Dose Response Effects of Dermally applied Diethanolamine on Neurogenesis in Fetal Mouse Hippocampus and Potential Exposure of Humans

doi:10.1093/toxsci/kfn227

ToxSci Advance Access originally published online on October 23, 2008
Toxicological Sciences 2009 107(1):220-226; doi:10.1093/toxsci/kfn227

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Dose Response Effects of Dermally applied Diethanolamine on Neurogenesis in Fetal Mouse Hippocampus and Potential Exposure of Humans

Corneliu N. Craciunescu^*, Mihai D. Niculescu^*, Zhong Guo^*, Amy R. Johnson^*, Leslie Fischer^* and Steven H. Zeisel^*^,^,1

^* Department of Nutrition, School of Public Health and Medicine, University of North Carolina at Chapel Hill, Chapel Hill, North Carolina 27599-7461 Nutrition Research Institute, University of North Carolina at Chapel Hill, Kannapolis, North Carolina 28081-4332

¹ To whom correspondence should be addressed at CB#7461, 2115A Michael Hooker Research Center, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599-7461. Fax: (919)-843-8555; E-mail: steven_zeisel{at}unc.edu.

Received June 9, 2008; accepted October 18, 2008

Abstract

Diethanolamine (DEA) is a common ingredient of personal careproducts. Dermal administration of DEA diminishes hepatic storesof the essential nutrient choline and alters brain development.We previously reported that 80 mg/kg/day of DEA during pregnancyin mice reduced neurogenesis and increased apoptosis in thefetal hippocampus. This study was designed to establish thedose-response relationships for this effect of DEA. Timed-pregnantC57BL/6 mouse dams were dosed dermally from gestation day 7–17with DEA at 0 (controls), 5, 40, 60, and 80 mg/kg body/day.Fetuses (embryonic day 17 [E17]) from dams treated dermallywith 80 mg/kg body/day DEA had decreased neural progenitor cellmitosis at the ventricular surface of the ventricular zone (hippocampus,54.1 ± 5.5%; cortex, 58.9 ± 6.8%; compared tocontrols; p < 0.01). Also, this dose of DEA to dams increasedrates of apoptosis in E17 fetal hippocampus (to 177.2 ±21.5% of control; measured using activated caspase-3; p <0.01). This dose of DEA resulted in accumulation of DEA andits metabolites in liver and in plasma. At doses of DEA lessthan 80 mg/kg body/day to dams, there were no differences betweentreated and control groups. In a small group of human subjects,dermal treatment for 1 month with a commercially available skinlotion containing 1.8 mg DEA per gram resulted in detectableplasma concentrations of DEA and dimethyldiethanolamine, butthese were far below those concentrations associated with perturbedbrain development in the mouse.

Key Words: diethanolamine; choline; pregnancy; brain development; mouse; hippocampus.

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