Advancements in the fight against globally distributed OXA-48 carbapenemase: evaluating the new generation of carbapenemase inhibitors.

IF 4.1 2区医学 Q2 MICROBIOLOGY

Antimicrobial Agents and Chemotherapy Pub Date : 2025-01-10 DOI:10.1128/aac.01614-24

Michelle Outeda-García, Jorge Arca-Suárez, Emilio Lence, Arianna Rodriguez-Coello, Romina Maceiras, Tania Blanco-Martin, Paula Guijarro-Sánchez, Lucia Gonzalez-Pinto, Isaac Alonso-Garcia, Andrea García-Pose, Andrea Muras, Salud Rodriguez-Pallares, Cristina Lasarte-Monterrubio, Concepción Gonzalez-Bello, Juan Carlos Vázquez-Ucha, German Bou, Alejandro Beceiro

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引用次数: 0

Abstract

Carbapenemase OXA-48 and its variants pose a serious threat to the development of effective treatments for bacterial infections. OXA-48-producing Enterobacterales are the most prevalent carbapenemase-producing bacteria in large parts of the world. Although these bacteria exhibit low-level carbapenem resistance in vitro, the infections they cause are challenging to treat with conventional therapies, owing to their spread and complex detection in clinical settings. However, numerous β-lactamase inhibitors (BLIs) are currently in the pipeline or late clinical stages. To assess the potential of these compounds, this study compared the efficacy against OXA-48 of novel β-lactamase inhibitors, specifically the 1,6-diazabicyclo[3,2,1]octanes (DBOs) avibactam, relebactam, zidebactam, nacubactam, and durlobactam, along with the cyclic and bicyclic boronates vaborbactam, taniborbactam, and xeruborbactam. The extensive kinetics assays identified xeruborbactam, taniborbactam, and durlobactam, together with the already established avibactam, as BLIs with superior biochemical performance. Susceptibility testing further validated these findings but also demonstrated significantly improved bacterial killing by the DBOs zidebactam, nacubactam, and durlobactam. On the other hand, binding studies demonstrated the superior inhibitory capacity of the BLIs durlobactam and xeruborbactam. Combinations, such as cefepime/zidebactam, meropenem/nacubactam, and sulbactam/durlobactam, show promising activity against OXA-48-producing Enterobacterales, while ceftazidime/avibactam, cefepime/taniborbactam, and meropenem/xeruborbactam combinations also appear highly active, largely due to the excellent kinetics of these new inhibitors. Overall, this comprehensive analysis provides important insights into the effectiveness of new BLIs against OXA-48-producing Enterobacterales, highlighting xeruborbactam, durlobactam, and avibactam as leading candidates. Additionally, BLIs like zidebactam, nacubactam, and taniborbactam also showed potential in addressing the clinical challenges posed by OXA-48-mediated antimicrobial resistance.

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对抗全球分布的OXA-48碳青霉烯酶的进展：评估新一代碳青霉烯酶抑制剂。

碳青霉烯酶OXA-48及其变异对细菌感染有效治疗的发展构成严重威胁。在世界大部分地区，产生oxa -48的肠杆菌是最普遍的产生碳青霉烯酶的细菌。尽管这些细菌在体外表现出低水平的碳青霉烯耐药性，但由于它们的传播和在临床环境中的复杂检测，它们引起的感染难以用常规疗法治疗。然而，许多β-内酰胺酶抑制剂（BLIs）目前正处于研发阶段或后期临床阶段。为了评估这些化合物的潜力，本研究比较了新型β-内酰胺酶抑制剂对OXA-48的疗效，特别是1,6-重氮杂环[3,2,1]辛烷（DBOs）阿维巴坦、乐巴坦、齐德巴坦、纳库巴坦和杜罗巴坦，以及环和双环硼酸盐瓦波巴坦、坦波巴坦和异鲁巴坦。广泛的动力学分析确定了xuborbactam， taniborbactam和durlobactam，以及已经建立的avibactam，作为具有优越生化性能的bli。药敏试验进一步证实了这些发现，但也证明了DBOs zidebactam， nacubactam和durlobactam显著改善了细菌杀灭。另一方面，结合研究表明BLIs durlobactam和xeruborbactam具有较好的抑制能力。诸如头孢吡肟/齐德巴坦、美罗培南/纳库巴坦和舒巴坦/杜罗巴坦的组合对产生oxa -48的肠杆菌显示出有希望的活性，而头孢他啶/阿维巴坦、头孢吡肟/塔尼波巴坦和美罗培南/希鲁巴坦的组合也表现出高活性，这主要是由于这些新抑制剂的良好动力学。总的来说，这项全面的分析为新的bli对产生oxa -48的肠杆菌的有效性提供了重要的见解，强调了xeruborbactam， durlobactam和avibactam是主要的候选药物。此外，zidebactam， nacubactam和taniborbactam等bli也显示出解决oxa -48介导的抗菌素耐药性所带来的临床挑战的潜力。

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

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.