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Reduced deformability of parasitized red blood cells as a biomarker for anti-malarial drug efficacy

机译:降低了被寄生虫的红细胞作为抗疟药功效的生物标志物的可变形性

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摘要

BackgroundMalaria remains a challenging and fatal infectious disease in developing nations and the urgency for the development of new drugs is even greater due to the rapid spread of anti-malarial drug resistance. While numerous parasite genetic, protein and metabolite biomarkers have been proposed for testing emerging anti-malarial compounds, they do not universally correspond with drug efficacy. The biophysical character of parasitized cells is a compelling alternative to these conventional biomarkers because parasitized erythrocytes become specifically rigidified and this effect is potentiated by anti-malarial compounds, such as chloroquine and artesunate. This biophysical biomarker is particularly relevant because of the mechanistic link between cell deformability and enhanced splenic clearance of parasitized erythrocytes.
机译:背景技术疟疾在发展中国家仍然是具有挑战性和致命性的传染病,由于抗疟疾药物耐药性的迅速传播,开发新药的紧迫性甚至更大。虽然已经提出了许多寄生虫的遗传,蛋白质和代谢物生物标志物来测试新兴的抗疟疾化合物,但它们并不普遍与药物功效相对应。寄生虫细胞的生物物理特性是这些常规生物标记物的引人注目的替代品,因为寄生虫化的红血球变得特别僵化,并且抗疟疾化合物(如氯喹和青蒿琥酯)可增强这种作用。由于细胞变形能力与寄生红细胞的脾脏清除增强之间的机械联系,这种生物物理生物标记物特别重要。

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