Abstract

Opioid dependence is an enduring public health problem and the extent of that problem has escalated because of its association with IV drug use and AIDS. Although widely accepted as a problem of urban areas, opioid dependence in rural areas has been less frequently recognized. This is unfortunate because opioid dependence occurs in, and is a public health problem for, rural areas. Moreover, this lack of recognition has often led to limited treatment alternatives for the rural opioid addict. In this application, we propose to continue the first and only outpatient detoxification clinic to provide pharmacotherapies for opioid dependence in the State of Vermont. Approximately 84 patients per year will participate in clinical pharmacology studies and/or a detoxification study examining buprenorphine, a promising new pharmacotherapy for opioid dependence. These studies will address aspects of buprenorphine's unique clinical pharmacology that will directly impact the manner in which buprenorphine is provided to patients. Specifically, we propose to answer six questions across three series of studies. In the first series, we will continue our research on alternative dosing schedules which has demonstrated that subjects can safely receive buprenorphine every other day or every three days by doubling or tripling the buprenorphine dose, respectively. These dosing schedules will eliminate the need for take- home medication for patients requiring days off from the clinic. In continuing this research, we will answer three questions. First, can buprenorphine be administered safely and effectively every four days? Second, what is the duration of buprenorphine's blockade of the effects of morphine-like opioids during 2-day, 3-day and 4-day dosing schedules? And third, do every 3-day and every 4-day dosing schedules function as reinforcers for opioid-dependent outpatients? In the second series, we will characterize the interaction between buprenorphine and opioid antagonists, to determine whether buprenorphine can facilitate the transition to, and be combined with, opioid antagonists. Specifically we will answer two questions. First, what are the range of conditions under which buprenorphine can be co-administered with naloxone or naltrexone without compromising agonist activity or precipitating withdrawal? And second, can buprenorphine and naltrexone be chronically co- administered without adverse effects? In the third series, we will conduct a detoxification study using daily and 3-day dosing schedules to address the extent to which the buprenorphine dosing schedule influences opioid abstinence and treatment retention during detoxification with buprenorphine. We plan to conduct a minimum of 9 clinical pharmacology studies and 1 detoxification study (for a total of 10 studies) in the five-year period. Overall, this research will provide critical knowledge about buprenorphine's clinical pharmacology that will permit buprenorphine to be used with the greatest efficacy and efficiency in clinical settings. Moreover, this project will positively contribute to the public health status of this region by providing the only outpatient pharmacotherapy services for opioid dependence in the State of Vermont.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA006969-10
Application #
2897828
Study Section
Special Emphasis Panel (SRCD)
Program Officer
Montoya, Ivan
Project Start
1990-09-30
Project End
2001-07-31
Budget Start
1999-08-01
Budget End
2001-07-31
Support Year
10
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Vermont & St Agric College
Department
Psychiatry
Type
Schools of Medicine
DUNS #
066811191
City
Burlington
State
VT
Country
United States
Zip Code
05405

  Publications

Gross, Anke; Marsch, Lisa A; Badger, Gary J et al. (2006) A comparison between low-magnitude voucher and buprenorphine medication contingencies in promoting abstinence from opioids and cocaine. Exp Clin Psychopharmacol 14:148-56
Marsch, Lisa A; Bickel, Warren K; Badger, Gary J et al. (2005) Buprenorphine treatment for opioid dependence: the relative efficacy of daily, twice and thrice weekly dosing. Drug Alcohol Depend 77:195-204
Petry, N M; Bickel, W K; Badger, G J (2001) Examining the limits of the buprenorphine interdosing interval: daily, every-third-day and every-fifth-day dosing regimens. Addiction 96:823-34
Gross, A; Jacobs, E A; Petry, N M et al. (2001) Limits to buprenorphine dosing: a comparison between quintuple and sextuple the maintenance dose every 5 days. Drug Alcohol Depend 64:111-6
Petry, N M; Bickel, W K; Piasecki, D et al. (2000) Elevated liver enzyme levels in opioid-dependent patients with hepatitis treated with buprenorphine. Am J Addict 9:265-9
Odum, A L; Madden, G J; Badger, G J et al. (2000) Needle sharing in opioid-dependent outpatients: psychological processes underlying risk. Drug Alcohol Depend 60:259-66
Petry, N M; Bickel, W K; Badger, G J (2000) A comparison of four buprenorphine dosing regimens using open-dosing procedures: is twice-weekly dosing possible? Addiction 95:1069-77
Petry, N M; Bickel, W K (2000) Gender differences in hostility of opioid-dependent outpatients: role in early treatment termination. Drug Alcohol Depend 58:27-33
Petry, N M; Bickel, W K; Badger, G J (1999) A comparison of four buprenorphine dosing regimens in the treatment of opioid dependence. Clin Pharmacol Ther 66:306-14
Jacobs, E A; Bickel, W K (1999) Modeling drug consumption in the clinic using simulation procedures: demand for heroin and cigarettes in opioid-dependent outpatients. Exp Clin Psychopharmacol 7:412-26

Showing the most recent 10 out of 19 publications