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2. Personalized matched targeted therapy in advanced pancreatic cancer: a pilot cohort analysis

Author

Shaya, Justin, Kato, Shumei, Adashek, Jacob J, Patel, Hitendra, Fanta, Paul T, Botta, Gregory P, Sicklick, Jason K, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Cancer, Rare Diseases, Digestive Diseases, Pancreatic Cancer, Clinical Research, Good Health and Well Being, Genetics, Medical biotechnology
Abstract

Despite progress, 2-year pancreatic cancer survival remains dismal. We evaluated a biomarker-driven, combination/N-of-one strategy in 18 patients (advanced/metastatic pancreatic cancer) (from Molecular Tumor Board). Targeted agents administered/patient = 2.5 (median) (range, 1-4); first-line therapy (N = 5); second line, (N = 13). Comparing patients (high versus low degrees of matching) (matching score ≥50% versus

Published
2023

3. Co-Localization of Gastrointestinal Stromal Tumors (GIST) and Peritoneal Mesothelioma: A Case Series

Author

Courelli, Asimina S, Sharma, Ashwyn K, Madlensky, Lisa, Choi, Yoon Young, Li, Sam, Sarno, Shirley, Kelly, Kaitlyn, Mehtsun, Winta, Horgan, Santiago, Harismendy, Olivier, Baumgartner, Joel M, and Sicklick, Jason K

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Clinical Research, Rare Diseases, Digestive Diseases, Cancer, Aged, Female, Gastrointestinal Neoplasms, Gastrointestinal Stromal Tumors, Humans, Male, Mesothelioma, Mesothelioma, Malignant, Middle Aged, Mutation, Peritoneal Neoplasms, Proto-Oncogene Proteins c-kit, Receptor, Platelet-Derived Growth Factor alpha, Retrospective Studies, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

PurposeGastrointestinal stromal tumor (GIST) is associated with increased risk of additional cancers. In this study, synchronous GIST, and peritoneal mesothelioma (PM) were characterized to evaluate the relationship between these two cancers.MethodsA retrospective chart review was conducted for patients diagnosed with both GIST and PM between July 2010 and June 2021. Patient demographics, past tumor history, intraoperative reports, cross-sectional imaging, peritoneal cancer index (PCI) scoring, somatic next-generation sequencing (NGS) analysis, and histology were reviewed.ResultsOf 137 patients who underwent primary GIST resection from July 2010 to June 2021, 8 (5.8%) were found to have synchronous PM, and 4 patients (50%) had additional cancers and/or benign tumors. Five (62.5%) were male, and the median age at GIST diagnosis was 57 years (range: 45-76). Seventy-five percent of GISTs originated from the stomach. Of the eight patients, one patient had synchronous malignant mesothelioma (MM), and the remaining had well-differentiated papillary mesothelioma (WDPM), which were primarily located in the region of the primary GIST (89%). The median PCI score was 2 in the WDPM patients. NGS of GIST revealed oncogenic KIT exon 11 (62.5%), PDGFRA D842V (25%), or SDH (12.5%) mutations, while NGS of the MM revealed BAP1 and PBRM1 alterations.ConclusionsOne in 17 GIST patients undergoing resection in this series have PM, which is significantly higher than expected if these two diseases were considered as independent events. Our results indicate that synchronous co-occurrence of GIST and PM is an underrecognized finding, suggesting a possible relationship that deserves further investigation.

Published
2022

5. Soft Tissue Sarcoma, Version 2.2022, NCCN Clinical Practice Guidelines in Oncology.

Author

von Mehren, Margaret, Kane, John M, Agulnik, Mark, Bui, Marilyn M, Carr-Ascher, Janai, Choy, Edwin, Connelly, Mary, Dry, Sarah, Ganjoo, Kristen N, Gonzalez, Ricardo J, Holder, Ashley, Homsi, Jade, Keedy, Vicki, Kelly, Ciara M, Kim, Edward, Liebner, David, McCarter, Martin, McGarry, Sean V, Mesko, Nathan W, Meyer, Christian, Pappo, Alberto S, Parkes, Amanda M, Petersen, Ivy A, Pollack, Seth M, Poppe, Matthew, Riedel, Richard F, Schuetze, Scott, Shabason, Jacob, Sicklick, Jason K, Spraker, Matthew B, Zimel, Melissa, Hang, Lisa E, Sundar, Hema, and Bergman, Mary Anne

Subjects
Biomedical and Clinical Sciences, Health Sciences, Clinical Sciences, Oncology and Carcinogenesis, Orphan Drug, Clinical Trials and Supportive Activities, Pediatric Cancer, Rare Diseases, Cancer, Clinical Research, Pediatric, Extremities, Humans, Medical Oncology, Sarcoma, Soft Tissue Neoplasms, Oncology & Carcinogenesis, Oncology and carcinogenesis, Health services and systems
Abstract

Soft tissue sarcomas (STS) are rare malignancies of mesenchymal cell origin that display a heterogenous mix of clinical and pathologic characteristics. STS can develop from fat, muscle, nerves, blood vessels, and other connective tissues. The evaluation and treatment of patients with STS requires a multidisciplinary team with demonstrated expertise in the management of these tumors. The complete NCCN Clinical Practice Guidelines in Oncology (NCCN Guidelines) for Soft Tissue Sarcoma provide recommendations for the diagnosis, evaluation, and treatment of extremity/superficial trunk/head and neck STS, as well as retroperitoneal/intra-abdominal STS, desmoid tumors, and rhabdomyosarcoma. This portion of the NCCN Guidelines discusses general principles for the diagnosis and treatment of retroperitoneal/intra-abdominal STS, outlines treatment recommendations, and reviews the evidence to support the guidelines recommendations.

Published
2022

10. Establishment of Patient-derived Succinate Dehydrogenase-deficient Gastrointestinal Stromal Tumor Models For Predicting Therapeutic Response

Author

Yebra, Mayra, Bhargava, Shruti, Kumar, Avi, Burgoyne, Adam M, Tang, Chih-Min, Yoon, Hyunho, Banerjee, Sudeep, Aguilera, Joseph, Cordes, Thekla, Sheth, Vipul, Noh, Sangkyu, Ustoy, Rowan, Li, Sam, Advani, Sunil J, Corless, Christopher L, Heinrich, Michael C, Kurzrock, Razelle, Lippman, Scott M, Fanta, Paul T, Harismendy, Olivier, Metallo, Christian, and Sicklick, Jason K

Subjects
Orphan Drug, Clinical Research, Rare Diseases, Cancer, Digestive Diseases, Good Health and Well Being, Adolescent, Gastrointestinal Neoplasms, Gastrointestinal Stromal Tumors, Humans, Mutation, Proto-Oncogene Proteins c-kit, Receptor, Platelet-Derived Growth Factor alpha, Succinate Dehydrogenase, Young Adult, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeGastrointestinal stromal tumor (GIST) is the most common sarcoma of the gastrointestinal tract, with mutant succinate dehydrogenase (SDH) subunits (A-D) comprising less than 7.5% (i.e., 150-200/year) of new cases annually in the United States. Contrary to GISTs harboring KIT or PDGFRA mutations, SDH-mutant GISTs affect adolescents/young adults, often metastasize, and are frequently resistant to tyrosine kinase inhibitors (TKI). Lack of human models for any SDH-mutant tumors, including GIST, has limited molecular characterization and drug discovery.Experimental designWe describe methods for establishing novel patient-derived SDH-mutant (mSDH) GIST models and interrogated the efficacy of temozolomide on these tumor models in vitro and in clinical trials of patients with mSDH GIST.ResultsMolecular and metabolic characterization of our patient-derived mSDH GIST models revealed that these models recapitulate the transcriptional and metabolic hallmarks of parent tumors and SDH deficiency. We further demonstrate that temozolomide elicits DNA damage and apoptosis in our mSDH GIST models. Translating our in vitro discovery to the clinic, a cohort of patients with SDH-mutant GIST treated with temozolomide (n = 5) demonstrated a 40% objective response rate and 100% disease control rate, suggesting that temozolomide represents a promising therapy for this subset of GIST.ConclusionsWe report the first methods to establish patient-derived mSDH tumor models, which can be readily employed for understanding patient-specific tumor biology and treatment strategies. We also demonstrate that temozolomide is effective in patients with mSDH GIST who are refractory to existing chemotherapeutic drugs (namely, TKIs) in clinic for GISTs, bringing a promising treatment option for these patients to clinic.See related commentary by Blakely et al., p. 3.

Published
2022

11. Location of Gastrointestinal Stromal Tumor (GIST) in the Stomach Predicts Tumor Mutation Profile and Drug Sensitivity

Author

Sharma, Ashwyn K, de la Torre, Jorge, IJzerman, Nikki S, Sutton, Thomas L, Zhao, Beiqun, Khan, Tahsin M, Banerjee, Sudeep, Cui, Christina, Nguyen, Vi, Alkhuziem, Maha, Snaebjornsson, Petur, van Boven, Hester, Bruining, Annemarie, Tang, Chih-Min, Yoon, Hyunho, De la Fuente, Alexa, Kato, Shumei, Patel, Hitendra, Heinrich, Michael C, Corless, Christopher L, Horgan, Santiago, Burgoyne, Adam M, Fanta, Paul, Mesirov, Jill P, Blakely, Andrew M, Davis, Jeremy L, Mayo, Skye C, van Houdt, Winan J, Steeghs, Neeltje, and Sicklick, Jason K

Subjects
Digestive Diseases, Cancer, Genetics, Rare Diseases, Clinical Research, Gastrointestinal Stromal Tumors, Humans, Mutation, Prognosis, Proto-Oncogene Proteins c-kit, Receptor, Platelet-Derived Growth Factor alpha, Stomach, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeGastrointestinal stromal tumors (GIST) commonly arise in different regions of the stomach and are driven by various mutations (most often in KIT, PDGFRA, and SDHx). We hypothesized that the anatomic location of gastric GIST is associated with unique genomic profiles and distinct driver mutations.Experimental designWe compared KIT versus non-KIT status with tumor location within the National Cancer Database (NCDB) for 2,418 patients with primary gastric GIST. Additionally, we compiled an international cohort (TransAtlantic GIST Collaborative, TAGC) of 236 patients and reviewed sequencing results, cross-sectional imaging, and operative reports. Subgroup analyses were performed for tumors located proximally versus distally. Risk factors for KIT versus non-KIT tumors were identified using multivariate regression analysis. A random forest machine learning model was then developed to determine feature importance.ResultsWithin the NCDB cohort, non-KIT mutants dominated distal tumor locations (P < 0.03). Proximal GIST were almost exclusively KIT mutant (96%) in the TAGC cohort, whereas 100% of PDGFRA and SDH-mutant GIST occurred in the distal stomach. On multivariate regression analysis, tumor location was associated with KIT versus non-KIT mutations. Using random forest machine learning analysis, stomach location was the most important feature for predicting mutation status.ConclusionsWe provide the first evidence that the mutational landscape of gastric GIST is related to tumor location. Proximal gastric GIST are overwhelmingly KIT mutant, irrespective of morphology or age, whereas distal tumors display non-KIT genomic diversity. Anatomic location of gastric GIST may therefore provide immediate guidance for clinical treatment decisions and selective confirmatory genomic testing when resources are limited.

Published
2021

13. High prevalence of clonal hematopoiesis‐type genomic abnormalities in cell‐free DNA in invasive gliomas after treatment

Author

Okamura, Ryosuke, Piccioni, David E, Boichard, Amélie, Lee, Suzanna, Jimenez, Rebecca E, Sicklick, Jason K, Kato, Shumei, and Kurzrock, Razelle

Subjects
Human Genome, Brain Cancer, Brain Disorders, Rare Diseases, Cancer, Neurosciences, Genetics, Adult, Aged, Aged, 80 and over, Brain Neoplasms, Cell-Free Nucleic Acids, Chemoradiotherapy, Clonal Hematopoiesis, DNA, Neoplasm, Glioma, High-Throughput Nucleotide Sequencing, Humans, Male, Middle Aged, Mutation, Prognosis, Sequence Analysis, DNA, Survival Analysis, Temozolomide, Treatment Outcome, Young Adult, cell&#8208, free DNA, CH, clonal hematopoiesis, glioblastoma multiforme, glioma, liquid biopsy, molecular profiling, cell-free DNA, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Plasma cell-free DNA (cfDNA) is emerging as an important diagnostic tool in cancer. However, cfDNA alterations may differ from those in tissue and sometimes may reflect processes unrelated to the cancer, including clonal hematopoiesis (CH). We examined plasma cfDNA, tested by next-generation sequencing (NGS), for characterized alterations (excluding variants of unknown significance) in 135 patients with invasive glioma. Overall, 21% (28/135) had ≥1 alteration; 17% (23/135) had CH-type cfDNA mutations. Temozolomide (a mutagenic alkylating agent) with concurrent radiation therapy prior to blood draw was significantly associated with an increase in CH-type mutations, even after age, race/ethnicity, and WHO-grade were considered as confounders (odds ratio [95% confidence interval, CI] 8.98 [1.13-71.46]; P = .04; multivariable analysis). Further, of 18 patients with invasive glioma who had both cfDNA and tissue DNA NGS and had ≥1 cfDNA alteration, 16 (89%) had ≥1 cfDNA alteration not found in their tissue DNA, including CH-type alterations in genes such as TP53 (most common), ATM, GNAS, and JAK2. Altogether, 87% of cfDNA alterations (20/23) observed in the 18 patients were implicated in CH. Finally, examining all 135 patients, CH-type cfDNA mutations were an independent prognostic factor for shorter survival (hazard ratio [95% CI] 3.28 [1.28-8.40]; P = .01). These findings emphasize that not all characterized cfDNA alterations detected in patients with solid tumors are cancer-related. Importantly, in patients with invasive gliomas who have had prior temozolomide and radiation, CH-related alterations in cfDNA are frequent and correlate with poor outcomes.

Published
2021

14. Development of a Soluble KIT Electrochemical Aptasensor for Cancer Theranostics

Author

Chung, Saeromi, Sicklick, Jason K, Ray, Partha, and Hall, Drew A

Subjects
Cancer, Aptamers, Nucleotide, Biosensing Techniques, Electrochemical Techniques, Humans, Neoplasms, Precision Medicine, KIT, aptamer, electrochemical sensor, cancer, square-wave voltammetry, aptasensor, theranostics, Analytical Chemistry, Biomedical Engineering, Nanotechnology
Abstract

An electrochemical sensor based on a conformation-changing aptamer is reported to detect soluble KIT, a cancer biomarker, in human serum. The sensor was fabricated with a ferrocene-labeled aptamer (Kd < 5 nM) conjugated to a gold electrode. Quantitative KIT detection was achieved using electrochemical impedance spectroscopy (EIS) and square-wave voltammetry (SWV). EIS was used to optimize experimental parameters such as the aptamer-to-spacer ratio, aptamer immobilization time, pH, and KIT incubation time, and the sensor surface was characterized using voltammetry. The assay specificity was demonstrated using interfering species and exhibited high specificity toward the target protein. The aptasensor showed a wide dynamic range, 10 pg/mL-100 ng/mL in buffer, with a 1.15 pg/mL limit of detection. The sensor also has a linear response to KIT spiked in human serum and successfully detected KIT in cancer-cell-conditioned media. The proposed aptasensor has applications as a continuous or intermittent approach for cancer therapy monitoring and diagnostics (theranostics).

Published
2021

15. Cancer-associated fibroblast secretion of PDGFC promotes gastrointestinal stromal tumor growth and metastasis

Author

Yoon, Hyunho, Tang, Chih-Min, Banerjee, Sudeep, Yebra, Mayra, Noh, Sangkyu, Burgoyne, Adam M, Torre, Jorge De la, Siena, Martina De, Liu, Mengyuan, Klug, Lillian R, Choi, Yoon Young, Hosseini, Mojgan, Delgado, Antonio L, Wang, Zhiyong, French, Randall P, Lowy, Andrew, DeMatteo, Ronald P, Heinrich, Michael C, Molinolo, Alfredo A, Gutkind, J Silvio, Harismendy, Olivier, and Sicklick, Jason K

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Digestive Diseases, Cancer, Rare Diseases, Aetiology, 2.1 Biological and endogenous factors, Cancer-Associated Fibroblasts, Cell Line, Tumor, Epithelial-Mesenchymal Transition, Gastrointestinal Stromal Tumors, Humans, Lymphokines, Neoplasm Metastasis, Paracrine Communication, Phosphatidylinositol 3-Kinases, Platelet-Derived Growth Factor, Protein Kinase Inhibitors, Receptor, Platelet-Derived Growth Factor alpha, Signal Transduction, Snail Family Transcription Factors, TOR Serine-Threonine Kinases, Tumor Microenvironment, Clinical Sciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

Targeted therapies for gastrointestinal stromal tumor (GIST) are modestly effective, but GIST cannot be cured with single agent tyrosine kinase inhibitors. In this study, we sought to identify new therapeutic targets in GIST by investigating the tumor microenvironment. Here, we identified a paracrine signaling network by which cancer-associated fibroblasts (CAFs) drive GIST growth and metastasis. Specifically, CAFs isolated from human tumors were found to produce high levels of platelet-derived growth factor C (PDGFC), which activated PDGFC-PDGFRA signal transduction in GIST cells that regulated the expression of SLUG, an epithelial-mesenchymal transition (EMT) transcription factor and downstream target of PDGFRA signaling. Together, this paracrine induce signal transduction cascade promoted tumor growth and metastasis in vivo. Moreover, in metastatic GIST patients, SLUG expression positively correlated with tumor size and mitotic index. Given that CAF paracrine signaling modulated GIST biology, we directly targeted CAFs with a dual PI3K/mTOR inhibitor, which synergized with imatinib to increase tumor cell killing and in vivo disease response. Taken together, we identified a previously unappreciated cellular target for GIST therapy in order to improve disease control and cure rates.

Published
2021

16. Transforming the Future of Surgeon-Scientists

Author

Ladner, Daniela P., Goldstein, Allan M., Billiar, Timothy R., Cameron, Andrew M., Carpizo, Darren R., Chu, Daniel I., Coopersmith, Craig M., DeMatteo, Ronald P., Feng, Sandy, Gallagher, Katherine A., Gillanders, William E., Lal, Brajesh K., Lipshutz, Gerald S., Liu, Annie, Maier, Ronald V., Mittendorf, Elizabeth A., Morris, Arden M., Sicklick, Jason K., Velazquez, Omaida C., Whitson, Bryan A., Wilke, Lee G., Yoon, Sam S., Zeiger, Martha A., Farmer, Diana L., and Hwang, E. Shelley

Published
2024
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18. Comprehensive genomic landscape and precision therapeutic approach in biliary tract cancers

Author

Okamura, Ryosuke, Kurzrock, Razelle, Mallory, Robert J, Fanta, Paul T, Burgoyne, Adam M, Clary, Bryan M, Kato, Shumei, and Sicklick, Jason K

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Human Genome, Clinical Research, Digestive Diseases, Biotechnology, Cancer, Genetics, Good Health and Well Being, Adult, Aged, Aged, 80 and over, Antineoplastic Agents, Biliary Tract Neoplasms, Circulating Tumor DNA, Class I Phosphatidylinositol 3-Kinases, Cyclin-Dependent Kinase Inhibitor p15, Cyclin-Dependent Kinase Inhibitor p16, DNA, Neoplasm, Feasibility Studies, Female, High-Throughput Nucleotide Sequencing, Humans, Male, Middle Aged, Precision Medicine, Proto-Oncogene Proteins p21(ras), Sequence Analysis, DNA, Survival Analysis, Treatment Outcome, Tumor Suppressor Protein p53, biliary tract cancers, biomarker, cholangiocarcinoma, circulating tumor DNA, liquid biopsy, molecular profiling, personalized cancer therapy, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

Biliary tract cancers have dismal prognoses even when cytotoxic chemotherapy is administered. There is an unmet need to develop precision treatment approaches using comprehensive genomic profiling. A total of 121 patients with biliary tract cancers were analyzed for circulating-tumor DNA (ctDNA) and/or tissue-based tumor DNA (tissue-DNA) using clinical-grade next-generation sequencing: 71 patients (59%) had ctDNA; 90 (74%), tissue-DNA; and 40 (33%), both. Efficacy of targeted therapeutic approaches was assessed based upon ctDNA and tissue-DNA. At least one characterized alteration was detected in 76% of patients (54/71) for ctDNA [median, 2 (range, 0-9)] and 100% (90/90) for tissue-DNA [median, 4 (range, 1-9)]. Most common alterations occurred in TP53 (38%), KRAS (28%), and PIK3CA (14%) for ctDNA vs TP53 (44%), CDKN2A/B (33%) and KRAS (29%) for tissue-DNA. In 40 patients who had both ctDNA and tissue-DNA sequencing, overall concordance was higher between ctDNA and metastatic site tissue-DNA than between ctDNA and primary tumor DNA (78% vs 65% for TP53, 100% vs 74% for KRAS and 100% vs 87% for PIK3CA [But not statistical significance]). Among 80 patients who received systemic treatment, the molecularly matched therapeutic regimens based on genomic profiling showed a significantly longer progression-free survival (hazard ratio [95%confidence interval], 0.60 [0.37-0.99]. P = .047 [multivariate]) and higher disease control rate (61% vs 35%, P = .04) than unmatched regimens. Evaluation of ctDNA and tissue-DNA is feasible in biliary tract cancers.

Published
2021

19. Targeting G1/S phase cell-cycle genomic alterations and accompanying co-alterations with individualized CDK4/6 inhibitor–based regimens

Author

Kato, Shumei, Okamura, Ryosuke, Adashek, Jacob J, Khalid, Noor, Lee, Suzanna, Nguyen, Van, Sicklick, Jason K, and Kurzrock, Razelle

Subjects
Human Genome, Clinical Trials and Supportive Activities, Cancer, Clinical Research, Genetics, Breast Cancer, Development of treatments and therapeutic interventions, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, 5.1 Pharmaceuticals, Good Health and Well Being, Adult, Aged, Aged, 80 and over, Cyclin D, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, Cyclin-Dependent Kinase Inhibitor p15, Cyclin-Dependent Kinase Inhibitor p16, Female, G1 Phase Cell Cycle Checkpoints, Genes, p16, Humans, MAP Kinase Signaling System, Male, Middle Aged, Neoplasms, Phosphatidylinositol 3-Kinases, Progression-Free Survival, Protein Kinase Inhibitors, Young Adult, Cell cycle, Molecular biology, Oncology
Abstract

BACKGROUNDAlthough CDK4/6 inhibitors are an established treatment for hormone receptor-positive, HER2-negative metastatic breast cancers, their benefit in other malignancies remains limited.METHODSWe investigated factors associated with clinical outcomes from CDK4/6 inhibitor-based therapy among patients with G1/S phase cell-cycle alterations (CDK4/6 amplifications, CCND1/2/3 amplifications, or CDKN2A/B alterations).RESULTSOverall, 2457 patients with diverse solid tumors that underwent clinical-grade, next-generation sequencing (182-465 genes) and therapy outcome of (non-breast cancer) patients treated with matched CDK4/6 inhibitors were analyzed. G1/S phase cell-cycle alterations occurred in 20.6% (507 of 2457) of patients; 99% of those patients (n = 501) harbored ≥1 characterized co-alteration (median, 4; range, 0-24). In 40 patients with G1/S phase cell-cycle alterations given CDK4/6 inhibitors as part of their regimen, significantly longer median progression-free survival (PFS) was observed when CDK4/6 inhibitor-based therapies matched a larger proportion of tumor alterations, often because CDK4/6 inhibitors were administered together with other drugs that were matched to genomic co-alterations, hence achieving a high matching score (high vs. low [≥50% vs.

Published
2021

21. Attrition of Patients on a Precision Oncology Trial: Analysis of the I-PREDICT Experience.

Author

Bohan, Sandy S, Sicklick, Jason K, Kato, Shumei, Okamura, Ryosuke, Miller, Vincent A, Leyland-Jones, Brian, Lippman, Scott M, and Kurzrock, Razelle

Subjects
Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

BackgroundPrecision oncology uses molecular profiling of tumors to identify biomarker-tailored therapies for patients in the hope of improving outcomes. Typically, only a minority of patients receives evaluable matched treatment. This study explored the reasons for attrition on a precision medicine trial.Materials and methodsStudy participants were 190 adult patients who consented to the I-PREDICT (Investigation of molecular Profile-Related Evidence Determining Individualized Cancer Therapy) trial. Patients had metastatic and/or unresectable incurable malignancies. Patients who were not evaluable were analyzed.ResultsOf consented patients, 44% were not evaluable. Men were twice as likely to be not evaluable as women. Prominently, 45% of patients who were not evaluable dropped off because of death, hospice referral, or decline in organ function.ConclusionHealth deterioration of consented patients is a significant barrier to being evaluable on the I-PREDICT trial. These data suggest that patients are enrolled on precision oncology trials too late in their disease course or with excessive disease burden.

Published
2020

22. Real-world data from a molecular tumor board demonstrates improved outcomes with a precision N-of-One strategy.

Author

Kato, Shumei, Kim, Ki Hwan, Lim, Hyo Jeong, Boichard, Amelie, Nikanjam, Mina, Weihe, Elizabeth, Kuo, Dennis J, Eskander, Ramez N, Goodman, Aaron, Galanina, Natalie, Fanta, Paul T, Schwab, Richard B, Shatsky, Rebecca, Plaxe, Steven C, Sharabi, Andrew, Stites, Edward, Adashek, Jacob J, Okamura, Ryosuke, Lee, Suzanna, Lippman, Scott M, Sicklick, Jason K, and Kurzrock, Razelle

Subjects
Humans, Neoplasms, Antineoplastic Agents, Disease-Free Survival, Treatment Outcome, Genome, Human, Adolescent, Adult, Aged, Aged, 80 and over, Middle Aged, Child, Child, Preschool, Female, Male, Young Adult, Precision Medicine, Circulating Tumor DNA, Genome, Human, and over, Preschool
Abstract

Next-generation sequencing (NGS) can identify novel cancer targets. However, interpreting the molecular findings and accessing drugs/clinical trials is challenging. Furthermore, many tumors show resistance to monotherapies. To implement a precision strategy, we initiated a multidisciplinary (basic/translational/clinical investigators, bioinformaticians, geneticists, and physicians from multiple specialties) molecular tumor board (MTB), which included a project manager to facilitate obtaining clinical-grade biomarkers (blood/tissue NGS, specific immunohistochemistry/RNA expression including for immune-biomarkers, per physician discretion) and medication-acquisition specialists/clinical trial coordinators/navigators to assist with medication access. The MTB comprehensively reviewed patient characteristics to develop N-of-One treatments implemented by the treating physician's direction under the auspices of a master protocol. Overall, 265/429 therapy-evaluable patients (62%) were matched to ≥1 recommended drug. Eighty-six patients (20%) matched to all drugs recommended by MTB, including combinatorial approaches, while 38% received physician's choice regimen, generally with unmatched approach/low degree of matching. Our results show that patients who receive MTB-recommended regimens (versus physician choice) have significantly longer progression-free (PFS) and overall survival (OS), and are better matched to therapy. High (≥50%) versus low (

Published
2020

23. Synchronous metastatic colon cancer and the importance of primary tumor laterality - A National Cancer Database analysis of right- versus left-sided colon cancer.

Author

Zhao, Beiqun, Lopez, Nicole E, Eisenstein, Samuel, Schnickel, Gabriel T, Sicklick, Jason K, Ramamoorthy, Sonia L, and Clary, Bryan M

Subjects
Humans, Colonic Neoplasms, Neoplasm Metastasis, Retrospective Studies, Databases, Factual, Aged, Middle Aged, Female, Male, Colon cancer, Laterality, Metastatic, NCDB, Outcomes, Cancer, Digestive Diseases, Colo-Rectal Cancer, Clinical Sciences, Surgery
Abstract

BackgroundThe role of laterality for patients with synchronous metastatic colon cancer (SMCC) is not well-defined.MethodsUsing the National Cancer Database (2010-2015), we compared patients with metastatic right- (RCC) versus left-sided colon cancer (LCC). We performed Kaplan-Meier analysis to compare overall survival (OS) for each metastatic site and utilized adjusted Cox proportional hazard analysis to identify predictors of OS.ResultsPatients with RCCs were more likely to be older, female, and have more comorbidities. LCCs were more likely to metastasize to liver and lung, whereas RCCs were more likely to metastasize to peritoneum and brain. There was equal likelihood to metastasize to bone. OS was significantly longer for LCCs for all metastatic sites. After controlling for multiple variables, RCC (HR 1.426, p

Published
2020

24. Precision oncology: the intention-to-treat analysis fallacy

Author

Sicklick, Jason K, Kato, Shumei, Okamura, Ryosuke, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Clinical Trials and Supportive Activities, Clinical Research, Cancer, 6.1 Pharmaceuticals, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Evaluation of treatments and therapeutic interventions, Good Health and Well Being, Bias, False Positive Reactions, Humans, Intention to Treat Analysis, Medical Oncology, Molecular Targeted Therapy, Neoplasms, Precision Medicine, Protein Kinase Inhibitors, Randomized Controlled Trials as Topic, Research Design, Treatment Outcome, Precision oncology, Intention-to-treat, Public Health and Health Services, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

It has recently been suggested that precision oncology studies should be reanalysed using the intention-to-treat (ITT) methodology developed for randomized controlled clinical trials. This reanalysis dramatically decreases response rates in precision medicine studies. We contend that the ITT analysis of precision oncology trials is invalid. The ITT methodology was developed three decades ago to mitigate the problems of randomized trials, which try to ensure that both arms have an unselected patient population free from confounders. In contrast, precision oncology trials specifically select patients for confounders (that is biomarkers) that predict response. To demonstrate the issues inherent in an ITT reanalysis for precision cancer medicine studies, we take as an example the drug larotrectinib (TRK inhibitor) approved because of remarkable responses in malignancies harbouring NTRK fusions. Based on large-scale studies, NTRK fusions are found in ~0.31% of tumours. In a non-randomized pivotal study of larotrectinib, 75% of the 55 treated patients responded. Based upon the prevalence of NTRK fusions, ~18,000 patients would need to be screened to enrol the 55 treated patients. Utilizing the ITT methodology, the revised response rate to larotrectinib would be 0.23%. This is, of course, a dramatic underestimation of the efficacy of this now Food and Drug Administration (FDA)-approved drug. Similar issues can be shown for virtually any biomarker-based precision clinical trial. Therefore, retrofitting the ITT analysis developed for unselected patient populations in randomized trials yields misleading conclusions in precision medicine studies.

Published
2020

25. Prognostic implications of RAS alterations in diverse malignancies and impact of targeted therapies

Author

Kato, Shumei, Okamura, Ryosuke, Sicklick, Jason K, Daniels, Gregory A, Hong, David S, Goodman, Aaron, Weihe, Elizabeth, Lee, Suzanna, Khalid, Noor, Collier, Rachel, Mareboina, Manvita, Riviere, Paul, Whitchurch, Theresa J, Fanta, Paul T, Lippman, Scott M, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Health Disparities, Precision Medicine, Genetics, Rare Diseases, Cancer, Aetiology, 2.1 Biological and endogenous factors, Aged, Aged, 80 and over, Antineoplastic Combined Chemotherapy Protocols, California, Female, Humans, MAP Kinase Signaling System, Male, Middle Aged, Mitogen-Activated Protein Kinase Kinases, Molecular Targeted Therapy, Mutation, Neoplasms, Observational Studies as Topic, Prognosis, Progression-Free Survival, Protein Kinase Inhibitors, ras Proteins, RAS, next-generation sequencing, targeted therapy, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

RAS alterations are often found in difficult-to-treat malignancies and are considered "undruggable." To better understand the clinical correlates and coaltered genes of RAS alterations, we used targeted next-generation sequencing (NGS) to analyze 1,937 patients with diverse cancers. Overall, 20.9% of cancers (405/1,937) harbored RAS alterations. Most RAS-altered cases had genomic coalterations (95.3%, median: 3, range: 0-51), often involving genes implicated in oncogenic signals: PI3K pathway (31.4% of 405 cases), cell cycle (31.1%), tyrosine kinase families (21.5%) and MAPK signaling (18.3%). Patients with RAS-altered versus wild-type RAS malignancies had significantly worse overall survival (OS; p = 0.02 [multivariate]), with KRAS alterations, in particular, showing shorter survival. Moreover, coalterations in both RAS and PI3K signaling or cell-cycle-associated genes correlated with worse OS (p = 0.004 and p

Published
2020

26. Anti-KIT DNA Aptamer for Targeted Labeling of Gastrointestinal Stromal Tumor

Author

Banerjee, Sudeep, Yoon, Hyunho, Yebra, Mayra, Tang, Chih-Min, Gilardi, Mara, Narayanan, Jayanth S Shankara, White, Rebekah R, Sicklick, Jason K, and Ray, Partha

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Cancer, Biotechnology, Digestive Diseases, Rare Diseases, Animals, Antibodies, Monoclonal, Apoptosis, Aptamers, Nucleotide, Cell Proliferation, Female, Gastrointestinal Neoplasms, Gastrointestinal Stromal Tumors, Humans, Mice, Mice, Nude, Proto-Oncogene Proteins c-kit, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Pharmacology and Pharmaceutical Sciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

Gastrointestinal stromal tumor (GIST), the most common sarcoma, is characterized by KIT protein overexpression, and tumors are frequently driven by oncogenic KIT mutations. Targeted inhibition of KIT revolutionized GIST therapy and ushered in the era of precision medicine for the treatment of solid malignancies. Here, we present the first use of a KIT-specific DNA aptamer for targeted labeling of GIST. We found that an anti-KIT DNA aptamer bound cells in a KIT-dependent manner and was highly specific for GIST cell labeling in vitro Functionally, the KIT aptamer bound extracellular KIT in a manner similar to KIT mAb staining, and was trafficked intracellularly in vitro The KIT aptamer bound dissociated primary human GIST cells in a mutation agnostic manner such that tumors with KIT and PDGFRA mutations were labeled. In addition, the KIT aptamer specifically labeled intact human GIST tissue ex vivo, as well as peritoneal xenografts in mice with high sensitivity. These results represent the first use of an aptamer-based method for targeted detection of GIST in vitro and in vivo.

Published
2020

27. ARID1A alterations function as a biomarker for longer progression-free survival after anti-PD-1/PD-L1 immunotherapy

Author

Okamura, Ryosuke, Kato, Shumei, Lee, Suzanna, Jimenez, Rebecca E, Sicklick, Jason K, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Clinical Research, Good Health and Well Being, Adult, Aged, Aged, 80 and over, B7-H1 Antigen, Biomarkers, Tumor, DNA-Binding Proteins, Female, Humans, Immunotherapy, Male, Middle Aged, Progression-Free Survival, Transcription Factors, Young Adult, ARID1A, PD-L1, immune checkpoint inhibitor, immunotherapy, tumor mutation burden, microsatellite instability, biomarker, Oncology and carcinogenesis
Abstract

BackgroundSeveral cancer types harbor alterations in the gene encoding AT-Rich Interactive Domain-containing protein 1A (ARID1A), but there are no approved therapies to address these alterations. Recent studies have shown that ARID1A deficiency compromises mismatch repair proteins. Herein, we analyzed 3403 patients who had tumor tissue next-generation sequencing.FindingsAmong nine cancer subtypes with >5% prevalence of ARID1A alterations, microsatellite instability-high as well as high tumor mutational burden was significantly more frequent in ARID1A-altered versus ARID1A wild-type tumors (20% vs 0.9%, p

Published
2020

28. Comprehensive Genomic Landscape and Precision Therapeutic Approach in Biliary Tract Cancers

Author

Okamura, Ryosuke, Kurzrock, Razelle, Mallory, Robert J, Fanta, Paul T, Burgoyne, Adam M, Clary, Bryan M, Kato, Shumei, and Sicklick, Jason K

Subjects
Digestive Diseases, Cancer, Genetics, Human Genome, Biotechnology, Good Health and Well Being, biliary tract cancer, cholangiocarcinoma, circulating tumor DNA, liquid biopsy, molecular oncology, biomarker, personalized cancer therapy
Published
2020

29. Revisiting Epidermal Growth Factor Receptor (EGFR) Amplification as a Target for Anti-EGFR Therapy: Analysis of Cell-Free Circulating Tumor DNA in Patients With Advanced Malignancies

Author

Kato, Shumei, Okamura, Ryosuke, Mareboina, Manvita, Lee, Suzanna, Goodman, Aaron, Patel, Sandip P, Fanta, Paul T, Schwab, Richard B, Vu, Peter, Raymond, Victoria M, Lanman, Richard B, Sicklick, Jason K, Lippman, Scott M, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Genetics, Clinical Research, Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Detection, screening and diagnosis, 4.1 Discovery and preclinical testing of markers and technologies, Good Health and Well Being, Oncology and carcinogenesis
Abstract

PurposeTo date, evidence for tissue epidermal growth factor receptor (EGFR) overexpression as a biomarker for anti-EGFR therapies has been weak. We investigated the genomic landscape of EGFR amplification in blood-derived cell-free tumor DNA (cfDNA) across diverse cancers and the role of anti-EGFR therapies in achieving response.MethodsWe assessed EGFR amplification status among 28,584 patients with malignancies evaluated by clinical-grade next-generation sequencing (NGS) of blood-derived cfDNA (54- to 73-gene panel). Furthermore, we curated the clinical characteristics of 1,434 patients at the University of California San Diego who had cfDNA testing by this NGS test.ResultsOverall, EGFR amplification was detected in cfDNA from 8.5% of patients (2,423 of 28,584), most commonly in colorectal (16.3% [458 of 2,807]), non-small-cell lung (9.0% [1,096 of 12,197]), and genitourinary cancers (8.1% [170 of 2,104]). Most patients had genomic coalterations (96.9% [95 of 98]), frequently involving genes affecting other tyrosine kinases (72.4% [71 of 98]), mitogen-activated protein kinase cascades (56.1% [55 of 98]), cell-cycle-associated signals (52.0% [51 of 98]), and the phosphoinositide 3-kinase pathway (35.7% [35 of 98]). EGFR amplification emerged in serial cfDNA after various anticancer therapies (n = 6), including checkpoint inhibitors (n = 4), suggesting a possible role for these amplifications in acquired resistance. Nine evaluable patients with EGFR amplification were treated with anti-EGFR-based regimens; five (55.6%) achieved partial responses, including three patients whose tissue NGS lacked EGFR amplification.ConclusionEGFR amplification was detected in cfDNA among 8.5% of 28,584 diverse cancers. Most patients had coexisting alterations. Responses were observed in five of nine patients who received EGFR inhibitors. Incorporating EGFR inhibitors into the treatment regimens of patients harboring EGFR amplification in cfDNA merits additional study.

Published
2019

30. Loss of the PTCH1 tumor suppressor defines a new subset of plexiform fibromyxoma

Author

Banerjee, Sudeep, Corless, Christopher L, Miettinen, Markku M, Noh, Sangkyu, Ustoy, Rowan, Davis, Jessica L, Tang, Chih-Min, Yebra, Mayra, Burgoyne, Adam M, and Sicklick, Jason K

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Biotechnology, Cancer, Adolescent, Adult, Aged, Carrier Proteins, Chromosome Deletion, Cyclin D1, Exons, Female, Fibroma, Genes, Tumor Suppressor, Hedgehog Proteins, High-Throughput Nucleotide Sequencing, Humans, Male, Membrane Glycoproteins, Middle Aged, Patched-1 Receptor, RNA, Long Noncoding, Retrospective Studies, Smoothened Receptor, Young Adult, Zinc Finger Protein GLI1, Submucosal tumor, Gastric mass, Patched 1, GLI1, Hedgehog pathway, SMO inhibitor, Sonidegib, Gastrointestinal stromal tumor, Next generation sequencing, Medical and Health Sciences, Immunology, Biomedical and clinical sciences, Health sciences
Abstract

BackgroundPlexiform fibromyxoma (PF) is a rare gastric tumor often confused with gastrointestinal stromal tumor. These so-called "benign" tumors often present with upper GI bleeding and gastric outlet obstruction. It was recently demonstrated that approximately one-third of PF have activation of the GLI1 oncogene, a transcription factor in the hedgehog (Hh) pathway, via a MALAT1-GLI1 fusion protein or GLI1 up-regulation. Despite this discovery, the biology of most PFs remains unknown.MethodsNext generation sequencing (NGS) was performed on formalin-fixed paraffin-embedded (FFPE) samples of PF specimens collected from three institutions (UCSD, NCI and OHSU). Fresh frozen tissue from one tumor was utilized for in vitro assays, including quantitative RT-PCR and cell viability assays following drug treatment.ResultsEight patients with PF were identified and 5 patients' tumors were analyzed by NGS. An index case had a mono-allelic PTCH1 deletion of exons 15-24 and a second case, identified in a validation cohort, also had a PTCH1 gene loss associated with a suspected long-range chromosome 9 deletion. Building on the role of Hh signaling in PF, PTCH1, a tumor suppressor protein, functions upstream of GLI1. Loss of PTCH1 induces GLI1 activation and downstream gene transcription. Utilizing fresh tissue from the index PF case, RT-qPCR analysis demonstrated expression of Hh pathway components, SMO and GLI1, as well as GLI1 transcriptional targets, CCND1 and HHIP. In turn, short-term in vitro treatment with a Hh pathway inhibitor, sonidegib, resulted in dose-dependent cell killing.ConclusionsFor the first time, we report a novel association between PTCH1 inactivation and the development of plexiform fibromyxoma. Hh pathway inhibition with SMO antagonists may represent a target to study for treating a subset of plexiform fibromyxomas.

Published
2019

31. MST1R kinase accelerates pancreatic cancer progression via effects on both epithelial cells and macrophages

Author

Babicky, Michele L, Harper, Megan M, Chakedis, Jeffery, Cazes, Alex, Mose, Evangeline S, Jaquish, Dawn V, French, Randall P, Childers, Betzaira, Alakus, Hakan, Schmid, Michael C, Foubert, Phillippe, Miyamoto, Jaclyn, Holman, Patrick J, Walterscheid, Zakkary J, Tang, Chih-Min, Varki, Nissi, Sicklick, Jason K, Messer, Karen, Varner, Judith A, Waltz, Susan E, and Lowy, Andrew M

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Pancreatic Cancer, Rare Diseases, Cancer, Digestive Diseases, Aetiology, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, 2.1 Biological and endogenous factors, Animals, Carcinoma, Pancreatic Ductal, Disease Progression, Epithelial Cells, Female, Gene Knockdown Techniques, Humans, Intracellular Signaling Peptides and Proteins, Macrophages, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Pancreatic Neoplasms, Proof of Concept Study, Protein Serine-Threonine Kinases, Receptor Protein-Tyrosine Kinases, Signal Transduction, Tumor Microenvironment, Clinical Sciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis
Abstract

The MST1R (RON) kinase is overexpressed in >80% of human pancreatic cancers, but its role in pancreatic carcinogenesis is unknown. In this study, we examined the relevance of Mst1r kinase to Kras driven pancreatic carcinogenesis using genetically engineered mouse models. In the setting of mutant Kras, Mst1r overexpression increased acinar-ductal metaplasia (ADM), accelerated the progression of pancreatic intraepithelial neoplasia (PanIN), and resulted in the accumulation of (mannose receptor C type 1) MRC1+, (arginase 1) Arg+ macrophages in the tumor microenvironment. Conversely, absence of a functional Mst1r kinase slowed PanIN initiation, resulted in smaller tumors, prolonged survival and a reduced tumor-associated macrophage content. Mst1r expression was associated with increased production of its ligand Mst1, and in orthotopic models, suppression of Mst1 expression resulted in reduced tumor size, changes in macrophage polarization and enhanced T cell infiltration. This study demonstrates the functional significance of Mst1r during pancreatic cancer initiation and progression. Further, it provides proof of concept that targeting Mst1r can modulate pancreatic cancer growth and the microenvironment. This study provides further rationale for targeting Mst1r as a therapeutic strategy.

Published
2019

32. Molecular profiling of cancer patients enables personalized combination therapy: the I-PREDICT study

Author

Sicklick, Jason K, Kato, Shumei, Okamura, Ryosuke, Schwaederle, Maria, Hahn, Michael E, Williams, Casey B, De, Pradip, Krie, Amy, Piccioni, David E, Miller, Vincent A, Ross, Jeffrey S, Benson, Adam, Webster, Jennifer, Stephens, Philip J, Lee, J Jack, Fanta, Paul T, Lippman, Scott M, Leyland-Jones, Brian, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Clinical Research, Cancer, Rare Diseases, Genetics, Clinical Trials and Supportive Activities, Biotechnology, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Good Health and Well Being, Adult, Aged, Aged, 80 and over, Combined Modality Therapy, Female, Gene Expression Profiling, High-Throughput Nucleotide Sequencing, Humans, Male, Middle Aged, Molecular Targeted Therapy, Neoplasms, Precision Medicine, Progression-Free Survival, Prospective Studies, Young Adult, Medical and Health Sciences, Immunology, Biomedical and clinical sciences, Health sciences
Abstract

Cancer treatments have evolved from indiscriminate cytotoxic agents to selective genome- and immune-targeted drugs that have transformed the outcomes of some malignancies1. Tumor complexity and heterogeneity suggest that the 'precision medicine' paradigm of cancer therapy requires treatment to be personalized to the individual patient2-6. To date, precision oncology trials have been based on molecular matching with predetermined monotherapies7-14. Several of these trials have been hindered by very low matching rates, often in the 5-10% range15, and low response rates. Low matching rates may be due to the use of limited gene panels, restrictive molecular matching algorithms, lack of drug availability, or the deterioration and death of end-stage patients before therapy can be implemented. We hypothesized that personalized treatment with combination therapies would improve outcomes in patients with refractory malignancies. As a first test of this concept, we implemented a cross-institutional prospective study (I-PREDICT, NCT02534675 ) that used tumor DNA sequencing and timely recommendations for individualized treatment with combination therapies. We found that administration of customized multidrug regimens was feasible, with 49% of consented patients receiving personalized treatment. Targeting of a larger fraction of identified molecular alterations, yielding a higher 'matching score', was correlated with significantly improved disease control rates, as well as longer progression-free and overall survival rates, compared to targeting of fewer somatic alterations. Our findings suggest that the current clinical trial paradigm for precision oncology, which pairs one driver mutation with one drug, may be optimized by treating molecularly complex and heterogeneous cancers with combinations of customized agents.

Published
2019

33. Current management of succinate dehydrogenase deficient gastrointestinal stromal tumors

Author

Neppala, Pushpa, Banerjee, Sudeep, Fanta, Paul T., Yerba, Mayra, Porras, Kevin A., Burgoyne, Adam M., and Sicklick, Jason K.

Abstract

Gastrointestinal stromal tumors (GIST) are increasingly recognized as having diverse biology. With the development of tyrosine kinase inhibitors molecularly matched to oncogenic KIT and PDGFRA mutations, GIST have become a quintessential model for precision oncology. However, about 5-10% of GIST lack these driver mutations and are deficient in succinate dehydrogenase (SDH), an enzyme that converts succinate to fumarate. SDH deficiency leads to accumulation of succinate, an oncometabolite that promotes tumorigenesis. SDH- deficient GIST are clinically unique in that they generally affect younger patients and are associated with GIST- paraganglioma hereditary syndrome, also known as Carney-Stratakis Syndrome. SDH-deficient GIST are generally resistant to tyrosine-kinase inhibitors, the standard treatment for advanced or metastatic GIST. Thus, surgical resection is the mainstay of treatment for localized disease, but recurrence is common. Clinical trials are currently underway investigating systemic agents for treatment of advanced SDH-deficient GIST. However, further studies are warranted to improve our understanding of SDH-deficient GIST disease biology, natural history, surgical approaches, and novel therapeutics.

Published
2019

34. Analysis of Circulating Tumor DNA and Clinical Correlates in Patients with Esophageal, Gastroesophageal Junction, and Gastric Adenocarcinoma

Author

Kato, Shumei, Okamura, Ryosuke, Baumgartner, Joel M, Patel, Hitendra, Leichman, Lawrence, Kelly, Kaitlyn, Sicklick, Jason K, Fanta, Paul T, Lippman, Scott M, and Kurzrock, Razelle

Subjects
Cancer, Human Genome, Digestive Diseases, Genetics, Biotechnology, Clinical Research, Good Health and Well Being, Adenocarcinoma, Adult, Aged, Aged, 80 and over, Biomarkers, Tumor, Circulating Tumor DNA, Esophageal Neoplasms, Esophagogastric Junction, Female, Gene Expression Profiling, Genetic Testing, High-Throughput Nucleotide Sequencing, Humans, Kaplan-Meier Estimate, Male, Middle Aged, Neoplasm Grading, Neoplasm Staging, Prognosis, Stomach Neoplasms, Treatment Outcome, Young Adult, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

PurposeEsophageal, gastroesophageal junction, and gastric adenocarcinoma (herein gastroesophageal adenocarcinomas) are associated with poor prognosis and limited systemic treatment options. To further understand the genomic landscape of gastroesophageal cancers and its clinical correlations, circulating tumor DNA (ctDNA) from patients' plasma was evaluated using next-generation sequencing (NGS).Experimental designWe analyzed genomic alterations of 55 patients (mostly advanced disease; 9, surgically resectable) with gastroesophageal adenocarcinomas using clinical-grade NGS performed on plasma-derived ctDNA (54-73 gene panel). The test detects single-nucleotide variants, as well as copy number amplifications, fusions, and indels in selected genes.ResultsSeventy-six percent of patients (42/55) had ≥1 genomic alteration [including variants of unknown significance (VUS)] and 69.1% (38/55) had ≥1 characterized alteration (excluding VUSs). The median number of alterations per patient was 2 (range, 0-15). TP53 (50.9%, 28/55), PIK3CA (16.4%, 9/55), ERBB2 (14.5%, 8/55), and KRAS (14.5%, 8/55) genes were most frequently affected characterized alterations. Thirty-one patients also had tissue NGS. Concordance between tissue and ctDNA ranged from 61.3% (TP53 alterations) to 87.1% (KRAS alterations). ERBB2 alterations were significantly associated with poor overall survival (HR, 14.06; 95% confidence interval, 2.44-81.03; P = 0.003 multivariate analysis). Among patients with ≥1 alteration, no 2 patients had identical molecular portfolios. All patients with ≥1 characterized alteration had theoretically targetable alterations by an FDA-approved agent (on- or off-label). Illustrative case treated with cognate agent is presented.ConclusionsEvaluation of ctDNA by NGS among patients with gastroesophageal adenocarcinoma is feasible. Patients harbored heterogeneous patterns of genomics, with most having alterations that are potentially pharmacologically tractable.

Published
2018

36. Retrospective Analysis of Retroperitoneal-Abdominal-Pelvic Ganglioneuromas: An International Study by the Transatlantic Australasian Retroperitoneal Sarcoma Working Group (TARPSWG)

Author

Noh, Sangkyu, Nessim, Carolyn, Keung, Emily Z., Roland, Christina L., Strauss, Dirk, Sivarajah, Gausihi, Fiore, Marco, Biasoni, Davide, Cioffi, Stefano Piero Bernardo, Mehtsun, Winta, Cananzi, Ferdinando Carlo Maria, Sicoli, Federico, Quagliuolo, Vittorio, Chen, Jun, Luo, Chenghua, Gladdy, Rebecca A., Swallow, Carol, Johnston, Wendy, Ford, Samuel J., Evenden, Caroline, Tirotta, Fabio, Almond, Max, Nguyen, Laura, Rutkowski, Piotr, Krotewicz, Maria, Pennacchioli, Elisabetta, Cardona, Kenneth, Gamboa, Adriana, Hompes, Daphne, Renard, Marleen, Kollár, Attila, Ryser, Christoph O., Vassos, Nikolaos, Raut, Chandrajit P., Fairweather, Mark, Krakorova, Dagmar Adamkova, Quildrian, Sergio, Perhavec, Andraz, Nizri, Eran, Farma, Jeffrey M., Greco, Stephanie H., Vincenzi, Bruno, Lopez, José Antonio González, Solerdecoll, Mireia Solans, Iwata, Shintaro, Fukushima, Suguru, Kim, Teresa, Tolomeo, Francesco, Snow, Hayden, Howlett-Jansen, Ynez, Tzanis, Dimitri, Nikulin, Maxim, Gronchi, Alessandro, and Sicklick, Jason K.

Published
2023
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43. Analysis of NTRK Alterations in Pan-Cancer Adult and Pediatric Malignancies: Implications for NTRK-Targeted Therapeutics.

Author

Okamura, Ryosuke, Boichard, Amélie, Kato, Shumei, Sicklick, Jason K, Bazhenova, Lyudmila, and Kurzrock, Razelle

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biotechnology, Human Genome, Genetics, Pediatric Cancer, Rare Diseases, Cancer, Pediatric, Good Health and Well Being, Oncology and carcinogenesis
Abstract

PurposeFusions that involve neurotrophic-tropomyosin receptor kinase (NTRK) genes are known drivers of oncogenesis. Therapies that target these ultra-rare, constitutionally active NTRK fusions have been remarkably effective. Herein, we analyze the prevalence of the full array of NTRK alterations-fusions, mutations, copy number alterations, and increased transcript expression-in diverse adult and pediatric tumor types to understand the landscape of NTRK aberrations in cancer.MethodsWe assessed 13,467 samples available from The Cancer Genome Atlas (adult tumors) and the St Jude PeCan database (pediatric tumors) for the prevalence of NTRK fusions, as well as associated genomic and transcriptomic co-aberrations in different tumor types.ResultsNTRK fusions were observed in 0.31% of adult tumors and in 0.34% of pediatric tumors. The most common gene partners were NTRK3 (0.16% of adult tumors) followed by NTRK1 (0.14% of pediatric tumors). NTRK fusions were found more commonly in pediatric melanoma (11.1% of samples), pediatric glioma (3.97%), and adult thyroid cancers (2.34%). Additional genomic and transcriptomic NTRK alterations- mutation, amplification, and mRNA overexpression-occurred in 14.2% of samples, whereas the frequency of alterations that implicated NTRK ligands and the NTRK co-receptor (p75NTR) ranged from 3.8% to 5.4%. Among 31 adult samples carrying NTRK fusions, co-alterations occurred often and usually involved the downstream phosphoinositide-3-kinase signaling pathway, cell-cycle machinery, other tyrosine-kinase receptors, and mitogen-activated protein kinase signals.ConclusionWhereas NTRK fusions are exceedingly rare, other NTRK abnormalities affect 14% of patients with cancer. Affecting these alterations has not yet been achievable in cancer. Genomic co-alterations occur frequently with NTRK fusions, but it is not known if co-targeting them can attenuate primary or secondary resistance to NTRK inhibitors.

Published
2018

44. Academic Surgical Oncologists’ Productivity Correlates with Gender, Grant Funding, and Institutional NCI Comprehensive Cancer Center Affiliation

Author

Nguyen, Vi, Marmor, Rebecca A, Ramamoorthy, Sonia L, Blair, Sarah L, Clary, Bryan M, and Sicklick, Jason K

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Pediatric, Academic Medical Centers, Biomedical Research, Efficiency, Female, Humans, Male, National Cancer Institute (U.S.), National Institutes of Health (U.S.), Oncologists, Publications, Research Support as Topic, Sex Factors, Surgical Oncology, United States, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

BackgroundA scholar's h-index is defined as the number of h papers published, each of which has been cited at least h times. We hypothesized that the h-index strongly correlates with the academic rank of surgical oncologists.MethodsWe utilized the National Cancer Institute (NCI) website to identify NCI-designated Comprehensive Cancer Centers (CCC) and Doximity to identify the 50 highest-ranked general surgery residency programs with surgical oncology divisions. Demographic data of respective academic surgical oncologists were collected from departmental websites and Grantome. Bibliometric data were obtained from Web of Science.ResultsWe identified 544 surgical oncologists from 64 programs. Increased h-index was associated with academic rank (p

Published
2018

45. Next-Generation Sequencing of Circulating Tumor DNA Reveals Frequent Alterations in Advanced Hepatocellular Carcinoma.

Author

Ikeda, Sadakatsu, Tsigelny, Igor F, Skjevik, Åge A, Kono, Yuko, Mendler, Michel, Kuo, Alexander, Sicklick, Jason K, Heestand, Gregory, Banks, Kimberly C, Talasaz, AmirAli, Lanman, Richard B, Lippman, Scott, and Kurzrock, Razelle

Subjects
Humans, Carcinoma, Hepatocellular, Prospective Studies, Adult, Aged, Middle Aged, Female, Male, High-Throughput Nucleotide Sequencing, Biomarkers, Tumor, Circulating Tumor DNA, Circulating tumor DNA, Hepatocellular carcinoma, Liquid biopsy, Next‐generation sequencing, Next-generation sequencing, Carcinoma, Hepatocellular, Biomarkers, Tumor, Human Genome, Liver Cancer, Liver Disease, Clinical Research, Cancer, Rare Diseases, Digestive Diseases, Genetics, Oncology & Carcinogenesis, Oncology and Carcinogenesis
Abstract

BACKGROUND:Because imaging has a high sensitivity to diagnose hepatocellular carcinoma (HCC) and tissue biopsies carry risks such as bleeding, the latter are often not performed in HCC. Blood-derived circulating tumor DNA (ctDNA) analysis can identify somatic alterations, but its utility has not been characterized in HCC. MATERIALS AND METHODS:We evaluated 14 patients with advanced HCC (digital ctDNA sequencing [68 genes]). Mutant relative to wild-type allele fraction was calculated. RESULTS:All patients (100%) had somatic alterations (median = 3 alterations/patient [range, 1-8]); median mutant allele fraction, 0.29% (range, 0.1%-37.77%). Mutations were identified in several genes: TP53 (57% of patients), CTNNB1 (29%), PTEN (7%), CDKN2A (7%), ARID1A (7%), and MET (7%); amplifications, in CDK6 (14%), EGFR (14%), MYC (14%), BRAF (7%), RAF1 (7%), FGFR1 (7%), CCNE1 (7%), PIK3CA (7%), and ERBB2/HER2 (7%). Eleven patients (79%) had ≥1 theoretically actionable alteration. No two patients had identical genomic portfolios, suggesting the need for customized treatment. A patient with a CDKN2A-inactivating and a CTNNB1-activating mutation received matched treatment: palbociclib (CDK4/6 inhibitor) and celecoxib (COX-2/Wnt inhibitor); des-gamma-carboxy prothrombin level decreased by 84% at 2 months (1,410 to 242 ng/mL [normal: ≤7.4 ng/mL]; alpha fetoprotein [AFP] low at baseline). A patient with a PTEN-inactivating and a MET-activating mutation (an effect suggested by in silico molecular dynamic simulations) received sirolimus (mechanistic target of rapamycin inhibitor) and cabozantinib (MET inhibitor); AFP declined by 63% (8,320 to 3,045 ng/mL [normal: 0-15 ng/mL]). CONCLUSION:ctDNA derived from noninvasive blood tests can provide exploitable genomic profiles in patients with HCC. IMPLICATIONS FOR PRACTICE:This study reports that blood-derived circulating tumor DNA can provide therapeutically exploitable genomic profiles in hepatocellular cancer, a malignancy that is known to be difficult to biopsy.

Published
2018

46. A Novel T-Stage Classification System for Adrenocortical Carcinoma: Proposal from the US Adrenocortical Carcinoma Study Group

Author

Poorman, Caroline E, Ethun, Cecilia G, Postlewait, Lauren M, Tran, Thuy B, Prescott, Jason D, Pawlik, Timothy M, Wang, Tracy S, Glenn, Jason, Hatzaras, Ioannis, Shenoy, Rivfka, Phay, John E, Keplinger, Kara, Fields, Ryan C, Jin, Linda X, Weber, Sharon M, Salem, Ahmed, Sicklick, Jason K, Gad, Shady, Yopp, Adam C, Mansour, John C, Duh, Quan-Yang, Seiser, Natalie, Solórzano, Carmen C, Kiernan, Colleen M, Votanopoulos, Konstantinos I, Levine, Edward A, Staley, Charles A, Poultsides, George A, and Maithel, Shishir K

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Adrenal Cortex Neoplasms, Adrenalectomy, Adrenocortical Carcinoma, Female, Follow-Up Studies, Humans, Lymphatic Metastasis, Male, Middle Aged, Neoplasm Invasiveness, Neoplasm Staging, Retrospective Studies, Risk Factors, Survival Rate, Treatment Outcome, Tumor Burden, United States, Oncology and Carcinogenesis, Oncology & Carcinogenesis, Oncology and carcinogenesis
Abstract

BACKGROUND:The 7th AJCC T-stage system for adrenocortical carcinoma (ACC), based on size and extra-adrenal invasion, does not adequately stratify patients by survival. Lymphovascular invasion (LVI) is a known poor prognostic factor. We propose a novel T-stage system that incorporates LVI to better risk-stratify patients undergoing resection for ACC. METHOD:Patients undergoing curative-intent resections for ACC from 1993 to 2014 at 13 institutions comprising the US ACC Group were included. Primary outcome was disease-specific survival (DSS). RESULTS:Of the 265 patients with ACC, 149 were included for analysis. The current T-stage system failed to differentiate patients with T2 versus T3 disease (p = 0.10). Presence of LVI was associated with worse DSS versus no LVI (36 mo vs. 168 mo; p = 0.001). After accounting for the individual components of the current T-stage system (size, extra-adrenal invasion), LVI remained a poor prognostic factor on multivariable analysis (hazard ratio 2.14, 95% confidence interval 1.05-4.38, p = 0.04). LVI positivity further stratified patients with T2 and T3 disease (T2: 37 mo vs. median not reached; T3: 36 mo vs. 96 mo; p = 0.03) but did not influence survival in patients with T1 or T4 disease. By incorporating LVI, a new T-stage classification system was created: [T1: ≤ 5 cm, (-)local invasion, (+/-)LVI; T2: > 5 cm, (-)local invasion, (-)LVI OR any size, (+)local invasion, (-)LVI; T3: > 5 cm, (-)local invasion, (+)LVI OR any size, (+)local invasion, (+)LVI; T4: any size, (+)adjacent organ invasion, (+/-)LVI]. Each progressive new T-stage group was associated with worse median DSS (T1: 167 mo; T2: 96 mo; T3: 37 mo; T4: 15 mo; p

Published
2018

48. Cumulative GRAS Score as a Predictor of Survival After Resection for Adrenocortical Carcinoma: Analysis From the U.S. Adrenocortical Carcinoma Database

Author

Baechle, Jordan J., Marincola Smith, Paula, Solórzano, Carmen C., Tran, Thuy B., Postlewait, Lauren M., Maithel, Shishir K., Prescott, Jason, Pawlik, Timothy, Wang, Tracy S., Glenn, Jason, Hatzaras, Ioannis, Shenoy, Rivfka, Phay, John E., Shirley, Lawrence A., Fields, Ryan C., Jin, Linda, Abbott, Daniel E., Ronnekleiv-Kelly, Sean, Sicklick, Jason K., Yopp, Adam, Mansour, John, Duh, Quan-Yang, Seiser, Natalie, Votanopoulos, Konstantinos, Levine, Edward A., Poultsides, George, and Kiernan, Colleen M.

Published
2021
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49. Duodenal-Jejunal Flexure GI Stromal Tumor Frequently Heralds Somatic NF1 and Notch Pathway Mutations

Author

Burgoyne, Adam M, De Siena, Martina, Alkhuziem, Maha, Tang, Chih-Min, Medina, Benjamin, Fanta, Paul T, Belinsky, Martin G, von Mehren, Margaret, Thorson, John A, Madlensky, Lisa, Bowler, Timothy, D'Angelo, Francesco, Stupack, Dwayne G, Harismendy, Olivier, DeMatteo, Ronald P, and Sicklick, Jason K

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Neurosciences, Rare Diseases, Biotechnology, Genetics, Neurofibromatosis, Human Genome, Digestive Diseases, Cancer, 2.1 Biological and endogenous factors, Aetiology, Oncology and carcinogenesis
Abstract

PurposeGI stromal tumors (GISTs) are commonly associated with somatic mutations in KIT and PDGFRA. However, a subset arises from mutations in NF1, most commonly associated with neurofibromatosis type 1. We define the anatomic distribution of NF1 alterations in GIST.MethodsWe describe the demographic/clinicopathologic features of 177 patients from two institutions whose GISTs underwent next-generation sequencing of ≥315 cancer-related genes.ResultsWe initially identified six (9.7%) of 62 GISTs with NF1 genomic alterations from the first cohort. Of these six patients, five (83.3%) had unifocal tumors at the duodenal-jejunal flexure (DJF). Two additional patients with DJF GISTs had non-NF1 (KIT and BRAF) genomic alterations. After excluding one DJF GIST with an NF1 single nucleotide polymorphism, four (57.1%) of seven sequenced DJF tumors demonstrated deleterious NF1 alterations, whereas only one (1.8%) of 55 sequenced non-DJF GISTs had a deleterious NF1 somatic mutation (P < .001). One patient with DJF GIST had a germline NF1 variant that was associated with incomplete penetrance of clinical neurofibromatosis type 1 features along with a somatic NF1 mutation. Of the five DJF GISTs with any NF1 alteration, three (60%) had KIT mutations, and three (60%) had Notch pathway mutations (NOTCH2, MAML2, CDC73). We validated these findings in a second cohort of 115 GISTs, where two (40%) of five unifocal NF1-mutated GISTs arose at the DJF, and one of these also had a Notch pathway mutation (EP300).ConclusionBroad genomic profiling of adult GISTs has revealed that NF1 alterations are enriched in DJF GISTs. These tumors also may harbor concurrent activating KIT and/or inactivating Notch pathway mutations. In some cases, germline NF1 genetic testing may be appropriate for patients with DJF GISTs.

Published
2017

50. Molecular Pathways: Targeting the Microenvironment of Liver Metastases

Author

Milette, Simon, Sicklick, Jason K, Lowy, Andrew M, and Brodt, Pnina

Subjects
Liver Disease, Digestive Diseases, Colo-Rectal Cancer, Cancer, 5.1 Pharmaceuticals, Aetiology, Development of treatments and therapeutic interventions, 2.1 Biological and endogenous factors, Gastrointestinal Neoplasms, Humans, Liver, Liver Neoplasms, Molecular Targeted Therapy, Neoplasm Metastasis, Tumor Microenvironment, Oncology and Carcinogenesis, Oncology & Carcinogenesis
Abstract

Curative treatment for metastatic solid cancers remains elusive. The liver, which is nourished by a rich blood supply from both the arterial and portal venous systems, is the most common site of visceral metastases, particularly from cancers arising in the gastrointestinal tract, with colorectal cancer being the predominant primary site in Western countries. A mounting body of evidence suggests that the liver microenvironment (LME) provides autocrine and paracrine signals originating from both parenchymal and nonparenchymal cells that collectively create both pre- and prometastatic niches for the development of hepatic metastases. These resident cells and their molecular mediators represent potential therapeutic targets for the prevention and/or treatment of liver metastases (LM). This review summarizes: (i) the current therapeutic options for treating LM, with a particular focus on colorectal cancer LM; (ii) the role of the LME in LM at each of its phases; (iii) potential targets in the LME identified through preclinical and clinical investigations; and (iv) potential therapeutic approaches for targeting elements of the LME before and/or after the onset of LM as the basis for future clinical trials. Clin Cancer Res; 23(21); 6390-9. ©2017 AACR.

Published
2017

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