Effects of all three trimester moderate binge alcohol exposure on the foetal hippocampal formation and olfactory bulb

Washburn, Shannon E.; Ramadoss, Jayanth; Chen, Wei‐Jung A.; Cudd, Timothy A.

doi:10.3109/02699052.2014.947629

Cited by 8 publications

(8 citation statements)

References 40 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Determining prenatal alcohol exposure is crucial to identify the children/population at risk, but it is not realistic to assess all infants with prenatal alcohol exposure. First, a “safe” dose of alcohol is controversial and highly debated [ 16 , 33 ]; second, patterns of alcohol consumption differ (chronic/acute) and their effect on the fetus is not the same [ 10 ]; and third, the developing brain has windows of vulnerability during which potential harm is greater [ 25 , 49 ]. These limits also contribute to the discrepancies between different cohort studies on the impact of alcohol consumption on the infant [ 26 , 31 , 45 ].…”

Section: Discussionmentioning

confidence: 99%

PLGF, a placental marker of fetal brain defects after in utero alcohol exposure

Lecuyer

Laquerrière

Bekri

et al. 2017

acta neuropathol commun

View full text Add to dashboard Cite

Most children with in utero alcohol exposure do not exhibit all features of fetal alcohol syndrome (FAS), and a challenge for clinicians is to make an early diagnosis of fetal alcohol spectrum disorders (FASD) to avoid lost opportunities for care. In brain, correct neurodevelopment requires proper angiogenesis. Since alcohol alters brain angiogenesis and the placenta is a major source of angiogenic factors, we hypothesized that it is involved in alcohol-induced brain vascular defects. In mouse, using in vivo repression and overexpression of PLGF, we investigated the contribution of placenta on fetal brain angiogenesis. In human, we performed a comparative molecular and morphological analysis of brain/placenta angiogenesis in alcohol-exposed fetuses. Results showed that prenatal alcohol exposure impairs placental angiogenesis, reduces PLGF levels and consequently alters fetal brain vasculature. Placental repression of PLGF altered brain VEGF-R1 expression and mimicked alcohol-induced vascular defects in the cortex. Over-expression of placental PGF rescued alcohol effects on fetal brain vessels. In human, alcohol exposure disrupted both placental and brain angiogenesis. PLGF expression was strongly decreased and angiogenesis defects observed in the fetal brain markedly correlated with placental vascular impairments. Placental PGF disruption impairs brain angiogenesis and likely predicts brain disabilities after in utero alcohol exposure. PLGF assay at birth could contribute to the early diagnosis of FASD.Electronic supplementary materialThe online version of this article (doi:10.1186/s40478-017-0444-6) contains supplementary material, which is available to authorized users.

show abstract

Section: Discussionmentioning

confidence: 99%

PLGF, a placental marker of fetal brain defects after in utero alcohol exposure

Lecuyer

Laquerrière

Bekri

et al. 2017

acta neuropathol commun

View full text Add to dashboard Cite

show abstract

“…Alcohol-related fetal and pregnancy outcomes and the severity thereof can vary depending on the timing of exposure; that is, effects linked with first trimester exposure [83] may be different from those associated with the second [84-86] or third trimester [87,88], and these in turn may differ from outcomes due to persistent use throughout the duration of pregnancy [89]. For example, alcohol consumption has been associated with oral clefts [83] during the first-trimester [83], adverse effects on rat brain weight during the second [84], and disruptions in rat neuroimmune systems [88].…”

Section: Alcoholmentioning

confidence: 99%

Substance Use in the Perinatal Period

Forray

Foster

2015

Curr Psychiatry Rep

121

View full text Add to dashboard Cite

Perinatal substance use remains a major public health problem and is associated with a number of deleterious maternal and fetal effects. Polysubstance use in pregnancy is common, and can potentiate adverse maternal and fetal outcomes. Tobacco is the most commonly used substance in pregnancy, followed by alcohol and illicit substances. The treatments for perinatal substance use are limited and consist mostly of behavioral and psychosocial interventions. Of these contingency management has shown the most efficacy. More recently, novel interventions such as progesterone for postpartum cocaine use have shown promise. The purpose of this review is to examine the recent literature on the use of tobacco, alcohol, cannabis, stimulants, and opioids in the perinatal period, their effects on maternal and fetal health and current treatments.

show abstract

“…Cudd and colleagues have further demonstrated changes in molecular pathways associated with the development of mental illness. Utilising the Suffolk sheep model, they treated dams with 1.75 g/kg ethanol intravenously, resulting in a BAL of 189 ± 19 mg/ dL, and demonstrated changes within offspring hippocampus including density and volume of dentate gyrus granular cells and cerebellar Purkinje cell loss 152,153 . This group also observed significant changes to the HPA axis within the foetus, including increased circulating cortisol and adrenocorticotropic hormone 154 .…”

Section: Pathways Underlying Mental Health Outcomesmentioning

confidence: 99%

Prenatal alcohol exposure and developmental programming of mental illness

Burgess

2020

J Dev Orig Health Dis

View full text Add to dashboard Cite

It is well established that high-dose alcohol consumption during pregnancy increases the risk for a plethora of adverse offspring outcomes. These include neurodevelopmental, cognitive and social deficits, as well as psychiatric illnesses, such as depression and anxiety. However, much less evidence is available on the effects of low- and early-dose alcohol exposure on mental health outcomes, regardless of the accumulating evidence that mental health outcomes should be considered in the context of the Developmental Origins of Health and Disease hypothesis. This review will discuss the evidence that indicates low-dose and early prenatal alcohol exposure can increase the risk of mental illness in offspring and discuss the mechanistic pathways that may be involved.

show abstract

Effects of all three trimester moderate binge alcohol exposure on the foetal hippocampal formation and olfactory bulb

Cited by 8 publications

References 40 publications

PLGF, a placental marker of fetal brain defects after in utero alcohol exposure

PLGF, a placental marker of fetal brain defects after in utero alcohol exposure

Substance Use in the Perinatal Period

Prenatal alcohol exposure and developmental programming of mental illness

Contact Info

Product

Resources

About