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Genome Diversification in Staphylococcus aureus: Molecular Evolution of a Highly Variable Chromosomal Region Encoding the Staphylococcal Exotoxin-Like Family of Proteins

机译:金黄色葡萄球菌的基因组多样化:编码蛋白质的葡萄球菌外毒素样家族的高度可变的染色体区域的分子进化。

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摘要

Recent genomic studies have revealed extensive variation in natural populations of many pathogenic bacteria. However, the evolutionary processes which contribute to much of this variation remain unclear. A previous whole-genome DNA microarray study identified variation at a large chromosomal region (RD13) of Staphylococcus aureus which encodes a family of proteins with homology to staphylococcal and streptococcal superantigens, designated staphylococcal exotoxin-like (SET) proteins. In the present study, RD13 was found in all 63 S. aureus isolates of divergent clonal, geographic, and disease origins but contained a high level of variation in gene content in different strains. A central variable region which contained from 6 to 10 different set genes, depending on the strain, was identified, and DNA sequence analysis suggests that horizontal gene transfer and recombination have contributed to the diversification of RD13. Phylogenetic analysis based on the RD13 DNA sequence of 18 strains suggested that loss of various set genes has occurred independently several times, in separate lineages of pathogenic S. aureus, providing a model to explain the molecular variation of RD13 in extant strains. In spite of multiple episodes of set deletion, analysis of the ratio of silent substitutions in set genes to amino acid replacements in their products suggests that purifying selection (selective constraint) is acting to maintain SET function. Further, concurrent transcription in vitro of six of the seven set genes in strain COL was detected, indicating that the expression of set genes has been maintained in contemporary strains, and Western immunoblot analysis indicated that multiple SET proteins are expressed during the course of human infections. Overall, we have shown that the chromosomal region RD13 has diversified extensively through episodes of gene deletion and recombination. The coexpression of many set genes and the production of multiple SET proteins during human infection suggests an important role in host-pathogen interactions.
机译:最近的基因组研究表明许多致病细菌的自然种群存在广泛的差异。但是,尚不清楚导致这种变化的大部分原因的进化过程。先前的全基因组DNA微阵列研究确定了金黄色葡萄球菌的较大染色体区域(RD13)的变异,该变异编码一种与葡萄球菌和链球菌超抗原同源的蛋白家族,称为葡萄球菌外毒素样(SET)蛋白。在本研究中,RD13在所有63个具有不同克隆,地理和疾病起源的金黄色葡萄球菌分离物中均发现,但在不同菌株中基因含量差异很大。鉴定了一个中央可变区,该可变区包含6至10个不同的设定基因,具体取决于菌株,DNA序列分析表明水平基因转移和重组有助于RD13的多样化。基于18个菌株的RD13 DNA序列的系统发育分析表明,在致病性金黄色葡萄球菌的不同谱系中,各种设定基因的丢失已经独立发生了几次,从而为解释现存菌株中RD13的分子变异提供了模型。尽管集合缺失多次发作,但分析集合基因中的沉默取代与产物中氨基酸置换的比率表明,纯化选择(选择性约束)可起到维持SET功能的作用。此外,在菌株COL中检测到七个设定基因中的六个的同时体外转录,这表明设定基因的表达已在当代菌株中得以维持,并且Western免疫印迹分析表明在人类感染过程中表达了多个SET蛋白。 。总的来说,我们已经表明,通过基因缺失和重组的发生,RD13染色体区域已经广泛多样化。在人类感染期间许多集合基因的共表达和多种SET蛋白的产生表明在宿主-病原体相互作用中起着重要作用。

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