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Effects of Artesunate on Parasite Recrudescence and Dormancy in the Rodent Malaria Model Plasmodium vinckei

机译:青蒿琥酯对啮齿类疟疾温氏疟原虫寄生虫再休眠和休眠的影响

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摘要

Artemisinin (ART) is the recommended first line therapy for treating uncomplicated and drug-resistant Plasmodium falciparum, the most pathogenic form of malaria. However, treatment failure following ART monotherapy is not uncommon and resistance to this rapidly acting drug has been reported in the Thai-Cambodian border. Recent in vitro studies have shown that following treatment with dihydroartemisinin (DHA), the development of ring-stage parasites is arrested for up to 20 days. These arrested (i.e. dormant) rings could be responsible for the recrudescence of infection that is observed following ART monotherapy. To develop a better understanding of the stage-specific effects of ART and determine if dormancy occurs in vivo, the ART derivative artesunate (AS) was used to treat mice infected with the synchronous rodent malaria parasites P. vinckei petteri (non-lethal) and P. v. vinckei (lethal). show that in both the non-lethal and lethal strains, ring-stage parasites are the least susceptible to treatment with AS and that the day of treatment has more of an impact on recrudescence than the total dose administered. Additionally, 24 hrs post-treatment with AS, dormant forms similar in morphology to those seen in vitro were observed. Finally, rate of recrudescence studies suggest that there is a positive correlation between the number of dormant parasites present and when recrudescence occurs in the vertebrate host. Collectively, these data suggest that dormancy occurs in vivo and contributes to recrudescence that is observed following AS treatment. It is possible that this may represent a novel mechanism of parasite survival following treatment with AS.
机译:青蒿素(ART)是推荐的一线疗法,可用于治疗最简单且耐药的恶性疟原虫(疟疾的致病性最高的形式)。但是,ART单一疗法后的治疗失败并不罕见,泰国-柬埔寨边境已经报道了对该快速反应药物的耐药性。最近的体外研究表明,在用双氢青蒿素(DHA)治疗后,环状阶段寄生虫的发育被阻止长达20天。这些停滞(即休眠)的环可能是ART单一疗法后观察到的感染复发的原因。为了更好地了解ART的阶段特异性作用并确定体内是否发生休眠,ART衍生物青蒿琥酯(AS)用于治疗感染了同步啮齿动物疟疾寄生虫vinckei petteri(非致死性)的小鼠。 P. v。Vinckei(致命)。结果表明,在非致死性和致死性菌株中,环期寄生虫对AS的治疗最不敏感,并且治疗当天对复发的影响大于总剂量。另外,在用AS处理24小时后,观察到了休眠形态,其形态类似于体外观察到的形态。最后,再发率研究表明,存在的休眠寄生虫数量与脊椎动物宿主再发时呈正相关。总体而言,这些数据表明休眠发生在体内,并有助于AS治疗后观察到的复发。这可能代表了AS治疗后寄生虫存活的新机制。

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