Identification of candidate genes that underlie the QTL on chromosome 1 that mediates genetic differences in stress-ethanol interactions

Author:

Cook Melloni N.1,Baker Jessica A.23,Heldt Scott A.2,Williams Robert W.4,Hamre Kristin M.2,Lu Lu45

Affiliation:

1. Department of Psychology, University of Memphis, Memphis, Tennessee;

2. Department of Anatomy and Neurobiology, University of Tennessee Health Science Center, Memphis, Tennessee;

3. Department of Neuroscience, Rhodes College, Memphis, Tennessee

4. Department of Genetics, Genomics and Informatics, University of Tennessee Health Science Center, Memphis, Tennessee;

5. Jiangsu Key Laboratory for Inflammation and Molecular Drug Target, Nantong University, Nantong, China; and

Abstract

Alcoholism, stress, and anxiety are strongly interacting heritable, polygenetic traits. In a previous study, we identified a quantitative trait locus (QTL) on murine chromosome (Chr) 1 between 23.0 and 31.5 Mb that modulates genetic differences in the effects of ethanol on anxiety-related phenotypes. The goal of the present study was to extend the analysis of this locus with a focus on identifying candidate genes using newly available data and tools. Anxiety-like behavior was evaluated with an elevated zero maze following saline or ethanol injections (1.8 g/kg) in C57BL/6J, DBA2J, and 72 BXD strains. We detected significant effects of strain and treatment and their interaction on anxiety-related behaviors, although surprisingly, sex was not a significant factor. The Chr1 QTL is specific to the ethanol-treated cohort. Candidate genes in this locus were evaluated using now standard bioinformatic criteria. Collagen 19a1 ( Col19a1) and family sequence 135a ( Fam135a) met most criteria but have lower expression levels and lacked biological verification and, therefore, were considered less likely candidates. In contrast, two other genes, the prenylated protein tyrosine phosphate family member Ptp4a1 (protein tyrosine phosphate 4a1) and the zinc finger protein Phf3 (plant homeoDomain finger protein 3) met each of our bioinformatic criteria and are thus strong candidates. These findings are also of translational relevance because both Ptp4a1 and Phf3 have been nominated as candidates genes for alcohol dependence in a human genome-wide association study. Our findings support the hypothesis that variants in one or both of these genes modulate heritable differences in the effects of ethanol on anxiety-related behaviors.

Funder

NIAAA

National Natural Science Foundation of China

Univeristy of Tennessee Health Science Center Bridge Funding

Publisher

American Physiological Society

Subject

Genetics,Physiology

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