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慢性恰加斯病中苯硝唑单药治疗及与伏沙康唑联合治疗的群体药代动力学-药效学分析(BENDITA)

Population pharmacokinetic-pharmacodynamic analysis of benznidazole monotherapy and combination therapy with fosravuconazole in chronic Chagas disease (BENDITA).

作者信息

Assmus Frauke, Cruz Cintia, Watson James A, White Nicholas J, Adehin Ayorinde, Hoglund Richard M, Blum de Oliveira Bethania, Barreira Fabiana, Scandale Ivan, Tarning Joel

机构信息

Mahidol Oxford Tropical Medicine Research Unit, Faculty of Tropical Medicine, Mahidol University, Bangkok, Thailand.

Centre for Tropical Medicine and Global Health, Nuffield Department of Medicine, University of Oxford, Oxford, United Kingdom.

出版信息

PLoS Negl Trop Dis. 2025 Sep 22;19(9):e0013522. doi: 10.1371/journal.pntd.0013522. eCollection 2025 Sep.

DOI:10.1371/journal.pntd.0013522
PMID:40982532
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12510642/
Abstract

INTRODUCTION

The currently recommended 8-week daily benznidazole regimen for Chagas disease is poorly tolerated. While shorter benznidazole monotherapy and combination regimens have been explored, the pharmacokinetic/pharmacodynamic (PK/PD) relationship remains poorly understood.

OBJECTIVES

i) To describe the population pharmacokinetics of benznidazole and assess drug-drug interactions with fosravuconazole in patients with chronic Chagas disease, ii) to explore the relationship between benznidazole exposure and anti-trypanosomal treatment effects.

METHODS

This was a secondary analysis based on data from the previously published BENDITA study (NCT03378661), a dose evaluation trial in adults with chronic indeterminate Chagas disease (n = 210). Patients were randomized to placebo, the standard benznidazole dose (300 mg/day for 8 weeks), or lower total dose regimens (300 mg/day for 4 or 2 weeks; 150 mg/day for 4 weeks alone or combined with fosravuconazole 300 mg/week; 300 mg/week for 8 weeks plus fosravuconazole 300 mg/week). Benznidazole pharmacokinetics were evaluated using nonlinear mixed-effects modeling. The relationship between individual benznidazole exposure and the pharmacodynamic (PD) endpoint was explored using beta binomial regression. The PD endpoint (qPCR positivity) was defined as the proportion of qPCR-positive blood samples collected post-treatment over 12 months of follow-up, capturing the frequency of detectable parasitemia per patient.

RESULTS

Benznidazole pharmacokinetics were well described by a transit-absorption model with one-compartment disposition. Bioavailability was 13% lower in men than in women, and coadministration of fosravuconazole increased benznidazole clearance by 18% (both effects considered not clinically relevant). In the placebo arm, nearly all patients (97%) remained qPCR positive, with most showing qPCR positivity above 40%. Among patients receiving benznidazole, post-treatment qPCR positivity was substantially lower. In the 2-week arm, three patients had multiple positive qPCR samples (up to 43% PCR positivity). In contrast, individual qPCR positivity in the 4-8-week arms did not exceed 20% (i.e., one or no positive samples), with one non-adherent exception. The PK/PD analysis did not identify a significant pharmacokinetic driver of treatment response. While the study was not powered for between-arm comparisons, the findings suggest that lower total dose regimens (4 weeks daily or 8 weeks weekly) may provide efficacy comparable to the standard 8-week regimen.

CONCLUSION

This study supports prior findings that the standard 8-week benznidazole regimen is excessive. Future trials using qPCR in factorial randomized designs should evaluate both treatment duration and dosing to optimize tolerability while maintaining efficacy.

摘要

引言

目前推荐的用于治疗恰加斯病的8周每日苯硝唑治疗方案耐受性较差。虽然已经探索了更短疗程的苯硝唑单药治疗和联合治疗方案,但对其药代动力学/药效学(PK/PD)关系仍知之甚少。

目的

i)描述苯硝唑在慢性恰加斯病患者中的群体药代动力学,并评估其与伏沙康唑的药物相互作用;ii)探索苯硝唑暴露量与抗锥虫治疗效果之间的关系。

方法

这是一项基于先前发表的BENDITA研究(NCT03378661)数据的二次分析,该研究是一项针对慢性不确定型恰加斯病成人患者(n = 210)的剂量评估试验。患者被随机分为安慰剂组、标准苯硝唑剂量组(300 mg/天,共8周)或较低总剂量方案组(300 mg/天,共4或2周;150 mg/天,单独使用4周或与伏沙康唑300 mg/周联合使用;300 mg/周,共8周加伏沙康唑300 mg/周)。使用非线性混合效应模型评估苯硝唑的药代动力学。使用贝塔二项式回归探索个体苯硝唑暴露量与药效学(PD)终点之间的关系。PD终点(qPCR阳性)定义为治疗后12个月随访期间收集的qPCR阳性血样的比例,反映每位患者可检测到的寄生虫血症频率。

结果

苯硝唑的药代动力学可用具有单室处置的转运吸收模型很好地描述。男性的生物利用度比女性低13%,伏沙康唑的联合使用使苯硝唑清除率提高了18%(两种效应均被认为与临床无关)。在安慰剂组中,几乎所有患者(97%)qPCR仍为阳性,大多数患者的qPCR阳性率高于40%。在接受苯硝唑治疗的患者中,治疗后qPCR阳性率显著降低。在2周治疗组中,有3名患者的qPCR样本多次呈阳性(PCR阳性率高达43%)。相比之下,4 - 8周治疗组中的个体qPCR阳性率不超过20%(即一个或无阳性样本),有一个未依从的例外情况。PK/PD分析未发现治疗反应的显著药代动力学驱动因素。虽然该研究没有足够的能力进行组间比较,但研究结果表明,较低总剂量方案(每日4周或每周8周)可能提供与标准8周方案相当的疗效。

结论

本研究支持先前的研究结果,即标准的8周苯硝唑治疗方案用药过量。未来使用qPCR进行析因随机设计的试验应评估治疗持续时间和给药剂量,以在保持疗效的同时优化耐受性。

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