Discovery and validation of genes driving drug-intake and related behavioral traits in mice

Tyler A Roy; Jason A Bubier; Price E Dickson; Troy D Wilcox; Juliet Ndukum; James W Clark; Stacey J Sukoff Rizzo; John C Crabbe; James M Denegre; Karen L Svenson; Robert E Braun; Vivek Kumar; Stephen A Murray; Jacqueline K White; Vivek M Philip; Elissa J Chesler

doi:10.1111/gbb.12875

Discovery and validation of genes driving drug-intake and related behavioral traits in mice

Genes Brain Behav. 2024 Jan 2;23(1):e12875. doi: 10.1111/gbb.12875. Online ahead of print.

Authors

Tyler A Roy¹, Jason A Bubier¹, Price E Dickson², Troy D Wilcox¹, Juliet Ndukum¹, James W Clark¹, Stacey J Sukoff Rizzo^{1

3}, John C Crabbe⁴, James M Denegre¹, Karen L Svenson¹, Robert E Braun¹, Vivek Kumar¹, Stephen A Murray¹, Jacqueline K White¹, Vivek M Philip¹, Elissa J Chesler¹

Affiliations

¹ Center for Addiction Biology, The Jackson Laboratory, Bar Harbor, Maine, USA.
² Joan C Edwards School of Medicine, Marshall University, Huntington, West Virginia, USA.
³ School of Medicine, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.
⁴ VA Portland Health Care System, Oregon Health & Science University, Portland, Oregon, USA.

Abstract

Substance use disorders are heritable disorders characterized by compulsive drug use, the biological mechanisms for which remain largely unknown. Genetic correlations reveal that predisposing drug-naïve phenotypes, including anxiety, depression, novelty preference and sensation seeking, are predictive of drug-use phenotypes, thereby implicating shared genetic mechanisms. High-throughput behavioral screening in knockout (KO) mice allows efficient discovery of the function of genes. We used this strategy in two rounds of candidate prioritization in which we identified 33 drug-use candidate genes based upon predisposing drug-naïve phenotypes and ultimately validated the perturbation of 22 genes as causal drivers of substance intake. We selected 19/221 KO strains (8.5%) that had a difference from control on at least one drug-naïve predictive behavioral phenotype and determined that 15/19 (~80%) affected the consumption or preference for alcohol, methamphetamine or both. No mutant exhibited a difference in nicotine consumption or preference which was possibly confounded with saccharin. In the second round of prioritization, we employed a multivariate approach to identify outliers and performed validation using methamphetamine two-bottle choice and ethanol drinking-in-the-dark protocols. We identified 15/401 KO strains (3.7%, which included one gene from the first cohort) that differed most from controls for the predisposing phenotypes. 8 of 15 gene deletions (53%) affected intake or preference for alcohol, methamphetamine or both. Using multivariate and bioinformatic analyses, we observed multiple relations between predisposing behaviors and drug intake, revealing many distinct biobehavioral processes underlying these relationships. The set of mouse models identified in this study can be used to characterize these addiction-related processes further.

Keywords: KOMP; addiction; addiction predicative; alcohol; genetic screen; knock-out; methamphetamine; mouse mutants; neurogenetics; nicotine; phenotyping.

Abstract

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