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Formation of 100S ribosomes in Staphylococcus aureus by the hibernation promoting factor homolog SaHPF

机译:冬眠促进因子同源物SaHPF在金黄色葡萄球菌中形成100S核糖体

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摘要

In the stationary growth phase of Escherichia coli, the 70S ribosomes are dimerized by the ribosome modulation factor (RMF) and hibernation promoting factor (HPF) proteins to form 100S ribosomes, which lose translational activity. In this study we found 100S ribosomes in the gram-positive bacterium Staphylococcus aureus, which has an HPF homolog (named SaHPF) but no RMF homolog. Unlike in E. coli, 100S ribosomes exist in all growth phases of S. aureus, with the highest levels at the transition from the exponential phase to the stationary phase. To find the key factors involved in 100S formation, we analyzed proteins associated with crude ribosomes using radical-free and highly reducing 2-D PAGE and MALDI TOF/MS. Only the SaHPF levels changed in parallel with the changes in 100S levels. SaHPF bound preferentially to 70S components in 100S ribosomes, with a molar ratio of 1 : 1 relative to the 70S, but some SaHPF was also detected in free 70S ribosomes. High-salt washing of the crude ribosomes released SaHPF and dissociated the 100S ribosomes to their 70S components. When these 70S components were incubated with purified SaHPF in vitro, they re-associated to form 100S. These results suggest that SaHPF is a key protein involved in 100S ribosome formation in S. aureus.
机译:在大肠杆菌的稳定生长阶段,70S核糖体被核糖体调节因子(RMF)和冬眠促进因子(HPF)蛋白二聚形成100S核糖体,失去了翻译活性。在这项研究中,我们在革兰氏阳性金黄色葡萄球菌中发现了100S核糖体,它具有HPF同源物(名为SaHPF),但没有RMF同源物。与大肠杆菌不同,金黄色葡萄球菌的所有生长阶段都存在100S核糖体,在从指数期到固定期的过渡期具有最高水平。为了找到参与100S形成的关键因素,我们使用无自由基且高度还原的2-D PAGE和MALDI TOF / MS分析了与粗核糖体相关的蛋白质。只有SaHPF级别与100S级别的变化并行变化。 SaHPF优先结合100S核糖体中的70S成分,相对于70S的摩尔比为1:1,但在游离的70S核糖体中也检测到一些SaHPF。粗核糖体的高盐洗涤会释放SaHPF,并使100S核糖体解离为其70S组分。当将这些70S成分与纯化的SaHPF体外孵育时,它们会重新缔合以形成100S。这些结果表明,SaHPF是金黄色葡萄球菌参与100S核糖体形成的关键蛋白。

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