中性粒细胞减少性白血病患者产生AmpC DHA-1菌血症的大肠杆菌：持续输注头孢他啶/阿维巴坦作为碳青霉烯保留方案

IF 3.3 Q2 INFECTIOUS DISEASES

JAC-Antimicrobial Resistance Pub Date : 2025-06-18 eCollection Date: 2025-06-01 DOI:10.1093/jacamr/dlaf109

S Giuliano, A Piccirilli, J Angelini, F Patriarca, R Fanin, L Martini, T Semenzin, M Fanin, S Lanini, R A Bonomo, M Perilli, C Tascini

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引用次数: 0

摘要

背景：大肠杆菌对第三代头孢菌素产生耐药性，主要是由于产生ESBLs和AmpC β-内酰胺酶，这对治疗提出了重大挑战，特别是在免疫功能低下的患者中。Ceftazidime/avibactam （CZA）已成为一种潜在的碳青霉烯保护选择，尽管其对产生ampc的肠杆菌的有效性数据仍然有限。方法：我们报告了一例由大肠杆菌菌株携带质粒介导的AmpC酶DHA-1引起的血液感染（BSI），患者在异基因造血干细胞移植后出现中性粒细胞减少症。通过全基因组测序和偶联分析对该菌株进行了鉴定。在增强肾清除率（ARC）的情况下，使用治疗药物监测（TDM）来指导持续输注CZA方案。结果：患者对CZA治疗反应良好（每8 h 2.5 g，连续输注9天），微生物清除迅速，临床改善。TDM证实头孢他啶（29.57 mg/L）和阿维巴坦（5.52 mg/L）的治疗血浆浓度。基因组分析显示该菌株存在多种抗性基因（blaDHA-1、qnrB4、mphA、dfrA7）和毒力因子，鉴定为大肠杆菌ST442，血清型O174:H9。早期从美罗培南到CZA的转换可能有助于微生物群的保存，并防止随后由产碳青霉烯酶的肺炎克雷伯菌感染。结论：该病例说明了由TDM指导的碳青霉烯保留策略在高危ARC患者中产生ampc的大肠杆菌BSI的临床应用。持续输注CZA达到了与治疗成功相关的药代动力学/药效学目标，提供了一种有希望的碳青霉烯类替代方案，同时降低了耐药发展和微生物群破坏的风险。

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Escherichia coli producing AmpC DHA-1 bacteraemia in neutropenic leukemic patient: continuous infusion ceftazidime/avibactam as a carbapenem sparing regimen.

Background: Escherichia coli resistant to third-generation cephalosporins, primarily due to the production of ESBLs and AmpC β-lactamases, poses a significant therapeutic challenge, particularly in immunocompromised patients. Ceftazidime/avibactam (CZA) has emerged as a potential carbapenem-sparing option, though data on its efficacy against AmpC-producing Enterobacterales remain limited.

Methods: We report a case of bloodstream infection (BSI) caused by an E. coli strain harbouring the plasmid-mediated AmpC enzyme DHA-1 in a neutropenic patient following allogeneic haematopoietic stem cell transplantation. The strain was characterized via whole-genome sequencing and conjugation assays. Therapeutic drug monitoring (TDM) was used to guide a continuous infusion CZA regimen in the context of augmented renal clearance (ARC).

Results: The patient responded favourably to CZA therapy (2.5 g every 8 h via continuous infusion for 9 days), with rapid microbiological clearance and clinical improvement. TDM confirmed therapeutic plasma concentrations of both ceftazidime (29.57 mg/L) and avibactam (5.52 mg/L). Genomic analysis revealed multiple resistance genes (blaDHA-1, qnrB4, mphA, dfrA7) and virulence factors, with the isolate identified as E. coli ST442, serotype O174:H9. The early switch from meropenem to CZA may have contributed to microbiota preservation and prevented subsequent infection by carbapenemase-producing Klebsiella pneumoniae, for which the patient was colonized.

Conclusions: This case illustrates the clinical utility of a carbapenem-sparing strategy guided by TDM in a high-risk, ARC patient with an AmpC-producing E. coli BSI. Continuous infusion CZA achieved pharmacokinetic/pharmacodynamic targets associated with therapeutic success, offering a promising alternative to carbapenems while mitigating the risk of resistance development and microbiota disruption.

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来源期刊

JAC-Antimicrobial Resistance Multiple-

CiteScore

5.30

自引率

0.00%

发文量

审稿时长

16 weeks