Effect of Developmental Exposure to Chlorpyrifos on the Expression of Neurotrophin Growth Factors and Cell-Specific Markers in Neonatal Rat Brain

doi:10.1093/toxsci/kfl004

ToxSci Advance Access originally published online on May 4, 2006
Toxicological Sciences 2006 92(2):500-506; doi:10.1093/toxsci/kfl004

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Effect of Developmental Exposure to Chlorpyrifos on the Expression of Neurotrophin Growth Factors and Cell-Specific Markers in Neonatal Rat Brain

Angela M. Betancourt, Shane C. Burgess and Russell L. Carr¹

Center for Environmental Health Sciences, College of Veterinary Medicine, Mississippi State University, Mississippi 39762

Received January 19, 2006; accepted April 20, 2006

Chlorpyrifos (CPS), a known neurotoxicant, is a widely usedagricultural organophosphorus insecticide. The effects of postnatalexposure to CPS on the expression of mRNA for two factors criticalto brain development, nerve growth factor (NGF) and reelin,were investigated in the forebrain of rats. In addition, theexpression of mRNA for the muscarinic acetylcholine receptor(mAChR) M₁ subtype and cell-specific markers for developingneurons (ß-III tubulin), astrocytes (glial fibrillaryacidic protein, GFAP), and oligodendrocytes (myelin-associatedglycoprotein, MAG) was also investigated. Oral administrationof CPS (1.5 or 3.0 mg/kg) or the corn oil vehicle was performeddaily from postnatal days (PNDs) 1 through 6. No signs of overttoxicity or of cholinergic hyperstimulation were observed afterCPS administration. Body weight was significantly differentfrom controls on PND7 in both males and females exposed to 3.0mg/kg CPS. Quantitative PCR was performed on the forebrain.The expression of NGF, reelin, and M₁ mAChR mRNA was significantlyreduced with both dosages of CPS in both sexes. ß-IIITubulin mRNA expression remained unchanged after exposure, whereasMAG mRNA expression was significantly decreased with both dosagesof CPS in both sexes, suggesting effects on the developing oligodendrocytes.In contrast, GFAP mRNA levels were significantly increased withboth dosages of CPS in both sexes, suggesting increased astrocytereactivity. Our findings indicate that dosages of CPS whichcause significant cholinesterase inhibition but do not exertovert toxicity can adversely affect the expression levels ofcritical genes involved in brain development during the earlypostnatal period in the rat.

Key Words: chlorpyrifos; nerve growth factor; reelin; ß-III tubulin; brain development; astrocytes; oligodendrocytes; muscarinic receptor.

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