首页> 外文期刊>Applied and Environmental Microbiology >Analysis of Strains Lacking Known Osmolyte Accumulation Mechanisms Reveals Contributions of Osmolytes and Transporters to Protection against Abiotic Stress
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Analysis of Strains Lacking Known Osmolyte Accumulation Mechanisms Reveals Contributions of Osmolytes and Transporters to Protection against Abiotic Stress

机译:菌株缺乏已知的渗透物积累机制的分析揭示渗透物和转运蛋白对抵抗非生物胁迫的贡献

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Osmolyte accumulation and release can protect cells from abiotic stresses. In Escherichia coli, known mechanisms mediate osmotic stress-induced accumulation of K+ glutamate, trehalose, or zwitterions like glycine betaine. Previous observations suggested that additional osmolyte accumulation mechanisms (OAMs) exist and their impacts may be abiotic stress specific. Derivatives of the uropathogenic strain CFT073 and the laboratory strain MG1655 lacking known OAMs were created. CFT073 grew without osmoprotectants in minimal medium with up to 0.9 M NaCl. CFT073 and its OAM-deficient derivative grew equally well in high- and low-osmolality urine pools. Urine-grown bacteria did not accumulate large amounts of known or novel osmolytes. Thus, CFT073 showed unusual osmotolerance and did not require osmolyte accumulation to grow in urine. Yeast extract and brain heart infusion stimulated growth of the OAM-deficient MG1655 derivative at high salinity. Neither known nor putative osmoprotectants did so. Glutamate and glutamine accumulated after growth with either organic mixture, and no novel osmolytes were detected. MG1655 derivatives retaining individual OAMs were created. Their abilities to mediate osmoprotection were compared at 15°C, 37°C without or with urea, and 42°C. Stress protection was not OAM specific, and variations in osmoprotectant effectiveness were similar under all conditions. Glycine betaine and dimethylsulfoniopropionate (DMSP) were the most effective. Trimethylamine-N-oxide (TMAO) was a weak osmoprotectant and a particularly effective urea protectant. The effectiveness of glycine betaine, TMAO, and proline as osmoprotectants correlated with their preferential exclusion from protein surfaces, not with their propensity to prevent protein denaturation. Thus, their effectiveness as stress protectants correlated with their ability to rehydrate the cytoplasm.
机译:渗透液的积累和释放可以保护细胞免受非生物胁迫。在大肠杆菌中,已知的机制介导渗透胁迫诱导的K +谷氨酸,海藻糖或两性离子如甘氨酸甜菜碱的积累。以前的观察结果表明,存在其他渗透压积累机制(OAM),其影响可能是非生物胁迫特异性的。创建了缺少已知OAM的尿毒症毒株CFT073和实验室毒株MG1655的衍生物。 CFT073在无渗透保护剂的最基本培养基中生长,最高达0.9 M NaCl。 CFT073及其缺乏OAM的衍生物在高渗透压和低渗透压尿液池中均生长良好。尿液中生长的细菌不会积聚大量已知或新的渗透物。因此,CFT073表现出不同寻常的渗透耐受性,不需要渗透液的积累即可在尿液中生长。酵母提取物和脑心输液刺激了高盐度下OAM缺陷型MG1655衍生物的生长。既不已知的也不是推定的渗透保护剂。谷氨酸和谷氨酰胺在与任何一种有机混合物一起生长后会积累,并且没有检测到新的渗透物。创建了保留单个OAM的MG1655衍生物。在15℃,37℃不加或不加尿素以及42℃下比较了它们介导的渗透保护能力。压力保护不是OAM特有的,并且在所有条件下渗透保护效力的变化都相似。甘氨酸甜菜碱和二甲基磺丙酸二甲酯(DMSP)最有效。三甲胺-N-氧化物(TMAO)是一种弱渗透保护剂,是一种特别有效的尿素保护剂。甘氨酸甜菜碱,TMAO和脯氨酸作为渗透保护剂的有效性与它们优先从蛋白质表面排除有关,而不与它们防止蛋白质变性的倾向有关。因此,它们作为应激保护剂的有效性与其使细胞质再水化的能力相关。

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