Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone: HIV prevention trials network 058

David S. Metzger; Deborah Donnell; David D. Celentano; J. Brooks Jackson; Yiming Shao; Apinun Aramrattana; Liu Wei; Liping Fu; Jun Ma; Gregory M. Lucas; Marek Chawarski; Yuhua Ruan; Paul Richardson; Katherine Shin; Ray Y. Chen; Jeremy Sugarman; Bonnie J. Dye; Scott M. Rose; Geetha Beauchamp; David N. Burns

doi:10.1097/QAI.0000000000000510

Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone: HIV prevention trials network 058

David S. Metzger, Deborah Donnell, David D. Celentano, J. Brooks Jackson, Yiming Shao, Apinun Aramrattana, Liu Wei, Liping Fu, Jun Ma, Gregory M. Lucas, Marek Chawarski, Yuhua Ruan, Paul Richardson, Katherine Shin, Ray Y. Chen, Jeremy Sugarman, Bonnie J. Dye, Scott M. Rose, Geetha Beauchamp, David N. Burns

Research output: Contribution to journal › Article › peer-review

22 Scopus citations

Abstract

Background: Injection opioid use plays a significant role in the transmission of HIV infection in many communities and several regions of the world. Access to evidence-based treatments for opioid use disorders is extremely limited. Methods: HIV Prevention Trials Network 058 (HPTN 058) was a randomized controlled trial designed to compare the impact of 2 medication-assisted treatment (MAT) strategies on HIV incidence or death among opioid-dependent people who inject drugs (PWID). HIV-negative opioid-dependent PWID were recruited from 4 communities in Thailand and China with historically high prevalence of HIV among PWID. A total of 1251 participants were randomly assigned to either (1) a 1-year intervention consisting of 2 opportunities for a 15-day detoxification with buprenorphine/naloxone (BUP/NX) combined with up to 21 sessions of behavioral drug and risk counseling [short-term medication-assisted treatment (ST-MAT)] or (2) thrice-weekly dosing for 48 weeks with BUP/NX and up to 21 counseling sessions [long-term medication-assisted treatment (LT-MAT)] followed by dose tapering. All participants were followed for 52 weeks after treatment completion to assess durability of impact. Results: Although the study was stopped early due to lower than expected occurrence of the primary end points, sufficient data were available to assess the impact of the interventions on drug use and injection-related risk behavior. At week 26, 22% of ST-MAT participants had negative urinalyses for opioids compared with 57% in the LT-MAT (P < 0.001). Differences disappeared in the year after treatment: at week 78, 35% in ST-MAT and 32% in the LT-MAT had negative urinalyses. Injection-related risk behaviors were significantly reduced in both groups after randomization. Conclusions: Participants receiving BUP/NX 3 times weekly were more likely to reduce opioid injection while on active treatment. Both treatment strategies were considered safe and associated with reductions in injection-related risk behavior. These data support the use of thrice-weekly BUP/NX as a way to reduce exposure to HIV risk. Continued access to BUP/NX may be required to sustain reductions in opioid use.

Original language	English (US)
Pages (from-to)	554-561
Number of pages	8
Journal	Journal of Acquired Immune Deficiency Syndromes
Volume	68
Issue number	5
DOIs	https://doi.org/10.1097/QAI.0000000000000510
State	Published - Apr 15 2015

Keywords

HIV prevention
PWID
buprenorphine/naloxone
medication-assisted treatment
opiates
substance use treatment

ASJC Scopus subject areas

Infectious Diseases
Pharmacology (medical)

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10.1097/QAI.0000000000000510

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Metzger, D. S., Donnell, D., Celentano, D. D., Jackson, J. B., Shao, Y., Aramrattana, A., Wei, L., Fu, L., Ma, J., Lucas, G. M., Chawarski, M., Ruan, Y., Richardson, P., Shin, K., Chen, R. Y., Sugarman, J., Dye, B. J., Rose, S. M., Beauchamp, G., & Burns, D. N. (2015). Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone: HIV prevention trials network 058. Journal of Acquired Immune Deficiency Syndromes, 68(5), 554-561. https://doi.org/10.1097/QAI.0000000000000510

Metzger, DS, Donnell, D, Celentano, DD, Jackson, JB, Shao, Y, Aramrattana, A, Wei, L, Fu, L, Ma, J, Lucas, GM, Chawarski, M, Ruan, Y, Richardson, P, Shin, K, Chen, RY, Sugarman, J, Dye, BJ, Rose, SM, Beauchamp, G & Burns, DN 2015, 'Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone: HIV prevention trials network 058', Journal of Acquired Immune Deficiency Syndromes, vol. 68, no. 5, pp. 554-561. https://doi.org/10.1097/QAI.0000000000000510

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title = "Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone: HIV prevention trials network 058",

abstract = "Background: Injection opioid use plays a significant role in the transmission of HIV infection in many communities and several regions of the world. Access to evidence-based treatments for opioid use disorders is extremely limited. Methods: HIV Prevention Trials Network 058 (HPTN 058) was a randomized controlled trial designed to compare the impact of 2 medication-assisted treatment (MAT) strategies on HIV incidence or death among opioid-dependent people who inject drugs (PWID). HIV-negative opioid-dependent PWID were recruited from 4 communities in Thailand and China with historically high prevalence of HIV among PWID. A total of 1251 participants were randomly assigned to either (1) a 1-year intervention consisting of 2 opportunities for a 15-day detoxification with buprenorphine/naloxone (BUP/NX) combined with up to 21 sessions of behavioral drug and risk counseling [short-term medication-assisted treatment (ST-MAT)] or (2) thrice-weekly dosing for 48 weeks with BUP/NX and up to 21 counseling sessions [long-term medication-assisted treatment (LT-MAT)] followed by dose tapering. All participants were followed for 52 weeks after treatment completion to assess durability of impact. Results: Although the study was stopped early due to lower than expected occurrence of the primary end points, sufficient data were available to assess the impact of the interventions on drug use and injection-related risk behavior. At week 26, 22% of ST-MAT participants had negative urinalyses for opioids compared with 57% in the LT-MAT (P < 0.001). Differences disappeared in the year after treatment: at week 78, 35% in ST-MAT and 32% in the LT-MAT had negative urinalyses. Injection-related risk behaviors were significantly reduced in both groups after randomization. Conclusions: Participants receiving BUP/NX 3 times weekly were more likely to reduce opioid injection while on active treatment. Both treatment strategies were considered safe and associated with reductions in injection-related risk behavior. These data support the use of thrice-weekly BUP/NX as a way to reduce exposure to HIV risk. Continued access to BUP/NX may be required to sustain reductions in opioid use.",

keywords = "HIV prevention, PWID, buprenorphine/naloxone, medication-assisted treatment, opiates, substance use treatment",

author = "Metzger, {David S.} and Deborah Donnell and Celentano, {David D.} and Jackson, {J. Brooks} and Yiming Shao and Apinun Aramrattana and Liu Wei and Liping Fu and Jun Ma and Lucas, {Gregory M.} and Marek Chawarski and Yuhua Ruan and Paul Richardson and Katherine Shin and Chen, {Ray Y.} and Jeremy Sugarman and Dye, {Bonnie J.} and Rose, {Scott M.} and Geetha Beauchamp and Burns, {David N.}",

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doi = "10.1097/QAI.0000000000000510",

language = "English (US)",

volume = "68",

pages = "554--561",

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T1 - Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone

T2 - HIV prevention trials network 058

AU - Metzger, David S.

AU - Donnell, Deborah

AU - Celentano, David D.

AU - Jackson, J. Brooks

AU - Shao, Yiming

AU - Aramrattana, Apinun

AU - Wei, Liu

AU - Fu, Liping

AU - Ma, Jun

AU - Lucas, Gregory M.

AU - Chawarski, Marek

AU - Ruan, Yuhua

AU - Richardson, Paul

AU - Shin, Katherine

AU - Chen, Ray Y.

AU - Sugarman, Jeremy

AU - Dye, Bonnie J.

AU - Rose, Scott M.

AU - Beauchamp, Geetha

AU - Burns, David N.

PY - 2015/4/15

Y1 - 2015/4/15

N2 - Background: Injection opioid use plays a significant role in the transmission of HIV infection in many communities and several regions of the world. Access to evidence-based treatments for opioid use disorders is extremely limited. Methods: HIV Prevention Trials Network 058 (HPTN 058) was a randomized controlled trial designed to compare the impact of 2 medication-assisted treatment (MAT) strategies on HIV incidence or death among opioid-dependent people who inject drugs (PWID). HIV-negative opioid-dependent PWID were recruited from 4 communities in Thailand and China with historically high prevalence of HIV among PWID. A total of 1251 participants were randomly assigned to either (1) a 1-year intervention consisting of 2 opportunities for a 15-day detoxification with buprenorphine/naloxone (BUP/NX) combined with up to 21 sessions of behavioral drug and risk counseling [short-term medication-assisted treatment (ST-MAT)] or (2) thrice-weekly dosing for 48 weeks with BUP/NX and up to 21 counseling sessions [long-term medication-assisted treatment (LT-MAT)] followed by dose tapering. All participants were followed for 52 weeks after treatment completion to assess durability of impact. Results: Although the study was stopped early due to lower than expected occurrence of the primary end points, sufficient data were available to assess the impact of the interventions on drug use and injection-related risk behavior. At week 26, 22% of ST-MAT participants had negative urinalyses for opioids compared with 57% in the LT-MAT (P < 0.001). Differences disappeared in the year after treatment: at week 78, 35% in ST-MAT and 32% in the LT-MAT had negative urinalyses. Injection-related risk behaviors were significantly reduced in both groups after randomization. Conclusions: Participants receiving BUP/NX 3 times weekly were more likely to reduce opioid injection while on active treatment. Both treatment strategies were considered safe and associated with reductions in injection-related risk behavior. These data support the use of thrice-weekly BUP/NX as a way to reduce exposure to HIV risk. Continued access to BUP/NX may be required to sustain reductions in opioid use.

AB - Background: Injection opioid use plays a significant role in the transmission of HIV infection in many communities and several regions of the world. Access to evidence-based treatments for opioid use disorders is extremely limited. Methods: HIV Prevention Trials Network 058 (HPTN 058) was a randomized controlled trial designed to compare the impact of 2 medication-assisted treatment (MAT) strategies on HIV incidence or death among opioid-dependent people who inject drugs (PWID). HIV-negative opioid-dependent PWID were recruited from 4 communities in Thailand and China with historically high prevalence of HIV among PWID. A total of 1251 participants were randomly assigned to either (1) a 1-year intervention consisting of 2 opportunities for a 15-day detoxification with buprenorphine/naloxone (BUP/NX) combined with up to 21 sessions of behavioral drug and risk counseling [short-term medication-assisted treatment (ST-MAT)] or (2) thrice-weekly dosing for 48 weeks with BUP/NX and up to 21 counseling sessions [long-term medication-assisted treatment (LT-MAT)] followed by dose tapering. All participants were followed for 52 weeks after treatment completion to assess durability of impact. Results: Although the study was stopped early due to lower than expected occurrence of the primary end points, sufficient data were available to assess the impact of the interventions on drug use and injection-related risk behavior. At week 26, 22% of ST-MAT participants had negative urinalyses for opioids compared with 57% in the LT-MAT (P < 0.001). Differences disappeared in the year after treatment: at week 78, 35% in ST-MAT and 32% in the LT-MAT had negative urinalyses. Injection-related risk behaviors were significantly reduced in both groups after randomization. Conclusions: Participants receiving BUP/NX 3 times weekly were more likely to reduce opioid injection while on active treatment. Both treatment strategies were considered safe and associated with reductions in injection-related risk behavior. These data support the use of thrice-weekly BUP/NX as a way to reduce exposure to HIV risk. Continued access to BUP/NX may be required to sustain reductions in opioid use.

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KW - substance use treatment

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Expanding substance use treatment options for HIV prevention with buprenorphine-naloxone: HIV prevention trials network 058

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