A novel human laboratory model for screening medications for alcohol use disorder

Diana Ho; Brandon Towns; Erica N Grodin; Lara A Ray

doi:10.1186/s13063-020-04842-w

A novel human laboratory model for screening medications for alcohol use disorder

Trials. 2020 Nov 23;21(1):947. doi: 10.1186/s13063-020-04842-w.

Authors

Diana Ho¹, Brandon Towns¹, Erica N Grodin¹, Lara A Ray^{2

3}

Affiliations

¹ Department of Psychology, University of California, Los Angeles, 1285 Franz Hall, Box 951563, Los Angeles, CA, 90095-1563, USA.
² Department of Psychology, University of California, Los Angeles, 1285 Franz Hall, Box 951563, Los Angeles, CA, 90095-1563, USA. lararay@psych.ucla.edu.
³ Department of Psychiatry and Biobehavioral Sciences, University of California, Los Angeles, Los Angeles, CA, USA. lararay@psych.ucla.edu.

Abstract

Background: Alcohol use disorder (AUD) is a highly prevalent, chronic relapsing disorder with a high disease burden in the USA. Pharmacotherapy is a promising treatment method for AUD; however, the few FDA-approved medications are only modestly effective. Medications development for AUD is a high priority research area, but the cumbersome drug development process hinders many potential compounds from reaching approval. One area with major opportunities for improvement is the process of screening novel compounds for initial efficacy, also known as early phase 2 trials. Early phase 2 trials incorporate human laboratory paradigms to assess relevant clinical constructs, such as craving and subjective responses to alcohol. However, these controlled paradigms often lack the ecological validity of clinical trials. Therefore, early phase 2 trials can be more efficient and clinically meaningful if they combine the internal validity of experimental laboratory testing with the external validity of clinical trials. To that end, the current study aims to develop and validate a novel early efficacy paradigm, informed by smoking cessation literature, to screen novel medications for AUD. As an established AUD medication, naltrexone will serve as an active control to test both the practice quit attempt model and the efficacy of a promising AUD pharmacotherapy, varenicline.

Methods: Individuals with current AUD reporting intrinsic motivation to change their drinking will complete a week-long "practice quit attempt" while on study medication. Participants are randomized and blinded to either naltrexone, varenicline, or placebo. During the practice quit attempt, participants will complete daily visits over the phone and fill out online questionnaires regarding their drinking, alcohol craving, and mood. Additionally, participants will undergo two alcohol cue-reactivity sessions.

Discussion: The successful completion of this study will advance medications development by proposing and validating a novel early efficacy model for screening AUD pharmacotherapies, which in turn can serve as an efficient strategy for making go/no-go decisions as to whether to proceed with clinical trials.

Trial registration: ClinicalTrials.gov NCT04249882 . Registered on 31 January 2020.

Keywords: Alcohol use disorder; Clinical trial; Medications development; Medications screening; Naltrexone; Varenicline.

Publication types

Randomized Controlled Trial

MeSH terms

Alcohol Drinking
Alcoholism* / diagnosis
Alcoholism* / drug therapy
Humans
Laboratories
Naltrexone / adverse effects
Varenicline / adverse effects

Substances

Naltrexone
Varenicline

Associated data

ClinicalTrials.gov/NCT04249882

Grants and funding

R21AA027180/AA/NIAAA NIH HHS/United States