PCB126 Exposure Disrupts ZebraFish Ventricular and Branchial but Not Early Neural Crest Development
PCB126 Exposure Disrupts ZebraFish Ventricular and Branchial but Not Early Neural Crest Development
We have used zebrafish and 3,3',4,4',5-pentachlorobiphenyl (PCB126) to investigate the developmental toxicity of polychlorinated biphenyls (PCBs) that exert their effects through the aryl hydrocarbon receptor (AHR). We found that cardiac and neural crest (NC)-derived jaw and branchial cartilages are specifically targeted early in development. The suite of malformations, which ultimately leads to circulatory failure, includes a severely dysmorphic heart with a reduced bulbus arteriosus and abnormal atrioventricular and outflow valve formation. Early NC migration and patterning of the jaw and branchial cartilages was normal. However, the jaw and branchial cartilages failed to grow to normal size. In the heart, the ventricular myocardium showed a reduction in cell number and size. The heart and jaw/branchial phenotype could be rescued by pifithrin-alpha, a blocker of p53. However, the function of pifithrin-alpha in this model may act as a competitive inhibitor of PCB at the AHR and is likely independent of p53. Morpholinos against p53 did not rescue the phenotype, nor were zebrafish with a mutant p53-null allele resistant to PCB126 toxicity. Morpholino knockdown of cardiac troponin T, which blocks the onset of cardiac function, prevented the PCB126-induced cardiac dysmorphogenesis but not the jaw/branchial phenotype. The cardiovascular characteristics appear to be similar to hypoplastic left heart syndrome (HLHS) and introduce the potential of zebrafish as a model to study this environmentally induced cardiovascular malformation. HLHS is a severe congenital cardiovascular malformation that has previously been linked to industrial releases of dioxins and PCBs.
- Institute for Molecular and Cellular Biology France
- Duke University United States
- Duke Medical Center United States
- Duke University Hospital United States
- Medical University of South Carolina United States
Heart Defects, Congenital, Time Factors, Cell Death, Heart Ventricles, Morpholines, Oligonucleotides, Cell Differentiation, Polychlorinated Biphenyls, Animals, Genetically Modified, Branchial Region, Phenotype, Jaw Abnormalities, Cell Movement, Neural Crest, Animals, Abnormalities, Multiple, Environmental Pollutants, Benzothiazoles, Body Patterning, Cell Proliferation
Heart Defects, Congenital, Time Factors, Cell Death, Heart Ventricles, Morpholines, Oligonucleotides, Cell Differentiation, Polychlorinated Biphenyls, Animals, Genetically Modified, Branchial Region, Phenotype, Jaw Abnormalities, Cell Movement, Neural Crest, Animals, Abnormalities, Multiple, Environmental Pollutants, Benzothiazoles, Body Patterning, Cell Proliferation
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