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Project Details

Overcoming resistance to tyrosine kinase inhibitors in lung cancer

Project Number5R01CA169259-05

Former Number5R01CA169259-04

Contact PI/Project LeaderKOBAYASHI, SUSUMU

Awardee OrganizationBETH ISRAEL DEACONESS MEDICAL CENTER

Description

Abstract Text

DESCRIPTION (provided by applicant): The discovery of somatic mutations in epidermal growth receptor (EGFR) in patients who show dramatic response to reversible EGFR tyrosine kinase inhibitors (TKIs) gefitinib or erlotinib has introduced the concept of "personalized therapy in lung cancer treatment. However, resistance to the inhibitors emerges within one to two years. The secondary EGFR-T790M mutation, in the "gate-keeper" position of the tyrosine kinase domain, is present in more than 50% of lung cancers with acquired resistance to gefitinib or erlotinib. Since treatment options for these patients are currently limited, novel strategies to prevent or overcome acquired resistance to EGFR TKIs are sorely needed. We have demonstrated that ß-catenin is upregulated and activated in lung cancer cells harboring EGFR mutations including EGFR-T790M. As aberrant activation of ß-catenin signaling can lead to human cancers, we hypothesize that ß-catenin plays an essential role in lung tumorigenesis caused by EGFR mutants and inhibiting its activation alone or in combination with irreversible EGFR inhibitors may be an alternative strategy to overcome resistance to gefitinib or erlotinib. Therefore, our specific aims are to: (1) Investigate the mechanisms by which EGFR mutants lead to accumulation, nuclear translocation, and activation of �-catenin; (2) Investigate whether activation of ß-catenin is required for EGFR- T790M-driven lung cancer formation/progression in vivo; and (3) Evaluate the effectiveness of ß-catenin inhibition as a novel therapeutic strategy to overcome resistance to erlotinib or gefitinib. We believe that the experiments proposed here will provide novel insights into the detailed mechanisms by which EGFR mutations cause tumorigenesis and innovative approaches to overcome resistance to gefitinib or erlotinib, significantly impacting care of patients with lung cancer in the near future.

Public Health Relevance Statement

PUBLIC HEALTH RELEVANCE: Lung cancer is number one cause of cancer-related deaths in the United States. Our major goal is to investigate the role of the ß-catenin signaling in tumors resistant to targeted therapies. A better understanding of lung tumorigenesis will lead to novel therapeutic strategies in the future.

NIH Spending Category

CancerLungLung Cancer

Project Terms

Amino AcidsBindingCancer EtiologyCancer cell lineCellsCessation of lifeClinicalClinical ResearchComplexDevelopmentDiagnostic radiologic examinationDissociationE-CadherinEGF geneEffectivenessEpidermal Growth Factor ReceptorErlotinibFutureGatekeepingGefitinibGenesGoalsGrowthGrowth FactorHumanLeadLung NeoplasmsMalignant NeoplasmsMalignant neoplasm of lungMediatingMethionineModelingMusMutationNon-Small-Cell Lung CarcinomaNuclear TranslocationOncogenicPathway interactionsPatient CarePatientsPlayPositioning AttributeProto-Oncogene Proteins c-aktReporterResistanceRoleSignal TransductionSomatic MutationTestingThreonineTransgenic MiceTransplantationTyrosine Kinase DomainTyrosine Kinase InhibitorTyrosine PhosphorylationUnited StatesWorkalpha cateninbasebeta catenincancer cellcancer therapychemotherapyexperimental studyglycogen synthase kinase 3 betain vivoinhibitor/antagonistinnovationinsightlung tumorigenesismouse modelmutantnovelnovel strategiesnovel therapeutic interventionnovel therapeuticspersonalized medicinepreventpublic health relevancereceptorresponsesmall moleculestandard caretargeted treatmenttumortumor growthtumor initiationtumorigenesis

Details

Contact PI/ Project Leader

Name

KOBAYASHI, SUSUMU

Title

ASSOCIATE PROFESSOR

Contact

Other PIs

Not Applicable

Program Official

Name

ALLEY, MICHAEL C

Contact

Organization

Name

BETH ISRAEL DEACONESS MEDICAL CENTER

City

BOSTON

Country

UNITED STATES (US)

Department Type

Unavailable

Organization Type

Independent Hospitals

State Code

Congressional District

Other Information

Opportunity Number

PA-11-260

Study Section

Basic Mechanisms of Cancer Therapeutics Study Section[BMCT]

Fiscal Year

2017

Award Notice Date

02-March-2017

Administering Institutes or Centers

National Cancer Institute

CFDA Code

395

DUNS Number

071723621

UEI

C1CPANL3EWK4

Project Start Date

06-March-2013

Project End Date

28-February-2019

Budget Start Date

01-March-2017

Budget End Date

28-February-2018

Project Funding Information for 2017

Total Funding

Direct Costs

Indirect Costs

Year	Funding IC	FY Total Cost by IC
2017	National Cancer Institute	$1

NIH Categorical SpendingClick here for more information on NIH Categorical Spending

Funding IC	FY Total Cost by IC	NIH Spending Category
NATIONAL CANCER INSTITUTE	$1	Cancer; Lung; Lung Cancer

Sub Projects

No Sub Projects information available for 5R01CA169259-05

Publications

Publications are associated with projects, but cannot be identified with any particular year of the project or fiscal year of funding. This is due to the continuous and cumulative nature of knowledge generation across the life of a project and the sometimes long and variable publishing timeline. Similarly, for multi-component projects, publications are associated with the parent core project and not with individual sub-projects.

No Publications available for 5R01CA169259-05

Patents

No Patents information available for 5R01CA169259-05

Outcomes

The Project Outcomes shown here are displayed verbatim as submitted by the Principal Investigator (PI) for this award. Any opinions, findings, and conclusions or recommendations expressed are those of the PI and do not necessarily reflect the views of the National Institutes of Health. NIH has not endorsed the content below.

No Outcomes available for 5R01CA169259-05

Clinical Studies

No Clinical Studies information available for 5R01CA169259-05

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