GeneSet Information

Tier III GS31782 • Gene Expression Correlations with Hippocampus Consortium M430v2 (Jun06) RMA for Localization of genes affecting alcohol drinking in mice Phillips et al (1994).

DESCRIPTION:

Preference for 10% ethanol (g/kg) in tap water offered vs. tap water; means are the average of days 2 and 4 of a 4-day 24-hr access period by Phillips TJ , et al

LABEL:

EtOH preference co-expression

SCORE TYPE:

P-Value

DATE ADDED:

2009-06-18

DATE UPDATED:

2024-04-25

SPECIES:

AUTHORS:

Phillips TJ, Crabbe JC, Metten P, Belknap JK

TITLE:

Localization of genes affecting alcohol drinking in mice.

JOURNAL:

Alcoholism, clinical and experimental research Aug 1994, Vol 18, pp. 931-41

ABSTRACT:

The genomic map locations of specific genes controlling behaviors can be identified by studying a panel of recombinant inbred (RI) mouse strains. The progenitor C57BL/6J (B6) and DBA/2J (D2) strains, and 19 of the BXD RI strains derived from an F2 cross of these progenitors, were tested for 3% and 10% ethanol (EtOH) intake. The test sequence began with two-bottle free choice between tap water and unsweetened ethanol, and ended with free choice between water and saccharin-sweetened ethanol. Saccharin preference was also measured. Correlational analyses indicated that 59% of the genetic variance in 10% ethanol and sweetened 10% ethanol consumption was held in common, 24% of the genetic variance in saccharin and sweetened 10% ethanol consumption was held in common, and only 7% of the genetic variance in saccharin and unsweetened 10% ethanol consumption was held in common. These percentages for 3% ethanol solutions were 21%, 36%, and 14%. In addition, the severity of handling-induced convulsions during ethanol withdrawal was found to be significantly associated with the amount of ethanol consumed from the sweetened ethanol drinking tubes, suggesting that genetic differences in avidity for ethanol could lead to the development of physical dependence. Quantitative trait loci (QTL) analyses revealed that several genetic markers were associated with ethanol consumption levels, including markers for the D2 dopamine receptor. QTL analyses of saccharin and sweetened ethanol consumption identified the sac locus, thought to determine the ability to detect saccharin. In general, our results suggest that saccharin and ethanol consumption are determined by the actions of multiple genes (QTL), some in common, and suggest specific map locations of several such QTL on the mouse genome. PUBMED: 7978106
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Annotation Information

No sequence read archive data associated with this GeneSet.


Aptitude (D001076)
Seizures (D012640)
Drinking (D004326)
Animals (D000818)
Species Specificity (D013045)
Behavior (D001519)
Solutions (D012996)
Chromosome Mapping (D002874)
Quantitative Trait Loci (D040641)
Genetic Markers (D005819)
Alcohol Drinking (D000428)
Recombination, Genetic (D011995)
Dopamine (D004298)
Mice, Inbred Strains (D008815)
Saccharin (D012439)
Receptors, Dopamine (D011954)
Ethanol (D000431)
Hippocampus (D006624)
hippocampus (MA:0000191)
saccharin preference (MP:0002850)
convulsive seizures (MP:0000947)
localization (GO:0051179)
gene expression (GO:0010467)

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