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首页> 外文期刊>Progress in Neuro-Psychopharmacology & Biological Psychiatry: An International Research, Review and News Journal >Exposure to the plasticizer, Di-(2-ethylhexyl) phthalate during juvenile period exacerbates autism-like behavior in adult BTBR T plus tf/J mice due to DNA hypomethylation and enhanced inflammation in brain and systemic immune cells
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Exposure to the plasticizer, Di-(2-ethylhexyl) phthalate during juvenile period exacerbates autism-like behavior in adult BTBR T plus tf/J mice due to DNA hypomethylation and enhanced inflammation in brain and systemic immune cells

机译:暴露于增塑剂,在幼年时期的二苯甲酸酯加剧了成年人BTBR T Plus TF / J小鼠中的自闭症样行为,由于DNA低甲基化和脑和全身免疫细胞的增强炎症

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Epigenetic modifications are known to play a crucial role in the behavioral modifications through regulation of gene expression. Environmental factors are known to regulate genetic transcription through DNA methylation which is one of the mechanisms of epigenetic modification. Di-2-ethylhexyl phthalate (DEHP) is one of the most abundant phthalate plasticizers in day-to-day products. Prenatal/postnatal DEHP administration has been reported to cause inflammation as well as behavioral dysregulation, however it is not known if exposure to DEHP during juvenile stage affects peripheral/neuronal inflammation and autism-like symptoms in BTBR mice at adulthood. This study investigated effect of DEHP exposure during juvenile period on DNA methylation (global DNA methylation/DNMT1 expression) and inflammation (IL-17A, IL-6, MCP-1, TNF-alpha) in CD4 + T cells/CD11c + DCs and cortex, and autism-like symptoms (three-chambered sociability test, self-grooming and marble burying test) in asocial BTBR and social C57 mice at adulthood. Our data reveal that BTBR mice exposed to DEHP during juvenile period have hypomethylated DNA/DNMT1 expression in CD11c + DCs and cortex as compared to vehicle-exposed BTBR mice. It was associated with upregulated inflammation in periphery [plasma IL-6/IL17A, CD11c + DCs (IL-6/MCP-1/TNF-alpha), and CD4+ T cells (IL-17A)] and cortex (IL-6, MCP-1, TNF-alpha), and aggravation in autism-like symptoms in DEHP-treated BTBR mice. These data propose that exposure of DEHP during juvenile period may affect autism-like behavior and inflammation in BTBR mice at adulthood through epigenetic regulation. Therefore, underlying genetic predisposition may play a crucial role in worsening of autistic symptoms in ASD subjects in adulthood if they are exposed to environmental pollutants such as DEHP during juvenile period.
机译:表观遗传修饰通过调节基因表达在行为修饰中起着至关重要的作用。已知环境因素通过DNA甲基化调节基因转录,这是表观遗传修饰的机制之一。邻苯二甲酸二-2-乙基己基酯(DEHP)是日常产品中含量最丰富的邻苯二甲酸酯增塑剂之一。据报道,产前/产后给予DEHP会引起炎症和行为失调,但尚不清楚幼年期接触DEHP是否会影响成年期BTBR小鼠的外周/神经元炎症和自闭症样症状。本研究调查了幼年期接触DEHP对成年期社交BTBR和社交C57小鼠CD4+T细胞/CD11c+DC和皮质中的DNA甲基化(整体DNA甲基化/DNMT1表达)和炎症(IL-17A、IL-6、MCP-1、TNF-α)的影响,以及自闭症样症状(三室社交测试、自我修饰和大理石掩埋测试)。我们的数据显示,与载体暴露的BTBR小鼠相比,幼年期暴露于DEHP的BTBR小鼠在CD11c+DC和皮质中有低甲基化DNA/DNMT1表达。在DEHP治疗的BTBR小鼠中,它与外周[血浆IL-6/IL-17A,CD11c+DC(IL-6/MCP-1/TNF-α)和CD4+T细胞(IL-17A)]和皮质(IL-6,MCP-1,TNF-α)的上调炎症以及自闭症样症状的加重有关。这些数据表明,幼年期接触DEHP可能通过表观遗传调节影响成年期BTBR小鼠的自闭症样行为和炎症。因此,如果ASD受试者在青少年时期接触DEHP等环境污染物,潜在的遗传易感性可能在成年期自闭症症状恶化中发挥关键作用。

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