grant

Testing Neurobiological Models of Alcohol Use Disorder Through Real World Cue Reactivity and Mood

Organization UNIVERSITY OF CALIFORNIA LOS ANGELESLocation LOS ANGELES, UNITED STATESPosted 1 Sept 2024Deadline 31 Aug 2026
NIHUS FederalResearch GrantFY2025Active Follow-upAddressAlcohol Chemical ClassAlcohol DrinkingAlcohol consumptionAlcoholic beverage heavy drinkerAlcoholsClinicalClinical ResearchClinical StudyCuesDevelopmentEnvironmentEtOH drinkingEtOH useExposure toFemaleFosteringHeavy DrinkerHeavy DrinkingHumanIncentivesIndividualInvestigatorsKnowledgeLaboratoriesLiteratureMentorsMethodologyMethodsModelingModern ManMoodsMotivationNRSANational Research Service AwardsNegative ReinforcementsNeurobiologyNeurosciencesOutcomePre-Clinical ModelPreclinical ModelsProcessReportingResearchResearch PersonnelResearchersRewardsSamplingScientistStimulantTestingTimeTrainingTranslatingTranslational ResearchTranslational ScienceTranslationsVisitWithdrawalactive followupaddictionaddictive disorderalcohol cravingalcohol cuealcohol effectalcohol ingestionalcohol intakealcohol product usealcohol related cuealcohol usealcohol use disorderalcoholic beverage consumptionalcoholic drink intakebiological sexclinical applicabilityclinical applicationcravingcue reactivitydemographicsdevelop therapydevelopmentaldiariesdrink heavilydrinkingethanol consumptionethanol cravingethanol cueethanol drinkingethanol effectethanol ingestionethanol intakeethanol product useethanol useethanol use disorderexcessive alcohol consumptionexcessive alcohol ingestionexcessive alcohol intakeexcessive drinkingexcessive ethanol ingestionexperienceextreme drinkingfollow upfollow up assessmentfollow-upfollowed upfollowupfollowup assessmentheavy alcohol useincentive salienceinnovateinnovationinnovativeinterestintervention developmentmethods to study multiple-level influencesmulti-level analysismulti-level modelmultilevel analysismultilevel modelmultilevel modelingnegative affectnegative affectivitynegative moodneuralneurobiologicalnext generationpre-clinicalpre-docpre-doctoralprecision medicineprecision-based medicinepreclinicaltheoriestherapy developmenttranslationtranslation researchtranslational investigationtranslational investigatortranslational researchertranslational scientisttreatment development
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Full Description

PROJECT SUMMARY/ ABSTRACT
The neuroscientific understanding of alcohol use disorder (AUD) has advanced tremendously over the

past three decades. However, translation from preclinical models to clinical studies lags behind the evolving

neuroscience literature. Two of the most prominent neurobiological models of addiction are the allostatic model

and the incentive-sensitization model. The allostatic model focuses on the transition from positive to negative

reinforcement as addiction progresses. The incentive-sensitization model also emphasizes dynamic processes

in addiction and focuses primarily on the transition from ‘liking’ to ‘wanting’ a substance. Given that the clinical

application of these two prominent models is underway, understanding the forward translation (pre-clinical to

clinical) of these neurobiological models is more important than ever before. Moreover, identifying

demographic moderators of the interaction between these models is a crucial next step in understanding the

potential application of these findings in treatment development. Further, these two prominent neurobiological

models are being used to inform precision medicine approaches even though the predictive utility of these

models on alcohol consumption is limited. Therefore, innovative methodology is necessary to increase the

translational efficacy of neurobiological models to human clinical samples. This proposal is based on recent

indications that there is an interactive effect between the allostatic model and incentive-sensitization model.

Specifically, a preliminary study in the Sponsor’s laboratory focused on the allostatic model and incentive-

sensitization model. Their combined effect showed that there is an interactive effect of negative mood and cue

exposure on drinking among individuals with AUD. The objective of this NRSA application is to foster the

applicant’s development as a clinical scientist with a focus on neurobiological models of addiction, translational

science of addiction, and quantitative methods. This proposal aims to fill the gap in the literature by examining

the interaction between the allostatic model and incentive-sensitization model, identifying moderators of this

interaction, and testing the predictive utility of these models. Specifically, Aim #1 tests the effects of negative

mood and cue exposure on same-day alcohol craving and alcohol use. Aim #2 tests the predictive effects of

the allostatic model and incentive-sensitization model on longitudinal alcohol use. Exploratory Aim tests

demographic moderators of the relationship between negative mood and cue reactivity. To address these Aims

64 individuals (32 females) with current AUD (mild to severe) will complete daily diary assessments of mood,

craving, cue-exposure, and drinking for 14 days and will complete remote follow-up visits at 4, 8, and 12-weeks

post daily diary. A sophisticated analytic approach including longitudinal multilevel modeling and multilevel

moderation will be used to test these aims. The present study represents an important step in furthering the

translation of neurobiological constructs of AUD and, with the support of the mentoring team, the applicant’s

scientific development as an independent researcher with an interest in translational science of addiction.

Grant Number: 5F31AA031914-02
NIH Institute/Center: NIH

Principal Investigator: Wave-Ananda Baskerville

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