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通过签名标签诱变鉴定伤口感染建立所需的必需基因。

Identification of Essential Genes of for Establishment of Wound Infection by Signature-Tagged Mutagenesis.

作者信息

Yamazaki Kohei, Kashimoto Takashige, Morita Mio, Kado Takehiro, Matsuda Kaho, Yamasaki Moeko, Ueno Shunji

机构信息

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

出版信息

Front Microbiol. 2019 Feb 1;10:123. doi: 10.3389/fmicb.2019.00123. eCollection 2019.

Abstract

can cause severe necrotic lesions within a short time. Recently, it has been reported that the numbers of wound infection cases in healthy hosts are increasing, for which surgical procedures are essential in many instances to eliminate the pathogen owing to its rapid proliferation. However, the mechanisms by which can achieve wound infection in healthy hosts have not been elucidated. Here, we advance a systematic understanding of wound infection through genome-wide identification of the relevant genes. Signature-tagged mutagenesis (STM) has been developed to identify functions required for the establishment of infection including colonization, rapid proliferation, and pathogenicity. Previously, STM had been regarded to be unsuitable for negative selection to detect the virulence genes of owing to the low colonization and proliferation ability of this pathogen in the intestinal tract and systemic circulation. Alternatively, we successfully identified the virulence genes by applying STM to a murine model of wound infection. We examined a total of 5418 independent transposon insertion mutants by signature-tagged transposon mutagenesis and detected 71 clones as attenuated mutants consequent to disruption of genes by the insertion of a transposon. This is the first report demonstrating that the pathogenicity of during wound infection is highly dependent on its characteristics: flagellar-based motility, siderophore-mediated iron acquisition system, capsular polysaccharide, lipopolysaccharide, and rapid chromosome partitioning. In particular, these functions during the wound infection process and are indispensable for proliferation in healthy hosts. Our results may thus allow the potential development of new strategies and reagents to control the proliferation of and prevent human infections.

摘要

可在短时间内导致严重的坏死性病变。最近有报道称,健康宿主中伤口感染病例的数量在增加,由于病原体快速增殖,在许多情况下手术操作对于消除病原体至关重要。然而,病原体在健康宿主中实现伤口感染的机制尚未阐明。在此,我们通过全基因组鉴定相关基因,对病原体伤口感染有了系统的认识。特征性转座子诱变(STM)已被开发用于鉴定感染建立所需的功能,包括定植、快速增殖和致病性。以前,由于该病原体在肠道和全身循环中的定植和增殖能力较低,STM被认为不适用于阴性选择来检测其毒力基因。另外,我们通过将STM应用于伤口感染的小鼠模型成功鉴定了毒力基因。我们通过特征性转座子诱变共检测了5418个独立的转座子插入突变体,并检测到71个因转座子插入导致基因破坏而减弱的突变体克隆。这是第一份表明病原体在伤口感染期间的致病性高度依赖其特性的报告:基于鞭毛的运动性、铁载体介导的铁获取系统、荚膜多糖、脂多糖和快速染色体分配。特别是,这些功能在伤口感染过程中发挥作用,对于在健康宿主中的增殖不可或缺。因此,我们的结果可能有助于开发控制病原体增殖和预防人类感染的新策略和试剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/34e1/6367243/6ba07ae06c15/fmicb-10-00123-g001.jpg

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