Clinical Trial: Laboratory Studies on Oxytocin for Treatment of Alcohol Use Disorder

Study Status: Recruiting
Recruit Status: Recruiting
Study Type: Interventional

Official Title: Laboratory Studies on Oxytocin for Treatment of Alcohol Use Disorder

Brief Summary: This study will examine the utility of the neuropeptide oxytocin (OT) as a potential new medication for the treatment of Alcohol use disorder (AUD). Non-treatment seeking men and women with AUD will be enrolled in a double blind placebo controlled phase I clinical trial. Participants will complete an 7-day inpatient protocol. During the first 3 days of the inpatient protocol, participants will complete alcohol abstinence in which withdrawal symptoms are measured,and urine will be collected to determine withdrawal symptom severity and urine levels of the stress hormone cortisol. Participants will then complete 3 laboratory procedures which measure 1) stress response, 2) motivation to drink alcohol and 3) subjective and physiological effects of alcohol. Finally, because participants are individuals with AUD, we will administer a brief intervention to address their risky alcohol drinking and problems before discharge.

Detailed Summary: This study will lay the necessary groundwork for future comprehensive research to examine the utility of the neuropeptide oxytocin (OT) as a potential new medication for the treatment of Alcohol use disorder (AUD). OT modulates a number of key systems involved in addiction processes, including dopamine (DA) mesolimbic reward circuitry, and hypothalamic-pituitary-adrenal (HPA) axis and corticotrophin-releasing factor (CRF) stress systems, and has low abuse liability. Our overarching hypothesis is that OT will attenuate several measures thought to drive compulsive alcohol drinking and relapse. Specifically, we will examine whether OT decreases acute stress responses, alleviates alcohol withdrawal symptoms, reduces craving and motivation to drink, and decreases alcohol self-administration. Since interactions with alcohol are an important focus of our study, we will enroll non-treatment seeking heavy drinkers with AUD in a double blind, placebo controlled inpatient protocol. Subjects will be randomized to receive intranasal OT (40 IU/dose) or placebo 3 times daily. Participants will complete alcohol detoxification; we will measure alcohol withdrawal symptoms, craving, and 24-hr urinary free CORT. Participants will then complete 3 laboratory procedures in fixed order. The Trier Social Stress Test (TSST) which includes public speaking and performance of mental arithmetic will be used to examine subjective and physiological stress responses. An alcohol motivated responding (AMR) procedure will be used to examine subjects' responding to earn either drinks or money. A cumulative alcohol-dosing (CAD) procedure will be used to examine physiological and subjective responses across several blood alcohol levels. CORT levels will also be assessed. This study will provide new information on OT efficacy across a range of different measures predictive of alcohol use and misuse, and, if OT shows efficacy, help clarify the mechanism of OT action.
Sponsor: Johns Hopkins University

Current Primary Outcome:

• Alcohol withdrawal severity [ Time Frame: first 3 days of alcohol abstinence ]
  Scores on CIWA-Ar, POMS short and Craving Scales
• Stress response [ Time Frame: days 1-4 of alcohol withdrawal ]
  urinary free cortisol during first 3 days of withdrawal and salivary cortisol after stress test
• Alcohol drinking [ Time Frame: 1 day ]
  Number of drinks earned and self-administered in the laboratory session
• Alcohol response [ Time Frame: 1 day ]
  self-reported drug effect and cardiovascular (heart rate) effects after controlled alcohol dosing

Original Primary Outcome: Same as current

Current Secondary Outcome:

• side effects [ Time Frame: 1 week ]
  Side effects reported on the SAFTEE
• alcohol effects [ Time Frame: 1 day ]
  stimulation and sedation effects effects after controlled alcohol administration
• mood changes [ Time Frame: 1 week ]
  scores on tension/anxiety subscales

Original Secondary Outcome: Same as current

Information By: Johns Hopkins University

Dates:
Date Received: March 30, 2015
Date Started: March 2015
Date Completion: July 2017
Last Updated: February 27, 2017
Last Verified: February 2017