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用外源化学物处理人外周血单个核细胞对细胞因子产生的体外抑制作用:对一般毒性和免疫毒性预测的意义。

Inhibition of in vitro cytokine production by human peripheral blood mononuclear cells treated with xenobiotics: implications for the prediction of general toxicity and immunotoxicity.

机构信息

Department of Pharmacology, Free University of Brussels (VUB), Brussels, Belgium.

出版信息

Toxicol In Vitro. 2010 Sep;24(6):1782-9. doi: 10.1016/j.tiv.2010.07.007. Epub 2010 Jul 13.

DOI:10.1016/j.tiv.2010.07.007
PMID:20633635
Abstract

The use of human peripheral blood mononuclear cells (PBMC) as an in vitro system to predict in vivo toxicity was investigated. For 58 chemicals, the effect on cytokine secretion (IL-5, IFNgamma and TNFalpha) by phytohaemagglutinin-activated PBMC was measured, IC50 values were calculated and correlations of these endpoints with human LC50 values were determined. The best result was obtained with IFNgamma as an endpoint for which the calculated R(2) value was 0.58 which is comparable with the R(2) values for the classical neutral red uptake (NRU) assays using murine 3T3 cells and normal human keratinocytes (R(2)=0.56 and 0.59, respectively). When for each chemical the lowest IC50 value of the three endpoints was correlated with LC50 the calculated R(2) increased slightly to 0.63. A specific strength of our test is that it corrects several outliers (diazepam, digoxin, malathion and verapamil hydrochloride) which do not fit in the linear regression analysis for IC50 values obtained with the classical 3T3 NRU assay. Furthermore, 2,4-dichlorophenoxyacetic acid, cyclosporine A and pentachlorophenol had a 10 times lower IC50 value than the estimated human LC50 value and were identified as immunotoxic alerts. In conclusion, new endpoints investigated in this study contribute to the prediction of immunotoxic effects and correct outliers of classical cytotoxicity assays.

摘要

本研究旨在利用人外周血单个核细胞(PBMC)作为体外系统,预测体内毒性。对 58 种化学物质,通过植物血凝素激活的 PBMC 测量细胞因子(IL-5、IFNgamma 和 TNFalpha)分泌的影响,计算 IC50 值,并确定这些终点与人体 LC50 值的相关性。以 IFNgamma 作为终点时,得到了最佳结果,计算得到的 R(2) 值为 0.58,与使用鼠 3T3 细胞和正常人角质形成细胞的经典中性红摄取(NRU)测定法的 R(2)值(分别为 0.56 和 0.59)相当。当将三个终点中每个化学物质的最低 IC50 值与 LC50 值相关联时,计算得到的 R(2) 值略有增加至 0.63。我们的测试的一个优势是,它纠正了几个异常值(地西泮、地高辛、马拉硫磷和盐酸维拉帕米),这些异常值与经典 3T3 NRU 测定法获得的 IC50 值的线性回归分析不匹配。此外,2,4-二氯苯氧基乙酸、环孢菌素 A 和五氯苯酚的 IC50 值比估计的人体 LC50 值低 10 倍,被鉴定为免疫毒性警示剂。总之,本研究中研究的新终点有助于预测免疫毒性效应,并纠正经典细胞毒性测定的异常值。

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