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1. Prediction of infectious diseases using sentiment analysis on social media data.

Author

Youngchul Song and Byungun Yoon

Subjects
Medicine, Science
Abstract

As the influence and risk of infectious diseases increase, efforts are being made to predict the number of confirmed infectious disease patients, but research involving the qualitative opinions of social media users is scarce. However, social data can change the psychology and behaviors of crowds through information dissemination, which can affect the spread of infectious diseases. Existing studies have used the number of confirmed cases and spatial data to predict the number of confirmed cases of infectious diseases. However, studies using opinions from social data that affect changes in human behavior in relation to the spread of infectious diseases are inadequate. Therefore, herein, we propose a new approach for sentiment analysis of social data by using opinion mining and to predict the number of confirmed cases of infectious diseases by using machine learning techniques. To build a sentiment dictionary specialized for predicting infectious diseases, we used Word2Vec to expand the existing sentiment dictionary and calculate the daily sentiment polarity by dividing it into positive and negative polarities from collected social data. Thereafter, we developed an algorithm to predict the number of confirmed infectious patients by using both positive and negative polarities with DNN, LSTM and GRU. The method proposed herein showed that the prediction results of the number of confirmed cases obtained using opinion mining were 1.12% and 3% better than those obtained without using opinion mining in LSTM and GRU model, and it is expected that social data will be used from a qualitative perspective for predicting the number of confirmed cases of infectious diseases.

Published
2024
Full Text
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2. Supplementary Material from mTOR Inhibition Specifically Sensitizes Colorectal Cancers with KRAS or BRAF Mutations to BCL-2/BCL-XL Inhibition by Suppressing MCL-1

Author

Jeffrey A. Engelman, Cyril H. Benes, Kenneth E. Hung, Sridhar Ramaswamy, Miguel N. Rivera, Ryan B. Corcoran, Rakesh K. Jain, David P. Kodack, Jatin Roper, Randy J. Milano, Jessica L. Boisvert, Ah Ting Tam, Youngchul Song, Elena J. Edelman, Alan T. Yeo, Aaron N. Hata, Hiromichi Ebi, Anahita Dastur, Carlotta Costa, Erin M. Coffee, and Anthony C. Faber

Abstract

PDF file140K, Supplementary figure legends

Published
2023

3. Supplementary Figures from mTOR Inhibition Specifically Sensitizes Colorectal Cancers with KRAS or BRAF Mutations to BCL-2/BCL-XL Inhibition by Suppressing MCL-1

Author

Jeffrey A. Engelman, Cyril H. Benes, Kenneth E. Hung, Sridhar Ramaswamy, Miguel N. Rivera, Ryan B. Corcoran, Rakesh K. Jain, David P. Kodack, Jatin Roper, Randy J. Milano, Jessica L. Boisvert, Ah Ting Tam, Youngchul Song, Elena J. Edelman, Alan T. Yeo, Aaron N. Hata, Hiromichi Ebi, Anahita Dastur, Carlotta Costa, Erin M. Coffee, and Anthony C. Faber

Abstract

PDF file 764K, Supp. Figures 1-10 include data describing in vitro and in vivo experiments in support of Faber at al

Published
2023

4. Supplementary Figures 1-10, Tables 1-2 from BIM Expression in Treatment-Naïve Cancers Predicts Responsiveness to Kinase Inhibitors

Author

Jeffrey A. Engelman, Rakesh K. Jain, Dora Dias-Santagata, Miguel N. Rivera, Carlos L. Arteaga, José Baselga, Henry L. Gómez, Cyril H. Benes, Erik J. Coffman, Sylvie Roberge, Eugene Lifshits, Alona Muzikansky, Youngchul Song, Sarah F. Pollack, Subba R. Digumarthy, Joao Incio, Euiheon Chung, Belinda A. Waltman, Lecia V. Sequist, Hiromichi Ebi, Ryan B. Corcoran, and Anthony C. Faber

Abstract

PDF file - 21944K

Published
2023

5. Interview with Dr. Engelman from BIM Expression in Treatment-Naïve Cancers Predicts Responsiveness to Kinase Inhibitors

Author

Jeffrey A. Engelman, Rakesh K. Jain, Dora Dias-Santagata, Miguel N. Rivera, Carlos L. Arteaga, José Baselga, Henry L. Gómez, Cyril H. Benes, Erik J. Coffman, Sylvie Roberge, Eugene Lifshits, Alona Muzikansky, Youngchul Song, Sarah F. Pollack, Subba R. Digumarthy, Joao Incio, Euiheon Chung, Belinda A. Waltman, Lecia V. Sequist, Hiromichi Ebi, Ryan B. Corcoran, and Anthony C. Faber

Abstract

mp3 file (8.8 MB). In the September edition of the Cancer Discovery podcast, Executive Editor Mark Landis talks with Jeffrey A. Engelman about his paper, which suggests that quantitation of pretreatment RNA levels of the pro-apoptotic factor BIM can predict the efficacy of tyrosine kinase inhibitor therapy in oncogene-addicted cancers.

Published
2023

6. Supplementary Table 4 from Activation of PI3K Signaling in Merkel Cell Carcinoma

Author

Dora Dias-Santagata, Jeffrey A. Engelman, James C. Cusack, Anthony J. Iafrate, Mai P. Hoang, Atul K. Bhan, Darrell R. Borger, David P. Ryan, Jeffrey Settleman, Hensin Tsao, Vanessa L. Scialabba, Kristin Bergethon, Beow Y. Yeap, Genevieve M. Boland, Anthony C. Faber, Quynh Lam, Arjola K. Cosper, Juan A. Santamaria-Barria, Youngchul Song, and Valentina Nardi

Abstract

PDF file - 52K

Published
2023

7. Supplementary Table 3 from Activation of PI3K Signaling in Merkel Cell Carcinoma

Author

Dora Dias-Santagata, Jeffrey A. Engelman, James C. Cusack, Anthony J. Iafrate, Mai P. Hoang, Atul K. Bhan, Darrell R. Borger, David P. Ryan, Jeffrey Settleman, Hensin Tsao, Vanessa L. Scialabba, Kristin Bergethon, Beow Y. Yeap, Genevieve M. Boland, Anthony C. Faber, Quynh Lam, Arjola K. Cosper, Juan A. Santamaria-Barria, Youngchul Song, and Valentina Nardi

Abstract

PDF file - 55K

Published
2023

8. Data from Ponatinib Inhibits Polyclonal Drug-Resistant KIT Oncoproteins and Shows Therapeutic Potential in Heavily Pretreated Gastrointestinal Stromal Tumor (GIST) Patients

Author

Victor M. Rivera, Sebastian Bauer, Jonathan A. Fletcher, Michael C. Heinrich, Tim Clackson, Frank Wang, Anna Kohlmann, Youngchul Song, Yaoyu Ning, Scott Wardwell, Julia Ketzer, Meijun Zhu, Grant Eilers, Cesar Serrano, Tianjun Zhou, Alexa Schrock, Sadanand Vodala, Rana Anjum, Joseph M. Gozgit, and Andrew P. Garner

Abstract

Purpose: KIT is the major oncogenic driver of gastrointestinal stromal tumors (GIST). Imatinib, sunitinib, and regorafenib are approved therapies; however, efficacy is often limited by the acquisition of polyclonal secondary resistance mutations in KIT, with those located in the activation (A) loop (exons 17/18) being particularly problematic. Here, we explore the KIT-inhibitory activity of ponatinib in preclinical models and describe initial characterization of its activity in patients with GIST.Experimental Design: The cellular and in vivo activities of ponatinib, imatinib, sunitinib, and regorafenib against mutant KIT were evaluated using an accelerated mutagenesis assay and a panel of engineered and GIST-derived cell lines. The ponatinib–KIT costructure was also determined. The clinical activity of ponatinib was examined in three patients with GIST previously treated with all three FDA-approved agents.Results: In engineered and GIST-derived cell lines, ponatinib potently inhibited KIT exon 11 primary mutants and a range of secondary mutants, including those within the A-loop. Ponatinib also induced regression in engineered and GIST-derived tumor models containing these secondary mutations. In a mutagenesis screen, 40 nmol/L ponatinib was sufficient to suppress outgrowth of all secondary mutants except V654A, which was suppressed at 80 nmol/L. This inhibitory profile could be rationalized on the basis of structural analyses. Ponatinib (30 mg daily) displayed encouraging clinical activity in two of three patients with GIST.Conclusion:Ponatinib possesses potent activity against most major clinically relevant KIT mutants and has demonstrated preliminary evidence of activity in patients with refractory GIST. These data strongly support further evaluation of ponatinib in patients with GIST. Clin Cancer Res; 20(22); 5745–55. ©2014 AACR.

Published
2023

10. Supplementary Table 1 from Activation of PI3K Signaling in Merkel Cell Carcinoma

Author

Dora Dias-Santagata, Jeffrey A. Engelman, James C. Cusack, Anthony J. Iafrate, Mai P. Hoang, Atul K. Bhan, Darrell R. Borger, David P. Ryan, Jeffrey Settleman, Hensin Tsao, Vanessa L. Scialabba, Kristin Bergethon, Beow Y. Yeap, Genevieve M. Boland, Anthony C. Faber, Quynh Lam, Arjola K. Cosper, Juan A. Santamaria-Barria, Youngchul Song, and Valentina Nardi

Abstract

PDF file - 25K

Published
2023

11. Supplementary methods, patient information and figure legends from Ponatinib Inhibits Polyclonal Drug-Resistant KIT Oncoproteins and Shows Therapeutic Potential in Heavily Pretreated Gastrointestinal Stromal Tumor (GIST) Patients

Author

Victor M. Rivera, Sebastian Bauer, Jonathan A. Fletcher, Michael C. Heinrich, Tim Clackson, Frank Wang, Anna Kohlmann, Youngchul Song, Yaoyu Ning, Scott Wardwell, Julia Ketzer, Meijun Zhu, Grant Eilers, Cesar Serrano, Tianjun Zhou, Alexa Schrock, Sadanand Vodala, Rana Anjum, Joseph M. Gozgit, and Andrew P. Garner

Abstract

Supplementary methods, patient information and figure legends

Published
2023

12. Data from The Potent ALK Inhibitor Brigatinib (AP26113) Overcomes Mechanisms of Resistance to First- and Second-Generation ALK Inhibitors in Preclinical Models

Author

Victor M. Rivera, William C. Shakespeare, David Dalgarno, Tim Clackson, Xiaotian Zhu, Juan Miret, Frank Wang, Narayana Narasimhan, Emily Ye, Hyun Gyung Jang, Qurish Mohemmad, Yihan Wang, Dong Zou, Shuangying Liu, Wei-Sheng Huang, Lauren Moran, Lindsey Eichinger, Youngchul Song, David Miller, Scott D. Wardwell, Yaoyu Ning, Jeff Keats, Tianjun Zhou, Sara Nadworny, Rachel Squillace, Rana Anjum, and Sen Zhang

Abstract

Purpose: Non–small cell lung cancers (NSCLCs) harboring ALK gene rearrangements (ALK+) typically become resistant to the first-generation anaplastic lymphoma kinase (ALK) tyrosine kinase inhibitor (TKI) crizotinib through development of secondary resistance mutations in ALK or disease progression in the brain. Mutations that confer resistance to second-generation ALK TKIs ceritinib and alectinib have also been identified. Here, we report the structure and first comprehensive preclinical evaluation of the next-generation ALK TKI brigatinib.Experimental Design: A kinase screen was performed to evaluate the selectivity profile of brigatinib. The cellular and in vivo activities of ALK TKIs were compared using engineered and cancer-derived cell lines. The brigatinib–ALK co-structure was determined.Results: Brigatinib potently inhibits ALK and ROS1, with a high degree of selectivity over more than 250 kinases. Across a panel of ALK+ cell lines, brigatinib inhibited native ALK (IC50, 10 nmol/L) with 12-fold greater potency than crizotinib. Superior efficacy of brigatinib was also observed in mice with ALK+ tumors implanted subcutaneously or intracranially. Brigatinib maintained substantial activity against all 17 secondary ALK mutants tested in cellular assays and exhibited a superior inhibitory profile compared with crizotinib, ceritinib, and alectinib at clinically achievable concentrations. Brigatinib was the only TKI to maintain substantial activity against the most recalcitrant ALK resistance mutation, G1202R. The unique, potent, and pan-ALK mutant activity of brigatinib could be rationalized by structural analyses.Conclusions: Brigatinib is a highly potent and selective ALK inhibitor. These findings provide the molecular basis for the promising activity being observed in ALK+, crizotinib-resistant patients with NSCLC being treated with brigatinib in clinical trials. Clin Cancer Res; 22(22); 5527–38. ©2016 AACR.

Published
2023

14. Supplementary Figure 2 from Human Breast Cancer Cells Harboring a Gatekeeper T798M Mutation in HER2 Overexpress EGFR Ligands and Are Sensitive to Dual Inhibition of EGFR and HER2

Author

Carlos L. Arteaga, Jeffrey A. Engelman, Youngchul Song, Anindita Chakrabarty, Mónica Valeria Estrada, Archana Narasanna, Ritwik Ghosh, and Brent N. Rexer

Abstract

Supplementary Figure 2 - PDF file 141K, Expression of T798M HER2 results in increased HER3 phosphorylation and HER3-p85 association

Published
2023

17. Supplementary Figure 1 from Human Breast Cancer Cells Harboring a Gatekeeper T798M Mutation in HER2 Overexpress EGFR Ligands and Are Sensitive to Dual Inhibition of EGFR and HER2

Author

Carlos L. Arteaga, Jeffrey A. Engelman, Youngchul Song, Anindita Chakrabarty, Mónica Valeria Estrada, Archana Narasanna, Ritwik Ghosh, and Brent N. Rexer

Abstract

Supplementary Figure 1 - PDF file 189K, Pan-ErbB inhibitor CI-1033 inhibits HER2 phosphorylation and cell growth of both wild-type and T798M mutant cells

Published
2023

19. Data from Activation of PI3K Signaling in Merkel Cell Carcinoma

Author

Dora Dias-Santagata, Jeffrey A. Engelman, James C. Cusack, Anthony J. Iafrate, Mai P. Hoang, Atul K. Bhan, Darrell R. Borger, David P. Ryan, Jeffrey Settleman, Hensin Tsao, Vanessa L. Scialabba, Kristin Bergethon, Beow Y. Yeap, Genevieve M. Boland, Anthony C. Faber, Quynh Lam, Arjola K. Cosper, Juan A. Santamaria-Barria, Youngchul Song, and Valentina Nardi

Abstract

Purpose: Merkel cell carcinoma (MCC) is an aggressive cutaneous neuroendocrine tumor, often metastatic at presentation, for which current chemotherapeutic regimens are largely ineffective. As its pathogenesis is still unknown, we hypothesized that deregulation of signaling pathways commonly activated in cancer may contribute to MCC tumorigenesis and may provide insights into targeted therapy approaches for this malignancy.Experimental Design: We retrospectively profiled 60 primary MCC samples using a SNaPshot-based tumor genotyping assay to screen for common mutations in 13 cancer genes.Results: We identified mutations in 9 (15%) MCC primary tumors, including mutations in TP53 (3 of 60) and activating mutations in the PIK3CA gene (6 of 60). Sanger sequencing of the primary MCC tumors detected one additional PIK3CA mutation (R19K) that had not been previously described in cancer. Merkel cell polyoma virus (MCPyV) was detected in 38 (66%) MCC cases and patients with MCPyV-positive cancers showed a trend toward better survival. With one exception, the presence of MCPyV and activating mutations in PIK3CA appeared mutually exclusive. We observed that signaling through the PI3K/pAKT pathway was active in one MCPyV-positive and in all MCPyV-negative MCC cell lines, as evidenced by AKT phosphorylation. Importantly, the presence of a PIK3CA-activating mutation was associated with sensitivity to treatment with ZST474, a specific phosphoinositide 3-kinase (PI3K) inhibitor, and to NVP-BEZ235, a dual PI3K/mTOR inhibitor, targeted agents under active clinical development.Conclusions: PI3K pathway activation may drive tumorigenesis in a subset of MCC and screening these tumors for PIK3CA mutations could help identify patients who may respond to treatment with PI3K pathway inhibitors. Clin Cancer Res; 18(5); 1227–36. ©2012 AACR.

Published
2023

20. Data from Human Breast Cancer Cells Harboring a Gatekeeper T798M Mutation in HER2 Overexpress EGFR Ligands and Are Sensitive to Dual Inhibition of EGFR and HER2

Author

Carlos L. Arteaga, Jeffrey A. Engelman, Youngchul Song, Anindita Chakrabarty, Mónica Valeria Estrada, Archana Narasanna, Ritwik Ghosh, and Brent N. Rexer

Abstract

Purpose: Mutations in receptor tyrosine kinase (RTK) genes can confer resistance to receptor-targeted therapies. A T798M mutation in the HER2 oncogene has been shown to confer resistance to the tyrosine kinase inhibitor (TKI) lapatinib. We studied the mechanisms of HER2-T798M–induced resistance to identify potential strategies to overcome that resistance.Experimental Design: HER2-T798M was stably expressed in BT474 and MCF10A cells. Mutant cells and xenografts were evaluated for effects of the mutation on proliferation, signaling, and tumor growth after treatment with combinations of inhibitors targeting the EGFR/HER2/HER3/PI3K axis.Results: A low 3% allelic frequency of the T798M mutant shifted 10-fold the IC50 of lapatinib. In mutant-expressing cells, lapatinib did not block basal phosphorylation of HER2, HER3, AKT, and ERK1/2. In vitro kinase assays showed increased autocatalytic activity of HER2-T798M. HER3 association with PI3K p85 was increased in mutant-expressing cells. BT474-T798M cells were also resistant to the HER2 antibody trastuzumab. These cells were sensitive to the pan-PI3K inhibitors BKM120 and XL147 and the irreversible HER2/EGFR TKI afatinib but not the MEK1/2 inhibitor CI-1040, suggesting continued dependence of the mutant cells on ErbB receptors and downstream PI3K signaling. BT474-T798M cells showed increased expression of the EGFR ligands EGF, TGFα, amphiregulin, and HB-EGF. Addition of the EGFR neutralizing antibody cetuximab or lapatinib restored trastuzumab sensitivity of BT474-T798M cells and xenografts, suggesting that increased EGFR ligand production was causally associated with drug resistance.Conclusions: Simultaneous blockade of HER2 and EGFR should be an effective treatment strategy against HER2 gene–amplified breast cancer cells harboring T798M mutant alleles. Clin Cancer Res; 19(19); 5390–401. ©2013 AACR.

Published
2023

21. Supplementary Tables from Ponatinib Inhibits Polyclonal Drug-Resistant KIT Oncoproteins and Shows Therapeutic Potential in Heavily Pretreated Gastrointestinal Stromal Tumor (GIST) Patients

Author

Victor M. Rivera, Sebastian Bauer, Jonathan A. Fletcher, Michael C. Heinrich, Tim Clackson, Frank Wang, Anna Kohlmann, Youngchul Song, Yaoyu Ning, Scott Wardwell, Julia Ketzer, Meijun Zhu, Grant Eilers, Cesar Serrano, Tianjun Zhou, Alexa Schrock, Sadanand Vodala, Rana Anjum, Joseph M. Gozgit, and Andrew P. Garner

Abstract

Supplementary Tables. Table S1. In Vitro Kinase IC50 Values (nM) for Native and Mutant Recombinant KIT. Table S2. Summary of Ba/F3 KIT Cell Lines Generated in this Study. Table S3. Summary of IC50 Viability Values in Ba/F3 KIT Cells. Table S4. Summary of KIT Driven Ba/F3 In Vivo Studies.

Published
2023

22. Supplementary Table 2 from Activation of PI3K Signaling in Merkel Cell Carcinoma

Author

Dora Dias-Santagata, Jeffrey A. Engelman, James C. Cusack, Anthony J. Iafrate, Mai P. Hoang, Atul K. Bhan, Darrell R. Borger, David P. Ryan, Jeffrey Settleman, Hensin Tsao, Vanessa L. Scialabba, Kristin Bergethon, Beow Y. Yeap, Genevieve M. Boland, Anthony C. Faber, Quynh Lam, Arjola K. Cosper, Juan A. Santamaria-Barria, Youngchul Song, and Valentina Nardi

Abstract

PDF file - 62K

Published
2023

23. Supplementary Figures from Ponatinib Inhibits Polyclonal Drug-Resistant KIT Oncoproteins and Shows Therapeutic Potential in Heavily Pretreated Gastrointestinal Stromal Tumor (GIST) Patients

Author

Victor M. Rivera, Sebastian Bauer, Jonathan A. Fletcher, Michael C. Heinrich, Tim Clackson, Frank Wang, Anna Kohlmann, Youngchul Song, Yaoyu Ning, Scott Wardwell, Julia Ketzer, Meijun Zhu, Grant Eilers, Cesar Serrano, Tianjun Zhou, Alexa Schrock, Sadanand Vodala, Rana Anjum, Joseph M. Gozgit, and Andrew P. Garner

Abstract

Supplementary Figures. Figure S1. Chemical structures of imatinib, sunitinib, regorafenib and ponatinib. Figure S2. Expression and activation of KIT in engineered Ba/F3 cells. Figure S3. Ponatinib inhibits the phosphorylation of exon 11primary activating, and secondary resistant mutant forms of KIT. Figure S4. Secondary mutants reduce ponatinib potency in Ex9 ins and V560D cell lines. Figure S5. Illustration of the optimal fit of ponatinib to KIT. Figure S6. Impact of compound treatment on KIT signaling in GIST-derived cell lines.

Published
2023

24. Supplementary Methods, Supplementary Results, Supplementary Table 1, Supplementary Figures 1-8 from The Potent ALK Inhibitor Brigatinib (AP26113) Overcomes Mechanisms of Resistance to First- and Second-Generation ALK Inhibitors in Preclinical Models

Author

Victor M. Rivera, William C. Shakespeare, David Dalgarno, Tim Clackson, Xiaotian Zhu, Juan Miret, Frank Wang, Narayana Narasimhan, Emily Ye, Hyun Gyung Jang, Qurish Mohemmad, Yihan Wang, Dong Zou, Shuangying Liu, Wei-Sheng Huang, Lauren Moran, Lindsey Eichinger, Youngchul Song, David Miller, Scott D. Wardwell, Yaoyu Ning, Jeff Keats, Tianjun Zhou, Sara Nadworny, Rachel Squillace, Rana Anjum, and Sen Zhang

Abstract

Supplementary Table 1. Brigatinib in vitro activity (IC50s) in a kinase panel (N=289); Supplementary Figure 1. Chemical structures of brigatinib, crizotinib, ceritinib, and alectinib; Supplementary Figure 2. Brigatinib-mediated inhibition of native or mutant ALK-, ROS1-,FLT3-, and EGFR-driven tumor activity in vitro; Supplementary Figure 3. Cellular and in vivo activity of brigatinib in ROS1 harboring models, compared with crizotinib; Supplementary Figure 4. Comparison of IGF-1R and INSR inhibitory activity of brigatinib with NVP-TAE684; Supplementary Figure 5. Inhibition of ALK phosphorylation in ALK+ cellular models by brigatinib, compared with crizotinib; Supplementary Figure 6. Inhibition of ALK phosphorylation and downstream signaling, and tolerability of brigatinib in vivo, compared with crizotinib; Supplementary Figure 7. TKI activity against parental, and native and mutant EML4-ALK driven Ba/F3 cells; Supplementary Figure 8. TKI antitumor activity against native and mutant EML4-ALK tumors, TKI plasma levels, and tolerability, in vivo.

Published
2023

25. Supplementary Methods, Figures 1-8, Table 1 from An ErbB3 Antibody, MM-121, Is Active in Cancers with Ligand-Dependent Activation

Author

Kwok-Kin Wong, Jeffrey A. Engelman, Ulrik B. Nielsen, Youngchul Song, Aaron Fulgham, Lin Nie, Zandra Walton, Emily Pace, Olga Burenkova, Matthew Onsum, Katherine Crosby, Mei-Chih Liang, Danan Li, Anthony C. Faber, and Birgit Schoeberl

Abstract

Supplementary Methods, Figures 1-8, Table 1 from An ErbB3 Antibody, MM-121, Is Active in Cancers with Ligand-Dependent Activation

Published
2023

26. Supplementary Materials and Methods from MEK Inhibition Leads to PI3K/AKT Activation by Relieving a Negative Feedback on ERBB Receptors

Author

Jeffrey A. Engelman, John M. Asara, Carlos L. Arteaga, Rebecca Cook, Carlotta Costa, Youngchul Song, and Alexa B. Turke

Abstract

PDF file - 104K, Supplemental Materials and Methods include additional materials and methods and supporting references, and provides more detailed explanation of cell lines and cell culture reagents, antibodies, shRNA haripin constructs, and mass spectrometry protocol.

Published
2023

29. Supplementary Figures 1 - 10 from Cytotoxic Activity of Tivantinib (ARQ 197) Is Not Due Solely to c-MET Inhibition

Author

Naoya Fujita, Jeffrey A. Engelman, Youngchul Song, Tomoko Oh-hara, Jie Qi, Takao Yamori, Aki Aoyama, and Ryohei Katayama

Abstract

PDF file - 800K, c-Met dependency of the used cell lines (S1); Antitumor activity of tivantinib on c-Met-non-addicted tumor cells (S2); Change in c-Met signaling after exposure to Tivantinib or Crizotinib for 24h (S3); Tivantinib did not inhibit c-MET activation in A549 cells (S4); Apoptosis induction by Tivantinib long time treatment in EBC-1 and MKN45 cells (S5); Tivantinib induces G2/M arrest as similar as tubulin inhibitor vincristine (S6); Growth inhibition against a panel of 39 human cancer cell lines by vincristine (S7); Tivantinib treatment led to a loss of microtubules in EBC1 cells (S8); Tivantinib short time treatment led to a loss of microtubules in A549 and EBC-1 cells (S9); Tivantinib inhibits tubulin polymerization in a dose dependent manner (S10).

Published
2023

31. Supplementary Figures 1-8 from MEK Inhibition Leads to PI3K/AKT Activation by Relieving a Negative Feedback on ERBB Receptors

Author

Jeffrey A. Engelman, John M. Asara, Carlos L. Arteaga, Rebecca Cook, Carlotta Costa, Youngchul Song, and Alexa B. Turke

Abstract

PDF file - 515K, Supplemenal figures 1-8 support the main figures in the manuscript, and include characterization of compounds and target inhibition, quantification of ERBB3 mRNA and HRG ligand, cell line characterization, and data supporting mass spectrometry experiments.

Published
2023

33. RET fusions observed in lung and colorectal cancers are sensitive to ponatinib

Author

Frank Wang, Henrik Edgren, Jie Cai, Justin R. Pritchard, Tzu Hsiu Chen, Joseph M. Gozgit, Henry Li, Victor M. Rivera, Youngchul Song, and Scott Wardwell

Subjects
0301 basic medicine, endocrine system, endocrine system diseases, Colorectal cancer, medicine.drug_class, medicine.medical_treatment, Cell, Genomics, colorectal cancer, Tyrosine-kinase inhibitor, Targeted therapy, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, tyrosine kinase inhibitor, medicine, ponatinib, Kinase activity, non-small cell lung cancer, Lung, business.industry, Ponatinib, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, 030220 oncology & carcinogenesis, Cancer research, business, RET, Research Paper
Abstract

Genomic studies are revolutionizing clinical oncology, but bridging the lab and the bedside requires the ability to efficiently interrogate rare genetic lesions in unexpected pathological settings using preclinical models. Oncogenes can exhibit intrinsic drug resistance to targeted therapy in different cells of origin, adding complexity to clinical interpretations of genomic findings. Here, we capitalize on the flexibility of engineered cell systems to rapidly profile known multi-kinase inhibitors that harbor rearranged during transfection (RET) kinase activity across multiple RET fusions. Identifying ponatinib as the most potent RET inhibitor tested, we used ponatinib to gauge therapeutic responsiveness in RET fusion-positive patient-derived xenograft (PDX) models. Using a genomics guided outlier approach, we identified 4 RET fusion PDX models with 3 different fusion partners (KIF5B, CCDC6, and NCOA4) in both non-small cell lung cancer and colorectal cancer. By comparing ponatinib activity in RET fusion-positive and RET fusion-negative PDX models alongside a standard of care chemotherapeutic agent, we show that RET fusions in colorectal tumors are therapeutically responsive to RET inhibition. Finally, we suggest that coupling engineered cell systems and genomics guided PDX model selection provides a rapid workflow to triage rare genomics findings.

Published
2018

34. Abstract PO-100: Expressed molecular barcoding coupled with single cell RNAseq enables a high resolution investigation into the evolution of drug tolerance

Author

Joel Wagner, Gaylor Boulay, Youngchul Song, Erick Morris, Peter S. Hammerman, Viveksagar Krisnamurthy Radhakrishna, Matthew J. Niederst, Jennifer L. Cotton, Xiaoyan Li, Michelle Piquet, Jeffrey A. Engelman, Katja Schumacher, Kathleen Sprouffske, Joshua M. Korn, David A. Ruddy, and Javier Estrada Diez

Subjects
Cancer Research, education.field_of_study, Mechanism (biology), Population, Computational biology, Biology, Somatic evolution in cancer, Minimal residual disease, Oncology, Drug tolerance, biology.protein, Epigenetics, Epidermal growth factor receptor, education, EGFR inhibitors
Abstract

EGFR targeted kinase inhibitors (TKIs) are the standard of care in non-small cell lung cancer (NSCLC) patients with activating mutations in the epidermal growth factor receptor (EGFR). Patients initially respond well to EGFR inhibitors, although the majority only achieve a partial response and a subset of drug-tolerant persister cells remain at minimal residual disease (MRD). These drug-tolerant persister cells represent a cell reservoir from which de novo genetic mutations, such as EGFRT790M or MET amplification, can arise to render the tumor fully drug-resistant. Previous studies suggest that drug-tolerant cells rely on an altered chromatin state to survive EGFR-inhibition. However, it is still unclear whether the drug-tolerant cell population emerges through selection for cells that pre-existed in that state or through and adaptation in response to drug. It is also unknown if drug-tolerant persister cells rely on a single survival mechanism that could be exploited to more effectively target this population or if multiple independent mechanisms are being utilized and need to be targeted to fully suppress drug tolerance. Despite the urgent clinical need to answer these questions, we have lacked the techniques capable of the dynamic resolution necessary to investigate the emergence of drug tolerance throughout the course of treatment within individual cell lineages. Here we present a strategy to investigate the clonal evolution of drug tolerance in EGFRmut NSCLC using an expressed molecular barcoding library coupled with single cell RNAseq (scRNAseq). We found that the cell lineages that are destined to become drug-tolerant are pre-defined, although the epigenetic drug-tolerant state does not pre-exist. We observed multiple distinct heterogeneous classes of drug-tolerant cells with unique gene expression signatures as well as distinct trajectories in response to EGFRi. We observed evidence of putative mechanisms of drug tolerance, such as EMT and adaptive MAPK signaling, in parallel trajectory classes across cell lines. Finally, we compared EGFRi/TKI drug combinations versus EGFRi/chemotherapy combinations to investigate which therapeutic approach was more efficacious in targeting multiple trajectory classes of drug tolerant cells. Taken together, our work presents a new technology that enables a comprehensive interrogation of drug response over time and provides greater insight into how drug-tolerant cells evolve over the course of drug treatment, which ultimately can help inform combination treatment strategies for patients in the clinic. Citation Format: Jennifer L. Cotton, Viveksagar Krisnamurthy Radhakrishna, Javier Estrada Diez, David A. Ruddy, Kathleen Sprouffske, Gaylor Boulay, Michelle Piquet, Joel Wagner, Youngchul Song, Xiaoyan Li, Katja Schumacher, Joshua Korn, Erick J. Morris, Peter S. Hammerman, Jeffrey A. Engelman, Matthew J. Niederst. Expressed molecular barcoding coupled with single cell RNAseq enables a high resolution investigation into the evolution of drug tolerance [abstract]. In: Proceedings of the AACR Virtual Special Conference on Tumor Heterogeneity: From Single Cells to Clinical Impact; 2020 Sep 17-18. Philadelphia (PA): AACR; Cancer Res 2020;80(21 Suppl):Abstract nr PO-100.

Published
2020

35. Abstract A122: Molecular barcoding and single cell approaches to investigate drug tolerance in EGFRmut NSCLC

Author

Viveksagar KrishnamurthyRadhakrishna, Joshua M. Korn, Raphael Thierry, Joel Wagner, Julie Chen, Xiaoyan Li, Gaylor Boulay, David A. Ruddy, Erick Morris, Youngchul Song, Nathaniel D. Kirkpatrick, Jeffrey A. Engelman, Matthew J. Niederst, Jennifer L. Cotton, Michelle Piquet, Katja Schumacher, Kathleen Sprouffske, and Peter S. Hammerman

Subjects
Cancer Research, education.field_of_study, biology, medicine.medical_treatment, Cell, Population, Cancer, medicine.disease, Minimal residual disease, Targeted therapy, medicine.anatomical_structure, Oncology, medicine, Cancer research, biology.protein, Epidermal growth factor receptor, education, Tyrosine kinase, EGFR inhibitors
Abstract

Patients with non-small cell lung cancer (NSCLC) that is driven by an activating mutation in the epidermal growth factor receptor (EGFR) are routinely treated with tyrosine kinase inhibitors (TKI) to specifically target the activated EGFR signaling pathway. EGFR-mutant NSCLC tumors initially respond well to EGFR inhibitors, however a subset of drug-tolerant persister cells remain at minimal residual disease (MRD) and represent a cell reservoir from which acquired genetic mutations, such as EGFRT790M or MET amplification, can emerge to render the tumor fully drug-resistant. Prior to the emergence of genetic mutations, little is known about how drug-tolerant persister cells are able to survive EGFR targeted therapy at MRD. To better understand this cell population, we investigated drug-tolerance using single cell cloning and scRNAseq in NSCLC cell lines. Using ClonTracer barcoding, we found that the same barcodes emerged after EGFR-inhibitor treatment across multiple replicates, indicating that drug-tolerance is both pre-defined and stable over many generations. Within each individual cell line, we observed multiple distinct heterogeneous subpopulations of drug-tolerant persister cells with unique gene expression signatures and proliferation rates. Additionally, we observed evidence of putative mechanisms of drug tolerance that were shared by persister cells across cells lines and used a drug combination treatment approach to target these distinct subpopulations of drug-tolerant persister cells. Taken together, our findings provide evidence that drug-tolerant persister cell subpopulations are both predefined and heterogeneous, as well as suggesting that drug-combination treatment approaches in the clinic would be more effective at targeting multiple persister cell survival mechanisms. Citation Format: Jennifer L. Cotton, Viveksagar KrishnamurthyRadhakrishna, Julie Chen, Michelle Piquet, Joel Wagner, Gaylor Boulay, Kathleen Sprouffske, Youngchul Song, Xiaoyan Li, Katja Schumacher, Raphael Thierry, Nathaniel D. Kirkpatrick, David A. Ruddy, Joshua Korn, Erick J. Morris, Peter S. Hammerman, Jeffrey A. Engelman, Matthew J. Niederst. Molecular barcoding and single cell approaches to investigate drug tolerance in EGFRmut NSCLC [abstract]. In: Proceedings of the AACR-NCI-EORTC International Conference on Molecular Targets and Cancer Therapeutics; 2019 Oct 26-30; Boston, MA. Philadelphia (PA): AACR; Mol Cancer Ther 2019;18(12 Suppl):Abstract nr A122. doi:10.1158/1535-7163.TARG-19-A122

Published
2019

36. Ponatinib Inhibits Polyclonal Drug-Resistant KIT Oncoproteins and Shows Therapeutic Potential in Heavily Pretreated Gastrointestinal Stromal Tumor (GIST) Patients

Author

Sebastian Bauer, Joseph M. Gozgit, Scott Wardwell, Frank Wang, Meijun Zhu, Julia Ketzer, Michael Heinrich, César Serrano, Andrew P. Garner, Grant Eilers, Yaoyu Ning, Tianjun Zhou, Victor M. Rivera, Jonathan A. Fletcher, Sadanand Vodala, Alexa B. Schrock, Anna Kohlmann, Youngchul Song, Rana Anjum, and Tim Clackson

Subjects
Models, Molecular, Cancer Research, Indoles, Medizin, Molecular Conformation, Pharmacology, Piperazines, chemistry.chemical_compound, Sunitinib, Stromal tumor, GiST, Ponatinib, Imidazoles, Exons, Tumor Burden, Pyridazines, Proto-Oncogene Proteins c-kit, Oncology, Benzamides, Imatinib Mesylate, Female, Protein Binding, medicine.drug, Gastrointestinal Stromal Tumors, Antineoplastic Agents, Biology, Article, Inhibitory Concentration 50, Cell Line, Tumor, Regorafenib, medicine, Animals, Humans, Pyrroles, Protein Kinase Inhibitors, neoplasms, Dose-Response Relationship, Drug, Cancer, Imatinib, medicine.disease, Xenograft Model Antitumor Assays, digestive system diseases, Disease Models, Animal, Pyrimidines, Imatinib mesylate, chemistry, Drug Resistance, Neoplasm, Mutation, Neoplasm Recurrence, Local, Tomography, X-Ray Computed
Abstract

Purpose: KIT is the major oncogenic driver of gastrointestinal stromal tumors (GIST). Imatinib, sunitinib, and regorafenib are approved therapies; however, efficacy is often limited by the acquisition of polyclonal secondary resistance mutations in KIT, with those located in the activation (A) loop (exons 17/18) being particularly problematic. Here, we explore the KIT-inhibitory activity of ponatinib in preclinical models and describe initial characterization of its activity in patients with GIST. Experimental Design: The cellular and in vivo activities of ponatinib, imatinib, sunitinib, and regorafenib against mutant KIT were evaluated using an accelerated mutagenesis assay and a panel of engineered and GIST-derived cell lines. The ponatinib–KIT costructure was also determined. The clinical activity of ponatinib was examined in three patients with GIST previously treated with all three FDA-approved agents. Results: In engineered and GIST-derived cell lines, ponatinib potently inhibited KIT exon 11 primary mutants and a range of secondary mutants, including those within the A-loop. Ponatinib also induced regression in engineered and GIST-derived tumor models containing these secondary mutations. In a mutagenesis screen, 40 nmol/L ponatinib was sufficient to suppress outgrowth of all secondary mutants except V654A, which was suppressed at 80 nmol/L. This inhibitory profile could be rationalized on the basis of structural analyses. Ponatinib (30 mg daily) displayed encouraging clinical activity in two of three patients with GIST. Conclusion:Ponatinib possesses potent activity against most major clinically relevant KIT mutants and has demonstrated preliminary evidence of activity in patients with refractory GIST. These data strongly support further evaluation of ponatinib in patients with GIST. Clin Cancer Res; 20(22); 5745–55. ©2014 AACR.

Published
2014

37. mTOR Inhibition Specifically Sensitizes Colorectal Cancers with KRAS or BRAF Mutations to BCL-2/BCL-XL Inhibition by Suppressing MCL-1

Author

Kenneth E. Hung, Sridhar Ramaswamy, Erin M. Coffee, Cyril H. Benes, Carlotta Costa, Aaron N. Hata, Youngchul Song, Miguel Rivera, Hiromichi Ebi, Rakesh K. Jain, Anthony C. Faber, Ah Ting Tam, Randy J. Milano, Ryan B. Corcoran, Anahita Dastur, Jessica L. Boisvert, Alan T. Yeo, David P. Kodack, Elena J. Edelman, Jatin Roper, and Jeffrey A. Engelman

Subjects
Proto-Oncogene Proteins B-raf, Colorectal cancer, Morpholines, medicine.medical_treatment, bcl-X Protein, Mice, Nude, Antineoplastic Agents, Mechanistic Target of Rapamycin Complex 2, mTORC1, Mechanistic Target of Rapamycin Complex 1, Biology, medicine.disease_cause, Article, Targeted therapy, Proto-Oncogene Proteins p21(ras), Mice, chemistry.chemical_compound, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Animals, Humans, Protein Kinase Inhibitors, neoplasms, PI3K/AKT/mTOR pathway, Sulfonamides, Mutation, Aniline Compounds, Navitoclax, TOR Serine-Threonine Kinases, medicine.disease, Mice, Mutant Strains, digestive system diseases, Proto-Oncogene Proteins c-bcl-2, Oncology, chemistry, Apoptosis, Multiprotein Complexes, ras Proteins, Cancer research, Myeloid Cell Leukemia Sequence 1 Protein, KRAS, Colorectal Neoplasms
Abstract

Colorectal cancers harboring KRAS or BRAF mutations are refractory to current targeted therapies. Using data from a high-throughput drug screen, we have developed a novel therapeutic strategy that targets the apoptotic machinery using the BCL-2 family inhibitor ABT-263 (navitoclax) in combination with a TORC1/2 inhibitor, AZD8055. This combination leads to efficient apoptosis specifically in KRAS- and BRAF-mutant but not wild-type (WT) colorectal cancer cells. This specific susceptibility results from TORC1/2 inhibition leading to suppression of MCL-1 expression in mutant, but not WT, colorectal cancers, leading to abrogation of BIM/MCL-1 complexes. This combination strategy leads to tumor regressions in both KRAS-mutant colorectal cancer xenograft and genetically engineered mouse models of colorectal cancer, but not in the corresponding KRAS-WT colorectal cancer models. These data suggest that the combination of BCL-2/BCL-XL inhibitors with TORC1/2 inhibitors constitutes a promising targeted therapy strategy to treat these recalcitrant cancers. Significance: Effective targeted therapies directed against colorectal cancer with activating mutations in KRAS remain elusive. We have leveraged drug-screen data from a large panel of human colorectal cancers to uncover an effective, rational targeted therapy strategy that has preferential activity in colorectal cancers with KRAS or BRAF mutations. This combination may be developed for clinical testing. Cancer Discov; 4(1); 42–52. ©2013 AACR. See related commentary by Russo et al., p. 19 This article is highlighted in the In This Issue feature, p. 1

Published
2014

38. Geometric and electronic properties of porphyrin molecules on Au(111) and NaCl surfaces

Author

Youngchul Song, Seong Heon Kim, Seong Joon Lim, Hae-Seong Jeong, Young Kuk, Jaejun Yu, and U.D. Ham

Subjects
Sodium, Scanning tunneling spectroscopy, Analytical chemistry, chemistry.chemical_element, Surfaces and Interfaces, Condensed Matter Physics, Porphyrin, Surfaces, Coatings and Films, law.invention, chemistry.chemical_compound, chemistry, law, Materials Chemistry, Molecule, Physical chemistry, Density functional theory, Scanning tunneling microscope, Platinum, HOMO/LUMO
Abstract

Geometric and electronic properties of platinum octaethyl porphyrin (PtOEP) molecules on thin insulating sodium chloride (NaCl) and bare Au(111) surfaces are studied using scanning tunneling microscopy and scanning tunneling spectroscopy (STS). In the STS study, a slight downward shift of a highest occupied molecular orbital peak is observed for a PtOEP molecule on NaCl(100)/Au(111). Density functional theory calculations for PtOEP molecules on the NaCl(100)/Au(111) and the bare Au(111) confirm the experimental findings.

Published
2013

39. Abstract P3-12-03: Combined targeting of HER2 and VEGFR2 for effective treatment of HER2-amplified breast cancer brain metastases

Author

Dai Fukumura, David P. Kodack, Youngchul Song, Yinyin Huang, Shom Goel, Bakhos A. Tannous, L Hiddingh, Rakesh K. Jain, Matija Snuderl, Walid S. Kamoun, Euiheon Chung, Christian T. Farrar, Hiroshi Yamashita, Jeffrey A. Engelman, Eleanor I Ager, Joao Incio, A Lussiez, and A Peters

Subjects
Oncology, Cancer Research, medicine.medical_specialty, Bevacizumab, Combination therapy, business.industry, Cancer, medicine.disease, Lapatinib, Metastatic breast cancer, Breast cancer, Trastuzumab, Internal medicine, medicine, skin and connective tissue diseases, business, neoplasms, medicine.drug, Brain metastasis
Abstract

Brain metastases remain a serious obstacle in the treatment of patients with human epidermal growth factor receptor-2 (HER2)-amplified breast cancer. Unlike HER2-amplified breast tumors growing in extra-cranial locations, brain metastases do not respond well to HER2 inhibitors and are often the reason for treatment failure. One of the major challenges in studying brain metastases is the lack of preclinical models. We developed a HER2-amplified mouse model of brain metastasis using an orthotopic xenograft of BT474 cells in mice. As seen in patients, the HER2 inhibitors trastuzumab and lapatinib failed to contain brain metastatic tumor growth. Based on previous findings from our laboratory suggesting a role of vascular endothelial growth factor (VEGF) in the resistance of HER2-overexpressing breast cancer brain metastases to trastuzumab, we combined HER2 inhibitors with the anti-VEGFR2 antibody DC101. The combination of either trastuzumab and DC101 or lapatinib and DC101 significantly slowed metastatic tumor growth in the brain, and resulted in a striking improvement in overall survival. The benefit is due largely to an anti-angiogenic effect. The combination of anti-HER2 and anti-VEGFR2 therapy reduced both the total and functional microvascular density in the brain metastatic tumors. Moreover, tumor tissues under combination therapy showed a marked increase in necrosis. Preclinical and clinical evidence suggest that the combination of trastuzumab and lapatinib is superior to either agent alone – though this has never been tested in the brain metastatic setting. We consistently observed increased phosphorylation of HER2 in breast tumor cells growing in the brain compared with the mammary fat pad. In addition, while short-term lapatinib treatment significantly reduced HER2 activation in the brain, it could do so only to the level of that observed in the untreated mammary fat pad - and this effect disappeared over time. We hypothesized that more pronounced HER2 inhibition would be beneficial to these brain metastases with increased HER2 activation. We show here a significant growth delay with the combination of the two HER2 inhibitors compared with monotherapy. Moreover, we found a dramatic brain metastatic tumor growth delay in mice treated with both HER2 inhibitors, trastuzumab and lapatinib, and DC101. The triple combination prolonged overall survival 5 times longer than control-treated mice. Brain metastasis from breast cancer is considered the “final frontier” of breast cancer research and treatment. Our findings support the clinical development of a three-drug regimen of trastuzumab, lapatinib and a VEGF pathway inhibitor for the treatment of HER2-amplified breast cancer brain metastases. While the anti-VEGF antibody bevacizumab in combination with trastuzumab and chemotherapy has shown some promise in HER2-positive metastatic breast cancer patient, there are no data on its efficacy in the context of brain metastases. A clinical trial is now recruiting patients to evaluate the efficacy of bevacizumab in breast cancer patients with active brain metastases, including its combination with trastuzumab in patients with HER2-positive disease. This trial may provide clinical evidence for the approach presented here. Citation Information: Cancer Res 2012;72(24 Suppl):Abstract nr P3-12-03.

Published
2012

40. The Potent ALK Inhibitor Brigatinib (AP26113) Overcomes Mechanisms of Resistance to First- and Second-Generation ALK Inhibitors in Preclinical Models

Author

Lauren Moran, Wei-Sheng Huang, Yaoyu Ning, Dong Zou, Scott Wardwell, Emily Y. Ye, Frank Wang, Rachel M. Squillace, Lindsey W. Eichinger, Victor M. Rivera, Jeff Keats, Sen Zhang, William C. Shakespeare, Yihan Wang, Sara Nadworny, Shuangying Liu, Tianjun Zhou, Youngchul Song, Xiaotian Zhu, Tim Clackson, David Miller, Hyun Gyung Jang, Narayana I. Narasimhan, Rana Anjum, David C. Dalgarno, Qurish K. Mohemmad, and Juan J. Miret

Subjects
0301 basic medicine, Alectinib, Cancer Research, Lung Neoplasms, Brigatinib, medicine.drug_class, Pyridines, Antineoplastic Agents, Biology, 03 medical and health sciences, 0302 clinical medicine, Organophosphorus Compounds, Crizotinib, hemic and lymphatic diseases, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, ROS1, Anaplastic lymphoma kinase, Humans, Anaplastic Lymphoma Kinase, Sulfones, Protein Kinase Inhibitors, Ceritinib, ALK Gene Rearrangement, Receptor Protein-Tyrosine Kinases, Hep G2 Cells, U937 Cells, ALK inhibitor, 030104 developmental biology, Pyrimidines, Oncology, Biochemistry, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Mutation, Cancer research, Pyrazoles, medicine.drug
Abstract

Purpose: Non–small cell lung cancers (NSCLCs) harboring ALK gene rearrangements (ALK+) typically become resistant to the first-generation anaplastic lymphoma kinase (ALK) tyrosine kinase inhibitor (TKI) crizotinib through development of secondary resistance mutations in ALK or disease progression in the brain. Mutations that confer resistance to second-generation ALK TKIs ceritinib and alectinib have also been identified. Here, we report the structure and first comprehensive preclinical evaluation of the next-generation ALK TKI brigatinib.Experimental Design: A kinase screen was performed to evaluate the selectivity profile of brigatinib. The cellular and in vivo activities of ALK TKIs were compared using engineered and cancer-derived cell lines. The brigatinib–ALK co-structure was determined.Results: Brigatinib potently inhibits ALK and ROS1, with a high degree of selectivity over more than 250 kinases. Across a panel of ALK+ cell lines, brigatinib inhibited native ALK (IC50, 10 nmol/L) with 12-fold greater potency than crizotinib. Superior efficacy of brigatinib was also observed in mice with ALK+ tumors implanted subcutaneously or intracranially. Brigatinib maintained substantial activity against all 17 secondary ALK mutants tested in cellular assays and exhibited a superior inhibitory profile compared with crizotinib, ceritinib, and alectinib at clinically achievable concentrations. Brigatinib was the only TKI to maintain substantial activity against the most recalcitrant ALK resistance mutation, G1202R. The unique, potent, and pan-ALK mutant activity of brigatinib could be rationalized by structural analyses.Conclusions: Brigatinib is a highly potent and selective ALK inhibitor. These findings provide the molecular basis for the promising activity being observed in ALK+, crizotinib-resistant patients with NSCLC being treated with brigatinib in clinical trials. Clin Cancer Res; 22(22); 5527–38. ©2016 AACR.

Published
2016

41. MEK Inhibition Leads to PI3K/AKT Activation by Relieving a Negative Feedback on ERBB Receptors

Author

John M. Asara, Rebecca S. Cook, Carlos L. Arteaga, Carlotta Costa, Youngchul Song, Jeffrey A. Engelman, and Alexa B. Turke

Subjects
Mitogen-Activated Protein Kinase Kinases, Cancer Research, Reverse Transcriptase Polymerase Chain Reaction, Akt/PKB signaling pathway, Chemistry, Receptor Protein-Tyrosine Kinases, Flow Cytometry, Article, Cell Line, Feedback, Cell biology, Enzyme Activation, Phosphatidylinositol 3-Kinases, ErbB Receptors, Oncology, Tandem Mass Spectrometry, ErbB, Gene Knockdown Techniques, Phosphorylation, ERBB3, Signal transduction, Proto-Oncogene Proteins c-akt, Protein kinase B, PI3K/AKT/mTOR pathway
Abstract

The phosphoinositide 3-kinase (PI3K)/AKT and RAF/MEK/ERK signaling pathways are activated in a wide range of human cancers. In many cases, concomitant inhibition of both pathways is necessary to block proliferation and induce cell death and tumor shrinkage. Several feedback systems have been described in which inhibition of one intracellular pathway leads to activation of a parallel signaling pathway, thereby decreasing the effectiveness of single-agent targeted therapies. In this study, we describe a feedback mechanism in which MEK inhibition leads to activation of PI3K/AKT signaling in EGFR and HER2-driven cancers. We found that MEK inhibitor–induced activation of PI3K/AKT resulted from hyperactivation of ERBB3 as a result of the loss of an inhibitory threonine phosphorylation in the conserved juxtamembrane domains of EGFR and HER2. Mutation of this amino acid led to increased ERBB receptor activation and upregulation of the ERBB3/PI3K/AKT signaling pathway, which was no longer responsive to MEK inhibition. Taken together, these results elucidate an important, dominant feedback network regulating central oncogenic pathways in human cancer. Cancer Res; 72(13); 3228–37. ©2012 AACR.

Published
2012

42. Activation of PI3K Signaling in Merkel Cell Carcinoma

Author

Vanessa L. Scialabba, Arjola K. Cosper, James C. Cusack, Anthony J. Iafrate, Dora Dias-Santagata, Jeffrey Settleman, Atul K. Bhan, Kristin Bergethon, Anthony C. Faber, Valentina Nardi, Genevieve M. Boland, Juan A. Santamaria-Barria, Hensin Tsao, Darrell R. Borger, David P. Ryan, Mai P. Hoang, Jeffrey A. Engelman, Quynh Lam, Beow Y. Yeap, and Youngchul Song

Subjects
Adult, Male, Cancer Research, Skin Neoplasms, Genotype, Class I Phosphatidylinositol 3-Kinases, medicine.medical_treatment, Biology, medicine.disease_cause, Malignancy, Article, Targeted therapy, Phosphatidylinositol 3-Kinases, Cell Line, Tumor, medicine, Carcinoma, Humans, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Aged, Neoplasm Staging, Phosphoinositide-3 Kinase Inhibitors, Aged, 80 and over, Base Sequence, Merkel cell carcinoma, food and beverages, Middle Aged, medicine.disease, Carcinoma, Merkel Cell, Enzyme Activation, medicine.anatomical_structure, Oncology, Mutation, Immunology, Cancer research, Female, Carcinogenesis, Merkel cell, Signal Transduction
Abstract

Purpose: Merkel cell carcinoma (MCC) is an aggressive cutaneous neuroendocrine tumor, often metastatic at presentation, for which current chemotherapeutic regimens are largely ineffective. As its pathogenesis is still unknown, we hypothesized that deregulation of signaling pathways commonly activated in cancer may contribute to MCC tumorigenesis and may provide insights into targeted therapy approaches for this malignancy. Experimental Design: We retrospectively profiled 60 primary MCC samples using a SNaPshot-based tumor genotyping assay to screen for common mutations in 13 cancer genes. Results: We identified mutations in 9 (15%) MCC primary tumors, including mutations in TP53 (3 of 60) and activating mutations in the PIK3CA gene (6 of 60). Sanger sequencing of the primary MCC tumors detected one additional PIK3CA mutation (R19K) that had not been previously described in cancer. Merkel cell polyoma virus (MCPyV) was detected in 38 (66%) MCC cases and patients with MCPyV-positive cancers showed a trend toward better survival. With one exception, the presence of MCPyV and activating mutations in PIK3CA appeared mutually exclusive. We observed that signaling through the PI3K/pAKT pathway was active in one MCPyV-positive and in all MCPyV-negative MCC cell lines, as evidenced by AKT phosphorylation. Importantly, the presence of a PIK3CA-activating mutation was associated with sensitivity to treatment with ZST474, a specific phosphoinositide 3-kinase (PI3K) inhibitor, and to NVP-BEZ235, a dual PI3K/mTOR inhibitor, targeted agents under active clinical development. Conclusions: PI3K pathway activation may drive tumorigenesis in a subset of MCC and screening these tumors for PIK3CA mutations could help identify patients who may respond to treatment with PI3K pathway inhibitors. Clin Cancer Res; 18(5); 1227–36. ©2012 AACR.

Published
2012

43. Receptor tyrosine kinases exert dominant control over PI3K signaling in human KRAS mutant colorectal cancers

Author

David P. Ryan, Kwok-Kin Wong, Lewis C. Cantley, Ryan B. Corcoran, Youngchul Song, Cyril H. Benes, Hiromichi Ebi, Jeffrey A. Meyerhardt, Jeffrey A. Engelman, Anurag K. Singh, Zhao Chen, Eugene Lifshits, and Jeffrey Settleman

Subjects
Male, Proto-Oncogene Proteins B-raf, MAPK/ERK pathway, Class I Phosphatidylinositol 3-Kinases, MAP Kinase Signaling System, Transplantation, Heterologous, Mice, Nude, Apoptosis, Biology, medicine.disease_cause, Receptor tyrosine kinase, Proto-Oncogene Proteins p21(ras), Mice, Phosphatidylinositol 3-Kinases, Downregulation and upregulation, Cell Line, Tumor, Proto-Oncogene Proteins, medicine, Animals, Humans, RNA, Small Interfering, Protein Kinase Inhibitors, Protein kinase B, PI3K/AKT/mTOR pathway, DNA Primers, Base Sequence, Receptor Protein-Tyrosine Kinases, General Medicine, Transplantation, Gene Knockdown Techniques, Mutation, ras Proteins, Cancer research, biology.protein, KRAS, Signal transduction, Colorectal Neoplasms, Proto-Oncogene Proteins c-akt, Neoplasm Transplantation, Signal Transduction, Research Article
Abstract

Therapies inhibiting receptor tyrosine kinases (RTKs) are effective against some human cancers when they lead to simultaneous downregulation of PI3K/AKT and MEK/ERK signaling. However, mutant KRAS has the capacity to directly activate ERK and PI3K signaling, and this is thought to underlie the resistance of KRAS mutant cancers to RTK inhibitors. Here, we have elucidated the molecular regulation of both the PI3K/AKT and MEK/ERK signaling pathways in KRAS mutant colorectal cancer cells and identified combination therapies that lead to robust cancer cell apoptosis. KRAS knockdown using shRNA suppressed ERK signaling in all of the human KRAS mutant colorectal cancer cell lines examined. However, no decrease, and actually a modest increase, in AKT phosphorylation was often seen. By performing PI3K immunoprecipitations, we determined that RTKs, often IGF-IR, regulated PI3K signaling in the KRAS mutant cell lines. This conclusion was also supported by the observation that specific RTK inhibition led to marked suppression of PI3K signaling and biochemical assessment of patient specimens. Interestingly, combination of RTK and MEK inhibitors led to concomitant inhibition of PI3K and MEK signaling, marked growth suppression, and robust apoptosis of human KRAS mutant colorectal cancer cell lines in vitro and upon xenografting in mice. These findings provide a framework for utilizing RTK inhibitors in the treatment of KRAS mutant colorectal cancers.

Published
2011

44. Using Tandem Mass Spectrometry in Targeted Mode to Identify Activators of Class IA PI3K in Cancer

Author

Lewis C. Cantley, Pasi A. Jänne, John M. Asara, Carlos L. Arteaga, Jie Qi, Todd W. Miller, Xuemei Yang, Alexa B. Turke, Jeffrey A. Engelman, Youngchul Song, and Brent N. Rexer

Subjects
Cancer Research, Lung Neoplasms, Class I Phosphatidylinositol 3-Kinases, medicine.drug_class, Receptor Protein-Tyrosine Kinases, Mice, Nude, Biology, Transfection, Tandem mass spectrometry, Article, Tyrosine-kinase inhibitor, Receptor tyrosine kinase, Mice, Phosphatidylinositol 3-Kinases, Tandem Mass Spectrometry, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Animals, Humans, RNA, Small Interfering, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Sirolimus, Kinase, Cancer, medicine.disease, Molecular biology, Class Ia Phosphatidylinositol 3-Kinase, Enzyme Activation, Oncology, Mutation, Cancer cell, Cancer research, biology.protein, Chromatography, Liquid, Transcription Factors
Abstract

Phosphatiditylinositide-3-kinase (PI3K) is activated in some cancers by direct mutation, but it is activated more commonly in cancer by mutation of upstream acting receptor tyrosine kinases (TK). At present, there is no systematic method to determine which TK signaling cascades activate PI3K in certain cancers, despite the likely utility of such information to help guide selection of tyrosine kinase inhibitor (TKI) drug strategies for personalized therapy. Here, we present a quantitative liquid chromatography tandem mass spectrometry approach that identifies upstream activators of PI3K both in vitro and in vivo. Using non–small cell lung carcinoma to illustrate this approach, we show a correct identification of the mechanism of PI3K activation in several models, thereby identifying the most appropriate TKI to downregulate PI3K signaling. This approach also determined the molecular mechanisms and adaptors required for PI3K activation following inhibition of the mTOR kinase TORC1. We further validated the approach in breast cancer cells with mutational activation of PIK3CA, where tandem mass spectrometry detected and quantitatively measured the abundance of a helical domain mutant (E545K) of PIK3CA connected to PI3K activation. Overall, our findings establish a mass spectrometric approach to identify functional interactions that govern PI3K regulation in cancer cells. Using this technique to define the pathways that activate PI3K signaling in a given tumor could help inform clinical decision making by helping guide personalized therapeutic strategies for different patients. Cancer Res; 71(18); 5965–75. ©2011 AACR.

Published
2011

45. Effective use of PI3K and MEK inhibitors to treat mutant Kras G12D and PIK3CA H1047R murine lung cancers

Author

Kate McNamara, Robert F. Padera, Angela Lightbown, S. Michel Maira, Samanthi A. Perera, Lucian R. Chirieac, Ramneet Kaur, Ralph Weissleder, Liang Chen, Katherine Crosby, Lewis C. Cantley, Alexander R. Guimaraes, Umar Mahmood, Jessica Simendinger, Jeffrey A. Engelman, Xiaohong Tan, Youngchul Song, Kwok-Kin Wong, Rabi Upadhyay, Carlos Garcia-Echeverria, and Timothy Q. Li

Subjects
Lung Neoplasms, Class I Phosphatidylinositol 3-Kinases, MAP Kinase Signaling System, Down-Regulation, Mice, Transgenic, Biology, Mitogen-activated protein kinase kinase, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Proto-Oncogene Proteins p21(ras), Mice, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Animals, c-Raf, Enzyme Inhibitors, Protein kinase A, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, 030304 developmental biology, Mitogen-Activated Protein Kinase Kinases, 0303 health sciences, Kinase, General Medicine, Molecular biology, 3. Good health, Gene Expression Regulation, Neoplastic, Protein kinase domain, 030220 oncology & carcinogenesis, Genetically Engineered Mouse, Mutation, ras Proteins, Cancer research, KRAS
Abstract

Somatic mutations that activate phosphoinositide 3-kinase (PI3K) have been identified in the p110-alpha catalytic subunit (encoded by PIK3CA). They are most frequently observed in two hotspots: the helical domain (E545K and E542K) and the kinase domain (H1047R). Although the p110-alpha mutants are transforming in vitro, their oncogenic potential has not been assessed in genetically engineered mouse models. Furthermore, clinical trials with PI3K inhibitors have recently been initiated, and it is unknown if their efficacy will be restricted to specific, genetically defined malignancies. In this study, we engineered a mouse model of lung adenocarcinomas initiated and maintained by expression of p110-alpha H1047R. Treatment of these tumors with NVP-BEZ235, a dual pan-PI3K and mammalian target of rapamycin (mTOR) inhibitor in clinical development, led to marked tumor regression as shown by positron emission tomography-computed tomography, magnetic resonance imaging and microscopic examination. In contrast, mouse lung cancers driven by mutant Kras did not substantially respond to single-agent NVP-BEZ235. However, when NVP-BEZ235 was combined with a mitogen-activated protein kinase kinase (MEK) inhibitor, ARRY-142886, there was marked synergy in shrinking these Kras-mutant cancers. These in vivo studies suggest that inhibitors of the PI3K-mTOR pathway may be active in cancers with PIK3CA mutations and, when combined with MEK inhibitors, may effectively treat KRAS mutated lung cancers.

Published
2008

46. MET Amplification Leads to Gefitinib Resistance in Lung Cancer by Activating ERBB3 Signaling

Author

Youngchul Song, Courtney Hyland, Christopher-Michael Gale, Joon Oh Park, Pasi A. Jänne, Tony Mok, Kreshnik Zejnullahu, Tetsuya Mitsudomi, Jeffrey A. Engelman, Xiaojun Zhao, Federico Cappuzzo, Alison J. Holmes, James J. Christensen, Lewis C. Cantley, Neal I. Lindeman, Takayuki Kosaka, Bruce E. Johnson, Andrew M. Rogers, and Charles Lee

Subjects
Indoles, Lung Neoplasms, Receptor, ErbB-3, Antineoplastic Agents, CHO Cells, Biology, Proto-Oncogene Mas, Phosphatidylinositol 3-Kinases, T790M, Cricetulus, Gefitinib, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Cricetinae, Proto-Oncogene Proteins, medicine, Animals, Humans, Receptors, Growth Factor, heterocyclic compounds, ERBB3, Sulfones, Epidermal growth factor receptor, Enzyme Inhibitors, Phosphorylation, skin and connective tissue diseases, Lung cancer, Erlotinib Hydrochloride, neoplasms, Cell Proliferation, Multidisciplinary, Gene Amplification, Proto-Oncogene Proteins c-met, medicine.disease, respiratory tract diseases, Drug Resistance, Neoplasm, Quinazolines, Cancer research, biology.protein, Erlotinib, EGFR Activating Mutation, Proto-Oncogene Proteins c-akt, Signal Transduction, medicine.drug
Abstract

The epidermal growth factor receptor (EGFR) kinase inhibitors gefitinib and erlotinib are effective treatments for lung cancers with EGFR activating mutations, but these tumors invariably develop drug resistance. Here, we describe a gefitinib-sensitive lung cancer cell line that developed resistance to gefitinib as a result of focal amplification of the MET proto-oncogene. inhibition of MET signaling in these cells restored their sensitivity to gefitinib. MET amplification was detected in 4 of 18 (22%) lung cancer specimens that had developed resistance to gefitinib or erlotinib. We find that amplification of MET causes gefitinib resistance by driving ERBB3 (HER3)–dependent activation of PI3K, a pathway thought to be specific to EGFR/ERBB family receptors. Thus, we propose that MET amplification may promote drug resistance in other ERBB-driven cancers as well.

Published
2007

47. Abstract 5008: The brain microenvironment mediates resistance in luminal breast cancer to PI3K inhibition through HER3 activation

Author

Christina Wong, Dai Fukumura, Jantima Tanboon, Valeria M. Estrada, Alexander Cao, Rita Das, Carlos L. Arteaga, Alan Huang, Jeffrey A. Engelman, Robert Schlegel, Dan G. Duda, Divya Bezwada, Mark Badeaux, David P. Kodack, Gino B. Ferraro, Elena F. Brachtel, Ram C. Shankaraiah, Carlotta Costa, Marni B. Siegel, Angela Tam, Vasileios Askoxylakis, Youngchul Song, Bhushankumar Patel, Shom Goel, Rakesh R. Ramjiawan, Melinda E. Sanders, Qing Sheng, Carey K. Anders, Ryan Miller, Xiaolong Qi, Jonas Kloepper, Rakesh K. Jain, and Kamila Naxerova

Subjects
Cancer Research, business.industry, Cancer, Therapeutic resistance, medicine.disease, Blockade, Breast cancer, Oncology, Immunology, medicine, Cancer research, Brain lesions, Tumor growth, business, PI3K/AKT/mTOR pathway
Abstract

Brain metastases represent a devastating progression of luminal breast cancer. While targeted therapies are often effective systemically, they fail to adequately control brain metastases. In preclinical models that faithfully recapitulate the disparate clinical responses in these microenvironments, we observed that brain metastases evade PI3K inhibition despite efficient drug delivery. In comparison to extracranial disease, there is increased HER3 expression and phosphorylation in the brain lesions. HER3 blockade overcomes the resistance of both HER2-amplified and/or PIK3CA-mutant breast cancer brain metastases to PI3K inhibitors, leading to striking tumor growth delay and significant improvement of mouse survival. Collectively, these data provide a mechanistic basis underlying therapeutic resistance in the brain microenvironment and identify rapidly translatable treatment strategiesfor HER2-amplified and/or PIK3CA-mutant breast cancer brain metastases. Citation Format: Gino B. Ferraro, David P. Kodack, Vasileios Askoxylakis, Qing Sheng, Mark Badeaux, Shom Goel, Xiaolong Qi, Ram Shankaraiah, Alexander Z. Cao, Rakesh R. Ramjiawan, Divya Bezwada, Bhushankumar Patel, Youngchul Song, Carlotta Costa, Kamila Naxerova, Christina Wong, Jonas Kloepper, Rita Das, Angela Tam, Jantima Tanboon, Dan G. Duda, Ryan C. Miller, Marni B. Siegel, Carey K. Anders, Melinda Sanders, Valeria M. Estrada, Robert Schlegel, Carlos L. Arteaga, Elena Brachtel, Alan Huang, Dai Fukumura, Jeffrey A. Engelman, Rakesh K. Jain. The brain microenvironment mediates resistance in luminal breast cancer to PI3K inhibition through HER3 activation [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 5008. doi:10.1158/1538-7445.AM2017-5008

Published
2017

48. PI3K regulates MEK/ERK signaling in breast cancer via the Rac-GEF, P-Rex1

Author

Anthony C. Faber, Dejan Juric, Youngchul Song, Cyril H. Benes, Patricia Della Pelle, Hiroshi Kotani, Hiromichi Ebi, Jeffrey A. Engelman, Mari Mino-Kenudson, Carlotta Costa, Madhuri Nishtala, and Seiji Yano

Subjects
MAPK/ERK pathway, rac1 GTP-Binding Protein, Class I Phosphatidylinositol 3-Kinases, MAP Kinase Signaling System, Receptor, ErbB-2, Immunoblotting, Mice, Nude, RAC1, Breast Neoplasms, Biology, Mice, Phosphatidylinositol 3-Kinases, Breast cancer, Databases, Genetic, medicine, Animals, Guanine Nucleotide Exchange Factors, Protein kinase A, Protein kinase B, PI3K/AKT/mTOR pathway, Phosphoinositide-3 Kinase Inhibitors, Multidisciplinary, Kinase, Neuropeptides, Computational Biology, Biological Sciences, medicine.disease, Cancer research, Female, Guanine nucleotide exchange factor
Abstract

The PI3K pathway is genetically altered in excess of 70% of breast cancers, largely through PIK3CA mutation and HER2 amplification. Preclinical studies have suggested that these subsets of breast cancers are particularly sensitive to PI3K inhibitors; however, the reasons for this heightened sensitivity are mainly unknown. We investigated the signaling effects of PI3K inhibition in PIK3CA mutant and HER2 amplified breast cancers using PI3K inhibitors currently in clinical trials. Unexpectedly, we found that in PIK3CA mutant and HER2 amplified breast cancers sensitive to PI3K inhibitors, PI3K inhibition led to a rapid suppression of Rac1/p21-activated kinase (PAK)/protein kinase C-RAF (C-RAF)/ protein kinase MEK (MEK)/ERK signaling that did not involve RAS. Furthermore, PI3K inhibition led to an ERK-dependent up-regulation of the proapoptotic protein, BIM, followed by induction of apoptosis. Expression of a constitutively active form of Rac1 in these breast cancer models blocked PI3Ki-induced down-regulation of ERK phosphorylation, apoptosis, and mitigated PI3K inhibitor sensitivity in vivo. In contrast, protein kinase AKT inhibitors failed to block MEK/ERK signaling, did not up-regulate BIM, and failed to induce apoptosis. Finally, we identified phosphatidylinositol 3,4,5-trisphosphate-dependent Rac exchanger 1 (P-Rex1) as the PI(3,4,5)P3-dependent guanine exchange factor for Rac1 responsible for regulation of the Rac1/C-RAF/MEK/ERK pathway in these cells. The expression level of P-Rex1 correlates with sensitivity to PI3K inhibitors in these breast cancer cell lines. Thus, PI3K inhibitors have enhanced activity in PIK3CA mutant and HER2 amplified breast cancers in which PI3K inhibition down-regulates both the AKT and Rac1/ERK pathways. In addition, P-Rex1 may serve as a biomarker to predict response to single-agent PI3K inhibitors within this subset of breast cancers.

Published
2013

49. Cytotoxic activity of tivantinib (ARQ 197) is not due solely to c-MET inhibition

Author

Ryohei Katayama, Takao Yamori, Youngchul Song, Jeffrey A. Engelman, Naoya Fujita, Aki Aoyama, Tomoko Oh-hara, and Jie Qi

Subjects
G2 Phase, Cancer Research, C-Met, Antineoplastic Agents, Biology, Microtubules, Article, Receptor tyrosine kinase, Microtubule polymerization, chemistry.chemical_compound, Tubulin, Cell Line, Tumor, medicine, Humans, Tivantinib, Phosphorylation, Extracellular Signal-Regulated MAP Kinases, Cell Proliferation, Crizotinib, Cell growth, Proto-Oncogene Proteins c-met, Pyrrolidinones, Tubulin Modulators, Oncology, chemistry, Cancer cell, Cancer research, biology.protein, Quinolines, Hepatocyte growth factor, Proto-Oncogene Proteins c-akt, Cell Division, medicine.drug
Abstract

The receptor tyrosine kinase c-MET is the high-affinity receptor for the hepatocyte growth factor (HGF). The HGF/c-MET axis is often dysregulated in tumors. c-MET activation can be caused by MET gene amplification, activating mutations, and auto- or paracrine mechanisms. Thus, c-MET inhibitors are under development as anticancer drugs. Tivantinib (ARQ 197) was reported as a small-molecule c-MET inhibitor and early clinical studies suggest antitumor activity. To assess whether the antitumor activity of tivantinib was due to inhibition of c-MET, we compared the activity of tivantinib with other c-MET inhibitors in both c-MET–addicted and nonaddicted cancer cells. As expected, other c-MET inhibitors, crizotinib and PHA-665752, suppressed the growth of c-MET-addicted cancers, but not the growth of cancers that are not addicted to c-MET. In contrast, tivantinib inhibited cell viability with similar potency in both c-MET-addicted and nonaddicted cells. These results suggest that tivantinib exhibits its antitumor activity in a manner independent of c-MET status. Tivantinib treatment induced a G2–M cell-cycle arrest in EBC1 cells similarly to vincristine treatment, whereas PHA-665752 or crizotinib treatment markedly induced G0–G1 cell-cycle arrest. To identify the additional molecular target of tivantinib, we conducted COMPARE analysis, an in silico screening of a database of drug sensitivities across 39 cancer cell lines (JFCR39), and identified microtubule as a target of tivantinib. Tivantinib-treated cells showed typical microtubule disruption similar to vincristine and inhibited microtubule assembly in vitro. These results suggest that tivantinib inhibits microtubule polymerization in addition to inhibiting c-MET. Cancer Res; 73(10); 3087–96. ©2013 AACR.

Published
2013

50. An Exploratory Study on the Cause of the Poor Performance of Climate Change in Korea

Author

Seongheon Kim, Yeongsin Kim, Youngchul Song, and Ji-Eun Lee

Subjects
Government, Work (electrical), Performance management, business.industry, Green growth, Environmental resource management, Exploratory research, Climate change, International community, Environmental economics, business, Variety (cybernetics)
Abstract

The relevant ministries, including the Ministry of Environment in Korea, provided Post-2020 Long-term Mitigation Target and Implementation Plan. The plan consisted of four Business As Usual (BAU) reduction levels by 14.7%, 19.2%, 25.7%, and 31.3% until 2030. The Korean government finalized the mitigation target of 37%. But all the initial alternatives were below the goal, 30% from BAU, that has been promised to the international community as well as set out in the Framework Act on Low Carbon Green Growth. In order to achieve a specific goal, performance management should pursue “Justify doing the right things.” Otherwise, performance management would not work properly. According to Kingdon’s Policy Stream Framework, abnormal alternatives are difficult to be presented as scenarios because alternative building should focus on the role of the need to adhere to the basic principles and professionals. Such a result is possible only when the policy actors does not balance themselves. Performance management statistics has been analyzed by 6 years CCPI data since 2011, taking into account the impact after enactment. This study also has been complemented by a variety of sources, including the media, documents, and artifacts during the period. As a result, raising awareness about climate change was analyzed as one of the solutions because the climate change issue affects the normal performance management throughout the life of the people to stay linked to the environment.

Published
2016

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