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Monitoring and manipulating cellular crosstalk during kidney fibrosis inside a 3D in vitro co-culture

机译:在3D体外共培养中监测和操纵肾脏纤维化期间的细胞串扰

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摘要

In pharmacological research the development of promising lead compounds requires a detailed understanding of the dynamics of disease progression. However, for many diseases, such as kidney fibrosis, gaining such understanding requires complex real-time, multi-dimensional analysis of diseased and healthy tissue. To allow for such studies with increased throughput we established a dextran hydrogel-based in vitro 3D co-culture as a disease model for kidney fibrosis aimed at the discovery of compounds modulating the epithelial/mesenchymal crosstalk. This platform mimics a simplified pathological renal microenvironment at the interface between tubular epithelial cells and surrounding quiescent fibroblasts. We combined this 3D technology with epithelial reporter cell lines expressing fluorescent biomarkers in order to visualize pathophysiological cell state changes resulting from toxin-mediated chemical injury. Epithelial cell damage onset was robustly detected by image-based monitoring, and injured epithelial spheroids induced myofibroblast differentiation of co-cultured quiescent human fibroblasts. The presented 3D co-culture system therefore provides a unique model system for screening of novel therapeutic molecules capable to interfere and modulate the dialogue between epithelial and mesenchymal cells.
机译:在药理研究中,有前途的先导化合物的开发需要对疾病进展动态的详细了解。但是,对于许多疾病,例如肾纤维化,要获得这种了解,就需要对患病和健康组织进行复杂的实时,多维分析。为了使此类研究具有更高的通量,我们建立了一种基于右旋糖酐水凝胶的体外3D共培养作为肾脏纤维化的疾病模型,旨在发现调节上皮/间质串扰的化合物。该平台模拟肾小管上皮细胞与周围的静止成纤维细胞之间界面的简化的病理性肾脏微环境。我们将这种3D技术与表达荧光生物标志物的上皮报道细胞系相结合,以观察由毒素介导的化学损伤导致的病理生理细胞状态变化。上皮细胞损伤的发生可以通过基于图像的监测得到强有力的检测,并且受损的上皮球体可以诱导共培养的静态人成纤维细胞分化为成纤维细胞。因此,提出的3D共培养系统提供了一个独特的模型系统,用于筛选能够干扰和调节上皮细胞与间充质细胞之间对话的新型治疗分子。

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