Investigation of a hepatotoxicity screening system in primary cell cultures --'what biomarkers would need to be addressed to estimate toxicity in conventional and new approaches?'.

Kikkawa R; Yamamoto T; Fukushima T; Yamada H; Horii I

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Investigation of a hepatotoxicity screening system in primary cell cultures --'what biomarkers would need to be addressed to estimate toxicity in conventional and new approaches?'.

机译：对原代细胞培养物中的肝毒性筛选系统的研究-“在常规方法和新方法中需要评估什么样的生物标志物来评估毒性？”。

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High throughput toxicological estimation is required for safety evaluation in the early stage of drug discovery. In this context, establishment of an in vitro screening system reflecting in vivo toxicity is demanded for earlier safety assessment. We investigated LDH release and mitochondrial respiration (WST-1 reduction assay; WST-1) to detect cytotoxicity, morphological evaluation, and proteomics for estimating the reliable and sensitive biomarkers by using rat primary hepatocytes exposed to the compounds (acetaminophen, amiodarone, tetracycline and carbon tetrachloride) that are known to induce hepatotoxicity. In LDH release, no significant difference was detected between the control and compound exposed cells after exposure for 3 or 6 hr, but a dose-dependent increase was observed after exposure for 24 hr. Regarding the WST-1 assay, a dose-dependent reduction was detected after exposure for 6 and 24 hr to all of the compounds evaluated. In the proteomics analysis, 31 candidate proteins were identified from among the 103 demonstrating altered expression spots after exposure to acetaminophen. It was concluded that the cytotoxicity was detected earlier by measuring WST-1 than by measuring LDH release because the reduction of mitochondrial respiration is an expressions of earlier toxicity for cellular function, while the measured increase in the LDH release occurs after the failure of the cell membrane. Mitochondrial respiration ability was a useful parameter for cytotoxicity in in vitro hepato-toxicity screening, as cytotoxicity can be detected during the early stage of exposure. In addition to the conventional biomarkers, several protein biomarkers which relate to oxidative stress and metabolism-regulation were detected. Further comprehensive analysis of defined proteins would be necessary to estimate the more sensitive toxicology biomarker.

机译：在药物开发的早期阶段，需要高通量毒理学评估来进行安全性评估。在这种情况下，需要建立反映体内毒性的体外筛选系统以进行较早的安全性评估。我们调查了LDH释放和线粒体呼吸作用（WST-1减少测定法; WST-1），以检测细胞毒性，形态评价和蛋白质组学，通过使用暴露于化合物（对乙酰氨基酚，胺碘酮，四环素和已知会引起肝毒性的四氯化碳）。在LDH释放中，暴露3小时或6小时后，对照细胞和化合物暴露的细胞之间未检测到显着差异，但是暴露24小时后，观察到剂量依赖性增加。关于WST-1分析，在暴露于所有评估的化合物6和24小时后，检测到剂量依赖性降低。在蛋白质组学分析中，从对乙酰氨基酚暴露后的103个表现出改变的表达点中鉴定出31种候选蛋白。结论是，通过测量WST-1比通过测量LDH释放更早检测到细胞毒性，因为线粒体呼吸的减少是对细胞功能的更早毒性的表达，而在细胞衰竭后LDH释放的增加是发生的。膜。线粒体呼吸能力是体外肝毒性筛选中细胞毒性的有用参数，因为可以在暴露的早期阶段检测到细胞毒性。除了常规的生物标志物，还检测了几种与氧化应激和代谢调节有关的蛋白质生物标志物。为了评估更敏感的毒理学生物标志物，必须对定义的蛋白质进行进一步的综合分析。

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《The Journal of toxicological sciences》 |2005年第1期|共12页
作者
Kikkawa R; Yamamoto T; Fukushima T; Yamada H; Horii I;
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正文语种 eng
中图分类药学;
关键词
Biological Markers; Toxic effect; Lifetime Drinking History; Discharge (release); 生物学标记;

机译：Biological Markers;Toxic effect;Lifetime Drinking History;Discharge (release);生物学标记;

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1. Investigation of a hepatotoxicity screening system in primary cell cultures --"what biomarkers would need to be addressed to estimate toxicity in conventional and new approaches?". [J] . Kikkawa R, Yamamoto T, Fukushima T, The Journal of toxicological sciences . 2005,第1期

机译：对原代细胞培养物中的肝毒性筛选系统的研究-“在常规方法和新方法中需要评估什么样的生物标志物来评估毒性？”。
2. Recent advances in 2D and 3D in vitro systems using primary hepatocytes, alternative hepatocyte sources and non-parenchymal liver cells and their use in investigating mechanisms of hepatotoxicity, cell signaling and ADME [J] . Patricio Godoy, Nicola J Hewitt, Ute Albrecht, Archives of Toxicology . 2013,第8期

机译：使用原代肝细胞，替代肝细胞来源和非实质性肝细胞的2D和3D体外系统的最新进展及其在研究肝毒性，细胞信号传导和ADME机制中的用途
3. Recent advances in 2D and 3D in vitro systems using primary hepatocytes, alternative hepatocyte sources and non-parenchymal liver cells and their use in investigating mechanisms of hepatotoxicity, cell signaling and ADME [J] . Patricio Godoy, Nicola J Hewitt, Ute Albrecht, Archives of Toxicology . 2013,第8期

机译：使用原代肝细胞，替代肝细胞来源和非实质性肝细胞的2D和3D体外系统的最新进展及其在研究肝毒性，细胞信号传导和ADME机制中的用途
4. Liver Enzymes as Biomarkers for Hepatotoxicity of Statins in Patients with Dyslipidemia [C] . N. Velickova, M. Nateva, S. Stojanovska International Conference on Medical and Biological Engineering . 2020

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5. Using a Real-Time Cellular Biosensor to Investigate in vitro Liver Culture Models; Exploring the Effect of Primary Cultures, Cell to Cell Interaction in Co-culture, and Cell to Extracellular Matrix Interactions [D] . Ciampa, Grace. 2019

机译：使用实时细胞生物传感器来研究体外肝培养模型;探讨原发性培养物，细胞对共培养细胞相互作用的影响，以及细胞对细胞基质相互作用
6. Recent advances in 2D and 3D in vitro systems using primary hepatocytes alternative hepatocyte sources and non-parenchymal liver cells and their use in investigating mechanisms of hepatotoxicity cell signaling and ADME [O] . Patricio Godoy, Nicola J. Hewitt, Ute Albrecht, -1

机译：使用原代肝细胞替代肝细胞来源和非实质性肝细胞的2D和3D体外系统的最新进展及其在研究肝毒性细胞信号传导和ADME机制中的用途
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机译：成体大鼠肝细胞原代培养中酮类化学诱导肝毒性的增强作用

Investigation of a hepatotoxicity screening system in primary cell cultures --'what biomarkers would need to be addressed to estimate toxicity in conventional and new approaches?'.

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