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早期生活抗抑郁药暴露破坏了血清素系统的发育,导致成年雌性后代的母性行为受损和血清素受体表达增加。

Disrupted serotonin system development via early life antidepressant exposure impairs maternal care and increases serotonin receptor expression in adult female offspring.

机构信息

School of Neuroscience, Virginia Polytechnic Institute and State University, Blacksburg, Virginia, USA.

Graduate Program in Translational Biology, Medicine, and Health, Virginia Polytechnic Institute and State University, Blacksburg, Virginia, USA.

出版信息

Dev Psychobiol. 2022 Sep;64(6):e22292. doi: 10.1002/dev.22292.

Abstract

Manipulating serotonin (5-HT) levels in the developing brain elicits a range of effects on brain function and behavior. For example, early-life exposure to selective 5-HT reuptake inhibitor (SSRI) antidepressants disrupts dorsal raphe function and triggers aberrant adult behaviors such as increased passive stress coping and anhedonia. However, much less is understood about how alterations in 5-HT signaling in early life impact outcomes in female offspring, including critical social functions such as maternal care. The present study shows that early-life SSRI exposure disrupts adult female offspring's maternal behavior. Pregnant/postpartum female Sprague-Dawley rats were treated with the SSRI citalopram in drinking water or provided regular tap water as control. Female offspring were raised to adulthood and mated with treatment-naïve males. Following parturition, we observed maternal behavior during portions of the light and dark phases of postnatal days (P)1-14. Relative to controls, dams with a history of early-life SSRI exposure exhibited decreased maternal care, including diminished arched-back nursing, reduced licking and grooming of pups, and increased behavioral inconsistency. Brains were collected from dams with and without a history of early-life SSRI exposure to measure relative mRNA expression of select 5-HT receptor transcripts (5HTR1A, -1B, -2A, -2C) in regions involved in maternal care. Early-life SSRI exposure augmented expression of 5-HTR1A in the medial preoptic area and 5-HTR1B, 5-HTR2A, and 5-HTR2C in the prefrontal cortex. These results demonstrate that early alterations to 5-HT signaling through SSRI exposure may disrupt nurturing parental behaviors and 5-HT receptor expression in affected female rat offspring.

摘要

在发育中的大脑中操纵 5-羟色胺(5-HT)水平会对大脑功能和行为产生一系列影响。例如,生命早期暴露于选择性 5-羟色胺再摄取抑制剂(SSRI)抗抑郁药会破坏背侧中缝功能,并引发异常的成年行为,如增加被动应对压力和快感缺失。然而,对于生命早期 5-HT 信号改变如何影响雌性后代的结果,包括关键的社会功能,如母性行为,了解甚少。本研究表明,生命早期 SSRI 暴露会破坏成年雌性后代的母性行为。给怀孕/产后的 Sprague-Dawley 大鼠用 SSRI 西酞普兰处理饮用水或提供常规自来水作为对照。雌性后代被抚养至成年并与未经处理的雄性交配。分娩后,我们观察了产后第 1-14 天白天和黑夜部分的母性行为。与对照组相比,有生命早期 SSRI 暴露史的母鼠表现出较少的母性行为,包括减少拱形哺乳、减少对幼鼠的舔舐和梳理,以及增加行为的不一致性。收集有和没有生命早期 SSRI 暴露史的母鼠的大脑,以测量参与母性行为的特定 5-HT 受体转录本(5HTR1A、-1B、-2A、-2C)的相对 mRNA 表达。生命早期 SSRI 暴露增强了中脑前脑区 5-HTR1A 和前额叶皮质 5-HTR1B、5-HTR2A 和 5-HTR2C 的表达。这些结果表明,通过 SSRI 暴露早期改变 5-HT 信号可能会破坏受影响的雌性大鼠后代的养育性父母行为和 5-HT 受体表达。

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