孕期中期母亲饮酒会通过内源性大麻素受体使胎儿脑动脉扩张。
Maternal alcohol exposure during mid-pregnancy dilates fetal cerebral arteries via endocannabinoid receptors.
作者信息
Seleverstov Olga, Tobiasz Ana, Jackson J Scott, Sullivan Ryan, Ma Dejian, Sullivan J Pierce, Davison Steven, Akkhawattanangkul Yada, Tate Danielle L, Costello Terry, Barnett Stacey, Li Wei, Mari Giancarlo, Dopico Alex M, Bukiya Anna N
机构信息
Department of Pharmacology, University of Tennessee Health Science Center, Memphis, TN, USA.
Department of Obstetrics and Gynecology, University of Tennessee Health Science Center, Memphis, TN, USA.
出版信息
Alcohol. 2017 Jun;61:51-61. doi: 10.1016/j.alcohol.2017.01.014. Epub 2017 May 18.
Prenatal alcohol exposure often results in fetal alcohol syndrome and fetal alcohol spectrum disorders. Mechanisms of fetal brain damage by alcohol remain unclear. We used baboons (Papio spp.) to study alcohol-driven changes in the fetal cerebral artery endocannabinoid system. Pregnant baboons were subjected to binge alcohol exposure via gastric infusion three times during a period equivalent to the second trimester of human pregnancy. A control group was infused with orange-flavored drink that was isocaloric to the alcohol-containing solution. Cesarean sections were performed at a time equivalent to the end of the second trimester of human pregnancy. Fetal cerebral arteries were harvested and subjected to in vitro pressurization followed by pharmacological profiling. During each alcohol-infusion episode, maternal blood alcohol concentrations (BAC) reached 80 mg/dL, that is, equivalent to the BAC considered legal intoxication in humans. Circulating anandamide (AEA) and 2-arachidonoylglycerol (2-AG) remained unchanged. Ultrasound studies on pregnant mothers revealed that fetal alcohol exposure decreased peak systolic blood velocity in middle cerebral arteries when compared to pre-alcohol levels. Moreover, ethanol-induced dilation was observed in fetal cerebral arteries pressurized in vitro. This dilation was abolished by the mixture of AM251 and AM630, which block cannabinoid receptors 1 and 2, respectively. In the presence of AM251, the cannabinoid receptor agonist AEA evoked a higher, concentration-dependent dilation of cerebral arteries from alcohol-exposed fetuses. The difference in AEA-induced cerebral artery dilation vanished in the presence of AM630. CB1 and CB2 receptor mRNA and protein levels were similar in cerebral arteries from alcohol-exposed and control-exposed fetuses. In summary, alcohol exposure dilates fetal cerebral arteries via endocannabinoid receptors and results in an increased function of CB2.
产前酒精暴露通常会导致胎儿酒精综合征和胎儿酒精谱系障碍。酒精对胎儿大脑造成损害的机制尚不清楚。我们使用狒狒(Papio spp.)来研究酒精驱动的胎儿脑动脉内源性大麻素系统的变化。在相当于人类妊娠中期的时间段内,对怀孕的狒狒通过胃内灌注进行三次暴饮酒精暴露。对照组灌注与含酒精溶液热量相等的橙汁饮料。在相当于人类妊娠中期结束时进行剖宫产。采集胎儿脑动脉并进行体外加压,随后进行药理学分析。在每次酒精灌注期间,母体血液酒精浓度(BAC)达到80mg/dL,即相当于人类法定醉酒的BAC。循环中的花生四烯酸乙醇胺(AEA)和2-花生四烯酸甘油酯(2-AG)保持不变。对怀孕母亲的超声研究表明,与酒精暴露前水平相比,胎儿酒精暴露会降低大脑中动脉的收缩期峰值血流速度。此外,在体外加压的胎儿脑动脉中观察到乙醇诱导的扩张。这种扩张被分别阻断大麻素受体1和2的AM251和AM630的混合物消除。在存在AM251的情况下,大麻素受体激动剂AEA引起酒精暴露胎儿脑动脉更高的、浓度依赖性的扩张。在存在AM630的情况下,AEA诱导的脑动脉扩张差异消失。酒精暴露胎儿和对照暴露胎儿的脑动脉中CB1和CB2受体mRNA和蛋白质水平相似。总之,酒精暴露通过内源性大麻素受体使胎儿脑动脉扩张,并导致CB2功能增强。
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