Impact of rapid identification by MALDI-TOF MS from positive blood cultures in Enterococcus spp. bloodstream infections.

IF 3.7 3区医学 Q2 INFECTIOUS DISEASES

European Journal of Clinical Microbiology & Infectious Diseases Pub Date : 2025-03-08 DOI:10.1007/s10096-025-05084-x

Diogo Lopes, Bruno Grandbastien, Christina Orasch, Gilbert Greub, Antony Croxatto, Guy Prod'Hom, Benoit Guery

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引用次数: 0

Abstract

Purpose: Regarding bloodstream infections (BSI) Enterococcus spp. rank among the top five most common organisms. Due to enterococci intrinsic resistance, empiric antibiotic therapy is often inappropriate and early identification becomes crucial. Our objective was to assess the clinical impact of MALDI-TOF identification directly from positive blood cultures (BC) in Enterococcus spp. BSI (E-BSI).

Methods: A retrospective cohort study included all adult patients with E-BSI from 2010 to 2017 in a tertiary hospital. ID consultation within 48 h and MALDI-TOF identification directly from BC within 24 h were inclusion criteria. The primary outcome was antimicrobial treatment change following MALDI-TOF and secondary outcomes included 30-day and 1-year mortality, length of stay (LOS) and antimicrobial de-escalation.

Results: Among 267 BSI episodes, E. faecalis was isolated in 130 episodes (48.7%), E. faecium in 122 (45.7%), and 104 (39%) were polymicrobial. Empiric antibiotic therapy was inappropriate in 60.3% of patients. The LOS was 36 (IQR 20-64) days, 30-day and 1-year mortality were 16.1% and 43.4%, respectively. Enterococci identification with MALDI-TOF at the species level was possible in 66.3% cases and in 73% of monomicrobial cases. Antibiotics were changed in 85.3% of the former vs. 63.3% in remaining patients (p < 10^- 4), and de-escalation occurred in 35% of subjects (vs. 12.2%,p = 10^- 4). Changing antibiotics after correct identification was associated with a shorter LOS. In multivariate analysis, appropriate antibiotic therapy before MALDI-TOF was protective against 30-day mortality (aOR 0.40(0.08-1.96)), and appropriate antibiotic therapy afterwards against 1-year mortality (aOR 0.21(0.05-0.84)).

Conclusion: In E-BSI, direct MALDI-TOF identification from positive BC has a significant clinical impact due to a more frequent antibiotic spectrum correction and de-escalation. This may improve patient outcomes, reducing LOS and potentially mortality.

Clinical trial number: Not applicable.

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MALDI-TOF质谱对血培养阳性肠球菌血液感染快速鉴定的影响。

目的：在血液感染（BSI）方面，肠球菌属（Enterococcus sp .）是五大最常见的微生物之一。由于肠球菌的内在耐药性，经验性抗生素治疗往往不合适，早期识别变得至关重要。我们的目的是评估直接从BSI肠球菌（E-BSI）阳性血培养（BC）中鉴定MALDI-TOF的临床影响。方法：一项回顾性队列研究纳入了2010年至2017年在某三级医院的所有成年E-BSI患者。纳入标准为48小时内的ID咨询和24小时内直接从BC确诊的MALDI-TOF。主要终点是MALDI-TOF后抗菌药物治疗的变化，次要终点包括30天和1年死亡率、住院时间（LOS）和抗菌药物降级。结果：267例BSI病例中，分离到粪肠球菌130例（48.7%），分离到粪肠球菌122例（45.7%），分离到多菌104例（39%）。60.3%的患者不适宜经验性抗生素治疗。死亡时间为36天（IQR 20 ~ 64）， 30天死亡率为16.1%，1年死亡率为43.4%。在66.3%的病例和73%的单菌病例中，MALDI-TOF在种水平上鉴定出肠球菌。前者有85.3%的患者更换了抗生素，其余患者为63.3% (p - 4)， 35%的患者出现了抗生素降级（p = 10- 4）。正确识别后更换抗生素与较短的LOS相关。在多因素分析中，在MALDI-TOF前适当的抗生素治疗对30天死亡率有保护作用（aOR 0.40(0.08-1.96)），在MALDI-TOF后适当的抗生素治疗对1年死亡率有保护作用（aOR 0.21(0.05-0.84)）。结论：在E-BSI中，由于更频繁的抗生素谱校正和降级，从阳性BC中直接鉴定MALDI-TOF具有显著的临床影响。这可能会改善患者的预后，降低LOS和潜在的死亡率。临床试验号：不适用。

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

European Journal of Clinical Microbiology & Infectious Diseases 医学-传染病学

CiteScore

10.40

自引率

2.20%

发文量

138

审稿时长

1 months

期刊介绍： EJCMID is an interdisciplinary journal devoted to the publication of communications on infectious diseases of bacterial, viral and parasitic origin.