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首页> 外文期刊>Birth defects research, Part A. Clinical and molecular teratology >Methanol, formaldehyde, and sodium formate exposure in rat and mouse conceptuses: a potential role of the visceral yolk sac in embryotoxicity.
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Methanol, formaldehyde, and sodium formate exposure in rat and mouse conceptuses: a potential role of the visceral yolk sac in embryotoxicity.

机译:大鼠和小鼠概念中的甲醇,甲醛和甲酸钠暴露:内脏卵黄囊在胚胎毒性中的潜在作用。

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BACKGROUND: Methanol (CH3OH) is believed to be teratogenic based on rodent studies. The mouse is more sensitive than the rat, but mechanisms of toxicity and identification of teratogenic metabolites are uncertain. METHODS: Rat and mouse whole embryo cultures are used to distinguish toxicity of CH3OH and its metabolites, formaldehyde (HCHO) and formate (HCOONa), which are produced following transit through the visceral yolk sac (VYS), via addition to culture medium, or by direct embryonic exposure through microinjection into the amnion. RESULTS: Embryonic viability, increased dysmorphogenesis, and decreased growth parameters were altered in a dose-dependent fashion for each compound. Mouse embryos were more sensitive than rat, as indicated by significant decreases in viability at comparable, lower concentrations. HCHO produced dysmorphogenesis and caused embryolethality at nearly 1000-fold lower concentrations (0.004 mg/ml) than seen with either CH3OH or HCOONa. All agents produced incomplete axial rotation and delayed neural tube closure in mice, but only CH3OH elicited similar effects in the rat. Increased growth retardation, blood pooling in the head and VYS, enlarged pericardium, accumulation of necrotic matter in the amnion, and hypoplastic prosencephalon were observed in both species with all compounds. Microinjection of compounds into the amnion produced higher mortality in mouse and rat, compared to equimolar amounts added to the culture medium. CH3OH did not prevent neural tube closure in the rat when microinjected. CONCLUSIONS: HCHO is the most embryotoxic CH3OH metabolite and elicits the entire spectrum of lesions produced by CH3OH. The VYS serves a general protective role against toxicity and inherent differences in the embryonic metabolism of CH3OH may determine species sensitivity.
机译:背景:根据啮齿动物的研究,甲醇(CH3OH)被认为具有致畸性。小鼠比大鼠更敏感,但是毒性和致畸产物的鉴定机制尚不确定。方法:使用大鼠和小鼠全胚培养物来区分CH3OH及其代谢产物甲醛(HCHO)和甲酸盐(HCOONa)的毒性,这些代谢物是通过向内脏卵黄囊(VYS)转移,通过添加培养基或通过将微量注射到羊膜中直接胚胎暴露。结果:每种化合物的胚胎生存力,异常形成增加和生长参数降低均以剂量依赖性方式改变。小鼠胚胎比大鼠更敏感,这在较低的可比浓度下存活率显着降低表明。与CH3OH或HCOONa相比,HCHO产生了畸形,并导致胚胎致死率降低了近1000倍(0.004 mg / ml)。所有试剂在小鼠中均产生不完全的轴向旋转并延迟了神经管的闭合,但是只有CH3OH在大鼠中引起了相似的作用。在所有化合物中,这两种物种均观察到生长迟缓,头部和VYS的血池增加,心包增大,羊膜中坏死物质的积累以及前脑发育不良。与向培养基中添加等摩尔量的化合物相比,向羊膜中微量注射化合物可在小鼠和大鼠中产生更高的死亡率。微量注射时,CH3OH不能阻止大鼠神经管的闭合。结论:HCHO是最具胚胎毒性的CH3OH代谢产物,并引发CH3OH产生的整个病变范围。 VYS具有抗毒性的一般保护作用,CH3OH胚胎代谢中的固有差异可能决定物种的敏感性。

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