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The rate of the molecular clock and the cost of gratuitous protein synthesis

机译:分子钟的速率和免费蛋白质合成的成本

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Background: The nature of the protein molecular clock, the protein-specific rate of amino acid substitutions, is among the central questions of molecular evolution. Protein expression level is the dominant determinant of the clock rate in a number of organisms. It has been suggested that highly expressed proteins evolve slowly in all species mainly to maintain robustness to translation errors that generate toxic misfolded proteins. Here we investigate this hypothesis experimentally by comparing the growth rate of Escherichia coli expressing wild type and misfolding-prone variants of the Lac Z protein. Results: We show that the cost of toxic protein misfolding is small compared to other costs associated with protein synthesis. Complementary computational analyses demonstrate that there is also a relatively weaker, but statistically significant, selection for increasing solubility and polarity in highly expressed E. coli proteins. Conclusions: Although we cannot rule out the possibility that selection against misfolding toxicity significantly affects the protein clock in species other than E. coli, our results suggest that it is unlikely to be the dominant and universal factor determining the clock rate in all organisms. We find that in this bacterium other costs associated with protein synthesis are likely to play an important role. Interestingly, our experiments also suggest significant costs associated with volume effects, such as jamming of the cellular environment with unnecessary proteins.
机译:背景:蛋白质分子钟的性质,即氨基酸置换的蛋白质特异性比率,是分子进化的中心问题。在许多生物中,蛋白质表达水平是时钟频率的主要决定因素。已经提出,高表达的蛋白质在所有物种中缓慢进化,主要是为了维持对产生有毒错误折叠蛋白质的翻译错误的鲁棒性。在这里,我们通过比较表达野生型和Lac Z蛋白易错折叠变体的大肠杆菌的生长速率,通过实验研究了这一假设。结果:我们显示,与蛋白质合成相关的其他成本相比,有毒蛋白质错误折叠的成本很小。补充的计算分析表明,对于在高表达的大肠杆菌蛋白质中增加的溶解度和极性,还有一个相对较弱但具有统计学意义的选择。结论:尽管我们不能排除针对错误折叠毒性的选择会显着影响除大肠杆菌以外的物种的蛋白质钟的可能性,但我们的结果表明,它不可能是决定所有生物钟频率的主要和普遍因素。我们发现在这种细菌中,与蛋白质合成相关的其他成本可能起重要作用。有趣的是,我们的实验还表明了与体积效应相关的巨大成本,例如细胞环境被不必要的蛋白质所干扰。

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