Literature DB >> 20033183

A method for mapping intralocus interactions influencing excessive alcohol drinking.

Tamara J Phillips1, Cheryl Reed, Sue Burkhart-Kasch, Na Li, Robert Hitzemann, Chia-Hua Yu, Lauren L Brown, Melinda L Helms, John C Crabbe, John K Belknap.   

Abstract

Excessive alcohol (ethanol) consumption is the hallmark of alcohol use disorders. The F1 hybrid cross between the C57BL/6J (B6) and FVB/NJ (FVB) inbred mouse strains consumes more ethanol than either progenitor strain. The purpose of this study was to utilize ethanol-drinking data and genetic information to map genes that result in overdominant (or heterotic) ethanol drinking. About 600 B6 x FVB F2 mice, half of each sex, were tested for ethanol intake and preference in a 24-h, two-bottle water versus ethanol choice procedure, with ascending ethanol concentrations. They were then tested for ethanol intake in a Drinking in the Dark (DID) procedure, first when there was no water choice and then when ethanol was offered versus water. DNA samples were obtained and genome-wide QTL analyses were performed to search for single QTLs (both additive and dominance effects) and interactions between pairs of QTLs, or epistasis. On average, F2 mice consumed excessive amounts of ethanol in the 24-h choice procedure, consistent with high levels of consumption seen in the F1 cross. Consumption in the DID procedure was similar or higher than amounts reported previously for the B6 progenitor. QTLs resulting in heightened consumption in heterozygous compared to homozygous animals were found on Chrs 11, 15, and 16 for 24-h choice 30% ethanol consumption, and on Chr 11 for DID. No evidence was found for epistasis between any pair of significant or suggestive QTLs. This indicates that the hybrid overdominance is due to intralocus interactions at the level of individual QTL.

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Year:  2009        PMID: 20033183      PMCID: PMC2850100          DOI: 10.1007/s00335-009-9239-9

Source DB:  PubMed          Journal:  Mamm Genome        ISSN: 0938-8990            Impact factor:   2.957


  31 in total

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4.  Genetic analysis of alcohol intake in recombinant inbred and congenic strains derived from A/J and C57BL/6J progenitors.

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Journal:  Mamm Genome       Date:  2005-05       Impact factor: 2.957

5.  Effects of a Drd2 deletion mutation on ethanol-induced locomotor stimulation and sensitization suggest a role for epistasis.

Authors:  Abraham A Palmer; Malcolm J Low; David K Grandy; Tamara J Phillips
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6.  A line of mice selected for high blood ethanol concentrations shows drinking in the dark to intoxication.

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  14 in total

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Review 4.  "Drinking in the dark" (DID) procedures: a model of binge-like ethanol drinking in non-dependent mice.

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8.  The μ opioid receptor is not involved in ethanol-stimulated dopamine release in the ventral striatum of C57BL/6J mice.

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Review 9.  High drinking in the dark mice: a genetic model of drinking to intoxication.

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10.  Neuropeptide Y response to alcohol is altered in nucleus accumbens of mice selectively bred for drinking to intoxication.

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