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影响HlyB的温度敏感突变的鉴定及初步表征,HlyB是大肠杆菌溶血素(HlyA)分泌所需的转运蛋白。

Identification and preliminary characterization of temperature-sensitive mutations affecting HlyB, the translocator required for the secretion of haemolysin (HlyA) from Escherichia coli.

作者信息

Blight M A, Pimenta A L, Lazzaroni J C, Dando C, Kotelevets L, Séror S J, Holland I B

机构信息

Institut de Génétique et Microbiologie URA (CNRS), Université de Paris, ORSAY, France.

出版信息

Mol Gen Genet. 1994 Nov 15;245(4):431-40. doi: 10.1007/BF00302255.

Abstract

We have carried out a genetic analysis of Escherichia coli HlyB using in vitro(hydroxylamine) mutagenesis and regionally directed mutagenesis. From random mutagenesis, three mutants, temperature sensitive (Ts) for secretion, were isolated and the DNA sequenced: Gly10Arg close to the N-terminus, Gly408Asp in a highly conserved small periplasmic loop region PIV, and Pro624Leu in another highly conserved region, within the ATP-binding region. Despite the Ts character of the Gly10 substitution, a derivative of HlyB, in which the first 25 amino acids were replaced by 21 amino acids of the lambda Cro protein, was still active in secretion of HlyA. This indicates that this region of HlyB is dispensable for function. Interestingly, the Gly408Asp substitution was toxic at high temperature and this is the first reported example of a conditional lethal mutation in HlyB. We have isolated 4 additional mutations in PIV by directed mutagenesis, giving a total of 5 out of 12 residues substituted in this region, with 4 mutations rendering HlyB defective in secretion. The Pro624 mutation, close to the Walker B-site for ATP binding in the cytoplasmic domain is identical to a mutation in HisP that leads to uncoupling of ATP hydrolysis from the transport of histidine. The expression of a fully functional haemolysin translocation system comprising HlyC,A,B and D increases the sensitivity of E. coli to vancomycin 2.5-fold, compared with cells expressing HlyB and HlyD alone. Thus, active translocation of HlyA renders the cells hyperpermeable to the drug. Mutations in hlyB affecting secretion could be assigned to two classes: those that restore the level of vancomycin resistance to that of E. coli not secreting HlyA and those that still confer hypersensitivity to the drug in the presence of HlyA. We propose that mutations that promote vancomycin resistance will include mutations affecting initial recognition of the secretion signal and therefore activation of a functional transport channel. Mutations that do not alter HlyA-dependent vancomycin sensitivity may, in contrast, affect later steps in the transport process.

摘要

我们利用体外(羟胺)诱变和区域定向诱变对大肠杆菌HlyB进行了遗传分析。通过随机诱变,分离出三个分泌温度敏感(Ts)的突变体并对其DNA进行测序:靠近N端的Gly10Arg、高度保守的小周质环区域PIV中的Gly408Asp,以及ATP结合区域内另一个高度保守区域中的Pro624Leu。尽管Gly10替换具有Ts特性,但HlyB的一种衍生物(其中前25个氨基酸被λ Cro蛋白的21个氨基酸取代)在HlyA分泌中仍具有活性。这表明HlyB的该区域对于功能是可有可无的。有趣的是,Gly408Asp替换在高温下具有毒性,这是HlyB中首次报道的条件致死突变实例。我们通过定向诱变在PIV中分离出另外4个突变,该区域12个残基中共有5个被取代,其中4个突变使HlyB分泌缺陷。靠近细胞质结构域中ATP结合的沃克B位点的Pro624突变与HisP中的一个突变相同,该突变导致ATP水解与组氨酸转运解偶联。与仅表达HlyB和HlyD的细胞相比,由HlyC、A、B和D组成的全功能溶血素转运系统的表达使大肠杆菌对万古霉素的敏感性提高了2.5倍。因此,HlyA的活性转运使细胞对该药物具有高通透性。影响分泌的hlyB突变可分为两类:一类可将万古霉素抗性水平恢复到不分泌HlyA的大肠杆菌的水平,另一类在存在HlyA时仍使细胞对该药物过敏。我们提出,促进万古霉素抗性的突变将包括影响分泌信号初始识别从而影响功能性转运通道激活的突变。相比之下,不改变HlyA依赖性万古霉素敏感性的突变可能影响转运过程的后期步骤。

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