在泰国试点实施期间,进行前瞻性观察性研究,以评估定量葡萄糖-6-磷酸脱氢酶(G6PD)检测后使用他非诺喹或伯氨喹进行适当根治的可行性和安全性。
Prospective observational study to assess the feasibility and safety of appropriate radical cure with tafenoquine or primaquine after quantitative G6PD testing during pilot implementation in Thailand.
作者信息
Sudathip Prayuth, Khantikul Nardlada, Saejeng Aungkana, Duparc Stephan, Grewal Daumerie Penny, Lynch Caroline, Jambert Elodie, Viboonsanti Saowanee, Areechokchai Darin, Kanjanasuwan Jerdsuda, Thong-Ard Thannika, Kowsurat Panupong, Borghini-Fuhrer Isabelle, Padungtod Chantana
机构信息
Department of Disease Control, Ministry of Public Health, Nonthaburi, Thailand
The Office of Disease Prevention and Control 1 Chiangmai, Division of Vector Borne Diseases, Ministry of Public Health, Nonthaburi, Thailand.
出版信息
BMJ Glob Health. 2025 Apr 24;10(4):e016720. doi: 10.1136/bmjgh-2024-016720.
INTRODUCTION
recurrence prevention using tafenoquine or primaquine is critical for achieving Thailand's malaria elimination targets. Both drugs may cause haemolysis in glucose-6-phosphate dehydrogenase (G6PD) deficient individuals. This study evaluated the operational feasibility and safety of administering tafenoquine or primaquine after quantitative G6PD point-of-care testing in Thailand.
METHODS
This prospective, observational, multicentre, longitudinal study was conducted between 23 May 2022 and 14 September 2023 during pilot implementation at seven sites in Yala and Mae Hong Son provinces. Eligible patients were ≥16 years old with uncomplicated malaria. G6PD enzyme activity was quantified using a point-of-care device. All patients received 3-day chloroquine plus (based on G6PD enzyme activity): single-dose tafenoquine 300 mg (≥6.1 U/g Hb), or primaquine 15 mg/day for 14 days (≥4.1 U/g Hb), or primaquine 45 mg/week for 8 weeks (≤4.0 U/g Hb), with follow-up on days 5 and 14. Hospital admissions were reviewed to confirm acute haemolytic anaemia cases. The primary endpoint was the percentage of patients ≥16 years old treated or not treated with tafenoquine in accordance with G6PD enzyme activity.
RESULTS
Of 316 . patients screened, 187 were enrolled. All patients completed quantitative G6PD testing. According to G6PD status, appropriate use or non-use was 100% (95% CI 97.2, 100 (132/132)) with tafenoquine, 100% (95% CI 96.5, 100 (104/104)) with daily primaquine and 99.5% (97.1, 100 (186/187)) with weekly primaquine. At day 5, adverse events possibly related to haemolysis occurred in 46.3% (37/80) of patients with tafenoquine, 56.8% (46/81) with daily primaquine and 77.8% (14/18) with weekly primaquine, with no confirmed drug-induced acute haemolytic anaemia cases.
CONCLUSION
Point-of-care quantitative G6PD testing prior to appropriate tafenoquine or primaquine administration was operationally feasible within the Thailand health system, with no concerning adverse events, supporting implementation of this treatment algorithm in areas of active transmission.
引言
使用他非诺喹或伯氨喹预防复发对于实现泰国的疟疾消除目标至关重要。这两种药物都可能在葡萄糖-6-磷酸脱氢酶(G6PD)缺乏的个体中引起溶血。本研究评估了在泰国进行即时定量G6PD检测后给予他非诺喹或伯氨喹的操作可行性和安全性。
方法
这项前瞻性、观察性、多中心纵向研究于2022年5月23日至2023年9月14日在也拉府和夜丰颂府的7个地点进行试点实施期间开展。符合条件的患者年龄≥16岁,患有非复杂性疟疾。使用即时检测设备对G6PD酶活性进行定量。所有患者接受3天氯喹加(根据G6PD酶活性):单剂量他非诺喹300毫克(G6PD酶活性≥6.1 U/g Hb),或伯氨喹15毫克/天,共14天(G6PD酶活性≥4.1 U/g Hb),或伯氨喹45毫克/周,共8周(G6PD酶活性≤4.0 U/g Hb),并在第5天和第14天进行随访。审查医院入院情况以确认急性溶血性贫血病例。主要终点是根据G6PD酶活性接受或未接受他非诺喹治疗的≥16岁患者的百分比。
结果
在316名筛查患者中,187名被纳入研究。所有患者均完成了G6PD定量检测。根据G6PD状态,他非诺喹的正确使用或不使用比例为100%(95%CI 97.2,100(132/132)),每日服用伯氨喹的比例为100%(95%CI 96.5,100(104/104)),每周服用伯氨喹的比例为99.5%(97.1,100(186/187))。在第5天,他非诺喹组4百分之6.3(37/80)的患者发生了可能与溶血相关的不良事件,每日服用伯氨喹组为56.8%(46/81),每周服用伯氨喹组为77.8%(14/18),没有确诊的药物性急性溶血性贫血病例。
结论
在泰国卫生系统中,在适当使用他非诺喹或伯氨喹之前进行即时定量G6PD检测在操作上是可行的,且没有令人担忧的不良事件,支持在疟疾活跃传播地区实施这种治疗方案。
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