A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence

Conrad J. Wong; Jennifer Witcher; Craig Mallinckrodt; Robert A. Dean; Raymond F. Anton; Yunfei Chen; Bonnie A. Fijal; Haojun Ouyang; Sweta Dharia; Scott S. Sundseth; Kory J. Schuh; Bruce J. Kinon

doi:10.1111/acer.12257

A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence

Conrad J. Wong, Jennifer Witcher, Craig Mallinckrodt, Robert A. Dean, Raymond F. Anton, Yunfei Chen, Bonnie A. Fijal, Haojun Ouyang, Sweta Dharia, Scott S. Sundseth, Kory J. Schuh, Bruce J. Kinon

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

11 Scopus citations

Abstract

Background: Endogenous opioid-mediated reward pathways may play a role in the development and maintenance of alcohol dependence. This study tested whether LY2196044, an opioid receptor antagonist, in combination with medical management would reduce drinking in alcohol-dependent patients. Methods: This was a multicenter, outpatient, randomized, double-blind, parallel, and placebo-controlled trial with a 16-week treatment period. Patients (N = 375) were alcohol-dependent, treatment-seeking adults. Patients were randomly assigned to once-daily LY2196044 (final doses of 125 or 250 mg/d) or placebo. DNA samples were collected at baseline. At each visit, patients underwent safety assessments, laboratory testing, efficacy measures, and medical management. Blood samples were also obtained for pharmacokinetic testing. The primary measure was the change from baseline in the percent heavy drinking days (HDD). Secondary efficacy measures were percent days abstinent per month and number of drinks per day. Results: The treatment difference in change from baseline in % HDD between LY2196044 and placebo was not statistically significant (-43.02 vs. -38.72%, respectively; p = 0.12). There was a trend toward greater change from baseline in the percent days abstinent per month for the LY2196044 group compared with the placebo group (33.49 vs. 28.12%, respectively; p = 0.051). The decrease from baseline for mean number of drinks per day was statistically significantly greater in the LY2196044 group compared with the placebo group (-5.37 vs. -4.66 drinks per day, respectively; p = 0.013). LY2196044-treated patients who were dopamine receptor type 4-variable number tandem repeat L carriers had greater reductions in % HDD (p = 0.0565), increased percent days abstinent (p = 0.0496), and reduced drinks per day (p = 0.0069) than placebo-treated L carriers. The safety profile for LY2196044 appeared similar to that of other opioid antagonists. Conclusions: The results from this proof-of-concept clinical trial warrant further evaluation of LY2196044 for the treatment of alcohol dependence.

Original language	English (US)
Pages (from-to)	511-520
Number of pages	10
Journal	Alcoholism: Clinical and Experimental Research
Volume	38
Issue number	2
DOIs	https://doi.org/10.1111/acer.12257
State	Published - Feb 2014
Externally published	Yes

Keywords

Alcohol
Antagonist
Dependence
LY2196044
Opioid

ASJC Scopus subject areas

Medicine (miscellaneous)
Toxicology
Psychiatry and Mental health

Access to Document

10.1111/acer.12257

Cite this

Wong, C. J., Witcher, J., Mallinckrodt, C., Dean, R. A., Anton, R. F., Chen, Y., Fijal, B. A., Ouyang, H., Dharia, S., Sundseth, S. S., Schuh, K. J., & Kinon, B. J. (2014). A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence. Alcoholism: Clinical and Experimental Research, 38(2), 511-520. https://doi.org/10.1111/acer.12257

Wong, CJ, Witcher, J, Mallinckrodt, C, Dean, RA, Anton, RF, Chen, Y, Fijal, BA, Ouyang, H, Dharia, S, Sundseth, SS, Schuh, KJ & Kinon, BJ 2014, 'A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence', Alcoholism: Clinical and Experimental Research, vol. 38, no. 2, pp. 511-520. https://doi.org/10.1111/acer.12257

@article{7c431bcab8f04a91a2559123cf1e5091,

title = "A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence",

abstract = "Background: Endogenous opioid-mediated reward pathways may play a role in the development and maintenance of alcohol dependence. This study tested whether LY2196044, an opioid receptor antagonist, in combination with medical management would reduce drinking in alcohol-dependent patients. Methods: This was a multicenter, outpatient, randomized, double-blind, parallel, and placebo-controlled trial with a 16-week treatment period. Patients (N = 375) were alcohol-dependent, treatment-seeking adults. Patients were randomly assigned to once-daily LY2196044 (final doses of 125 or 250 mg/d) or placebo. DNA samples were collected at baseline. At each visit, patients underwent safety assessments, laboratory testing, efficacy measures, and medical management. Blood samples were also obtained for pharmacokinetic testing. The primary measure was the change from baseline in the percent heavy drinking days (HDD). Secondary efficacy measures were percent days abstinent per month and number of drinks per day. Results: The treatment difference in change from baseline in % HDD between LY2196044 and placebo was not statistically significant (-43.02 vs. -38.72%, respectively; p = 0.12). There was a trend toward greater change from baseline in the percent days abstinent per month for the LY2196044 group compared with the placebo group (33.49 vs. 28.12%, respectively; p = 0.051). The decrease from baseline for mean number of drinks per day was statistically significantly greater in the LY2196044 group compared with the placebo group (-5.37 vs. -4.66 drinks per day, respectively; p = 0.013). LY2196044-treated patients who were dopamine receptor type 4-variable number tandem repeat L carriers had greater reductions in % HDD (p = 0.0565), increased percent days abstinent (p = 0.0496), and reduced drinks per day (p = 0.0069) than placebo-treated L carriers. The safety profile for LY2196044 appeared similar to that of other opioid antagonists. Conclusions: The results from this proof-of-concept clinical trial warrant further evaluation of LY2196044 for the treatment of alcohol dependence.",

keywords = "Alcohol, Antagonist, Dependence, LY2196044, Opioid",

author = "Wong, {Conrad J.} and Jennifer Witcher and Craig Mallinckrodt and Dean, {Robert A.} and Anton, {Raymond F.} and Yunfei Chen and Fijal, {Bonnie A.} and Haojun Ouyang and Sweta Dharia and Sundseth, {Scott S.} and Schuh, {Kory J.} and Kinon, {Bruce J.}",

year = "2014",

month = feb,

doi = "10.1111/acer.12257",

language = "English (US)",

volume = "38",

pages = "511--520",

journal = "Alcoholism: Clinical and Experimental Research",

issn = "0145-6008",

publisher = "Wiley-Blackwell",

number = "2",

}

TY - JOUR

T1 - A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence

AU - Wong, Conrad J.

AU - Witcher, Jennifer

AU - Mallinckrodt, Craig

AU - Dean, Robert A.

AU - Anton, Raymond F.

AU - Chen, Yunfei

AU - Fijal, Bonnie A.

AU - Ouyang, Haojun

AU - Dharia, Sweta

AU - Sundseth, Scott S.

AU - Schuh, Kory J.

AU - Kinon, Bruce J.

PY - 2014/2

Y1 - 2014/2

N2 - Background: Endogenous opioid-mediated reward pathways may play a role in the development and maintenance of alcohol dependence. This study tested whether LY2196044, an opioid receptor antagonist, in combination with medical management would reduce drinking in alcohol-dependent patients. Methods: This was a multicenter, outpatient, randomized, double-blind, parallel, and placebo-controlled trial with a 16-week treatment period. Patients (N = 375) were alcohol-dependent, treatment-seeking adults. Patients were randomly assigned to once-daily LY2196044 (final doses of 125 or 250 mg/d) or placebo. DNA samples were collected at baseline. At each visit, patients underwent safety assessments, laboratory testing, efficacy measures, and medical management. Blood samples were also obtained for pharmacokinetic testing. The primary measure was the change from baseline in the percent heavy drinking days (HDD). Secondary efficacy measures were percent days abstinent per month and number of drinks per day. Results: The treatment difference in change from baseline in % HDD between LY2196044 and placebo was not statistically significant (-43.02 vs. -38.72%, respectively; p = 0.12). There was a trend toward greater change from baseline in the percent days abstinent per month for the LY2196044 group compared with the placebo group (33.49 vs. 28.12%, respectively; p = 0.051). The decrease from baseline for mean number of drinks per day was statistically significantly greater in the LY2196044 group compared with the placebo group (-5.37 vs. -4.66 drinks per day, respectively; p = 0.013). LY2196044-treated patients who were dopamine receptor type 4-variable number tandem repeat L carriers had greater reductions in % HDD (p = 0.0565), increased percent days abstinent (p = 0.0496), and reduced drinks per day (p = 0.0069) than placebo-treated L carriers. The safety profile for LY2196044 appeared similar to that of other opioid antagonists. Conclusions: The results from this proof-of-concept clinical trial warrant further evaluation of LY2196044 for the treatment of alcohol dependence.

AB - Background: Endogenous opioid-mediated reward pathways may play a role in the development and maintenance of alcohol dependence. This study tested whether LY2196044, an opioid receptor antagonist, in combination with medical management would reduce drinking in alcohol-dependent patients. Methods: This was a multicenter, outpatient, randomized, double-blind, parallel, and placebo-controlled trial with a 16-week treatment period. Patients (N = 375) were alcohol-dependent, treatment-seeking adults. Patients were randomly assigned to once-daily LY2196044 (final doses of 125 or 250 mg/d) or placebo. DNA samples were collected at baseline. At each visit, patients underwent safety assessments, laboratory testing, efficacy measures, and medical management. Blood samples were also obtained for pharmacokinetic testing. The primary measure was the change from baseline in the percent heavy drinking days (HDD). Secondary efficacy measures were percent days abstinent per month and number of drinks per day. Results: The treatment difference in change from baseline in % HDD between LY2196044 and placebo was not statistically significant (-43.02 vs. -38.72%, respectively; p = 0.12). There was a trend toward greater change from baseline in the percent days abstinent per month for the LY2196044 group compared with the placebo group (33.49 vs. 28.12%, respectively; p = 0.051). The decrease from baseline for mean number of drinks per day was statistically significantly greater in the LY2196044 group compared with the placebo group (-5.37 vs. -4.66 drinks per day, respectively; p = 0.013). LY2196044-treated patients who were dopamine receptor type 4-variable number tandem repeat L carriers had greater reductions in % HDD (p = 0.0565), increased percent days abstinent (p = 0.0496), and reduced drinks per day (p = 0.0069) than placebo-treated L carriers. The safety profile for LY2196044 appeared similar to that of other opioid antagonists. Conclusions: The results from this proof-of-concept clinical trial warrant further evaluation of LY2196044 for the treatment of alcohol dependence.

KW - Alcohol

KW - Antagonist

KW - Dependence

KW - LY2196044

KW - Opioid

UR - http://www.scopus.com/inward/record.url?scp=84893652535&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84893652535&partnerID=8YFLogxK

U2 - 10.1111/acer.12257

DO - 10.1111/acer.12257

M3 - Article

C2 - 24010675

AN - SCOPUS:84893652535

SN - 0145-6008

VL - 38

SP - 511

EP - 520

JO - Alcoholism: Clinical and Experimental Research

JF - Alcoholism: Clinical and Experimental Research

IS - 2

ER -

A Phase 2, Placebo-Controlled Study of the Opioid Receptor Antagonist LY2196044 for the Treatment of Alcohol Dependence

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this