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Project Details

RHO PROTEINS AND MASS SPECTROMETRY

Parent Project Number2P41RR000954-33

Sub-Project ID8583

Contact PI/Project LeaderPETERSON, JEFFREY R

Awardee OrganizationWASHINGTON UNIVERSITY

Description

Abstract Text

This subproject is one of many research subprojects utilizing the resources provided by a Center grant funded by NIH/NCRR. The subproject and investigator (PI) may have received primary funding from another NIH source, and thus could be represented in other CRISP entries. The institution listed is for the Center, which is not necessarily the institution for the investigator. Like Ras, the Rho family of small GTP-binding proteins contributes to tumorigenesis and metastasis through the activation of downstream effector proteins. In response to diverse upstream signals, Rho proteins exchange bound GDP for GTP and can then bind and activate a very large and functionally diverse set of effectors including enzymes and scaffolding proteins. These effectors mediate complex cellular responses including cell cycle progression, cytoskeletal rearrangements, cell polarity, and gene transcription but how they contribute to the cancer phenotype is largely unknown. Our long-term goal is to provide a comprehensive and quantitative description of the signaling pathways operating through the Rho proteins and to understand the biological importance of these pathways, how they are regulated, and how they are corrupted in human diseases. One major approach we are using to elucidate the functions of particular effectors is the identification of small-molecule inhibitors for specific effectors through high-throughput screening. These drug-like molecules are then used to reveal the consequence of protein loss of function, as small-molecule inhibitors are powerful tools to explore the biology of highly dynamic signaling pathways (Peterson and Mitchison, Chem. Biol., 9: 1275, 2002). In addition, these compounds may represent leads for novel therapeutics. Since many Rho family effectors are regulated by autoinhibition, we are particularly interested in compounds that inhibit effectors by allosterically stabilizing their native, autoinhibited conformation. We have proposed that this strategy could be used to develop highly specific inhibitors of a large class of signaling proteins that play central roles in cancer in other diseases but that have been largely ignored by the pharmaceutical industry (Peterson and Golemis, J. Cell. Biochem., 93: 68, 2004)--from Peterson Web Site.

Public Health Relevance Statement

Data not available.

NIH Spending Category

BiotechnologyCancer

Project Terms

BindingBiologicalBiologyCell Cycle ProgressionCell PolarityCellsComplexComputer Retrieval of Information on Scientific Projects DatabaseDNA Sequence RearrangementDiseaseDrug IndustryEnzymesFamilyFundingGTP-Binding ProteinsGenetic TranscriptionGoalsGrantGuanosine TriphosphateInstitutionMalignant NeoplasmsMass Spectrum AnalysisMediatingMolecular ConformationNeoplasm MetastasisPathway interactionsPharmaceutical PreparationsPhenotypePlayProteinsResearchResearch PersonnelResourcesRoleScaffolding ProteinSignal PathwaySignal TransductionSignaling ProteinSourceUnited States National Institutes of Healthhigh throughput screeninghuman diseaseinhibitor/antagonistinterestloss of functionnovel therapeuticsresponserhosmall moleculetooltumorigenesisweb site

Details

Contact PI/ Project Leader

Name

PETERSON, JEFFREY R

Title

Contact

Other PIs

Not Applicable

Program Official

Name

Contact

Email not available

Organization

Name

WASHINGTON UNIVERSITY

City

SAINT LOUIS

Country

UNITED STATES (US)

Department Type

INTERNAL MEDICINE/MEDICINE

Organization Type

SCHOOLS OF MEDICINE

State Code

Congressional District

Other Information

Opportunity Number

PAR-08-259

Study Section

Special Emphasis Panel[ZRG1-BCMB-K(40)P]

Fiscal Year

2010

Award Notice Date

10-March-2010

Administering Institutes or Centers

National Center for Research Resources

CFDA Code

389

DUNS Number

068552207

UEI

L6NFUM28LQM5

Project Start Date

10-March-2010

Project End Date

31-December-2010

Budget Start Date

10-March-2010

Budget End Date

31-December-2010

Project Funding Information for 2010

Total Funding

$191

Direct Costs

$151

Indirect Costs

$40

Year	Funding IC	FY Total Cost by IC
2010	National Center for Research Resources	$191

NIH Categorical SpendingClick here for more information on NIH Categorical Spending

Funding IC	FY Total Cost by IC	NIH Spending Category
NATIONAL CENTER FOR RESEARCH RESOURCES	$191	Biotechnology; Cancer

Sub Projects

No Sub Projects information available for 2P41RR000954-33 8583

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 2P41RR000954-33 8583

Patents

No Patents information available for 2P41RR000954-33 8583

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 2P41RR000954-33 8583

Clinical Studies

No Clinical Studies information available for 2P41RR000954-33 8583

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