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Viability of developmental stages of Schistosoma mansoni quantified with xCELLigence worm real-time motility assay (xWORM)

机译:用xCELLigence蠕虫实时运动分析(xWORM)定量测定曼氏血吸虫发育阶段的生存力

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摘要

Infection with helminth parasites causes morbidity and mortality in billions of people and livestock worldwide. Where anthelmintic drugs are available, drug resistance is a major problem in livestock parasites, and a looming threat to public health. Monitoring the efficacy of these medicines and screening for new drugs has been hindered by the lack of objective, high-throughput approaches. Several cell monitoring technologies have been adapted for parasitic worms, including video-, fluorescence-, metabolism enzyme- and impedance-based tools that minimize the screening bottleneck. Using the xCELLigence impedance-based system we previously developed a motility-viability assay that is applicable for a range of helminth parasites. Here we have improved substantially the assay by using diverse frequency settings, and have named it the xCELLigence worm real-time motility assay (xWORM). By utilizing strictly standardized mean difference analysis we compared the xWORM output measured with 10, 25 and 50 kHz frequencies to quantify the motility of schistosome adults (human blood flukes) and hatching of schistosome eggs. Furthermore, we have described a novel application of xWORM to monitor movement of schistosome cercariae, the developmental stage that is infectious to humans. For all three stages, 25 kHz was either optimal or near-optimal for monitoring and quantifying schistosome motility. These improvements in methodology sensitivity should enhance the capacity to screen small compound libraries for new drugs both for schistosomes and other helminth pathogens at large.
机译:蠕虫寄生虫感染导致全世界数十亿人和牲畜的发病和死亡。在可以使用驱虫药的地方,耐药性是牲畜寄生虫的主要问题,对公共健康的威胁日益凸显。缺乏客观,高通量的方法阻碍了监测这些药物的疗效和筛选新药。几种细胞监测技术已经适应寄生虫,包括基于视频,荧光,代谢酶和阻抗的工具,这些工具可最大程度地减少筛选瓶颈。使用基于xCELLigence阻抗的系统,我们之前开发了一种运动力-活力测定法,适用于多种蠕虫寄生虫。在这里,我们通过使用多种频率设置大大改进了该检测方法,并将其命名为xCELLigence蠕虫实时运动检测(xWORM)。通过使用严格标准化的均值差异分析,我们比较了在10、25和50 kHz频率下测得的xWORM输出,以量化血吸虫成虫(人血吸虫)的活动性和血吸虫卵的孵化率。此外,我们描述了xWORM在监测血吸虫尾c运动的新应用,血cer尾,是对人类具有传染性的发育阶段。对于所有三个阶段,25 kHz是监测或定量血吸虫运动性的最佳或接近最佳状态。方法学敏感性的这些改进将增强针对小分子化合物库筛查血吸虫和其他寄生虫病原体的新药的能力。

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