Abstract

Lung cancer is the leading cause of cancer-related death worldwide, exceeding that attributable to breast, prostate, colon, kidney, and liver cancer combined. Recently, the identification of recurrent genetic alterations has led to molecularly-targeted therapies for a subset of lung cancers. Activating mutations in RAS-family oncoproteins are among the most frequent genomic alterations in non-small cell lung cancer (NSCLC) and are mutated in up to 30% of all human cancers. Despite intensive efforts to target KRAS, no molecularly targeted therapies exist and patients still receive cytotoxic and largely ineffective chemotherapies. Indeed, direct pharmacological inhibition of mutant RAS has remained difficult, and targeting of other downstream RAS effectors, in particular the MAPK pathway, has been ineffective due to toxicities and adaptive drug resistance mechanisms. In response to the urgent need for developing strategies to target KRAS mutant cancers, this Program Project has explored that action of agents that target the RAS network, producing insights into adaptive resistance mechanisms and characterizing the first direct KRAS mutant inhibitors. Our project, together with Rosen (RP2), established that the rebound in MAPK signaling occurring after MEK inhibition is responsible for adaptive drug resistance and, though a functional genomics screen, identified upstream activation of the FGFR1 signaling axis as contributing to this effect. Consequently, FGFR1 is an induced dependency produced by MEK inhibition and therapeutic approaches targeting MEK and FGFR1 are being developed as a clinical strategy for treating KRAS mutant lung cancers. Our renewal builds on these successes towards the goal of identifying additional combinatorial strategies targeting KRAS mutant cancers. Expanding upon extensive preliminary data, we study effectors required for tumor maintenance in KRAS driven lung cancers treated with MAPK or KRAS inhibitors, explore novel and existing strategies for combinatorial target inhibition, and examine the interplay between pathway inhibition, tissue and genomic context, and immune surveillance. The project builds on existing collaborations and incorporates innovative technology and mouse modeling systems into the program; it interacts with, and benefits from, each of the other projects and cores. Successful completion of the proposed work will provide critical insights into RAS signaling and form a foundation for bringing targeted therapy for KRAS mutant lung cancer into the clinical arena.

Public Health Relevance

Although KRAS is the most frequently mutated oncogene in human lung cancer and represents a compelling therapeutic target, lung cancer patients harboring KRAS mutant cancers are currently treated with ineffective and toxic chemotherapies. This proposal uses optimized genetic and modeling platforms to reveal mechanisms of signaling plasticity and immune surveillance following treatment with RAS network inhibitors with the goal of identifying molecular targeted and/or immune oncology agents that could be used in combination to effectively treat KRAS mutant lung cancers.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA129243-12
Application #
9784748
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2019-09-01
Budget End
2020-08-31
Support Year
12
Fiscal Year
2019
Total Cost
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

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
Ruscetti, Marcus; Leibold, Josef; Bott, Matthew J et al. (2018) NK cell-mediated cytotoxicity contributes to tumor control by a cytostatic drug combination. Science 362:1416-1422
Du, Zhenfang; Lovly, Christine M (2018) Mechanisms of receptor tyrosine kinase activation in cancer. Mol Cancer 17:58
Yu, Helena A; Suzawa, Ken; Jordan, Emmet et al. (2018) Concurrent Alterations in EGFR-Mutant Lung Cancers Associated with Resistance to EGFR Kinase Inhibitors and Characterization of MTOR as a Mediator of Resistance. Clin Cancer Res 24:3108-3118
Westover, D; Zugazagoitia, J; Cho, B C et al. (2018) Mechanisms of acquired resistance to first- and second-generation EGFR tyrosine kinase inhibitors. Ann Oncol 29:i10-i19
Li, Bob T; Shen, Ronglai; Buonocore, Darren et al. (2018) Ado-Trastuzumab Emtansine for Patients With HER2-Mutant Lung Cancers: Results From a Phase II Basket Trial. J Clin Oncol 36:2532-2537
Fan, Pang-Dian; Narzisi, Giuseppe; Jayaprakash, Anitha D et al. (2018) YES1 amplification is a mechanism of acquired resistance to EGFR inhibitors identified by transposon mutagenesis and clinical genomics. Proc Natl Acad Sci U S A 115:E6030-E6038
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

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