Birnbaum L S
U.S. Environmental Protection Agency, Health Effects Research Laboratory, Research Triangle Park, North Carolina 27711.
Environ Health Perspect. 1994 Nov;102 Suppl 9(Suppl 9):157-67. doi: 10.1289/ehp.94102s9157.
Risk characterization involves hazard identification, determination of dose-response relationships, and exposure assessment. Improvement of the risk assessment process requires inclusion of the best available science. Recent findings in the area of dioxin toxicity have led to a major effort to reassess its risk. 2,3,7,8-Tetrachlorodibenzo-p-dioxin (TCDD), commonly referred to as "dioxin," is the most toxic member of a class of related chemicals including the polyhalogenated dibenzo-p-dioxins, dibenzofurans, biphenyls, naphthalenes, azo- and azoxy-benzenes, whose toxicities can be expressed as fractional equivalencies of TCDD. These chemicals exert their effects through interaction with a specific intracellular protein, the Ah receptor. While binding to the receptor is necessary, it is not sufficient to bring about a chain of events leading to various responses including enzyme induction, immunotoxicity, reproductive and endocrine effects, developmental toxicity, chloracne, tumor promotion, etc. Some of these responses appear to be linear at low doses. Immunotoxicity and effects on the reproductive system appear to be among the most sensitive responses. The Ah receptor functions as a transcriptional enhancer, interacting with a number of other regulatory proteins (heat shock proteins, kinases, translocases, DNA binding species). Interaction with specific base sequences in the DNA appear to be modulated by the presence of other growth factors, hormones and their receptors as well as other regulatory proteins. Thus, dioxin appears to function as a hormone, initiating a cascade of events that is dependent upon the environment of each cell and tissue. While Ah receptor variants exist, all vertebrates examined have demonstrated such a protein with similar numbers of receptors and binding affinity for TCDD. Most species respond similarly to dioxin and related compounds. While a given species may be an outlier for a given response, it will behave like other animals for other responses. For both in vivo and in vitro end points where animal and human data exist, such as enzyme induction, chloracne, immunotoxicity, developmental toxicity, and cancer, the sensitivity of humans appears similar to that of experimental animals. Current levels of environmental exposure to this class of chemicals may be resulting in subtle responses in populations at special risk such as subsistence fisherman and the developing infant, as well as in the general population. Increased understanding of the mechanism of dioxin's effects as well as elucidation of exposure-dose relationships is leading to the development of a biologically based dose-response model in the ongoing process of incorporating the best science into the risk assessment of TCDD and related compounds.
风险特征描述涉及危害识别、剂量反应关系的确定以及暴露评估。改进风险评估过程需要纳入现有的最佳科学知识。二噁英毒性领域的最新研究结果促使人们大力重新评估其风险。2,3,7,8 - 四氯二苯并 - p - 二噁英(TCDD),通常被称为“二噁英”,是一类相关化学物质中毒性最强的成员,这类化学物质包括多卤代二苯并 - p - 二噁英、二苯并呋喃、联苯、萘、偶氮苯和氧化偶氮苯,它们的毒性可以表示为TCDD的分数当量。这些化学物质通过与一种特定的细胞内蛋白质——芳烃受体(Ah受体)相互作用发挥作用。虽然与受体结合是必要的,但这不足以引发一系列导致各种反应的事件,这些反应包括酶诱导、免疫毒性、生殖和内分泌影响、发育毒性、氯痤疮、肿瘤促进等。其中一些反应在低剂量时似乎呈线性关系。免疫毒性和对生殖系统的影响似乎是最敏感的反应之一。Ah受体作为一种转录增强子,与许多其他调节蛋白(热休克蛋白、激酶、转位酶、DNA结合蛋白)相互作用。与DNA中特定碱基序列的相互作用似乎受到其他生长因子、激素及其受体以及其他调节蛋白的存在的调节。因此,二噁英似乎起着激素的作用,引发一系列依赖于每个细胞和组织环境的事件。虽然存在Ah受体变体,但所有被检测的脊椎动物都证明存在这样一种蛋白质,其受体数量和对TCDD的结合亲和力相似。大多数物种对二噁英和相关化合物的反应相似。虽然给定物种对于给定反应可能是个例外,但它在其他反应中会表现得与其他动物相似。对于存在动物和人类数据的体内和体外终点指标,如酶诱导、氯痤疮、免疫毒性、发育毒性和癌症,人类的敏感性似乎与实验动物相似。目前这类化学物质的环境暴露水平可能正在导致处于特殊风险的人群,如自给渔民和发育中的婴儿,以及一般人群出现微妙的反应。对二噁英作用机制的进一步了解以及对暴露 - 剂量关系的阐明,正在促使在将最佳科学知识纳入TCDD和相关化合物风险评估的持续过程中,开发基于生物学的剂量反应模型。