大鼠生殖前应激和氟西汀治疗会影响后代A-to-I RNA编辑、基因表达和社会行为

IF 4.8 Q1 GENETICS & HEREDITY
Environmental Epigenetics Pub Date : 2018-08-08 eCollection Date: 2018-04-01 DOI:10.1093/eep/dvy021
Hiba Zaidan, Gokul Ramaswami, Michal Barak, Jin B Li, Inna Gaisler-Salomon
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引用次数: 0

摘要

腺苷到肌苷的RNA编辑是一种表观遗传过程,需要在作用于RNA的腺苷脱氨酶(ADARs)的催化下对双链RNA分子进行特定位点修饰。最近,我们利用多重微流控 PCR 和深度测序技术发现,让青春期雌性大鼠在繁殖前长期暴露于不可预测的压力下会影响其新生后代的前额叶皮层和杏仁核的编辑,尤其是5-羟色胺受体5-HT2c(由Htr2c编码)的编辑。在这里,我们使用同样的技术来确定应激后、生殖前母体使用氟西汀(5 毫克/千克,7 天)是否会逆转应激对编辑的影响。我们还检测了这些区域中ADAR酶的mRNA表达,并询问成年后代的社会行为是否会因母体暴露于应激和/或氟西汀而发生改变。母体使用氟西汀会改变出生后代杏仁核中的Htr2c编辑,增强前额叶皮层中Htr2c mRNA和RNA编辑酶的表达,并逆转生殖前应激对该区域Htr2c编辑的影响。此外,母体氟西汀治疗会增强对照组大鼠和应激暴露大鼠后代之间谷氨酸受体编辑的差异,并导致成年后代的社会偏好增强。我们的研究结果表明,妊娠前氟西汀治疗会以区域特异性的方式影响新生后代大脑中的RNA编辑和编辑酶表达模式,并与生殖前应激相互作用。总之,这些研究结果表明,即使在妊娠前停止治疗,氟西汀治疗也会影响后代大脑中的血清素能信号传导,而且其影响可能取决于之前所承受的压力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Pre-reproductive stress and fluoxetine treatment in rats affect offspring A-to-I RNA editing, gene expression and social behavior.

Pre-reproductive stress and fluoxetine treatment in rats affect offspring A-to-I RNA editing, gene expression and social behavior.

Pre-reproductive stress and fluoxetine treatment in rats affect offspring A-to-I RNA editing, gene expression and social behavior.

Pre-reproductive stress and fluoxetine treatment in rats affect offspring A-to-I RNA editing, gene expression and social behavior.

Adenosine to inosine RNA editing is an epigenetic process that entails site-specific modifications in double-stranded RNA molecules, catalyzed by adenosine deaminases acting on RNA (ADARs). Using the multiplex microfluidic PCR and deep sequencing technique, we recently showed that exposing adolescent female rats to chronic unpredictable stress before reproduction affects editing in the prefrontal cortex and amygdala of their newborn offspring, particularly at the serotonin receptor 5-HT2c (encoded by Htr2c). Here, we used the same technique to determine whether post-stress, pre-reproductive maternal treatment with fluoxetine (5 mg/kg, 7 days) reverses the effects of stress on editing. We also examined the mRNA expression of ADAR enzymes in these regions, and asked whether social behavior in adult offspring would be altered by maternal exposure to stress and/or fluoxetine. Maternal treatment with fluoxetine altered Htr2c editing in offspring amygdala at birth, enhanced the expression of Htr2c mRNA and RNA editing enzymes in the prefrontal cortex, and reversed the effects of pre-reproductive stress on Htr2c editing in this region. Furthermore, maternal fluoxetine treatment enhanced differences in editing of glutamate receptors between offspring of control and stress-exposed rats, and led to enhanced social preference in adult offspring. Our findings indicate that pre-gestational fluoxetine treatment affects patterns of RNA editing and editing enzyme expression in neonatal offspring brain in a region-specific manner, in interaction with pre-reproductive stress. Overall, these findings imply that fluoxetine treatment affects serotonergic signaling in offspring brain even when treatment is discontinued before gestation, and its effects may depend upon prior exposure to stress.

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来源期刊
Environmental Epigenetics
Environmental Epigenetics GENETICS & HEREDITY-
CiteScore
6.50
自引率
5.30%
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审稿时长
17 weeks
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