在国际关注的突发公共卫生事件中基于模型的药物开发：加速辛诺瑞韦的上市许可。

IF 4.5 2区医学 Q2 MICROBIOLOGY

Antimicrobial Agents and Chemotherapy Pub Date : 2025-09-18 DOI:10.1128/aac.00614-25

Bu-Fan Yao, Yang Yang, Shan-Sen Xu, Bo-Hao Tang, Jia Chen, Zi-Jia Guo, Hong-Lin Hu, Wei Zhang, Shu-Meng Fu, Xin-Fang Zhang, Guo-Xiang Hao, Xin-Mei Yang, Lin-Lin Song, Pan-Pan Ye, Lian Liu, Shun-Wei Zhu, Yi Zheng, Wei Zhao

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引用次数: 0

摘要

在国际关注的突发公共卫生事件（PHEIC）期间，快速开发药物至关重要，但传统的临床试验既耗时又高风险。本研究以2019冠状病毒病（COVID-19）为例，强调模型知情药物开发（MIDD）在加快用于治疗COVID-19的3CLpro抑制剂simnotrelvir在中国的上市授权方面的关键作用。采用MIDD方法对三项simnotrelvir临床试验（Ia、Ib、II/III期）进行了优化。使用非线性混合效应模型研究药代动力学，通过蒙特卡罗模拟和贝叶斯估计计算暴露量，并使用线性/逻辑回归模型分析暴露-疗效/安全性关系。MIDD方法始于一项转化研究，利用首次人体试验数据、临床前数据和药效学替代标记物预测患者的起始剂量。根据模拟结果，90.6%的参与者抗omicron变异的谷浓度超过EC90，建议使用750mg / 100mg辛诺瑞韦/利托那韦的剂量水平。然后，一项研究剂量-暴露-反应关系的生物标志物确认研究发现，在Ib期，750 mg抑制病毒载量超过300 mg （-4.995 vs -4.236 log10拷贝/mL， P = 0.0367）。最后，一项确认获益-风险比的随机对照试验发现，与安慰剂相比，simnotrelvir/ritonavir使11种临床综合征的持续缓解时间缩短了1.5天，无严重不良事件。并且在批准剂量下，与病毒载量降低、持续消退时间和≥2级治疗后出现的不良事件发生率之间存在平坦的暴露-反应关系。MIDD提高了临床试验的成功率，优化了收益-风险概况，并加快了新药开发的上市许可，以应对国际关注的突发公共卫生事件。临床试验：本研究在ClinicalTrials.gov注册为NCT05339646、NCT05369676和NCT05506176。

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Model-informed drug development in public health emergency of international concern: accelerating marketing authorization of simnotrelvir.

During a Public Health Emergency of International Concern (PHEIC), rapid drug development is critical, but traditional clinical trials are time-consuming and high-risk. This study used coronavirus disease 2019 (COVID-19) as an example to highlight the pivotal role of model-informed drug development (MIDD) in expediting the marketing authorization of simnotrelvir in China, a 3CL^pro inhibitor for COVID-19 treatment. Three simnotrelvir clinical trials (Phase Ia, Ib, II/III) were optimized using the MIDD approach. Pharmacokinetics was investigated using nonlinear mixed-effects models, exposure was calculated through Monte Carlo simulation and Bayes estimation, and exposure-efficacy/safety relationships were analyzed using linear/logistic regression models. The MIDD approach began with a translational study to predict patients' starting doses using first-in-human data, preclinical data, and pharmacodynamic surrogate marker. A dose level of 750 mg/100 mg simnotrelvir/ritonavir was recommended, using simulation results with 90.6% of participants' trough concentration exceeding EC₉₀ for anti-Omicron variant. Then, a biomarker confirmation study to investigate dose-exposure-response relationship found that 750 mg suppressed viral load more than 300 mg (-4.995 vs. -4.236 log₁₀ copies/mL, P = 0.0367) in Phase Ib. Finally, a randomized controlled trial to confirm benefit-risk ratio found that simnotrelvir/ritonavir reduced time to sustained resolution of 11 clinical syndromes by 1.5 days compared with placebo, had no serious adverse events, and had a flat exposure-response relationship with viral load reduction, time to sustained resolution, and ≥2 grade treatment-emergent adverse event rate with approved dosage. MIDD enhanced clinical trial success, optimized the benefit-risk profile, and expedited marketing authorization for new drug development in response to PHEIC.CLINICAL TRIALSThis study is registered with ClinicalTrials.gov as NCT05339646, NCT05369676, and NCT05506176.

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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.