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Project Details

Development of Orexin-1 Receptor Antagonists for Drug Addiction

Project Number5P01DA033622-02

Contact PI/Project LeaderKAMENECKA, THEODORE M
Other PIs

Awardee OrganizationSCRIPPS RESEARCH INSTITUTE, THE

Description

Abstract Text

DESCRIPTION (provided by applicant): This application describes a highly integrated series of projects aiming to develop orexin-1 (OX1) receptor antagonists for treatment of tobacco dependence. Project 1 will utilize iterative medicinal chemistry based on structure-activity relationships (SAR) to discover new classes of potent and selective OX1 receptor antagonists. SAR will be used to optimize new classes of OX1 receptor antagonists for drug metabolism and pharmacokinetics (DMPK), and brain penetration properties. We have already generated excellent OX1 receptor antagonists as starting points for SAR based on our ongoing medicinal chemistry efforts. Project 2 will support SAR by testing new compounds in in vitro cell-based functional assays for OX1 receptors (and appropriate counter-screens) to determine potency and selectivity. We have already established and validated a range of OX1 receptor cell-based assays, and have successfully used these assays to identify starting points for SAR. Project 3 will test new classes of potent and selective OX1 receptor antagonists to identify those with the most favorable physiochemical and brain penetration profiles, and identify those least likely to have toxicity in humans. Project 4 will test the in vivo efficacy of novel OX1 receptor antagonists in cutting-edge behavioral procedures that assess addiction-related behavioral effects of nicotine. Importantly, have developed a new IV nicotine self-administration procedure for mice, and will assess novel OX1 receptor antagonists in wild type and OX1 receptor knockout mice to determine their behavioral selectivity. This integrated multidisciplinary research plan will capitalize on the unique drug discovery capabilities at Scripps Florida, and promises to yield novel therapeutic entities for the prevention of relapse in human tobacco smokers.

Public Health Relevance Statement

Tobacco smoking results in greater than 5 million deaths each year. Even when using the most effective smoking cessation agents available, approximately 80% of smoking attempting to quit will relapse. We plan to develop novel therapeutics to facilitate smoking cessation based on an entirely new mechanism of action, which may have a significant positive impact on human health. OVERALL PROGRAM PROJECT

NIH Spending Category

No NIH Spending Category available.

Project Terms

AccountingAnimal ModelBehaviorBehavioralBiological AssayBrainCalciumCell LineCellsCessation of lifeCircadian RhythmsClinicalClinical assessmentsCuesCyclic AMPDataDevelopmentDiseaseDrug AddictionDrug KineticsDrug TargetingDrug toxicityFamilyFloridaFluorescenceG alpha q ProteinGoalsHealthHumanHypothalamic structureIn VitroInositol PhosphatesInterdisciplinary StudyIntravenousKnockout MiceLaboratoriesLateralMalignant neoplasm of lungMediatingMetabolicMonitorMusNeuronsNeuropeptidesNicotineNicotine DependencePathway interactionsPenetrationPharmaceutical ChemistryPharmaceutical PreparationsPlayPre-Clinical ModelProceduresPropertyRattusReceptor CellRelapseResearchRewardsRoleSelf AdministrationSelf StimulationSeriesSignal TransductionSiteSmokerSmokingStressStructure-Activity RelationshipSubstance abuse problemSystemTestingTherapeutic AgentsTimeTobaccoTobacco DependenceTobacco smokeTobacco smokingToxic effectWild Type Mouseaddictionbasebehavior testdisorder later incidence preventiondrug addictdrug discoverydrug metabolismheuristicshypocretinin vivonovelnovel therapeuticsnull mutationorexin 1 receptororexin Aorexin Borexin B receptorreceptorreceptor couplingreceptor functionreceptor internalizationresponsescreeningsmoking cessationtooltransmission process

Details

Contact PI/ Project Leader

Name

KAMENECKA, THEODORE M

Title

Contact

Other PIs

Name

KENNY, PAUL J.

Program Official

Name

SHIH, MING L

Contact

Organization

Name

SCRIPPS RESEARCH INSTITUTE, THE

City

LA JOLLA

Country

UNITED STATES (US)

Department Type

Unavailable

Organization Type

Other Domestic Non-Profits

State Code

Congressional District

Other Information

Opportunity Number

RFA-DA-12-005

Study Section

ZDA1-JXR-D(09)R

Fiscal Year

2013

Award Notice Date

17-April-2013

Administering Institutes or Centers

National Institute on Drug Abuse

CFDA Code

279

DUNS Number

781613492

UEI

PHZJFZ32NKH4

Project Start Date

15-May-2012

Project End Date

31-August-2017

Budget Start Date

01-May-2013

Budget End Date

31-August-2014

Project Funding Information for 2013

Total Funding

$1,624,668

Direct Costs

$820,540

Indirect Costs

$804,128

Year	Funding IC	FY Total Cost by IC
2013	National Institute on Drug Abuse	$1,624,668

Sub Projects

No Sub Projects information available for 5P01DA033622-02

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 5P01DA033622-02

Patents

No Patents information available for 5P01DA033622-02

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 5P01DA033622-02

Clinical Studies

No Clinical Studies information available for 5P01DA033622-02

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