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Hypersensitivity to sertraline in the absence of hippocampal 5-HT1AR and 5-HTT gene expression changes following paternal corticosterone treatment

机译:父亲皮质酮治疗后海马5-HT1AR和5-HTT基因表达不存在时对舍曲林的超敏反应

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摘要

The male germ line is capable of transmitting a legacy of stress exposure to the next generation of offspring. This transgenerational process manifests by altering offspring affective behaviours, cognition and metabolism. Paternal early life trauma causes hippocampal serotonergic dysregulation in male offspring. We previously showed a transgenerational modification to male offspring anxiety-like behaviours by treatment of adult male breeders with corticosterone (CORT) prior to mating. In the present study, we used offspring from our paternal CORT model and characterised offspring serotonergic function by examining their responses to the 5HT1AR agonist, 8-OH-DPAT, and the selective serotonin reuptake inhibitor, sertraline. We also examined whether post-weaning environmental enrichment, a paradigm well-known to modulate serotonergic signalling in the brain, had the capacity to normalise the anxiety phenotype of male offspring. Finally, we assessed gene expression levels of 5HT1AR and serotonin transporter in the offspring hippocampus to determine whether deficits in gene transcription contributed to the male-only anxiety phenotype. We report that male and female offspring of CORT-treated fathers are hypersensitive to sertraline but have normal hypothermic responses to 8-OH-DPAT. No deficits in htr1a and sert were found in association with paternal CORT treatment, and environmental enrichment did not rescue the anxiety phenotype of male offspring on the elevated-plus maze. These findings indicate that varying forms of paternal stress exert different effects on offspring brain serotonergic function.
机译:雄性种系能够将压力暴露的遗产传播给下一代后代。通过改变后代的情感行为,认知和新陈代谢来体现这种跨代过程。父亲早期生命创伤导致雄性后代的海马血清素能失调。我们以前通过交配之前用皮质酮(CORT)治疗成年雄性种鸽,证明了对雄性后代焦虑样行为的跨世代修饰。在本研究中,我们使用了父亲CORT模型的后代,并通过检查后代对5HT1AR激动剂8-OH-DPAT和选择性5-羟色胺再摄取抑制剂舍曲林的反应来表征后代血清素能功能。我们还检查了断奶后环境富集(一种众所周知的调节大脑中血清素能信号传导的范例)是否具有使雄性后代焦虑表型正常化的能力。最后,我们评估了后代海马中5HT1AR和5-羟色胺转运蛋白的基因表达水平,以确定基因转录缺陷是否促成仅男性焦虑症表型。我们报告说,接受CORT治疗的父亲的男性和女性后代对舍曲林过敏,但对8-OH-DPAT的体温反应正常。在父本CORT治疗中,未发现htr1a和sert缺陷,并且环境富集并不能挽救高架迷宫中雄性后代的焦虑表型。这些发现表明,不同形式的父亲压力对后代的脑血清素能功能具有不同的作用。

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