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丙烯酰胺:在评估人类摄入风险和安全性时对物种差异和非线性过程的考量。

Acrylamide: Consideration of species differences and nonlinear processes in estimating risk and safety for human ingestion.

作者信息

Gargas M L, Kirman C R, Sweeney L M, Tardiff R G

机构信息

The Sapphire Group, Inc, Dayton, OH, United States.

出版信息

Food Chem Toxicol. 2009 Apr;47(4):760-8. doi: 10.1016/j.fct.2008.12.032. Epub 2009 Jan 9.

DOI:10.1016/j.fct.2008.12.032
PMID:19166901
Abstract

Acrylamide in cooked foods results in wide-spread, low-level human exposure. Potential risks from dietary intake remain unclear due to apparent conflicting results from cancer bioassays conducted in rats that reported tumors and epidemiology studies that are suggestive but provide little or no evidence of increased cancer. Risk estimation often includes two common assumptions: (1) tumor response rates in test species can be extrapolated systematically to estimate human response rates and (2) tumor rates observed following high-dose exposures can be linearly extrapolated to predict response rates following low-dose exposures. The validity of these assumptions was evaluated for acrylamide based upon the examination of relevant toxicokinetic and toxicodynamic differences between humans and rats, including sources of nonlinearity that modify high to low dose extrapolation of cancer incidence. Important species differences and sources of nonlinearity are identified, and recommendations for addressing them within the quantitative framework of a PBTK/TD model are discussed. These differences are likely to estimate risk levels up to several orders of magnitude lower in humans than in rats. Quantitative inclusion of these TK/TD factors will more closely estimate actual human cancer risk derived from high-dose rodent studies, since detoxification processes for acrylamide and glycidamide appear adequately protective against toxicity from human dietary doses.

摘要

熟食中的丙烯酰胺会导致人类广泛的低水平接触。由于在大鼠身上进行的癌症生物测定报告了肿瘤,而流行病学研究虽有暗示但几乎没有或没有提供癌症增加的证据,饮食摄入的潜在风险仍不明确。风险评估通常包括两个常见假设:(1)测试物种中的肿瘤反应率可以系统地外推以估计人类反应率;(2)高剂量暴露后观察到的肿瘤发生率可以线性外推以预测低剂量暴露后的反应率。基于对人和大鼠之间相关毒代动力学和毒效动力学差异的研究,包括改变癌症发病率从高剂量到低剂量外推的非线性来源,对这些假设对丙烯酰胺的有效性进行了评估。确定了重要的物种差异和非线性来源,并讨论了在PBTK/TD模型的定量框架内解决这些问题的建议。这些差异可能使人类的风险水平估计比大鼠低几个数量级。由于丙烯酰胺和缩水甘油酰胺的解毒过程似乎对人类饮食剂量的毒性有足够的保护作用,在定量中纳入这些TK/TD因素将更准确地估计从高剂量啮齿动物研究得出的实际人类癌症风险。

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Acrylamide: Consideration of species differences and nonlinear processes in estimating risk and safety for human ingestion.丙烯酰胺:在评估人类摄入风险和安全性时对物种差异和非线性过程的考量。
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