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Genome Sequence of a Nephritogenic and Highly Transformable M49 Strain of Streptococcus pyogenes▿ †

机译:化脓性链球菌的产肾和高度转化性M49菌株的基因组序列▿†

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摘要

The 1,815,783-bp genome of a serotype M49 strain of Streptococcus pyogenes (group A streptococcus [GAS]), strain NZ131, has been determined. This GAS strain (FCT type 3; emm pattern E), originally isolated from a case of acute post-streptococcal glomerulonephritis, is unusually competent for electrotransformation and has been used extensively as a model organism for both basic genetic and pathogenesis investigations. As with the previously sequenced S. pyogenes genomes, three unique prophages are a major source of genetic diversity. Two clustered regularly interspaced short palindromic repeat (CRISPR) regions were present in the genome, providing genetic information on previous prophage encounters. A unique cluster of genes was found in the pathogenicity island-like emm region that included a novel Nudix hydrolase, and, further, this cluster appears to be specific for serotype M49 and M82 strains. Nudix hydrolases eliminate potentially hazardous materials or prevent the unbalanced accumulation of normal metabolites; in bacteria, these enzymes may play a role in host cell invasion. Since M49 S. pyogenes strains have been known to be associated with skin infections, the Nudix hydrolase and its associated genes may have a role in facilitating survival in an environment that is more variable and unpredictable than the uniform warmth and moisture of the throat. The genome of NZ131 continues to shed light upon the evolutionary history of this human pathogen. Apparent horizontal transfer of genetic material has led to the existence of highly variable virulence-associated regions that are marked by multiple rearrangements and genetic diversification while other regions, even those associated with virulence, vary little between genomes. The genome regions that encode surface gene products that will interact with host targets or aid in immune avoidance are the ones that display the most sequence diversity. Thus, while natural selection favors stability in much of the genome, it favors diversity in these regions.
机译:已经确定了化脓性链球菌M49血清型(A组链球菌[GAS])菌株NZ131的1,815,783-bp基因组。最初从急性链球菌性肾小球肾炎病例中分离出的这种GAS菌株(FCT类型3; emm模式E)具有非凡的电转化能力,已被广泛用作基础遗传和发病机理研究的模型生物。与以前的化脓性链球菌基因组一样,三个独特的原噬菌体是遗传多样性的主要来源。基因组中存在两个成簇的规则间隔的短回文重复序列(CRISPR),可提供有关先前遭遇噬菌体的遗传信息。在致病性岛状emm区域发现了一个独特的基因簇,其中包括一种新型Nudix水解酶,而且,该簇似乎对M49和M82血清型具有特异性。 Nudix水解酶消除了潜在的有害物质或防止了正常代谢产物的不平衡积累;在细菌中,这些酶可能在宿主细胞入侵中起作用。由于已知化脓性链球菌M49菌株与皮肤感染有关,因此Nudix水解酶及其相关基因可能在促进生存的环境中起着重要作用,该环境比喉咙的均匀温暖和湿润更易变且难以预测。 NZ131的基因组继续阐明这种人类病原体的进化史。遗传物质的明显水平转移导致存在高度可变的与毒力相关的区域,这些区域以多重重排和遗传多样性为特征,而其他区域,甚至与毒力相关的区域,在基因组之间变化很小。编码将与宿主靶标相互作用或有助于免疫避免的表面基因产物的基因组区域是显示最多序列多样性的区域。因此,尽管自然选择有利于大部分基因组的稳定性,但自然选择却有利于这些区域的多样性。

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