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Project Details

Regulation of Claudin-1 mediated Colon Tumor Progression and Metastasis

Project Number3R01CA124977-04S1

Contact PI/Project LeaderDHAWAN, PUNITA

Awardee OrganizationVANDERBILT UNIVERSITY

Description

Abstract Text

DESCRIPTION (provided by applicant): Changes in the expression and/or cellular localization of cell-cell junction proteins is a hallmark of tumorigenesis, especially metastasis and invasion. The role of adherent junction proteins has been studied extensively in cancer; however, the role of tight junction proteins is less well understood. Claudins are a family of recently identified proteins that are integral to the structure and function of tight junctions (TJs). Recent studies have shown differential and tissue specific changes in expression/cellular localization for claudins during tumorigenesis; however, a cause and effect relationship has yet to be established. We have recently reported that in colon cancer, claudin-1 expression is increased in a tumor stage specific manner (normal>carcinoma>metastasis), and is predominantly localized to cell nucleus and cytoplasm. Most importantly, using over-expression or genetic inhibition of claudin-1 in non-metastatic & highly metastatic colon cancer cells, we demonstrated a role of claudin-1 in the regulation of tumor progression and metastasis. In this grant proposal, we have extended our previous studies to the determination of mechanism underlying the role of claudin-1 as a tumor promoter and metastasis. Since, metastasis is the principal cause of tumor related deaths, we have elected to first define the signaling and molecular mechanisms using anoikis as the model of study, which could potentially be applicable to in vivo model of metastasis and invasion. In addition, we have proposed to examine the mechanisms underlying the novel nuclear localization of claudin-1 in colon metastasis samples and cell lines and its correlation with metastasis. Also, we have proposed to determine the regulation of colon cancer specific expression/cellular localization of claudin-1 through the regulation of APC. It is noteworthy that APC mutation is a hallmark of colorectal cancer. The work described in this proposal is intended to provide insight for the mechanism of claudin-1 mediated regulation as well as its regulation and would help in future studies for development of therapeutic reagents or small molecule inhibitors to test their clinical relevance.

Public Health Relevance Statement

Data not available.

NIH Spending Category

CancerColo-Rectal CancerDigestive Diseases

Project Terms

Adenomatous Polyposis ColiAnoikisApplications GrantsCancer cell lineCarcinomaCell LineCell NucleusCellsCessation of lifeColonColon CarcinomaColonic NeoplasmsColorectal CancerCytoplasmDataDiagnostic Neoplasm StagingE-CadherinFamilyFrequenciesFutureGeneticGenus ColaGrowthIntegrinsIntercellular JunctionsInvestigationMalignant NeoplasmsMediatingMolecularMutationNeoplasm MetastasisNuclearNuclear ExportPathway interactionsPlayProteinsReagentRegulationReportingResistanceRoleSamplingSignal TransductionStructureStudy modelsTestingTight JunctionsTissue SampleTissuesTranscriptional RegulationTumor PromotersTumor Suppressor ProteinsTumor stageWorkadherent junctionapical membranebasecancer cellclaudin-1 proteinclinically relevantcolon carcinogenesishuman tissuein vivo Modelinhibitor/antagonistinsightmetastatic colorectalmouse modelnovelprotein protein interactionsmall moleculetherapeutic developmenttumortumor growthtumor progressiontumorigenesis

Details

Contact PI/ Project Leader

Name

DHAWAN, PUNITA

Title

Contact

Other PIs

Not Applicable

Program Official

Name

OGUNBIYI, PETER

Contact

Organization

Name

VANDERBILT UNIVERSITY

City

Nashville

Country

UNITED STATES (US)

Department Type

SURGERY

Organization Type

SCHOOLS OF MEDICINE

State Code

Congressional District

Other Information

Opportunity Number

Study Section

Tumor Microenvironment Study Section[TME]

Fiscal Year

2010

Award Notice Date

07-September-2010

Administering Institutes or Centers

National Cancer Institute

CFDA Code

396

DUNS Number

965717143

UEI

GTNBNWXJ12D5

004413456

DWH7MSXKA2A8

Project Start Date

05-July-2007

Project End Date

31-May-2012

Budget Start Date

01-June-2010

Budget End Date

31-May-2011

Project Funding Information for 2010

Total Funding

$44,293

Direct Costs

$28,789

Indirect Costs

$15,504

Year	Funding IC	FY Total Cost by IC
2010	National Cancer Institute	$44,293

NIH Categorical SpendingClick here for more information on NIH Categorical Spending

Funding IC	FY Total Cost by IC	NIH Spending Category
NATIONAL CANCER INSTITUTE	$44,293	Cancer; Colo-Rectal Cancer; Digestive Diseases

Sub Projects

No Sub Projects information available for 3R01CA124977-04S1

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 3R01CA124977-04S1

Patents

No Patents information available for 3R01CA124977-04S1

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 3R01CA124977-04S1

Clinical Studies

No Clinical Studies information available for 3R01CA124977-04S1

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