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Developmental and behavioral neurotoxicity of endocrine disrupting chemicals.

机译:内分泌干​​扰物的发育和行为神经毒性。

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Endocrine disrupting chemicals (EDCs) are environmental contaminants that mimic or interfere with hormones. Many EDCs are estrogenic and may have the potential to cause alterations in reproduction or development at environmental exposure levels. The brain of rodents is extremely sensitive to estradiol and has long been a model for sexual differentiation. The hypothesis is that sexual differentiation of the rat brain is altered after exposure to EDCs during estrogen-sensitive periods of development and may be a model for studying mechanisms of action of EDCs. Prenatal exposure to 5 mg/kg of the estrogenic pesticide, chlordecone (CD), on day 16 of gestation altered sexually differentiated behaviors and brain morphology. Exposed female rats had decreased anxiety in the open field, and increased homotypic and heterotypic sex behaviors as compared to female controls. Exposed male rats had no change in activity levels in the open field or elevated plus maze, but had increased homotypic and heterotypic sex behaviors as compared to male controls. The volume of the sexually dimorphic nucleus of the preoptic area (SDN-POA), a morphological measure of exposure to estrogen during development, was not different between CD-exposed and control adult animals of either gender. When SDN-POA volume was analyzed during the neonatal period, prenatal CD exposure increased SDN-POA volume in female rats at postnatal day (PN) 6--8. Increased incidence of pyknotic cells in the SDN-POA occurred at PN 8 and may explain the return to control values at PN 10. Prenatal exposure to 5 mug/kg of the synthetic estrogen diethylstilbestrol (DES), caused a similar increase in SDN volume at PN 6, but not at PN 12 or 18, and exposure to 5 mg/kg bisphenol A (BPA), a weak estrogen in plastics, did not alter SDN-POA volume. In conclusion, prenatal exposure to relatively low doses of some EDCs altered the function and development of the brain in male and female rats. Changes in the SDN-POA volume occurred in females only during the neonatal period and were associated with changes in cell death. The transient effects detected in the SDN-POA suggest that developmental changes may have occurred in brain regions involved in adult behavior.
机译:破坏内分泌的化学物质(EDC)是模仿或干扰激素的环境污染物。许多EDC具有雌激素性,并可能在环境暴露水平下引起繁殖或发育变化。啮齿动物的大脑对雌二醇极为敏感,长期以来一直是性别分化的模型。假设是在雌激素敏感的发育阶段,暴露于EDCs后大鼠脑的性别分化会改变,这可能是研究EDCs作用机理的模型。妊娠第16天,产前暴露于5 mg / kg的雌激素杀虫剂十氯酮(CD),会改变性分化行为和大脑形态。与雌性对照相比,暴露的雌性大鼠在旷野中的焦虑减轻,同型和异型性行为增加。暴露的雄性大鼠在旷野或升高的迷宫中的活动水平没有变化,但是与雄性对照相比,其同型和异型性行为增加。暴露于CD的成年动物和对照组的雌雄同体,视前区性二形核(SDN-POA)的体积(发育过程中暴露于雌激素的形态学指标)没有差异。在新生儿期分析SDN-POA量时,产前CD暴露(PN)6--8时,产前CD暴露会增加雌性大鼠的SDN-POA量。 SDN-POA中泌尿生殖细胞的发生率增加在PN 8发生,这可能解释了PN 10的控制值恢复。产前暴露于5杯/ kg的合成雌激素二乙基己烯雌酚(DES),导致SDN体积在类似情况下增加。 PN 6,而不是PN 12或18,并且暴露于5 mg / kg双酚A(BPA)(塑料中的雌性激素较弱)不会改变SDN-POA的量。总之,产前暴露于相对低剂量的一些EDC会改变雄性和雌性大鼠大脑的功能和发育。 SDN-POA量的变化仅在新生儿期间发生,并且与细胞死亡的变化有关。在SDN-POA中检测到的瞬时效应表明,发育变化可能已经在涉及成人行为的大脑区域发生。

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