首页> 美国卫生研究院文献>FEMS Microbiology Letters >Pleiotropic consequences of gene knockouts in the phthiocerol dimycocerosate and phenolic glycolipid biosynthetic gene cluster of the opportunistic human pathogen Mycobacterium marinum
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Pleiotropic consequences of gene knockouts in the phthiocerol dimycocerosate and phenolic glycolipid biosynthetic gene cluster of the opportunistic human pathogen Mycobacterium marinum

机译:机会性人类病原体海洋分枝杆菌的苯二酚二羟癸酸酯和酚糖​​脂生物合成基因簇中基因敲除的多效性后果

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摘要

Phthiocerol dimycocerosates (PDIMs) and phenolic glycolipids (PGLs) contribute to the pathogenicity of several mycobacteria. Biosynthesis of these virulence factors requires polyketide synthases and other enzymes that represent potential targets for the development of adjuvant antivirulence drugs. We used six isogenic Mycobacterium marinum mutants, each with a different gene knockout in the PDIM/PGL biosynthetic pathway, to probe the pleiotropy of mutations leading to PDIM PGL, PDIM+ PGL or PDIM PGL+ phenotypes. We evaluated the M. marinum mutants for changes in antibiotic susceptibility, cell envelope permeability, biofilm formation, surface properties, sliding motility and virulence in an amoeba model. The analysis also permitted us to begin exploring the hypothesis that different gene knockouts rendering the same PDIM and/or PGL deficiency phenotypes lead to M. marinum mutants with equivalent pleiotropic profiles. Overall, the results of our study revealed a complex picture of pleiotropic patterns emerging from different gene knockouts, uncovered unexpected phenotypic inequalities between mutants, and provided new insight into the phenotypic consequences of gene knockouts in the PDIM/PGL biosynthetic pathway.
机译:苯二酚二椰油酸酯(PDIM)和酚糖脂(PGL)导致了几种分枝杆菌的致病性。这些毒力因子的生物合成需要聚酮化合物合酶和其他酶,这些酶代表开发辅助抗毒力药物的潜在目标。我们使用六个等基因的海洋分枝杆菌突变体,每个突变体在PDIM / PGL生物合成途径中具有不同的基因敲除,以探测导致PDIM - PGL -,PDIM的突变的多向性 + PGL -或PDIM - PGL + 表型。我们在变形虫模型中评估了M. marinum突变体在抗生素敏感性,细胞包膜通透性,生物膜形成,表面性质,滑动运动性和毒性方面的变化。该分析还允许我们开始探索这样的假说:呈现相同PDIM和/或PGL缺陷表型的不同基因敲除导致具有相同多效性特征的海藻分枝杆菌突变体。总的来说,我们的研究结果揭示了由不同基因敲除产生的多效性模式的复杂情况,揭示了突变体之间意料之外的表型不平等,并为PDIM / PGL生物合成途径中基因敲除的表型后果提供了新见解。

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