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Reproducibility of the Dose‐Response Curve of Steroid‐Induced Cleft Palate in Mice

机译:类固醇诱导的小鼠腭裂剂量反应曲线的可重复性

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Pregnant CD‐1 mice were exposed to cortisone acetate at doses ranging from 20 to 100 mg/kg/ day on days 10‐13 by oral and intramuscular routes. Multiple replicate assays were conducted under identical conditions to assess the reproducibility of the dose–response curve for cleft palate. The data were fitted to the probit, logistic, multistage or Armitage‐Doll, and Weibull dose‐response model separately for each route of exposure. The curves were then tested for parallel slopes (probit and logistic models) or coincidence of model parameters (multistage and Weibull models). The 19 replicate experiments had a wide range of slope estimates, wider for the oral than for the intramuscular experiments. For all models and both routes of exposure the null hypothesis of equality of slopes was rejected at a significant level ofp<0.001. For the intramuscular group of replicates, rejection of slope equality could in part be explained by not maintaining a standard dosing regime. The rejection of equivalence of dose‐response curves from replicate studies showed that it is difficult to reproduce dose‐response data of a single study within the limits defined by the dose‐response model. This has important consequences for quantitative risk assessment, public health measures, or development of mechanistic theories which are typically based on a single
机译:怀孕的CD-1小鼠在第10-13天通过口服和肌肉注射途径暴露于醋酸可的松,剂量范围为20至100mg / kg /天。在相同条件下进行多次重复测定,以评估腭裂剂量-反应曲线的可重复性。对于每种暴露途径,数据分别拟合到概率模型、逻辑模型、多阶段模型或阿米蒂奇-娃娃模型和威布尔剂量反应模型中。然后对曲线进行平行斜率(概率和逻辑模型)或模型参数的重合(多阶段和威布尔模型)的重合测试。19 个重复实验的斜率估计范围很广,口服实验比肌肉注射实验更宽。对于所有模型和两种暴露途径,斜率相等的原假设在p<0.001的显著水平上被拒绝。对于肌肉注射重复组,斜率相等的拒绝可以部分解释为没有保持标准的给药方案。重复研究对剂量反应曲线等效性的否定表明,在剂量反应模型定义的范围内,很难重现单个研究的剂量反应数据。这对定量风险评估、公共卫生措施或通常基于单一的机理理论的发展具有重要影响

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