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四型淋病奈瑟菌(Tpc),一种影响上皮细胞侵袭、自然转化能力和细胞分离的新型淋病奈瑟菌基因型。

Tetrapac (tpc), a novel genotype of Neisseria gonorrhoeae affecting epithelial cell invasion, natural transformation competence and cell separation.

作者信息

Fussenegger M, Kahrs A F, Facius D, Meyer T F

机构信息

Max-Planck-Institut für Biologie, Abteilung Infektionsbiologie, Tübingen, Germany.

出版信息

Mol Microbiol. 1996 Mar;19(6):1357-72. doi: 10.1111/j.1365-2958.1996.tb02479.x.

Abstract

We characterized a novel mutant phenotype (tetrapac, tpc) of Neisseria gonorrhoeae (Ngo) associated with a distinctive rough-colony morphology and bacterial growth in clusters of four. This phenotype, suggesting a defect in cell division, was isolated from a mutant library of Ngo MS11 generated with the phoA minitransposon TnMax4. The tpc mutant shows a 30% reduction in the overall murein hydrolase activity using Escherichia coli murein as substrate. Tetrapacs can be resolved by co-cultivation with wild-type Ngo, indicating that Tpc is a diffusible protein. Interestingly, Tpc is absolutely required for the natural transformation competence of piliated Ngo. Mutants in tpc grow normally, but show a approximately 10-fold reduction in their ability to invade human epithelial cells. The tpc sequence reveals an open reading frame of approximately 1 kb encoding a protein (Tpc) of 37 kDa. The primary gene product exhibits an N-terminal leader sequence typical of lipoproteins, but palmitoylation of Tpc could not be demonstrated. The ribosomal binding site of tpc is immediately downstream of the translational stop codon of the folC gene coding for an enzyme involved in folic acid biosynthesis and one-carbon metabolism. The tpc gene is probably co-transcribed from the folC promoter and a promoter located within the folC gene. The latter promoter sequence shares significant homology with E. coli gearbox consensus promoters. All three mutant phenotypes, i.e. the cell separation defect, the transformation deficiency and the defect in cell invasion can be restored by complementation of the mutant with an intact tpc gene. To some extent the tcp phenotype is reminiscent of iap in Listeria, lytA in Streptococcus pneumoniae and lyt in Bacillus subtilis, all of which are considered to represent murein hydrolase defects.

摘要

我们鉴定了淋病奈瑟菌(Ngo)的一种新型突变表型(tetrapac,tpc),该表型与独特的粗糙菌落形态以及四个一组的细菌生长簇相关。这种表型表明细胞分裂存在缺陷,是从用phoA微型转座子TnMax4构建的Ngo MS11突变文库中分离得到的。tpc突变体以大肠杆菌胞壁质为底物时,其总体胞壁质水解酶活性降低了30%。通过与野生型Ngo共培养可解决tetrapacs问题,这表明Tpc是一种可扩散的蛋白质。有趣的是,Tpc对于有菌毛的Ngo的自然转化能力是绝对必需的。tpc突变体生长正常,但其侵袭人上皮细胞的能力降低了约10倍。tpc序列揭示了一个约1 kb的开放阅读框,编码一个37 kDa的蛋白质(Tpc)。主要基因产物具有脂蛋白典型的N端前导序列,但未证实Tpc存在棕榈酰化。tpc的核糖体结合位点紧接在编码参与叶酸生物合成和一碳代谢的一种酶的folC基因的翻译终止密码子下游。tpc基因可能从folC启动子以及位于folC基因内的一个启动子共同转录。后一个启动子序列与大肠杆菌齿轮箱共有启动子具有显著同源性。所有三种突变表型,即细胞分离缺陷、转化缺陷和细胞侵袭缺陷,都可以通过用完整的tpc基因对突变体进行互补来恢复。在某种程度上,tcp表型让人联想到李斯特菌中的iap、肺炎链球菌中的lytA和枯草芽孢杆菌中的lyt,所有这些都被认为代表胞壁质水解酶缺陷。

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