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Antiparasitic Properties of Cardiovascular Agents against Human Intravascular Parasite Schistosoma mansoni

机译:心血管剂对人血管内寄生虫血吸虫的抗遗传性质

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摘要

The intravascular parasitic worm Schistosoma mansoni is a causative agent of schistosomiasis, a disease of great global public health significance. Praziquantel is the only drug available to treat schistosomiasis and there is an urgent demand for new anthelmintic agents. Adopting a phenotypic drug screening strategy, here, we evaluated the antiparasitic properties of 46 commercially available cardiovascular drugs against S. mansoni. From these screenings, we found that amiodarone, telmisartan, propafenone, methyldopa, and doxazosin affected the viability of schistosomes in vitro, with effective concentrations of 50% (EC50) and 90% (EC90) values ranging from 8 to 50 µM. These results were further supported by scanning electron microscopy analysis. Subsequently, the most effective drug (amiodarone) was further tested in a murine model of schistosomiasis for both early and chronic S. mansoni infections using a single oral dose of 400 mg/kg or 100 mg/kg daily for five consecutive days. Amiodarone had a low efficacy in chronic infection, with the worm and egg burden reduction ranging from 10 to 30%. In contrast, amiodarone caused a significant reduction in worm and egg burden in early infection (>50%). Comparatively, treatment with amiodarone is more effective in early infection than praziquantel, demonstrating the potential role of this cardiovascular drug as an antischistosomal agent.
机译:血管内寄生虫血吸虫曼逊是一种血吸虫病的致病因子,其疾病巨大的全球性公众健康意义。 Praziquantel是唯一可治疗血吸虫病的药物,并且对新的Anthelmintic代理人进行了紧迫的需求。在这里,采用表型药物筛选策略,我们评估了46个市售心血管药物的抗促进性质,对阵Mansoni。从这些筛查中发现,胺碘酮,替米沙坦,丙唑胺,甲基甲戊基和多唑嗪在体外影响血吸虫的可行性,有效浓度为50%(EC50)和90%(EC90)值范围为8至50μm。通过扫描电子显微镜分析进一步支持这些结果。随后,在连续五天每天使用400mg / kg或100mg / kg的单次口服剂量,在早期和慢性S. mansoni感染中进一步测试最有效的药物(胺碘酮)在血吸虫病的鼠模型中进行了进一步测试。胺碘酮对慢性感染的疗效低,蠕虫和蛋负荷减少的10%至30%。相比之下,胺碘酮导致早期感染的蠕虫和卵子负担显着降低(> 50%)。相比之下,胺碘酮的处理在早期感染中比吡喹酮更有效,展示了这种心血管药物作为抗血栓药剂的潜在作用。

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