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In Vitro Inflammation Inhibition Model Based on Semi-Continuous Toll-Like Receptor Biosensing

机译:基于半连续性收费受体生物传感的体外炎症抑制模型

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摘要

A chemical inhibition model of inflammation is proposed by semi-continuous monitoring the density of toll-like receptor 1 (TLR1) expressed on mammalian cells following bacterial infection to investigate an in vivo-mimicked drug screening system. The inflammation was induced by adding bacterial lysate (e.g., Pseudomonas aeruginosa) to a mammalian cell culture (e.g., A549 cell line). The TLR1 density on the same cells was immunochemically monitored up to three cycles under optimized cyclic bacterial stimulation-and-restoration conditions. The assay was carried out by adopting a cell-compatible immunoanalytical procedure and signal generation method. Signal intensity relative to the background control obtained without stimulation was employed to plot the standard curve for inflammation. To suppress the inflammatory response, sodium salicylate, which inhibits nuclear factor-κB activity, was used to prepare the standard curve for anti-inflammation. Such measurement of differential TLR densities was used as a biosensing approach discriminating the anti-inflammatory substance from the non-effector, which was simulated by using caffeic acid phenethyl ester and acetaminophen as the two components, respectively. As the same cells exposed to repetitive bacterial stimulation were semi-continuously monitored, the efficacy and toxicity of the inhibitors may further be determined regarding persistency against time. Therefore, this semi-continuous biosensing model could be appropriate as a substitute for animal-based experimentation during drug screening prior to pre-clinical tests.
机译:通过半连续监测细菌感染后哺乳动物细胞上表达的Toll样受体1(TLR1)的密度,提出了一种炎症的化学抑制模型,以研究体内模拟的药物筛选系统。通过向哺乳动物细胞培养物(例如A549细胞系)中加入细菌裂解物(例如铜绿假单胞菌)来诱发炎症。在优化的循环细菌刺激和恢复条件下,最多可对三个细胞的TLR1密度进行免疫化学监测。通过采用细胞相容的免疫分析方法和信号产生方法进行测定。相对于没有刺激而获得的背景对照的信号强度被用于绘制炎症的标准曲线。为了抑制炎症反应,使用了抑制核因子-κB活性的水杨酸钠来制备抗炎的标准曲线。这种差异TLR密度的测量方法被用作区分抗炎物质和非效应物质的生物传感方法,该方法分别通过使用咖啡酸苯乙酯和对乙酰氨基酚作为两种成分进行模拟。由于半连续监测暴露于重复细菌刺激的相同细胞,因此可进一步确定抑制剂对时间的持久性的功效和毒性。因此,这种半连续的生物传感模型可能适合替代临床前测试之前的药物筛选过程中基于动物的实验。

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  • 年(卷),期 -1(9),8
  • 年度 -1
  • 页码 e105212
  • 总页数 10
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