TY - JOUR
T1 - Moderate-level prenatal alcohol exposure alters striatal dopamine system function in rhesus monkeys
AU - Schneider, Mary L.
AU - Moore, Colleen F.
AU - Barnhart, Todd E.
AU - Larson, Julie A.
AU - DeJesus, Onofre T.
AU - Mukherjee, Jogeshwar
AU - Nickles, Robert J.
AU - Converse, Alexander K.
AU - Roberts, Andrew D.
AU - Kraemer, Gary W.
PY - 2005/9
Y1 - 2005/9
N2 - Background: Moderate prenatal alcohol exposure can cause impairments even in the absence of gross morphological defects associated with fetal alcohol syndrome. The basal ganglia, which include the dopamine-rich striatum, are sensitive to fetal alcohol-induced injury. In this study, we manipulated the timing of moderate-level alcohol exposure and compared the risk of adverse effects on striatal dopamine (DA) system function in rhesus monkeys. Methods: Thirty-five young adult rhesus monkeys (Macaco mulatta) from four groups of females were assessed: (1) an early alcohol-exposed group (n = 9), in which mothers voluntarily consumed 0.6 g/kg alcohol solution on gestational days O through 50; (2) a middle-to-late gestation alcohol-exposed group (n = 7), in which mothers voluntarily consumed 0.6 g/kg alcohol solution on gestational days 50 through 135; (3) a continuous-exposure group (n = 9), in which mothers voluntarily consumed 0.6 g/kg alcohol solution on days O through 135; and (4) controls (n = 10), in which mothers voluntarily consumed an isocaloric control solution on gestational days O through 50,50 through 135, or 0 through 135. We studied striatal DA system function by positron emission tomography in separate scans for trapping of [ 18F]fallypride and 6-[ 18F]fluoro-m- tyrosine to assess striatal DA D 2 receptor (D 2R) binding and DA synthesis, respectively, via dopadecarboxylase activity. Results: Moderate-level alcohol exposure during early gestation and continuous exposure throughout gestation (early + middle-to-late exposure) reduced the striatal D 2R binding to DA synthesis ratio, whereas middle-to-late alcohol gestation exposure increased the striatal D 2R binding to DA synthesis ratio. The continuous-exposure group showed the largest effect. Moreover, the D 2R binding/DA synthesis ratio was related to neonatal neurobehavior measures in control monkeys, but these relationships were disrupted in the fetal alcohol-exposed monkeys. Conclusion: These results suggest that the vulnerability of the DA system to the effects of moderate doses of alcohol during gestation depend on the timing of the alcohol exposure. Early-gestation moderate alcohol exposure resulted in a reduction or blunting of dopaminergic function in adulthood, whereas middle to late exposure (without early exposure) either induced the opposite pattern or heightened dopaminergic function. Continuously exposed monkeys showed the largest effect, suggesting that the sooner women stop drinking, the better it is for the fetus. Copyright © 2005 by the Research Society on Alcoholism.
AB - Background: Moderate prenatal alcohol exposure can cause impairments even in the absence of gross morphological defects associated with fetal alcohol syndrome. The basal ganglia, which include the dopamine-rich striatum, are sensitive to fetal alcohol-induced injury. In this study, we manipulated the timing of moderate-level alcohol exposure and compared the risk of adverse effects on striatal dopamine (DA) system function in rhesus monkeys. Methods: Thirty-five young adult rhesus monkeys (Macaco mulatta) from four groups of females were assessed: (1) an early alcohol-exposed group (n = 9), in which mothers voluntarily consumed 0.6 g/kg alcohol solution on gestational days O through 50; (2) a middle-to-late gestation alcohol-exposed group (n = 7), in which mothers voluntarily consumed 0.6 g/kg alcohol solution on gestational days 50 through 135; (3) a continuous-exposure group (n = 9), in which mothers voluntarily consumed 0.6 g/kg alcohol solution on days O through 135; and (4) controls (n = 10), in which mothers voluntarily consumed an isocaloric control solution on gestational days O through 50,50 through 135, or 0 through 135. We studied striatal DA system function by positron emission tomography in separate scans for trapping of [ 18F]fallypride and 6-[ 18F]fluoro-m- tyrosine to assess striatal DA D 2 receptor (D 2R) binding and DA synthesis, respectively, via dopadecarboxylase activity. Results: Moderate-level alcohol exposure during early gestation and continuous exposure throughout gestation (early + middle-to-late exposure) reduced the striatal D 2R binding to DA synthesis ratio, whereas middle-to-late alcohol gestation exposure increased the striatal D 2R binding to DA synthesis ratio. The continuous-exposure group showed the largest effect. Moreover, the D 2R binding/DA synthesis ratio was related to neonatal neurobehavior measures in control monkeys, but these relationships were disrupted in the fetal alcohol-exposed monkeys. Conclusion: These results suggest that the vulnerability of the DA system to the effects of moderate doses of alcohol during gestation depend on the timing of the alcohol exposure. Early-gestation moderate alcohol exposure resulted in a reduction or blunting of dopaminergic function in adulthood, whereas middle to late exposure (without early exposure) either induced the opposite pattern or heightened dopaminergic function. Continuously exposed monkeys showed the largest effect, suggesting that the sooner women stop drinking, the better it is for the fetus. Copyright © 2005 by the Research Society on Alcoholism.
KW - Dopamine
KW - Fetal Alcohol Exposure
KW - Neurobehavior
KW - Positron Emission Tomography
KW - Rhesus Monkey
KW - Striatum
U2 - 10.1097/01.alc.0000179409.80370.25
DO - 10.1097/01.alc.0000179409.80370.25
M3 - Article
SN - 0145-6008
VL - 29
SP - 1685
EP - 1697
JO - Alcoholism: Clinical and Experimental Research
JF - Alcoholism: Clinical and Experimental Research
IS - 9
ER -