Genomic investigation of MRSA bacteremia relapse reveals diverse genomic profiles but convergence in bacteremia-associated genes.

medRxiv : the preprint server for health sciences Pub Date : 2025-03-28 DOI:10.1101/2025.03.24.25324140

Brooke M Talbot, Natasia F Jacko, Katrina S Hofstetter, Tara Alahakoon, Kevin Bouiller, Timothy D Read, Michael Z David

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Abstract

Background: Recurrence of methicillin-resistant Staphylococcus aureus (MRSA) bacteremia is a high risk complication for patients. Distinguishing persistent lineages from new infections is not standardized across clinical studies.

Methods: We investigated factors contributing to recurrence of MRSA bacteremia among subjects in Philadelphia, Pennsylvania. Subject demographics and clinical history were collected and paired with whole-genome sequences of infection isolates. Recurrent bacteremia episodes were recorded and defined as relapse infections (same lineage) or new infections by genomic criteria, where a relapse contains isolates <=25 single nucleotide polymorphisms (SNP) different, and by clinical criteria. All isolates were assessed for pairwise SNP distances, common mutations, and signatures of within-host adaptation using the McDonald-Kreitman test. Clusters of transmission between relapse-associated isolates and other subject lineages were identified.

Results: Among 411 sequential subjects with MRSA bacteremia, 32 experienced recurrent bacteremia episodes, with 24 subjects having exclusively relapse infections, six with infections exclusively from a new strain, and two patients with both relapse and new infections. No concordance between a genomic and a clinical definition of relapse was evident (Cohen's Kappa = 0.18, CI: -0.41). Recurrence-associated lineages exhibited signatures of positive selection(G- test:<0.01) . Genes with SNPs occurring in multiple relapse lineages have roles in antibiotic resistance and virulence, including 5 lineages with mutations in mprF and 3 lineages with mutations in rpoB, which corresponded with evolved phenotypic changes in daptomycin and rifampin resistance.

Conclusions: Recurrent infections have a diverse strain background. Relapses can be readily distinguished from newly acquired infections using genomic sequencing but not clinical criteria.

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MRSA菌血症复发的基因组研究揭示了不同的基因组谱，但在菌血症相关基因趋同。

背景：耐甲氧西林金黄色葡萄球菌（MRSA）菌血症复发是患者的高风险并发症。在临床研究中，区分持续性谱系和新发感染并没有标准化。方法：我们在宾夕法尼亚州费城调查导致MRSA菌血症复发的因素。收集受试者人口统计资料和临床病史，并与感染分离株的全基因组序列配对。记录复发性菌血症发作，并将其定义为复发感染（同一谱系）或基因组标准的新感染，其中复发包含分离株。结果：在411例MRSA菌血症患者中，32例出现复发性菌血症发作，24例完全复发感染，6例完全来自新菌株感染，2例复发和新感染。复发的基因组和临床定义之间没有明显的一致性（Cohen’s Kappa = 0.18, CI: -0.41）。复发相关谱系表现出正选择特征（G-检验：mprF）和3个rpoB突变谱系，这与进化的达托霉素和利福平耐药表型变化相对应。结论：反复感染具有多种菌株背景。复发可以很容易地与新获得性感染区分使用基因组测序，但不是临床标准。

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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medRxiv : the preprint server for health sciences

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