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A Non-Radioactive DAPI-based High-Throughput In Vitro Assay to Assess Plasmodium falciparum Responsiveness to Antimalarials—Increased Sensitivity of P. falciparum to Chloroquine in Senegal

机译:评估恶性疟原虫对抗疟药的反应性的基于非放射性DAPI的高通量体外测定-塞内加尔恶性疟原虫对氯喹的敏感性增加

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摘要

The spread of Plasmodium falciparum drug resistance is outpacing new antimalarial development and compromising effective malaria treatment. Combination therapy is widely implemented to prolong the effectiveness of currently approved antimalarials. To maximize utility of available drugs, periodic monitoring of drug efficacy and gathering of accurate information regarding parasite-sensitivity changes are essential. We describe a high-throughput, non-radioactive, field-based assay to evaluate in vitro antimalarial drug sensitivity of P. falciparum isolates from 40 Senegalese patients. Compared with earlier years, we found a significant decrease in chloroquine in vitro and in genotypic resistances (> 50% and > 65%, respectively, in previous studies) with only 23% of isolates showing resistance. This is possibly caused by a withdrawal of chloroquine from Senegal in 2002. We also found a range of artemisinin responses. Prevalence of drug resistance is dynamic and varies by region. Therefore, the implementation of non-radioactive, robust, high-throughput antimalarial sensitivity assays is critical for defining region-specific prophylaxis and treatment guidelines.
机译:恶性疟原虫耐药性的蔓延超过了新的抗疟疾发展,并削弱了有效的疟疾治疗。广泛使用联合疗法以延长目前批准的抗疟药的有效性。为了最大程度地利用可用药物,定期监测药物功效并收集有关寄生虫敏感性变化的准确信息至关重要。我们描述了一种高通量,非放射性,基于现场的测定方法,以评估来自40个塞内加尔患者的恶性疟原虫分离株的体外抗疟药敏感性。与早些年相比,我们发现氯喹的体外和基因型耐药性显着降低(在以前的研究中分别为> 50%和> 65%),只有23%的分离株显示出耐药性。这可能是由于2002年从塞内加尔撤出氯喹引起的。我们还发现了一系列的青蒿素反应。耐药性的流行是动态的,并且随地区而变化。因此,实施非放射性,稳健,高通量的抗疟疾敏感性测定方法对于定义区域特异性的预防和治疗指南至关重要。

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