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Ribosome Mediated Quinary Interactions Modulate In-Cell Protein Activities

机译:核糖体介导的奇酸相互作用调节细胞蛋白质活性

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摘要

Ribosomes are present inside bacterial cells at micromolar concentrations and occupy up to 20% of the cell volume. Under these conditions, even weak quinary interactions between ribosomes and cytosolic proteins can affect protein activity. By using in-cell and in vitro NMR spectroscopy, and biophysical techniques, we show that the enzymes, adenylate kinase and dihydrofolate reductase, and the respective coenzymes, ATP and NADPH, bind to ribosomes with micromolar affinity, and that this interaction suppresses the enzymatic activities of both enzymes. Conversely, thymidylate synthase, which works together with dihydrofolate reductase in the thymidylate synthetic pathway, is activated by ribosomes. We also show that ribosomes impede diffusion of green fluorescent protein in vitro and contribute to the decrease in diffusion in vivo. These results strongly suggest that ribosome-mediated quinary interactions contribute to the differences between in vitro and in vivo protein activities and that ribosomes play a previously under-appreciated nontranslational role in regulating cellular biochemistry.
机译:核糖体存在于微摩尔浓度下的细菌细胞内,占据细胞体积的20%。在这些条件下,核糖体和细胞源蛋白之间的弱核相互作用甚至可以影响蛋白质活性。通过使用细胞和体外的NMR光谱和生物物理学技术,我们表明酶,腺苷酸激酶和二氢糖苷还原酶和各辅酶,ATP和NADPH,与微摩尔亲和力结合核糖体,并且该相互作用抑制酶促两种酶的活动。相反,用胸苷合成途径在胸苷合成途径中与二氢醇还原酶一起使用的胸苷合酶合成酶被通过核糖体激活。我们还表明,核糖体阻碍了绿色荧光蛋白在体外扩散,并有助于体内扩散的降低。这些结果强烈表明,核糖体介导的奇酸相互作用有助于体外和体内蛋白质活性之间的差异,并且核糖体在调节细胞生物化学方面发挥以前不受贸易的作用。

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