Imipenem Pharmacokinetics/Pharmacodynamics in Preclinical Hollow Fiber Model, Dose Finding in Virtual Patients, and Clinical Evidence of Efficacy for Mycobacterium abscessus Lung Disease.

IF 4.5 2区医学 Q2 IMMUNOLOGY

Journal of Infectious Diseases Pub Date : 2025-07-11 DOI:10.1093/infdis/jiae601

Sanjay Singh, Tawanda Gumbo, Jann-Yuan Wang, Gunavanthi D Boorgula, Andrew Burke, Hung-Ling Huang, Pamela J McShane, Rodolfo Amaro-Galvez, Jane E Gross, Santosh Aryal, Scott K Heysell, Shashikant Srivastava

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引用次数: 0

Abstract

Background: Guideline-based therapy (GBT) for Mycobacterium abscessus (Mab) lung disease achieves sputum culture conversion (SCC) rates of 35%. This poor GBT efficacy is mirrored in the hollow fiber system model of Mab (HFS-Mab). While imipenem is part of GBT, its biologic effect, with or without β-lactamase inhibitors, is unproven.

Methods: We performed imipenem-relebactam minimum inhibitory concentration (MIC) in 122 Mab isolates, and an exposure-response study in the HFS-Mab using human intrapulmonary pharmacokinetics. The percentage of time that concentration persisted above the MIC (TMIC), mediating maximal effect in the HFS-Mab, was used as the exposure target for dose finding in a Monte Carlo experiment including 10 000 virtual patients. For real-world evidence, we performed a patient, intervention (imipenem), comparison (no β-lactam), and outcome (SCC) (PICO) analysis.

Results: Imipenem killed 1.32 log10 colony-forming units/mL below the day 0 level in HFS-Mab. The average target exposure for imipenem was a TMIC of 47.9% (SD, 9.77%). Infusion of 1 g every 6 hours achieved the target in >90% of virtual patients in Monte Carlo experiments. The pharmacokinetic-pharmacodynamic MIC break point was 1 mg/L. In PICO analyses, the median time to SCC was 470 days in comparators, 311 days for imipenem added on to a failing regimen, and 37 days in newly treated patients (P = .049). The odds ratio for SCC when imipenem was part of the initial regimen, versus comparators, was 12.5 (95% confidence interval, 1.47--84.55). No patients receiving imipenem experienced treatment-limiting adverse events, compared with 2 of 7 comparators (P = .046). Middlebrook 7H9 broth MIC distribution, read at 24 hours, was better correlated with patient responses than cation-adjusted Mueller-Hinton broth.

Conclusions: Imipenem demonstrated biologic effect in the HFS-Mab and in patients. Imipenem-relebactam doses of 1 g every 6 hours are recommended.

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亚胺培南在临床前中空纤维模型中的药代动力学/药效学，虚拟患者的剂量发现，以及对脓肿分枝杆菌肺病疗效的临床证据

背景：脓肿分枝杆菌（Mab）肺病的指导原则疗法（GBT）的痰培养转化率（SCC）仅为 35%。GBT 疗效不佳的情况也反映在脓肿分枝杆菌的中空纤维系统模型（HFS-Mab）中。虽然亚胺培南是 GBT 的一部分，但在使用或不使用 β-内酰胺酶抑制剂的情况下，其生物效果尚未得到证实：方法：我们在 122 个马巴分离物中进行了亚胺培南/雷巴坦最低抑菌浓度（MIC）研究，并利用人体肺内药代动力学在 HFS-Mab 中进行了暴露-反应研究。在基于蒙特卡洛实验（MCE）的剂量测定中，将 HFS-Mab 中介导最大效应的浓度持续高于 MIC 的时间百分比（TMIC）作为 10,000 个虚拟受试者的暴露目标。对于真实世界的证据，我们进行了患者、干预（亚胺培南）、对比（无β-内酰胺）和结果（SCC）（PICO）分析：结果：亚胺培南在HFS-Mab中第0天以下杀死了1.32 log10 CFU/mL。亚胺培南目标暴露率为 TMIC=47.9±9.77%。在 MCEs 中，每 6 小时输注 1g 可使超过 90% 的虚拟患者达到目标。药代动力学/药效学 MIC 断点为 1mg/L。在 PICO 分析中，比较者发生 SCC 的中位天数为 470 天，在失败方案中添加亚胺培南为 311 天，新治疗者为 37 天（P=0.049）。亚胺培南作为初始治疗方案的一部分时，与对比者相比，SCC的几率比为12.5（95%置信区间：1.47至84.55）。使用亚胺培南的患者没有出现限制治疗的不良事件，而使用亚胺培南的患者中有 2/7 出现了限制治疗的不良事件（P=0.0457）。与阳离子调整的穆勒辛顿肉汤相比，24小时读取的米德尔布鲁克7H9肉汤MIC分布与患者反应的相关性更好：结论：亚胺培南在 HFS-Mab 和患者中均显示出生物效应。建议每 6 小时使用 1 克亚胺培南/雷巴坦。

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

Journal of Infectious Diseases 医学-传染病学

CiteScore

13.50

自引率

3.10%

发文量

449

审稿时长

2-4 weeks

期刊介绍： Published continuously since 1904, The Journal of Infectious Diseases (JID) is the premier global journal for original research on infectious diseases. The editors welcome Major Articles and Brief Reports describing research results on microbiology, immunology, epidemiology, and related disciplines, on the pathogenesis, diagnosis, and treatment of infectious diseases; on the microbes that cause them; and on disorders of host immune responses. JID is an official publication of the Infectious Diseases Society of America.