Neurotoxic Consequences of Chronic Alcohol Withdrawal: Expression Profiling Reveals Importance of Gender Over Withdrawal Severity

Hashimoto, Joel G.; Wiren, Kristine M.

doi:10.1038/sj.npp.1301494

Cited by 67 publications

(124 citation statements)

References 72 publications

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“…Female B6 mice had significantly greater intake of 6E, with a trend for an increase in 10E, when compared to their male counterparts. Nonetheless, these findings are consistent with clinical and preclinical studies documenting the existence of sex differences in sensitivity to a number of alcohol-related behaviors associated with neuroadaptation and reinforcement (e.g., Devaud et al, 2003;Finn et al, 2004aFinn et al, , 2004bGreen et al, 1999;Hashimoto and Wiren, 2007;Lancaster, 1995;Middaugh and Kelly, 1999;Rhodes et al, 2007;Vivian et al, 2001;Wiren et al 2006). …”

Section: Discussionsupporting

confidence: 82%

Voluntary ethanol consumption in 22 inbred mouse strains

Yoneyama

Crabbe

Ford

et al. 2008

Alcohol

273

269

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Inbred strains are genetically stable across time and laboratories, allowing scientists to accumulate a record of phenotypes, including physiological characteristics and behaviors. To date, the C57/C58 family of inbred mouse strains has been identified as having the highest innate ethanol consumption, but some lineages have rarely or never been surveyed. Thus, the purpose of the present experiment was to measure ethanol preference and intake in 22 inbred mouse strains, some of which have never been tested for ethanol consumption. Male and female mice (A/J, BALB/cByJ, BTBR+T tf/tf , BUB/ BnJ, C57BL/6J, C57BLKS/J, C58/J, CZECH/Ei, DBA/2J, FVB/NJ, I/LnJ, LP/J, MA/MyJ, NOD/ LtJ, NON/LtJ, NZB/B1NJ, NZW/LacJ, PERA/Ei, RIIIS/J, SEA/GnJ, SM/J, and 129S1/SvlmJ) were individually housed and given unlimited access in a two-bottle choice procedure to one bottle containing tap water and a second containing increasing concentrations of ethanol (3%, 6%, 10%), 0.2% saccharin, and then increasing concentrations of ethanol (3%, 6%, 10%) plus 0.2% saccharin. Mice were given access to each novel solution for a total of 4 days, with a bottle side change every other day. Consistent with previous studies, C57BL/6J (B6) mice consumed an ethanol dose of > 10g/kg/day while DBA/2J (D2) mice consumed < 2g/kg/day. No strain voluntarily consumed greater doses of ethanol than B6 mice. While the C58 and C57BLKS strains showed high ethanol consumption levels that were comparable to B6 mice, the BUB and BTBR strains exhibited low ethanol intakes similar to D2 mice. The addition of 0.2% saccharin to the ethanol solutions significantly increased ethanol intake by most strains and altered the strain distribution pattern. Strong positive correlations (rs ≥ 0.83) were determined between consumption of the unsweetened versus sweetened ethanol solutions. Consumption of saccharin alone was significantly positively correlated with the sweetened ethanol solutions (rs = 0.62 -0.81), but the correlation with unsweetened ethanol solutions was considerably lower (rs = 0.37 -0.45). These results add new strains to the strain mean database that will facilitate the identification of genetic relationships between voluntary ethanol consumption, saccharin preference, and other phenotypes.

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Section: Discussionsupporting

confidence: 82%

Voluntary ethanol consumption in 22 inbred mouse strains

Yoneyama

Crabbe

Ford

et al. 2008

Alcohol

273

269

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“…Nevertheless, increased vulnerability to EtOH-induced neurotoxicity in females remains controversial [reviewed in (51)] with additional studies needed to support or refute this hypothesis. This finding is buttressed by the observation that chronic ethanol exposure is associated with a strongly sexually dimorphic transcriptional response (44,118,119). In those studies, significantly regulated transcripts included several genes that are exclusively or predominantly expressed in astrocytes, suggesting that a component of the neuroadapative response in the brain after ethanol exposure reflects changes in astrocyte gene expression that are distinct between males and females.…”

Section: Introductionmentioning

confidence: 73%

“…Females have higher rates or greater severity of cardiomyopathy, peripheral neuropathy, some types of cancer and liver cirrhosis (5,59). Increased vulnerability to ethanol-induced brain damage in the prefrontal cortex in females has been observed in some studies (44,118). Other studies have not confirmed female vulnerability, but have noted different "brain morphological deficits" between males and females supporting the notion that neurodamage occurs via different mechanisms depending on sex (94).…”

Section: Introductionmentioning

confidence: 92%

“…We have recently shown that following chronic intoxication in vivo, females exhibit a pro-inflammatory response in the medial prefrontal cortex that includes increased Tnf expression, while males show a pattern consistent with immune suppression (118,119). Associated with this pro-inflammatory tone, females also exhibit increased neurotoxicity (44,118). Combined, our studies suggest the possibility that sexually dimorphic ethanol-induced neurotoxicity in the frontal cortex may be mediated in part by astrocytes both via induction and modulation of inflammatory signaling and through changes in astrocyte function including dysregulation of glutamate homeostasis.…”

Section: Introductionmentioning

confidence: 93%

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Astrocyte Dysfunction Induced by Alcohol in Females but Not Males

et al. 2015

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Chronic alcohol abuse is associated with brain damage in a sex-specific fashion, but the mechanisms involved are poorly described and remain controversial. Previous results have suggested that astrocyte gene expression is influenced by ethanol intoxication and during abstinence in vivo. Here, bioinformatic analysis of astrocyte-enriched ethanol-regulated genes in vivo revealed ubiquitin pathways as an ethanol target, but with sexually dimorphic cytokine signaling and changes associated with brain aging in females and not males. Consistent with this result, astrocyte activation was observed after exposure in female but not male animals, with reduced S100β levels in the anterior cingulate cortex and increased GFAP(+) cells in the hippocampus. In primary culture, the direct effects of chronic ethanol exposure followed by recovery on sex-specific astrocyte function were examined. Male astrocyte responses were consistent with astrocyte deactivation with reduced GFAP expression during ethanol exposure. In contrast, female astrocytes exhibited increased expression of Tnf, reduced expression of the neuroprotective cytokine Tgfb1, disrupted bioenergetics and reduced excitatory amino acid uptake following exposure or recovery. These results indicate widespread astrocyte dysfunction in ethanol-exposed females and suggest a mechanism that may underlie increased vulnerability to ethanol-induced neurotoxicity in females.

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“…However, the effect of sex was revealed in a recent study on gene expression in male and female rodent brains after 72 h exposure to ethanol vapours followed by 8 h withdrawal (49) .…”

Section: Sex-specific Action Of Alcoholmentioning

confidence: 99%

The effect of alcohol and nicotine abuse on gene expression in the brain

Flatscher-Bader

Wilce

2009

Nutr. Res. Rev.

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Alcohol intake at levels posing an acute heath risk is common amongst teenagers. Alcohol abuse is the second most common mental disorder worldwide. The incidence of smoking is decreasing in the Western world but increasing in developing countries and is the leading cause of preventable death worldwide. Considering the longstanding history of alcohol and tobacco consumption in human societies, it might be surprising that the molecular mechanisms underlying alcohol and smoking dependence are still incompletely understood. Effective treatments against the risk of relapse are lacking. Drugs of abuse exert their effect manipulating the dopaminergic mesocorticolimbic system. In this brain region, alcohol has many potential targets including membranes and several ion channels, while other drugs, for example nicotine, act via specific receptors or binding proteins. Repeated consumption of drugs of abuse mediates adaptive changes within this region, resulting in addiction. The high incidence of alcohol and nicotine co-abuse complicates analysis of the molecular basis of the disease. Gene expression profiling is a useful approach to explore novel drug targets in the brain. Several groups have utilised this technology to reveal drug-sensitive pathways in the mesocorticolimbic system of animal models and in human subjects. These studies are the focus of the present review.

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Neurotoxic Consequences of Chronic Alcohol Withdrawal: Expression Profiling Reveals Importance of Gender Over Withdrawal Severity

Cited by 67 publications

References 72 publications

Voluntary ethanol consumption in 22 inbred mouse strains

Voluntary ethanol consumption in 22 inbred mouse strains

Astrocyte Dysfunction Induced by Alcohol in Females but Not Males

The effect of alcohol and nicotine abuse on gene expression in the brain

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