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Unique clustering genes in the bacterial chromosome affecting the type-III secretion of enterohaemorrhagic Escherichia coli

机译:细菌染色体中独特的聚类基因影响肠出血性大肠杆菌的III型分泌

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Bioinformatics analysis was used to search for unknown genes that might influence the phenotypic presentations of enterohaemorrhagic Escherichia coli (EHEC). By so doing and using the known genomic data from EHEC O157? :?H7 and K-12, it has been deduced that genes Z4863 to Z4866 of EHEC do not exist in K-12 strains. These four gene sequences have low degrees of homology (18–40?% amino acid identities) to a set of genes in K-12, which have been known to encode fatty acid biosynthesis enzymes. We referred these four consecutive genes as a fasyn cluster and found that deletion of fasyn from EHEC resulted in a defective type-III secretion (T3S). This deletion apparently did not decrease the amounts of the T3S proteins ectopically expressed from plasmids. Examination of the corresponding mRNAs by real-time PCR revealed that the mRNAs readily decreased in the fasyn-deleted mutant and this suppressive effect on the mRNA levels appeared to spread across all lee operons. Complementation with fasyn reverted the T3S-deficient phenotype. Furthermore, this reversion was also seen when the mutant was supplemented with locus of enterocyte effacement activators (Ler or GrlA). Thus, these unique clustering genes located apart from locus of enterocyte effacement on the bacterial chromosome also play a role in affecting T3S of EHEC.
机译:使用生物信息学分析来搜索可能影响肠出血性大肠杆菌(EHEC)表型表现的未知基因。通过这样做并使用来自EHEC O157的已知基因组数据? :H7和K-12,已经推论出EHEC的基因Z4863至Z4866在K-12菌株中不存在。这四个基因序列与K-12中的一组基因具有较低的同源性(18-40 %%的氨基酸同一性),已知这些基因编码脂肪酸生物合成酶。我们将这四个连续的基因称为fasyn簇,发现从EHEC中删除fasyn会导致有缺陷的III型分泌(T3S)。这种缺失显然不会减少从质粒异位表达的T3S蛋白的数量。通过实时PCR检查相应的mRNA显示,在fasyn缺失的突变体中,mRNA容易下降,并且这种对mRNA水平的抑制作用似乎遍及所有lee操纵子。补充fasyn恢复了T3S缺陷型。此外,当突变体中补充了肠上皮细胞表面活化剂(Ler或GrlA)基因座时,也可以看到这种逆转。因此,这些独特的聚类基因与细菌染色体上肠上皮细胞消失的部位分开,在影响EHEC的T3S中也起作用。

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