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Community-acquired pneumonia due to pandemic A(H1N1)2009 influenzavirus and methicillin resistant Staphylococcus aureus co-infection

机译:大流行性A(H1N1)2009流感病毒和耐甲氧西林金黄色葡萄球菌共感染引起的社区获得性肺炎

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Background: Bacterial pneumonia is a well described complication of influenza. In recent years, community-onset methicillin-resistant Staphylococcus aureus (cMRSA) infection has emerged as a contributor to morbidity and mortality in patients with influenza. Since the emergence and rapid dissemination of pandemic A(H1N1)2009 influenzavirus in April 2009, initial descriptions of the clinical features of patients hospitalized with pneumonia have contained few details of patients with bacterial co-infection. Methodology/Principal Findings: Patients with community-acquired pneumonia (CAP) caused by co-infection with pandemic A(H1N1)2009 influenzavirus and cMRSA were prospectively identified at two tertiary hospitals in one Australian city during July to September 2009, the period of intense influenza activity in our region. Detailed characterization of the cMRSA isolates was performed. 252 patients with pandemic A(H1N1)2009 influenzavirus infection were admitted at the two sites during the period of study. Three cases of CAP due to pandemic A(H1N1)2009/cMRSA co-infection were identified. The clinical features of these patients were typical of those with S. aureus co-infection or sequential infection following influenza. The 3 patients received appropriate empiric therapy for influenza, but inappropriate empiric therapy for cMRSA infection; all 3 survived. In addition, 2 fatal cases of CAP caused by pandemic A(H1N1)2009/cMRSA co-infection were identified on post-mortem examination. The cMRSA infections were caused by three different cMRSA clones, only one of which contained genes for Panton-Valentine Leukocidin (PVL). Conclusions/Significance: Clinicians managing patients with pandemic A(H1N1)2009 influenzavirus infection should be alert to the possibility of co-infection or sequential infection with virulent, antimicrobial-resistant bacterial pathogens such as cMRSA. PVL toxin is not necessary for the development of cMRSA pneumonia in the setting of pandemic A( H1N1) 2009 influenzavirus co-infection.
机译:背景:细菌性肺炎是流行性感冒的并发症。近年来,社区发作的耐甲氧西林金黄色葡萄球菌(cMRSA)感染已成为导致流感患者发病率和死亡率的原因。自2009年4月大流行性A(H1N1)2009流感病毒出现并迅速传播以来,对肺炎住院患者的临床特征的初步描述几乎没有涉及细菌共感染患者的细节。方法/主要发现:2009年7月至2009年9月,在澳大利亚一个城市的两家三级医院中,前瞻性地发现了由大流行性A(H1N1)2009流感病毒和cMRSA共同感染导致的社区获得性肺炎(CAP)患者我们地区的流感活动。对cMRSA分离株进行了详细的表征。在研究期间,在这两个地点收治了252例大流行性A(H1N1)2009流感病毒感染患者。确认了3例大流行性A(H1N1)2009 / cMRSA共感染引起的CAP病例。这些患者的临床特征是流感后金黄色葡萄球菌共感染或继发感染的典型患者。 3例患者接受了适当的经验性流感治疗,但不适当的经验性治疗cMRSA感染;全部3个幸存下来。此外,在死后检查中发现了2例由大流行性A(H1N1)2009 / cMRSA共同感染引起的CAP致命病例。 cMRSA感染是由三个不同的cMRSA克隆引起的,其中只有一个包含Panton-Valentine Leukocidin(PVL)的基因。结论/意义:处理大流行性A(H1N1)2009流感病毒感染的患者的临床医生应警惕可能与cMRSA等强力,抗药性细菌病原体同时感染或继发感染。在大流行性A(H1N1)2009流感病毒共感染的情况下,PVL毒素对于cMRSA肺炎的发生不是必需的。

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