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首页> 外文期刊>International journal of toxicology >Oral (drinking water) developmental toxicity study of ammonium perchlorate in sprague-dawley rats.
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Oral (drinking water) developmental toxicity study of ammonium perchlorate in sprague-dawley rats.

机译:高氯酸铵对sprague-dawley大鼠的口服(饮用水)发育毒性研究。

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A developmental toxicity study was conducted with ammonium perchlorate (AP) in the drinking water at doses of 0.0, 0.01, 0.1, 1.0, and 30.0 mg/kg-day beginning 14 days before cohabitation and continuing through sacrifice. Twenty-four rats/group were cesarean-sectioned on day of gestation (DG) 21 and fetuses examined for visceral and skeletal alterations. An additional 16 litters/group were sacrificed on DG 21 for maternal and fetal serum TSH, T(3), and T(4) (thyroid-stimulating hormone, triiodothyronine, and thyroxine) levels and thyroid histopathology. Clinical and necropsy observations, body weights, feed and water consumption, and cesarean-sectioning parameters were comparable among the groups with only delays in ossification observed in the 30 mg/kg-day group. Maternal thyroid weights were increased in the 30.0 mg/kg-day group. Decreased colloid was present in male and female fetal thyroids in the 1.0 and 30.0 mg/kg-day groups. Maternal TSH was increased and T(4) was decreased at all levels, and T(3) was reduced at 30.0 mg/kg-day. Fetal TSH was increased at 1.0 and 30.0 mg/kg-day, T(4) was reduced at 30.0 mg/kg-day, and T(3) was decreased at all levels. The maternal no-observable-adverse-effect level (NOAEL) was 1.0 mg/kg-day; exposures of 30.0 mg/kg-day increased absolute and relative maternal thyroid weights and histopathology findings. The developmental NOAEL was 1.0 mg/kg-day; developmental delays in ossification occurred in the 30.0 mg/kg-day group. The colloid depletion in the thyroids and increased TSH and decreased T(3) and T(4) levels at lower exposures were considered adaptive and not adverse. No adverse effects on development at occurred levels that did not cause maternal toxicity. AP is not a selective developmental toxicant.
机译:在同居前14天开始,以0.0、0.01、0.1、1.0和30.0 mg / kg-day的剂量在饮用水中用高氯酸铵(AP)进行发育毒性研究。 24只大鼠/组在妊娠第21天进行剖腹产,检查胎儿的内脏和骨骼变化。 DG 21处死每组额外的16胎,用于母体和胎儿血清TSH,T(3)和T(4)(促甲状腺激素,三碘甲状腺素和甲状腺素)水平和甲状腺组织病理学检查。在各组之间的临床和尸检观察,体重,饲料和水的消耗以及剖宫产参数是可比较的,在30 mg / kg-day的组中仅观察到骨化延迟。 30.0 mg / kg-day组孕妇甲状腺重量增加。 1.0和30.0 mg / kg-day组的男性和女性胎儿甲状腺中胶体含量减少。母体TSH在所有水平上均升高而T(4)降低,而T(3)在30.0 mg / kg-day时降低。胎儿TSH在1.0和30.0 mg / kg-day时升高,T(4)在30.0 mg / kg-day时降低,而T(3)在所有水平上均降低。孕妇无不良反应水平(NOAEL)为1.0 mg / kg·天;每天30.0 mg / kg的暴露量会增加孕妇的绝对和相对甲状腺重量以及组织病理学发现。发育NOAEL为1.0 mg / kg-天; 30.0 mg / kg-day组发生骨化的发育延迟。在较低的暴露量下,甲状腺中的胶体耗竭和TSH升高以及T(3)和T(4)水平降低被认为是适应性的,而不是不利的。在不引起母体毒性的水平上,对发育没有不利影响。 AP不是选择性的发育毒物。

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