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首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Statistical model to estimate a threshold dose and its confidence limits for the analysis of sublinear dose-response relationships, exemplified for mutagenicity data.
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Statistical model to estimate a threshold dose and its confidence limits for the analysis of sublinear dose-response relationships, exemplified for mutagenicity data.

机译:统计模型,用于估计阈值剂量及其置信极限,用于分析亚线性剂量-反应关系,以致突变性数据为例。

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摘要

Strongly sublinear dose-response relationships (slope increasing with dose) raise the question about a putative threshold dose below which no biologically relevant effect would be expected. A mathematical threshold with a break in the curve at the threshold dose is generally rejected for consequences of genotoxicity such as mutation, because proportionality between low dose and the rate of DNA-adduct formation is a reasonable hypothesis. In view of an increasing database for distinct deviation from linearity for mutagenicity, we offer a statistical model to analyze continuous response data and estimate a threshold dose together with its confidence limits, thereby taking data quality and degree of sublinearity into account. The simplest mathematical threshold model is a hockey stick defined by a low-dose part with slope zero at background level a to a theoretical break point at threshold dose td, followed by a linear increase above td with slope b. The function is y (dose d)=a+bx(d-td)x1([d>td]). Using the free statistics software package "R", we make a procedure available to estimate the parameters a, b, and td. Confidence intervals are calculated for all parameters at a significance level that can be defined by the user. If the lower limit of the confidence interval for td is >0, linearity is rejected. The procedure is illustrated by two examples. A small data set with three replicates per dose group, indicating a threshold for the induction of thymidine kinase mutants in L5178Y tk(+/-) mouse lymphoma cells treated with methyl methanesulfonate, did not achieve significance. On the other hand, the large data set reported in this issue (Gocke et al.) on lacZ mutants in bone marrow cells of transgenic mice treated with ethyl methanesulfonate strongly favoured the hockey stick model. The question of a theoretically expected linear dose-related increase below the threshold dose is addressed by linear regression of the data below the break point and estimation of an upper limit of the slope. The question of biological relevance of the resulting slope is discussed against the normal variation of background measures in the control group.
机译:强烈的亚线性剂量反应关系(斜率随剂量增加)提出了有关推定阈值剂量的问题,在该阈值以下不会产生生物学相关影响。由于遗传毒性的后果(例如突变),通常会拒绝在阈值剂量下出现曲线断裂的数学阈值,因为低剂量和DNA加合物形成速率之间的比例是合理的假设。鉴于不断增加的针对诱变性的线性差异明显的数据库,我们提供了一种统计模型来分析连续响应数据,并估计阈值剂量及其置信度,从而考虑数据质量和亚线性程度。最简单的数学阈值模型是一个曲棍球杆,它由一个低剂量的零件定义,其背景水平a处的斜率为零,到达阈值剂量td处的理论断裂点,然后线性上升至td以上且斜率b。函数为y(剂量d)= a + bx(d-td)x1([d> td])。使用免费的统计软件包“ R”,我们提供了一个过程来估计参数a,b和td。在用户可以定义的重要级别上计算所有参数的置信区间。如果td的置信区间的下限> 0,则线性被拒绝。该过程由两个示例说明。每个剂量组具有三个重复的小数据集,表明用甲磺酸甲酯处理的L5178Y tk(+/-)小鼠淋巴瘤细胞中胸苷激酶突变体的诱导阈值没有达到显着性。另一方面,本期报道(Gocke等人)有关使用甲磺酸乙酯处理的转基因小鼠骨髓细胞中lacZ突变体的大量数据,强烈支持曲棍球棒模型。通过低于折点以下的数据进行线性回归并估计斜率的上限,可以解决理论上预期的线性剂量相关的低于阈值剂量的增加的问题。针对对照组中背景测量值的正常变化,讨论了所得坡度的生物学相关性问题。

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