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Project Details

THE ROLE OF TELOMERASE REGULATORS IN TELOMERE MAINTENANCE AND GENOMIC INSTABILITY

Project Number1R01CA211653-01

Contact PI/Project LeaderSONGYANG, ZHOU

Awardee OrganizationBAYLOR COLLEGE OF MEDICINE

Description

Abstract Text

Project Summary Mammalian chromosome ends or telomeres are tightly regulated by the telomerase that mediates telomere elongation and telomere-binding proteins that cap and protect telomere ends. Telomere DNA normally adopts a closed conformation, capped and protected by a multitude of telomere-binding proteins, to prevent DNA damage and genome instability. Telomeres become open and linear during DNA replication to enable telomerase access for telomere elongation. Exposed and critically short telomeres, as a result of mutations in telomerase and telomere regulators, also become open and susceptible to damage and genome instability, ultimately leading to cancer. Mutations in telomere-binding proteins and the TERT promoter have been identified in a number of cancers. Most cancer cells have up-regulated telomerase expression and activities, and cancer cells appear highly sensitive to perturbations in telomerase activities and telomere capping, making the telomerase attractive for therapeutic targeting. A comprehensive study of telomerase regulators therefore should greatly facilitate our understanding of telomerase dysregulation in cancer and the discovery of new drug targets. We have developed an arrayed whole-genome protein interaction network screening strategy based on the Bi-molecular Fluorescence Protein Complementation (BiFC) assay. A pilot TERT BiFC screen identified several proteins as key components of the telomerase complex, including a protein we named TARP1 that has never been characterized before. We propose here to screen genome wide for cell cycle-dependent regulators of the telomerase, and to examine the mechanisms and function of the TARP1-telomerase complex. We will use inducible TARP1 knockout cells generated by CRISPR/Cas9 as well as mouse xenograft models for these studies. Our work will have important implications in devising effective treatment strategies for cancers that result from telomere dysfunction induced genome instability.

Public Health Relevance Statement

Project Narrative Mammalian telomeres are maintained by the telomerase that mediates telomere elongation and telomere-binding proteins that cap and protect telomere ends. We will examine the consequences of disrupting the regulation of telomerase regulators in cells and animal models. These studies will have important implications in devising effective treatment strategies for cancers that result from telomere dysfunction induced genome instability.

NIH Spending Category

CancerGeneticsHuman Genome

Project Terms

AdoptedAffectAnimal ModelBiogenesisBiological AssayBiologyCRISPR/Cas technologyCancer Cell GrowthCancer EtiologyCell CycleCell modelCellsChronic Lymphocytic LeukemiaComplementComplexDNADNA DamageDNA FoldingDNA biosynthesisDataDevelopmentDyskeratosis CongenitaFluorescenceFunctional disorderGenomic InstabilityGrantGrowthHoloenzymesHumanInvestigationKnock-outLeadLengthLibrariesLinkMalignant NeoplasmsMammalian ChromosomesMediatingMethodsMolecularMolecular ConformationMusMutationNamesOncogenicOpen Reading FramesPathway interactionsPatientsPhysiologicalPredispositionProteinsRegulationRoleStudy modelsTelomeraseTelomere CappingTelomere MaintenanceTelomere ShorteningTelomere-Binding ProteinsValidationVitronectinWorkXenograft Modelbasecancer cellcancer diagnosiscancer therapyeffective therapyfollow-upgenetic regulatory proteingenome-wide analysismelanomamutantnew therapeutic targetnoveloverexpressionpreventpromoterscreeningtelomeretelomere losstherapeutic targettraffickingtreatment strategytumortumor growthwhole genome

Details

Contact PI/ Project Leader

Name

SONGYANG, ZHOU

Title

Contact

Other PIs

Not Applicable

Program Official

Name

WITKIN, KEREN L

Contact

Organization

Name

BAYLOR COLLEGE OF MEDICINE

City

HOUSTON

Country

UNITED STATES (US)

Department Type

BIOCHEMISTRY

Organization Type

SCHOOLS OF MEDICINE

State Code

Congressional District

Other Information

Opportunity Number

PA-13-302

Study Section

Cancer Genetics Study Section[CG]

Fiscal Year

2017

Award Notice Date

27-December-2016

Administering Institutes or Centers

National Cancer Institute

CFDA Code

393

DUNS Number

051113330

UEI

FXKMA43NTV21

Project Start Date

01-January-2017

Project End Date

31-December-2021

Budget Start Date

01-January-2017

Budget End Date

31-December-2017

Project Funding Information for 2017

Total Funding

$362,569

Direct Costs

$228,750

Indirect Costs

$133,819

Year	Funding IC	FY Total Cost by IC
2017	National Cancer Institute	$362,569

NIH Categorical SpendingClick here for more information on NIH Categorical Spending

Funding IC	FY Total Cost by IC	NIH Spending Category
NATIONAL CANCER INSTITUTE	$362,569	Cancer; Genetics; Human Genome

Sub Projects

No Sub Projects information available for 1R01CA211653-01

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 1R01CA211653-01

Patents

No Patents information available for 1R01CA211653-01

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 1R01CA211653-01

Clinical Studies

No Clinical Studies information available for 1R01CA211653-01

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