首页> 美国卫生研究院文献>Frontiers in Neuroscience >Subjecting Dams to Early Life Stress and Perinatal Fluoxetine Treatment Differentially Alters Social Behavior in Young and Adult Rat Offspring
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Subjecting Dams to Early Life Stress and Perinatal Fluoxetine Treatment Differentially Alters Social Behavior in Young and Adult Rat Offspring

机译:使大坝经受早期生活压力和围产期氟西汀的治疗,差异性地改变了幼年和成年大鼠后代的社会行为

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摘要

Recently, the putative association between selective serotonin reuptake inhibitor (SSRI) exposure during pregnancy and the development of social disorders in children has gained increased attention. However, clinical studies struggle with the confounding effects of maternal depression typically co-occurring with antidepressant treatment. Furthermore, preclinical studies using an animal model of maternal depression to study effects of perinatal SSRI exposure on offspring social behavior are limited. Therefore, the aim of this study was to investigate effects of perinatal fluoxetine exposure on juvenile and adult social behavior in male and female rat offspring, using an animal model of maternal vulnerability. We exposed heterozygous serotonin transporter (SERT) deficient female rats to early life maternal separation stress, and used this as a model for maternal vulnerability. Control and early life stressed heterozygous serotonin transporter knockout (SERT) dams were treated with the SSRI fluoxetine or vehicle throughout gestation and lactation. Subsequently, both male and female wildtype (SERT+/+) and heterozygous (SERT+/-) rat offspring were tested for pup ultrasonic vocalizations (USVs), juvenile social play behavior and adult social interaction. Fluoxetine treatment of the dams resulted in a reduced total USV duration in pups at postnatal day 6, especially in SERT+/+ males. Perinatal fluoxetine exposure lowered social play behavior in male offspring from both control and early life stressed dams. However, in females a fluoxetine-induced reduction in juvenile play behavior was only present in offspring from control dams. Offspring genotype did not affect juvenile play behavior. Despite fluoxetine-induced behavioral effects at juvenile age, fluoxetine reduced male adult social behavior in offspring from control dams only. Effects of fluoxetine on female adult social behavior were virtually absent. Interestingly, early life stress in dams increased adult social exploration in vehicle exposed SERT+/+ female offspring and total social behavior in fluoxetine exposed adult SERT+/- male offspring. Furthermore, SERT+/- males appeared less social during adulthood compared to SERT+/+ males. Overall, the present study shows that chronic blockade of the serotonin transporter by fluoxetine during early development has a considerable impact on pup USVs, juvenile social play behavior in both male and female offspring, and to a lesser extent on male social interaction in adulthood.
机译:最近,怀孕期间选择性5-羟色胺再摄取抑制剂(SSRI)暴露与儿童社交障碍的发展之间的推测联系已引起越来越多的关注。然而,临床研究难以克服通常与抗抑郁药同时发生的产妇抑郁症的混杂效应。此外,使用母体抑郁症动物模型研究围产期SSRI暴露对后代社交行为影响的临床前研究有限。因此,本研究的目的是使用母体脆弱性动物模型研究围产期氟西汀暴露对雄性和雌性大鼠后代少年和成年社交行为的影响。我们将杂合性5-羟色胺转运蛋白(SERT)缺陷的雌性大鼠暴露于生命早期的母体分离应激,并将其用作母体脆弱性的模型。在整个妊娠和哺乳期间,均使用SSRI氟西汀或赋形剂处理对照和早期应激的杂合性血清素转运蛋白敲除(SERT)大坝。随后,对雄性和雌性野生型(SERT + / + )和杂合子(SERT +/- )大鼠后代进行幼仔超声发声(USV),青少年社交活动的测试行为和成人社交互动。氟西汀对大坝的治疗导致出生后第6天幼崽的总USV持续时间减少,特别是在SERT + / + 雄性中。围产期氟西汀暴露降低了控制和早期生活压力大坝的雄性后代的社交行为。然而,在雌性中,氟西汀诱导的青少年游戏行为减少仅存在于对照大坝的后代中。后代的基因型不影响青少年的游戏行为。尽管氟西汀在幼年时引起了行为影响,但氟西汀仅减少了对照大坝后代的成年男性社交行为。实际上没有氟西汀对女性成年社交行为的影响。有趣的是,大坝的早期生活压力增加了暴露于车辆的SERT + / + 雌性后代的成年社会探索,以及氟西汀暴露的成年SERT +/- 雄性后代的总体社会行为。此外,与SERT + / + 男性相比,成年男性SERT +/- 的社交活动较少。总体而言,本研究表明,氟西汀在早期发育过程中对5-羟色胺转运蛋白的慢性阻断对幼仔USV,雄性和雌性后代的青少年社交行为有相当大的影响,而对成年期男性社交互动的影响较小。

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