Chip-based human liver–intestine and liver–skin co-cultures – A first step toward systemic repeated dose substance testing in vitro

人体皮肤 体内 首过效应 药理学 医学 药品 病理 生物 生物技术 遗传学
作者
Ilka Maschmeyer,Tobias Hasenberg,Annika Jaenicke,Marcus Lindner,Alexandra Lorenz,Julie Zech,Leif‐Alexander Garbe,Frank Sonntag,Patrick Hayden,Seyoum Ayehunie,Roland Lauster,Uwe Marx,Eva-Maria Materne
出处
期刊:European Journal of Pharmaceutics and Biopharmaceutics [Elsevier]
卷期号:95 (Pt A): 77-87 被引量:209
标识
DOI:10.1016/j.ejpb.2015.03.002
摘要

Systemic repeated dose safety assessment and systemic efficacy evaluation of substances are currently carried out on laboratory animals and in humans due to the lack of predictive alternatives. Relevant international regulations, such as OECD and ICH guidelines, demand long-term testing and oral, dermal, inhalation, and systemic exposure routes for such evaluations. So-called “human-on-a-chip” concepts are aiming to replace respective animals and humans in substance evaluation with miniaturized functional human organisms. The major technical hurdle toward success in this field is the life-like combination of human barrier organ models, such as intestine, lung or skin, with parenchymal organ equivalents, such as liver, at the smallest biologically acceptable scale. Here, we report on a reproducible homeostatic long-term co-culture of human liver equivalents with either a reconstructed human intestinal barrier model or a human skin biopsy applying a microphysiological system. We used a multi-organ chip (MOC) platform, which provides pulsatile fluid flow within physiological ranges at low media-to-tissue ratios. The MOC supports submerse cultivation of an intact intestinal barrier model and an air–liquid interface for the skin model during their co-culture with the liver equivalents respectively at 1/100.000 the scale of their human counterparts in vivo. To increase the degree of organismal emulation, microfluidic channels of the liver–skin co-culture could be successfully covered with human endothelial cells, thus mimicking human vasculature, for the first time. Finally, exposure routes emulating oral and systemic administration in humans have been qualified by applying a repeated dose administration of a model substance – troglitazone – to the chip-based co-cultures.
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