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In vitro cardiotoxicity assessment of environmental chemicals using an organotypic human induced pluripotent stem cell-derived model

机译:使用有机型人诱导多能干细胞衍生模型的环境化学品的体外心脏毒性评估

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An important target area for addressing data gaps through in vitro screening is the detection of potential cardiotoxicants. Despite the fact that current conservative estimates relate at least 23% of all cardiovascular disease cases to environmental exposures, the identities of the causative agents remain largely uncharacterized. Here, we evaluate the feasibility of a combinatorial in vitro/in silica screening approach for functional and mechanistic cardiotoxicity profiling of environmental hazards using a library of 69 representative environmental chemicals and drugs. Human induced pluripotent stem cell-derived cardiomyocytes were exposed in concentration-response for 30 min or 24 h and effects on cardiomyocyte beating and cellular and mitochondria( toxicity were assessed by kinetic measurements of intracellular Ca2+ flux and high-content imaging using the nuclear dye Hoechst 33342, the cell viability marker Calcein AM, and the mitochondrial depolarization probe JC-10. More than half of the tested chemicals exhibited effects on cardiomyocyte beating after 30 min of exposure. In contrast, after 24 h, effects on cell beating without concomitant cytotoxicity were observed in about one third of the compounds. Concentration-response data for in vitro bioactivity phenotypes visualized using the Toxicological Prioritization Index (ToxPi) showed chemical class-specific clustering of environmental chemicals, including pesticides, flame retardants, and polycyclic aromatic hydrocarbons. For environmental chemicals with human exposure predictions, the activity-to-exposure ratios between modeled blood concentrations and in vitro bioactivity were between one and five orders of magnitude. These findings not only demonstrate that some ubiquitous environmental pollutants might have the potential at high exposure levels to alter cardiomyocyte function, but also indicate similarities in the mechanism of these effects both within and among chemicals and classes. (C) 2017 Published by Elsevier Inc.
机译:通过体外筛选解决数据间隙的重要目标区域是检测潜在的心脏毒性。尽管目前的保守估计值将所有心血管疾病病例的至少23%涉及环境暴露,但致病剂的身份仍然很大程度上是无表的。在这里,我们使用69名代表性环境化学品和药物的图书馆评估组合体内/在二氧化硅筛选方法的可行性,用于环境危害的功能和机械心脏毒性分析。将人诱导的多能干细胞衍生的心肌细胞浓缩 - 反应浓缩30分钟或24小时,并且对心肌细胞跳动和细胞和线粒体的影响(通过细胞内Ca2 +通量的动力学测量评估毒性和使用核染料的高含量成像评估33342,细胞活力标记Calcein AM和线粒体去极化探针JC-10。超过一半的测试化学品表现出对30分钟暴露后的心肌细胞跳动的影响。相比之下,24小时后,在没有伴随细胞毒性的情况下对细胞搏动的影响在大约三分之一的化合物中观察到。使用毒理学优先级指数(TOXPI)可视化的体外生物活性表型的浓度 - 响应数据显示了环境化学品的化学类特异性聚类,包括农药,阻燃剂和多环芳烃。对于环境化学品,具有人类暴露预测,活动 - 建模血液浓度和体外生物活性之间的暴露比在一个和五个数量级之间。这些发现不仅表明一些无处不在的环境污染物可能具有高暴露水平的潜力来改变心肌细胞功能,而且表明化学品和类别中的这些作用机制的相似性。 (c)2017年由elsevier公司发布

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