Abstract

Alcohol is a potent neurotoxicant and prenatal alcohol exposure is a leading cause of mental disability. One affected population is the neural crest. Clinically relevant ethanoi levels (20-80 mM) cause neural crest (NC) apoptosis. Our past work under this award showed that the apoptosis results from an ethanol-stimulated intracellular calcium (Ca2+) transient originating from the CPy-mediated activation of PLC-IP3. The current award shows that the Ca2+ transient activates CaMKII, which in turn destabilizes the transcriptional effector beta-catenin, which mediates canonical Wnt signaling and NC survival. Proposed studies directly extend this work to ask How does beta-catenin loss cause neural crest apoptosis? We will test the hypothesis that beta- catenin maintains NC cell adhesion and expression ofthe survival factor snail2 (formerly slug). We further posit that the ethanol-mediated loss of beta-catenin initiates premature NC cell delamination and suppresses snail2, thus activating NC apoptosis.
Aim 1 tests whether snail2 loss directly initiates NC apoptosis because it controls the expression ofthe apoptosis regulators bcl2 and bax.
Aim 2 tests the role of beta-catenin in NC cell adhesion and whether beta-catenin loss stimulates precocious NC delamination and apoptosis.
Aim 3 extends our work to test if acute ethanoi exposure similarly destabilizes beta-catenin and its transcriptional activity in other neuronal populations in which p-catenin controls cell fate, specifically the fetal brain and adult hippocampus. Finally, our ARRA supplement performs high-throughput RNA-Seq of ethanol-sensitive and - resistant NC to identify calcium-dependent factors upstream of beta-catenin that govern NC survival.
Aim 4 tests the efficacy of these candidate genes in controlling NC responses to ethanoi. This work is a logical extension ofthe current award. We continue using our established chick embryo model, which replicates the alcohol responses of mammals including humans, has well-described NC development, and is amenable to genetic manipulation. Beta-Catenin dysregulation contributes to several neuropathologies, suggesting it may also modulate alcohol action in the fetus and the adult.

Public Health Relevance

Fetal alcohol spectrum disorders (FASD) are a major cause of cognitive and behavioral disability in children. How ethanoi damages the embryo and fetus is incompletely understood. Because it is difficult to prevent gestational alcohol abuse, there is increased interest in strategies to blunt ethanol's damage. Identification of its toxicity mechanism suggests targets for intervention, i.e. pharmacological agents that stabilize beta-catenin.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
4R37AA011085-20
Application #
9040771
Study Section
Special Emphasis Panel (NSS)
Program Officer
Hereld, Dale
Project Start
1996-07-01
Project End
2017-03-31
Budget Start
2016-04-01
Budget End
2017-03-31
Support Year
20
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Nutrition
Type
Earth Sciences/Resources
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Helfrich, Kaylee K; Saini, Nipun; Kling, Pamela J et al. (2018) Maternal iron nutriture as a critical modulator of fetal alcohol spectrum disorder risk in alcohol-exposed pregnancies. Biochem Cell Biol 96:204-212
Flentke, George R; Smith, Susan M (2018) The avian embryo as a model for fetal alcohol spectrum disorder. Biochem Cell Biol 96:98-106
Huebner, Shane M; Helfrich, Kaylee K; Saini, Nipun et al. (2018) Dietary Iron Fortification Normalizes Fetal Hematology, Hepcidin, and Iron Distribution in a Rat Model of Prenatal Alcohol Exposure. Alcohol Clin Exp Res 42:1022-1033
Berres, Mark E; Garic, Ana; Flentke, George R et al. (2017) Transcriptome Profiling Identifies Ribosome Biogenesis as a Target of Alcohol Teratogenicity and Vulnerability during Early Embryogenesis. PLoS One 12:e0169351
Huebner, Shane M; Blohowiak, Sharon E; Kling, Pamela J et al. (2016) Prenatal Alcohol Exposure Alters Fetal Iron Distribution and Elevates Hepatic Hepcidin in a Rat Model of Fetal Alcohol Spectrum Disorders. J Nutr 146:1180-8
Amos-Kroohs, Robyn M; Fink, Birgit A; Smith, Carol J et al. (2016) Abnormal Eating Behaviors Are Common in Children with Fetal Alcohol Spectrum Disorder. J Pediatr 169:194-200.e1
Huebner, Shane M; Tran, Tuan D; Rufer, Echoleah S et al. (2015) Maternal iron deficiency worsens the associative learning deficits and hippocampal and cerebellar losses in a rat model of fetal alcohol spectrum disorders. Alcohol Clin Exp Res 39:2097-107
Smith, Susan M; Garic, Ana; Flentke, George R et al. (2014) Neural crest development in fetal alcohol syndrome. Birth Defects Res C Embryo Today 102:210-20
Flentke, George R; Klingler, Rebekah H; Tanguay, Robert L et al. (2014) An evolutionarily conserved mechanism of calcium-dependent neurotoxicity in a zebrafish model of fetal alcohol spectrum disorders. Alcohol Clin Exp Res 38:1255-65
Garic, Ana; Berres, Mark E; Smith, Susan M (2014) High-throughput transcriptome sequencing identifies candidate genetic modifiers of vulnerability to fetal alcohol spectrum disorders. Alcohol Clin Exp Res 38:1874-82

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