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禁食和进食状态下人体胃液对六价铬的还原作用。I. 化学还原及致突变性的减轻

Reduction of hexavalent chromium by fasted and fed human gastric fluid. I. Chemical reduction and mitigation of mutagenicity.

作者信息

De Flora Silvio, Camoirano Anna, Micale Rosanna T, La Maestra Sebastiano, Savarino Vincenzo, Zentilin Patrizia, Marabotto Elisa, Suh Mina, Proctor Deborah M

机构信息

Department of Health Sciences, University of Genoa, 16132 Genoa, Italy.

Gastroenterology Unit, Department of Internal Medicine, University of Genoa, 16132 Genoa, Italy.

出版信息

Toxicol Appl Pharmacol. 2016 Sep 1;306:113-9. doi: 10.1016/j.taap.2016.07.004. Epub 2016 Jul 9.

Abstract

Evaluation of the reducing capacity of human gastric fluid from healthy individuals, under fasted and fed conditions, is critical for assessing the cancer hazard posed by ingested hexavalent chromium [Cr(VI)] and for developing quantitative physiologically-based pharmacokinetic models used in risk assessment. In the present study, the patterns of Cr(VI) reduction were evaluated in 16 paired pre- and post-meal gastric fluid samples collected from 8 healthy volunteers. Human gastric fluid was effective both in reducing Cr(VI), as measured by using the s-diphenylcarbazide colorimetric method, and in attenuating mutagenicity in the Ames test. The mean (±SE) Cr(VI)-reducing ability of post-meal samples (20.4±2.6μgCr(VI)/mL gastric fluid) was significantly higher than that of pre-meal samples (10.2±2.3μgCr(VI)/mL gastric fluid). When using the mutagenicity assay, the decrease of mutagenicity produced by pre-meal and post-meal samples corresponded to reduction of 13.3±1.9 and 25.6±2.8μgCr(VI)/mL gastric fluid, respectively. These data are comparable to parallel results conducted by using speciated isotope dilution mass spectrometry. Cr(VI) reduction was rapid, with >70% of total reduction occurring within 1min and 98% of reduction is achieved within 30min with post-meal gastric fluid at pH2.0. pH dependence was observed with decreasing Cr(VI) reducing capacity at higher pH. Attenuation of the mutagenic response is consistent with the lack of DNA damage observed in the gastrointestinal tract of rodents following administration of ≤180ppm Cr(VI) for up to 90days in drinking water. Quantifying Cr(VI) reduction kinetics in the human gastrointestinal tract is necessary for assessing the potential hazards posed by Cr(VI) in drinking water.

摘要

评估健康个体在空腹和进食条件下胃液的还原能力,对于评估摄入的六价铬[Cr(VI)]所带来的癌症风险以及开发用于风险评估的基于生理学的定量药代动力学模型至关重要。在本研究中,对从8名健康志愿者收集的16对餐前和餐后胃液样本中Cr(VI)的还原模式进行了评估。人胃液在用二苯卡巴肼比色法测量时,对还原Cr(VI)有效,并且在Ames试验中可减弱致突变性。餐后样本的平均(±SE)Cr(VI)还原能力(20.4±2.6μgCr(VI)/mL胃液)显著高于餐前样本(10.2±2.3μgCr(VI)/mL胃液)。在使用致突变性试验时,餐前和餐后样本产生的致突变性降低分别对应于胃液中13.3±1.9和25.6±2.8μgCr(VI)/mL的还原。这些数据与使用特定同位素稀释质谱法得到的平行结果相当。Cr(VI)的还原很快,在pH2.0的餐后胃液中,总还原量的>70%在1分钟内发生,98%的还原在30分钟内完成。观察到pH依赖性,在较高pH下Cr(VI)还原能力降低。致突变反应的减弱与在饮用水中给予≤180ppm Cr(VI)长达90天的啮齿动物胃肠道中未观察到DNA损伤一致。量化人体胃肠道中Cr(VI)的还原动力学对于评估饮用水中Cr(VI)所带来的潜在危害是必要的。

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