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子宫内可卡因暴露对恒河猴胎儿中编码多巴胺转运体以及D1、D2和D5多巴胺受体亚型的mRNA表达的影响。

Effects of in utero cocaine exposure on the expression of mRNAS encoding the dopamine transporter and the D1, D2 and D5 dopamine receptor subtypes in fetal rhesus monkey.

作者信息

Choi W S, Rønnekleiv O K

机构信息

Department of Physiology and Pharmacology, Oregon Health Sciences University, Portland 97201, USA.

出版信息

Brain Res Dev Brain Res. 1996 Oct 23;96(1-2):249-60. doi: 10.1016/0165-3806(96)00123-x.

DOI:10.1016/0165-3806(96)00123-x
PMID:8922687
Abstract

The effects of in utero cocaine exposure on the development of the mRNAs encoding the dopamine transporter (DAT) and the D1, D2 and D5 dopamine receptor subtypes were determined in fetal monkey brains at day 45 and day 60 of gestation. Pregnant monkeys were treated with cocaine 3 mg/kg or saline i.m., four times a day from day 18 of gestation until the pregnancy was terminated at day 45 or day 60. The fetal brains were dissected, and tissue RNA extracted and quantified using ribonuclease protection assay analysis. In day 45 fetal monkeys, dopamine D1 and D2 receptor subtype mRNAs and DAT mRNA were found in low quantities both in control and cocaine-treated subjects. In day 60 fetal monkeys, D1 receptor mRNA levels were highest in the frontal cortex/striatal area, and low to moderate quantities were found in diencephalic and mesencephalic fetal brain regions. Dopamine D2 receptor mRNA levels were highest in the frontal cortex/striatal area, diencephalon and the midbrain, moderate in the brainstem and low in the caudal temporal lobe and surrounding cortical areas. Dopamine D5 receptor mRNA was expressed in low quantities throughout the day 60 fetal monkey brain, whereas DAT mRNA was found in the midbrain only. In utero cocaine exposure caused a significant increase in dopamine D1, D2 and D5 receptor subtype mRNAs in the frontal cortex/striatal area of day 60 fetal monkeys. These results support the hypothesis that dopamine synthesis and release may be reduced in cocaine-treated fetuses, which results in dopamine receptor up-regulation.

摘要

在妊娠第45天和第60天的胎猴大脑中,研究了子宫内可卡因暴露对编码多巴胺转运体(DAT)以及D1、D2和D5多巴胺受体亚型的mRNA发育的影响。怀孕的猴子从妊娠第18天开始,每天接受4次3mg/kg可卡因或生理盐水的肌肉注射,直至在第45天或第60天终止妊娠。解剖胎脑,提取组织RNA并使用核糖核酸酶保护分析进行定量。在第45天的胎猴中,对照组和可卡因处理组的多巴胺D1和D2受体亚型mRNA以及DAT mRNA含量均较低。在第60天的胎猴中,D1受体mRNA水平在额叶皮质/纹状体区域最高,在间脑和中脑胎脑区域中含量低至中等。多巴胺D2受体mRNA水平在额叶皮质/纹状体区域、间脑和中脑最高,在脑干中中等,在颞叶尾部和周围皮质区域中较低。多巴胺D5受体mRNA在整个第60天的胎猴大脑中表达量较低,而DAT mRNA仅在中脑中发现。子宫内可卡因暴露导致第60天胎猴额叶皮质/纹状体区域的多巴胺D1、D2和D5受体亚型mRNA显著增加。这些结果支持了以下假设:可卡因处理的胎儿中多巴胺的合成和释放可能减少,从而导致多巴胺受体上调。

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