grant

Precision Medicine Approaches to Obesity Pharmacotherapy in Youth with Severe Obesity

Organization UNIVERSITY OF MINNESOTALocation MINNEAPOLIS, UNITED STATESPosted 1 Aug 2020Deadline 31 May 2026
NIHUS FederalResearch GrantFY20242,3-4,5-bis-O-(1-methylethylidene)-beta-D-fructopyranose sulfamate21+ years old4-Aminobutanoic Acid4-Aminobutyric Acid4-amino-butanoic acidAdultAdult HumanAdult-Onset Diabetes MellitusAffectAgeAgonistAminalonAminaloneAntidiabetic HormoneAppetiteAppetite stimulatedApplied GeneticsBMIBMI percentileBMI z-scoreBasic ResearchBasic ScienceBehavioralBinge EatingBody Weight decreasedBody mass indexCarbonate hydro-lyaseCarbonic AnhydrasesCardiovascular DiseasesCareer Development AwardsCareer Development Awards and ProgramsCareer Development Programs K-SeriesCategoriesCharacteristicsChildhoodClinicalClinical ResearchClinical StudyCo-TransportersD-GlucoseDNADataDeoxyribonucleic AcidDesire for foodDextroseDopamineDoseDrug KineticsDrug PrescribingDrug PrescriptionsDrug TherapyDrugsEXTMREating BehaviorEffectivenessElectronic Health RecordExtramuralExtramural ActivitiesFDA approvedFastingFemaleFundingFutureGABAGLP-1GLP-1 receptorGLP-I receptorGenesGeneticGenetic PredispositionGenetic Predisposition to DiseaseGenetic RiskGenetic SusceptibilityGenetic propensityGlucagonGlucoseGlukagonGlutamatesGoalsHG-FactorHealthHydroxytyramineHyperglycemic-Glycogenolytic FactorIncreased food appetiteIndividualInfrastructureInherited PredispositionInherited SusceptibilityInterventionIntervention StrategiesInvestigatorsK-AwardsK-Series Research Career ProgramsKetosis-Resistant Diabetes MellitusL-GlutamateLife Style ModificationMaturity-Onset Diabetes MellitusMedicationMedicineMentorshipMetabolicMethodsMorbid ObesityNIDDMNa elementNational Institutes of HealthNon-Insulin Dependent DiabetesNon-Insulin-Dependent Diabetes MellitusNoninsulin Dependent DiabetesNoninsulin Dependent Diabetes MellitusObesityOutcomePK/PDParticipantPathway interactionsPatientsPersonsPharmaceutical PreparationsPharmacogenomicsPharmacokineticsPharmacological TreatmentPharmacotherapyPhenotypePhysiciansPlayPopulationPredictive FactorProspective, cohort studyQuetelet indexRegimenResearchResearch Career ProgramResearch PersonnelResearchersRetrospective cohort studyRiskRoleScientistSeizuresSevere obesitySingle Base PolymorphismSingle Nucleotide PolymorphismSlow-Onset Diabetes MellitusSodiumSpecialistStable Diabetes MellitusT2 DMT2DT2DMTechniquesTherapeuticTrainingTraining ProgramsType 2 Diabetes MellitusType 2 diabetesType II Diabetes MellitusType II diabetesUnited States National Institutes of HealthWeight LossWeight ReductionYouthYouth 10-21adiposityadult onset diabetesadulthoodagesbariatric surgerybody weight losscarbonate dehydratasecardiovascular disorderchild adipositychild obesitychildhood adipositychildhood obesityclinical careclinical decision-makingclinical significanceclinically significantcompulsive eatingcompulsive feedingcompulsive overeatingcorpulencedesigndesigningdose individualizationdrug treatmentdrug/agentelectronic health care recordelectronic health medical recordelectronic health plan recordelectronic health registryelectronic medical health recordextreme obesityfastedfastsfood cravinggamma-Aminobutyric Acidgastric bandinggastric bypass surgerygenetic etiologygenetic mechanism of diseasegenetic vulnerabilitygenetically predisposedglucagon-like peptide 1glucagon-like peptide-1 receptorglutamatergichigh BMIhigh body mass indeximplantable gastric stimulation bandingimprovedimproved outcomeincreased appetiteincreased hungerindividual heterogeneityindividual variabilityindividual variationinhibitorinterventional strategyketosis resistant diabeteslifestyle modificationmaturity onset diabetesmedication prescriptionmultidisciplinaryobese childrenobese patientsobesity during childhoodobesity in childrenobesity interventionobesity managementobesity riskobesity surgeryobesity therapyobesity treatmentpathwaypatient populationpatients with obesitypediatricpediatric obesitypharmacodynamic modelpharmacokinetics and pharmacodynamicspharmacometricsprecision medicineprecision-based medicinepredict responsivenesspredicting responseprescribed medicationrecruitresponserisk for obesityrisk minimizationrisk of obesityrisk selectionsexsingle nucleotide variantskillssocial rolestomach staplingsurgery risksurgical risksymportertopiramatetype 2 DMtype II DMtype two diabetesweight loss surgerywt-lossγ-Aminobutyric Acid
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Full Description

PROJECT SUMMARY
Pediatric severe obesity (defined as body mass index (BMI) ≥1.2 times the 95th percentile or BMI ≥35 kg/m2) is

the fastest growing obesity category, affecting ~6% of youth in the U.S. Youth with severe obesity are at

significant risk for developing obesity-related health consequences including type 2 diabetes and cardiovascular

disease. Obesity pharmacotherapy is a promising adjunct to lifestyle modification (LSM) therapy for severe

pediatric obesity treatment, as LSM alone generally fails to result in clinically significant and durable weight loss

and metabolic/bariatric surgery is invasive, carries surgical risks, and is not widely available. While obesity

pharmacotherapies are associated with overall mean weight loss, there is substantial variability in their individual-

level effectiveness. The National Institutes of Health (NIH) has recognized the importance of identifying

phenotypic characteristics associated with medication responsiveness, using pharmacogenomics approaches

to develop precision pharmacologic treatments, and optimizing medication dosing based upon a person’s

characteristics, in order to improve treatment of pediatric severe obesity. The objective of this proposal is to

utilize techniques that can be used in precision medicine to identify person-specific characteristics associated

with weight loss response to and affecting dosing of obesity pharmacotherapies. Specifically, we will use (1)

electronic health record (EHR)-enabled clinical discovery to identify phenotypic characteristics predicting weight

loss response, (2) genetic risk scores to determine the role genetic susceptibility plays in weight loss response,

and (3) pharmacokinetic/pharmacodynamic (PK/PD) modeling to begin identifying individualized dosing

regimens of obesity pharmacotherapies in youth with severe obesity. We will be applying these techniques to

topiramate, a medication commonly prescribed for weight loss in youth with severe obesity that has been

associated with highly variable individual-level effectiveness. This project will generate critical preliminary data

to inform the design of an R01 evaluating predictors of response to topiramate and other obesity

pharmacotherapies in youth with severe obesity, including agents that are currently (e.g., glucagon-like peptide-

1 (GLP1) receptor agonists) and will be (e.g., glucagon-GLP1 co-agonists, sodium glucose co-transporter 2/1

inhibitors) available in the future. Completing this K23 training program will allow me to establish skills in EHR-

enabled clinical discovery and applying genetic risk scores and PK/PD modeling to clinical research that I will

need in order to become a leader in the field of precision medicine for obesity management. Further, the

multidisciplinary mentorship that I will receive during this career development award will prepare me to become

an extramurally funded physician scientist capable of implementing both independent and collaborative large-

scale clinical studies.

Grant Number: 5K23DK125668-05
NIH Institute/Center: NIH

Principal Investigator: Eric Bomberg

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