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产前暴露于氟西汀(百忧解)会使大鼠后代大脑中的血清素转运体产生位点特异性和年龄依赖性改变:来自放射自显影研究的证据。

Prenatal exposure to fluoxetine (Prozac) produces site-specific and age-dependent alterations in brain serotonin transporters in rat progeny: evidence from autoradiographic studies.

作者信息

Cabrera-Vera T M, Battaglia G

机构信息

Department of Pharmacology and Experimental Therapeutics, Loyola University of Chicago, Stritch School of Medicine, Maywood, Illinois, USA.

出版信息

J Pharmacol Exp Ther. 1998 Sep;286(3):1474-81.

PMID:9732413
Abstract

The present study provides the first autoradiographic evidence of age-dependent regional changes in the density of serotonin (5-HT) transporters in offspring following prenatal exposure to fluoxetine. Pregnant rats received either saline or fluoxetine (10 mg/kg, s.c.) daily from gestational day 13 through 20. The density of [3H]citalopram-labeled 5-HT transporters was determined in forebrain regions and in midbrain raphe nuclei of prepubescent and adult male offspring. Brain regions representing integral components of the limbic system were particularly sensitive to the prenatal treatment. For example, prenatal fluoxetine exposure significantly altered the density of 5-HT transporters in subregions of the hypothalamus (dorsomedial nucleus, -21%; lateral hypothalamus, +21%), hippocampus (CA2, +47%; CA3, +38%), and amygdala (basolateral nucleus, +32%; medial nucleus, +44%) in prepubescent offspring. However, 5-HT transporter density in the dorsal and median raphe was unaltered in this same group of offspring. In adult offspring, 5-HT transporter densities, in all brain regions examined, were not significantly altered by prenatal exposure to fluoxetine. The present study also identifies significant age-related differences in 5-HT transporter densities between prepubescent and adult control offspring. For example, in adult control offspring, densities of 5-HT transporters were significantly greater in the cingulate cortex (+33%), basolateral amygdala (+58%), and CA1 area of the hippocampus (+78%); but significantly lower in the temporal cortex (-65%) and median raphe (-25%). The age-dependent and site-specific alterations in the density of 5-HT transporters suggests that either 5-HT innervation and/or 5-HT neuron function in various forebrain regions may be altered by prenatal exposure to fluoxetine.

摘要

本研究首次提供了放射自显影证据,证明产前暴露于氟西汀的后代中,血清素(5-羟色胺,5-HT)转运体密度存在年龄依赖性区域变化。怀孕大鼠从妊娠第13天至20天每天接受生理盐水或氟西汀(10毫克/千克,皮下注射)。在青春期前和成年雄性后代的前脑区域和中脑缝际核中测定[3H]西酞普兰标记的5-HT转运体的密度。代表边缘系统组成部分的脑区对产前治疗特别敏感。例如,产前暴露于氟西汀显著改变了青春期前后代下丘脑各亚区(背内侧核,-21%;外侧下丘脑,+21%)、海马体(CA2,+47%;CA3,+38%)和杏仁核(基底外侧核,+32%;内侧核,+44%)中5-HT转运体的密度。然而,在同一组后代中,背侧和中缝际的5-HT转运体密度未发生改变。在成年后代中,产前暴露于氟西汀并未显著改变所有检测脑区的5-HT转运体密度。本研究还发现青春期前和成年对照后代之间5-HT转运体密度存在显著的年龄相关差异。例如,在成年对照后代中,5-HT转运体密度在扣带回皮质(+33%)、基底外侧杏仁核(+58%)和海马体CA1区(+78%)显著更高;但在颞叶皮质(-65%)和中缝际(-25%)显著更低。5-HT转运体密度的年龄依赖性和位点特异性改变表明,产前暴露于氟西汀可能会改变各个前脑区域的5-HT神经支配和/或5-HT神经元功能。

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