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针对耐甲氧西林菌血症分离株未充分利用的β-内酰胺类联合用药的鉴定。

identification of underutilized β-lactam combinations against methicillin-resistant bacteremia isolates.

作者信息

Davis Kathleen P, McDermott Laura A, Snydman David R, Aldridge Bree B

机构信息

Department of Molecular Biology and Microbiology, Tufts University School of Medicine, Boston, Massachusetts, USA.

The Stuart B. Levy Center for Integrated Management of Antimicrobial Resistance, Tufts University School of Medicine, Boston, Massachusetts, USA.

出版信息

Microbiol Spectr. 2024 Aug 6;12(8):e0097624. doi: 10.1128/spectrum.00976-24. Epub 2024 Jun 25.

Abstract

Methicillin-resistant (MRSA) bacteremia is a serious clinical challenge with high mortality rates. Antibiotic combination therapy is currently used in cases of persistent infection; however, the limited development of new antibiotics will likely increase the need for combination therapy, and better methods are needed for identifying effective combinations for treating persistent bacteremia. To identify pairwise combinations with the most consistent potential for benefit compared to monotherapy with a primary anti-MRSA agent, we conducted a systematic study with an high-throughput methodology. We tested daptomycin and vancomycin each in combination with gentamicin, rifampicin, cefazolin, and oxacillin, and ceftaroline with daptomycin, gentamicin, and rifampicin. Combining cefazolin with daptomycin lowered the daptomycin concentration required to reach 95% growth inhibition (IC) for all isolates tested and lowered daptomycin IC below the sensitivity breakpoint for five out of six isolates that had daptomycin minimum inhibitory concentrations at or above the sensitivity breakpoint. Similarly, vancomycin ICs were decreased when vancomycin was combined with cefazolin for 86.7% of the isolates tested. This was a higher percentage than was achieved by adding any other secondary antibiotic to vancomycin. Adding rifampicin to daptomycin or vancomycin did not always reduce ICs and failed to produce synergistic interaction in any of the isolates tested; the addition of rifampicin to ceftaroline was frequently synergistic and always lowered the amount of ceftaroline required to reach the IC. These analyses rationalize further evaluation of three drug pairs for MRSA bacteremia: daptomycin+cefazolin, vancomycin+cefazolin, and ceftaroline+rifampicin.IMPORTANCEBloodstream infections caused by methicillin-resistant (MRSA) have a high mortality rate despite the availability of vancomycin, daptomycin, and newer antibiotics including ceftaroline. With the slow output of the antibiotic pipeline and the serious clinical challenge posed by persistent MRSA infections, better strategies for utilizing combination therapy are becoming increasingly necessary. We demonstrated the value of a systematic high-throughput approach, adapted from prior work testing antibiotic combinations against tuberculosis and other mycobacteria, by using this approach to test antibiotic pairs against a panel of MRSA isolates with diverse patterns of antibiotic susceptibility. We identified three antibiotic pairs-daptomycin+cefazolin, vancomycin+cefazolin, and ceftaroline+rifampicin-where the addition of the second antibiotic improved the potency of the first antibiotic across all or most isolates tested. Our results indicate that these pairs warrant further evaluation in the clinical setting.

摘要

耐甲氧西林金黄色葡萄球菌(MRSA)菌血症是一项具有高死亡率的严峻临床挑战。目前,抗生素联合疗法用于持续性感染病例;然而,新抗生素研发受限可能会增加联合疗法的需求,因此需要更好的方法来确定治疗持续性菌血症的有效联合用药方案。为了确定与使用主要抗MRSA药物进行单药治疗相比,具有最一致潜在获益可能性的药物组合,我们采用高通量方法进行了一项系统性研究。我们测试了达托霉素和万古霉素分别与庆大霉素、利福平、头孢唑林和苯唑西林的联合使用情况,以及头孢洛林与达托霉素、庆大霉素和利福平的联合使用情况。头孢唑林与达托霉素联合使用降低了所有测试菌株达到95%生长抑制(IC)所需的达托霉素浓度,并且对于六株达托霉素最低抑菌浓度处于或高于敏感断点的菌株中的五株,将达托霉素IC降至敏感断点以下。同样,对于86.7%的测试菌株,万古霉素与头孢唑林联合使用时万古霉素IC降低。这一比例高于万古霉素与任何其他二线抗生素联合使用时的比例。在达托霉素或万古霉素中添加利福平并非总能降低IC,并且在任何测试菌株中均未产生协同相互作用;在头孢洛林中添加利福平通常具有协同作用,并且总能降低达到IC所需的头孢洛林用量。这些分析为进一步评估用于MRSA菌血症的三对药物组合提供了依据:达托霉素 + 头孢唑林、万古霉素 + 头孢唑林以及头孢洛林 + 利福平。

重要性

尽管有万古霉素、达托霉素以及包括头孢洛林在内的新型抗生素,但耐甲氧西林金黄色葡萄球菌(MRSA)引起的血流感染死亡率仍然很高。鉴于抗生素研发进展缓慢以及持续性MRSA感染带来的严峻临床挑战,更好地利用联合疗法的策略变得越来越必要。我们通过采用一种系统性高通量方法,该方法改编自先前针对结核病和其他分枝杆菌测试抗生素组合的研究,用此方法针对一组具有不同抗生素敏感性模式的MRSA菌株测试抗生素组合,证明了这种方法的价值。我们确定了三对抗生素组合——达托霉素 + 头孢唑林、万古霉素 + 头孢唑林以及头孢洛林 + 利福平——在所有或大多数测试菌株中,添加第二种抗生素可提高第一种抗生素的效力。我们的结果表明,这些组合值得在临床环境中进一步评估。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b61/11302340/e662b7949679/spectrum.00976-24.f001.jpg

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