Your search keyword '"Dylan Fingerman"' showing total 20 results

1. Disrupting MLV integrase:BET protein interaction biases integration into quiescent chromatin and delays but does not eliminate tumor activation in a MYC/Runx2 mouse model.

Author

Lorenz Loyola, Vasudevan Achuthan, Kathryn Gilroy, Gillian Borland, Anna Kilbey, Nancy Mackay, Margaret Bell, Jodie Hay, Sriram Aiyer, Dylan Fingerman, Rodrigo A Villanueva, Ewan Cameron, Christine A Kozak, Alan N Engelman, James Neil, and Monica J Roth

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Murine leukemia virus (MLV) integrase (IN) lacking the C-terminal tail peptide (TP) loses its interaction with the host bromodomain and extraterminal (BET) proteins and displays decreased integration at promoter/enhancers and transcriptional start sites/CpG islands. MLV lacking the IN TP via an altered open reading frame was used to infect tumorigenesis mouse model (MYC/Runx2) animals to observe integration patterns and phenotypic effects, but viral passage resulted in the restoration of the IN TP through small deletions. Mice subsequently infected with an MLV IN lacking the TP coding sequence (TP-) showed an improved median survival by 15 days compared to wild type (WT) MLV infection. Recombination with polytropic endogenous retrovirus (ERV), Pmv20, was identified in seven mice displaying both fast and slow tumorigenesis, highlighting the strong selection within the mouse to maintain the full-length IN protein. Mapping the genomic locations of MLV in tumors from an infected mouse with no observed recombination with ERVs, TP-16, showed fewer integrations at TSS and CpG islands, compared to integrations observed in WT tumors. However, this mouse succumbed to the tumor in relatively rapid fashion (34 days). Analysis of the top copy number integrants in the TP-16 tumor revealed their proximity to known MLV common insertion site genes while maintaining the MLV IN TP- genotype. Furthermore, integration mapping in K562 cells revealed an insertion preference of MLV IN TP- within chromatin profile states associated with weakly transcribed heterochromatin with fewer integrations at histone marks associated with BET proteins (H3K4me1/2/3, and H3K27Ac). While MLV IN TP- showed a decreased overall rate of tumorigenesis compared to WT virus in the MYC/Runx2 model, MLV integration still occurred at regions associated with oncogenic driver genes independently from the influence of BET proteins, either stochastically or through trans-complementation by functional endogenous Gag-Pol protein.

Published

2019

2. Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

Author

Vaibhav Jain, Sandra L. Harper, Amanda M. Versace, Dylan Fingerman, Gregory Schuyler Brown, Monika Bhardwaj, Mary Ann S. Crissey, Aaron R. Goldman, Gordon Ruthel, Qin Liu, Aleksandra Zivkovic, Holgar Stark, Meenhard Herlyn, Phyllis A. Gimotty, David W. Speicher, and Ravi K. Amaravadi

Subjects

Oncology

Abstract

Lysosomal autophagy inhibition (LAI) with hydroxychloroquine or DC661 can enhance cancer therapy, but tumor regrowth is common. To elucidate LAI resistance, proteomics and immunoblotting demonstrated that LAI induced lipid metabolism enzymes in multiple cancer cell lines. Lipidomics showed that LAI increased cholesterol, sphingolipids, and glycosphingolipids. These changes were associated with striking levels of GM1+ membrane microdomains (GMM) in plasma membranes and lysosomes. Inhibition of cholesterol/sphingolipid metabolism proteins enhanced LAI cytotoxicity. Targeting UDP-glucose ceramide glucosyltransferase (UGCG) synergistically augmented LAI cytotoxicity. Although UGCG inhibition decreased LAI-induced GMM and augmented cell death, UGCG overexpression led to LAI resistance. Melanoma patients with high UGCG expression had significantly shorter disease-specific survival. The FDA-approved UGCG inhibitor eliglustat combined with LAI significantly inhibited tumor growth and improved survival in syngeneic tumors and a therapy-resistant patient-derived xenograft. These findings nominate UGCG as a new cancer target, and clinical trials testing UGCG inhibition in combination with LAI are warranted. Significance: We discovered UGCG-dependent lipid remodeling drives resistance to LAI. Targeting UGCG with a drug approved for a lysosomal storage disorder enhanced LAI antitumor activity without toxicity. LAI and UGCG inhibition could be tested clinically in multiple cancers. This article is highlighted in the In This Issue feature, p. 247

Published

2022

3. ERK Hyperactivation Serves as a Unified Mechanism of Escape in Intrinsic and Acquired CDK4/6 Inhibitor Resistance in Acral Lentiginous Melanoma

Author

Vito Rebecca, Kasturee Jagirdar, Marie Portuallo, Meihan Wei, Matthew Wilhide, Jeremy Bravo, Bailey Robertson, Gretchen Alicea, Crsytal Aguh, Min Xiao, Tetiana Godok, Dylan Fingerman, Gregory Brown, Meenhard Herlyn, Brian Guo, Eneda Toska, Daniel Zabransky, Bradley Wubbenhorst, Katherine Nathanson, Shawn Kwatra, Yogesh Goyal, Hongkai Ji, and Qin Liu

Abstract

Patients with metastatic acral lentiginous melanoma (ALM) suffer worse outcomes relative to patients with other forms of cutaneous melanoma (CM), and do not benefit as well to approved melanoma therapies. Identification of cyclin-dependent kinase 4 and 6 (CDK4/6) pathway gene alterations in > 60% of ALMs has led to clinical trials of the CDK4/6 inhibitor (CDK4i/6i) palbociclib for ALM; however, median progression free survival with CDK4i/6i treatment was only 2.2 months, suggesting existence of resistance mechanisms. Therapy resistance in ALM remains poorly understood; here we report hyperactivation of MAPK signaling and elevated cyclin D1 expression are a unified mechanism of both intrinsic and acquired CDK4i/6i resistance. MEK and/or ERK inhibition increases CDK4i/6i efficacy in a patient-derived xenograft (PDX) model of ALM and promotes a defective DNA repair, cell cycle arrested and apoptotic program. Notably, gene alterations poorly correlate with protein expression of cell cycle proteins in ALM or efficacy of CDK4i/6i, urging additional strategies when stratifying patients for CDK4i/6i trial inclusion. Concurrent targeting of the MAPK pathway and CDK4/6 represents a new approach to improve outcomes for patients with advanced ALM.

Published

2023

4. Supplementary Data Tables S1-S2 from Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

Author

Ravi K. Amaravadi, David W. Speicher, Phyllis A. Gimotty, Meenhard Herlyn, Holgar Stark, Aleksandra Zivkovic, Qin Liu, Gordon Ruthel, Aaron R. Goldman, Mary Ann S. Crissey, Monika Bhardwaj, Gregory Schuyler Brown, Dylan Fingerman, Amanda M. Versace, Sandra L. Harper, and Vaibhav Jain

Abstract

Supplemental Table S1: Patient Characteristics by UGCG expression defined Risk Groups in the Learning Dataset; Supplemental Table S2: Patient Characteristics by UGCG expression defined Risk Groups in the Validation Dataset (Cirenajwis et al., 2015)

Published

2023

5. Supplementary Data Figures S1-S5 from Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

Author

Ravi K. Amaravadi, David W. Speicher, Phyllis A. Gimotty, Meenhard Herlyn, Holgar Stark, Aleksandra Zivkovic, Qin Liu, Gordon Ruthel, Aaron R. Goldman, Mary Ann S. Crissey, Monika Bhardwaj, Gregory Schuyler Brown, Dylan Fingerman, Amanda M. Versace, Sandra L. Harper, and Vaibhav Jain

Abstract

Supplemental Figure S1: LAI remodels the lipidome of melanoma cells. Supplemental Figure S2: LAI induces UGCG, and UGCG inhibition augments DC661 cytotoxicity, and this effect is not seen by blocking cholesterol synthesis and key earlier steps of autophagy. Supplemental Figure S3: LAI increases the formation of GMM in cancer cells. Supplemental Figure S4: UGCG inhibition synergistically augments LAI induced cytotoxicity and abrogates GMM formation without elevating ceramide levels. Supplemental Figure S5: LAI induces UGCG-associated GMM formation in PDX cells, a combination of DC661 and eliglustat impairs tumor growth in a therapy-resistant PDX tumor model.

Published

2023

6. Data from Targeting UGCG Overcomes Resistance to Lysosomal Autophagy Inhibition

Author

Ravi K. Amaravadi, David W. Speicher, Phyllis A. Gimotty, Meenhard Herlyn, Holgar Stark, Aleksandra Zivkovic, Qin Liu, Gordon Ruthel, Aaron R. Goldman, Mary Ann S. Crissey, Monika Bhardwaj, Gregory Schuyler Brown, Dylan Fingerman, Amanda M. Versace, Sandra L. Harper, and Vaibhav Jain

Abstract

Lysosomal autophagy inhibition (LAI) with hydroxychloroquine or DC661 can enhance cancer therapy, but tumor regrowth is common. To elucidate LAI resistance, proteomics and immunoblotting demonstrated that LAI induced lipid metabolism enzymes in multiple cancer cell lines. Lipidomics showed that LAI increased cholesterol, sphingolipids, and glycosphingolipids. These changes were associated with striking levels of GM1+ membrane microdomains (GMM) in plasma membranes and lysosomes. Inhibition of cholesterol/sphingolipid metabolism proteins enhanced LAI cytotoxicity. Targeting UDP-glucose ceramide glucosyltransferase (UGCG) synergistically augmented LAI cytotoxicity. Although UGCG inhibition decreased LAI-induced GMM and augmented cell death, UGCG overexpression led to LAI resistance. Melanoma patients with high UGCG expression had significantly shorter disease-specific survival. The FDA-approved UGCG inhibitor eliglustat combined with LAI significantly inhibited tumor growth and improved survival in syngeneic tumors and a therapy-resistant patient-derived xenograft. These findings nominate UGCG as a new cancer target, and clinical trials testing UGCG inhibition in combination with LAI are warranted.Significance:We discovered UGCG-dependent lipid remodeling drives resistance to LAI. Targeting UGCG with a drug approved for a lysosomal storage disorder enhanced LAI antitumor activity without toxicity. LAI and UGCG inhibition could be tested clinically in multiple cancers.This article is highlighted in the In This Issue feature, p. 247

Published

2023

7. Figure S6 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Dario C. Altieri, Emmanuel Skordalakes, Alessandra Martorella, Dylan Fingerman, Min Xiao, Meenhard Herlyn, Vito W. Rebecca, Valentina Vaira, Massimo Giroda, Davide Tosi, Manuela Caroli, Gabriella Gaudioso, Stefano Ferrero, Alessandra Maria Storaci, Prashanth K. Shastrula, David W. Speicher, Lucia R. Languino, Dmitry I. Gabrilovich, Ekta Agarwal, Hsin-Yao Tang, Yu Geon Lee, Andrew V. Kossenkov, Young Chan Chae, and Jae Ho Seo

Abstract

Anti-glioma activity of MFF peptidomimetic

Published

2023

8. Table S1 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Dario C. Altieri, Emmanuel Skordalakes, Alessandra Martorella, Dylan Fingerman, Min Xiao, Meenhard Herlyn, Vito W. Rebecca, Valentina Vaira, Massimo Giroda, Davide Tosi, Manuela Caroli, Gabriella Gaudioso, Stefano Ferrero, Alessandra Maria Storaci, Prashanth K. Shastrula, David W. Speicher, Lucia R. Languino, Dmitry I. Gabrilovich, Ekta Agarwal, Hsin-Yao Tang, Yu Geon Lee, Andrew V. Kossenkov, Young Chan Chae, and Jae Ho Seo

Abstract

MFF1 synthetic peptides used in this study

Published

2023

9. Supplementary Movie S1 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Dario C. Altieri, Emmanuel Skordalakes, Alessandra Martorella, Dylan Fingerman, Min Xiao, Meenhard Herlyn, Vito W. Rebecca, Valentina Vaira, Massimo Giroda, Davide Tosi, Manuela Caroli, Gabriella Gaudioso, Stefano Ferrero, Alessandra Maria Storaci, Prashanth K. Shastrula, David W. Speicher, Lucia R. Languino, Dmitry I. Gabrilovich, Ekta Agarwal, Hsin-Yao Tang, Yu Geon Lee, Andrew V. Kossenkov, Young Chan Chae, and Jae Ho Seo

Abstract

Morphology of MFF targeting in tumor cells

Published

2023

10. Supplementary Figure S2 from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Dario C. Altieri, Emmanuel Skordalakes, Alessandra Martorella, Dylan Fingerman, Min Xiao, Meenhard Herlyn, Vito W. Rebecca, Valentina Vaira, Massimo Giroda, Davide Tosi, Manuela Caroli, Gabriella Gaudioso, Stefano Ferrero, Alessandra Maria Storaci, Prashanth K. Shastrula, David W. Speicher, Lucia R. Languino, Dmitry I. Gabrilovich, Ekta Agarwal, Hsin-Yao Tang, Yu Geon Lee, Andrew V. Kossenkov, Young Chan Chae, and Jae Ho Seo

Abstract

MFF-VDAC1 complex in cancer

Published

2023

11. Data from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Dario C. Altieri, Emmanuel Skordalakes, Alessandra Martorella, Dylan Fingerman, Min Xiao, Meenhard Herlyn, Vito W. Rebecca, Valentina Vaira, Massimo Giroda, Davide Tosi, Manuela Caroli, Gabriella Gaudioso, Stefano Ferrero, Alessandra Maria Storaci, Prashanth K. Shastrula, David W. Speicher, Lucia R. Languino, Dmitry I. Gabrilovich, Ekta Agarwal, Hsin-Yao Tang, Yu Geon Lee, Andrew V. Kossenkov, Young Chan Chae, and Jae Ho Seo

Abstract

The regulators of mitochondrial cell death in cancer have remained elusive, hampering the development of new therapies. Here, we showed that protein isoforms of mitochondrial fission factor (MFF1 and MFF2), a molecule that controls mitochondrial size and shape, that is, mitochondrial dynamics, were overexpressed in patients with non–small cell lung cancer and formed homo- and heterodimeric complexes with the voltage-dependent anion channel-1 (VDAC1), a key regulator of mitochondrial outer membrane permeability. MFF inserted into the interior hole of the VDAC1 ring using Arg225, Arg236, and Gln241 as key contact sites. A cell-permeable MFF Ser223-Leu243 d-enantiomeric peptidomimetic disrupted the MFF–VDAC1 complex, acutely depolarized mitochondria, and triggered cell death in heterogeneous tumor types, including drug-resistant melanoma, but had no effect on normal cells. In preclinical models, treatment with the MFF peptidomimetic was well-tolerated and demonstrated anticancer activity in patient-derived xenografts, primary breast and lung adenocarcinoma 3D organoids, and glioblastoma neurospheres. These data identify the MFF–VDAC1 complex as a novel regulator of mitochondrial cell death and an actionable therapeutic target in cancer.Significance:These findings describe mitochondrial fission regulation using a peptidomimetic agent that disturbs the MFF–VDAC complex and displays anticancer activity in multiple tumor models.See related commentary by Rao, p. 6074

Published

2023

12. Supplementary Data from MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Dario C. Altieri, Emmanuel Skordalakes, Alessandra Martorella, Dylan Fingerman, Min Xiao, Meenhard Herlyn, Vito W. Rebecca, Valentina Vaira, Massimo Giroda, Davide Tosi, Manuela Caroli, Gabriella Gaudioso, Stefano Ferrero, Alessandra Maria Storaci, Prashanth K. Shastrula, David W. Speicher, Lucia R. Languino, Dmitry I. Gabrilovich, Ekta Agarwal, Hsin-Yao Tang, Yu Geon Lee, Andrew V. Kossenkov, Young Chan Chae, and Jae Ho Seo

Abstract

Complete Supplementary Data with Figures embedded

Published

2023

13. Author Reply to Peer Reviews of Metastatic potential in clonal melanoma cells is driven by a rare, early-invading subpopulation

Author

Amanpreet Kaur, Karun Kiani, Dylan Fingerman, Margaret Dunagin, Jingxin Li, Ian Dardani, Eric M Sanford, Jordan Pemberton, Yogesh Goyal, Ashani Weeraratna, Meenhard Herlyn, and Arjun Raj

Published

2023

14. Dasatinib Resensitizes MAPK Inhibitor Efficacy in Standard-of-Care Relapsed Melanomas

Author

Vito W. Rebecca, Min Xiao, Andrew Kossenkov, Tetiana Godok, Gregory Schuyler Brown, Dylan Fingerman, Gretchen M. Alicea, Meihan Wei, Hongkai Ji, Jeremy Bravo, Yeqing Chen, Mitchell E. Fane, Jessie Villanueva, Katherine Nathanson, Qin Liu, Y. N. Vashisht Gopal, Michael A. Davies, and Meenhard Herlyn

Abstract

Resistance to combination BRAF/MEK inhibitor (BRAFi/MEKi) therapy arises in nearly every patient withBRAFV600E/Kmelanoma, despite promising initial responses. Achieving cures in this expanding BRAFi/MEKi-resistant cohort represents one of the greatest challenges to the field; few experience additional durable benefit from immunotherapy and no alternative therapies exist. To better personalize therapy in cancer patients to address therapy relapse, umbrella trials have been initiated whereby genomic sequencing of a panel of potentially actionable targets guide therapy selection for patients; however, the superior efficacy of such approaches remains to be seen. We here test the robustness of the umbrella trial rationale by analyzing relationships between genomic status of a gene and the downstream consequences at the protein level of related pathway, which find poor relationships between mutations, copy number amplification, and protein level. To profile candidate therapeutic strategies that may offer clinical benefit in the context of acquired BRAFi/MEKi resistance, we established a repository ofpatient-derivedxenograft models from heavily pretreated patients with resistance to BRAFi/MEKi and/or immunotherapy (R-PDX). With these R-PDXs, we executedin vivocompound repurposing screens using 11 FDA-approved agents from an NCI-portfolio with pan-RTK, non-RTK and/or PI3K-mTOR specificity. We identify dasatinib as capable of restoring BRAFi/MEKi antitumor efficacy in ∼70% of R-PDX tested. A systems-biology analysis indicates elevated baseline protein expression of canonical drivers of therapy resistance (e.g., AXL, YAP, HSP70, phospho-AKT) as predictive of MAPKi/dasatinib sensitivity. We therefore propose that dasatinib-based MAPKi therapy may restore antitumor efficacy in patients that have relapsed to standard-of-care therapy by broadly targeting proteins critical in melanoma therapy escape. Further, we submit that this experimental PDX paradigm could potentially improve preclinical evaluation of therapeutic modalities and augment our ability to identify biomarker-defined patient subsets that may respond to a given clinical trial.SINGLE SENTENCE SUMMARYBroad target inhibition effective as a salvage strategy in BRAF/MEK inhibitor-acquired resistance PDX

Published

2023

15. ERK Hyperactivation Represents a Unified Mechanism of Escape in Intrinsic and Acquired CDK4/6 Inhibitor Resistance in Acral Lentiginous Melanoma

Author

Kasturee Jagirdar, Marie Portuallo, Matthew Wilhide, Waqar Ahmed, Meihan Wei, Bailey Robertson, Jeremy Bravo, Gretchen Alicea, Crystal Aguh, Min Xiao, Tetiana Godok, Dylan Fingerman, Gregory Brown, Meenhard Herlyn, Brian Guo, Eneda Toska, Daniel Zabransky, Bradley Wubbenhorst, Katherine Nathanson, Hongkai Ji, Qin Liu, and Vito Rebecca

Abstract

Patients with metastatic acral lentiginous melanoma (ALM) suffer worse outcomes relative to patients with other forms of cutaneous melanoma (CM), and do not benefit as well to approved melanoma therapies. Identification of cyclin-dependent kinase 4 and 6 (CDK4/6) pathway gene alterations in >60% of ALMs has led to clinical trials of the CDK4/6 inhibitor (CDK4i/6i) palbociclib for ALM; however, median progression free survival with CDK4i/6i treatment was only 2.2 months, suggesting existence of resistance mechanisms. Therapy resistance in ALM remains poorly understood; here we report hyperactivation of MAPK signaling and elevated cyclin D1 expression are a unified mechanism of both intrinsic and acquired CDK4i/6i resistance. MEK or ERK inhibition increases CDK4i/6i efficacy in a patient-derived xenograft (PDX) models of ALM and promotes a defective DNA repair, cell cycle arrested and apoptotic program. Concurrent targeting of the MAPK pathway and CDK4/6 represents a new approach to improve outcomes for patients with advanced ALM.

Published

2022

16. Comprehensive characterization of 536 patient-derived xenograft models prioritizes candidatesfor targeted treatment

Author

Li Chen, Jacqueline Mudd, Michael Ittmann, Carol J. Bult, Amanda R. Kirane, Jelena Randjelovic, Stephen Scott, Yige Wu, Li Ding, Vashisht G. Yennu-Nanda, Jing Wang, Christopher D. Lanier, Maihi Fujita, Emilio Cortes-Sanchez, Sienna Rocha, Susan G. Hilsenbeck, Kian-Huat Lim, Fernanda Martins Rodrigues, Jill Rubinstein, Nicholas Mitsiades, Haiyin Lin, Jayamanna Wickramasinghe, Andrew Butterfield, Bryan E. Welm, Alana L. Welm, Jose P. Zevallos, Jason Held, Nicole B. Coggins, Song Cao, Yuanxin Xi, Brenda C. Timmons, Paul Lott, David Menter, Shunqiang Li, Tina Primeau, Fei Yang, Andrea Wang-Gillam, Ramaswamy Govindan, Dali Li, Brandi Davis-Dusenbery, Sara Seepo, Michael C. Wendl, Jeffrey Grover, Brian S. White, Clifford G. Tepper, Peter N. Robinson, Michael A. Davies, Zhengtao Chu, Michael W. Lloyd, Hua Sun, Xiaoshan Zhang, Tamara Stankovic, Dylan Fingerman, Anuj Srivastava, Luis G. Carvajal-Carmona, Don L. Gibbons, Lijun Yao, Rebecca Aft, Hongyong Zhang, Ismail Meraz, John DiGiovanna, Scott Kopetz, Ling Zhao, Guadalupe Polanco-Echeverry, Feng Chen, Jeremy Hoog, Matthew A. Wyczalkowski, George Xu, John D. Minna, Yi Xu, Julie Belmar, Xiaowei Xu, Luc Girard, Dennis A. Dean, Tijana Borovski, Chong-xian Pan, Cynthia X. Ma, Alexa Morales Arana, Yize Li, Turcin Saridogan, Steven B. Neuhauser, Sandra Scherer, Vicki Chin, Rose Tipton, David R. Gandara, Sherri R. Davies, Argun Akcakanat, Rajesh Patidar, Julie K. Schwarz, Soner Koc, Gao Boning, Michael Kim, Bryce P. Kirby, Yvonne A. Evrard, Hyunsil Park, Christian Frech, Chia-Kuei Mo, Ran Zhang, Brian A. Van Tine, Jonathan W. Reiss, Min Xiao, Xing Yi Woo, Tiffany Le, Ana Estrada, Xiaofeng Zheng, Jeffrey A. Moscow, Mourad Majidi, Nadezhda V. Terekhanova, Katherine Fuh, Erkan Yuca, Timothy A. Yap, Jianhua Zhang, Matthew J. Ellis, Shannon Westin, James H. Doroshow, Vito W. Rebecca, Moon S. Chen, Coya Tapia, Reyka G Jayasinghe, Jack A. Roth, Jithesh Augustine, Ryan C. Fields, Michae T. Tetzlaff, Michael T. Lewis, Kurt W. Evans, Ralph W. deVere White, Brian J. Sanderson, May Cho, Jeffrey H. Chuang, Tiffany Wallace, Ryan Jeon, Ted Toal, Matthew H. Bailey, Bert W. O'Malley, Katherine L. Nathanson, Qin Liu, Benjamin J. Raphael, Jingqin Luo, Salma Kaochar, Huiqin Chen, Rajasekharan Somasundaram, Daniel Cui Zhou, John F. DiPersio, Andrew V. Kossenkov, Bingliang Fang, Vanessa Jensen, Simone Zaccaria, Alexey Sorokin, Ai-Hong Ma, Sidharth V. Puram, Min Jin Ha, Meenhard Herlyn, R. Jay Mashl, Kelly Gale, Bingbing Dai, Lacey E. Dobrolecki, Chieh-Hsiang Yang, and Funda Meric-Bernstam

Subjects

endocrine system, Science, Druggability, General Physics and Astronomy, Genomics, Computational biology, Biology, Genome, digestive system, General Biochemistry, Genetics and Molecular Biology, Article, Research community, Multiple time, medicine, Cancer genomics, Cancer models, Tumor xenograft, Multidisciplinary, Cancer, General Chemistry, medicine.disease, Pharmacogenomics, Data integration, hormones, hormone substitutes, and hormone antagonists

Abstract

Development of candidate cancer treatments is a resource-intensive process, with the research community continuing to investigate options beyond static genomic characterization. Toward this goal, we have established the genomic landscapes of 536 patient-derived xenograft (PDX) models across 25 cancer types, together with mutation, copy number, fusion, transcriptomic profiles, and NCI-MATCH arms. Compared with human tumors, PDXs typically have higher purity and fit to investigate dynamic driver events and molecular properties via multiple time points from same case PDXs. Here, we report on dynamic genomic landscapes and pharmacogenomic associations, including associations between activating oncogenic events and drugs, correlations between whole-genome duplications and subclone events, and the potential PDX models for NCI-MATCH trials. Lastly, we provide a web portal having comprehensive pan-cancer PDX genomic profiles and source code to facilitate identification of more druggable events and further insights into PDXs’ recapitulation of human tumors., Patient-derived xenograft models (PDX) have been extensively used to study the molecular and clinical features of cancers. Here the authors present a cohort of 536 PDX models from 25 cancers, as well as their genomic and evolutionary profiles and their suitability for clinical trials.

Published

2021

17. fMetastatic potential in clonal melanoma cells is driven by a rare, early-invading subpopulation

Author

Amanpreet Kaur, Luciann Cuenca, Karun Kiani, Gianna T. Busch, Dylan Fingerman, Margaret C. Dunagin, Jingxin Li, Ian Dardani, Eric M. Sanford, Jordan Pemberton, Yogesh Goyal, Ashani T. Weeraratna, Meenhard Herlyn, and Arjun Raj

Abstract

Metastasis occurs when tumor cells leave the primary tumor site and disseminate to distal organs. Even though most cells remain in the primary tumor, the circumstances by which a small fraction of them disseminate remain unclear. Here, we show that a rare, highly invasive subpopulation of melanoma cells can be detected within clonal cell lines due to non-genetic fluctuations in gene expression. The highly invasive phenotype was intrinsic to the cells, independent of their environment, and was marked by transiently high levels ofSEMA3Cexpression, as revealed by RNA-sequencing analysis. Furthermore, the invasive subpopulation drove the bulk dissemination of tumor cells to distal locations in a mouse model of melanoma. The transcription factorNKX2.2regulated the proportion of invasive cells in the melanoma 1205Lu cell line. Furthermore, an overall tradeoff between proliferation and invasion in single cells was observed. Our results suggest that phenotypes like metastasis may arise from intrinsic differences stemming from non-genetic fluctuations between single cells.

Published

2022

18. Pre-determined diversity in resistant fates emerges from homogenous cells after anti-cancer drug treatment

Author

Yogesh Goyal, Ian P. Dardani, Gianna T. Busch, Benjamin Emert, Dylan Fingerman, Amanpreet Kaur, Naveen Jain, Ian A. Mellis, Jingxin Li, Karun Kiani, Mitchell E. Fane, Ashani T. Weeraratna, Meenhard Herlyn, and Arjun Raj

Abstract

Even amongst genetically identical cancer cells, therapy resistance often only emerges from a very small subset of those cells. Much effort has gone into uncovering the molecular differences in rare individual cells in the initial population that may allow certain cells to become therapy resistant; however, comparatively little is known about variability in the resistant outcomes themselves. Here, we develop and apply FateMap, a framework that combines DNA barcoding with single-cell RNA sequencing to reveal the fates of hundreds of thousands of clones exposed to anti-cancer therapies. We show that resistant clones emerging from single-cell-derived cancer cells adopt molecularly, morphologically, and functionally distinct fate types. These different resistant types are largely predetermined by molecular differences between cells before addition of drug and not by extrinsic cell-specific microenvironmental factors. Changes in dose and kind of drug can, however, switch the resistant fate type of an initial cell, even resulting in the generation and elimination of certain fate types. Diversity in resistant fates was observed across several single-cell-derived cancer cell lines and types treated with a variety of drugs. Cell fate diversity as a result of variability in intrinsic cell states may be a generic feature of response to external cues.

Published

2021

19. MFF Regulation of Mitochondrial Cell Death Is a Therapeutic Target in Cancer

Author

Alessandra Martorella, Prashanth Krishna Shastrula, David W. Speicher, Hsin Yao Tang, Dylan Fingerman, Valentina Vaira, Young Chan Chae, Dario C. Altieri, Dmitry I. Gabrilovich, Lucia R. Languino, Andrew V. Kossenkov, Gabriella Gaudioso, Vito W. Rebecca, Yu Geon Lee, Emmanuel Skordalakes, Ekta Agarwal, Jae Ho Seo, Stefano Ferrero, Manuela Caroli, Massimo Giroda, Davide Tosi, Meenhard Herlyn, Min Xiao, and Alessandra Maria Storaci

Subjects

0301 basic medicine, Male, Cancer Research, Programmed cell death, Mitochondrial fission factor, Lung Neoplasms, Peptidomimetic, Apoptosis, Mitochondrion, Mitochondrial Size, Mitochondrial Dynamics, Permeability, Mitochondrial Proteins, 03 medical and health sciences, Mice, 0302 clinical medicine, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Animals, Humans, Chemistry, Voltage-Dependent Anion Channel 1, Cancer, Membrane Proteins, medicine.disease, Xenograft Model Antitumor Assays, Mitochondria, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Mitochondrial Membranes, Cancer research, Mitochondrial fission, Protein Multimerization, VDAC1

Abstract

The regulators of mitochondrial cell death in cancer have remained elusive, hampering the development of new therapies. Here, we showed that protein isoforms of mitochondrial fission factor (MFF1 and MFF2), a molecule that controls mitochondrial size and shape, that is, mitochondrial dynamics, were overexpressed in patients with non–small cell lung cancer and formed homo- and heterodimeric complexes with the voltage-dependent anion channel-1 (VDAC1), a key regulator of mitochondrial outer membrane permeability. MFF inserted into the interior hole of the VDAC1 ring using Arg225, Arg236, and Gln241 as key contact sites. A cell-permeable MFF Ser223-Leu243 d-enantiomeric peptidomimetic disrupted the MFF–VDAC1 complex, acutely depolarized mitochondria, and triggered cell death in heterogeneous tumor types, including drug-resistant melanoma, but had no effect on normal cells. In preclinical models, treatment with the MFF peptidomimetic was well-tolerated and demonstrated anticancer activity in patient-derived xenografts, primary breast and lung adenocarcinoma 3D organoids, and glioblastoma neurospheres. These data identify the MFF–VDAC1 complex as a novel regulator of mitochondrial cell death and an actionable therapeutic target in cancer. Significance: These findings describe mitochondrial fission regulation using a peptidomimetic agent that disturbs the MFF–VDAC complex and displays anticancer activity in multiple tumor models. See related commentary by Rao, p. 6074

Published

2019

20. Disrupting MLV integrase:BET protein interaction biases integration into quiescent chromatin and delays but does not eliminate tumor activation in a MYC/Runx2 mouse model

Author

Jodie Hay, Margaret Bell, Nancy Mackay, Sriram Aiyer, Alan Engelman, Anna Kilbey, Gillian Borland, Christine A. Kozak, James C. Neil, Rodrigo A. Villanueva, Vasudevan Achuthan, Dylan Fingerman, Monica J. Roth, Kathryn Gilroy, Lorenz Loyola, and Ewan R. Cameron

Subjects

Carcinogenesis, viruses, Genes, myc, Gene Expression, Endogenous retrovirus, Core Binding Factor Alpha 1 Subunit, Artificial Gene Amplification and Extension, medicine.disease_cause, Polymerase Chain Reaction, Biochemistry, Mice, Murine leukemia virus, Medicine and Health Sciences, Biology (General), 0303 health sciences, Mammalian Genomics, DNA methylation, biology, Chromosome Biology, 030302 biochemistry & molecular biology, Animal Models, Genomics, Chromatin, 3. Good health, Integrase, Leukemia Virus, Murine, Nucleic acids, Experimental Organism Systems, Oncology, CpG site, Epigenetics, DNA modification, Chromatin modification, Research Article, QH301-705.5, Virus Integration, Genetic Vectors, Immunology, Mice, Transgenic, Mouse Models, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Model Organisms, Virology, Genetics, medicine, Animals, Humans, Molecular Biology Techniques, Protein Interactions, Molecular Biology, 030304 developmental biology, Leukemia, Experimental, Integrases, Wild type, Biology and Life Sciences, Computational Biology, Proteins, Cell Biology, DNA, RC581-607, Genome Analysis, Genomic Libraries, biology.organism_classification, Molecular biology, Disease Models, Animal, Tumor Virus Infections, Animal Genomics, Animal Studies, biology.protein, Parasitology, Immunologic diseases. Allergy, K562 Cells, Retroviridae Infections

Abstract

Murine leukemia virus (MLV) integrase (IN) lacking the C-terminal tail peptide (TP) loses its interaction with the host bromodomain and extraterminal (BET) proteins and displays decreased integration at promoter/enhancers and transcriptional start sites/CpG islands. MLV lacking the IN TP via an altered open reading frame was used to infect tumorigenesis mouse model (MYC/Runx2) animals to observe integration patterns and phenotypic effects, but viral passage resulted in the restoration of the IN TP through small deletions. Mice subsequently infected with an MLV IN lacking the TP coding sequence (TP-) showed an improved median survival by 15 days compared to wild type (WT) MLV infection. Recombination with polytropic endogenous retrovirus (ERV), Pmv20, was identified in seven mice displaying both fast and slow tumorigenesis, highlighting the strong selection within the mouse to maintain the full-length IN protein. Mapping the genomic locations of MLV in tumors from an infected mouse with no observed recombination with ERVs, TP-16, showed fewer integrations at TSS and CpG islands, compared to integrations observed in WT tumors. However, this mouse succumbed to the tumor in relatively rapid fashion (34 days). Analysis of the top copy number integrants in the TP-16 tumor revealed their proximity to known MLV common insertion site genes while maintaining the MLV IN TP- genotype. Furthermore, integration mapping in K562 cells revealed an insertion preference of MLV IN TP- within chromatin profile states associated with weakly transcribed heterochromatin with fewer integrations at histone marks associated with BET proteins (H3K4me1/2/3, and H3K27Ac). While MLV IN TP- showed a decreased overall rate of tumorigenesis compared to WT virus in the MYC/Runx2 model, MLV integration still occurred at regions associated with oncogenic driver genes independently from the influence of BET proteins, either stochastically or through trans-complementation by functional endogenous Gag-Pol protein., Author summary Many different retroviruses, including murine leukemia virus (MLV), are used as vectors for human gene therapy and cancer immunotherapies (CAR-T) because of their stable and efficient delivery of genetic material into the host DNA. However, this process can result in activation and/or disruption of cellular genes, which has resulted in the outgrowth of tumors in previous clinical trials. Of critical importance is the preferred location within the host genome at which the retrovirus integrates. Our study presents a modified MLV virus that has lost the ability to bind to the host BET proteins, the drivers of insertion at promoter/enhancer regions of highly activated genes. This is the first direct study within an animal model to examine whether infection with this type of modified MLV virus affects tumor progression. We found that the modified virus improved the survival of the well-characterized MYC/Runx2 mouse compared to infections with the wild-type MLV. Most modified viral integrants mapped into less active regions of the genome, but some integration events still occurred near cancer-related genes. Thus, while the modified MLV virus can be a safer vector than the wildtype virus, it still maintains the potential to activate oncogenes. This study provides new insights on how to improve the safety of MLV retroviral vectors.

Published

2019