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Effects of valproic acid on the placental barrier in the pregnant mouse: Optical imaging and transporter expression studies

机译:丙戊酸对妊娠小鼠胎盘屏障的影响:光学成像和转运蛋白表达研究

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Our aim was to evaluate the effects of valproic acid (VPA) on the function of the placental barrier in vivo, in pregnant mice. Studies were conducted on gestational days 12.5 (mid-gestation) or 17.5 (late gestation), following intraperitoneal treatment with 200 mg/kg VPA or the vehicle. Indocyanine green (ICG; 0.167 mg, i.v.) was used as a marker for the placental barrier permeability. Transporter expression was evaluated by quantitative -PCR. VPA treatment was associated with a 40% increase (p < 0.05) in accumulation of ICG in maternal liver in mid-pregnancy and a decrease by one fifth (p < 0.05) in late pregnancy. Ex vivo, VPA treatment led to a 20% increase (p < 0.05) in fetal ICG emission in mid-pregnancy. Also in mid-pregnancy, the placental expression of the L-type amino acid transporter, the organic anion-transporting polypeptide (Oatp) 4a1 (thyroid hormone transporter), and the reduced folate carrier was lower in VPA-treated mice (p < 0.05). In late pregnancy, hepatic Oatp4a1 levels were 40% less than in controls (p > 0.05). The observed changes in placental transporter expression and function support further research into the potential role of the placenta in the adverse pregnancy outcomes of VPA. Near-infrared imaging provides a noninvasive, nonradioactive tool for future studies on the effects of epilepsy and antiepileptic drugs on tissue transport functions.
机译:我们的目的是评估丙戊酸(VPA)对妊娠小鼠体内胎盘屏障功能的影响。在以200 mg / kg V​​PA或赋形剂腹膜内治疗后,在妊娠第12.5天(妊娠中期)或17.5天(妊娠晚期)进行研究。吲哚菁绿(ICG; 0.167mg,i.v。)用作胎盘屏障渗透性的标记。通过定量-PCR评估转运蛋白表达。 VPA治疗与妊娠中期孕妇肝脏中ICG积累增加40%(p <0.05)和妊娠晚期减少五分之一(p <0.05)有关。在离体时,VPA治疗导致中期妊娠胎儿ICG排放增加20%(p <0.05)。同样在妊娠中期,在VPA处理的小鼠中,L型氨基酸转运蛋白,有机阴离子转运多肽(Oatp)4a1(甲状腺激素转运蛋白)和还原型叶酸载体的胎盘表达较低(p <0.05)。 )。在妊娠晚期,肝脏Oatp4a1水平比对照组低40%(p> 0.05)。观察到的胎盘转运蛋白表达和功能变化支持进一步研究胎盘在VPA不良妊娠结局中的潜在作用。近红外成像为癫痫和抗癫痫药物对组织转运功能的影响进行进一步研究提供了一种非侵入性,非放射性的工具。

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