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皮肤接触粘性油产品的致癌潜力指数的制定。

Development of a carcinogenic potency index for dermal exposure to viscous oil products.

作者信息

Brandt H C, Booth E D, de Groot P C, Watson W P

机构信息

Shell International Oil Products BV, Shell Research and Technology Centre, Amsterdam, The Netherlands.

出版信息

Arch Toxicol. 1999 Apr-May;73(3):180-8. doi: 10.1007/s002040050604.

Abstract

Polycyclic aromatic compounds (PACs) present in oil streams and formulated products are important determinants of possible carcinogenicity. Following dermal exposures the transport of the PACs from oil (the carrier) into the skin is a factor that may affect macromolecular (DNA) adduct formation and thus determine carcinogenicity. We have developed a mathematical model, which describes the flux into the skin for a representative carcinogenic PAC, benzo(a)pyrene. The model is based on measurements of the amount of benzo(a)pyrene bound to skin DNA or blood observed in mouse skin painting studies. The degree of adduct formation from a particular oil product, which we term the Bioavailability Index (BI), was shown to be a function of both the viscosity of the oil product, which affected the transport of the PAC through the carrier, and the aromaticity, which affected the partition of PAC between the carrier and the skin. Literature data were analysed from mouse skin painting studies with mineral oils of known carcinogenicity. A linear relationship was shown between the amount of DNA adduct formation, expressed as alkylation frequency, and the arithmetic product of the total (3-6) ring PAC content and the BI, which we have termed the Carcinogenic Potency Index (CPI). Comparison of literature data on DNA alkylation frequencies for oil products and their carcinogenicity indicated that oils giving rise to an alkylation frequency below a certain threshold (ca. 1 adduct in 10(8) nucleotides) are non-carcinogenic to mouse skin. This threshold level can be translated into a value for the CPI, below which the genotoxic carcinogenic risk arising from skin contact with the oil product is considered to be negligible. The CPI for bitumens is well below this value, being both due to the low BI from bitumen, but more so, due to their low PAC content. For some bitumens diluted with solvents, i.e. cutback-bitumens, the CPI may exceed this value, indicating a possible carcinogenic risk for some of the cutback-bitumens. The main determining factor is the PAC content which is principally determined by the nature of the diluent used.

摘要

油流和配方产品中存在的多环芳烃化合物(PACs)是可能致癌性的重要决定因素。经皮肤接触后,PACs从油(载体)进入皮肤的转运是一个可能影响大分子(DNA)加合物形成从而决定致癌性的因素。我们开发了一个数学模型,该模型描述了代表性致癌PAC苯并(a)芘进入皮肤的通量。该模型基于在小鼠皮肤涂抹研究中观察到的与皮肤DNA或血液结合的苯并(a)芘量的测量。特定油品形成加合物的程度,我们称之为生物利用度指数(BI),它被证明是油品粘度和芳香性的函数,其中粘度影响PAC通过载体的转运,芳香性影响PAC在载体和皮肤之间的分配。分析了来自对已知致癌性矿物油进行小鼠皮肤涂抹研究的文献数据。以烷基化频率表示的DNA加合物形成量与总(3 - 6)环PAC含量和BI的算术乘积之间呈现线性关系,我们将该乘积称为致癌潜能指数(CPI)。油品DNA烷基化频率及其致癌性的文献数据比较表明,导致烷基化频率低于某个阈值(约每10⁸个核苷酸中有1个加合物)的油品对小鼠皮肤无致癌性。这个阈值水平可以转化为CPI的值,低于该值时,因皮肤接触油品而产生的遗传毒性致癌风险被认为可以忽略不计。沥青的CPI远低于此值,这既是因为沥青的BI较低,但更主要的是由于其PAC含量较低。对于一些用溶剂稀释的沥青,即稀释沥青,CPI可能会超过该值,这表明一些稀释沥青可能存在致癌风险。主要决定因素是PAC含量,而PAC含量主要由所用稀释剂的性质决定。

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