A phase I, single-center, randomized, open-label, three-period crossover study to evaluate the drug-drug interaction between ZSP1273 and oseltamivir in healthy Chinese subjects.

IF 4.1 2区医学 Q2 MICROBIOLOGY

Antimicrobial Agents and Chemotherapy Pub Date : 2025-04-02 Epub Date: 2025-02-24 DOI:10.1128/aac.01729-24

Yanqing Pang, Haijun Li, Xuemei Chen, Yingying Cao, Hui Jiang, Jufang Huang, Yiming Liu

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引用次数: 0

Abstract

ZSP1273 is a novel small-molecule anti-influenza drug that targets the RNA polymerase PB2 subunit, while oseltamivir is the first-line medication that inhibits neuraminidase. ZSP1273 showed high efficacy against human influenza viruses both in vitro and in vivo, including oseltamivir-resistant strains in vitro. In future clinical applications, the combination of these two antiviral drugs with different mechanisms can reduce the potential for antiviral resistance that may arise from monotherapy. To evaluate the drug-drug interaction between ZSP1273 and oseltamivir by the pharmacokinetics and safety of co-administration in healthy subjects, a phase I, single-center, randomized, open-label, three-period crossover study was conducted. Thirty-six subjects enrolled were randomized in a 1:1:1 ratio into three crossover treatment sequences with oral administration detailed as follows: treatment A: ZSP1273 tablets 600 mg once daily (QD) for 5 days; treatment B: oseltamivir capsules 75 mg twice daily (BID) for 5 days; treatment C: ZSP1273 tablets 600 mg once daily (QD) + oseltamivir capsules 75 mg twice daily (BID) for 5 days. Plasma samples were collected from all subjects at scheduled time points after drug administration to measure the plasma concentrations of ZSP1273, oseltamivir, and its active metabolite oseltamivir carboxylate, for pharmacokinetic analysis. Compared with monotherapy, the geometric mean ratios (90% confidence intervals) of C_max,ss, AUC_0-t,ss, AUC_0-τ,ss, and AUC_0-∞,ss for ZSP1273 after co-administration were all within the ineffective boundary range of 80% to 125%, supporting that no drug-drug interaction occurs with ZSP1273. After co-administration, the AUC_0-t,ss, AUC_0-τ,ss, and AUC_0-∞,ss of oseltamivir were all within 80% to 125%, while C_max,ss decreased by 39.9%. The pharmacokinetic parameters above of oseltamivir carboxylate remained within 80%-125%, except only the lower bound of the 90% CI for C_max,ss slightly below 80% (77.0%). Considering the rapid metabolism of oseltamivir into the active metabolite oseltamivir carboxylate and the minor impact of co-administration on the pharmacokinetic parameters of oseltamivir carboxylate, it is believed that no clinically significant drug-drug interaction was observed with the combination of these two drugs. During the trial, the safety and tolerability of both combination therapy and monotherapy were good, with no increased safety risks observed from the combination therapy.CLINICAL TRIALSThis study is registered with ClinicalTrials.gov as NCT05108051.

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一项I期、单中心、随机、开放标签、三期交叉研究，旨在评估ZSP1273与奥司他韦在中国健康受试者中的药物相互作用。

ZSP1273是一种靶向RNA聚合酶PB2亚基的新型小分子抗流感药物，而奥司他韦是抑制神经氨酸酶的一线药物。ZSP1273在体外和体内对人流感病毒（包括体外抗奥司他韦毒株）均表现出较高的抗病毒效果。在未来的临床应用中，这两种不同机制的抗病毒药物联合使用可以减少单药治疗可能产生的抗病毒耐药性。为了评价ZSP1273与奥司他韦在健康受试者体内的药代动力学相互作用及合用安全性，我们进行了一项I期、单中心、随机、开放标签、三期交叉研究。36名受试者按1:1:1的比例随机分为三个交叉治疗组，口服给药方法如下：治疗组a: ZSP1273片600 mg，每日1次，连用5天；治疗B：奥司他韦胶囊75 mg，每日2次（BID），连用5天；治疗方案C: ZSP1273片600 mg，每日一次(QD) +奥司他韦胶囊75 mg，每日两次（BID），连用5天。在给药后的规定时间点采集所有受试者血浆样本，测定ZSP1273、奥司他韦及其活性代谢物羧酸奥司他韦的血浆浓度，进行药代动力学分析。与单药治疗相比，共给药后ZSP1273的Cmax、ss、AUC0-t、ss、AUC0-τ、ss和AUC0-∞、ss的几何平均比值（90%置信区间）均在80% ~ 125%的无效边界范围内，支持与ZSP1273不发生药物相互作用。联合给药后，奥司他韦的AUC0-t、ss、AUC0-τ、ss和AUC0-∞、ss均在80% ~ 125%范围内，Cmax、ss下降39.9%。羧酸奥司他韦以上药代动力学参数均在80% ~ 125%之间，Cmax仅为90% CI的下界，略低于80%（77.0%）。考虑到奥司他韦代谢为活性代谢物羧酸奥司他韦的速度较快，且合用对羧酸奥司他韦药动学参数影响较小，认为两药合用未观察到临床显著的药物相互作用。在试验期间，联合治疗和单药治疗的安全性和耐受性都很好，联合治疗未观察到安全风险增加。临床试验：该研究已在ClinicalTrials.gov注册为NCT05108051。

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来源期刊

Antimicrobial Agents and Chemotherapy 医学-微生物学

CiteScore

10.00

自引率

8.20%

发文量

762

审稿时长

3 months

期刊介绍： Antimicrobial Agents and Chemotherapy (AAC) features interdisciplinary studies that build our understanding of the underlying mechanisms and therapeutic applications of antimicrobial and antiparasitic agents and chemotherapy.