超抗原对于金黄色葡萄球菌感染性心内膜炎、脓毒症和急性肾损伤至关重要。
Superantigens are critical for Staphylococcus aureus Infective endocarditis, sepsis, and acute kidney injury.
机构信息
Department of Microbiology, University of Iowa Carver College of Medicine, Iowa City, Iowa, USA.
出版信息
mBio. 2013 Aug 20;4(4):e00494-13. doi: 10.1128/mBio.00494-13.
UNLABELLED
Infective endocarditis and kidney infections are serious complications of Staphylococcus aureus sepsis. We investigated the role of superantigens (SAgs) in the development of lethal sepsis, infective endocarditis, and kidney infections. SAgs cause toxic shock syndrome, but it is unclear if SAgs contribute to infective endocarditis and kidney infections secondary to sepsis. We show in the methicillin-resistant S. aureus strain MW2 that lethal sepsis, infective endocarditis, and kidney infections in rabbits are critically dependent on high-level SAgs. In contrast, the isogenic strain lacking staphylococcal enterotoxin C (SEC), the major SAg in this strain, is attenuated in virulence, while complementation restores disease production. SAgs' role in infective endocarditis appears to be both superantigenicity and direct endothelial cell stimulation. Maintenance of elevated blood pressure by fluid therapy significantly protects from infective endocarditis, possibly through preventing bacterial accumulation on valves and increased SAg elimination. These data should facilitate better methods to manage these serious illnesses.
IMPORTANCE
The Centers for Disease Control and Prevention reported in 2007 that Staphylococcus aureus is the most significant cause of serious infectious diseases in the United States (R. M. Klevens, M. A. Morrison, J. Nadle, S. Petit, K. Gershman, et al., JAMA 298:1763-1771, 2007). Among these infections are sepsis, infective endocarditis, and acute kidney injury. Infective endocarditis occurs in 30 to 60% of patients with S. aureus bacteremia and carries a mortality rate of 40 to 50%. Over the past decades, infective endocarditis outcomes have not improved, and infection rates are steadily increasing (D. H. Bor, S. Woolhandler, R. Nardin, J. Brusch, D. U. Himmelstein, PLoS One 8:e60033, 2013). There is little understanding of the S. aureus virulence factors that are key for infective endocarditis development and kidney abscess formation. We demonstrate that superantigens are critical in the causation of all three infections. We show that their association results from both superantigenicity and direct toxic effects on endothelial cells, the latter likely contributing to delayed endothelium healing. Our studies contribute significantly to understanding the development of these illnesses and are expected to lead to development of important therapies to treat such illnesses.
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金黄色葡萄球菌脓毒症会引起感染性心内膜炎和肾脏感染等严重并发症。我们研究了超抗原(SAgs)在致死性脓毒症、感染性心内膜炎和肾脏感染发展中的作用。SAgs 可引起中毒性休克综合征,但目前尚不清楚 SAg 是否会导致脓毒症继发的感染性心内膜炎和肾脏感染。我们在耐甲氧西林金黄色葡萄球菌 MW2 株中表明,兔的致死性脓毒症、感染性心内膜炎和肾脏感染严重依赖于高水平的 SAg。相比之下,缺乏葡萄球菌肠毒素 C(SEC)的同基因株(该菌株中的主要 SAg)毒力减弱,而补体则恢复了疾病的产生。SAgs 在感染性心内膜炎中的作用似乎既是超抗原性的,也是直接刺激内皮细胞的作用。通过液体疗法维持血压升高可显著预防感染性心内膜炎,这可能是通过防止细菌在瓣膜上积聚和增加 SAg 清除来实现的。这些数据应有助于更好地管理这些严重疾病。
重要性
疾病控制与预防中心(Centers for Disease Control and Prevention)于 2007 年报告称,金黄色葡萄球菌是美国导致严重传染病的最主要原因(R.M. Klevens、M.A. Morrison、J. Nadle、S. Petit、K. Gershman 等人,JAMA 298:1763-1771,2007)。这些感染包括脓毒症、感染性心内膜炎和急性肾损伤。金黄色葡萄球菌菌血症患者中有 30%至 60%会发生感染性心内膜炎,死亡率为 40%至 50%。在过去几十年中,感染性心内膜炎的治疗效果并未改善,感染率却在稳步上升(D.H. Bor、S. Woolhandler、R. Nardin、J. Brusch、D.U. Himmelstein,PLoS One 8:e60033,2013)。人们对金黄色葡萄球菌的毒力因子知之甚少,这些因子是感染性心内膜炎发展和肾脏脓肿形成的关键。我们证明超抗原在所有三种感染的发病机制中至关重要。我们发现,它们的关联既来自超抗原性,也来自对内皮细胞的直接毒性作用,后者可能导致内皮愈合延迟。我们的研究极大地促进了对这些疾病发展的了解,有望开发出重要的治疗方法来治疗这些疾病。
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