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一种自转运蛋白的进化:结构域重排及从致病性嗜血杆菌到奈瑟菌的横向转移。

Evolution of an autotransporter: domain shuffling and lateral transfer from pathogenic Haemophilus to Neisseria.

作者信息

Davis J, Smith A L, Hughes W R, Golomb M

机构信息

Division of Biological Sciences and Department of Molecular Microbiology and Immunology, School of Medicine, University of Missouri-Columbia, Columbia, MO 65211, USA.

出版信息

J Bacteriol. 2001 Aug;183(15):4626-35. doi: 10.1128/JB.183.15.000-000.2001.

Abstract

The genomes of pathogenic Haemophilus influenzae strains are larger than that of Rd KW20 (Rd), the nonpathogenic laboratory strain whose genome has been sequenced. To identify potential virulence genes, we examined genes possessed by Int1, an invasive nonencapsulated isolate from a meningitis patient, but absent from Rd. Int1 was found to have a novel gene termed lav, predicted to encode a member of the AIDA-I/VirG/PerT family of virulence-associated autotransporters (ATs). Associated with lav are multiple repeats of the tetranucleotide GCAA, implicated in translational phase variation of surface molecules. Laterally acquired by H. influenzae, lav is restricted in distribution to a few pathogenic strains, including H. influenzae biotype aegyptius and Brazilian purpuric fever isolates. The DNA sequence of lav is surprisingly similar to that of a gene previously described for Neisseria meningitidis. Sequence comparisons suggest that lav was transferred relatively recently from Haemophilus to Neisseria, shortly before the divergence of N. meningitidis and Neisseria gonorrhoeae. Segments of lav predicted to encode passenger and beta-domains differ sharply in G+C base content, supporting the idea that AT genes have evolved by fusing domains which originated in different genomes. Homology and base sequence comparisons suggest that a novel biotype aegyptius AT arose by swapping an unrelated sequence for the passenger domain of lav. The unusually mobile lav locus joins a growing list of genes transferred from H. influenzae to Neisseria. Frequent gene exchange suggests a common pool of hypervariable contingency genes and may help to explain the origin of invasiveness in certain respiratory pathogens.

摘要

致病性流感嗜血杆菌菌株的基因组比Rd KW20(Rd)的基因组大,Rd是一种非致病性实验室菌株,其基因组已被测序。为了鉴定潜在的毒力基因,我们研究了Int1所拥有的基因,Int1是从一名脑膜炎患者身上分离出的侵袭性非包膜菌株,但Rd没有这些基因。发现Int1有一个名为lav的新基因,预计编码毒力相关自转运蛋白(ATs)的AIDA-I/VirG/PerT家族的一个成员。与lav相关的是四核苷酸GCAA的多个重复序列,这与表面分子的翻译相变异有关。lav是流感嗜血杆菌横向获得的,其分布仅限于少数致病菌株,包括埃及生物型流感嗜血杆菌和巴西紫癜热分离株。lav的DNA序列与先前描述的脑膜炎奈瑟菌的一个基因惊人地相似。序列比较表明,lav是在脑膜炎奈瑟菌和淋病奈瑟菌分化前不久,相对较近地从流感嗜血杆菌转移到奈瑟菌的。预计编码乘客域和β域的lav片段在G+C碱基含量上有很大差异,这支持了AT基因是通过融合起源于不同基因组的域而进化的观点。同源性和碱基序列比较表明,一种新的埃及生物型AT是通过用一个不相关的序列替换lav的乘客域而产生的。异常活跃的lav基因座加入了从流感嗜血杆菌转移到奈瑟菌的越来越多的基因名单中。频繁的基因交换表明存在一个高变应急基因的共同库,这可能有助于解释某些呼吸道病原体侵袭性的起源。

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