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单胺转运体与可卡因的神经行为致畸学

Monoamine transporters and the neurobehavioral teratology of cocaine.

作者信息

Meyer J S, Shearman L P, Collins L M

机构信息

Department of Psychology, University of Massachusetts, Amherst 01003, USA.

出版信息

Pharmacol Biochem Behav. 1996 Dec;55(4):585-93. doi: 10.1016/s0091-3057(96)00280-8.

Abstract

Prenatal cocaine exposure has been associated with various postnatal behavioral abnormalities in human infants, and also with changes in locomotor activity, learning deficits, and altered responses to drug challenge in nonhuman offspring. Several studies have further demonstrated that cocaine exerts an activating effect on fetal behavior. A variety of mechanisms have been proposed to account for the neurobehavioral teratogenic effects of developmental cocaine treatment, including inhibition of fetal brain neurotransmitter uptake and fetal hypoxemia secondary to constriction of the uteroplacental vascular bed. In support of the hypothesis that cocaine effects may be mediated partly by monoamine uptake inhibition, we and other investigators have recently demonstrated the presence of functional dopamine (DA), serotonin (5-HT), and norepinephrine (NE) transporters in the fetal rat brain. Transporter-related cocaine recognition sites are found in a number of fetal brain areas and could mediate the acute effects of cocaine on these areas as well as developmental changes that are manifested postnatally. For example, DA transporter blockade may underlie the above-mentioned activational effects of cocaine on fetal behavior. Time-dependent changes in DA or 5-HT transporter expression produced by prenatal cocaine exposure could likewise play an important role in some of the behavioral effects observed when offspring are tested postnatally.

摘要

产前接触可卡因与人类婴儿出生后的各种行为异常有关,也与非人类后代的运动活动变化、学习缺陷以及对药物刺激的反应改变有关。多项研究进一步表明,可卡因对胎儿行为有激活作用。人们提出了多种机制来解释发育过程中接触可卡因的神经行为致畸作用,包括抑制胎儿脑内神经递质摄取以及子宫胎盘血管床收缩继发的胎儿低氧血症。为支持可卡因效应可能部分由单胺摄取抑制介导这一假说,我们和其他研究人员最近证明了胎鼠脑内存在功能性多巴胺(DA)、5-羟色胺(5-HT)和去甲肾上腺素(NE)转运体。转运体相关的可卡因识别位点存在于多个胎儿脑区,可介导可卡因对这些区域的急性效应以及出生后表现出的发育变化。例如,多巴胺转运体阻断可能是上述可卡因对胎儿行为激活作用的基础。产前接触可卡因导致的多巴胺或5-羟色胺转运体表达的时间依赖性变化同样可能在后代出生后测试时观察到的一些行为效应中起重要作用。

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