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Long-term effects on hypothalamic neuropeptides after developmental exposure to chlorpyrifos in mice.

机译:在小鼠体内毒死rif暴露后对下丘脑神经肽的长期影响。

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BACKGROUND: Increasing evidence from animal and human studies indicates that chlorpyrifos (CPF), similar to other organophosphorus insecticides still widely used, is a developmental neurotoxicant. Developmental exposure to CPF in rodents induces sex-dimorphic behavioral changes at adulthood, including social and agonistic responses, which suggests that CPF may interfere with maturation of neuroendocrine mechanisms. OBJECTIVES: We assessed the hypothesis that CPF affects the levels of neurohypophyseal hormones acting as modulators of social behavior in mammals, such as oxytocin (OT), arginine vasopressin (AVP), and prolactin (PRL). METHODS: Pregnant female mice were orally administered with either vehicle (peanut oil) or 3 or 6 mg/kg CPF on gestational day (GD) 15 to GD18, and offspring were treated subcutaneously with either vehicle or 1 or 3 mg/kg CPF on postnatal days (PNDs) 11 to PND14. Dose levels were chosen to avoid systemic toxicity and inhibition of brain acetylcholinesterase. Offspring were sacrificed at 5 months of age, and expression of OT, AVP, and PRL was analyzed in the hypothalamus by Western blot or enzyme-linked immunosorbent assay (ELISA) analysis. RESULTS: Both male and female mice showed dose-related enhancement of OT expression, with males presenting the more intense effect. AVP expression was significantly reduced in male mice at the higher prenatal and postnatal dose. We observed no significant effect on PRL expression in either sex. Overall, outcomes were mainly attributable to fetal exposure, whereas postnatal doses appeared to potentiate the prenatal effects. CONCLUSIONS: Our data indicate that developmental exposure to CPF may permanently interfere with specific key signaling proteins of the hypothalamic peptidergic system, with time-, dose-, and sex-related effects still evident at adulthood.
机译:背景:动物和人体研究的越来越多的证据表明,毒死rif(CPF)与仍广泛使用的其他有机磷杀虫剂类似,是一种发育中的神经毒剂。啮齿动物的CPF发育暴露会在成年期引起性别-双态行为变化,包括社交和激动反应,这表明CPF可能会干扰神经内分泌机制的成熟。目的:我们评估了以下假设:CPF影响神经下垂体激素的水平,后者是催产素(OT),精氨酸加压素(AVP)和催乳素(PRL)充当哺乳动物社会行为的调节剂。方法:妊娠雌性小鼠在妊娠第15天至GD18时口服赋形剂(花生油)或3或6 mg / kg CPF口服,对后代皮下注射赋形剂或1或3 mg / kg CPF。产后天数(PND)11至PND14。选择剂量水平以避免全身毒性和抑制脑乙酰胆碱酯酶。在5个月大时处死后代,并通过Western印迹或酶联免疫吸附分析(ELISA)分析下丘脑中OT,AVP和PRL的表达。结果:雄性和雌性小鼠均表现出剂量相关的OT表达增强,雄性小鼠表现出更强的作用。在较高的产前和产后剂量下,雄性小鼠的AVP表达显着降低。我们观察到对两种性别的PRL表达均无明显影响。总体而言,结局主要归因于胎儿暴露,而产后剂量似乎能增强产前影响。结论:我们的数据表明,发展性暴露于CPF可能会永久干扰下丘脑肽能系统的特定关键信号蛋白,在成年期仍明显存在时间,剂量和性别相关的影响。

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