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高丝氨酸-O-琥珀酰基转移酶(MetA)的稳定化降低了应激条件下大肠杆菌中持留菌的频率。

Stabilization of homoserine-O-succinyltransferase (MetA) decreases the frequency of persisters in Escherichia coli under stressful conditions.

作者信息

Mordukhova Elena A, Pan Jae-Gu

机构信息

Superbacteria Research Center, Korea Research Institute of Bioscience and Biotechnology (KRIBB), Daejeon, Korea.

出版信息

PLoS One. 2014 Oct 17;9(10):e110504. doi: 10.1371/journal.pone.0110504. eCollection 2014.

Abstract

Bacterial persisters are a small subpopulation of cells that exhibit multi-drug tolerance without genetic changes. Generally, persistence is associated with a dormant state in which the microbial cells are metabolically inactive. The bacterial response to unfavorable environmental conditions (heat, oxidative, acidic stress) induces the accumulation of aggregated proteins and enhances formation of persister cells in Escherichia coli cultures. We have found that methionine supplementation reduced the frequency of persisters at mild (37°C) and elevated (42°C) temperatures, as well as in the presence of acetate. Homoserine-o-succinyltransferase (MetA), the first enzyme in the methionine biosynthetic pathway, is prone to aggregation under many stress conditions, resulting in a methionine limitation in E. coli growth. Overexpression of MetA induced the greatest number of persisters at 42°C, which is correlated to an increased level of aggregated MetA. Substitution of the native metA gene on the E. coli K-12 WE chromosome by a mutant gene encoding the stabilized MetA led to reduction in persisters at the elevated temperature and in the presence of acetate, as well as lower aggregation of the mutated MetA. Decreased persister formation at 42°C was confirmed also in E. coli K-12 W3110 and a fast-growing WErph+ mutant harboring the stabilized MetA. Thus, this is the first study to demonstrate manipulation of persister frequency under stressful conditions by stabilization of a single aggregation-prone protein, MetA.

摘要

细菌持留菌是一小部分细胞亚群,它们在无基因变化的情况下表现出多药耐受性。一般来说,持留性与一种休眠状态相关,在这种状态下微生物细胞代谢不活跃。细菌对不利环境条件(热、氧化、酸性应激)的反应会诱导聚集蛋白的积累,并增强大肠杆菌培养物中持留菌细胞的形成。我们发现,补充甲硫氨酸可降低在温和温度(37°C)和升高温度(42°C)下以及在乙酸存在时持留菌的频率。甲硫氨酸生物合成途径中的第一个酶高丝氨酸 - O - 琥珀酰转移酶(MetA)在许多应激条件下易于聚集,导致大肠杆菌生长中甲硫氨酸受限。MetA的过表达在42°C时诱导出最多数量的持留菌,这与聚集的MetA水平升高相关。用编码稳定化MetA的突变基因替代大肠杆菌K - 12 WE染色体上的天然metA基因,导致在升高温度和乙酸存在时持留菌减少,以及突变的MetA聚集减少。在大肠杆菌K - 12 W3110和携带稳定化MetA的快速生长的WErph + 突变体中也证实了在42°C时持留菌形成减少。因此,这是第一项证明通过稳定单一易于聚集的蛋白MetA来操纵应激条件下持留菌频率的研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6ca8/4201533/9672cb306b49/pone.0110504.g001.jpg

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