Quantifying Plasmodium vivax radical cure efficacy: a modelling study integrating clinical trial data and transmission dynamics

IF 36.4 1区医学 Q1 INFECTIOUS DISEASES

Lancet Infectious Diseases Pub Date : 2025-01-13 DOI:10.1016/s1473-3099(24)00689-3

Constanze Ciavarella, Chris Drakeley, Ric N Price, Ivo Mueller, Michael White

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引用次数: 0

Abstract

Background

Plasmodium vivax forms dormant liver stages (hypnozoites) that can reactivate weeks to months after primary infection. Radical cure requires a combination of antimalarial drugs to kill both the blood-stage and liver-stage parasites. Hypnozoiticidal efficacy of the liver-stage drugs primaquine and tafenoquine cannot be estimated directly because hypnozoites are undetectable. We aimed to estimate hypnozoiticidal efficacy from clinical trial data, and quantify the community-level impact of implementing case management with radical cure.

Methods

We calibrated a novel P vivax Recurrence Model to publicly available data from prospective clinical trials to estimate the hypnozoiticidal efficacy of different supervised primaquine (3·5 mg/kg or 7 mg/kg over 7 or 14 days) and tafenoquine (5 mg/kg or 7·5 mg/kg single dose) regimens in patients with normal glucose-6-phosphate dehydrogenase (G6PD) activity. We used an existing P vivax Individual-Based Model to quantify the 5-year impact of case management with unsupervised primaquine or tafenoquine regimens across various transmission settings.

Findings

We estimated median hypnozoiticidal efficacies of 99·1% (95% credible interval 96·0–100) for primaquine 7 mg/kg over 14 days; 96·3% (90·8–99·7) for primaquine 7 mg/kg over 7 days; 72·3% (68·1–76·3) for primaquine 3·5 mg/kg over 7 or 14 days; 62·4% (49·1–76·3) for tafenoquine 5 mg/kg single dose; and 87·5% (62·1–99·3) for tafenoquine 7·5 mg/kg single dose. 5 years of community-level tafenoquine case management was estimated to reduce P vivax transmission by 74–79% where pre-intervention prevalence as measured by PCR was low (<2%) and by 17–20% where prevalence as measured by PCR was high (around 35%). Similar 5-year reductions were estimated with primaquine case management only when adherence to the primaquine regimen was above 50%.

Interpretation

Substantial reductions in prevalence as measured by PCR were predicted with primaquine and tafenoquine regimens if these could be implemented with high coverage and adherence. The benefits of preventing P vivax relapses need to be balanced against the risks of inducing severe haemolysis in patients with G6PD deficiency.

Funding

Bill & Melinda Gates Foundation and Horizon Europe.

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量化间日疟原虫根治疗效：整合临床试验数据和传播动态的建模研究

背景间日疟原虫（Plasmodium vivax）会在肝脏中形成休眠期寄生虫（hypnozoites），这些寄生虫会在原发性感染数周至数月后重新活化。根治需要联合使用多种抗疟药物，以杀死血期和肝期寄生虫。肝阶段药物伯氨喹和他非诺喹的杀亚寄生虫疗效无法直接估算，因为无法检测到亚寄生虫。我们的目标是根据临床试验数据估算低佐虫杀灭效果，并量化实施根治性病例管理对社区的影响。方法我们根据前瞻性临床试验的公开数据校准了新型间日疟复发模型，以估算在葡萄糖-6-磷酸脱氢酶（G6PD）活性正常的患者中，不同的伯氨喹（3-5 毫克/千克或 7 毫克/千克，7 天或 14 天）和他非诺喹（5 毫克/千克或 7-5 毫克/千克，单剂量）督导方案的降虫疗效。我们利用现有的基于个体的鼠疫模型，量化了在不同传播环境下使用无监督伯氨喹或他喹方案进行病例管理的 5 年影响。研究结果我们估计，伯氨喹 7 毫克/千克，14 天的中位杀虫效果为 99-1%（95% 可信区间为 96-0-100）；伯氨喹 7 毫克/千克，7 天的中位杀虫效果为 96-3%（90-8-99-7）；伯氨喹 3-5 毫克/千克，7 天或 14 天的中位杀虫效果为 72-3%（68-1-76-3）；他芬喹 5 毫克/千克，单剂量的中位杀虫效果为 62-4%（49-1-76-3）；他芬喹 7-5 毫克/千克，单剂量的中位杀虫效果为 87-5%（62-1-99-3）。据估计，如果干预前通过 PCR 测定的流行率较低（2%），5 年的社区级他芬喹病例管理可将间日疟原虫传播率降低 74-79%；如果通过 PCR 测定的流行率较高（约 35%），则可降低 17-20%。只有在伯氨喹治疗方案的依从性超过 50%时，伯氨喹病例管理的 5 年减少率估计与此相似。释义如果伯氨喹和他非诺喹治疗方案能够在高覆盖率和依从性的情况下实施，则根据 PCR 测量的流行率预计会大幅下降。预防间日疟复发的益处需要与诱发 G6PD 缺乏症患者严重溶血的风险相平衡。

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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来源期刊

Lancet Infectious Diseases 医学-传染病学

CiteScore

60.90

自引率

0.70%

发文量

1064

审稿时长

6-12 weeks

期刊介绍： The Lancet Infectious Diseases was launched in August, 2001, and is a lively monthly journal of original research, review, opinion, and news covering international issues relevant to clinical infectious diseases specialists worldwide.The infectious diseases journal aims to be a world-leading publication, featuring original research that advocates change or sheds light on clinical practices related to infectious diseases. The journal prioritizes articles with the potential to impact clinical practice or influence perspectives. Content covers a wide range of topics, including anti-infective therapy and immunization, bacterial, viral, fungal, and parasitic infections, emerging infectious diseases, HIV/AIDS, malaria, tuberculosis, mycobacterial infections, infection control, infectious diseases epidemiology, neglected tropical diseases, and travel medicine. Informative reviews on any subject linked to infectious diseases and human health are also welcomed.