土拉菌菌株Schu 4基因组测序揭示了shikimate和嘌呤代谢途径,这是构建合理减毒的营养缺陷疫苗的目标。

J Karlsson, R G Prior, K Williams, L Lindler, K A Brown, N Chatwell, K Hjalmarsson, N Loman, K A Mack, M Pallen, M Popek, G Sandström, A Sjöstedt, T Svensson, I Tamas, S G Andersson, B W Wren, P C Oyston, R W Titball
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引用次数: 54

摘要

土拉菌是土拉菌病的病原,土拉菌病是北半球一些国家的一种严重疾病。这种生物有严格的生长要求,在遗传和分子水平上对其了解甚少。由于缺乏关于这种生物的数据,我们对其基因组进行了样本测序。构建了兔拉菌高毒力菌株(Schu 4)的DNA片段随机文库,测定了13904个克隆片段的核苷酸序列,并将其组装成353个contigs。共获得1.83 Mb的核苷酸序列,G+C含量为33.2%。位于质粒pOM1和pNFL10上的基因缺失,这些基因先前已从低毒力的土拉菌菌株中分离出来,但所有其他已知的土拉菌基因在组装的数据中都有体现。F. tularensis Schu4能够在缺乏芳香氨基酸的情况下生长,并且在其他细菌中发现了可以编码莽草酸途径酶的基因同源物。嘌呤生物合成过程中所有酶的编码基因和嘌呤回收途径中大部分酶的编码基因也得到了鉴定。这些数据将用于开发确定的合理的土拉菌减毒突变体,这些突变体可用于替代现有基因未确定的活疫苗菌株。
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Sequencing of the Francisella tularensis strain Schu 4 genome reveals the shikimate and purine metabolic pathways, targets for the construction of a rationally attenuated auxotrophic vaccine.

Francisella tularensis is the etiological agent of tularemia, a serious disease in several Northern hemisphere countries. The organism has fastidious growth requirements and is very poorly understood at the genetic and molecular levels. Given the lack of data on this organism, we undertook the sample sequencing of its genome. A random library of DNA fragments from a highly virulent strain (Schu 4) of F. tularensis was constructed and the nucleotide sequences of 13,904 cloned fragments were determined and assembled into 353 contigs. A total of 1.83 Mb of nucleotide sequence was obtained that had a G+C content of 33.2%. Genes located on plasmids pOM1 and pNFL10, which had been previously isolated from low virulence strains of F. tularensis, were absent but all of the other known F. tularensis genes were represented in the assembled data. F. tularensis Schu4 was able to grow in the absence of aromatic amino acids and orthologues of genes which could encode enzymes in the shikimate pathway in other bacteria were identified in the assembled data. Genes that could encode all of the enzymes in the purine biosynthetic and most of the en- zymes in the purine salvage pathways were also identified. This data will be used to develop defined rationally attenuated mutants of F. tularensis, which could be used as replacements for the existing genetically undefined live vaccine strain.

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