A GABRA2 polymorphism improves a model for prediction of drinking initiation

Samuel Kuperman; Grace Chan; John Kramer; Leah Wetherill; Laura Acion; Howard J. Edenberg; Tatiana M. Foroud; John Nurnberger; Arpana Agrawal; Andrey Anokhin; Andrew Brooks; Victor Hesselbrock; Michie Hesselbrock; Marc Schuckit; Jay Tischfield; Xiangtao Liu

doi:10.1016/j.alcohol.2017.03.003

A GABRA2 polymorphism improves a model for prediction of drinking initiation

Samuel Kuperman, Grace Chan, John Kramer, Leah Wetherill, Laura Acion, Howard J. Edenberg, Tatiana M. Foroud, John Nurnberger, Arpana Agrawal, Andrey Anokhin, Andrew Brooks, Victor Hesselbrock, Michie Hesselbrock, Marc Schuckit, Jay Tischfield, Xiangtao Liu

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

4 Scopus citations

Abstract

Background Survival analysis was used to explore the addition of a single nucleotide polymorphism (SNP) and covariates (sex, interview age, and ancestry) on a previously published model's ability to predict onset of drinking. A SNP variant of rs279871, in the chromosome 4 gene encoding gamma-aminobutyric acid receptor (GABRA2), was selected due to its associations with alcoholism in young adults and with behaviors that increased risk for early drinking. Methods A subsample of 674 adolescents (ages 14–17) participating in the Collaborative Study on the Genetics of Alcoholism (COGA) was examined using a previously derived Cox proportional hazards model containing: 1) number of non-drinking related conduct disorder (CD) symptoms, 2) membership in a high-risk alcohol-dependent (AD) family, 3) most best friends drank (MBFD), 4) Achenbach Youth Self Report (YSR) externalizing score, and 5) YSR social problems score. The above covariates along with the SNP variant of GABRA2, rs279871, were added to this model. Five new prototype models were examined. The most parsimonious model was chosen based on likelihood ratio tests and model fit statistics. Results The final model contained four of the five original predictors (YSR social problems score was no longer significant and hence dropped from subsequent models), the three covariates, and a recessive GABRA2 rs279871 TT genotype (two copies of the high-risk allele containing thymine). The model indicated that adolescents with the high-risk TT genotype were more likely to begin drinking than those without this genotype. Conclusions The joint effect of the gene (rs279871 TT genotype) and environment (MBFD) on adolescent alcohol initiation is additive, but not interactive, after controlling for behavior problems (CD and YSR externalizing score). This suggests that the impact of the high-risk TT genotype on the onset of drinking is affected by controlling for peer drinking and does not include genotype-by-environment interactions.

Original language	English (US)
Pages (from-to)	1-8
Number of pages	8
Journal	Alcohol
Volume	63
DOIs	https://doi.org/10.1016/j.alcohol.2017.03.003
State	Published - Sep 2017

All Science Journal Classification (ASJC) codes

Health(social science)
Biochemistry
Toxicology
Neurology
Behavioral Neuroscience

Keywords

Adolescent
Alcohol
Drinking initiation
GABRA2
Rs279871
Survival analysis modeling

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10.1016/j.alcohol.2017.03.003

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Kuperman, S., Chan, G., Kramer, J., Wetherill, L., Acion, L., Edenberg, H. J., Foroud, T. M., Nurnberger, J., Agrawal, A., Anokhin, A., Brooks, A., Hesselbrock, V., Hesselbrock, M., Schuckit, M., Tischfield, J., & Liu, X. (2017). A GABRA2 polymorphism improves a model for prediction of drinking initiation. Alcohol, 63, 1-8. https://doi.org/10.1016/j.alcohol.2017.03.003

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title = "A GABRA2 polymorphism improves a model for prediction of drinking initiation",

abstract = "Background Survival analysis was used to explore the addition of a single nucleotide polymorphism (SNP) and covariates (sex, interview age, and ancestry) on a previously published model's ability to predict onset of drinking. A SNP variant of rs279871, in the chromosome 4 gene encoding gamma-aminobutyric acid receptor (GABRA2), was selected due to its associations with alcoholism in young adults and with behaviors that increased risk for early drinking. Methods A subsample of 674 adolescents (ages 14–17) participating in the Collaborative Study on the Genetics of Alcoholism (COGA) was examined using a previously derived Cox proportional hazards model containing: 1) number of non-drinking related conduct disorder (CD) symptoms, 2) membership in a high-risk alcohol-dependent (AD) family, 3) most best friends drank (MBFD), 4) Achenbach Youth Self Report (YSR) externalizing score, and 5) YSR social problems score. The above covariates along with the SNP variant of GABRA2, rs279871, were added to this model. Five new prototype models were examined. The most parsimonious model was chosen based on likelihood ratio tests and model fit statistics. Results The final model contained four of the five original predictors (YSR social problems score was no longer significant and hence dropped from subsequent models), the three covariates, and a recessive GABRA2 rs279871 TT genotype (two copies of the high-risk allele containing thymine). The model indicated that adolescents with the high-risk TT genotype were more likely to begin drinking than those without this genotype. Conclusions The joint effect of the gene (rs279871 TT genotype) and environment (MBFD) on adolescent alcohol initiation is additive, but not interactive, after controlling for behavior problems (CD and YSR externalizing score). This suggests that the impact of the high-risk TT genotype on the onset of drinking is affected by controlling for peer drinking and does not include genotype-by-environment interactions.",

keywords = "Adolescent, Alcohol, Drinking initiation, GABRA2, Rs279871, Survival analysis modeling",

author = "Samuel Kuperman and Grace Chan and John Kramer and Leah Wetherill and Laura Acion and Edenberg, {Howard J.} and Foroud, {Tatiana M.} and John Nurnberger and Arpana Agrawal and Andrey Anokhin and Andrew Brooks and Victor Hesselbrock and Michie Hesselbrock and Marc Schuckit and Jay Tischfield and Xiangtao Liu",

note = "Publisher Copyright: {\textcopyright} 2017 Elsevier Inc.",

year = "2017",

month = sep,

doi = "10.1016/j.alcohol.2017.03.003",

language = "English (US)",

volume = "63",

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T1 - A GABRA2 polymorphism improves a model for prediction of drinking initiation

AU - Kuperman, Samuel

AU - Chan, Grace

AU - Kramer, John

AU - Wetherill, Leah

AU - Acion, Laura

AU - Edenberg, Howard J.

AU - Foroud, Tatiana M.

AU - Nurnberger, John

AU - Agrawal, Arpana

AU - Anokhin, Andrey

AU - Brooks, Andrew

AU - Hesselbrock, Victor

AU - Hesselbrock, Michie

AU - Schuckit, Marc

AU - Tischfield, Jay

AU - Liu, Xiangtao

PY - 2017/9

Y1 - 2017/9

N2 - Background Survival analysis was used to explore the addition of a single nucleotide polymorphism (SNP) and covariates (sex, interview age, and ancestry) on a previously published model's ability to predict onset of drinking. A SNP variant of rs279871, in the chromosome 4 gene encoding gamma-aminobutyric acid receptor (GABRA2), was selected due to its associations with alcoholism in young adults and with behaviors that increased risk for early drinking. Methods A subsample of 674 adolescents (ages 14–17) participating in the Collaborative Study on the Genetics of Alcoholism (COGA) was examined using a previously derived Cox proportional hazards model containing: 1) number of non-drinking related conduct disorder (CD) symptoms, 2) membership in a high-risk alcohol-dependent (AD) family, 3) most best friends drank (MBFD), 4) Achenbach Youth Self Report (YSR) externalizing score, and 5) YSR social problems score. The above covariates along with the SNP variant of GABRA2, rs279871, were added to this model. Five new prototype models were examined. The most parsimonious model was chosen based on likelihood ratio tests and model fit statistics. Results The final model contained four of the five original predictors (YSR social problems score was no longer significant and hence dropped from subsequent models), the three covariates, and a recessive GABRA2 rs279871 TT genotype (two copies of the high-risk allele containing thymine). The model indicated that adolescents with the high-risk TT genotype were more likely to begin drinking than those without this genotype. Conclusions The joint effect of the gene (rs279871 TT genotype) and environment (MBFD) on adolescent alcohol initiation is additive, but not interactive, after controlling for behavior problems (CD and YSR externalizing score). This suggests that the impact of the high-risk TT genotype on the onset of drinking is affected by controlling for peer drinking and does not include genotype-by-environment interactions.

AB - Background Survival analysis was used to explore the addition of a single nucleotide polymorphism (SNP) and covariates (sex, interview age, and ancestry) on a previously published model's ability to predict onset of drinking. A SNP variant of rs279871, in the chromosome 4 gene encoding gamma-aminobutyric acid receptor (GABRA2), was selected due to its associations with alcoholism in young adults and with behaviors that increased risk for early drinking. Methods A subsample of 674 adolescents (ages 14–17) participating in the Collaborative Study on the Genetics of Alcoholism (COGA) was examined using a previously derived Cox proportional hazards model containing: 1) number of non-drinking related conduct disorder (CD) symptoms, 2) membership in a high-risk alcohol-dependent (AD) family, 3) most best friends drank (MBFD), 4) Achenbach Youth Self Report (YSR) externalizing score, and 5) YSR social problems score. The above covariates along with the SNP variant of GABRA2, rs279871, were added to this model. Five new prototype models were examined. The most parsimonious model was chosen based on likelihood ratio tests and model fit statistics. Results The final model contained four of the five original predictors (YSR social problems score was no longer significant and hence dropped from subsequent models), the three covariates, and a recessive GABRA2 rs279871 TT genotype (two copies of the high-risk allele containing thymine). The model indicated that adolescents with the high-risk TT genotype were more likely to begin drinking than those without this genotype. Conclusions The joint effect of the gene (rs279871 TT genotype) and environment (MBFD) on adolescent alcohol initiation is additive, but not interactive, after controlling for behavior problems (CD and YSR externalizing score). This suggests that the impact of the high-risk TT genotype on the onset of drinking is affected by controlling for peer drinking and does not include genotype-by-environment interactions.

KW - Adolescent

KW - Alcohol

KW - Drinking initiation

KW - GABRA2

KW - Rs279871

KW - Survival analysis modeling

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JO - Alcohol

JF - Alcohol

ER -

A GABRA2 polymorphism improves a model for prediction of drinking initiation

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