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非单调剂量反应关系的统计分析:暴露于甲醛的大鼠鼻细胞增殖的研究设计与分析

Statistical analysis of nonmonotonic dose-response relationships: research design and analysis of nasal cell proliferation in rats exposed to formaldehyde.

作者信息

Gaylor David W, Lutz Werner K, Conolly Rory B

机构信息

Gaylor and Associates, Eureka Springs, Arkansas 72631, USA.

出版信息

Toxicol Sci. 2004 Jan;77(1):158-64. doi: 10.1093/toxsci/kfh008. Epub 2003 Nov 4.

DOI:10.1093/toxsci/kfh008
PMID:14600280
Abstract

Statistical analyses of nonmonotonic dose-response curves are proposed, experimental designs to detect low-dose effects of J-shaped curves are suggested, and sample sizes are provided. For quantal data such as cancer incidence rates, much larger numbers of animals are required than for continuous data such as biomarker measurements. For example, 155 animals per dose group are required to have at least an 80% chance of detecting a decrease from a 20% incidence in controls to an incidence of 10% at a low dose. For a continuous measurement, only 14 animals per group are required to have at least an 80% chance of detecting a change of the mean by one standard deviation of the control group. Experimental designs based on three dose groups plus controls are discussed to detect nonmonotonicity or to estimate the zero equivalent dose (ZED), i.e., the dose that produces a response equal to the average response in the controls. Cell proliferation data in the nasal respiratory epithelium of rats exposed to formaldehyde by inhalation are used to illustrate the statistical procedures. Statistically significant departures from a monotonic dose response were obtained for time-weighted average labeling indices with an estimated ZED at a formaldehyde dose of 5.4 ppm, with a lower 95% confidence limit of 2.7 ppm. It is concluded that demonstration of a statistically significant bi-phasic dose-response curve, together with estimation of the resulting ZED, could serve as a point-of departure in establishing a reference dose for low-dose risk assessment.

摘要

本文提出了对非单调剂量反应曲线的统计分析方法,建议了用于检测J形曲线低剂量效应的实验设计,并给出了样本量。对于癌症发病率等计数资料,所需动物数量比生物标志物测量等连续资料要多得多。例如,每个剂量组需要155只动物,才能至少有80%的机会检测到低剂量时从对照组20%的发病率降至10%的发病率变化。对于连续测量,每组仅需14只动物,就能至少有80%的机会检测到均值变化一个对照组标准差。讨论了基于三个剂量组加对照组的实验设计,以检测非单调性或估计零等效剂量(ZED),即产生与对照组平均反应相等反应的剂量。用吸入甲醛的大鼠鼻呼吸上皮细胞增殖数据来说明统计程序。对于时间加权平均标记指数,在甲醛剂量为5.4 ppm时获得了与单调剂量反应有统计学显著差异的结果,其95%置信下限为2.7 ppm。得出的结论是,证明具有统计学显著意义的双相剂量反应曲线,并估计由此产生的ZED,可作为建立低剂量风险评估参考剂量的出发点。

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