Fetal Alcohol Exposure and Temporal Vulnerability: Regional Differences in Alcohol‐Induced Microencephaly as a Function of the Timing of Binge‐Like Alcohol Exposure During Rat Brain Development

Maier, Susan E.; Chen, Wei‐Jung A.; Miller, Jennifer A.; West, John C

doi:10.1111/j.1530-0277.1997.tb04471.x

Cited by 93 publications

(73 citation statements)

References 41 publications

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“…During the study period, men accounted for 81% of all binge-drinking episodes (Table 1), and they were approximately 3 times as likely as women to report binge drinking (eg, 22 …”

Section: Resultsmentioning

confidence: 99%

Binge Drinking Among US Adults

Naimi

Brewer

Mokdad

et al. 2003

JAMA

858

611

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Context Binge drinking (consuming Ն5 alcoholic drinks on 1 occasion) generally results in acute impairment and has numerous adverse health consequences. Reports indicate that binge drinking may be increasing in the United States.Objectives To quantify episodes of binge drinking among US adults in 1993-2001, to characterize adults who engage in binge drinking, and to describe state and regional differences in binge drinking. Design, Setting, and ParticipantsThe Behavioral Risk Factor Surveillance System, a random-digit telephone survey of adults aged 18 years or older that is conducted annually in all states. The sample size ranged from 102263 in 1993 to 212510 in 2001.Main Outcome Measures Binge-drinking prevalence, episodes, and episodes per person per year.Results Between 1993 and 2001, the total number of binge-drinking episodes among US adults increased from approximately 1.2 billion to 1.5 billion; during this time, bingedrinking episodes per person per year increased by 17% (from 6.3 to 7.4, P for trend=.03). Between 1995 and 2001, binge-drinking episodes per person per year increased by 35% (P for trend=.005). Men accounted for 81% of binge-drinking episodes in the study years. Although rates of binge-drinking episodes were highest among those aged 18 to 25 years, 69% of binge-drinking episodes during the study period occurred among those aged 26 years or older. Overall, 47% of binge-drinking episodes occurred among otherwise moderate (ie, non-heavy) drinkers, and 73% of all binge drinkers were moderate drinkers. Binge drinkers were 14 times more likely to drive while impaired by alcohol compared with non-binge drinkers. There were substantial state and regional differences in per capita binge-drinking episodes.Conclusions Binge drinking is common among most strata of US adults, including among those aged 26 years or older. Per capita binge-drinking episodes have increased, particularly since 1995. Binge drinking is strongly associated with alcoholimpaired driving. Effective interventions to prevent the mortality and morbidity associated with binge drinking should be widely adopted, including screening patients for alcohol abuse in accordance with national guidelines.

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“…During the study period, men accounted for 81% of all binge-drinking episodes (Table 1), and they were approximately 3 times as likely as women to report binge drinking (eg, 22 …”

Section: Resultsmentioning

confidence: 99%

Binge Drinking Among US Adults

Naimi

Brewer

Mokdad

et al. 2003

JAMA

858

611

View full text Add to dashboard Cite

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“…This concentration, while slightly greater then those associated with impaired mental capabilities and coordination (10 mM) or ataxia (20 mM) in humans is within the physiological relevant range. That is, this ethanol concentration, is similar to, or less, then the blood alcohol levels achieved in animal models of binge-like alcohol exposure [Thomas et al, 1996;Maier et al, 1997;Goodlett et al, 1997]. Further, studies in drinking women have reported blood alcohol concentrations above 50 mM [Urso et al, 1981;Church and Gerkin, 1988;Hammond et al, 1973;Wells and Barhill, 1996], including a report of one women with a blood alcohol level of approximately 330 mM (1.5%) [Johnson et al, 1982].…”

Section: Discussionmentioning

confidence: 78%

Ethanol inhibits prolactin-induced activation of the JAK/STAT pathway in cultured astrocytes

DeVito

Stone

1999

J. Cell. Biochem.

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Alcohol consumption has multiple effects in the central nervous system (CNS). Whereas, alcohol is an immunosuppressive drug the effect of alcohol on the neuroimmune system, remains unclear. In cultured astrocytes, prolactin (PRL) induces mitogenesis and the expression of inflammatory cytokines, including tumor necrosis factor-alpha (TNF alpha). We have recently shown that whereas ethanol does not inhibit PRL receptor binding, it markedly inhibits PRL-induced mitogenesis and TNF alpha secretion in cultured astrocytes. It is clear that PRL activates the tyrosine phosphorylation of several proteins, including members of a novel family of protein tyrosine kinases, the Janus Kinases (JAKs). The aims of this study were to characterize PRL-induced activation of the JAK/STAT (signal transducers and activators of transcription) pathway, and to determine if ethanol affects JAK/STAT activation in cultured astrocytes. We found that PRL specifically increases the tyrosine phosphorylation of JAK2, but not JAK1, JAK3, or Tyk2, and the subsequent phosphorylation of STAT1 alpha, STAT5a, and STAT5b. Preincubation of astrocytes with ethanol markedly inhibited phosphorylation of JAK2, STAT1 alpha, STAT5a, and STAT5b. In PRL-stimulated astrocytes, ethanol inhibited binding of nuclear proteins to oligonucleotides corresponding to the gamma-interferon activated sequence (GAS). Further, ethanol blocked PRL-induced increases in interferon regulatory factor-1 (IRF-1) mRNA, a PRL/cytokine inducible transcription factor involved in the regulation of a number of cytokine inducible genes. The inhibition of tyrosine phosphorylation by ethanol was not a general effect, however, as we found that ethanol increased basal and NGF-induced tyrosine phosphorylation of extracellular signal-activated protein kinase-1 (ERK-1). These data indicate that ethanol inhibits PRL-induced tyrosine phosphorylation of the JAK/STAT pathway resulting in decreased nuclear GAS DNA binding and inhibition of the PRL inducible gene, IRF-1. Thus, suggesting that ethanol-induced inhibition of JAK2 phosphorylation may be one mechanism though which ethanol could after the brain's response to injury or infection.

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“…CONSEQUENCES OF PRENATAL TOBACCO AND NICOTINE EXPOSURE 7 (Probyn et al, 2012). Furthermore, the head and brain are not spared from the effects of prenatal ethanol exposure, with reduced head size reported in both humans (Day et al, 1989;Elliott et al, 2008;Feldman et al, 2012) and animal models (Maier et al, 1997;Kaminen-Ahola et al, 2010b).…”

Section: Evidence In Animal Modelsmentioning

confidence: 99%

A study of the consequences of early gestational ethanol and/or nicotine exposure in the mouse

Yamada¹

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The in utero environment is a critical determinant of the immediate and future health of the developing fetus. In Australia, two of the most commonly used drugs during pregnancy are alcohol and nicotine. Prolonged periods of gestational exposure to alcohol and nicotine, separately, have been associated with a range of adverse outcomes in the offspring, in both humans and experimental animal models. The consequences of ethanol and nicotine exposure restricted to early gestation on resultant offspring are poorly characterised, and few animal models exist to build greater understanding. Moreover, the immediate molecular changes associated with exposures to ethanol and/or nicotine restricted to early gestation has yet to be described.This thesis utilised mouse models of early gestational ethanol and/or nicotine exposure to explore the impact of each of these exposures on offspring growth, as well as their associated transcriptional and epigenetic changes. In each model, pregnant C57BL/6 dams were provided with ad libitum access to solutions of 10% ethanol and/or 100 µg/ml nicotine from fertilisation (0.5 dpc) to midgestation (8.5 dpc). The exposure window utilised in each of the models is developmentally equivalent to the first three to four weeks of a human pregnancy.Previously, our laboratory identified reduced growth, microcephaly, and gene expression changes in the liver and hippocampus of the postnatal offspring of the model of prenatal ethanol exposure utilised in this thesis. In contrast, at mid-gestation (9.5 dpc), there was no evidence of developmental delay (somite number), reduced growth (crown-rump length), or microcephaly.Further, a genome-wide gene expression microarray (targeting 30 855 genes) and a screen of the expression of 641 microRNAs, identified only one gene (Bcl11b) as differentially expressed in male 9.5 dpc whole embryos following the ethanol exposure. These data suggest that there is a delay between the ethanol exposure and the onset of adverse phenotypes -arguing that the embryo is somehow able to form a memory of the ethanol exposure. The absence of widespread transcriptional changes suggests that changes in embryonic mRNA and microRNA expression are unlikely to be major contributors to the memory of the exposure.A early gestational model of nicotine exposure was newly established in this thesis. This nicotine exposure resulted in an average serum cotinine (metabolite of nicotine) concentration similar to that reported in humans who smoke 10 to 15 cigarettes per day. This exposure was sufficient to induce a reduction in body size both at mid-gestation and postnatally, but not at late gestation. Furthermore, the increased expression of Zscan10 in the whole male 9.5 dpc embryo was identified and validated across multiple cohorts. Zscan10 encodes for a transcription factor expressed throughout development, with a proposed role in the regulation of progenitor cells. The increased expression of Zscan10 in the nicotine-exposed embryos was associated with a reduction in DNA methylation ...

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Fetal Alcohol Exposure and Temporal Vulnerability: Regional Differences in Alcohol‐Induced Microencephaly as a Function of the Timing of Binge‐Like Alcohol Exposure During Rat Brain Development

Cited by 93 publications

References 41 publications

Binge Drinking Among US Adults

Binge Drinking Among US Adults

Ethanol inhibits prolactin-induced activation of the JAK/STAT pathway in cultured astrocytes

A study of the consequences of early gestational ethanol and/or nicotine exposure in the mouse

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