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The Use of Artemether-Lumefantrine for the Treatment of Uncomplicated Plasmodium vivax Malaria

机译:蒿甲醚-卢美他汀在单纯性间日疟原虫疟疾治疗中的应用

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摘要

The long-standing dearth of knowledge surrounding Plasmodium vivax, the most widely distributed of the malaria species, merits urgent attention. A growing awareness of the true burden of this parasite and its potential to cause severe disease, and the identification of increasing parasite resistance in many areas of the world to chloroquine, the mainstay of vivax treatment, underscores the need to identify new and effective treatment strategies. Artemisinin-based combination therapies (ACTs) have been widely adopted as first-line treatment for P. falciparum malaria and would offer logistic benefits in areas of co-endemicity. However, while ACTs show high and similar efficacy against the blood stages of P. vivax, neither ACTs nor chloroquine are active against vivax hypnozoites and must be complemented with a full course of primaquine to eradicate dormant vivax hypnozoites and prevent relapses. Artemether-lumefantrine (AL), the most commonly deployed ACT, has shown rapid clearance of P. vivax parasitemia and fever. The relatively short half-life of lumefantrine would appear beneficial in terms of reducing risk of resistance when compared to other ACTs. However, it has a shorter capability to suppress vivax relapses or prevent de novo infections, which generally translates into comparatively lower in vivo short-term measures of efficacy (e.g., day 28 or day 42 uncorrected cure rates). Assuming that the different artemisinin derivatives have equivalent efficacy against vivax, differences between AL and other ACTs may be restricted to the duration of plasma therapeutic levels of the partner drug, a variable of limited clinical relevance, particularly in regions with low vivax transmission rates or in cases where primaquine is added to the regimen to prevent relapses. More rigorous assessment of the use of ACTs in general, and AL in particular, for the treatment of P. vivax infections, either alone or in combination with primaquine, is merited. In the meantime, AL treatment of vivax malaria may be a pragmatic choice for areas with chloroquine-resistant P. vivax, and in co-endemic areas where AL is already used routinely against P. falciparum and parasitological differentiation is not routinely performed or only clinical diagnosis is used.
机译:间日疟原虫(疟疾分布最广泛)周围的长期知识匮乏值得紧急关注。人们日益认识到这种寄生虫的真正负担及其潜在的导致严重疾病的能力,并认识到世界许多地区对寄生虫抗药性喹诺酮类药物的抗药性日益增强,这凸显了确定新的有效治疗策略的必要性。基于青蒿素的联合疗法(ACTs)已被广泛用作恶性疟原虫疟疾的一线治疗,将在共流行领域提供后勤方面的好处。但是,尽管ACTs对间日疟原虫的血液阶段显示出很高且相似的功效,但ACTs和氯喹均不对间日疟原虫具有活性,因此必须配合全程伯氨喹来根除休眠的间日疟原虫并防止复发。 Artemether-lumefantrine(AL)是最常用的ACT,已显示出间日疟原虫寄生虫病和发烧的快速清除。与其他ACT相比,lumantantrine相对较短的半衰期在降低耐药风险方面似乎是有益的。然而,它具有更短的抑制间日病毒复发或预防从头感染的能力,这通常转化为相对较低的体内短期疗效量度(例如,第28天或第42天未校正的治愈率)。假设不同的青蒿素衍生物具有同等的抗间充质功效,则AL和其他ACT之间的差异可能会限制于伴侣药物的血浆治疗水平持续时间,这是临床相关性有限的变量,特别是在间质传播率低或在方案中加入伯氨喹以防止复发的情况。通常,应更严格地评估ACTs的使用,特别是AL在单独或与伯氨喹联用治疗间日疟原虫感染中的应用。同时,AL治疗间日疟疾可能是对氯喹耐药的间日疟原虫区域的实用选择,而在已经普遍使用AL对抗恶性疟原虫且未常规进行寄生虫学鉴别或仅临床临床的共同流行地区诊断被使用。

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