Longitudinal analysis of HIV-risk behaviors of participants in a randomized trial of prison-initiated buprenorphine

Thomas R. Blue; Michael S. Gordon; Robert P. Schwartz; Kathryn Couvillion; Frank J. Vocci; Terrence T. Fitzgerald; Kevin E. O’Grady

doi:10.1186/s13722-019-0172-2

Addiction Science & Clinical Practice (Dec 2019)

Longitudinal analysis of HIV-risk behaviors of participants in a randomized trial of prison-initiated buprenorphine

Thomas R. Blue,
Michael S. Gordon,
Robert P. Schwartz,
Kathryn Couvillion,
Frank J. Vocci,
Terrence T. Fitzgerald,
Kevin E. O’Grady

Affiliations

Thomas R. Blue: Friends Research Institute Inc.
Michael S. Gordon: Friends Research Institute Inc.
Robert P. Schwartz: Friends Research Institute Inc.
Kathryn Couvillion: Friends Research Institute Inc.
Frank J. Vocci: Friends Research Institute Inc.
Terrence T. Fitzgerald: Glenwood Life Counseling Center
Kevin E. O’Grady: Department of Psychology, University of Maryland, College Park

DOI: https://doi.org/10.1186/s13722-019-0172-2
Journal volume & issue: Vol. 14, no. 1
pp. 1 – 11

Abstract

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Abstract Background It has been estimated that approximately 15% of people who are incarcerated in the US have histories of opioid use disorder. Relapse to opioid use after release from prison poses a serious risk of HIV infection. Prison-initiated buprenorphine may help to reduce HIV infection given the association between opioid use and HIV-risk behaviors. Methods The present study is a secondary analysis of longitudinal data gathered from a randomized controlled trial of buprenorphine-naloxone for people who were incarcerated (N = 211) between 2008 and 2012. It compares the impact of assignment to initiate buprenorphine in prison (N = 106 randomized, N = 104 analyzed) versus in the community (N = 107 randomized, N = 107 analyzed) and whether or not participants entered community treatment on the frequency of HIV-risk behaviors in the 12 months following release from prison. Data were analyzed hierarchically and for each outcome variable, a multilevel, over-dispersed Poisson model was fit to the data. Outcome variables were the number of times the following behaviors occurred in the last 30 days: (1) having sex without a condom (2) injecting drugs (3) using unsterilized needles, and (4) sharing injection paraphernalia. Results Participants assigned to begin buprenorphine in the community experienced a greater decrease in injection drug use over time compared to participants assigned to begin buprenorphine in prison. There were no significant associations between treatment assignment or community treatment entry and instances of having sex without a condom, sharing injection paraphernalia, or using unsterilized needles. Conclusions Overall, the present study did not find support for the initiation of buprenorphine in prison (as opposed to the community) as a means to reduce incidences of HIV-risk behaviors. Avenues for future research in the nexus of HIV-risk reduction, criminal justice, and pharmacotherapy are discussed. Trial registration This study was supported by the National Institute on Drug Abuse (NIDA), Buprenorphine for Prisoners (PI: Kinlock; R01DA021579). ClinicalTrials.gov identifier: NCT 00574067

Published in Addiction Science & Clinical Practice

ISSN: 1940-0632 (Print); 1940-0640 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General); Social Sciences: Social pathology. Social and public welfare. Criminology
Website: http://ascpjournal.biomedcentral.com

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