Developing an in vitro screening assay platform for evaluation of antifibrotic drugs using precision-cut liver slices.

Fibrogenesis & Tissue Repair Pub Date : 2014-12-16 eCollection Date: 2015-01-01 DOI:10.1186/s13069-014-0017-2
Satish Kumar Sadasivan, Nethra Siddaraju, Khaiser Mehdi Khan, Balamuralikrishna Vasamsetti, Nimisha R Kumar, Vibha Haridas, Madhusudhan B Reddy, Somesh Baggavalli, Anup M Oommen, Raghavendra Pralhada Rao
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引用次数: 15

Abstract

Background: Precision-cut liver slices present different cell types of liver in a physiological context, and they have been explored as effective in vitro model systems to study liver fibrosis. Inducing fibrosis in the liver slices using toxicants like carbon tetrachloride is of less relevance to human disease conditions. Our aim for this study was to establish physiologically relevant conditions in vitro to induce fibrotic phenotypes in the liver slices.

Results: Precision-cut liver slices of 150 μm thickness were obtained from female C57BL/6 J mice. The slices were cultured for 24 hours in media containing a cocktail of 10 nM each of TGF-β, PDGF, 5 μM each of lysophosphatidic acid and sphingosine 1 phosphate and 0.2 μg/ml of lipopolysaccharide along with 500 μM of palmitate and were analyzed for triglyceride accumulation, stress and inflammation, myofibroblast activation and extracellular matrix (ECM) accumulation. Incubation with the cocktail resulted in increased triglyceride accumulation, a hallmark of steatosis. The levels of Acta2, a hallmark of myofibroblast activation and the levels of inflammatory genes (IL-6, TNF-α and C-reactive protein) were significantly elevated. In addition, this treatment resulted in increased levels of ECM markers - collagen, lumican and fibronectin.

Conclusions: This study reports the experimental conditions required to induce fibrosis associated with steatohepatitis using physiologically relevant inducers. The system presented here captures various aspects of the fibrosis process like steatosis, inflammation, stellate cell activation and ECM accumulation and serves as a platform to study the liver fibrosis in vitro and to screen small molecules for their antifibrotic activity.

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建立一种利用精确切割肝片评价抗纤维化药物的体外筛选实验平台。
背景:精确切割的肝切片在生理背景下呈现了不同类型的肝脏细胞,它们已被探索作为有效的体外模型系统来研究肝纤维化。使用四氯化碳等有毒物质在肝切片中诱导纤维化与人类疾病状况的相关性较小。我们这项研究的目的是在体外建立生理相关条件来诱导肝切片纤维化表型。结果:获得了C57BL/ 6j雌性小鼠的肝脏精密切片,切片厚度为150 μm。将切片在含TGF-β、PDGF各10 nM、溶血磷脂酸和鞘氨醇1磷酸各5 μM、脂多糖0.2 μg/ml和棕榈酸500 μM的混合培养基中培养24小时,分析甘油三酯积累、应激和炎症、肌成纤维细胞活化和细胞外基质(ECM)积累情况。与鸡尾酒一起孵卵导致甘油三酯积累增加,这是脂肪变性的标志。肌成纤维细胞活化标志Acta2水平和炎症基因(IL-6、TNF-α和c反应蛋白)水平显著升高。此外,这种治疗导致ECM标志物-胶原蛋白,lumican和纤维连接蛋白水平升高。结论:本研究报告了使用生理相关诱导剂诱导脂肪性肝炎相关纤维化所需的实验条件。该系统捕获了纤维化过程的各个方面,如脂肪变性、炎症、星状细胞活化和ECM积累,并作为体外研究肝纤维化和筛选小分子抗纤维化活性的平台。
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