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化脓性链球菌M3菌株的基因组序列揭示了侵袭性菌株中的大规模基因组重排以及噬菌体进化的新见解。

Genome sequence of an M3 strain of Streptococcus pyogenes reveals a large-scale genomic rearrangement in invasive strains and new insights into phage evolution.

作者信息

Nakagawa Ichiro, Kurokawa Ken, Yamashita Atsushi, Nakata Masanobu, Tomiyasu Yusuke, Okahashi Nobuo, Kawabata Shigetada, Yamazaki Kiyoshi, Shiba Tadayoshi, Yasunaga Teruo, Hayashi Hideo, Hattori Masahira, Hamada Shigeyuki

机构信息

Department of Oral and Molecular Microbiology, Osaka University Graduate School of Dentistry, Suita-Osaka 565-0871, Japan.

出版信息

Genome Res. 2003 Jun;13(6A):1042-55. doi: 10.1101/gr.1096703.

Abstract

Group Astreptococcus (GAS) is a gram-positive bacterial pathogen that causes various suppurative infections and nonsuppurative sequelae. Since the late 1980s, streptococcal toxic-shock like syndrome (STSS) and severe invasive GAS infections have been reported globally. Here we sequenced the genome of serotype M3 strain SSI-1, isolated from an STSS patient in Japan, and compared it with those of other GAS strains. The SSI-1 genome is composed of 1,884,275 bp, and 1.7 Mb of the sequence is highly conserved relative to strain SF370 (serotype M1) and MGAS8232 (serotype M18), and almost completely conserved relative to strain MGAS315 (serotype M3). However, a large genomic rearrangement has been shown to occur across the replication axis between the homologous rrn-comX1 regions and between two prophage-coding regions across the replication axis. Atotal of 1 Mb of chromosomal DNA is inverted across the replication axis. Interestingly, the recombinations between the prophage regions are within the phage genes, and the genes encoding superantigens and mitogenic factors are interchanged between two prophages. This genomic rearrangement occurs in 65% of clinical isolates (64/94) collected after 1990, whereas it is found in only 25% of clinical isolates (7/28) collected before 1985. These observations indicate that streptococcal phages represent important plasticity regions in the GAS chromosome where recombination between homologous phage genes can occur and result not only in new phage derivatives, but also in large chromosomal rearrangements.

摘要

A群链球菌(GAS)是一种革兰氏阳性细菌病原体,可引起各种化脓性感染和非化脓性后遗症。自20世纪80年代末以来,全球已报告了链球菌中毒性休克样综合征(STSS)和严重侵袭性GAS感染。在此,我们对从一名日本STSS患者分离出的M3血清型菌株SSI-1的基因组进行了测序,并将其与其他GAS菌株的基因组进行了比较。SSI-1基因组由1,884,275 bp组成,相对于菌株SF370(M1血清型)和MGAS8232(M18血清型),该序列的1.7 Mb高度保守,相对于菌株MGAS315(M3血清型)几乎完全保守。然而,已显示在同源rrn-comX1区域之间以及复制轴上的两个原噬菌体编码区域之间,沿着复制轴发生了大规模的基因组重排。总共1 Mb的染色体DNA沿着复制轴发生了倒位。有趣的是,原噬菌体区域之间的重组发生在噬菌体基因内,并且编码超抗原和促有丝分裂因子的基因在两个原噬菌体之间互换。这种基因组重排发生在1990年后收集的65%的临床分离株(64/94)中,而在1985年前收集的临床分离株中仅发现25%(7/28)。这些观察结果表明,链球菌噬菌体代表了GAS染色体中的重要可塑性区域,同源噬菌体基因之间可在此发生重组,不仅导致新的噬菌体衍生物,还会引起大规模的染色体重排。

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