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秀丽隐杆线虫作为药物化合物快速毒性评估的模型系统。

Caenorhabditis elegans as model system for rapid toxicity assessment of pharmaceutical compounds.

作者信息

Dengg Marlene, van Meel Jacques C A

机构信息

Boehringer Ingelheim Austria GmbH, Dr. Boehringer-Gasse 5-11, Vienna 1121, Austria.

出版信息

J Pharmacol Toxicol Methods. 2004 Nov-Dec;50(3):209-14. doi: 10.1016/j.vascn.2004.04.002.

DOI:10.1016/j.vascn.2004.04.002
PMID:15519907
Abstract

INTRODUCTION

The model organism Caenorhabditis elegans is widely used for genetic studies as well as a living biomonitor in ecotoxicology. In this study, we investigated whether C. elegans may represent a suitable model for rapid preliminary toxicity studies of pharmaceutical compounds.

METHODS

For this purpose, we used the EGFR kinase inhibitors BIBU1361, BIBX1382, and an inactive chemical analogue BIBU1476. As a first parameter to score for toxicity, we determined lethality of the wild-type C. elegans strain N2 (Bristol) in the presence of the compounds. The transgenic C. elegans strain PC72 (lacZ, heat shock protein-16 [hsp-16] construct) was used as a report organism for toxic effects. PC72 expresses beta-Galactosidase which is induced by hsp-16 in direct response when exposed to toxic compounds. The expression of beta-Galactosidase in cells was subsequently visualized by histochemical staining with X-Gal.

RESULTS

A rank order of potency with respect to lethality was established: BIBU1361>BIBX1382>>BIB1476. The induction of beta-Galactosidase was concentration-dependent for each compound and demonstrated the same order of potency as observed for lethality. Furthermore, these compounds showed the same order for lethality in rodents, the first requirement of validation.

DISCUSSION

These results indicate that wild-type C. elegans and the transgenic strain PC72 are both suitable models to determine the toxicity of pharmaceutical compounds. This approach allows for an easy and fast ranking of compound toxicity, which may lead to a more rational choice for further in vivo tests.

摘要

引言

模式生物秀丽隐杆线虫广泛用于遗传学研究以及生态毒理学中的活体生物监测。在本研究中,我们调查了秀丽隐杆线虫是否可作为药物化合物快速初步毒性研究的合适模型。

方法

为此,我们使用了表皮生长因子受体(EGFR)激酶抑制剂BIBU1361、BIBX1382以及一种无活性的化学类似物BIBU1476。作为毒性评分的首个参数,我们测定了野生型秀丽隐杆线虫N2(布里斯托尔株)在这些化合物存在时的致死率。转基因秀丽隐杆线虫株PC72(含β-半乳糖苷酶基因、热休克蛋白-16 [hsp-16]构建体)用作毒性效应的报告生物。PC72表达β-半乳糖苷酶,当暴露于有毒化合物时,hsp-16会直接诱导其表达。随后通过用X-Gal进行组织化学染色来观察细胞中β-半乳糖苷酶的表达。

结果

确定了致死率方面的效力等级顺序:BIBU1361 > BIBX1382 >> BIB1476。每种化合物诱导β-半乳糖苷酶的表达呈浓度依赖性,并且显示出与致死率相同的效力顺序。此外,这些化合物在啮齿动物中的致死率顺序相同,这是验证的首要要求。

讨论

这些结果表明,野生型秀丽隐杆线虫和转基因株PC72都是确定药物化合物毒性的合适模型。这种方法能够轻松快速地对化合物毒性进行排序,这可能会为进一步的体内试验带来更合理的选择。

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