The Genetics of Fetal Alcohol Spectrum Disorders

Eberhart, Johann K.; Parnell, Scott E.

doi:10.1111/acer.13066

Cited by 96 publications

(96 citation statements)

References 137 publications

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“…Only a handful of gene-ethanol interactions have been identified to date. A detailed discussion of these interactions can be found elsewhere, 87,88 whereas here, we focus on findings in zebrafish. The many genetic tools available in zebrafish have proven successful in expanding our understanding of developmental biology.…”

Section: Identifying Gene-ethanol Interactions: the Way Of The Fishmentioning

confidence: 99%

Fishing for Fetal Alcohol Spectrum Disorders: Zebrafish as a Model for Ethanol Teratogenesis

2016

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Fetal Alcohol Spectrum Disorders (FASD) describes a wide array of ethanol-induced developmental defects, including craniofacial dysmorphology and cognitive impairments. It affects *1 in 100 children born in the United States each year. Due to the pleiotropic effects of ethanol, animal models have proven critical in characterizing the mechanisms of ethanol teratogenesis. In this review, we focus on the utility of zebrafish in characterizing ethanolinduced developmental defects. A growing number of laboratories have focused on using zebrafish to examine ethanol-induced defects in craniofacial, cardiac, ocular, and neural development, as well as cognitive and behavioral impairments. Growing evidence supports that genetic predisposition plays a role in these ethanol-induced defects, yet little is understood about these gene-ethanol interactions. With a high degree of genetic amenability, zebrafish is at the forefront of identifying and characterizing the gene-ethanol interactions that underlie FASD.

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Section: Identifying Gene-ethanol Interactions: the Way Of The Fishmentioning

confidence: 99%

Fishing for Fetal Alcohol Spectrum Disorders: Zebrafish as a Model for Ethanol Teratogenesis

2016

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“…Many of the hallmark phenotypes of FASD are also produced with disruption of gene function in zebrafish (Eberhart et al, 2016). Relevant to these studies, our previous work showed agrin morphants displayed similar ocular defects to those induced by ethanol exposure, suggesting agrin as a target of prenatal ethanol exposure (Zhang et al, 2011).…”

Section: Discussionmentioning

confidence: 99%

Comparison of molecular marker expression in early zebrafish brain development following chronic ethanol or morpholino treatment

2017

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This study was undertaken to ascertain whether defined markers of early zebrafish brain development are affected by chronic ethanol exposure or morpholino knockdown of agrin, sonic hedgehog, retinoic acid and fibroblast growth factors, four signaling molecules that are suggested to be ethanol sensitive. Zebrafish embryos were exposed to 2% ethanol from 6–24 hpf or injected with agrin, shha, aldh1a3 or fgf8a morpholinos. In situ hybridization was employed to analyze otx2, pax6a, epha4a, krx20, pax2a, fgf8a, wnt1 and eng2b expression during early brain development. Our results showed that pax6a mRNA expression was decreased in eye, forebrain and hindbrain of both chronic ethanol exposed and select MO treatments. Epha4a expression in rhombomere R1 boundary was decreased in chronic ethanol exposure and aldh1a3 morphants, lost in fgf8a morphants, but largely unaffected in agrin and shha morphants. Ectopic pax6a and epha4a expression in midbrain was only found in fgf8a morphants. These results suggest that while chronic ethanol induces obvious morphological change in brain architecture, many molecular markers of these brain structures are relatively unaffected by ethanol exposure.

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“…Among the proposed models in this group are: alteration of the normal DNA methylation pattern and other epigenetic changes at the level of chromatin modifications, aberrant cell death (apoptosis), changes in growth and signaling factor expression (including IGF, EGF, and Shh), changes in cell adhesion, cytoskeleton and migration, abnormal inflammatory responses, changes in cholesterol homeostasis, deficient neurotransmitter signaling (choline), and changes in miRNA expression. The different models to explain FASD have been reviewed in a number of instances over the years (Caputo, Wood, & Jabbour, ; Chater‐Diehl, Laufer, & Singh, ; Eberhart & Parnell, ; Ehrhart et al, ; Gilbert‐Barness, ; Gupta, Gupta, & Shirasaka, ; Kalisch‐Smith & Moritz, ; Kane & Drew, ; Lunde et al, ; Lussier, Weinberg, & Kobor, ; Mandal, Halder, Jung, & Chai, ; Shabtai & Fainsod, ; Shenoda, ; Wells, Bhatia, Drake, & Miller‐Pinsler, ). In this review, we will focus on the reduction of retinoic acid signaling by alcohol exposure during early development and briefly summarize a few of the other related changes.…”

Section: The Etiology Of Fasdmentioning

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 Genetics of Fetal Alcohol Spectrum Disorders

Cited by 96 publications

References 137 publications

Fishing for Fetal Alcohol Spectrum Disorders: Zebrafish as a Model for Ethanol Teratogenesis

Fishing for Fetal Alcohol Spectrum Disorders: Zebrafish as a Model for Ethanol Teratogenesis

Comparison of molecular marker expression in early zebrafish brain development following chronic ethanol or morpholino treatment

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

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