Thulin Pontus, Johansson Linda, Low Donald E, Gan Bing S, Kotb Malak, McGeer Allison, Norrby-Teglund Anna
Center for Infectious Medicine, Karolinska Institute, Department of Medicine, Karolinska University Hospital, Stockholm, Sweden.
PLoS Med. 2006 Mar;3(3):e53. doi: 10.1371/journal.pmed.0030053.
Group A streptococcal severe soft tissue infections, such as necrotizing fasciitis, are rapidly progressive infections associated with high mortality. Group A streptococcus is typically considered an extracellular pathogen, but has been shown to reside intracellularly in host cells.
We characterized in vivo interactions between group A streptococci (GAS) and cells involved in innate immune responses, using human biopsies (n = 70) collected from 17 patients with soft tissue infections. Immunostaining and in situ image analysis revealed high amounts of bacteria in the biopsies, even in those collected after prolonged antibiotic therapy. Viability of the streptococci was assessed by use of a bacterial viability stain, which demonstrated viable bacteria in 74% of the biopsies. GAS were present both extracellularly and intracellularly within phagocytic cells, primarily within macrophages. Intracellular GAS were predominantly noted in biopsies from newly involved tissue characterized by lower inflammation and bacterial load, whereas purely extracellular GAS or a combination of intra- and extracellular GAS dominated in severely inflamed tissue. The latter tissue was also associated with a significantly increased amount of the cysteine protease streptococcal pyrogenic exotoxin SpeB. In vitro studies confirmed that macrophages serve as reservoirs for viable GAS, and infection with a speB-deletion mutant produced significantly lower frequencies of cells with viable GAS following infection as compared to the wild-type bacteria.
This is the first study to demonstrate that GAS survive intracellularly in macrophages during acute invasive infections. This intracellular presence may have evolved as a mechanism to avoid antibiotic eradication, which may explain our finding that high bacterial load is present even in tissue collected after prolonged intravenous antibiotic therapy. This new insight into the pathogenesis of streptococcal soft tissue infections highlights a need for alternative therapeutic strategies.
A 组链球菌引起的严重软组织感染,如坏死性筋膜炎,是进展迅速且死亡率高的感染性疾病。A 组链球菌通常被认为是一种胞外病原体,但已证明它可在宿主细胞内生存。
我们利用从 17 例软组织感染患者身上采集的 70 份人体活检样本,对 A 组链球菌(GAS)与参与固有免疫反应的细胞之间的体内相互作用进行了表征。免疫染色和原位图像分析显示活检样本中有大量细菌,即使是在长期抗生素治疗后采集的样本中也是如此。通过使用细菌活力染色剂评估链球菌的活力,结果表明 74%的活检样本中有活细菌。GAS 在吞噬细胞的细胞外和细胞内均有存在,主要存在于巨噬细胞内。细胞内 GAS 主要见于炎症较轻和细菌载量较低的新受累组织的活检样本中,而在严重发炎的组织中,主要是纯细胞外 GAS 或细胞内和细胞外 GAS 的组合。后一种组织中半胱氨酸蛋白酶链球菌致热外毒素 SpeB 的含量也显著增加。体外研究证实巨噬细胞是活 GAS 的储存库,与野生型细菌相比,感染 speB 缺失突变体后,感染后含有活 GAS 的细胞频率显著降低。
这是第一项证明 GAS 在急性侵袭性感染期间能在巨噬细胞内生存的研究。这种细胞内存在可能是作为一种避免被抗生素根除的机制而进化而来的,这可能解释了我们的发现,即即使在长期静脉抗生素治疗后采集的组织中也存在高细菌载量。对链球菌软组织感染发病机制的这一新见解凸显了对替代治疗策略的需求。
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