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蒿甲醚与吡喹酮:起源、作用方式、影响及有效控制人类血吸虫病的建议应用

Artemether and Praziquantel: Origin, Mode of Action, Impact, and Suggested Application for Effective Control of Human Schistosomiasis.

作者信息

Bergquist Robert, Elmorshedy Hala

机构信息

Ingerod, SE-454 94 Brastad, Sweden.

College of Medicine, Princess Nourah bint Abdulrahman University, Riyadh 11671, Saudi Arabia.

出版信息

Trop Med Infect Dis. 2018 Dec 19;3(4):125. doi: 10.3390/tropicalmed3040125.

Abstract

The stumbling block for the continued, single-drug use of praziquantel (PZQ) against schistosomiasis is less justified by the risk of drug resistance than by the fact that this drug is inactive against juvenal parasites, which will mature and start egg production after chemotherapy. Artemisinin derivatives, currently used against malaria in the form of artemisinin-based combination therapy (ACT), provide an opportunity as these drugs are not only active against malaria plasmodia, but surprisingly also against juvenile schistosomes. An artemisinin/PZQ combination would be complimentary, and potentially additive, as it would kill two schistosome life cycle stages and thus confer a transmission-blocking modality to current chemotherapy. We focus here on single versus combined regimens in endemic settings. Although the risk of artemisinin resistance, already emerging with respect to malaria therapy in Southeast Asia, prevents use in countries where ACT is needed for malaria care, an artemisinin-enforced praziquantel treatment (APT) should be acceptable in North Africa (including Egypt), the Middle East, China, and Brazil, as these countries are not endemic for malaria. Thanks to recent progress with respect to high-resolution diagnostics, based on circulating schistosome antigens in humans and molecular approaches for snail surveys, it should be possible to keep areas scheduled for schistosomiasis elimination under surveillance, bringing rapid response to bear on problems arising. The next steps would be to investigate where and for how long APT should be applied to make a lasting impact. A large-scale field trial in an area with modest transmission should tell how apt this approach is.

摘要

吡喹酮(PZQ)持续单一用药治疗血吸虫病的障碍,与其说是耐药风险,不如说是该药物对幼年寄生虫无活性这一事实,这些幼年寄生虫在化疗后会成熟并开始产卵。目前以青蒿素联合疗法(ACT)形式用于治疗疟疾的青蒿素衍生物提供了一个机会,因为这些药物不仅对疟原虫有活性,而且令人惊讶的是对幼年血吸虫也有活性。青蒿素/吡喹酮联合用药将具有互补性,甚至可能具有相加作用,因为它能杀死血吸虫生命周期的两个阶段,从而为当前的化疗赋予一种阻断传播的方式。我们在此关注的是流行地区的单一疗法与联合疗法。尽管青蒿素耐药性风险在东南亚的疟疾治疗中已经出现,这使得在需要ACT治疗疟疾的国家无法使用,但在北非(包括埃及)、中东、中国和巴西,青蒿素强化吡喹酮治疗(APT)应该是可以接受的,因为这些国家并非疟疾流行区。由于基于人体循环血吸虫抗原和蜗牛调查分子方法的高分辨率诊断技术取得了最新进展,应该能够对计划消除血吸虫病的地区进行监测,对出现的问题迅速做出反应。接下来的步骤将是研究APT应在何处应用以及应用多长时间才能产生持久影响。在一个传播程度适中的地区进行大规模现场试验将能说明这种方法的适用性如何。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/de91/6306701/a90f12df560b/tropicalmed-03-00125-g001.jpg

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