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Project Details

INHIBITING SURFACE HSP90 TO LIMIT METASTASIS

Project Number5R01CA116642-04

Contact PI/Project LeaderJAY, DANIEL G.

Awardee OrganizationTUFTS UNIVERSITY BOSTON

Description

Abstract Text

DESCRIPTION (provided by applicant): The vast majority of breast cancer-related deaths are due to secondary tumors after metastasis. There is currently no effective therapy to limit metastasis. Our long term objective is to develop new therapies that reduce cancer invasion, a critical first step in metastasis. This proposal is based on our observations that a novel extracellular form of the molecular chaperone hsp90a is required for cancer invasion by the activation of the matrix metalloproteinase MMP2. Hsp90 has been implicated in cancer and hsp90 inhibitors with anti-tumor activity are currently in clinical trials. These drugs may be problematic in that they interfere with the many intracellular functions of hsp90. Our findings suggest our main hypothesis that inhibiting extracellular hsp90a will decrease invasion and thus limit metastasis. This presents an opportunity for novel anti-cancer therapy by inhibiting invasion without interfering with the myriad intracellular functions of hsp90. To support this idea, we will address three specific aims. We will determine the mechanism of how hsp90a functions on the outside of cancer cells (Aim 1). We will then use this information to develop and test extracellular hsp90 inhibitors (Aim 2). We already have one impermeant hsp90 inhibitor in hand and several candidates for neutralizing single chain antibodies from our collaborators at NCI and Xerion Pharmaceuticals. Finally, we will test the best of these inhibitors of extracellular hsp90a for their ability to limit metastasis in a new model developed by our collaborators at Tufts using human breast cancer cells metastasizing to human bone explants in immunocompromised mice (Aim 3). Thus, these experiments take us from an initial discovery of hsp90a function with cell-based assays to in vivo animal models taking an interdisciplinary approach to address a key issue of human health: limiting metastasis to improve breast cancer prognosis. These studies aim to expedite the translation of our basic research into a potential therapy. If successful, the proposed work would provide data for developing future clinical studies and thus impact human health.

Public Health Relevance Statement

Data not available.

NIH Spending Category

BiotechnologyBreast CancerCancer**Orphan Drug

Project Terms

ATP phosphohydrolaseAddressAnimal ModelAntibodiesBasic ScienceBindingBiological AssayBlocking AntibodiesBone TissueBreast Cancer CellBreast CarcinomaCancer PrognosisCell surfaceCellsCessation of lifeClinicalClinical ResearchClinical TrialsCombined Modality TherapyDataDevelopmentDrug KineticsEnd PointExtracellular MatrixFutureGelatinase AGenesGoalsHandHealthHumanHumulusImageImmunocompromised HostIn VitroLeadLibrariesLightLuciferasesMDA MB 231MMP2 geneMalignant Epithelial CellMalignant NeoplasmsMass Spectrum AnalysisMatrix MetalloproteinasesMembraneMembrane ProteinsModelingMolecular ChaperonesMusNeoplasm MetastasisPathway interactionsPeptide Signal SequencesPhage DisplayPharmaceutical PreparationsPharmacologic SubstancePrimary NeoplasmProcessProtein IsoformsProtein OverexpressionProteinsProteomePusReagentResearch PersonnelRoleScreening procedureSurfaceTestingTherapeuticTimeToxic effectTranslational ResearchTranslationsWorkXenograft Modelanimal databasebonecancer cellcancer therapydosageexperienceextracellularfibrosarcomafluorophoreimprovedin vitro Modelin vivoinhibitor/antagonistinterdisciplinary approachmalignant breast neoplasmmutantneutralizing antibodynovelprogramsprotein functionreagent testingresearch studyscaffoldsmall moleculetumor

Details

Contact PI/ Project Leader

Name

JAY, DANIEL G.

Title

PROFESSOR

Contact

Other PIs

Not Applicable

Program Official

Name

FORRY, SUZANNE L

Contact

Organization

Name

TUFTS UNIVERSITY BOSTON

City

BOSTON

Country

UNITED STATES (US)

Department Type

PHYSIOLOGY

Organization Type

SCHOOLS OF MEDICINE

State Code

Congressional District

Other Information

Opportunity Number

Study Section

Developmental Therapeutics Study Section[DT]

Fiscal Year

2008

Award Notice Date

30-May-2008

Administering Institutes or Centers

National Cancer Institute

CFDA Code

395

DUNS Number

039318308

UEI

C1F5LNUF7W86

Project Start Date

01-August-2005

Project End Date

31-May-2010

Budget Start Date

01-June-2008

Budget End Date

31-May-2009

Project Funding Information for 2008

Total Funding

$275,562

Direct Costs

$168,539

Indirect Costs

$107,023

Year	Funding IC	FY Total Cost by IC
2008	National Cancer Institute	$275,562

NIH Categorical SpendingClick here for more information on NIH Categorical Spending

Funding IC	FY Total Cost by IC	NIH Spending Category
NATIONAL CANCER INSTITUTE	$275,562	Biotechnology; Breast Cancer; Cancer; Orphan Drug

Sub Projects

No Sub Projects information available for 5R01CA116642-04

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 5R01CA116642-04

Patents

No Patents information available for 5R01CA116642-04

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 5R01CA116642-04

Clinical Studies

No Clinical Studies information available for 5R01CA116642-04

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