Fetal Alcohol Syndrome (FAS) in C57BL/6 Mice Detected Through Proteomics Screening of the Amniotic Fluid

Overview

Journal Birth Defects Res A Clin Mol Teratol

Publisher Wiley

Date 2008 Feb 2

PMID 18240165

Citations 15

Authors

Susmita Datta

Delano Turner

Reetu Singh

L Bruno Ruest

William M Pierce Jr

Thomas B Knudsen

Affiliations

Soon will be listed here.

Abstract

Background: Fetal Alcohol Syndrome (FAS), a severe consequence of the Fetal Alcohol Spectrum Disorders, is associated with craniofacial defects, mental retardation, and stunted growth. Previous studies in C57BL/6J and C57BL/6N mice provide evidence that alcohol-induced pathogenesis follows early changes in gene expression within specific molecular pathways in the embryonic headfold. Whereas the former (B6J) pregnancies carry a high-risk for dysmorphogenesis following maternal exposure to 2.9 g/kg alcohol (two injections spaced 4.0 h apart on gestation day 8), the latter (B6N) pregnancies carry a low-risk for malformations. The present study used this murine model to screen amniotic fluid for biomarkers that could potentially discriminate between FAS-positive and FAS-negative pregnancies.

Methods: B6J and B6N litters were treated with alcohol (exposed) or saline (control) on day 8 of gestation. Amniotic fluid aspirated on day 17 (n = 6 replicate litters per group) was subjected to trypsin digestion for analysis by matrix-assisted laser desorption-time of flight mass spectrometry with the aid of denoising algorithms, statistical testing, and classification methods.

Results: We identified several peaks in the proteomics screen that were reduced consistently and specifically in exposed B6J litters. Preliminary characterization by liquid chromatography tandem mass spectrometry and multidimensional protein identification mapped the reduced peaks to alpha fetoprotein (AFP). The predictive strength of AFP deficiency as a biomarker for FAS-positive litters was confirmed by area under the receiver operating characteristic curve.

Conclusions: : These findings in genetically susceptible mice support clinical observations in maternal serum that implicate a decrease in AFP levels following prenatal alcohol damage.

Citing Articles

Murine Models for the Study of Fetal Alcohol Spectrum Disorders: An Overview.

Almeida L, Andreu-Fernandez V, Navarro-Tapia E, Aras-Lopez R, Serra-Delgado M, Martinez L Front Pediatr. 2020; 8:359.

PMID: 32760684 PMC: 7373736. DOI: 10.3389/fped.2020.00359.

Ethanol-Induced Alterations in Placental and Fetal Cerebrocortical Annexin-A4 and Cerebral Cavernous Malformation Protein 3 Are Associated With Reductions in Fetal Cortical VEGF Receptor Binding and Microvascular Density.

Savage D, Rosenberg M, Coquet L, Porch M, Allen N, Roux C Front Neurosci. 2020; 14:519.

PMID: 32655346 PMC: 7325964. DOI: 10.3389/fnins.2020.00519.

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

Holbrook B, Davies S, Cano S, Shrestha S, Jantzie L, Rayburn W Birth Defects Res. 2019; 111(12):749-759.

PMID: 30891944 PMC: 6946025. DOI: 10.1002/bdr2.1488.

Review and gap analysis: molecular pathways leading to fetal alcohol spectrum disorders.

Ehrhart F, Roozen S, Verbeek J, Koek G, Kok G, van Kranen H Mol Psychiatry. 2018; 24(1):10-17.

PMID: 29892052 PMC: 6325721. DOI: 10.1038/s41380-018-0095-4.

Fetal regional brain protein signature in FASD rat model.

Davis-Anderson K, Wesseling H, Siebert L, Lunde-Young E, Naik V, Steen H Reprod Toxicol. 2018; 76:84-92.

PMID: 29408587 PMC: 5834402. DOI: 10.1016/j.reprotox.2018.01.004.

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