Healthcare-associated MRSA (HA-MRSA)

  • 文章类型: Journal Article
    通过全基因组测序基于单核苷酸多态性(SNP)的系统发育分析被认为是探查医院传播的标准方法。然而,WGS的应用受到设备成本高和需要多种分析工具的限制,这限制了它在临床实验室环境中的广泛使用。在日本,基于PCR的开放阅读框分型(POT)用于追踪耐甲氧西林金黄色葡萄球菌(MRSA)传播途径的普遍使用归因于其简单易用.虽然POT的辨别力被认为不足以用于医院传播分析,缺乏支持这一概念的结论性数据。这项研究评估了SNP分析和POT对64种临床MRSA菌株的辨别能力。ST5/SCCmecIIa的所有21株MRSA,有超过16个SNP,展示了不同的克隆。相反,两个菌株共享相同的POT编号,并被鉴定为A组。在具有超过9个SNP的ST8/SCCmecIVl的12个MRSA菌株中,五人进入POTB组,将ST8/SCCmecIVa的4株MRSA菌株归入POTD组,尽管它们包括具有30多个SNP的菌株。在ST1/SCCmecIVa的27株MRSA菌株中,14人被归类为POT组。然而,除了两个簇(每个簇包含两个或三个菌株),所有SNP计数均>10(图1-D)。对CC1/SCCmecIV中MRSA的SNP分析显示,几个菌株在POT数量中具有相同数量的SNP(106-183-37),即使在SNPs>100的细菌中,表明POT在详细的医院传播分析中的使用有限。
    Phylogenetic analysis based on single-nucleotide polymorphism (SNP)-based through whole-genome sequencing is recognized as the standard method for probing nosocomial transmission. However, the application of WGS is constrained by the high cost of equipment and the need for diverse analysis tools, which limits its widespread use in clinical laboratory settings. In Japan, the prevalent use of PCR-based open reading frame typing (POT) for tracing methicillin-resistant Staphylococcus aureus (MRSA) transmission routes is attributed to its simplicity and ease of use. Although POT\'s discriminatory power is considered insufficient for nosocomial transmission analysis, conclusive data supporting this notion is lacking. This study assessed the discriminatory capabilities of SNP analysis and POT across 64 clinical MRSA strains. All 21 MRSA strains of ST5/SCCmec IIa, having more than 16 SNPs, demonstrated distinct clones. Conversely, two strains shared the same POT number and were identified as group A. Among the 12 MRSA strains of ST8/SCCmec IVl with over nine SNPs, five fell into POT group B, and five into POT group C. All four MRSA strains of ST8/SCCmec IVa were classified into POT group D, although they included strains with more than 30 SNPs. Among the 27 MRSA strains of ST1/SCCmec IVa, 14 were classified into POT group E. However, except for two clusters (each comprising two or three strains), all had SNP counts >10 (Fig. 1-D). SNP analysis of MRSA in CC1/SCCmec IV showed that several strains had the same number of SNPs in POT number (106-183-37), even among bacteria with >100 SNPs, indicating POT\'s limited use in detailed nosocomial transmission analysis.
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  • 文章类型: Journal Article
    Panton-Valentine杀白细胞素(PVL)阴性社区相关的耐甲氧西林金黄色葡萄球菌(CA-MRSA)最初在日本传播,此后取代了与医疗保健相关的MRSA(HA-MRSA)。然而,CA-MRSA菌血症(CA-MRSAB)与HA-MRSA菌血症(HA-MRSAB)相比的临床特征尚不清楚.我们旨在阐明PVL阴性CA-MRSA的临床表现和与血浆生物膜形成相关的毒力基因之间的差异并研究其相关性。从2011年到2021年,当CA-MRSA大幅取代HA-MRSA时,从血液培养物中收集79株MRSA菌株,并通过SCCmec分型和靶向毒力基因(lukSF-PV,cna,和fnbB)检测。CA-MRSAB的转移性感染发生率明显高于HA-MRSAB。PVL基因均为阴性,尽管在55.6%(20/36)和50%(18/36)的CA-MRSA菌株以及3.7%(1/27)和7.4%(2/27)的HA-MRSA菌株中cna和fnbB呈阳性,分别。cna和fnbB携带与MRSAB转移感染的发展无关;然而,有cna的CA-MRSAB的菌血症持续时间明显更长.CA-MRSAB可能比HA-MRSAB更容易引起转移性感染。由于CA-MRSA在日本占主导地位,应通过计算机断层扫描识别可疑的转移性感染灶,磁共振成像,和超声心动图在治疗MRSAB时。
    Panton-Valentine leucocidin (PVL)-negative community-associated methicillin-resistant Staphylococcus aureus (CA-MRSA) was originally disseminated in Japan and has since replaced healthcare-associated MRSA (HA-MRSA). However, the clinical characteristics of CA-MRSA bacteremia (CA-MRSAB) compared with those of HA-MRSA bacteremia (HA-MRSAB) are unknown. We aim to clarify differences and investigate associations between the clinical manifestations and virulence genes associated with plasma-biofilm formation in PVL-negative CA-MRSA. From 2011 to 2021, when CA-MRSA dramatically replaced HA-MRSA, 79 MRSA strains were collected from blood cultures and analyzed via SCCmec typing and targeted virulence gene (lukSF-PV, cna, and fnbB) detection. The incidence of metastatic infection was significantly higher in CA-MRSAB than in HA-MRSAB. PVL genes were all negative, although cna and fnbB were positive in 55.6% (20/36) and 50% (18/36) of CA-MRSA strains and 3.7% (1/27) and 7.4% (2/27) of HA-MRSA strains, respectively. cna and fnbB carriage were not associated with the development of metastatic infections in MRSAB; however, the bacteremia duration was significantly longer in CA-MRSAB harboring cna. CA-MRSAB may be more likely to cause metastatic infections than HA-MRSAB. Since CA-MRSA is dominant in Japan, suspected metastatic infection foci should be identified by computed tomography, magnetic resonance imaging, and echocardiography when treating MRSAB.
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