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鉴定和表征犬链球菌的精氨酸脱亚氨酶系统。

Identification and characterization of the arginine deiminase system of Streptococcus canis.

机构信息

Department of Medical Microbiology, Helmholtz Centre for Infection Research, Braunschweig, Germany.

出版信息

Vet Microbiol. 2013 Feb 22;162(1):270-7. doi: 10.1016/j.vetmic.2012.08.004. Epub 2012 Aug 16.

DOI:10.1016/j.vetmic.2012.08.004
PMID:22939986
Abstract

Although Streptococcus (S.) canis is known to cause severe infections in dogs and cats and harbors a clear zoonotic potential, knowledge about physiology and pathogenesis is mostly elusive. The arginine deiminase system (ADS) has been described in certain streptococcal species and its role in the establishment of infection has been suggested. In this study we focused on the identification and characterization of the ADS in S. canis. Using genome sequencing and subsequent in silico analysis we identified the ADS of S. canis as a gene cluster composed of seven genes. RT-PCR analysis revealed that the ADS of S. canis is transcribed in four transcriptional units, comprising three monocistronical mRNAs and one operon structure. As a secondary metabolic pathway, the ADS of S. canis is strictly regulated by carbon catabolite repression (CCR) and arginine as demonstrated on transcriptional, translational, and enzymatical level, respectively. Furthermore, growth kinetics with a chemically defined medium clearly showed that arginine, the substrate of the ADS, is essential for the biological fitness of S. canis. Using Immuno-electron microscopy analysis, we observed a surface-exposed localization of the ADS enzymes arginine deiminase (ArcA), ornithine carbamoyltransferase (ArcB), and carbamate kinase (ArcC), respectively, which might suggest the contribution of the ADS to the development of streptococcal infections.

摘要

虽然犬链球菌(S. canis)已知会导致犬猫严重感染,并具有明显的人畜共患病潜力,但对其生理学和发病机制的了解大多难以捉摸。精氨酸脱亚氨酶系统(ADS)已在某些链球菌物种中描述,并已表明其在感染建立中的作用。在本研究中,我们专注于鉴定和表征 S. canis 的 ADS。通过基因组测序和随后的计算机分析,我们确定 S. canis 的 ADS 由七个基因组成的基因簇。RT-PCR 分析显示,S. canis 的 ADS 转录为四个转录单元,包括三个单顺反子 mRNA 和一个操纵子结构。作为一种次级代谢途径,ADS 受到严格的碳分解代谢物阻遏(CCR)和精氨酸的调控,这分别在转录、翻译和酶学水平上得到了证实。此外,使用化学定义培养基进行的生长动力学研究清楚地表明,ADS 的底物精氨酸对 S. canis 的生物学适应性至关重要。通过免疫电子显微镜分析,我们观察到 ADS 酶精氨酸脱氨酶(ArcA)、鸟氨酸氨甲酰转移酶(ArcB)和氨基甲酰磷酸激酶(ArcC)分别定位于表面暴露位置,这可能表明 ADS 对链球菌感染的发展有贡献。

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