Effects of the antimalarial drugs ferroquine and artesunate on Plasmodium yoelii yoelii gametocytegenesis and vectorial transmission.

Kamla Mustfa, Irène Landau, Alain-Gabriel Chabaud, Jean-Marc Chavatte, Jacques Chandenier, Thanh Hai Duong, Dominique Richard-Lenoble
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引用次数: 3

Abstract

Chemistry still has a role in the management of malaria, alongside the mosquito netting soaked in insecticide that is used increasingly, as we continue to await the long anticipated vaccine. During its cycle, the hematozoon parasite develops through three major periods. The first, malarial infection, corresponds to the intrahepatic development of infective forms from the mosquito vector; this period is not sensitive to treatment and is often asymptomatic. The period of erythrocytic schizogony is the most urgent, and treatment activity is primordial. Finally, the phase of sexual reproduction, when gametocytes develop within the erythrocytes ensures the perpetuation of the species when these reach the blood-feeding female anopheles mosquitoes. The aim of our work was to study the effect on gametocytes of drugs known to be effective on the asexual blood forms of the protozoan and thus the potential repercussions on malaria transmission. This experimental study was conducted with an animal model whose parasite cycle and modes of transmission are close to those of human malaria: Plasmodium yoelii, maintained on Swiss mice, with the Anopheles stephensi vector (maintained in an animal facility at the National Museum of Natural History in Paris). Two drugs were tested: ferroquine (a chloroquine derivative with a ferrocene molecule at the lateral carbon chain that restores its efficacy against chloroquine-resistant strains) and artesunate (a derivative of artemisinin, from ginghao, a Chinese plant also known as artemisia annua, or sweet wormwood), a treatment of choice in the combined therapies recommended by WHO. The efficacy of these drugs, prescribed at doses subcurative for the asexual forms, were tested against gametocyte production, quantitatively by counting them in the blood and qualitatively by counting the quantity of oocysts developed on the mosquito's midgut, which are indicators of gametocyte activity. The mice that were parasite-infected and then treated served as their own controls: lots of 30 mosquitoes fed on each mouse before treatment and then 90  minutes and 5  hours after treatment. Quantitatively, the comparison of the blood parasite level and the gametocyte index shows that treated mice had a higher level of circulating gametocytes than untreated parasite infested mice, regardless of drug or dose (5 or 10  mg/kg). For artesunate at 5  mg/kg, we noted that the blood gametocyte level was almost double that of the controls. On the other hand, qualitatively, the first results obtained with optical and electronic microscopy showed morphologic alterations of the circulating gametocytes (pigment clumping and lateralisation within red blood cells) and reduced infectivity of the gametocytes for the mosquitoes that fed at 1 and 5  hours after treatment. We were able to demonstrate statistically that the infectivity of gametocytes, measured by the quantity of oocysts counted in the mosquito midgut, was reduced by 70% for those treated with ferroquine and by 85% for those from mice treated by artesunate. Complementary studies will seek to specify the populations (age) of gametocytes damaged by treatment and the importance and nature of their morphologic alterations.

抗疟药物亚铁喹和青蒿琥酯对约尔疟原虫配子细胞发生和媒介传播的影响。
在我们继续等待期待已久的疫苗问世之际,化学在疟疾管理中仍然发挥着作用,同时也在越来越多地使用浸泡在杀虫剂中的蚊帐。在其周期中,血吸虫寄生虫的发育经历三个主要时期。第一种是疟疾感染,与来自蚊子媒介的感染形式的肝内发展相对应;这一时期对治疗不敏感,通常无症状。红细胞分裂的时期是最紧迫的,治疗活动是原始的。最后,有性繁殖阶段,当配子体在红细胞内发育时,当这些配子体到达吸血的雌性按蚊时,确保了物种的延续。我们的工作目的是研究已知对原生动物无性血型有效的药物对配子体的影响,从而对疟疾传播产生潜在影响。这项实验研究是用一种动物模型进行的,其寄生虫周期和传播方式与人类疟疾的周期和传播方式接近:在瑞士小鼠身上维持的约利疟原虫,以及在巴黎国家自然历史博物馆动物设施中维持的斯氏按蚊载体。试验了两种药物:亚铁喹(一种氯喹衍生物,在侧碳链上有二茂铁分子,可恢复其对氯喹耐药菌株的效力)和青蒿琥酯(青蒿素的衍生物,来自青蒿,一种中国植物,也称为青蒿或蒿),这是世卫组织推荐的联合疗法中的一种选择。这些药物的剂量低于治疗剂量,用于治疗无性繁殖的蚊子。研究人员测试了这些药物对配子细胞产生的影响,定量方法是计算蚊子血液中的配子细胞数量,定性方法是计算蚊子中肠上卵囊的数量,卵囊是配子细胞活性的指标。被寄生虫感染并接受治疗的小鼠作为自己的对照:在治疗前和治疗后90分钟和5小时,每只小鼠分别被30只蚊子叮咬。定量地比较血液寄生虫水平和配子体指数表明,无论药物或剂量(5或10 mg/kg),治疗小鼠的循环配子体水平均高于未治疗的寄生虫感染小鼠。对于5 mg/kg的青蒿琥酯,我们注意到血液配子细胞水平几乎是对照组的两倍。另一方面,通过光学和电子显微镜获得的第一个定性结果显示,在治疗后1和5小时进食的蚊子循环配子细胞的形态改变(红细胞内色素聚集和偏侧化),配子细胞的传染性降低。我们能够从统计学上证明配子体的传染性,通过计算蚊子中肠中卵囊的数量来衡量,用亚铁喹治疗的小鼠的感染性降低了70%,用青蒿琥酯治疗的小鼠的感染性降低了85%。补充研究将寻求明确受治疗损害的配子体的种群(年龄)及其形态改变的重要性和性质。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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