Abstract

Alcohol is one of the most widely used and misused drugs in the US. There is a critical need to continue to improve AUD treatment and develop new medications to reduce alcohol use and to include nicotine co-use in evaluations of candidate medications. This project proposes to investigate biobehavioral mechanisms underlying alcohol and nicotine use and co-use, and to test candidate medications in two animal models developed specifically for testing medications for alcohol abuse, and alcohol and nicotine co-use. The first model uses a Chained Schedule of Reinforcement (CSR) procedure in which seeking and consumption occur in the context of distinct environmental cues and behavioral contingencies to the influence of environmental stimuli on the drive to drink and the persistence of behaviors associated with chronic drinking. Two 2 matched groups of NHP with extensive histories of self-administration of alcohol (Alcohol group) or the non-alcoholic beverage (Control group) will be utilized. The second model is a new Alcohol and Nicotine Concurrent Access (ANCA) procedure in which oral alcohol and IV nicotine were concurrently available for self-administration. A functional assessment battery provides assessment of drug side effects.
Aim 1 will determine whether test drugs reduce alcohol seeking and self-administration in the CSR under conditions of ongoing drinking and abstinence.
Aim 2 will determine whether test drugs reduce alcohol and nicotine self-administration independently or concurrently under single drug access or ANCA procedures.
Aim 3 will determine incidence of side effects of test drugs in the functional assessment battery. Drug candidates include bifunctional and universal opioid receptor (OR) ligands with different pharmacological profiles at OR subtypes, a universal OR/nociception opioid peptide (NOP) receptor ligand, the cannabinoid constituent cannabidiol (CBD), the neuropeptide oxytocin, and a nicotinic acetylcholine receptor partial agonist/antagonist varenicline. Naltrexone will be tested as a positive control and comparator. A drug with therapeutic potential would be one that reduces cue-maintained seeking, and decreases alcohol self-administration, and has a low side-effect profile. A drug with therapeutic potential in alcohol and nicotine co-users would decrease alcohol self-administration without increasing nicotine self-administration, and ideally would reduce self-administration of both drugs. Integration these data will provide new information on the behavioral and neuropharmacological mechanisms involved in alcohol abuse and alcohol/nicotine co-use. Comparison of dose effect functions and efficacy across models can inform treatment strategies for optimal dosing and timing of treatment. This information will ultimately facilitate medication development for the treatment of alcohol misuse and AUD.

Public Health Relevance

Characteristic drinking patterns of ?drinking too much, too fast? (binge drinking) and ?drinking too often? and co- use of tobacco/nicotine products are well recognized risks for AUD and health problems. The goal of the current project is to test candidate medications in preclinical models of alcohol abuse and alcohol and nicotine co-use. Examining rationally selected compounds and specific pharmacological targets to reduce alcohol and nicotine self-administration will ultimately advance medications development for AUD.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA015971-12
Application #
9906835
Study Section
Neurotoxicology and Alcohol Study Section (NAL)
Program Officer
Egli, Mark
Project Start
2007-09-28
Project End
2024-03-31
Budget Start
2020-04-01
Budget End
2021-03-31
Support Year
12
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Psychiatry
Type
Schools of Medicine
DUNS #
001910777
City
Baltimore
State
MD
Country
United States
Zip Code
21205

  Publications

Holtyn, August F; Kaminski, Barbara J; Weerts, Elise M (2017) Baclofen and naltrexone effects on alcohol self-administration: Comparison of treatment initiated during abstinence or ongoing alcohol access in baboons. Drug Alcohol Depend 179:47-54
Holtyn, August F; Tiruveedhula, V V N Phani Babu; Stephen, Michael Rajesh et al. (2017) Effects of the benzodiazepine GABAA ?1-preferring antagonist 3-isopropoxy-?-carboline hydrochloride (3-ISOPBC) on alcohol seeking and self-administration in baboons. Drug Alcohol Depend 170:25-31
Lee, Mary R; Weerts, Elise M (2016) Oxytocin for the treatment of drug and alcohol use disorders. Behav Pharmacol 27:640-648
Kaminski, Barbara J; Weerts, Elise M (2014) The effects of varenicline on alcohol seeking and self-administration in baboons. Alcohol Clin Exp Res 38:376-83
Holtyn, August F; Kaminski, Barbara J; Wand, Gary S et al. (2014) Differences in extinction of cue-maintained conditioned responses associated with self-administration: alcohol versus a nonalcoholic reinforcer. Alcohol Clin Exp Res 38:2639-46
Duke, Angela N; Kaminski, Barbara J; Weerts, Elise M (2014) Baclofen effects on alcohol seeking, self-administration and extinction of seeking responses in a within-session design in baboons. Addict Biol 19:16-26
Kaminski, Barbara J; Van Linn, Michael L; Cook, James M et al. (2013) Effects of the benzodiazepine GABAA ?1-preferring ligand, 3-propoxy-?-carboline hydrochloride (3-PBC), on alcohol seeking and self-administration in baboons. Psychopharmacology (Berl) 227:127-36
Kaminski, Barbara J; Duke, Angela N; Weerts, Elise M (2012) Effects of naltrexone on alcohol drinking patterns and extinction of alcohol seeking in baboons. Psychopharmacology (Berl) 223:55-66
Kaminski, Barbara J; Goodwin, Amy K; Wand, Gary et al. (2008) Dissociation of alcohol-seeking and consumption under a chained schedule of oral alcohol reinforcement in baboons. Alcohol Clin Exp Res 32:1014-22