Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis

Haloperidol is an efficacious antipsychotic drug that has serious, unpredictable motor side effects that limit its utility and cause noncompliance in many patients. Using a drug–placebo diallel of the eight founder strains of the Collaborative Cross and their F(1) hybrids, we characterized aggregate...

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Autores principales: Crowley, James J., Kim, Yunjung, Lenarcic, Alan B., Quackenbush, Corey R., Barrick, Cordelia J., Adkins, Daniel E., Shaw, Ginger S., Miller, Darla R., de Villena, Fernando Pardo-Manuel, Sullivan, Patrick F., Valdar, William
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Genetics Society of America 2014
Materias:
Investigations
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3872195/
https://www.ncbi.nlm.nih.gov/pubmed/24240528
http://dx.doi.org/10.1534/genetics.113.156901
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author Crowley, James J.
Kim, Yunjung
Lenarcic, Alan B.
Quackenbush, Corey R.
Barrick, Cordelia J.
Adkins, Daniel E.
Shaw, Ginger S.
Miller, Darla R.
de Villena, Fernando Pardo-Manuel
Sullivan, Patrick F.
Valdar, William
author_facet Crowley, James J.
Kim, Yunjung
Lenarcic, Alan B.
Quackenbush, Corey R.
Barrick, Cordelia J.
Adkins, Daniel E.
Shaw, Ginger S.
Miller, Darla R.
de Villena, Fernando Pardo-Manuel
Sullivan, Patrick F.
Valdar, William
author_sort Crowley, James J.
collection PubMed
description Haloperidol is an efficacious antipsychotic drug that has serious, unpredictable motor side effects that limit its utility and cause noncompliance in many patients. Using a drug–placebo diallel of the eight founder strains of the Collaborative Cross and their F(1) hybrids, we characterized aggregate effects of genetics, sex, parent of origin, and their combinations on haloperidol response. Treating matched pairs of both sexes with drug or placebo, we measured changes in the following: open field activity, inclined screen rigidity, orofacial movements, prepulse inhibition of the acoustic startle response, plasma and brain drug level measurements, and body weight. To understand the genetic architecture of haloperidol response we introduce new statistical methodology linking heritable variation with causal effect of drug treatment. Our new estimators, “difference of models” and “multiple-impute matched pairs”, are motivated by the Neyman–Rubin potential outcomes framework and extend our existing Bayesian hierarchical model for the diallel (Lenarcic et al. 2012). Drug-induced rigidity after chronic treatment was affected by mainly additive genetics and parent-of-origin effects (accounting for 28% and 14.8% of the variance), with NZO/HILtJ and 129S1/SvlmJ contributions tending to increase this side effect. Locomotor activity after acute treatment, by contrast, was more affected by strain-specific inbreeding (12.8%). In addition to drug response phenotypes, we examined diallel effects on behavior before treatment and found not only effects of additive genetics (10.2–53.2%) but also strong effects of epistasis (10.64–25.2%). In particular: prepulse inhibition showed additivity and epistasis in about equal proportions (26.1% and 23.7%); there was evidence of nonreciprocal epistasis in pretreatment activity and rigidity; and we estimated a range of effects on body weight that replicate those found in our previous work. Our results provide the first quantitative description of the genetic architecture of haloperidol response in mice and indicate that additive, dominance-like inbreeding and parent-of-origin effects contribute strongly to treatment effect heterogeneity for this drug.
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spelling pubmed-38721952013-12-26 Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis Crowley, James J. Kim, Yunjung Lenarcic, Alan B. Quackenbush, Corey R. Barrick, Cordelia J. Adkins, Daniel E. Shaw, Ginger S. Miller, Darla R. de Villena, Fernando Pardo-Manuel Sullivan, Patrick F. Valdar, William Genetics Investigations Haloperidol is an efficacious antipsychotic drug that has serious, unpredictable motor side effects that limit its utility and cause noncompliance in many patients. Using a drug–placebo diallel of the eight founder strains of the Collaborative Cross and their F(1) hybrids, we characterized aggregate effects of genetics, sex, parent of origin, and their combinations on haloperidol response. Treating matched pairs of both sexes with drug or placebo, we measured changes in the following: open field activity, inclined screen rigidity, orofacial movements, prepulse inhibition of the acoustic startle response, plasma and brain drug level measurements, and body weight. To understand the genetic architecture of haloperidol response we introduce new statistical methodology linking heritable variation with causal effect of drug treatment. Our new estimators, “difference of models” and “multiple-impute matched pairs”, are motivated by the Neyman–Rubin potential outcomes framework and extend our existing Bayesian hierarchical model for the diallel (Lenarcic et al. 2012). Drug-induced rigidity after chronic treatment was affected by mainly additive genetics and parent-of-origin effects (accounting for 28% and 14.8% of the variance), with NZO/HILtJ and 129S1/SvlmJ contributions tending to increase this side effect. Locomotor activity after acute treatment, by contrast, was more affected by strain-specific inbreeding (12.8%). In addition to drug response phenotypes, we examined diallel effects on behavior before treatment and found not only effects of additive genetics (10.2–53.2%) but also strong effects of epistasis (10.64–25.2%). In particular: prepulse inhibition showed additivity and epistasis in about equal proportions (26.1% and 23.7%); there was evidence of nonreciprocal epistasis in pretreatment activity and rigidity; and we estimated a range of effects on body weight that replicate those found in our previous work. Our results provide the first quantitative description of the genetic architecture of haloperidol response in mice and indicate that additive, dominance-like inbreeding and parent-of-origin effects contribute strongly to treatment effect heterogeneity for this drug. Genetics Society of America 2014-01 2013-11-11 /pmc/articles/PMC3872195/ /pubmed/24240528 http://dx.doi.org/10.1534/genetics.113.156901 Text en Copyright © 2014 by the Genetics Society of America Available freely online through the author-supported open access option.
spellingShingle Investigations
Crowley, James J.
Kim, Yunjung
Lenarcic, Alan B.
Quackenbush, Corey R.
Barrick, Cordelia J.
Adkins, Daniel E.
Shaw, Ginger S.
Miller, Darla R.
de Villena, Fernando Pardo-Manuel
Sullivan, Patrick F.
Valdar, William
Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis
title Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis
title_full Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis
title_fullStr Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis
title_full_unstemmed Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis
title_short Genetics of Adverse Reactions to Haloperidol in a Mouse Diallel: A Drug–Placebo Experiment and Bayesian Causal Analysis
title_sort genetics of adverse reactions to haloperidol in a mouse diallel: a drug–placebo experiment and bayesian causal analysis
topic Investigations
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3872195/
https://www.ncbi.nlm.nih.gov/pubmed/24240528
http://dx.doi.org/10.1534/genetics.113.156901
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