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胎儿行为与多巴胺系统:D1和D2受体操作的活性效应

Fetal behavior and the dopamine system: activity effects of D1 and D2 receptor manipulations.

作者信息

Moody C A, Robinson S R, Spear L P, Smotherman W P

机构信息

Department of Psychology, Binghamton University, NY 13902-6000.

出版信息

Pharmacol Biochem Behav. 1993 Apr;44(4):843-50. doi: 10.1016/0091-3057(93)90015-l.

Abstract

Binding studies have indicated that D1 and D2 dopamine receptor subtypes are present in rats before birth, but it is not known whether these receptors are functional during the prenatal period. In the present study, day-21 rat fetuses were prepared for direct observation after pharmacological manipulation of D1 and/or D2 receptors. The D1 agonist SK&F38393 induced a marked increase in fetal activity (i.e., forelimb, rearlimb, and head movements) while the D2 agonist quinpirole produced a slight suppression in activity. Coadministration of both agonists resulted in low levels of fetal activity, suggesting an interaction between D1 and D2 receptors. Administration of the D2 antagonist sulpiride resulted in little change in fetal behavior but was effective in blocking the behavioral activation induced by the D1 agonist. The D1 antagonist SCH23390, administered alone or in combination with the D2 antagonist, produced a modest increase in fetal activity that included mouthing and facial wiping behavior. These data provide evidence that the dopamine system is functional and capable of mediating behavioral effects in the near-term rat fetus. Further, manipulation of dopamine receptors results in a different pattern of behavioral effects than has been reported in older animals. The observation that fetal behavior is influenced by these pharmacological challenges suggests that drugs of abuse known to affect the dopamine system, such as cocaine, may cause profound changes in fetal behavior in utero that could consequently lead to alterations in behavioral and CNS development.

摘要

结合研究表明,多巴胺D1和D2受体亚型在大鼠出生前就已存在,但尚不清楚这些受体在产前阶段是否具有功能。在本研究中,对妊娠21天的大鼠胎儿进行了D1和/或D2受体的药理学操作后,准备进行直接观察。D1激动剂SK&F38393可使胎儿活动(即前肢、后肢和头部运动)显著增加,而D2激动剂喹吡罗则使活动略有抑制。两种激动剂同时给药导致胎儿活动水平较低,提示D1和D2受体之间存在相互作用。给予D2拮抗剂舒必利对胎儿行为影响不大,但能有效阻断D1激动剂诱导的行为激活。单独给予或与D2拮抗剂联合给予D1拮抗剂SCH23390,会使胎儿活动适度增加,包括咂嘴和擦脸行为。这些数据证明多巴胺系统具有功能,并且能够介导近足月大鼠胎儿的行为效应。此外,多巴胺受体的操作所产生的行为效应模式与在年长动物中所报道的不同。胎儿行为受到这些药理学刺激的影响这一观察结果表明,已知会影响多巴胺系统的滥用药物,如可卡因,可能会在子宫内导致胎儿行为发生深刻变化,进而可能导致行为和中枢神经系统发育的改变。

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