of these patients remains limited, because treatment responses are typically incomplete. One potential explanation for the lack of complete and durable responses is that oncogene-driven cancers with activating mutations of EGFR often harbor additional co-occurring genetic alterations. This hypothesis remains untested for most genetic alterations that co-occur with mutant EGFR. Here, we report the functional impact of inactivating genetic alterations of the mRNA splicing factor RNA-binding motif 10 (RBM10) that co-occur with mutant EGFR. RBM10 deficiency decreased EGFR inhibitor efficacy in patient-derived EGFR-mutant tumor models. RBM10 modulated mRNA alternative splicing of the mitochondrial apoptotic regulator Bcl-x to regulate tumor cell apoptosis during treatment. Genetic inactivation of RBM10 diminished EGFR inhibitor–mediated apoptosis by decreasing the ratio of (proapoptotic) Bcl-xS to (antiapoptotic) Bcl-xL isoforms of Bcl-x. RBM10 deficiency was a biomarker of poor response to EGFR inhibitor treatment in clinical samples. Coinhibition of Bcl-xL and mutant EGFR overcame the resistance induced by RBM10 deficiency. This study sheds light on the role of co-occurring genetic alterations and on the effect of splicing factor deficiency on the modulation of sensitivity to targeted kinase inhibitor cancer therapy.

Published

2022

6. Structure–function analysis of oncogenic EGFR Kinase Domain Duplication reveals insights into activation and a potential approach for therapeutic targeting

Author

Zhenfang Du, Benjamin P. Brown, Soyeon Kim, Donna Ferguson, Dean C. Pavlick, Gowtham Jayakumaran, Ryma Benayed, Jean-Nicolas Gallant, Yun-Kai Zhang, Yingjun Yan, Monica Red-Brewer, Siraj M. Ali, Alexa B. Schrock, Ahmet Zehir, Marc Ladanyi, Adam W. Smith, Jens Meiler, and Christine M. Lovly

Subjects

Science

Abstract

An EGFR mutant with kinase domain duplication (EGFR-KDD) was previously identified in an index patient, but the functional and therapeutic implications remain unclear. Here, the authors show that KDD occurs in other ErbB receptors in multiple cancers, and characterize the mechanism and inhibition of EGFR-KDD.

Published

2021

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

Author

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

Subjects

Desmoplastic small round cell tumor, Sarcoma, Genomic profiling, FGFR4, Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Desmoplastic 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. Methods Tumor 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. Results Comprehensive 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. Conclusions In 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

8. Exceptional Response to Everolimus in a Patient with Metastatic Castrate-Resistant Prostate Cancer Harboring a PTEN Inactivating Mutation

Author

Jamie A. Kmak, Nikita Agarwal, Yuting He, Andreas M. Heilmann, Vincent A. Miller, Jeffrey S. Ross, Sumanta Kumar Pal, Siraj M. Ali, and Deepak Kilari

Subjects

pten, prostate cancer, everolimus, castration resistant, mtor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Prostate cancer is among the most common types of cancer in men. Early detection and proper medical intervention is crucial to ensuring successful treatment. Here we describe a patient clinically presenting with castrate-resistant prostate carcinoma. Comprehensive genomic profiling identified a PTEN inactivating mutation in the patient’s tumor. After being heavily pretreated, the patient showed stable disease on everolimus, a PI3K-Akt-mTOR pathway inhibitor.

Published

2020

9. Genomic profiling of solid tumors harboring BRD4-NUT and response to immune checkpoint inhibitors

Author

Jonathan W. Riess, Shaila Rahman, Waleed Kian, Claire Edgerly, Andreas M. Heilmann, Russell Madison, Shakti H. Ramkissoon, Shai Shlomi Klaitman, Jon H. Chung, Sally E. Trabucco, Dexter X. Jin, Brian M. Alexander, Samuel J. Klempner, Lee A. Albacker, Garrett M. Frampton, Laila C. Roisman, Vincent A. Miller, Jeffrey S. Ross, Alexa B. Schrock, Jeffrey P. Gregg, Nir Peled, Ethan S. Sokol, and Siraj M. Ali

Subjects

NUT midline carcinoma, NUT carcinoma, BRD4-NUT, Checkpoint inhibitor, PD-L1, BRD4, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background: The translocation t(15:19) produces the oncogenic BRD4-NUT fusion which is pathognomonic for NUT carcinoma (NC), which is a rare, but extremely aggressive solid tumor. Comprehensive genomic profiling (CGP) by hybrid-capture based next generation sequencing of 186+ genes of a cohort of advanced cancer cases with a variety of initial diagnoses harboring BRD4-NUT may shed further insight into the biology of these tumors and possible options for targeted treatment. Case presentation: Thirty-one solid tumor cases harboring a BRD4-NUT translocation are described, with only 16% initially diagnosed as NC and the remainder carrying other diagnoses, most commonly NSCLCNOS (22%) and lung squamous cell carcinoma (NSCLC-SCC) (16%). The cohort was all microsatellite stable and harbored a low Tumor Mutational Burden (TMB, mean 1.7 mut/mb, range 0–4). In two index cases, patients treated with immune checkpoint inhibitors (ICPI) had unexpected partial or better responses of varying duration. Notably, four cases – including the two index cases - were negative for PD-L1 expression. Neo-antigen prediction for BRD4-NUT and then affinity modeling of the peptide-MHC (pMHC) complex for an assessable index case predicted very high affinity binding, both on a ranked (99.9%) and absolute (33 nM) basis. Conclusions: CGP identifies BRD4-NUT fusions in advanced solid tumors which carry a broad range of initial diagnoses and which should be re-diagnosed as NC per guidelines. A hypothesized mechanism underlying responses to ICPI in the low TMB, PD-L1 negative index cases is the predicted high affinity of the BRD4-NUT fusion peptide to MHC complexes. Further study of pMHC affinity and response to immune checkpoint inhibitors in patients with NC harboring BRD4-NUT is needed to validate this therapeutic hypothesis.

Published

2021

10. Responsiveness to immune checkpoint inhibitors versus other systemic therapies in RET-aberrant malignancies

Author

Jessica Lee, Vivek Subbiah, Shuang Liu, Jason Roszik, David Hong, Funda Meric-Bernstam, John Heymach, Ramona Dadu, Kenneth Hess, Le Huang, Aparna Hegde, Alexander Y Andreev-Drakhlin, Maria Cabanillas, Mimi I Hu, Naifa L Busaidy, Steven I Sherman, Elizabeth G Grubbs, Siraj M Ali, Yasir Y Elamin, George R Simon, George R Blumenschein, Jr, and Vassiliki A Papadimitrakopoulou

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Purpose The receptor tyrosine kinase rearranged during transfection (RET) can be oncogenically activated by gene fusions or point mutations. Multikinase inhibitors such as cabozantinib, lenvatinib and vandetanib have demonstrated activity in RET-dependent malignancies, and selective RET inhibitors (Selpercatinib and Pralsetinib) are in clinical trials. However, the responsiveness of RET-dependent malignancies to immune checkpoint inhibitors (ICIs) is unknown. We compared the time to treatment discontinuation (TTD) for ICI versus non-ICI therapy in patients with malignancies harbouring activating RET mutations or fusions (RET+).Methods A retrospective review of all RET+ patients who were referred to the phase I clinical trials programme at the University of Texas MD Anderson Cancer Center was conducted. TTD was estimated using Kaplan-Meier analysis. Multivariate analysis using the Cox proportional hazard model was performed to identify independent risk factors of treatment discontinuation.Results Of 70 patients who received systemic therapy for RET+ malignancies, 20 (28.6%) received ICI and 50 (71.4%) received non-ICI therapy. Non-ICI therapy was associated with decreased risk for treatment discontinuation compared with ICI in the overall population (HR=0.31; 95% CI 0.16–0.62; p=0.000834) and in patients with RET point mutations (HR=0.13; 95% CI 0.04–0.45; p=0.00134). In patients with RET fusions, non-ICI therapy was associated with a non-statistically significant decreased risk of treatment discontinuation (HR=0.59; 95% CI 0.25–1.4; p=0.24). ICI therapy and a diagnosis other than medullary thyroid cancer (MTC) were independent risk factors for treatment discontinuation.Conclusion Our study supports the prioritisation of non-ICI over ICI therapy in patients with RET+ tumours.

Published

2020

11. RET rearrangements are actionable alterations in breast cancer

Author

Bhavna S. Paratala, Jon H. Chung, Casey B. Williams, Bahar Yilmazel, Whitney Petrosky, Kirstin Williams, Alexa B. Schrock, Laurie M. Gay, Ellen Lee, Sonia C. Dolfi, Kien Pham, Stephanie Lin, Ming Yao, Atul Kulkarni, Frances DiClemente, Chen Liu, Lorna Rodriguez-Rodriguez, Shridar Ganesan, Jeffrey S. Ross, Siraj M. Ali, Brian Leyland-Jones, and Kim M. Hirshfield

Subjects

Science

Abstract

Fusions of the gene RET have been described in thyroid and lung cancers. Here, the AUs identify RET gene alterations, including known fusions, novel fusions, and rearrangements in breast cancer (BC) that are involved in the tumorigenic process and show the benefit of RET therapy in a recurrent BC patient carrying the NCOA4-RET fusion.

Published

2018

12. Clinical utility of tumor genomic profiling in patients with high plasma circulating tumor DNA burden or metabolically active tumors

Author

Cathy Zhou, Zilong Yuan, Weijie Ma, Lihong Qi, Angelique Mahavongtrakul, Ying Li, Hong Li, Jay Gong, Reggie R. Fan, Jin Li, Michael Molmen, Travis A. Clark, Dean Pavlick, Garrett M. Frampton, Brady Forcier, Elizabeth H. Moore, David K. Shelton, Matthew Cooke, Siraj M. Ali, Vincent A. Miller, Jeffrey P. Gregg, Philip J. Stephens, and Tianhong Li

Subjects

Next-generation sequencing (NGS), Plasma, Cell-free DNA (cfDNA), Circulating tumor DNA (ctDNA), Genomic alterations (GAs), Maximum somatic allele frequency (MSAF), Diseases of the blood and blood-forming organs, RC633-647.5, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background This retrospective study was undertaken to determine if the plasma circulating tumor DNA (ctDNA) level and tumor biological features in patients with advanced solid tumors affected the detection of genomic alterations (GAs) by a plasma ctDNA assay. Method Cell-free DNA (cfDNA) extracted from frozen plasma (N = 35) or fresh whole blood (N = 90) samples were subjected to a 62-gene hybrid capture-based next-generation sequencing assay FoundationACT. Concordance was analyzed for 51 matched FoundationACT and FoundationOne (tissue) cases. The maximum somatic allele frequency (MSAF) was used to estimate the amount of tumor fraction of cfDNA in each sample. The detection of GAs was correlated with the amount of cfDNA, MSAF, total tumor anatomic burden (dimensional sum), and total tumor metabolic burden (SUVmax sum) of the largest ten tumor lesions on PET/CT scans. Results FoundationACT detected GAs in 69 of 81 (85%) cases with MSAF > 0. Forty-two of 51 (82%) cases had ≥ 1 concordance GAs matched with FoundationOne, and 22 (52%) matched to the National Comprehensive Cancer Network (NCCN)-recommended molecular targets. FoundationACT also detected 8 unique molecular targets, which changed the therapy in 7 (88%) patients who did not have tumor rebiopsy or sufficient tumor DNA for genomic profiling assay. In all samples (N = 81), GAs were detected in plasma cfDNA from cancer patients with high MSAF quantity (P = 0.0006) or high tumor metabolic burden (P = 0.0006) regardless of cfDNA quantity (P = 0.2362). Conclusion This study supports the utility of using plasma-based genomic assays in cancer patients with high plasma MSAF level or high tumor metabolic burden.

Published

2018

13. A Common Cell of Origin for Inflammatory Myofibroblastic Tumor and Lung Adenocarcinoma with ALK rearrangement

Author

Vasyl Nesteryuk, Omar Hamdani, Raymond Gong, Nava Almog, Brian M. Alexander, Steffan Soosman, Ken Yoneda, Siraj M. Ali, Alexander D. Borowsky, and Jonathan W. Riess

Subjects

Pulmonary and Respiratory Medicine, Cancer Research, Oncology

Published

2022

14. Analysis of 100,000 human cancer genomes reveals the landscape of tumor mutational burden

Author

Zachary R. Chalmers, Caitlin F. Connelly, David Fabrizio, Laurie Gay, Siraj M. Ali, Riley Ennis, Alexa Schrock, Brittany Campbell, Adam Shlien, Juliann Chmielecki, Franklin Huang, Yuting He, James Sun, Uri Tabori, Mark Kennedy, Daniel S. Lieber, Steven Roels, Jared White, Geoffrey A. Otto, Jeffrey S. Ross, Levi Garraway, Vincent A. Miller, Phillip J. Stephens, and Garrett M. Frampton

Subjects

Tumor mutational burden, Cancer genomics, Mismatch repair, PMS2, Medicine, Genetics, QH426-470

Abstract

Abstract Background High tumor mutational burden (TMB) is an emerging biomarker of sensitivity to immune checkpoint inhibitors and has been shown to be more significantly associated with response to PD-1 and PD-L1 blockade immunotherapy than PD-1 or PD-L1 expression, as measured by immunohistochemistry (IHC). The distribution of TMB and the subset of patients with high TMB has not been well characterized in the majority of cancer types. Methods In this study, we compare TMB measured by a targeted comprehensive genomic profiling (CGP) assay to TMB measured by exome sequencing and simulate the expected variance in TMB when sequencing less than the whole exome. We then describe the distribution of TMB across a diverse cohort of 100,000 cancer cases and test for association between somatic alterations and TMB in over 100 tumor types. Results We demonstrate that measurements of TMB from comprehensive genomic profiling are strongly reflective of measurements from whole exome sequencing and model that below 0.5 Mb the variance in measurement increases significantly. We find that a subset of patients exhibits high TMB across almost all types of cancer, including many rare tumor types, and characterize the relationship between high TMB and microsatellite instability status. We find that TMB increases significantly with age, showing a 2.4-fold difference between age 10 and age 90 years. Finally, we investigate the molecular basis of TMB and identify genes and mutations associated with TMB level. We identify a cluster of somatic mutations in the promoter of the gene PMS2, which occur in 10% of skin cancers and are highly associated with increased TMB. Conclusions These results show that a CGP assay targeting ~1.1 Mb of coding genome can accurately assess TMB compared with sequencing the whole exome. Using this method, we find that many disease types have a substantial portion of patients with high TMB who might benefit from immunotherapy. Finally, we identify novel, recurrent promoter mutations in PMS2, which may be another example of regulatory mutations contributing to tumorigenesis.

Published

2017

15. AENEAS: A Randomized Phase III Trial of Aumolertinib Versus Gefitinib as First-Line Therapy for Locally Advanced or MetastaticNon–Small-Cell Lung Cancer With EGFR Exon 19 Deletion or L858R Mutations

Author

Shun Lu, Xiaorong Dong, Hong Jian, Jianhua Chen, Gongyan Chen, Yuping Sun, Yinghua Ji, Ziping Wang, Jianhua Shi, Junguo Lu, Shaoshui Chen, Dongqing Lv, Guojun Zhang, Chunling Liu, Juan Li, Xinmin Yu, Zhong Lin, Zhuang Yu, Zhehai Wang, Jiuwei Cui, Xingxiang Xu, Jian Fang, Jifeng Feng, Zhi Xu, Rui Ma, Jie Hu, Nong Yang, Xiangdong Zhou, Xiaohong Wu, Chengping Hu, Zhihong Zhang, You Lu, Yanping Hu, Liyan Jiang, Qiming Wang, Renhua Guo, Jianying Zhou, Baolan Li, Chunhong Hu, Wancheng Tong, Helong Zhang, Lin Ma, Yuan Chen, Zhijun Jie, Yu Yao, Longzhen Zhang, Weng Jie, Weidong Li, Jianping Xiong, Xianwei Ye, Jianchun Duan, Haihua Yang, Meili Sun, Changan Sun, Hongying Wei, Chuan Li, Siraj M. Ali, Vincent A. Miller, and Qiong Wu

Subjects

Cancer Research, Oncology

Abstract

PURPOSE Aumolertinib (formerly almonertinib; HS-10296) is a novel third-generation epidermal growth factor receptor tyrosine kinase inhibitor approved in China. This double-blind phase III trial evaluated the efficacy and safety of aumolertinib compared with gefitinib as a first-line treatment for locally advanced or metastatic EGFR-mutated non–small-cell lung cancer (NSCLC; ClinicalTrials.gov identifier: NCT03849768 ). METHODS Patients at 53 sites in China were randomly assigned 1:1 to receive either aumolertinib (110 mg) or gefitinib (250 mg) once daily. The primary end point was progression-free survival (PFS) per investigator assessment. RESULTS A total of 429 patients who were naïve to treatment for locally advanced or metastatic NSCLC were enrolled. PFS was significantly longer with aumolertinib compared with gefitinib (hazard ratio, 0.46; 95% CI, 0.36 to 0.60; P < .0001). The median PFS with aumolertinib was 19.3 months (95% CI, 17.8 to 20.8) versus 9.9 months with gefitinib (95% CI, 8.3 to 12.6). Objective response rate and disease control rate were similar in the aumolertinib and gefitinib groups (objective response rate, 73.8% and 72.1%, respectively; disease control rate, 93.0% and 96.7%, respectively). The median duration of response was 18.1 months (95% CI, 15.2 to not applicable) with aumolertinib versus 8.3 months (95% CI, 6.9 to 11.1) with gefitinib. Adverse events of grade ≥ 3 severity (any cause) were observed in 36.4% and 35.8% of patients in the aumolertinib and gefitinib groups, respectively. Rash and diarrhea (any grade) were observed in 23.4% and 16.4% of patients who received aumolertinib compared with 41.4% and 35.8% of those who received gefitinib, respectively. CONCLUSION Aumolertinib is a well-tolerated third-generation epidermal growth factor receptor tyrosine kinase inhibitor that could serve as a treatment option for EGFR-mutant NSCLC in the first-line setting.

Published

2022

16. Supplementary Figure from The Genomics of Colorectal Cancer in Populations with African and European Ancestry

Author

Siraj M. Ali, Sanjay Goel, Srilakshmi M. Raj, John M. Greally, Amit Verma, Leonard Augenlicht, Sudipto Das, Alexa B. Schrock, Jeffrey M. Venstrom, Jeffery S. Ross, Garrett M. Frampton, Samuel J. Klempner, Carmen R. Isasi, Justin Y. Newberg, Kith Pradhan, Russell W. Madison, Jessica K. Lee, and Parvathi A. Myer

Abstract

Supplementary Figure from The Genomics of Colorectal Cancer in Populations with African and European Ancestry

Published

2023

17. Data from The Genomics of Colorectal Cancer in Populations with African and European Ancestry

Author

Siraj M. Ali, Sanjay Goel, Srilakshmi M. Raj, John M. Greally, Amit Verma, Leonard Augenlicht, Sudipto Das, Alexa B. Schrock, Jeffrey M. Venstrom, Jeffery S. Ross, Garrett M. Frampton, Samuel J. Klempner, Carmen R. Isasi, Justin Y. Newberg, Kith Pradhan, Russell W. Madison, Jessica K. Lee, and Parvathi A. Myer

Abstract

Black people have a higher incidence of colorectal cancer and worse survival rates when compared with white people. Comprehensive genomic profiling was performed in 46,140 colorectal adenocarcinoma cases. Ancestry-informative markers identified 5,301 patients of African descent (AFR) and 33,770 patients of European descent (EUR). AFR were younger, had fewer microsatellite instability–high (MSI-H) tumors, and had significantly more frequent alterations in KRAS, APC, and PIK3CA. AFR had increased frequency of KRAS mutations, specifically KRASG12D and KRASG13. There were no differences in rates of actionable kinase driver alterations (HER2, MET, NTRK, ALK, ROS1, and RET). In patients with young-onset colorectal cancer (APC mutations by age, as well as differences in MAPK pathway alterations. These findings inform treatment decisions, impact prognosis, and underscore the need for model systems representative of the diverse U.S. population.Significance:KRAS (particularly KRASG12D/G13), APC, and PIK3CA were more frequently altered in AFR who had a lower frequency of MSI-H tumors. There were no differences in actionable kinase driver alterations. In young-onset colorectal cancer, both ancestries had a similar frequency of MSI-H/TMB-H tumors, but strikingly different trends in APC.See related commentary by Eng and Holowatyj, p. 1187.This article is highlighted in the In This Issue feature, p. 1171

Published

2023

18. Supplementary Methods, Figures 1 - 5, Tables 1 - 5 from Diverse and Targetable Kinase Alterations Drive Histiocytic Neoplasms

Author

Omar Abdel-Wahab, Tanja A. Gruber, Neal Rosen, Jean-Francois Emile, Ahmet Dogan, Zahir Amoura, Christopher Y. Park, Barry S. Taylor, Filip Janku, José Baselga, David M. Hyman, David B. Solit, Jean Donadieu, Sebastien Héritier, Jared Block, Omotayo Fasan, Samuel R. Briggs, Siraj M. Ali, Jeffrey S. Ross, Vincent A. Miller, Philip J. Stephens, William A. Gahl, Mario Lacouture, Juvianee Estrada-Veras, David W. Ellison, James D. Dalton, Chezi Ganzel, Joy Nakitandwe, Paul Zappile, Adriana Heguy, Olga Aminova, Igor Dolgalev, Brooke Sylvester, Michael P. Walsh, Patrick Campbell, Jean-Baptiste Micol, Yijun Gao, Stanley Chun-Wei Lee, Fleur Cohen-Aubart, Eunhee Kim, John Choi, Zhaoming Wang, Sameer A. Parikh, Jing Ma, Zhan Yao, Julien Haroche, Benjamin H. Durham, and Eli L. Diamond

Abstract

Supplementary Figure 1. Somatic mutations detected in histiocytic neoplasms. Supplementary Figure 2. Frequencies of known activating kinase mutations in histiocytic neoplasms. Supplementary Figure 3. ARAF mutations and variants of unknown significance detected in BRAFV600E-wildtype, non-Langerhans Cell Histiocytic neoplasms. Supplementary Figure 4. Clinical and histological images of the non-Langerhans cell histiocytosis (non-LCH) lesions from index patients with kinase fusions identified by RNA-seq. Supplementary Figure 5. Gene expression analysis of histiocytic neoplasms by RNA-seq. Supplementary Table 1. Characteristics of patient samples with histiocytic neoplasms used in this study and genomic analysis utilized for each sample. Supplementary Table 2. Whole exome sequencing metrics. Supplementary Table 3. Somatic variants identified by whole exome and whole transcriptome sequencing and validated by droplet-digital PCR and/or custom-capture targeted next-generation sequencing with variant allele frequencies (VAFs). Supplementary Table 4. List of the top 1% of differentially expressed genes across histiocytic samples from mRNA sequencing. Supplementary Table 5. PCR primers with M13F2 and M13R2 tails (blue) for Sanger sequencing used in the targeted sequencing recurrence testing for MAP2K1 exons 2 and 3 and all coding regions of ARAF.

Published

2023

19. Supplementary Methods, Figure Legends, Table Legends from EGFR Fusions as Novel Therapeutic Targets in Lung Cancer

Author

Christine M. Lovly, Siraj M. Ali, Vincent A. Miller, Philip J. Stephens, Jeffrey S. Ross, Deborah Morosini, Jens Meiler, Jonathan H. Sheehan, Yingjun Yan, Heidi Chen, Andrew Whiteley, Tiziana Vavalà, Beth Eaby-Sandy, Satyanarayan K. Reddy, Suresh S. Ramalingam, Vijay Peddareddigari, Taofeek K. Owonikoko, Eiki Ichihara, Kyle Gowen, Barbara J. Gitlitz, Francis J. Giles, Young Kwang Chae, Jean-Nicolas Gallant, and Kartik Konduri

Abstract

Supplementary Methods, Supplementary References, Supplementary Table Legends, and Supplementary Figure Legends.

Published

2023

20. Supplementary Table S3 from Comprehensive Genomic Profiling of Pancreatic Acinar Cell Carcinomas Identifies Recurrent RAF Fusions and Frequent Inactivation of DNA Repair Genes

Author

Philip J. Stephens, David S. Klimstra, Vincent A. Miller, William Pao, Roman Yelensky, Doron Lipson, Sohail Balasubramanian, Olca Basturk, Jeffrey S. Ross, Siraj M. Ali, Julia Elvin, Chanjuan Shi, Adrienne Johnson, Zachary R. Chalmers, Garrett M. Frampton, Katherine E. Hutchinson, and Juliann Chmielecki

Abstract

Supplementary Table S3: Genomic alterations across selected targets. See Figure 3 for additional details. Zoomable PDF.

Published

2023

21. Data from Targeted Next Generation Sequencing Identifies Markers of Response to PD-1 Blockade

Author

Christine M. Lovly, Jeffrey A. Sosman, Ryan J. Sullivan, Philip J. Stephens, Vincent A. Miller, Yu Shyr, Harlan Robins, Catherine Sanders, Jeffrey S. Ross, Justin M. Cates, Justin M. Balko, Igor Puzanov, Dennie T. Frederick, Yuting He, James X. Sun, Sohail Balasubramanian, Siraj M. Ali, Joel Greenbowe, Zachary R. Chalmers, David Fabrizio, Riley C. Ennis, Xingyi Guo, Yaomin Xu, Erik Yusko, Matthew J. Rioth, Garrett M. Frampton, and Douglas B. Johnson

Abstract

Therapeutic antibodies blocking programmed death-1 and its ligand (PD-1/PD-L1) induce durable responses in a substantial fraction of melanoma patients. We sought to determine whether the number and/or type of mutations identified using a next-generation sequencing (NGS) panel available in the clinic was correlated with response to anti–PD-1 in melanoma. Using archival melanoma samples from anti–PD-1/PD-L1-treated patients, we performed hybrid capture–based NGS on 236–315 genes and T-cell receptor (TCR) sequencing on initial and validation cohorts from two centers. Patients who responded to anti–PD-1/PD-L1 had higher mutational loads in an initial cohort (median, 45.6 vs. 3.9 mutations/MB; P = 0.003) and a validation cohort (37.1 vs. 12.8 mutations/MB; P = 0.002) compared with nonresponders. Response rate, progression-free survival, and overall survival were superior in the high, compared with intermediate and low, mutation load groups. Melanomas with NF1 mutations harbored high mutational loads (median, 62.7 mutations/MB) and high response rates (74%), whereas BRAF/NRAS/NF1 wild-type melanomas had a lower mutational load. In these archival samples, TCR clonality did not predict response. Mutation numbers in the 315 genes in the NGS platform strongly correlated with those detected by whole-exome sequencing in The Cancer Genome Atlas samples, but was not associated with survival. In conclusion, mutational load, as determined by an NGS platform available in the clinic, effectively stratified patients by likelihood of response. This approach may provide a clinically feasible predictor of response to anti–PD-1/PD-L1. Cancer Immunol Res; 4(11); 959–67. ©2016 AACR.

Published

2023

22. Supplementary Figures 1 - 3 from RICTOR Amplification Defines a Novel Subset of Patients with Lung Cancer Who May Benefit from Treatment with mTORC1/2 Inhibitors

Author

Roman Perez-Soler, Bilal Piperdi, Vincent A. Miller, Philip J. Stephens, Matthew Hawryluk, Geoff Otto, Doron Lipson, Roman Yelensky, Kira Gritsman, Yiting Yu, Jidong Shan, Changcheng Zhu, Edward L. Schwartz, Sanjay Goel, Abraham Chachoua, Cristina Montagna, Amit Verma, Huijie Liu, Siraj M. Ali, Balazs Halmos, Xuewen Liu, Kai Wang, Jeffrey S. Ross, Yiyu Zou, and Haiying Cheng

Abstract

Supplementary Figure 1 shows RICTOR amplification/overexpression in the index patient by FISH and IHC. Supplementary Figure 2 shows analysis of TCGA database for RICTOR alteration in all types of cancers, including NSCLC. Supplementary figure 3A shows the gene alterations in each individual with RICTOR-amplified tumors. 3B shows the absolute and relative frequency of each gene alteration found in RICTOR-amplified lung cancer samples from FM NGS database.

Published

2023

23. Supplementary Tables S1 - S3 from EGFR Fusions as Novel Therapeutic Targets in Lung Cancer

Author

Christine M. Lovly, Siraj M. Ali, Vincent A. Miller, Philip J. Stephens, Jeffrey S. Ross, Deborah Morosini, Jens Meiler, Jonathan H. Sheehan, Yingjun Yan, Heidi Chen, Andrew Whiteley, Tiziana Vavalà, Beth Eaby-Sandy, Satyanarayan K. Reddy, Suresh S. Ramalingam, Vijay Peddareddigari, Taofeek K. Owonikoko, Eiki Ichihara, Kyle Gowen, Barbara J. Gitlitz, Francis J. Giles, Young Kwang Chae, Jean-Nicolas Gallant, and Kartik Konduri

Abstract

Supplementary Tables S1 - S3. Supplementary Table S1. Summary of EGFR alterations in NSCLC identified by FoundationOne. Supplementary Table S2. Summary of genomic coordinates for the kinase fusions identified in this study. Supplementary Table S3. Results of MTT curve fitting from Prism.

Published

2023

24. Supplementary Figure S3 from Comprehensive Genomic Profiling of Pancreatic Acinar Cell Carcinomas Identifies Recurrent RAF Fusions and Frequent Inactivation of DNA Repair Genes

Author

Philip J. Stephens, David S. Klimstra, Vincent A. Miller, William Pao, Roman Yelensky, Doron Lipson, Sohail Balasubramanian, Olca Basturk, Jeffrey S. Ross, Siraj M. Ali, Julia Elvin, Chanjuan Shi, Adrienne Johnson, Zachary R. Chalmers, Garrett M. Frampton, Katherine E. Hutchinson, and Juliann Chmielecki

Abstract

Supplementary Fig. S3: Co-mutation across all PACC tumors.

Published

2023

25. Supplementary Methods from Comprehensive Genomic Profiling of Pancreatic Acinar Cell Carcinomas Identifies Recurrent RAF Fusions and Frequent Inactivation of DNA Repair Genes

Author

Philip J. Stephens, David S. Klimstra, Vincent A. Miller, William Pao, Roman Yelensky, Doron Lipson, Sohail Balasubramanian, Olca Basturk, Jeffrey S. Ross, Siraj M. Ali, Julia Elvin, Chanjuan Shi, Adrienne Johnson, Zachary R. Chalmers, Garrett M. Frampton, Katherine E. Hutchinson, and Juliann Chmielecki

Abstract

Additional detailed methods.

Published

2023

26. Supplementary Tables 1 through 3 and Supplementary Figures 1 through 4 from Targeted Next Generation Sequencing Identifies Markers of Response to PD-1 Blockade

Author

Christine M. Lovly, Jeffrey A. Sosman, Ryan J. Sullivan, Philip J. Stephens, Vincent A. Miller, Yu Shyr, Harlan Robins, Catherine Sanders, Jeffrey S. Ross, Justin M. Cates, Justin M. Balko, Igor Puzanov, Dennie T. Frederick, Yuting He, James X. Sun, Sohail Balasubramanian, Siraj M. Ali, Joel Greenbowe, Zachary R. Chalmers, David Fabrizio, Riley C. Ennis, Xingyi Guo, Yaomin Xu, Erik Yusko, Matthew J. Rioth, Garrett M. Frampton, and Douglas B. Johnson

Abstract

Supplementary Table 1: Results for samples obtained (less than or equal to) 12 months prior to therapy (optimal) vs. those obtained >12 months from treatment or shortly after starting therapy (non-optimal). Supplementary Table 2: Cox proportional hazards model of OS adjusting for baseline variables. Supplementary Table 3: Cox proportional hazards model of PFS adjusting for baseline variables. Figure S1: (A) Performance of mutational load across a range of potential thresholds. (B) Receiver Operating Curve (ROC) for mutational loads cutoffs of 3.3 mutations/MB (low mutational load group) and 23.1 mutations/MB (high mutational load group). Figure S2: (A) Mutational load in tumors with cutaneous/unknown primaries in responders vs. non-responders. (B) Mutational load in tumors with non-cutaneous primaries (acral, mucosal, uveal) in responders vs. non-responders. (C) Gene amplifications and deletions in responders vs. non-responders. Figure S3: (A) LRP1B mutations/variants of unknown significance in responders vs. non-responders. (B) Total number of mutations among melanomas with and without LRP1B mutations. (C) Association between number of LRP1B mutations and total mutations in the melanoma TCGA. Figure S4: (A) T cell receptor (TCR) clonality in responders vs. non-responders. (B) T cell fraction in responders vs. non-responders. (C) TCR clonality in responders vs. non-responders in ideal samples, defined as those obtained within 4 months of anti-PD-1/PD-L1 treatment without other prior therapies. (D) T cell fraction in these ideal samples. Figure S5: Mutation load correlated with (A) T cell receptor (TCR) clonality and (B) T cell fraction.

Published

2023

27. Supplementary Figures S1 - S10 from EGFR Fusions as Novel Therapeutic Targets in Lung Cancer

Author

Christine M. Lovly, Siraj M. Ali, Vincent A. Miller, Philip J. Stephens, Jeffrey S. Ross, Deborah Morosini, Jens Meiler, Jonathan H. Sheehan, Yingjun Yan, Heidi Chen, Andrew Whiteley, Tiziana Vavalà, Beth Eaby-Sandy, Satyanarayan K. Reddy, Suresh S. Ramalingam, Vijay Peddareddigari, Taofeek K. Owonikoko, Eiki Ichihara, Kyle Gowen, Barbara J. Gitlitz, Francis J. Giles, Young Kwang Chae, Jean-Nicolas Gallant, and Kartik Konduri

Abstract

Supplementary Figures S1 - S10. Supplementary Figure S1. Additional information for Patient 1. Supplementary Figure S2. Additional information for Patient 2. Supplementary Figure S3. Additional information for Patient 3. Supplementary Figure S4. Additional clinical information for Patient 4. Supplementary Figure S5. Characterization of EGFR-RAD51 in NR6 cells. Supplementary Figure S6. Relative stability of EGFR-WT, -L858R, and -RAD51. Supplementary Figure S7. Structural model of EGFR-RAD51 filaments. Supplementary Figure S8. On-target inhibition of EGFR-RAD51 by EGFR TKI. Supplementary Figure S9. Cetuximab inhibits ligand-induced activation of downstream signaling pathways in cells expressing EGFR-RAD51. Supplementary Figure S10. cDNA sequence of EGFR-RAD51.

Published

2023

28. Supplementary Figures 1 - 6, Table 1 from EGFR Kinase Domain Duplication (EGFR-KDD) Is a Novel Oncogenic Driver in Lung Cancer That Is Clinically Responsive to Afatinib

Author

Christine M. Lovly, Jens Meiler, Siraj M. Ali, Vincent A. Miller, Marc Ladanyi, Jennifer A. Pietenpol, Mark G. Kris, Sally J. York, Monica Red Brewer, Raghu Chandramohan, Doron Lipson, Mark Bailey, Timothy M. Shaver, Jonathan H. Sheehan, and Jean-Nicolas Gallant

Abstract

This document contains Supplementary Figures 1-6 and Supplementary Table 1. Supplementary Figure 1. Sequencing reads of EGFR-KDD in index patient with lung adenocarcinoma. Supplementary Figure 2. cDNA sequence of EGFR-KDD. Supplementary Figure 3. Sequencing reads identifying EGFR-KDD in a lung adenocarcinoma tumor from The Cancer Genome Atlas. Supplementary Figure 4. Autophosphorylation of endogenous EGFR-KDD in A1235 cells. Supplementary Figure 5. Colony formation of NR6 cells expressing EGFR variants. Supplementary Figure 6. Efficacy of EGFR TKIs in endogenous and ectopic models of the EGFR-KDD. Supplementary Table 1. Results of MTT curve fitting from Prism.

Published

2023

29. Supplementary Table S3 from Activation of MET via Diverse Exon 14 Splicing Alterations Occurs in Multiple Tumor Types and Confers Clinical Sensitivity to MET Inhibitors

Author

Vincent A. Miller, Philip J. Stephens, Malte Peters, Eric Collisson, Jeffrey S. Ross, Deborah Morosini, Roman Yelensky, Doron Lipson, Robert Schlegel, Joel Greshock, Jared White, Steven Roels, Eric M. Sanford, Caitlin McMahon, Depinder Khaira, Adrienne Johnson, Joel Greenbowe, Kyle A. Gowen, Alex Fichtenholtz, Rachel Erlich, Julia A. Elvin, Alan Huang, Savina Jaeger, Zachary R. Chalmers, Tim Brennan, Ravi Salgia, Sai-Hong Ignatius Ou, Rick Hoover, David Jentz, Carrie Lee, Jose A. Bufill, Mikhail Akimov, Todd M. Bauer, Xinyuan Lu, Juliann Chmielecki, Mark Rosenzweig, Siraj M. Ali, and Garrett M. Frampton

Abstract

Genomic alterations in lung adenocarcinoma displayed in Figure 2A.

Published

2023

30. Supplementary Methods, Figure Legends, Table Legend from EGFR Kinase Domain Duplication (EGFR-KDD) Is a Novel Oncogenic Driver in Lung Cancer That Is Clinically Responsive to Afatinib

Author

Christine M. Lovly, Jens Meiler, Siraj M. Ali, Vincent A. Miller, Marc Ladanyi, Jennifer A. Pietenpol, Mark G. Kris, Sally J. York, Monica Red Brewer, Raghu Chandramohan, Doron Lipson, Mark Bailey, Timothy M. Shaver, Jonathan H. Sheehan, and Jean-Nicolas Gallant

Abstract

This document contains Supplementary Methods, Supplementary Figure Legends, and Supplementary Table Legend.

Published

2023

31. Data from Activation of MET via Diverse Exon 14 Splicing Alterations Occurs in Multiple Tumor Types and Confers Clinical Sensitivity to MET Inhibitors

Author

Vincent A. Miller, Philip J. Stephens, Malte Peters, Eric Collisson, Jeffrey S. Ross, Deborah Morosini, Roman Yelensky, Doron Lipson, Robert Schlegel, Joel Greshock, Jared White, Steven Roels, Eric M. Sanford, Caitlin McMahon, Depinder Khaira, Adrienne Johnson, Joel Greenbowe, Kyle A. Gowen, Alex Fichtenholtz, Rachel Erlich, Julia A. Elvin, Alan Huang, Savina Jaeger, Zachary R. Chalmers, Tim Brennan, Ravi Salgia, Sai-Hong Ignatius Ou, Rick Hoover, David Jentz, Carrie Lee, Jose A. Bufill, Mikhail Akimov, Todd M. Bauer, Xinyuan Lu, Juliann Chmielecki, Mark Rosenzweig, Siraj M. Ali, and Garrett M. Frampton

Abstract

Focal amplification and activating point mutation of the MET gene are well-characterized oncogenic drivers that confer susceptibility to targeted MET inhibitors. Recurrent somatic splice site alterations at MET exon 14 (METex14) that result in exon skipping and MET activation have been characterized, but their full diversity and prevalence across tumor types are unknown. Here, we report analysis of tumor genomic profiles from 38,028 patients to identify 221 cases with METex14 mutations (0.6%), including 126 distinct sequence variants. METex14 mutations are detected most frequently in lung adenocarcinoma (3%), but also frequently in other lung neoplasms (2.3%), brain glioma (0.4%), and tumors of unknown primary origin (0.4%). Further in vitro studies demonstrate sensitivity to MET inhibitors in cells harboring METex14 alterations. We also report three new patient cases with METex14 alterations in lung or histiocytic sarcoma tumors that showed durable response to two different MET-targeted therapies. The diversity of METex14 mutations indicates that diagnostic testing via comprehensive genomic profiling is necessary for detection in a clinical setting.Significance: Here we report the identification of diverse exon 14 splice site alterations in MET that result in constitutive activity of this receptor and oncogenic transformation in vitro. Patients whose tumors harbored these alterations derived meaningful clinical benefit from MET inhibitors. Collectively, these data support the role of METex14 alterations as drivers of tumorigenesis, and identify a unique subset of patients likely to derive benefit from MET inhibitors. Cancer Discov; 5(8); 850–9. ©2015 AACR.See related commentary by Ma, p. 802.See related article by Paik et al., p. 842.This article is highlighted in the In This Issue feature, p. 783

Published

2023

32. Supplementary Table S1A - S1B from Comprehensive Genomic Profiling of Pancreatic Acinar Cell Carcinomas Identifies Recurrent RAF Fusions and Frequent Inactivation of DNA Repair Genes

Author

Philip J. Stephens, David S. Klimstra, Vincent A. Miller, William Pao, Roman Yelensky, Doron Lipson, Sohail Balasubramanian, Olca Basturk, Jeffrey S. Ross, Siraj M. Ali, Julia Elvin, Chanjuan Shi, Adrienne Johnson, Zachary R. Chalmers, Garrett M. Frampton, Katherine E. Hutchinson, and Juliann Chmielecki

Abstract

Supplementary Table S1A: Genes analyzed for base substitutions, short insertions/deletions, and copy number alterations (DNA). Supplementary Table S1B: Genes analyzed for rearrangements (DNA).

Published

2023

33. A Combination of Targeted Therapy with Chemotherapy Backbone Induces Response in a Treatment-Resistant Triple-Negative MCL1-Amplified Metastatic Breast Cancer Patient

Author

Siraj M. Ali, Jessica Watson, Kai Wang, Jon H. Chung, Caitlin McMahon, Jeffrey S. Ross, and Karel A. Dicke

Subjects

Everolimus, Triple-negative breast cancer, MCL1, BAP1, Sorafenib, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

After failure of anthracycline- and platinum-based therapy, no effective therapies exist for management of metastatic triple-negative breast cancer (TNBC). We report a case of metastatic TNBC harboring MCL1 amplification, as identified by comprehensive genomic profiling in the course of clinical care. MCL1 is an antiapoptotic gene in the BCL2 family, and MCL1 amplification is common in TNBC (at least 20%). A personalized dose-reduced regimen centered on a combination of sorafenib and vorinostat was implemented, based on preclinical evidence demonstrating treatment synergy in the setting of MCL1 amplification. Although hospice care was being considered before treatment initiation, the personalized regimen yielded 6 additional months of life for this patient. Further rigorous studies are needed to confirm that this regimen or derivatives thereof can benefit the MCL1-amplified subset of TNBC patients.

Published

2016

34. The Genomics of Colorectal Cancer in Populations with African and European Ancestry

Author

Parvathi A. Myer, Jessica K. Lee, Russell W. Madison, Kith Pradhan, Justin Y. Newberg, Carmen R. Isasi, Samuel J. Klempner, Garrett M. Frampton, Jeffery S. Ross, Jeffrey M. Venstrom, Alexa B. Schrock, Sudipto Das, Leonard Augenlicht, Amit Verma, John M. Greally, Srilakshmi M. Raj, Sanjay Goel, and Siraj M. Ali

Subjects

Proto-Oncogene Proteins p21(ras), Oncology, Class I Phosphatidylinositol 3-Kinases, Proto-Oncogene Proteins, Mutation, Humans, Microsatellite Instability, Genomics, Protein-Tyrosine Kinases, Colorectal Neoplasms, neoplasms

Abstract

Black people have a higher incidence of colorectal cancer and worse survival rates when compared with white people. Comprehensive genomic profiling was performed in 46,140 colorectal adenocarcinoma cases. Ancestry-informative markers identified 5,301 patients of African descent (AFR) and 33,770 patients of European descent (EUR). AFR were younger, had fewer microsatellite instability–high (MSI-H) tumors, and had significantly more frequent alterations in KRAS, APC, and PIK3CA. AFR had increased frequency of KRAS mutations, specifically KRASG12D and KRASG13. There were no differences in rates of actionable kinase driver alterations (HER2, MET, NTRK, ALK, ROS1, and RET). In patients with young-onset colorectal cancer ( Significance: KRAS (particularly KRASG12D/G13), APC, and PIK3CA were more frequently altered in AFR who had a lower frequency of MSI-H tumors. There were no differences in actionable kinase driver alterations. In young-onset colorectal cancer, both ancestries had a similar frequency of MSI-H/TMB-H tumors, but strikingly different trends in APC. See related commentary by Eng and Holowatyj, p. 1187. This article is highlighted in the In This Issue feature, p. 1171

Published

2022

35. Figure S1 from Optimized EGFR Blockade Strategies in EGFR Addicted Gastroesophageal Adenocarcinomas

Author

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

Abstract

Supplementary Figure 1

Published

2023

36. Supplemental methods from Profiling of 149 Salivary Duct Carcinomas, Carcinoma Ex Pleomorphic Adenomas, and Adenocarcinomas, Not Otherwise Specified Reveals Actionable Genomic Alterations

Author

Daniel W. Bowles, Jeffrey S. Ross, Hilary S. Serracino, Philip J. Stephens, Vincent A. Miller, Doron Lipson, Roman Yelensky, Juliann Chmielecki, Stuart J. Wong, Donna Washburn, Dwight S. Oldham, Carrie Marshall, Molly Murray, Siraj M. Ali, Timothy A. Jennings, Adrienne Johnson, Depinder Khaira, Julia A. Elvin, Jessica D. McDermott, Jeffery S. Russell, and Kai Wang

Abstract

Expanded methods for the study.

Published

2023

37. Supplemental figure legend from Profiling of 149 Salivary Duct Carcinomas, Carcinoma Ex Pleomorphic Adenomas, and Adenocarcinomas, Not Otherwise Specified Reveals Actionable Genomic Alterations

Author

Daniel W. Bowles, Jeffrey S. Ross, Hilary S. Serracino, Philip J. Stephens, Vincent A. Miller, Doron Lipson, Roman Yelensky, Juliann Chmielecki, Stuart J. Wong, Donna Washburn, Dwight S. Oldham, Carrie Marshall, Molly Murray, Siraj M. Ali, Timothy A. Jennings, Adrienne Johnson, Depinder Khaira, Julia A. Elvin, Jessica D. McDermott, Jeffery S. Russell, and Kai Wang

Abstract

This is the legend for the supplemental figure

Published

2023

38. Supplementary table 2 from Oncogenic ALK Fusion in Rare and Aggressive Subtype of Colorectal Adenocarcinoma as a Potential Therapeutic Target

Author

Howard Safran, Jeffrey S. Ross, Siraj M. Ali, Philip J. Stephens, Vincent A. Miller, James Sun, Kyle Gowen, Kai Wang, Anthony J. Gill, Kyoung-Mee Kim, Jeeyun Lee, Kara A. Lombardo, Cynthia L. Jackson, Michael Wheeler, Shamlal Mangray, Murray B. Resnick, and Evgeny Yakirevich

Abstract

ALK genomic alterations revealed by comprehensive genomic profiling in clinical cases of colorectal carcinoma

Published

2023

39. Table S1 from Optimized EGFR Blockade Strategies in EGFR Addicted Gastroesophageal Adenocarcinomas

Author

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

Abstract

Supplementary Table 1

Published

2023

40. Data from Optimized EGFR Blockade Strategies in EGFR Addicted Gastroesophageal Adenocarcinomas

Author

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

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

2023

41. Data from Individualized Molecular Analyses Guide Efforts (IMAGE): A Prospective Study of Molecular Profiling of Tissue and Blood in Metastatic Triple-Negative Breast Cancer

Author

Ben H. Park, Vered Stearns, Jane Zorzi, Zhe Zhang, Daniel J. Zabransky, Lauren E. Young, Antonio C. Wolff, Dustin A. VanDenBerg, Philip J. Stephens, Shannon Slater, Jeffrey S. Ross, Gary L. Rosner, Geoff A. Otto, Vincent A. Miller, Doron Lipson, Justin Lee, Josh Lauring, Mark R. Kennedy, Stacie C. Jeter, Christopher D. Gocke, Travis A. Clark, Sarah Croessmann, Rory L. Cochran, Roisin M. Connolly, David Chu, Jennifer Axilbund, Siraj M. Ali, Ashley Cimino-Mathews, Julia A. Beaver, and Heather A. Parsons

Abstract

Purpose: The clinical utility of next-generation sequencing (NGS) in breast cancer has not been demonstrated. We hypothesized that we could perform NGS of a new biopsy from patients with metastatic triple-negative breast cancer (TNBC) in a clinically actionable timeframe.Experimental Design: We planned to enroll 40 patients onto a prospective study, Individualized Molecular Analyses Guide Efforts (IMAGE), to evaluate the feasibility of obtaining a new biopsy of a metastatic site, perform NGS (FoundationOne), and convene a molecular tumor board to formulate treatment recommendations within 28 days. We collected blood at baseline and at time of restaging to assess cell-free circulating plasma tumor DNA (ptDNA).Results: We enrolled 26 women with metastatic TNBC who had received ≥1 line of prior chemotherapy, and 20 (77%) underwent NGS of a metastatic site biopsy. Twelve (60%) evaluable patients received treatment recommendations within 28 days of consent. The study closed after 20 patients underwent NGS, based on protocol-specified interim futility analysis. Three patients went on to receive genomically directed therapies. Twenty-four of 26 patients had genetic alterations successfully detected in ptDNA. Among 5 patients, 4 mutations found in tumor tissues were not identified in blood, and 4 mutations found in blood were not found in corresponding tumors. In 9 patients, NGS of follow-up blood samples showed 100% concordance with baseline blood samples.Conclusions: This study demonstrates challenges of performing NGS on prospective tissue biopsies in patients with metastatic TNBC within 28 days, while also highlighting the potential use of blood as a more time-efficient and less invasive method of mutational assessment. Clin Cancer Res; 23(2); 379–86. ©2016 AACR.

Published

2023

42. Supplemental table 1 from Profiling of 149 Salivary Duct Carcinomas, Carcinoma Ex Pleomorphic Adenomas, and Adenocarcinomas, Not Otherwise Specified Reveals Actionable Genomic Alterations

Author

Daniel W. Bowles, Jeffrey S. Ross, Hilary S. Serracino, Philip J. Stephens, Vincent A. Miller, Doron Lipson, Roman Yelensky, Juliann Chmielecki, Stuart J. Wong, Donna Washburn, Dwight S. Oldham, Carrie Marshall, Molly Murray, Siraj M. Ali, Timothy A. Jennings, Adrienne Johnson, Depinder Khaira, Julia A. Elvin, Jessica D. McDermott, Jeffery S. Russell, and Kai Wang

Abstract

Detailed genetic results

Published

2023

43. Supplemental figure 1 from Profiling of 149 Salivary Duct Carcinomas, Carcinoma Ex Pleomorphic Adenomas, and Adenocarcinomas, Not Otherwise Specified Reveals Actionable Genomic Alterations

Author

Daniel W. Bowles, Jeffrey S. Ross, Hilary S. Serracino, Philip J. Stephens, Vincent A. Miller, Doron Lipson, Roman Yelensky, Juliann Chmielecki, Stuart J. Wong, Donna Washburn, Dwight S. Oldham, Carrie Marshall, Molly Murray, Siraj M. Ali, Timothy A. Jennings, Adrienne Johnson, Depinder Khaira, Julia A. Elvin, Jessica D. McDermott, Jeffery S. Russell, and Kai Wang

Abstract

Photomicrographs of two ETV6-NTRK3 fusion cases.

Published

2023

44. Data from Oncogenic ALK Fusion in Rare and Aggressive Subtype of Colorectal Adenocarcinoma as a Potential Therapeutic Target

Author

Howard Safran, Jeffrey S. Ross, Siraj M. Ali, Philip J. Stephens, Vincent A. Miller, James Sun, Kyle Gowen, Kai Wang, Anthony J. Gill, Kyoung-Mee Kim, Jeeyun Lee, Kara A. Lombardo, Cynthia L. Jackson, Michael Wheeler, Shamlal Mangray, Murray B. Resnick, and Evgeny Yakirevich

Abstract

Purpose: Chromosomal translocations in the anaplastic lymphoma kinase (ALK) gene have been identified as oncogenic drivers in lung adenocarcinomas and other tumors, recently including rare cases of colorectal carcinoma. We identified a patient with refractory metastatic colorectal carcinoma harboring a STRN–ALK gene fusion who achieved an exceptional clinical benefit to the ALK inhibitor ceritinib. Our goal was to further define the clinicopathologic features of ALK-rearranged colorectal carcinoma in a large cohort.Experimental Design: Clinical cases of colorectal carcinoma evaluated by comprehensive genomic profiling (CGP) or by ALK immunohistochemistry (IHC) were reviewed retrospectively. FISH and microsatellite instability (MSI) analyses were performed.Results: Nine colorectal carcinoma cases harbored ALK gene fusions. Six cases were identified by CGP of 3,157 colorectal carcinoma (0.2%) and three by IHC of 2,980 colorectal carcinoma (0.1%). The ALK fusions involved known ALK partners EML4, C2orf44, CAD, and the novel STRN, PPP1R21, SENPF, MAPRE3, and PRKAP1B partners. These advanced-stage colorectal carcinomas lacked mutations in other oncogenic drivers, predominantly involved the proximal colon, and often exhibited MSI and mucinous phenotype. The index patient was treated with the ALK inhibitor ceritinib, resulting in a marked decrease in size of a skin metastasis, and resolution by computerized tomography of all contrast enhancing tumor. After 9 months of treatment, biopsy of progressive disease demonstrated a KRAS mutation, consistent with acquired resistance to ceritinib.Conclusions: Colorectal carcinoma harboring ALK fusions represent a rare aggressive subtype of colorectal carcinoma with distinct clinicopathologic features. This report provides the first clinical evidence that such patients may benefit from targeted monotherapy with ALK inhibitors. Clin Cancer Res; 22(15); 3831–40. ©2016 AACR.

Published

2023

45. Supplementary table 1 from Oncogenic ALK Fusion in Rare and Aggressive Subtype of Colorectal Adenocarcinoma as a Potential Therapeutic Target

Author

Howard Safran, Jeffrey S. Ross, Siraj M. Ali, Philip J. Stephens, Vincent A. Miller, James Sun, Kyle Gowen, Kai Wang, Anthony J. Gill, Kyoung-Mee Kim, Jeeyun Lee, Kara A. Lombardo, Cynthia L. Jackson, Michael Wheeler, Shamlal Mangray, Murray B. Resnick, and Evgeny Yakirevich

Abstract

Previously reported cases of colorectal carcinoma harboring ALK fusions

Published

2023

46. Supplemental Tables and Figures 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

Supplemental Figure 1. Distribution of EGFR extracellular domain (ECD) mutations in ctDNA samples from patients with CRC. Supplemental Figure 2. Response to crizotinib in a patient with small bowel adenocarcinoma and GOPC-ROS1 fusion. Supplemental Figure 3. Detection of copy number amplification is associated with increased ctDNA fraction. Supplemental Table 1. List of 62 genes sequenced in this study using the FoundationACT ctDNA assay. Supplemental Table 2. Genomic alterations detected in temporally matched ctDNA and tissue samples.

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2023

47. Figure S1, Figure S2, Table S1 from Anaplastic Lymphoma Kinase Mutation (ALK F1174C) in Small Cell Carcinoma of the Prostate and Molecular Response to Alectinib

Author

Sarki A. Abdulkadir, Francis J. Giles, Young K. Chae, Massimo Cristofanilli, Siraj M. Ali, Julia A. Elvin, Laurie Gay, Jeffrey S. Ross, Timothy M. Kuzel, Richard B. Lanman, Rebecca J. Nagy, Rubens B. Costa, Ximing J. Yang, HuiYing Han, Kenji Unno, Vinay Sagar, Ami N. Shah, Sahithi Pamarthy, and Benedito A. Carneiro

Abstract

Figure S1 ALK genomic alterations and mRNA expression in human cancers. Figure S2 Efficacy of ALK inhibitors in prostate cancer cell lines. Table S1 Summary of mutations and their percentages identified by ctDNA profiling.

Published

2023

48. Data from Anaplastic Lymphoma Kinase Mutation (ALK F1174C) in Small Cell Carcinoma of the Prostate and Molecular Response to Alectinib

Author

Sarki A. Abdulkadir, Francis J. Giles, Young K. Chae, Massimo Cristofanilli, Siraj M. Ali, Julia A. Elvin, Laurie Gay, Jeffrey S. Ross, Timothy M. Kuzel, Richard B. Lanman, Rebecca J. Nagy, Rubens B. Costa, Ximing J. Yang, HuiYing Han, Kenji Unno, Vinay Sagar, Ami N. Shah, Sahithi Pamarthy, and Benedito A. Carneiro

Abstract

Purpose: Small cell carcinoma of the prostate (SCCP) is an aggressive disease that can arise de novo or by transdifferentiation from prostate adenocarcinoma. Alterations in anaplastic lymphoma kinase (ALK) gene are involved in neuroblastoma, lung cancer, and other malignancies, but its role in SCCP has not been documented. We describe a patient with refractory de novo SCCP with ALK F1174C–activating mutation who obtained clinical benefit from treatment with ALK inhibitor.Experimental Design: Next-generation sequencing (NGS) was used to analyze primary and circulating tumor DNA (ctDNA). Prostate cancer databases were queried for alterations in ALK gene, mRNA, and its impact in clinical outcomes. In vitro prostate cell line/organoid models were generated by lentiviral-mediated expression of ALK and ALK F1174C and assessed for response to ALK inhibitors crizotinib and alectinib.Results: NGS analysis of the primary tumor and ctDNA of a 39-year-old patient with refractory SSCP identified ALK F1174C mutation. Treatment with second-generation ALK inhibitor alectinib resulted in radiographic stable disease for over 6 months, symptomatic improvement, and significant molecular response as reflected by declining ctDNA allele fraction. Analysis of prostate cancer datasets showed that ALK amplification was associated with poor outcome. In prostate cancer cells and organoids, ALK F1174C expression enhanced growth and induced expression of the neuroendocrine marker neuron-specific enolase. Alectinib was more effective than crizotinib in inhibiting ALK F1174C–expressing cell growth.Conclusions: These findings implicate ALK-activating mutations in SCCP pathogenesis and suggest the therapeutic potential of targeting ALK molecular alterations in some patients with SCCP. Clin Cancer Res; 24(12); 2732–9. ©2018 AACR.

Published

2023

49. Data from Profiling of 149 Salivary Duct Carcinomas, Carcinoma Ex Pleomorphic Adenomas, and Adenocarcinomas, Not Otherwise Specified Reveals Actionable Genomic Alterations

Author

Daniel W. Bowles, Jeffrey S. Ross, Hilary S. Serracino, Philip J. Stephens, Vincent A. Miller, Doron Lipson, Roman Yelensky, Juliann Chmielecki, Stuart J. Wong, Donna Washburn, Dwight S. Oldham, Carrie Marshall, Molly Murray, Siraj M. Ali, Timothy A. Jennings, Adrienne Johnson, Depinder Khaira, Julia A. Elvin, Jessica D. McDermott, Jeffery S. Russell, and Kai Wang

Abstract

Purpose: We sought to identify genomic alterations (GA) in salivary gland adenocarcinomas, not otherwise specified (NOS), salivary duct carcinomas (SDC), carcinoma ex pleomorphic adenoma (ca ex PA), and salivary carcinoma, NOS.Experimental Design: DNA was extracted from 149 tumors. Comprehensive genomic profiling (CGP) was performed on hybridization-captured adaptor ligation-based libraries of 182 or 315 cancer-related genes plus introns from 14 or 28 genes frequently rearranged for cancer and evaluated for all classes of GAs.Results: A total of 590 GAs were found in 157 unique genes (mean 3.9/tumor). GAs in the PI3K/AKT/mTOR pathway were more common in SDC (53.6%) than other histologies (P = 0.019) Cyclin-dependent kinase GAs varied among all histotypes: adenocarcinoma, NOS (34.6%); SDC (12.2%); ca ex PA (16.7%); carcinoma, NOS (31.2%; P = 0.043). RAS GAs were observed: adenocarcinoma, NOS (17.3%); SDC (26.8%); ca ex PA (4.2%); and carcinoma, NOS (9.4%; P = 0.054). ERBB2 GAs, including amplifications and mutations, were common: adenocarcinoma, NOS (13.5%); SDC (26.8%); ca ex PA (29.2%); carcinoma, NOS (18.8; P = 0.249). Other notable GAs include TP53 in >45% of each histotype; NOTCH1: adenocarcinoma, NOS (7.7%), ca ex PA (8.3%), carcinoma, NOS (21.6%); NF1: adenocarcinoma, NOS (9.6%), SDC (17.1%), carcinoma, NOS (18.8%). RET fusions were identified in one adenocarcinoma, NOS (CCDC6-RET) and two SDCs (NCOA4-RET). Clinical responses were observed in patients treated with anti-HER2 and anti-RET–targeted therapies.Conclusions: CGP of salivary adenocarcinoma, NOS, SDCs, ca ex PA, and carcinoma, NOS revealed diverse GAs that may lead to novel treatment options. Clin Cancer Res; 22(24); 6061–8. ©2016 AACR.

Published

2023

50. 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