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首页> 外文期刊>Journal of biomedical informatics. >MPM: A knowledge-based functional model of medical practice
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MPM: A knowledge-based functional model of medical practice

机译:MPM:基于知识的医学实践功能模型

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Recent studies have reported that bisphenol A (BPA) influences brain development in fetal exposure to mice. The X-chromosome codes many neurodevelopment-related genes leading to abnormal development, such as mental retardation and intellectual deficiency. For females, most of expressions of X-linked genes are regulated by X-chromosome inactivation (XCI), which occurs during fetal period, and this mechanism is regulated by Xist and its antisense, Tsix. To clarify the possibility of X-mediated effect as a mechanism of neurodevelopmental disorders by BPA, pregnant ICR mice were orally administered 0.02 or 50 mg/kg of BPA on gestational days 6 and 15. Postnatally at days 2, 4 and weeks 3 and 7, mRNA expression of XCI-regulating factors (Xist and Tsix), X-linked neurodevelopment-related genes (Fmr1, Gdi1, Nlgn3, Pak3 and Ophn1), and sexual differentiation-related genes (ERα, ERβ and AR) were examined in cerebrums of female pups. Anogenital distance (AGD) and serum estradiol were also examined. In the 50 mg/kg exposed-group, reduced Xist, Fmr1, Gdi1, Nlgn3, and Pak3 and increased Tsix were observed simultaneously. Moderately reduced Xist, Gdi1, Nlgn3 and Pak3 were observed at 0.02 mg/kg BPA. ERα, ERβ and AR expression changes, shortened AGDs and reduced estradiol levels were observed in each exposure group. Fetal exposure to BPA changed expression of XCI-regulating factors and may alter the expression levels of X-linked neurodevelopment-related genes disrupting the XCI mechanism and function. This X-mediated effect is considered one of the mechanisms of various BPA-induced neurodevelopmental disorders.
机译:最近的研究报道,双酚A(BPA)影响胎儿与小鼠接触时的大脑发育。 X染色体编码许多与神经发育相关的基因,这些基因导致异常发育,例如智力低下和智力缺陷。对于女性而言,大多数X连锁基因的表达都受到胎儿期发生的X染色体失活(XCI)的调节,这种机制受Xist及其反义词Tsix的调节。为了阐明X介导的作用可能是BPA引起神经发育障碍的机制,在妊娠第6和15天口服孕产ICR小鼠口服0.02或50 mg / kg BPA,在产后第2、4和3和7周进行口服,检查XCI调节因子(Xist和Tsix)的mRNA表达,X连锁神经发育相关基因(Fmr1,Gdi1,Nlgn3,Pak3和Ophn1)以及性分化相关基因(ERα,ERβ和AR)。的幼崽。还检查了肛门生殖器距离(AGD)和血清雌二醇。在50 mg / kg暴露组中,同时观察到Xist,Fmr1,Gdi1,Nlgn3和Pak3降低,而Tsix升高。在0.02 mg / kg BPA下观察到适度降低的Xist,Gdi1,Nlgn3和Pak3。在每个暴露组中观察到ERα,ERβ和AR表达变化,AGD缩短和雌二醇水平降低。胎儿接触BPA会改变XCI调节因子的表达,并可能改变X连锁的神经发育相关基因的表达水平,从而破坏XCI的机制和功能。这种X介导的作用被认为是各种BPA诱导的神经发育障碍的机制之一。

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