Reward drinking and naltrexone treatment response among young adult heavy drinkers

Corey R. Roos; Krysten W. Bold; Katie Witkiewitz; Robert F. Leeman; Kelly S. DeMartini; Lisa M. Fucito; William R. Corbin; Karl Mann; Henry R. Kranzler; Stephanie S. O'Malley

doi:10.1111/add.15453

Reward drinking and naltrexone treatment response among young adult heavy drinkers

Corey R. Roos, Krysten W. Bold, Katie Witkiewitz, Robert F. Leeman, Kelly S. DeMartini, Lisa M. Fucito, William R. Corbin, Karl Mann, Henry R. Kranzler, Stephanie S. O'Malley

Psychology

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

13 Scopus citations

Abstract

Aims: Theory-driven, exploratory study to: (i) identify a reward drinking phenotype in young adults; (ii) evaluate this phenotype as a predictor of naltrexone response; and (iii) examine mechanisms of naltrexone in reward drinkers. Design: Secondary analysis of a randomized controlled trial. Setting: USA. Participants: A total of 128 young adult (ages 18–25) heavy drinkers. Interventions: Naltrexone versus placebo. Measurements: Daily surveys assessed affect, urge, drinking, and context. The Drinking Motives Questionnaire was used to identify phenotypes based on reward (enhancement motives) and relief (coping motives) drinking. Findings: We identified three profiles: “Low reward/Low relief” (14.1%; low enhancement/low coping motives); “Reward drinkers” (62.2%; high enhancement/low coping motives); and “High reward/High relief” (22.7%; high enhancement/high coping motives). Among reward drinkers (versus low profile), naltrexone significantly reduced percent days drinking to intoxication (blood alcohol concentration [BAC] ≥0.08) (PDI) (d = 0.56; 95% CI [0.17, 0.96]) and percent high intensity drinking days (PHID) (8/10 drinks for women/men) (d = 0.32; 95% CI [0.01, 0.68]). Among the high reward/high relief profile drinkers (versus low profile), naltrexone reduced PHID (d = 0.69; 95% CI [0.02, 1.50]). Using profile-informed cutoffs and observed scores (for clinical applicability): (i) among cutoff-derived reward drinkers, we found a medium-to-large (d = 0.66; 95% CI [0.24, 1.16]) and small effect (d = 0.28; 95% CI [0.04, 0.72]) of naltrexone in reducing PDI and PHID, respectively; and (ii) among the cutoff-derived high reward/high relief subgroup, we found a medium-to-large effect (d = 0.63; 95% CI [0.05, 1.1]) of naltrexone in reducing PHID. Among reward drinkers (not other profiles), naltrexone reduced drinking on days a drinking event occurred by weakening the within-day association between positive affect and urges (P < 0.05). Conclusions: Naltrexone has pronounced effects in reducing risky drinking among young adult reward drinkers (high reward/low relief) by reducing urges on days when individuals have higher positive affect and are exposed to a drinking event. Naltrexone also appears to reduce risky drinking among young adult high reward/high relief drinkers, but not via the same mechanism.

Original language	English (US)
Pages (from-to)	2360-2371
Number of pages	12
Journal	Addiction
Volume	116
Issue number	9
DOIs	https://doi.org/10.1111/add.15453
State	Published - Sep 2021

Keywords

Heavy drinking
mechanisms
naltrexone
precision medicine
reward drinker
young adults

ASJC Scopus subject areas

Medicine (miscellaneous)
Psychiatry and Mental health

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10.1111/add.15453

Cite this

@article{039e2eef65974e79b700104129aa52cd,

title = "Reward drinking and naltrexone treatment response among young adult heavy drinkers",

abstract = "Aims: Theory-driven, exploratory study to: (i) identify a reward drinking phenotype in young adults; (ii) evaluate this phenotype as a predictor of naltrexone response; and (iii) examine mechanisms of naltrexone in reward drinkers. Design: Secondary analysis of a randomized controlled trial. Setting: USA. Participants: A total of 128 young adult (ages 18–25) heavy drinkers. Interventions: Naltrexone versus placebo. Measurements: Daily surveys assessed affect, urge, drinking, and context. The Drinking Motives Questionnaire was used to identify phenotypes based on reward (enhancement motives) and relief (coping motives) drinking. Findings: We identified three profiles: “Low reward/Low relief” (14.1%; low enhancement/low coping motives); “Reward drinkers” (62.2%; high enhancement/low coping motives); and “High reward/High relief” (22.7%; high enhancement/high coping motives). Among reward drinkers (versus low profile), naltrexone significantly reduced percent days drinking to intoxication (blood alcohol concentration [BAC] ≥0.08) (PDI) (d = 0.56; 95% CI [0.17, 0.96]) and percent high intensity drinking days (PHID) (8/10 drinks for women/men) (d = 0.32; 95% CI [0.01, 0.68]). Among the high reward/high relief profile drinkers (versus low profile), naltrexone reduced PHID (d = 0.69; 95% CI [0.02, 1.50]). Using profile-informed cutoffs and observed scores (for clinical applicability): (i) among cutoff-derived reward drinkers, we found a medium-to-large (d = 0.66; 95% CI [0.24, 1.16]) and small effect (d = 0.28; 95% CI [0.04, 0.72]) of naltrexone in reducing PDI and PHID, respectively; and (ii) among the cutoff-derived high reward/high relief subgroup, we found a medium-to-large effect (d = 0.63; 95% CI [0.05, 1.1]) of naltrexone in reducing PHID. Among reward drinkers (not other profiles), naltrexone reduced drinking on days a drinking event occurred by weakening the within-day association between positive affect and urges (P < 0.05). Conclusions: Naltrexone has pronounced effects in reducing risky drinking among young adult reward drinkers (high reward/low relief) by reducing urges on days when individuals have higher positive affect and are exposed to a drinking event. Naltrexone also appears to reduce risky drinking among young adult high reward/high relief drinkers, but not via the same mechanism.",

keywords = "Heavy drinking, mechanisms, naltrexone, precision medicine, reward drinker, young adults",

author = "Roos, {Corey R.} and Bold, {Krysten W.} and Katie Witkiewitz and Leeman, {Robert F.} and DeMartini, {Kelly S.} and Fucito, {Lisa M.} and Corbin, {William R.} and Karl Mann and Kranzler, {Henry R.} and O'Malley, {Stephanie S.}",

note = "Publisher Copyright: {\textcopyright} 2021 Society for the Study of Addiction",

year = "2021",

month = sep,

doi = "10.1111/add.15453",

language = "English (US)",

volume = "116",

pages = "2360--2371",

journal = "Addiction",

issn = "0965-2140",

publisher = "Wiley-Blackwell",

number = "9",

}

TY - JOUR

T1 - Reward drinking and naltrexone treatment response among young adult heavy drinkers

AU - Roos, Corey R.

AU - Bold, Krysten W.

AU - Witkiewitz, Katie

AU - Leeman, Robert F.

AU - DeMartini, Kelly S.

AU - Fucito, Lisa M.

AU - Corbin, William R.

AU - Mann, Karl

AU - Kranzler, Henry R.

AU - O'Malley, Stephanie S.

PY - 2021/9

Y1 - 2021/9

N2 - Aims: Theory-driven, exploratory study to: (i) identify a reward drinking phenotype in young adults; (ii) evaluate this phenotype as a predictor of naltrexone response; and (iii) examine mechanisms of naltrexone in reward drinkers. Design: Secondary analysis of a randomized controlled trial. Setting: USA. Participants: A total of 128 young adult (ages 18–25) heavy drinkers. Interventions: Naltrexone versus placebo. Measurements: Daily surveys assessed affect, urge, drinking, and context. The Drinking Motives Questionnaire was used to identify phenotypes based on reward (enhancement motives) and relief (coping motives) drinking. Findings: We identified three profiles: “Low reward/Low relief” (14.1%; low enhancement/low coping motives); “Reward drinkers” (62.2%; high enhancement/low coping motives); and “High reward/High relief” (22.7%; high enhancement/high coping motives). Among reward drinkers (versus low profile), naltrexone significantly reduced percent days drinking to intoxication (blood alcohol concentration [BAC] ≥0.08) (PDI) (d = 0.56; 95% CI [0.17, 0.96]) and percent high intensity drinking days (PHID) (8/10 drinks for women/men) (d = 0.32; 95% CI [0.01, 0.68]). Among the high reward/high relief profile drinkers (versus low profile), naltrexone reduced PHID (d = 0.69; 95% CI [0.02, 1.50]). Using profile-informed cutoffs and observed scores (for clinical applicability): (i) among cutoff-derived reward drinkers, we found a medium-to-large (d = 0.66; 95% CI [0.24, 1.16]) and small effect (d = 0.28; 95% CI [0.04, 0.72]) of naltrexone in reducing PDI and PHID, respectively; and (ii) among the cutoff-derived high reward/high relief subgroup, we found a medium-to-large effect (d = 0.63; 95% CI [0.05, 1.1]) of naltrexone in reducing PHID. Among reward drinkers (not other profiles), naltrexone reduced drinking on days a drinking event occurred by weakening the within-day association between positive affect and urges (P < 0.05). Conclusions: Naltrexone has pronounced effects in reducing risky drinking among young adult reward drinkers (high reward/low relief) by reducing urges on days when individuals have higher positive affect and are exposed to a drinking event. Naltrexone also appears to reduce risky drinking among young adult high reward/high relief drinkers, but not via the same mechanism.

AB - Aims: Theory-driven, exploratory study to: (i) identify a reward drinking phenotype in young adults; (ii) evaluate this phenotype as a predictor of naltrexone response; and (iii) examine mechanisms of naltrexone in reward drinkers. Design: Secondary analysis of a randomized controlled trial. Setting: USA. Participants: A total of 128 young adult (ages 18–25) heavy drinkers. Interventions: Naltrexone versus placebo. Measurements: Daily surveys assessed affect, urge, drinking, and context. The Drinking Motives Questionnaire was used to identify phenotypes based on reward (enhancement motives) and relief (coping motives) drinking. Findings: We identified three profiles: “Low reward/Low relief” (14.1%; low enhancement/low coping motives); “Reward drinkers” (62.2%; high enhancement/low coping motives); and “High reward/High relief” (22.7%; high enhancement/high coping motives). Among reward drinkers (versus low profile), naltrexone significantly reduced percent days drinking to intoxication (blood alcohol concentration [BAC] ≥0.08) (PDI) (d = 0.56; 95% CI [0.17, 0.96]) and percent high intensity drinking days (PHID) (8/10 drinks for women/men) (d = 0.32; 95% CI [0.01, 0.68]). Among the high reward/high relief profile drinkers (versus low profile), naltrexone reduced PHID (d = 0.69; 95% CI [0.02, 1.50]). Using profile-informed cutoffs and observed scores (for clinical applicability): (i) among cutoff-derived reward drinkers, we found a medium-to-large (d = 0.66; 95% CI [0.24, 1.16]) and small effect (d = 0.28; 95% CI [0.04, 0.72]) of naltrexone in reducing PDI and PHID, respectively; and (ii) among the cutoff-derived high reward/high relief subgroup, we found a medium-to-large effect (d = 0.63; 95% CI [0.05, 1.1]) of naltrexone in reducing PHID. Among reward drinkers (not other profiles), naltrexone reduced drinking on days a drinking event occurred by weakening the within-day association between positive affect and urges (P < 0.05). Conclusions: Naltrexone has pronounced effects in reducing risky drinking among young adult reward drinkers (high reward/low relief) by reducing urges on days when individuals have higher positive affect and are exposed to a drinking event. Naltrexone also appears to reduce risky drinking among young adult high reward/high relief drinkers, but not via the same mechanism.

KW - Heavy drinking

KW - mechanisms

KW - naltrexone

KW - precision medicine

KW - reward drinker

KW - young adults

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ER -

Reward drinking and naltrexone treatment response among young adult heavy drinkers

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