DNA methylation as a predictor of fetal alcohol spectrum disorder

Lussier, Alexandre A.; Morin, Alexander M.; MacIsaac, Julia L.; Salmon, Jenny; Weinberg, Joanne; Reynolds, James N.; Pavlidis, Paul; Chudley, Albert E.; Kobor, Michæl S.

doi:10.1186/s13148-018-0439-6

Cited by 92 publications

(89 citation statements)

References 75 publications

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“…The few studies that have measured cardiac function in FASD animal models support the hypothesis that CHDs arising from ethanol exposure could have a significant contribution from abnormal function [26]. Abnormal embryonic cardiac function (as well as abnormal valves) was identified through ultrasound and histology, respectively at late stages (embryonic day 15.5) [italics researchers] of mouse development after ethanol exposure at gastrulation [27,28]. Functional and structural defects, including anomalies in heart volume/ morphology and conduction, were observed in latestage zebrafish after ethanol exposure, thus mimicking malformations occurring in patients with FASD [29].…”

Section: Congenital Heart Defects and Fetal Alcohol Spectrum Disordermentioning

confidence: 99%

“…As interventions may have the greatest impact at an early age, Salmon postulates that accurate biomarkers are needed to identify children at risk for FASD. Consequently, DNA methylation signature is being used to develop a possible epigenetic predictor of FASD [10,27]. However, despite the fact that alcohol was identified as a teratogen many decades ago, recent data indicate that in the US over 500,000 women per year report drinking during pregnancy with one in five of this population admitting to binge drinking [27].…”

Section: Discussionmentioning

confidence: 99%

“…Consequently, DNA methylation signature is being used to develop a possible epigenetic predictor of FASD [10,27]. However, despite the fact that alcohol was identified as a teratogen many decades ago, recent data indicate that in the US over 500,000 women per year report drinking during pregnancy with one in five of this population admitting to binge drinking [27]. Salmon also reports binge drinking by many of the women in her NZ study, some of whom were not aware that they were pregnant at the time [10].…”

Section: Discussionmentioning

confidence: 99%

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Fetal Alcohol Spectrum Disorder: Risk for Diabetes and Congenital Heart Defects

Salmon

2018

IDCD

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Excessive use of alcohol can be a cause for many disease and injury conditions. These include amongst many others, myocardial infarction, diabetes mellitus, atrial fibrillation, nonischaemic cardiomyopathy, fetal alcohol spectrum disorder (FASD), congenital heart defects (CHD) and liver cirrhosis. Even low levels of prenatal alcohol (ethanol) exposure, such as in a single dose, can produce birth defects termed fetal alcohol syndrome (FAS) which is the highest marker on the spectrum. Diabetes is regarded as a major cause of cardiovascular disease whilst prenatal alcohol exposure (PAE) can range from no observable adverse effects to mortality. CHD are stated to be the most prevalent cause of mortality in individuals with FASD. The dimension of the problems is still greatest in the Western world although it is stated to be the leading cause of mental retardation in North America.FASD is a neurodevelopmental disability which can be occasioned when a pregnant woman consumes alcohol. The diagnostic criteria for FASD includes growth impairment, abnormal facial features and neurocognitive impairments. The most frequently reported abnormal facial features in FASD are thin upper lip, indistinct or smooth philtrum and short palpebral fissure length. Other features are microganthia, low set ears, ptosis, absent or indistinct philtral ridge, epicanthal folds, cleft palate, flat nasal bridge and midface hypoplasia. The neurocognitive features commonly reported in FASD are microcephaly, intellectual disability, attention-deficit hyperactivity disorder (ADHD) and behavioural impairments. Central nervous system (CNS) injury is also seen and is debilitating. Structural abnormalities of the CNS can include microcephaly, agenesis/absence of the corpus callosum and multiple severe brain malformations. This review article seeks to address the association of FASD with diabetes and CHD.

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Section: Congenital Heart Defects and Fetal Alcohol Spectrum Disordermentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Fetal Alcohol Spectrum Disorder: Risk for Diabetes and Congenital Heart Defects

Salmon

2018

IDCD

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“…Methylome changes have also been observed in individuals with FASD (Krishnamoorthy et al, ; Portales‐Casamar et al, ). These alterations in DNA methylation are being characterized as possible biomarkers to diagnose FASD (Legault, Bertrand‐Lehouillier, & McGraw, ; Lussier et al, ; Portales‐Casamar et al, ).…”

Section: The Etiology Of Fasdmentioning

confidence: 99%

“…As folate is the main methyl group donor in the cell, this ethanol-induced reduction could affect many methylation reactions (Salbaum & Kappen, 2012). To date, there is no mechanism, biochemical, molecular or enzymatic that could explain this reduction in folate, although ethanol has been shown to also induce changes in the transport of folate (Legault, Bertrand-Lehouillier, & McGraw, 2018;Lussier et al, 2018;Portales-Casamar et al, 2016).…”

Section: Epigenetic Changesmentioning

confidence: 99%

Insights into retinoic acid deficiency and the induction of craniofacial malformations and microcephaly in fetal alcohol spectrum disorder

Petrelli

Bendelac

Hicks

et al. 2019

Genesis

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Summary Fetal Alcohol Spectrum Disorder (FASD) is a set of neurodevelopmental malformations caused by maternal consumption of alcohol during pregnancy. FASD sentinel facial features are unique to the disorder, and microcephaly is common in severe forms of FASD. Retinoic acid deficiency has been shown to cause craniofacial malformations and microcephaly in animal models reminiscent of those caused by prenatal alcohol exposure. Alcohol exposure affects the migration and survival of cranial neural crest cells, which are required for proper frontonasal prominence and pharyngeal arch development. Defects in craniofacial development are further amplified by the many downstream pathways that are transcriptionally controlled retinoic acid target genes, including Shh signaling. Recent evidence shows that alcohol exposure itself is sufficient to induce retinoic acid deficiency in the embryo. These data suggest that retinoic acid deficiency is an important underlying etiology of FASD. In disorders like Vitamin A Deficiency, FASD, DiGeorge (22q11.2 Deletion Syndrome), CHARGE, Smith‐Magenis, Matthew‐Wood, and Congenital Zika Syndromes, evidence is accumulating to link reduced retinoic acid signaling with developmental defects like craniofacial malformations and microcephaly. Research focus on characterizing the effects of retinoic acid deficiency during early development and on understanding the downstream signaling pathways involved in aberrant head, and craniofacial development will reveal underlying etiologies of these disorders.

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The association between prenatal alcohol exposure and protein expression in human placenta

Holbrook

Davies

Cano

et al. 2019

Birth Defects Research

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Background. The need for earlier recognition of children at risk for neurobehavioral problems associated with prenatal ethanol exposure (PAE) has prompted investigations of biomarkers prognostic for altered fetal development. Here, we examined whether PAE alters the expression of these proteins in human placenta, along with other angiogenesis-related proteins and cytokines in subjects selected from an ENRICH prospective cohort. Methods. PAE was ascertained by screening questionnaires, Time-line Follow-back interviews and a panel of ethanol biomarkers at two study visits. After delivery, placental tissue samples were collected for protein analysis. Results. No significant differences in the prevalence of substance use, demographic or medical characteristics were observed between the No PAE and PAE groups. PAE was associated with significant reductions in placental expression of VEGFR2 and Annexin-A4, while the levels of VEGFR1 and CCM-3 trended downward. A trend towards higher expression of the cytokines TNF-α and IL-13 was also observed in the PAE group. ROC analyses of the data demonstrated a moderate-to-high degree of diagnostic accuracy for individual placental proteins. Combinations of proteins substantially increased their ability to differentiate between PAE and No PAE subjects. Conclusions. These results establish the feasibility of harvesting placental tissue for protein analyses of PAE in a prospective manner. In addition, given the importance of vascular remodeling in both placenta and developing brain, the role of angiogenic and cytokine proteins in this process warrants further investigation for their utility for predicting alterations in brain development, as well as their mechanistic role in PAE-induced pathology.

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DNA methylation as a predictor of fetal alcohol spectrum disorder

Cited by 92 publications

References 75 publications

Fetal Alcohol Spectrum Disorder: Risk for Diabetes and Congenital Heart Defects

Fetal Alcohol Spectrum Disorder: Risk for Diabetes and Congenital Heart Defects

Insights into retinoic acid deficiency and the induction of craniofacial malformations and microcephaly in fetal alcohol spectrum disorder

The association between prenatal alcohol exposure and protein expression in human placenta

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