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伊曲康唑是一种细胞色素 P450 抑制剂,可增强吡喹酮对曼氏血吸虫感染的疗效,并减轻小鼠的肝损伤。

Itraconazole, a cytochrome P450 inhibitor, enhanced the efficacy of praziquantel against Schistosoma mansoni infection and alleviated liver injury in mice.

机构信息

Professor of Pharmacology, Theodor Bilharz Research Institute, Giza, Egypt.

Lecturer of Pharmacology, Theodor Bilharz Research Institute, Giza, Egypt.

出版信息

Exp Parasitol. 2022 Aug;239:108293. doi: 10.1016/j.exppara.2022.108293. Epub 2022 Jun 3.

DOI:10.1016/j.exppara.2022.108293
PMID:35667394
Abstract

Treatment of schistosomiasis is heavily reliant on the single antischistosomal drug praziquantel (PZQ). The use of synergistic drug-drug interactions is one possible solution, which could be used to mitigate PZQ's poor and variable bioavailability. Itraconazole (ITZ), a triazole antifungal agent, is a potent CYP3A inhibitor that can cause significant drug-drug interactions when used with CYP3A substrates. This study investigates the effect of ITZ as adjuvant therapy with PZQ on worm load, egg deposition and maturation, and the consequent histopathology and biochemical abnormalities in the liver during the immature and mature stages of Schistosoma mansoni (S. mansoni) infection. S. mansoni-infected mice were divided into five groups of eight-ten mice each: (I) infected untreated, (II) infected and treated with PZQ 3 weeks PI, (III) infected and treated with both ITZ and PZQ 3 weeks PI, (IV) infected and treated with PZQ 7 weeks PI, and (V) infected and treated with both ITZ and PZQ 7 weeks PI. All mice were killed by rapid decapitation 9 weeks PI. Data revealed that ITZ in combination with PZQ at both immature and mature stages improved the parasitological criteria of cure, and greatly reduced inflammation, granuloma and fibrotic tissue formation, and apoptosis versus PZQ alone. Furthermore, it showed the greatest impact on improving liver injury and oxidative stress markers. Notably, the effect was considerably stronger at the mature stage of S. mansoni infection. These findings support the notion that ITZ increased PZQ's antischistosomal activity by inhibiting CYP450 expression, potentially reducing PZQ metabolism and increasing systemic exposure.

摘要

血吸虫病的治疗严重依赖于唯一的抗血吸虫药物吡喹酮(PZQ)。利用协同的药物-药物相互作用是一种可能的解决方案,可以用来减轻 PZQ 较差和可变的生物利用度。伊曲康唑(ITZ)是一种三唑类抗真菌药物,是一种强效的 CYP3A 抑制剂,当与 CYP3A 底物一起使用时,会引起显著的药物-药物相互作用。本研究探讨了 ITZ 作为辅助治疗与 PZQ 对曼氏血吸虫(S. mansoni)感染的未成熟和成熟阶段的虫负荷、卵沉积和成熟以及随后的肝组织病理学和生化异常的影响。曼氏血吸虫感染的小鼠分为五组,每组 8-10 只:(I)感染未治疗,(II)感染并在感染后 3 周用 PZQ 治疗,(III)感染并用 ITZ 和 PZQ 治疗在感染后 3 周,(IV)感染并在感染后 7 周用 PZQ 治疗,(V)感染并用 ITZ 和 PZQ 治疗在感染后 7 周。所有小鼠在感染后 9 周通过快速断头处死。数据显示,ITZ 与 PZQ 在未成熟和成熟阶段联合使用可改善寄生虫学治愈标准,并大大减少炎症、肉芽肿和纤维组织形成以及凋亡与单独使用 PZQ 相比。此外,它对改善肝损伤和氧化应激标志物的影响最大。值得注意的是,这种效果在曼氏血吸虫感染的成熟阶段更为显著。这些发现支持了 ITZ 通过抑制 CYP450 表达增加 PZQ 的抗血吸虫活性的观点,这可能会降低 PZQ 的代谢并增加全身暴露。

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