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趋化性浸润深部软组织是坏死病变进展的必要条件。

Chemotactic invasion in deep soft tissue by is essential for the progression of necrotic lesions.

机构信息

Laboratory of Veterinary Public Health, School of Veterinary Medicine, Kitasato University , Aomori, Japan.

Division of Infection Control and Prevention, Osaka University Hospital , Osaka, Japan.

出版信息

Virulence. 2020 Dec;11(1):840-848. doi: 10.1080/21505594.2020.1782707.

Abstract

Necrotizing soft tissue infections (NSTI) progress to severe necrosis and result in fatal sepsis within a short time. is a causative agent and can spread from the initial infection site through soft tissue finally to the systemic circulation of the host. The motility and chemotaxis of this bacterium are essential for proliferation and lethality in a murine model of the infection, but their role in pathogenicity has not been characterized. In this study, we revealed the roles of motility and chemotaxis during the process of infection. We compared a nonmotile mutant and two nonchemotactic mutants with their parent strain (WT) with regard to bacterial spread using an in vivo imaging system (IVIS) and invasion by detection of bacteria from the muscle and spleen of a murine infection model. WT rapidly spread throughout the infected thigh and invaded deep muscle causing severe tissue damage. The detection rate in the systemic circulation and the lethality were high. On the other hand, the nonmotile mutant stayed at the inoculation site, and the nonchemotactic mutants spread only slowly through the soft tissue of the infected thigh. Detection in the systemic circulation, the degree of tissue damage, and the lethality of nonchemotactic mutants were significantly reduced in mice compared with WT. This study demonstrated that chemotaxis is essential for invasion from the infection site to the deep and distant tissues and the main pathogenic factor for the rapid progression leading to sepsis in NSTI.

摘要

坏死性软组织感染(NSTI)会迅速进展为严重坏死,并在短时间内导致致命性脓毒症。 是一种病原体,可从初始感染部位通过软组织传播,最终进入宿主的全身循环。该细菌的运动性和趋化性对于在感染的小鼠模型中增殖和致死性至关重要,但它们在致病性中的作用尚未得到表征。在这项研究中,我们揭示了运动性和趋化性在 感染过程中的作用。我们使用体内成像系统(IVIS)比较了非运动突变体和两个非趋化突变体与其亲本菌株(WT)在细菌传播方面的差异,并通过检测来自感染模型的肌肉和脾脏中的细菌来评估细菌侵袭。WT 迅速扩散到受感染的大腿,并侵入深部肌肉,导致严重的组织损伤。在全身循环中的检测率和致死率很高。另一方面,非运动突变体停留在接种部位,非趋化突变体仅缓慢地通过受感染大腿的软组织扩散。与 WT 相比,非趋化突变体在小鼠中的全身循环检测、组织损伤程度和致死率明显降低。这项研究表明,趋化性对于从感染部位侵入深部和远处组织至关重要,是导致 NSTI 中快速进展并引发脓毒症的主要致病因素。

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