Your search keyword '"Samantha J. Bilton"' showing total 9 results

1. Data from Exploiting MCL1 Dependency with Combination MEK + MCL1 Inhibitors Leads to Induction of Apoptosis and Tumor Regression in KRAS-Mutant Non–Small Cell Lung Cancer

Author

Aaron N. Hata, Paul E. Hughes, Cyril H. Benes, Angela Coxon, Sean P. Brown, Kristopher A. Sarosiek, Justin F. Gainor, Christopher G. Azzoli, Anna F. Farago, Zofia Piotrowska, Lecia V. Sequist, Colleen Keyes, John H. Shin, Daniel P. Cahill, Kevin A. Raskin, Cameron D. Wright, Michael Lanuti, Lorin A. Ferris, Kristof Vajda, Diamanda Rigas, Cameron Fraser, Chendi Li, Hannah L. Archibald, Maria Gomez-Caraballo, Nicole Phan, Samantha J. Bilton, Daria Timonina, Sean Caenepeel, Faria M. Siddiqui, and Varuna Nangia

Abstract

BH3 mimetic drugs, which inhibit prosurvival BCL2 family proteins, have limited single-agent activity in solid tumor models. The potential of BH3 mimetics for these cancers may depend on their ability to potentiate the apoptotic response to chemotherapy and targeted therapies. Using a novel class of potent and selective MCL1 inhibitors, we demonstrate that concurrent MEK + MCL1 inhibition induces apoptosis and tumor regression in KRAS-mutant non–small cell lung cancer (NSCLC) models, which respond poorly to MEK inhibition alone. Susceptibility to BH3 mimetics that target either MCL1 or BCL-xL was determined by the differential binding of proapoptotic BCL2 proteins to MCL1 or BCL-xL, respectively. The efficacy of dual MEK + MCL1 blockade was augmented by prior transient exposure to BCL-xL inhibitors, which promotes the binding of proapoptotic BCL2 proteins to MCL1. This suggests a novel strategy for integrating BH3 mimetics that target different BCL2 family proteins for KRAS-mutant NSCLC.Significance:Defining the molecular basis for MCL1 versus BCL-xL dependency will be essential for effective prioritization of BH3 mimetic combination therapies in the clinic. We discover a novel strategy for integrating BCL-xL and MCL1 inhibitors to drive and subsequently exploit apoptotic dependencies of KRAS-mutant NSCLCs treated with MEK inhibitors.See related commentary by Leber et al., p. 1511.This article is highlighted in the In This Issue feature, p. 1494

Published

2023

2. Supplementary Data from Exploiting MCL1 Dependency with Combination MEK + MCL1 Inhibitors Leads to Induction of Apoptosis and Tumor Regression in KRAS-Mutant Non–Small Cell Lung Cancer

Author

Aaron N. Hata, Paul E. Hughes, Cyril H. Benes, Angela Coxon, Sean P. Brown, Kristopher A. Sarosiek, Justin F. Gainor, Christopher G. Azzoli, Anna F. Farago, Zofia Piotrowska, Lecia V. Sequist, Colleen Keyes, John H. Shin, Daniel P. Cahill, Kevin A. Raskin, Cameron D. Wright, Michael Lanuti, Lorin A. Ferris, Kristof Vajda, Diamanda Rigas, Cameron Fraser, Chendi Li, Hannah L. Archibald, Maria Gomez-Caraballo, Nicole Phan, Samantha J. Bilton, Daria Timonina, Sean Caenepeel, Faria M. Siddiqui, and Varuna Nangia

Abstract

Supplementary Figure 1-5, Supplementary Tables 1-3

Published

2023

3. Antibody Responses In Non-Severe SARS-CoV-2 Infections Are Driven By CD4+ T cells and Age

Author

Amelie E. Murrell, Ewono Eyoh, Jeffrey G. Shaffer, Monika L. Dietrich, Ivy V. Trinh, Thomas J. Yockachonis, Shuangyi Bai, Crystal Y. Zheng, Celia V. Mayne, Sofia E. Cabrera, Anyssa Aviles-Amaro, Addison E. Stone, Saraswatie Rambaran, Sruti Chandra, Debra H. Elliott, Ashley R. Smira, Sara N. Harris, Katharine E. Olson, Samantha J. Bilton, Medea J. Gabriel, Nicole D. Falgout, Emily J. Engel, Alisha D. Prystowsky, Bo Ning, Tony Hu, Jay K. Kolls, Samuel J. Landry, Stacy S. Drury, John S. Schieffelin, Kevin J. Zwezdaryk, James E. Robinson, Bronwyn M. Gunn, and Elizabeth B. Norton

Abstract

SUMMARYSARS-CoV-2 infection causes a spectrum of clinical outcomes and diverse memory responses. Population studies indicate that viral neutralizing antibody responses are protective, but do not always develop post-infection. Other antiviral antibody effector functions, T-cell responses, or immunity to seasonal coronaviruses (OC43, 229E) have been implicated but not defined in all ages. Here, we identify that children and adult subjects generate polyfunctional antibodies to the spike protein after asymptomatic infection or mild disease, with some subjects developing cellular responses without seroconversion. Diversity in immunity was explained by two clusters distinguished by CD4+ T-cell cytokines, age, and antibodies to seasonal coronaviruses. Post-vaccination neutralizing responses were predicted by specific post-infection immune measures, including IL-2, spike-IgA, OC43-IgG1, 229E-IgM. We confirm a key role for CD4+ T cell cytokines in functionality of anti-spike antibodies, and show that antibody diversity is impacted by age, Th/Th2 cytokine biases, and antibody isotypes to SARS-CoV-2 and seasonal coronaviruses.

Published

2022

4. Targeting FGFR overcomes EMT-mediated resistance in EGFR mutant non-small cell lung cancer

Author

Daria Timonina, Fei Ji, Samantha J. Bilton, Krystina E. Kattermann, Peter S. Hammerman, Aaron N. Hata, Daniel P. Rakiec, Varuna Nangia, Max Greenberg, Emma Labrot, Nafeeza Hafeez, Jordi Barretina, David A. Ruddy, Jeffrey A. Engelman, Cyril H. Benes, Matthew J. Niederst, August Williams, Lecia V. Sequist, Leah J. Damon, Sana Raoof, Sosathya Sovath, Joshua M. Korn, Zofia Piotrowska, Iain Mulford, Yotam Drier, and Heidie Frisco-Cabanos

Subjects

0301 basic medicine, Cancer Research, Epithelial-Mesenchymal Transition, Lung Neoplasms, medicine.drug_class, FGFR Inhibition, Mice, Nude, Drug resistance, Fibroblast growth factor, Article, Tyrosine-kinase inhibitor, Mice, 03 medical and health sciences, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Antineoplastic Combined Chemotherapy Protocols, Tumor Cells, Cultured, Genetics, medicine, Animals, Humans, Molecular Targeted Therapy, Receptor, Fibroblast Growth Factor, Type 1, Epidermal growth factor receptor, RNA, Small Interfering, Lung cancer, Protein Kinase Inhibitors, Molecular Biology, Cell Proliferation, biology, Fibroblast growth factor receptor 1, medicine.disease, Xenograft Model Antitumor Assays, 3. Good health, ErbB Receptors, 030104 developmental biology, Drug Resistance, Neoplasm, Fibroblast growth factor receptor, 030220 oncology & carcinogenesis, Mutation, Cancer research, biology.protein, Female

Abstract

Evolved resistance to tyrosine kinase inhibitor (TKI)-targeted therapies remains a major clinical challenge. In epidermal growth factor receptor (EGFR) mutant non-small-cell lung cancer (NSCLC), failure of EGFR TKIs can result from both genetic and epigenetic mechanisms of acquired drug resistance. Widespread reports of histologic and gene expression changes consistent with an epithelial-to-mesenchymal transition (EMT) have been associated with initially surviving drug-tolerant persister cells, which can seed bona fide genetic mechanisms of resistance to EGFR TKIs. While therapeutic approaches targeting fully resistant cells, such as those harboring an EGFRT790M mutation, have been developed, a clinical strategy for preventing the emergence of persister cells remains elusive. Using mesenchymal cell lines derived from biopsies of patients who progressed on EGFR TKI as surrogates for persister populations, we performed whole-genome CRISPR screening and identified fibroblast growth factor receptor 1 (FGFR1) as the top target promoting survival of mesenchymal EGFR mutant cancers. Although numerous previous reports of FGFR signaling contributing to EGFR TKI resistance in vitro exist, the data have not yet been sufficiently compelling to instigate a clinical trial testing this hypothesis, nor has the role of FGFR in promoting the survival of persister cells been elucidated. In this study, we find that combining EGFR and FGFR inhibitors inhibited the survival and expansion of EGFR mutant drug-tolerant cells over long time periods, preventing the development of fully resistant cancers in multiple vitro models and in vivo. These results suggest that dual EGFR and FGFR blockade may be a promising clinical strategy for both preventing and overcoming EMT-associated acquired drug resistance and provide motivation for the clinical study of combined EGFR and FGFR inhibition in EGFR-mutated NSCLCs.

Published

2019

5. KRAS G12C NSCLC Models Are Sensitive to Direct Targeting of KRAS in Combination with PI3K Inhibition

Author

Sandra Misale, Samantha J. Bilton, Patrick P. Zarrinkar, Maria Gomez-Caraballo, Daria Timonina, Giovanna T. Stein, Jackson P. Fatherree, Dana Lee, Ellen Murchie, Matthew R. Janes, Max Greenberg, Eliane Cortez, Joseph McClanaghan, Aaron N. Hata, Yi Liu, Regina K. Egan, Chendi Li, Varuna Nangia, Patricia Greninger, Cyril H. Benes, David T. Myers, and Lian-Sheng Li

Subjects

0301 basic medicine, MAPK/ERK pathway, Cancer Research, Drug resistance, Biology, medicine.disease_cause, Proto-Oncogene Proteins p21(ras), Mice, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, 0302 clinical medicine, In vivo, Cell Line, Tumor, medicine, Animals, Humans, Gene silencing, Gene Silencing, Protein Kinase Inhibitors, Alleles, PI3K/AKT/mTOR pathway, Cell Proliferation, Phosphoinositide-3 Kinase Inhibitors, In vitro, 3. Good health, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mutation, Cancer cell, Cancer research, KRAS, Drug Screening Assays, Antitumor, Signal Transduction

Abstract

Purpose: KRAS-mutant lung cancers have been recalcitrant to treatments including those targeting the MAPK pathway. Covalent inhibitors of KRAS p.G12C allele allow for direct and specific inhibition of mutant KRAS in cancer cells. However, as for other targeted therapies, the therapeutic potential of these inhibitors can be impaired by intrinsic resistance mechanisms. Therefore, combination strategies are likely needed to improve efficacy. Experimental Design: To identify strategies to maximally leverage direct KRAS inhibition we defined the response of a panel of NSCLC models bearing the KRAS G12C–activating mutation in vitro and in vivo. We used a second-generation KRAS G12C inhibitor, ARS1620 with improved bioavailability over the first generation. We analyzed KRAS downstream effectors signaling to identify mechanisms underlying differential response. To identify candidate combination strategies, we performed a high-throughput drug screening across 112 drugs in combination with ARS1620. We validated the top hits in vitro and in vivo including patient-derived xenograft models. Results: Response to direct KRAS G12C inhibition was heterogeneous across models. Adaptive resistance mechanisms involving reactivation of MAPK pathway and failure to induce PI3K–AKT pathway inactivation were identified as likely resistance events. We identified several model-specific effective combinations as well as a broad-sensitizing effect of PI3K-AKT–mTOR pathway inhibitors. The G12Ci+PI3Ki combination was effective in vitro and in vivo on models resistant to single-agent ARS1620 including patient-derived xenografts models. Conclusions: Our findings suggest that signaling adaptation can in some instances limit the efficacy of ARS1620 but combination with PI3K inhibitors can overcome this resistance.

Published

2019

6. Exploiting MCL1 Dependency with Combination MEK + MCL1 Inhibitors Leads to Induction of Apoptosis and Tumor Regression in KRAS-Mutant Non–Small Cell Lung Cancer

Author

Lorin A. Ferris, Kristof Vajda, Hannah L. Archibald, Daniel P. Cahill, Justin F. Gainor, Diamanda Rigas, Sean P. Brown, Anna F. Farago, Aaron N. Hata, Chendi Li, Cyril H. Benes, Kevin A. Raskin, Varuna Nangia, Michael Lanuti, Cameron D. Wright, John H. Shin, Kristopher A. Sarosiek, Lecia V. Sequist, Christopher G. Azzoli, Angela Coxon, Daria Timonina, Faria M. Siddiqui, Zofia Piotrowska, Paul E. Hughes, Sean Caenepeel, Cameron Fraser, Maria Gomez-Caraballo, Nicole Phan, Colleen Keyes, and Samantha J. Bilton

Subjects

0301 basic medicine, A549 cell, Chemotherapy, Chemistry, medicine.medical_treatment, Mutant, medicine.disease, medicine.disease_cause, Article, 03 medical and health sciences, 030104 developmental biology, Oncology, Cell culture, Apoptosis, medicine, Cancer research, MCL1, KRAS, Lung cancer, neoplasms

Abstract

BH3 mimetic drugs, which inhibit prosurvival BCL2 family proteins, have limited single-agent activity in solid tumor models. The potential of BH3 mimetics for these cancers may depend on their ability to potentiate the apoptotic response to chemotherapy and targeted therapies. Using a novel class of potent and selective MCL1 inhibitors, we demonstrate that concurrent MEK + MCL1 inhibition induces apoptosis and tumor regression in KRAS-mutant non–small cell lung cancer (NSCLC) models, which respond poorly to MEK inhibition alone. Susceptibility to BH3 mimetics that target either MCL1 or BCL-xL was determined by the differential binding of proapoptotic BCL2 proteins to MCL1 or BCL-xL, respectively. The efficacy of dual MEK + MCL1 blockade was augmented by prior transient exposure to BCL-xL inhibitors, which promotes the binding of proapoptotic BCL2 proteins to MCL1. This suggests a novel strategy for integrating BH3 mimetics that target different BCL2 family proteins for KRAS-mutant NSCLC. Significance: Defining the molecular basis for MCL1 versus BCL-xL dependency will be essential for effective prioritization of BH3 mimetic combination therapies in the clinic. We discover a novel strategy for integrating BCL-xL and MCL1 inhibitors to drive and subsequently exploit apoptotic dependencies of KRAS-mutant NSCLCs treated with MEK inhibitors. See related commentary by Leber et al., p. 1511. This article is highlighted in the In This Issue feature, p. 1494

Published

2018

7. Sensitive tracking of circulating viral RNA through all stages of SARS-CoV-2 infection

Author

Alex Niu, Bo Ning, James E. Robinson, Monika L. Dietrich, Elizabeth B. Norton, Alyssa C. Fears, Jim Yee, Weihua Lai, Nakhle S. Saba, Chandler H. Monk, Kevin J. Zwezdaryk, Joshua P. Linhuber, Zhen Huang, Samantha J. Bilton, Christopher J. Lyon, Brady M. Youngquist, Xiao-Ming Yin, He S. Yang, Zhen Zhao, Brandon J. Beddingfield, Jay Rappaport, John W Scott, Amelie E. Murrell, Tony Y. Hu, and Chad J. Roy

Subjects

0301 basic medicine, Adult, Male, Allergy, Time Factors, Coronavirus disease 2019 (COVID-19), Adolescent, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Sensitivity and Specificity, Child health, Virus, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Humans, Viral rna, Longitudinal Studies, Child, Pandemics, Aged, business.industry, SARS-CoV-2, RNA, COVID-19, Infant, General Medicine, Middle Aged, medicine.disease, Virology, Macaca mulatta, Disease Models, Animal, 030104 developmental biology, Nasal Swab, 030220 oncology & carcinogenesis, COVID-19 Nucleic Acid Testing, Child, Preschool, RNA, Viral, Female, Clinical Medicine, CRISPR-Cas Systems, business, Cell-Free Nucleic Acids

Abstract

BACKGROUND: Circulating severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) RNA may represent a more reliable indicator of infection than nasal RNA, but quantitative reverse transcription PCR (RT-qPCR) lacks diagnostic sensitivity for blood samples. METHODS: A CRISPR-augmented RT-PCR assay that sensitively detects SARS-CoV-2 RNA was employed to analyze viral RNA kinetics in longitudinal plasma samples from nonhuman primates (NHPs) after virus exposure; to evaluate the utility of blood SARS-CoV-2 RNA detection for coronavirus disease 2019 (COVID-19) diagnosis in adults cases confirmed by nasal/nasopharyngeal swab RT-PCR results; and to identify suspected COVID-19 cases in pediatric and at-risk adult populations with negative nasal swab RT-qPCR results. All blood samples were analyzed by RT-qPCR to allow direct comparisons. RESULTS: CRISPR-augmented RT-PCR consistently detected SARS-CoV-2 RNA in the plasma of experimentally infected NHPs from 1 to 28 days after infection, and these increases preceded and correlated with rectal swab viral RNA increases. In a patient cohort (n = 159), this blood-based assay demonstrated 91.2% diagnostic sensitivity and 99.2% diagnostic specificity versus a comparator RT-qPCR nasal/nasopharyngeal test, whereas RT-qPCR exhibited 44.1% diagnostic sensitivity and 100% specificity for the same blood samples. This CRISPR-augmented RT-PCR assay also accurately identified patients with COVID-19 using one or more negative nasal swab RT-qPCR results. CONCLUSION: Results of this study indicate that sensitive detection of SARS-CoV-2 RNA in blood by CRISPR-augmented RT-PCR permits accurate COVID-19 diagnosis, and can detect COVID-19 cases with transient or negative nasal swab RT-qPCR results, suggesting that this approach could improve COVID-19 diagnosis and the evaluation of SARS-CoV-2 infection clearance, and predict the severity of infection. TRIAL REGISTRATION: ClinicalTrials.gov. NCT04358211. FUNDING: Department of Defense, National Institute of Allergy and Infectious Diseases, National Institute of Child Health and Human Development, and the National Center for Research Resources.

Published

2021

8. APOBEC3A drives acquired resistance to targeted therapies in non-small cell lung cancer

Author

Mandeep Banwait, Pégah Jalili, Jiachen Lin, Heidie Frisco-Cabanos, S. Oh, Nicole Phan, Lee Zou, Zofia Piotrowska, Marcello Stanzione, Daria Timonina, L.V. Sequist, Jeffrey A. Engelman, Varuna Nangia, Rémi Buisson, Faria M. Siddiqui, Rosemary Cobb, Aaron N. Hata, K. Dionne, Jaewon J. Lee, Hannah L. Archibald, Cyril H. Benes, Amanda K. Riley, Nicholas J. Dyson, Michael W. Lawlor, Cheong Xin Chan, Christopher J. Ott, H. Isozaki, A. Abbasi, Maria Gomez-Caraballo, Gad Getz, Adam Langenbucher, Samantha J. Bilton, Alice T. Shaw, Yosef E. Maruvka, Wenjia Su, Michael S. Lawrence, and N. Nikpour

Subjects

business.industry, medicine.medical_treatment, Mutagenesis (molecular biology technique), Drug resistance, Cytidine deaminase, medicine.disease, Targeted therapy, Acquired resistance, Cancer cell, medicine, Cancer research, APOBEC3A, Lung cancer, business

Abstract

Acquired drug resistance to even the most effective anti-cancer targeted therapies remains an unsolved clinical problem. Although many drivers of acquired drug resistance have been identified1‒6, the underlying molecular mechanisms shaping tumor evolution during treatment are incompletely understood. The extent to which therapy actively drives tumor evolution by promoting mutagenic processes7 or simply provides the selective pressure necessary for the outgrowth of drug-resistant clones8 remains an open question. Here, we report that lung cancer targeted therapies commonly used in the clinic induce the expression of cytidine deaminase APOBEC3A (A3A), leading to sustained mutagenesis in drug-tolerant cancer cells persisting during therapy. Induction of A3A facilitated the formation of double-strand DNA breaks (DSBs) in cycling drug-treated cells, and fully resistant clones that evolved from drug-tolerant intermediates exhibited an elevated burden of chromosomal aberrations such as copy number alterations and structural variations. Preventing therapy-induced A3A mutagenesis either by gene deletion or RNAi-mediated suppression delayed the emergence of drug resistance. Finally, we observed accumulation of A3A mutations in lung cancer patients who developed drug resistance after treatment with sequential targeted therapies. These data suggest that induction of A3A mutagenesis in response to targeted therapy treatment may facilitate the development of acquired resistance in non-small-cell lung cancer. Thus, suppressing expression or enzymatic activity of A3A may represent a potential therapeutic strategy to prevent or delay acquired resistance to lung cancer targeted therapy.

Published

2021

9. Abstract 2163: Combined targeting of MEK and MCL-1 induces apoptosis and tumor regression of KRAS mutant NSCLC

Author

Paul E. Hughes, Daria Timonina, Faria M. Siddiqui, Samantha J. Bilton, Varuna Nangia, Maria Gomez-Caraballo, Aaron N. Hata, Sean Caenepeel, and Angela Coxon

Subjects

Trametinib, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Colorectal cancer, MEK inhibitor, Mutant, Cancer, medicine.disease, medicine.disease_cause, In vivo, Apoptosis, Internal medicine, medicine, KRAS, business, neoplasms

Abstract

There are currently no effective targeted therapeutic strategies for KRAS mutant non-small cell lung cancer (NSCLC). Single agent MEK inhibitors have demonstrated showed disappointing clinical activity, partly due to inability to induce a robust apoptotic response. Combining MEK inhibitors with BCL-XL/BCL-2 inhibitors may be effective for a subset of KRAS mutant cancers that are dependent on BCL-XL for survival, however this combination is unlikely to be an effective strategy for cancers dependent on MCL-1. We investigated the effect of combining the MEK inhibitor trametinib with a novel MCL-1 inhibitor (compound A), which possesses potent and selective anti-MCL-1 activity in vitro and in vivo, on KRAS mutant cancers. In contrast to colorectal cancer models, which are largely sensitive to combined MEK + BCL-XL inhibition, a subset of cell line and patient-derived mouse xenograft (PDX) KRAS mutant NSCLC models were significantly more sensitive to MEK + MCL-1 inhibition compared to MEK + BCL-XL. To model potential clinical strategies, we tested intermittent dosing regimens and unexpectedly discovered a method strategy for dramatically sensitizing KRAS mutant NSCLC cells to the MEK + MCL-1 combination. These studies provide rationale for the clinical evaluation of combined MEK + MCL-1 inhibitors for KRAS mutant NSCLC. Citation Format: Aaron N. Hata, Faria M. Siddiqui, Maria Gomez-Caraballo, Samantha J. Bilton, Daria Timonina, Varuna Nangia, Angela Coxon, Sean Caenepeel, Paul Hughes. Combined targeting of MEK and MCL-1 induces apoptosis and tumor regression of KRAS mutant NSCLC [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 2163. doi:10.1158/1538-7445.AM2017-2163

Published

2017