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Microengineered cell and tissue systems for drug screening and toxicology applications: Evolution of in-vitro liver technologies

机译:用于药物筛选和毒理学应用的微工程细胞和组织系统:体外肝脏技术的发展

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摘要

The liver performs many key functions, the most prominent of which is serving as the metabolic hub of the body. For this reason, the liver is the focal point of many investigations aimed at understanding an organism’s toxicological response to endogenous and exogenous challenges. Because so many drug failures have involved direct liver toxicity or other organ toxicity from liver generated metabolites, the pharmaceutical industry has constantly sought superior, predictive in-vitro models that can more quickly and efficiently identify problematic drug candidates before they incur major development costs, and certainly before they are released to the public. In this broad review, we present a survey and critical comparison of in-vitro liver technologies along a broad spectrum, but focus on the current renewed push to develop “organs-on-a-chip”. One prominent set of conclusions from this review is that while a large body of recent work has steered the field towards an ever more comprehensive understanding of what is needed, the field remains in great need of several key advances, including establishment of standard characterization methods, enhanced technologies that mimic the in-vivo cellular environment, and better computational approaches to bridge the gap between the in-vitro and in-vivo results.
机译:肝脏执行许多关键功能,其中最突出的功能是充当人体的新陈代谢枢纽。因此,肝脏是许多旨在了解生物体对内源性和外源性挑战的毒理反应的研究的重点。由于如此多的药物失败都涉及肝脏产生的代谢产物直接引起的肝毒性或其他器官毒性,因此制药行业一直在寻求卓越的,可预测的体外模型,该模型可以更快,更有效地识别出有问题的候选药物,而不产生重大的开发成本,并且肯定是在它们发布给公众之前。在这篇广泛的综述中,我们将对广泛范围内的体外肝技术进行调查和关键比较,但重点是当前重新开发“单片器官”的努力。这次审查得出的一组重要结论是,尽管最近的大量工作引导该领域朝着对所需条件的更加全面的了解,但该领域仍然急需几项关键的进展,包括建立标准的表征方法,模仿了体内细胞环境的增强技术,以及更好的计算方法来弥合体外和体内结果之间的差距。

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