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首页> 外文期刊>Toxicological sciences: An official journal of the Society of Toxicology >Assessment of hepatocytes and liver slices as in vitro test systems to predict in vivo gene expression.
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Assessment of hepatocytes and liver slices as in vitro test systems to predict in vivo gene expression.

机译:评估肝细胞和肝切片作为体外测试系统,以预测体内基因表达。

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摘要

The use of in vitro systems to predict in vivo responses to chemical agents provides the benefits of requiring fewer animals, reducing variability between samples, requiring less test material, and enabling higher throughput. In the present study rat tissue slices and primary hepatocytes were compared as in vitro systems to predict in vivo changes in gene expression in response to treatment with known liver toxicants or inducers. Five compounds (phenobarbital, carbon tetrachloride, Wy-14,634, alpha-napthylisothiocyanate, and tacrine) were chosen for their established and diverse mechanisms of hepatoxicity or microsomal induction. Expression profiles from male Sprague-Dawley rats or in vitro systems treated for 24 h were measured by DNA oligonucleotide microarrays containing 8700 probe sets. Qualitative comparison of expression revealed a >80% concordance between in vivo liver and both in vitro systems; however, the responsiveness of both in vitro systems to compound-induced changes in gene expression was far less than that of in vivo. Furthermore, both in vitro systems appeared similar in their ability to reproduce compound-induced changes in gene expression observed in vivo.
机译:使用体外系统预测体内对化学试剂的反应具有以下优点:需要更少的动物,减少样品之间的变异性,需要更少的测试材料并实现更高的通量。在本研究中,将大鼠组织切片和原代肝细胞作为体外系统进行了比较,以预测体内基因表达在响应已知肝毒物或诱导剂治疗后的体内变化。选择了五种化合物(苯巴比妥,四氯化碳,Wy-14,634,α-萘基异硫氰酸酯和他克林)以确立其多样的肝毒性或微粒体诱导机制。用包含8700个探针组的DNA寡核苷酸微阵列测量雄性Sprague-Dawley大鼠或处理24小时的体外系统的表达谱。表达的定性比较显示,体内肝脏与两个体外系统之间的一致性> 80%;然而,两个体外系统对化合物诱导的基因表达变化的响应性都远小于体内。此外,两种体外系统在重现体内观察到的化合物诱导的基因表达变化方面均表现出相似的能力。

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