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一项针对石棉相关癌症风险的荟萃分析,该分析涉及纤维大小和矿物类型。

A meta-analysis of asbestos-related cancer risk that addresses fiber size and mineral type.

作者信息

Berman D Wayne, Crump Kenny S

机构信息

Aeolus, Inc, Albany, California 94706-1026, USA.

出版信息

Crit Rev Toxicol. 2008;38 Suppl 1:49-73. doi: 10.1080/10408440802273156.

Abstract

Quantitative estimates of the risk of lung cancer or mesothelioma in humans from asbestos exposure made by the U.S. Environmental Protection Agency (EPA) make use of estimates of potency factors based on phase-contrast microscopy (PCM) and obtained from cohorts exposed to asbestos in different occupational environments. These potency factors exhibit substantial variability. The most likely reasons for this variability appear to be differences among environments in fiber size and mineralogy not accounted for by PCM. In this article, the U.S. Environmental Protection Agency (EPA) models for asbestos-related lung cancer and mesothelioma are expanded to allow the potency of fibers to depend upon their mineralogical types and sizes. This is accomplished by positing exposure metrics composed of nonoverlapping fiber categories and assigning each category its own unique potency. These category-specific potencies are estimated in a meta-analysis that fits the expanded models to potencies for lung cancer (KL's) or mesothelioma (KM's) based on PCM that were calculated for multiple epidemiological studies in our previous paper (Berman and Crump, 2008). Epidemiological study-specific estimates of exposures to fibers in the different fiber size categories of an exposure metric are estimated using distributions for fiber size based on transmission electron microscopy (TEM) obtained from the literature and matched to the individual epidemiological studies. The fraction of total asbestos exposure in a given environment respectively represented by chrysotile and amphibole asbestos is also estimated from information in the literature for that environment. Adequate information was found to allow KL's from 15 epidemiological studies and KM's from 11 studies to be included in the meta-analysis. Since the range of exposure metrics that could be considered was severely restricted by limitations in the published TEM fiber size distributions, it was decided to focus attention on four exposure metrics distinguished by fiber width: "all widths," widths > 0.2 micro m, widths < 0.4 microm, and widths < 0.2 microm, each of which has historical relevance. Each such metric defined by width was composed of four categories of fibers: chrysotile or amphibole asbestos with lengths between 5 microm and 10 microm or longer than 10 microm. Using these metrics three parameters were estimated for lung cancer and, separately, for mesothelioma: KLA, the potency of longer (length > 10 microm) amphibole fibers; rpc, the potency of pure chrysotile (uncontaminated by amphibole) relative to amphibole asbestos; and rps, the potency of shorter fibers (5 microm < length < 10 microm) relative to longer fibers. For mesothelioma, the hypothesis that chrysotile and amphibole asbestos are equally potent (rpc = 1) was strongly rejected by every metric and the hypothesis that (pure) chrysotile is nonpotent for mesothelioma was not rejected by any metric. Best estimates for the relative potency of chrysotile ranged from zero to about 1/200th that of amphibole asbestos (depending on metric). For lung cancer, the hypothesis that chrysotile and amphibole asbestos are equally potent (rpc = 1) was rejected (p < or = .05) by the two metrics based on thin fibers (length < 0.4 microm and < 0.2 microm) but not by the metrics based on thicker fibers. The "all widths" and widths < 0.4 microm metrics provide the best fits to both the lung cancer and mesothelioma data over the other metrics evaluated, although the improvements are only marginal for lung cancer. That these two metrics provide equivalent (for mesothelioma) and nearly equivalent (for lung cancer) fits to the data suggests that the available data sets may not be sufficiently rich (in variation of exposure characteristics) to fully evaluate the effects of fiber width on potency. Compared to the metric with widths > 0.2 microm with both rps and rpc fixed at 1 (which is nominally equivalent to the traditional PCM metric), the "all widths" and widths < 0.4 microm metrics provide substantially better fits for both lung cancer and, especially, mesothelioma. Although the best estimates of the potency of shorter fibers (5 < length < 10 microm) is zero for the "all widths" and widths < 0.4 microm metrics (or a small fraction of that of longer fibers for the widths > 0.2 microm metric for mesothelioma), the hypothesis that these shorter fibers were nonpotent could not be rejected for any of these metrics. Expansion of these metrics to include a category for fibers with lengths < 5 microm did not find any consistent evidence for any potency of these shortest fibers for either lung cancer or mesothelioma. Despite the substantial improvements in fit over that provided by the traditional use of PCM, neither the "all widths" nor the widths < 0.4 microm metrics (or any of the other metrics evaluated) completely resolve the differences in potency factors estimated in different occupational studies. Unresolved in particular is the discrepancy in potency factors for lung cancer from Quebec chrysotile miners and workers at the Charleston, SC, textile mill, which mainly processed chrysotile from Quebec. A leading hypothesis for this discrepancy is limitations in the fiber size distributions available for this analysis. Dement et al. (2007) recently analyzed by TEM archived air samples from the South Carolina plant to determine a detailed distribution of fiber lengths up to lengths of 40 microm and greater. If similar data become available for Quebec, perhaps these two size distributions can be used to eliminate the discrepancy between these two studies.

摘要

美国环境保护局(EPA)对人类因接触石棉而患肺癌或间皮瘤风险的定量估计,利用了基于相差显微镜(PCM)且从不同职业环境中接触石棉的队列研究得出的效力因子估计值。这些效力因子存在很大差异。造成这种差异的最可能原因似乎是不同环境中纤维大小和矿物学特征的差异,而PCM并未考虑这些因素。在本文中,美国环境保护局(EPA)针对与石棉相关的肺癌和间皮瘤的模型得到了扩展,使纤维的效力取决于其矿物学类型和大小。这是通过设定由不重叠的纤维类别组成的接触指标,并为每个类别赋予其独特的效力来实现的。这些特定类别的效力在一项荟萃分析中进行估计,该分析将扩展后的模型与基于PCM的肺癌(KL)或间皮瘤(KM)效力进行拟合,这些效力是根据我们之前论文(Berman和Crump,2008年)中多项流行病学研究计算得出的。使用从文献中获取并与个体流行病学研究相匹配的基于透射电子显微镜(TEM)的纤维大小分布,来估计接触指标中不同纤维大小类别的纤维接触的特定流行病学研究估计值。还从该环境的文献信息中估计了温石棉和闪石石棉在给定环境中占总石棉接触量的比例。发现有足够的信息可将15项流行病学研究的KL和11项研究的KM纳入荟萃分析。由于已发表的TEM纤维大小分布的局限性严重限制了可考虑的接触指标范围,因此决定将注意力集中在由纤维宽度区分的四个接触指标上:“所有宽度”、宽度>0.2微米、宽度<0.4微米和宽度<0.2微米,每个指标都具有历史相关性。每个由宽度定义的此类指标由四类纤维组成:长度在5微米至10微米之间或长于10微米的温石棉或闪石石棉。使用这些指标,分别针对肺癌和间皮瘤估计了三个参数:KLA,较长(长度>10微米)闪石纤维的效力;rpc,纯温石棉(未被闪石污染)相对于闪石石棉的效力;以及rps,较短纤维(5微米<长度<10微米)相对于较长纤维的效力。对于间皮瘤,温石棉和闪石石棉效力相同(rpc = 1)的假设被每个指标强烈拒绝,而(纯)温石棉对间皮瘤无效力的假设未被任何指标拒绝。温石棉相对效力的最佳估计值范围从零到闪石石棉的约1/200(取决于指标)。对于肺癌,温石棉和闪石石棉效力相同(rpc = 1)的假设被基于细纤维(长度<0.4微米和<0.2微米)的两个指标拒绝(p≤0.05),但未被基于粗纤维的指标拒绝。在评估的其他指标中,“所有宽度”和宽度<0.4微米的指标对肺癌和间皮瘤数据的拟合效果最佳,尽管对肺癌的改善仅为边际改善。这两个指标对数据提供了等效(对于间皮瘤)和几乎等效(对于肺癌)的拟合,这表明可用数据集可能不够丰富(在接触特征的变化方面),无法充分评估纤维宽度对效力的影响。与rps和rpc都固定为1的宽度>0.2微米的指标(名义上等同于传统的PCM指标)相比,“所有宽度”和宽度<0.4微米的指标对肺癌尤其是间皮瘤提供了实质上更好的拟合。尽管对于“所有宽度”和宽度<0.4微米的指标,较短纤维(5<长度<10微米)效力的最佳估计值为零(或者对于间皮瘤的宽度>0.2微米指标,为较长纤维效力的一小部分),但对于这些指标中的任何一个,都无法拒绝这些较短纤维无效力的假设。将这些指标扩展以包括长度<5微米的纤维类别,未发现任何一致的证据表明这些最短纤维对肺癌或间皮瘤有任何效力。尽管与传统使用PCM相比拟合有了实质性改善,但“所有宽度”指标和宽度<0.4微米的指标(或评估的任何其他指标)都未完全解决不同职业研究中估计的效力因子差异。特别未解决的是魁北克温石棉矿工和南卡罗来纳州查尔斯顿纺织厂工人的肺癌效力因子差异,该纺织厂主要加工来自魁北克的温石棉。对此差异的一个主要假设是可用于此分析的纤维大小分布存在局限性。Dement等人(2007年)最近通过TEM分析了南卡罗来纳州工厂的存档空气样本,以确定长达40微米及更长纤维长度的详细分布。如果魁北克也能获得类似数据,也许这两个大小分布可用于消除这两项研究之间的差异。

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