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寄生虫过度感染和低剂量用药是抗疟药物产生抗药性的一个重要原因。

Hyperparasitaemia and low dosing are an important source of anti-malarial drug resistance.

机构信息

Mahidol - Oxford Tropical Medicine Research Unit, Faculty of Tropical Medicine, Mahidol University, 420/6 Rajvithi Road, Bangkok 10400, Thailand.

出版信息

Malar J. 2009 Nov 11;8:253. doi: 10.1186/1475-2875-8-253.

Abstract

BACKGROUND

Preventing the emergence of anti-malarial drug resistance is critical for the success of current malaria elimination efforts. Prevention strategies have focused predominantly on qualitative factors, such as choice of drugs, use of combinations and deployment of multiple first-line treatments. The importance of anti-malarial treatment dosing has been underappreciated. Treatment recommendations are often for the lowest doses that produce "satisfactory" results.

METHODS

The probability of de-novo resistant malaria parasites surviving and transmitting depends on the relationship between their degree of resistance and the blood concentration profiles of the anti-malarial drug to which they are exposed. The conditions required for the in-vivo selection of de-novo emergent resistant malaria parasites were examined and relative probabilities assessed.

RESULTS

Recrudescence is essential for the transmission of de-novo resistance. For rapidly eliminated anti-malarials high-grade resistance can arise from a single drug exposure, but low-grade resistance can arise only from repeated inadequate treatments. Resistance to artemisinins is, therefore, unlikely to emerge with single drug exposures. Hyperparasitaemic patients are an important source of de-novo anti-malarial drug resistance. Their parasite populations are larger, their control of the infection insufficient, and their rates of recrudescence following anti-malarial treatment are high. As use of substandard drugs, poor adherence, unusual pharmacokinetics, and inadequate immune responses are host characteristics, likely to pertain to each recurrence of infection, a small subgroup of patients provides the particular circumstances conducive to de-novo resistance selection and transmission.

CONCLUSION

Current dosing recommendations provide a resistance selection opportunity in those patients with low drug levels and high parasite burdens (often children or pregnant women). Patients with hyperparasitaemia who receive outpatient treatments provide the greatest risk of selecting de-novo resistant parasites. This emphasizes the importance of ensuring that only quality-assured anti-malarial combinations are used, that treatment doses are optimized on the basis of pharmacodynamic and pharmacokinetic assessments in the target populations, and that patients with heavy parasite burdens are identified and receive sufficient treatment to prevent recrudescence.

摘要

背景

防止抗疟药物耐药性的出现对于当前消除疟疾工作的成功至关重要。预防策略主要集中在定性因素上,例如药物的选择、联合用药和多种一线治疗方法的应用。抗疟治疗剂量的重要性一直被低估。治疗建议通常是使用产生“满意”结果的最低剂量。

方法

新出现的抗疟寄生虫耐药性疟原虫存活和传播的概率取决于它们的耐药程度与它们所暴露的抗疟药物的血液浓度曲线之间的关系。检查了体内选择新出现的抗疟药物耐药性寄生虫所需的条件,并评估了相对概率。

结果

复发是新出现的耐药性传播的关键。对于快速消除的抗疟药物,高等级耐药性可能仅来自单次药物暴露,但低等级耐药性仅来自重复的不充分治疗。因此,单次药物暴露不太可能出现对抗疟药物的耐药性。高寄生虫血症患者是新出现的抗疟药物耐药性的重要来源。他们的寄生虫种群更大,对感染的控制不足,并且在抗疟药物治疗后复发的比率很高。由于使用不合格药物、不遵医嘱、异常药代动力学和免疫反应不足是宿主特征,可能与每次感染复发有关,一小部分患者提供了有利于新出现的耐药性选择和传播的特殊情况。

结论

目前的剂量建议在药物水平低且寄生虫负荷高的患者(通常是儿童或孕妇)中提供了耐药性选择的机会。接受门诊治疗的高寄生虫血症患者存在选择新出现的耐药寄生虫的最大风险。这强调了确保仅使用质量保证的抗疟药物组合、根据目标人群的药效学和药代动力学评估优化治疗剂量以及识别并为高寄生虫血症患者提供足够的治疗以防止复发的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f3f/2784792/63502f3dcfb8/1475-2875-8-253-1.jpg

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