面对肠杆菌中金属-β-内酰胺酶产生的耐药性,解读β-内酰胺的功效:肉汤中的超生理锌是罪魁祸首

Kamilia Abdelraouf, C. Gill, Matthew Gethers, G. Tiseo, Simona Barnini, Marco Falcone, Francesco Menichetti, David P. Nicolau
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摘要

据报道,β-内酰胺类药物对产金属-ß-内酰胺酶(MBL)肠杆菌的体外-体内活性不一致。我们的目的是评估这种不一致性是否归因于体外测试介质中的超生理锌浓度。 我们对新德里产金属ß-内酰胺酶肺炎克雷伯氏菌引起的血流感染患者进行了临床和微生物学观察研究。记录了采用非 MBL 活性 β-内酰胺疗法(碳青霉烯类和头孢他啶/阿维巴坦)和 MBL 活性 β-内酰胺疗法(头孢他啶/阿维巴坦 + 阿曲南等)进行经验性治疗的患者的疗效。用患者的分离物诱发小鼠败血症,并记录美罗培南治疗后的存活率。在标准培养基和生理锌浓度下测定美罗培南的 MIC。 将接受经验性非 MBL 活性 β-内酰胺类药物(中位持续时间为 4 天)治疗的 29 名患者与接受 MBL 活性 β-内酰胺类药物治疗的 29 名患者进行了比较。14天的死亡率分别为21%和14%。在小鼠脓毒血症模型中,美罗培南治疗可防止死亡(与锌未调整肉汤中的 MIC 相比,P 低 16 倍(≥64 mg/L))。 我们的数据为使用生理锌浓度下的 MICs 建立 PK/PD 关系提供了基础支持,这可以更好地预测 β-内酰胺类药物的治疗结果。
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Deciphering the Efficacy of the β-Lactams in the Face of Metallo-β-lactamase Derived Resistance in Enterobacterales: Supraphysiologic Zinc in the Broth is the Culprit
In vitro-in vivo discordance in β-lactams activities against metallo-ß-lactamase (MBL)-producing Enterobacterales has been described. We aimed to assess whether this discordance was attributed to the supra-physiologic zinc concentration in the in vitro testing media. A clinical and microbiological observational study of patients with bloodstream infections due to New Delhi metallo-ß-lactamase-producing Klebsiella pneumoniae was performed. Outcomes of patients treated empirically with non-MBL-active β-lactam therapy (carbapenems and ceftazidime/avibactam) and MBL-active β-lactam therapy (ceftazidime/avibactam +aztreonam) were documented. The patients’ isolates were used to induce septicemia in mice and survival upon meropenem treatment was recorded. Meropenem MICs were determined in standard media and in presence of physiological zinc concentrations. Twenty-nine patients receiving empiric non-MBL-active β-lactams (median duration 4 days) were compared to 29 receiving MBL-active β-lactams. The 14-day-mortality rates were 21% and 14%, respectively. In the murine septicemia model, meropenem treatment resulted in protection from mortality(P < 0.0001). Meropenem MICs in the physiologic zinc concentration broth were 1- to >16-fold lower versus MICs in zinc-unadjusted broth (≥64 mg/L). Our data provide foundational support to establish PK/PD relationships using MICs derived in physiologic zinc concentration which may better predict β-lactam therapy outcome.
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