Your search keyword '"Red-Brewer, Monica"' showing total 23 results

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

Author

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

Published

2021

2. An ERBB1-3 Neutralizing Antibody Mixture With High Activity Against Drug-Resistant HER2+ Breast Cancers With ERBB Ligand Overexpression

Author

Schwarz, Luis J., Hutchinson, Katherine E., Rexer, Brent N., Estrada, Mónica Valeria, Gonzalez Ericsson, Paula I., Sanders, Melinda E., Dugger, Teresa C., Formisano, Luigi, Guerrero-Zotano, Angel, Red-Brewer, Monica, Young, Christian D., Lantto, Johan, Pedersen, Mikkel W., Kragh, Michael, Horak, Ivan D., and Arteaga, Carlos L.

Published

2017

3. LYN-activating mutations mediate antiestrogen resistance in estrogen receptor-positive breast cancer

Author

Schwarz, Luis J., Fox, Emily M., Balko, Justin M., Garret, Joan T., Kuba, Maria Gabriela, Estrada, Monica Valeria, Gonzalez-Angulo, Ana Maria, Mills, Gordon B., Red-Brewer, Monica, Mayer, Ingrid A., Abramson, Vandana, Rizzo, Monica, Kelley, Mark C., Meszoely, Ingrid M., and Arteaga, Carlos L.

Subjects

Gene mutations -- Health aspects -- Research, Estrogen -- Analysis -- Physiological aspects -- Research -- Genetic aspects, Breast cancer -- Risk factors -- Genetic aspects -- Research, Health care industry

Abstract

Estrogen receptor-positive ([ER.sup.+]) breast cancers adapt to hormone deprivation and become resistant to antiestrogen therapy. Here, we performed deep sequencing on ER* tumors that remained highly proliferative after treatment with the aromatase inhibitor letrozole and identified a D189Y mutation in the inhibitory SH2 domain of the SRC family kinase (SFK) LYN. Evaluation of 463 breast tumors in The Cancer Genome Atlas revealed four LYN mutations, two of which affected the SH2 domain. In addition, LYN was upregulated in multiple ER* breast cancer lines resistant to long-term estrogen deprivation (LTED). An RNAi-based kinome screen revealed that LYN is required for growth of ER* LTED breast cancer cells. Kinase assays and immunoblot analyses of SRC substrates in transfected cells indicated that [LYN.sup.D189Y] has higher catalytic activity than WT protein. Further, [LYN.sup.D189Y] exhibited reduced phosphorylation at the inhibitory Y507 site compared with [LYN.sup.WT]. Other SH2 domain LYN mutants, E159K and K209N, also exhibited higher catalytic activity and reduced inhibitory site phosphorylation. [LYN.sup.D189Y] overexpression abrogated growth inhibition by fulvestrant and/or the PI3K inhibitor BKM120 in 3 ER* breast cancer cell lines. The SFK inhibitor dasatinib enhanced the antitumor effect of BKM120 and fulvestrant against estrogen- deprived ER* xenografts but not [LYN.sup.D189Y]-expressing xenografts. These results suggest that LYN mutations mediate escape from antiestrogens in a subset of ER* breast cancers., Introduction LYN is a member of the SRC family of protein tyrosine kinases (SFKs), key regulators of several cellular processes, including cancer cell growth, migration, invasion, and survival (1, 2). [...]

Published

2014

4. Functional effects of glycosylation at Asn-579 of epidermal growth factor receptor

Author

Whitson, Kristin B., Whitson, Stefanie R., Red-Brewer, Monica L., McCoy, Austin J., Vitali, Angela A., Walker, Francessca, Johns, Terrance G., Beth, Albert H., and Staros, James V.

Subjects

Epidermal growth factor -- Chemical properties, Glycosylation -- Research, Proteins -- Chemical properties, Biological sciences, Chemistry

Abstract

An investigation of functional effects of glycosylation at N(super 579) of the epidermal growth factor (EGFR) is presented. It is revealed that EGF-stimulated phosphorylation in cells expressing N579Q-EGFRs results in notable differences in the pattern of tyrosine phosphorylated proteins compared with that obtained in cells expressing (wild type) WT-EGFRs.

Published

2005

5. Hyperactivation of TORC1 Drives Resistance to the Pan-HER Tyrosine Kinase Inhibitor Neratinib in HER2-Mutant Cancers

Author

Sudhan, Dhivya R., primary, Guerrero-Zotano, Angel, additional, Won, Helen, additional, González Ericsson, Paula, additional, Servetto, Alberto, additional, Huerta-Rosario, Mariela, additional, Ye, Dan, additional, Lee, Kyung-min, additional, Formisano, Luigi, additional, Guo, Yan, additional, Liu, Qi, additional, Kinch, Lisa N., additional, Red Brewer, Monica, additional, Dugger, Teresa, additional, Koch, James, additional, Wick, Michael J., additional, Cutler, Richard E., additional, Lalani, Alshad S., additional, Bryce, Richard, additional, Auerbach, Alan, additional, Hanker, Ariella B., additional, and Arteaga, Carlos L., additional

Published

2020

6. Co-Occurring Gain-of-Function Mutations in HER2 and HER3 Modulate HER2/HER3 Activation, Breast Cancer Progression, and HER2 Inhibitor Sensitivity

Author

Hanker, Ariella, primary, Harikrishna, S., additional, Marin, Arnaldo, additional, Ye, Dan, additional, Lin, Chang-Ching, additional, Sudhan, Dhivya R., additional, Akamatsu, Hiroaki, additional, Red Brewer, Monica, additional, Sheehan, Jonathan, additional, Koch, James P., additional, Servetto, Alberto, additional, He, Jie, additional, Lalani, Alshad S., additional, Meiler, Jens, additional, and Arteaga, Carlos, additional

Published

2020

7. Abstract 867: EGFR kinase domain duplication (EGFR-KDD) is activated by asymmetric intra-molecular dimerization

Author

Du, Zhenfang, primary, Gallant, Jean-Nicolas, additional, Red-Brewer, Monica, additional, Brown, Benjamin, additional, Sheehan, Jonathan, additional, Meiler, Jens, additional, and Lovly, Christine M., additional

Published

2019

8. EpCAM: Another Surface-to-Nucleus Missile

Author

Carpenter, Graham and Red Brewer, Monica

Published

2009

9. JAK2 inhibition sensitizes resistant EGFR-mutant lung adenocarcinoma to tyrosine kinase inhibitors

Author

Gao, Sizhi P., primary, Chang, Qing, additional, Mao, Ninghui, additional, Daly, Laura A., additional, Vogel, Robert, additional, Chan, Tyler, additional, Liu, Shu Hui, additional, Bournazou, Eirini, additional, Schori, Erez, additional, Zhang, Haiying, additional, Red Brewer, Monica, additional, Pao, William, additional, Morris, Luc, additional, Ladanyi, Marc, additional, Arcila, Maria, additional, Manova-Todorova, Katia, additional, de Stanchina, Elisa, additional, Norton, Larry, additional, Levine, Ross L., additional, Altan-Bonnet, Gregoire, additional, Solit, David, additional, Zinda, Michael, additional, Huszar, Dennis, additional, Lyden, David, additional, and Bromberg, Jacqueline F., additional

Published

2016

10. HER2 missense mutations have distinct effects on oncogenic signaling and migration

Author

Zabransky, Daniel J., primary, Yankaskas, Christopher L., additional, Cochran, Rory L., additional, Wong, Hong Yuen, additional, Croessmann, Sarah, additional, Chu, David, additional, Kavuri, Shyam M., additional, Red Brewer, Monica, additional, Rosen, D. Marc, additional, Dalton, W. Brian, additional, Cimino-Mathews, Ashley, additional, Cravero, Karen, additional, Button, Berry, additional, Kyker-Snowman, Kelly, additional, Cidado, Justin, additional, Erlanger, Bracha, additional, Parsons, Heather A., additional, Manto, Kristen M., additional, Bose, Ron, additional, Lauring, Josh, additional, Arteaga, Carlos L., additional, Konstantopoulos, Konstantinos, additional, and Park, Ben Ho, additional

Published

2015

11. Abstract PD5-8: HER2/PIK3CAH1047R transgenic mammary tumors develop acquired resistance to triple therapy with trastuzumab, pertuzumab and PI3K inhibitors via multiple mechanisms

Author

Hanker, Ariella B, primary, Bulen, Benjamin, additional, Red Brewer, Monica, additional, Young, Christian D, additional, Farrar, Kirsten M, additional, Cook, Rebecca S, additional, Stricker, Thomas P, additional, and Arteaga, Carlos L, additional

Published

2015

12. Rationale for co-targeting IGF-1R and ALK in ALK fusion-positive lung cancer

Author

Lovly, Christine M., McDonald, Nerina T., Chen, Heidi, Ortiz-Cuaran, Sandra, Heukamp, Lukas C., Yan, Yingjun, Florin, Alexandra, Ozretic, Luka, Lim, Diana, Wang, Lu, Chen, Zhao, Chen, Xi, Lu, Pengcheng, Paik, Paul K., Shen, Ronglai, Jin, Hailing, Buettner, Reinhard, Ansen, Sascha, Perner, Sven, Brockmann, Michael, Bos, Marc, Wolf, Juergen, Gardizi, Masyar, Wright, Gavin M., Solomon, Benjamin, Russell, Prudence A., Rogers, Toni-Maree, Suehara, Yoshiyuki, Red-Brewer, Monica, Tieu, Rudy, de Stanchina, Elisa, Wang, Qingguo, Zhao, Zhongming, Johnson, David H., Horn, Leora, Wong, Kwok-Kin, Thomas, Roman K., Ladanyi, Marc, Pao, William, Lovly, Christine M., McDonald, Nerina T., Chen, Heidi, Ortiz-Cuaran, Sandra, Heukamp, Lukas C., Yan, Yingjun, Florin, Alexandra, Ozretic, Luka, Lim, Diana, Wang, Lu, Chen, Zhao, Chen, Xi, Lu, Pengcheng, Paik, Paul K., Shen, Ronglai, Jin, Hailing, Buettner, Reinhard, Ansen, Sascha, Perner, Sven, Brockmann, Michael, Bos, Marc, Wolf, Juergen, Gardizi, Masyar, Wright, Gavin M., Solomon, Benjamin, Russell, Prudence A., Rogers, Toni-Maree, Suehara, Yoshiyuki, Red-Brewer, Monica, Tieu, Rudy, de Stanchina, Elisa, Wang, Qingguo, Zhao, Zhongming, Johnson, David H., Horn, Leora, Wong, Kwok-Kin, Thomas, Roman K., Ladanyi, Marc, and Pao, William

Abstract

Crizotinib, a selective tyrosine kinase inhibitor (TKI), shows marked activity in patients whose lung cancers harbor fusions in the gene encoding anaplastic lymphoma receptor tyrosine kinase (ALK), but its efficacy is limited by variable primary responses and acquired resistance. In work arising from the clinical observation of a patient with ALKfusion-positive lung cancer who had an exceptional response to an insulin-like growth factor 1 receptor (IGF-1R)-specific antibody, we define a therapeutic synergism between ALK and IGF-1R inhibitors. Similar to IGF-1R, ALK fusion proteins bind to the adaptor insulin receptor substrate 1 (IRS-1), and IRS-1 knockdown enhances the antitumor effects of ALK inhibitors. In models of ALK TKI resistance, the IGF-1R pathway is activated, and combined ALK and IGF-1R inhibition improves therapeutic efficacy. Consistent with this finding, the levels of IGF-1R and IRS-1 are increased in biopsy samples from patients progressing on crizotinib monotherapy. Collectively these data support a role for the IGF-1R-IRS-1 pathway in both ALK TKI-sensitive and ALK TKI-resistant states and provide a biological rationale for further clinical development of dual ALK and IGF-1R inhibitors.

Published

2014

13. Rationale for co-targeting IGF-1R and ALK in ALK fusion–positive lung cancer

Author

Lovly, Christine M, primary, McDonald, Nerina T, additional, Chen, Heidi, additional, Ortiz-Cuaran, Sandra, additional, Heukamp, Lukas C, additional, Yan, Yingjun, additional, Florin, Alexandra, additional, Ozretić, Luka, additional, Lim, Diana, additional, Wang, Lu, additional, Chen, Zhao, additional, Chen, Xi, additional, Lu, Pengcheng, additional, Paik, Paul K, additional, Shen, Ronglai, additional, Jin, Hailing, additional, Buettner, Reinhard, additional, Ansén, Sascha, additional, Perner, Sven, additional, Brockmann, Michael, additional, Bos, Marc, additional, Wolf, Jürgen, additional, Gardizi, Masyar, additional, Wright, Gavin M, additional, Solomon, Benjamin, additional, Russell, Prudence A, additional, Rogers, Toni-Maree, additional, Suehara, Yoshiyuki, additional, Red-Brewer, Monica, additional, Tieu, Rudy, additional, de Stanchina, Elisa, additional, Wang, Qingguo, additional, Zhao, Zhongming, additional, Johnson, David H, additional, Horn, Leora, additional, Wong, Kwok-Kin, additional, Thomas, Roman K, additional, Ladanyi, Marc, additional, and Pao, William, additional

Published

2014

14. Abstract A109: AZD9291: an irreversible, potent and selective third generation tyrosine kinase inhibitor (TKI) targeting EGFR activating (EGFRm+) and resistance (T790M) mutations in advanced lung adenocarcinoma.

Author

Cross, Darren, primary, Ashton, Sue, additional, Nebhan, Caroline, additional, Eberlein, Cath, additional, Finlay, M. Raymond V., additional, Hughes, Gareth, additional, Jacobs, Vivien, additional, Mellor, Martine, additional, Red Brewer, Monica, additional, Meador, Catherine, additional, Orme, Jonathon, additional, Spitzler, Paula, additional, Powell, Steve, additional, Rahi, Amar, additional, Taylor, Paula, additional, Ward, Richard A., additional, Daunt, Paula, additional, Galer, Anne, additional, Klinowska, Teresa, additional, Richmond, Graham, additional, and Pao, William, additional

Published

2013

15. Mechanism for activation of mutated epidermal growth factor receptors in lung cancer

Author

Red Brewer, Monica, primary, Yun, Cai-Hong, additional, Lai, Darson, additional, Lemmon, Mark A., additional, Eck, Michael J., additional, and Pao, William, additional

Published

2013

16. Abstract 1106: Mechanism for activation of mutated EGF receptors in lung cancer.

Author

Red Brewer, Monica L., primary, Lai, Darson, additional, Lemmon, Mark A., additional, and Pao, William, additional

Published

2013

17. The Juxtamembrane Region of the EGF Receptor Functions as an Activation Domain

Author

Red Brewer, Monica, primary, Choi, Sung Hee, additional, Alvarado, Diego, additional, Moravcevic, Katarina, additional, Pozzi, Ambra, additional, Lemmon, Mark A., additional, and Carpenter, Graham, additional

Published

2009

18. Functional Effects of Glycosylation at Asn-579 of the Epidermal Growth Factor Receptor

Author

Whitson, Kristin B., primary, Whitson, Stefanie R., additional, Red-Brewer, Monica L., additional, McCoy, Austin J., additional, Vitali, Angela A., additional, Walker, Francesca, additional, Johns, Terrance G., additional, Beth, Albert H., additional, and Staros, James V., additional

Published

2005

19. Hyperactivation of TORC1 drives resistance to the pan-HER tyrosine kinase inhibitor neratinib in HER2-mutant cancers

Author

Teresa C. Dugger, Dhivya R. Sudhan, Helen Won, Carlos L. Arteaga, Mariela Huerta-Rosario, Kyungmin Lee, Alan J. Auerbach, Richard E. Cutler, Angel Guerrero-Zotano, James P. Koch, Alberto Servetto, Michael J. Wick, Richard Bryce, Dan Ye, Lisa N. Kinch, Paula Gonzalez Ericsson, Qi Liu, Yan Guo, Luigi Formisano, Alshad S. Lalani, Ariella B. Hanker, Monica Red Brewer, Sudhan, Dhivya R, Guerrero-Zotano, Angel, Won, Helen, González Ericsson, Paula, Servetto, Alberto, Huerta-Rosario, Mariela, Ye, Dan, Lee, Kyung-Min, Formisano, Luigi, Guo, Yan, Liu, Qi, Kinch, Lisa N, Red Brewer, Monica, Dugger, Teresa, Koch, Jame, Wick, Michael J, Cutler, Richard E, Lalani, Alshad S, Bryce, Richard, Auerbach, Alan, Hanker, Ariella B, and Arteaga, Carlos L

Subjects

0301 basic medicine, Cancer Research, Receptor, ErbB-2, medicine.drug_class, Mutant, Breast Neoplasms, Drug resistance, Mechanistic Target of Rapamycin Complex 1, Biology, Tyrosine-kinase inhibitor, Article, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Humans, HER2 mutation, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, drug resistance, Everolimus, Hyperactivation, Chemistry, RNA, TORC1, neratinib, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, precision oncology, 030220 oncology & carcinogenesis, Cancer cell, Neratinib, Quinolines, biology.protein, Cancer research, Signal Transduction, RHEB, medicine.drug

Abstract

We developed neratinib-resistant HER2-mutant cancer cells by gradual dose escalation. RNA sequencing identified TORC1 signaling as an actionable mechanism of drug resistance. Primary and acquired neratinib resistance in HER2-mutant breast cancer patient-derived xenografts (PDXs) was also associated with TORC1 hyperactivity. Genetic suppression of RAPTOR or RHEB ablated P-S6 and restored sensitivity to the tyrosine kinase inhibitor. The combination of the TORC1 inhibitor everolimus and neratinib potently arrested the growth of neratinib-resistant xenografts and organoids established from neratinib-resistant PDXs. RNA and whole-exome sequencing revealed RAS-mediated TORC1 activation in a subset of neratinib-resistant models. DNA sequencing of HER2-mutant tumors clinically refractory to neratinib, as well as circulating tumor DNA profiling of patients who progressed on neratinib, showed enrichment of genomic alterations that converge to activate the mTOR pathway.

Published

2020

20. An ERBB1-3 Neutralizing Antibody Mixture With High Activity Against Drug-Resistant HER2+ Breast Cancers With ERBB Ligand Overexpression.

Author

Schwarz LJ, Hutchinson KE, Rexer BN, Estrada MV, Gonzalez Ericsson PI, Sanders ME, Dugger TC, Formisano L, Guerrero-Zotano A, Red-Brewer M, Young CD, Lantto J, Pedersen MW, Kragh M, Horak ID, and Arteaga CL

Subjects

Ado-Trastuzumab Emtansine, Animals, Antibodies, Monoclonal, Humanized therapeutic use, Breast Neoplasms chemistry, Cell Line, Tumor, Drug Resistance, Neoplasm, ErbB Receptors antagonists & inhibitors, Female, Humans, Lapatinib, Ligands, Maytansine analogs & derivatives, Maytansine therapeutic use, Mice, Mice, Nude, Quinazolines therapeutic use, Receptor, ErbB-2 antagonists & inhibitors, Receptor, ErbB-3 antagonists & inhibitors, Trastuzumab therapeutic use, Xenograft Model Antitumor Assays, Antibodies, Neutralizing therapeutic use, Antineoplastic Agents therapeutic use, Breast Neoplasms drug therapy

Abstract

Background: Plasticity of the ERBB receptor network has been suggested to cause acquired resistance to anti-human epidermal growth factor receptor 2 (HER2) therapies. Thus, we studied whether a novel approach using an ERBB1-3-neutralizing antibody mixture can block these compensatory mechanisms of resistance., Methods: HER2+ cell lines and xenografts (n ≥ 6 mice per group) were treated with the ERBB1-3 antibody mixture Pan-HER, trastuzumab/lapatinib (TL), trastuzumab/pertuzumab (TP), or T-DM1. Downregulation of ERBB receptors was assessed by immunoblot analysis and immunohistochemistry. Paired pre- and post-T-DM1 tumor biopsies from patients (n = 11) with HER2-amplified breast cancer were evaluated for HER2 and P-HER3 expression by immunohistochemistry and/or fluorescence in situ hybridization. ERBB ligands were measured by quantitative reverse transcription polymerase chain reaction. Drug-resistant cells were generated by chronic treatment with T-DM1. All statistical tests were two-sided., Results: Treatment with Pan-HER inhibited growth and promoted degradation of ERBB1-3 receptors in a panel of HER2+ breast cancer cells. Compared with TL, TP, and T-DM1, Pan-HER induced a similar antitumor effect against established BT474 and HCC1954 tumors, but was superior to TL against MDA-361 xenografts (TL mean = 2026 mm 3 , SD = 924 mm 3 , vs Pan-HER mean = 565 mm 3 , SD = 499 mm 3 , P = .04). Pan-HER-treated BT474 xenografts did not recur after treatment discontinuation, whereas tumors treated with TL, TP, and T-DM1 did. Post-TP and post-T-DM1 recurrent tumors expressed higher levels of neuregulin-1 (NRG1), HER3 and P-HER3 (all P < .05). Higher levels of P-HER3 protein and NRG1 mRNA were also observed in HER2+ breast cancers progressing after T-DM1 and trastuzumab (NRG1 transcript fold change ± SD; pretreatment = 2, SD = 1.9, vs post-treatment = 11.4, SD = 10.3, P = .04). The HER3-neutralizing antibody LJM716 resensitized the drug-resistant cells to T-DM1, suggesting a causal association between the NRG1-HER3 axis and drug resistance. Finally, Pan-HER treatment inhibited growth of HR6 trastuzumab- and T-DM1-resistant xenografts., Conclusions: These data suggest that upregulation of a NRG1-HER3 axis can mediate escape from anti-HER2 therapies. Further, multitargeted antibody mixtures, such as Pan-HER, can simultaneously remove and/or block targeted ERBB receptor and ligands, thus representing an effective approach against drug-sensitive and -resistant HER2+ cancers., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please e-mail: journals.permissions@oup.com.)

Published

2017

21. EGFR Kinase Domain Duplication (EGFR-KDD) Is a Novel Oncogenic Driver in Lung Cancer That Is Clinically Responsive to Afatinib.

Author

Gallant JN, Sheehan JH, Shaver TM, Bailey M, Lipson D, Chandramohan R, Red Brewer M, York SJ, Kris MG, Pietenpol JA, Ladanyi M, Miller VA, Ali SM, Meiler J, and Lovly CM

Subjects

Adult, Afatinib, Antineoplastic Agents pharmacology, Drug Resistance, Neoplasm genetics, ErbB Receptors antagonists & inhibitors, ErbB Receptors chemistry, Gene Frequency, Humans, Lung Neoplasms diagnosis, Male, Models, Molecular, Molecular Targeted Therapy, Mutation, Neoplasm Staging, Protein Conformation, Protein Kinase Inhibitors pharmacology, Protein Multimerization, Quinazolines pharmacology, Tomography, X-Ray Computed, Treatment Outcome, Antineoplastic Agents therapeutic use, ErbB Receptors genetics, Gene Duplication, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Protein Interaction Domains and Motifs genetics, Protein Kinase Inhibitors therapeutic use, Quinazolines therapeutic use

Abstract

Unlabelled: Oncogenic EGFR mutations are found in 10% to 35% of lung adenocarcinomas. Such mutations, which present most commonly as small in-frame deletions in exon 19 or point mutations in exon 21 (L858R), confer sensitivity to EGFR tyrosine kinase inhibitors (TKI). In analyzing the tumor from a 33-year-old male never-smoker, we identified a novel EGFR alteration in lung cancer: EGFR exon 18-25 kinase domain duplication (EGFR-KDD). Through analysis of a larger cohort of tumor samples, we detected additional cases of EGFR-KDD in lung, brain, and other cancers. In vitro, EGFR-KDD is constitutively active, and computational modeling provides potential mechanistic support for its auto-activation. EGFR-KDD-transformed cells are sensitive to EGFR TKIs and, consistent with these in vitro findings, the index patient had a partial response to the EGFR TKI afatinib. The patient eventually progressed, at which time resequencing revealed an EGFR-dependent mechanism of acquired resistance to afatinib, thereby validating EGFR-KDD as a driver alteration and therapeutic target., Significance: We identified oncogenic and drug-sensitive EGFR-KDD that is recurrent in lung, brain, and soft-tissue cancers and documented that a patient with metastatic lung adenocarcinoma harboring the EGFR-KDD derived significant antitumor response from treatment with the EGFR inhibitor afatinib. Findings from these studies will be immediately translatable, as there are already several approved EGFR inhibitors in clinical use., (©2015 American Association for Cancer Research.)

Published

2015

22. AZD9291, an irreversible EGFR TKI, overcomes T790M-mediated resistance to EGFR inhibitors in lung cancer.

Author

Cross DA, Ashton SE, Ghiorghiu S, Eberlein C, Nebhan CA, Spitzler PJ, Orme JP, Finlay MR, Ward RA, Mellor MJ, Hughes G, Rahi A, Jacobs VN, Red Brewer M, Ichihara E, Sun J, Jin H, Ballard P, Al-Kadhimi K, Rowlinson R, Klinowska T, Richmond GH, Cantarini M, Kim DW, Ranson MR, and Pao W

Subjects

Acrylamides chemistry, Acrylamides pharmacology, Aniline Compounds chemistry, Aniline Compounds pharmacology, Animals, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cell Proliferation drug effects, Disease Models, Animal, ErbB Receptors chemistry, Female, Genes, erbB-2, Humans, Lung Neoplasms pathology, Male, Middle Aged, Models, Molecular, Molecular Conformation, Phosphorylation, Protein Binding, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacology, Signal Transduction drug effects, Treatment Outcome, Tumor Burden drug effects, Xenograft Model Antitumor Assays, Acrylamides therapeutic use, Aniline Compounds therapeutic use, Antineoplastic Agents therapeutic use, Drug Resistance, Neoplasm genetics, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Mutation, Protein Kinase Inhibitors therapeutic use

Abstract

Unlabelled: First-generation EGFR tyrosine kinase inhibitors (EGFR TKI) provide significant clinical benefit in patients with advanced EGFR-mutant (EGFRm(+)) non-small cell lung cancer (NSCLC). Patients ultimately develop disease progression, often driven by acquisition of a second T790M EGFR TKI resistance mutation. AZD9291 is a novel oral, potent, and selective third-generation irreversible inhibitor of both EGFRm(+) sensitizing and T790M resistance mutants that spares wild-type EGFR. This mono-anilino-pyrimidine compound is structurally distinct from other third-generation EGFR TKIs and offers a pharmacologically differentiated profile from earlier generation EGFR TKIs. Preclinically, the drug potently inhibits signaling pathways and cellular growth in both EGFRm(+) and EGFRm(+)/T790M(+) mutant cell lines in vitro, with lower activity against wild-type EGFR lines, translating into profound and sustained tumor regression in EGFR-mutant tumor xenograft and transgenic models. The treatment of 2 patients with advanced EGFRm(+) T790M(+) NSCLC is described as proof of principle., Significance: We report the development of a novel structurally distinct third-generation EGFR TKI, AZD9291, that irreversibly and selectively targets both sensitizing and resistant T790M(+) mutant EGFR while harboring less activity toward wild-type EGFR. AZD9291 is showing promising responses in a phase I trial even at the first-dose level, with first published clinical proof-of-principle validation being presented., (©2014 American Association for Cancer Research.)

Published

2014

23. Maximizing the benefits of off-target kinase inhibitor activity.

Author

Red Brewer M and Pao W

Subjects

Animals, Humans, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Mutation, Protein Kinase Inhibitors pharmacology

Abstract

Investigators report the identification of novel mutant-specific inhibition of EGF receptor (EGFR) T790M by bis-indole-based inhibitors of protein kinase C using a small-molecule cancer cell line-based screening platform. This study shows the power of high-throughput drug screening in cancer cell lines and provides new lead scaffolds for optimization against resistant EGFR mutants in lung cancer.

Published

2013