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Development of a semi-automated image-based high-throughput drug screening system

机译:开发半自动图像的高通量药物筛选系统

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We previously reported that the innate sensing of the endosymbiont Leishmania RNA virus 1 (LRV1) within Leishmania (Viannia) guyanensis through Toll-like receptor 3, worsens the pathogenesis of parasite infection in mice. The presence of LRV1 has been associated with the failure of first-line treatment in patients infected with LRV1 containing -L. guyanensis and -L braziliensis parasites. Here, we established a semi-automated image-based high-throughput drug screening (HTDS) protocol to measure parasiticidal activity of the Prestwick chemical library in primary murine macrophages infected with LRV1-containing L. guyanensis. The two-independent screens generated 14 hit compounds with over sixty-nine percent reduction in parasite growth compared to control, at a single dose in both screens. Our screening strategy offers great potential in the search for new drugs and accelerates the discovery rate in the field of drug repurposing against Leishmania. Moreover, this technique allows the concomitant assessment of the effect of drug toxicity on host cell number.
机译:我们以前报道,通过Toll样受体3,Leishmania(viannia)Guishmenia(viannnia)umeranensis内的indosymbiont Leishmania的先天性感测到鼠李,恶化了小鼠寄生虫感染的发病机制。 LRV1的存在已经与含有-L的LRV1感染的患者的一线治疗失败有关。 Guyanensis和-L Braziliensis Parasites。在这里,我们建立了一种半自动图像的高通量药物筛选(HTDS)方案,以测量含有LRV1的L. Guyanensis的初级鼠巨噬细胞中Prestwick化学文库的寄生活性。与对照相比,双独立屏幕生成14个麦芽酸血液生长减少超过六十九倍的化合物,以在两个屏幕中的单剂量上进行。我们的筛选战略在寻找新药方面提供了极大的潜力,并加速了对利什曼潜行的药物修复领域的发现率。此外,该技术允许伴随对药物毒性对宿主细胞数作用的影响。

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