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利用北极细菌的必需基因构建稳定、温度敏感型细菌疫苗。

Essential genes from Arctic bacteria used to construct stable, temperature-sensitive bacterial vaccines.

机构信息

Department of Biochemistry and Microbiology, University of Victoria, Victoria, BC, V8W 3P6, Canada.

出版信息

Proc Natl Acad Sci U S A. 2010 Jul 27;107(30):13456-60. doi: 10.1073/pnas.1004119107. Epub 2010 Jul 12.

Abstract

All bacteria share a set of evolutionarily conserved essential genes that encode products that are required for viability. The great diversity of environments that bacteria inhabit, including environments at extreme temperatures, place adaptive pressure on essential genes. We sought to use this evolutionary diversity of essential genes to engineer bacterial pathogens to be stably temperature-sensitive, and thus useful as live vaccines. We isolated essential genes from bacteria found in the Arctic and substituted them for their counterparts into pathogens of mammals. We found that substitution of nine different essential genes from psychrophilic (cold-loving) bacteria into mammalian pathogenic bacteria resulted in strains that died below their normal-temperature growth limits. Substitution of three different psychrophilic gene orthologs of ligA, which encode NAD-dependent DNA ligase, resulted in bacterial strains that died at 33, 35, and 37 degrees C. One ligA gene was shown to render Francisella tularensis, Salmonella enterica, and Mycobacterium smegmatis temperature-sensitive, demonstrating that this gene functions in both Gram-negative and Gram-positive lineage bacteria. Three temperature-sensitive F. tularensis strains were shown to induce protective immunity after vaccination at a cool body site. About half of the genes that could be tested were unable to mutate to temperature-resistant forms at detectable levels. These results show that psychrophilic essential genes can be used to create a unique class of bacterial temperature-sensitive vaccines for important human pathogens, such as S. enterica and Mycobacterium tuberculosis.

摘要

所有细菌都共享一组进化保守的必需基因,这些基因编码的产物是生存所必需的。细菌栖息的环境多样性很大,包括极端温度环境,这对必需基因施加了适应性压力。我们试图利用必需基因的这种进化多样性来工程化细菌病原体,使其成为稳定的温度敏感型,从而可用作活疫苗。我们从北极发现的细菌中分离出必需基因,并将其替代哺乳动物病原体中的相应基因。我们发现,将 9 种不同的来自嗜冷(喜冷)细菌的必需基因替代哺乳动物致病菌中的相应基因,会导致菌株在低于正常生长温度限制的温度下死亡。替代三个不同的嗜冷基因 orthologs of ligA,其编码 NAD 依赖性 DNA 连接酶,导致细菌菌株在 33、35 和 37°C 下死亡。一个 ligA 基因使弗朗西斯菌、沙门氏菌和分枝杆菌成为温度敏感型,表明该基因在革兰氏阴性和革兰氏阳性菌系细菌中均起作用。三种温度敏感型 F. tularensis 菌株在凉爽的接种部位接种后显示出诱导保护性免疫的能力。大约一半可以测试的基因都不能以可检测水平突变为耐热形式。这些结果表明,嗜冷必需基因可用于为重要的人类病原体(如沙门氏菌和结核分枝杆菌)创建一类独特的细菌温度敏感型疫苗。

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