Abstract

Despite inducing radiographic regressions in patients whose lung adenocarcinomas harbor somatic mutations in the exons encoding the kinase domain of EGFR, the EGFR tyrosine kinase inhibitors (TKIs), gefitinib and erlotinib, rarely induce complete responses and do not cure patients. This suggests that not all lung adenocarcinoma cells """"""""respond"""""""" by undergoing cell death and/or that there are potential defects in pathways within cells that prevent complete tumor elimination. Consistent with this, in our preliminary studies, we have identified four human EGFR-mutant cell lines that appear """"""""addicted"""""""" to mutant EGFR, i.e., they display nanomolarsensitivity to erlotinib;however, while three of these cell lines undergo apoptosis when exposed to erlotinib, one line does not. The goal of this project - which is a logical extension ofour published work - is to understand further why EGFR mutant cells persist after initial treatment with EGFR TKIs. These studies will be bolstered by cooperation with the other co-investigators in this application, through the sharing of data, protocols, and reagents, and the formation and use of core facilities. Using human lung adenocarcinoma cell lines and xenografts, human lung adenocarcinomas, and mouse lung adenocarcinomas, all of which harbor EGFR kinase domain mutations, and a variety of molecular, biochemical, and pharmacological approaches, our specific aims are to: 1) define the mode of response to EGFR TKIs in drug-""""""""sensitive"""""""" EGFR mutant cells, 2) identify collateral targets in erlotinib-sensitive EGFR mutant cells that could be manipulated to maximize tumor cell killing, and 3) correlate our findings from Aims 1 and 2 with data from a unique collection of human lung adenocarcinoma specimens obtained from patients with """"""""persistent"""""""" disease, i.e., with EGFR-mutant cancer cells remaining after initial short-term treatment with EGFR TKIs. An enhanced understanding of the molecular events involved in """"""""persistent"""""""" disease could 1) lead to the identification of new targets to optimize tumor cell death, 2) provide insight into subsequent mechanisms of acquired resistance to EGFR TKIs, and 3) establish a framework upon which to prioritize the study of new anti-apoptotic drugs emerging in the clinic.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA129243-03
Application #
7893053
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2009-07-01
Budget End
2010-06-30
Support Year
3
Fiscal Year
2009
Total Cost
$220,515
Indirect Cost

  Institution

Name
Sloan-Kettering Institute for Cancer Research
Department
Type
DUNS #
064931884
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Mo, Qianxing; Shen, Ronglai; Guo, Cui et al. (2018) A fully Bayesian latent variable model for integrative clustering analysis of multi-type omics data. Biostatistics 19:71-86
Childress, Merrida A; Himmelberg, Stephen M; Chen, Huiqin et al. (2018) ALK Fusion Partners Impact Response to ALK Inhibition: Differential Effects on Sensitivity, Cellular Phenotypes, and Biochemical Properties. Mol Cancer Res 16:1724-1736
Gao, Yijun; Chang, Matthew T; McKay, Daniel et al. (2018) Allele-Specific Mechanisms of Activation of MEK1 Mutants Determine Their Properties. Cancer Discov 8:648-661
Arbour, Kathryn C; Jordan, Emmett; Kim, Hyunjae Ryan et al. (2018) Effects of Co-occurring Genomic Alterations on Outcomes in Patients with KRAS-Mutant Non-Small Cell Lung Cancer. Clin Cancer Res 24:334-340
Gallant, Jean-Nicolas; Lovly, Christine M (2018) Established, emerging and elusive molecular targets in the treatment of lung cancer. J Pathol 244:565-577
Hellmann, Matthew D; Nathanson, Tavi; Rizvi, Hira et al. (2018) Genomic Features of Response to Combination Immunotherapy in Patients with Advanced Non-Small-Cell Lung Cancer. Cancer Cell 33:843-852.e4
Yao, Zhan; Gao, Yijun; Su, Wenjing et al. (2018) RAF inhibitor PLX8394 selectively disrupts BRAF dimers and RAS-independent BRAF-mutant-driven signaling. Nat Med :
Suzawa, Ken; Offin, Michael; Lu, Daniel et al. (2018) Activation of KRAS Mediates Resistance to Targeted Therapy in MET Exon 14-mutant Non-small Cell Lung Cancer. Clin Cancer Res :
Yu, Helena A; Planchard, David; Lovly, Christine M (2018) Sequencing Therapy for Genetically Defined Subgroups of Non-Small Cell Lung Cancer. Am Soc Clin Oncol Educ Book :726-739
Yuan, Tina L; Amzallag, Arnaud; Bagni, Rachel et al. (2018) Differential Effector Engagement by Oncogenic KRAS. Cell Rep 22:1889-1902

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