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A high-throughput screening assay based on automated microscopy for monitoring antibiotic susceptibility of Mycobacterium tuberculosis phenotypes

机译:一种基于自动显微镜的高通量筛选测定,用于监测结核分枝杆菌表型的抗生素敏感性

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Efficient high-throughput drug screening assays are necessary to enable the discovery of new anti-mycobacterial drugs. The purpose of our work was to develop and validate an assay based on live-cell imaging which can monitor the growth of two distinct phenotypes of Mycobacterium tuberculosis and to test their susceptibility to commonly used TB drugs. Both planktonic and cording phenotypes were successfully monitored as fluorescent objects using the live-cell imaging system IncuCyte S3, allowing collection of data describing distinct characteristics of aggregate size and growth. The quantification of changes in total area of aggregates was used to define IC50 and MIC values of selected TB drugs which revealed that the cording phenotype grew more rapidly and displayed a higher susceptibility to rifampicin. In checkerboard approach, testing pair-wise combinations of sub-inhibitory concentrations of drugs, rifampicin, linezolid and pretomanid demonstrated superior growth inhibition of cording phenotype. Our results emphasize the efficiency of using automated live-cell imaging and its potential in high-throughput whole-cell screening to evaluate existing and search for novel antimycobacterial drugs.
机译:有效的高通量药物筛选测定是能够发现新的抗分枝杆菌药物。我们的作品的目的是根据活细胞成像开发和验证测定,可以监测分枝杆菌的两种不同表型的生长,并测试其对常用结核病药物的易感性。使用活细胞成像系统的荧光物体S3成功地监测了浮游和线虫表型,允许收集描述聚集大小和生长的不同特征的数据。聚集体总面积变化的定量用于定义所选结核药物的IC50和MIC值,显示出滤芯表型更快地增长并且对利福平的易感性显示出更高的易感性。在棋盘方法中,测试药物,利福平,线唑和伪造症的副抑制浓度的配对组合表现出优异的脊髓表型生长抑制。我们的结果强调了使用自动化活细胞成像的效率及其在高通量全细胞筛查中的潜力,以评估现有和寻找新型抗细菌药物。

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