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氨基酸生物合成的进化保守优化

Evolutionarily conserved optimization of amino acid biosynthesis.

作者信息

Perlstein Ethan O, de Bivort Benjamin L, Kunes Samuel, Schreiber Stuart L

机构信息

Howard Hughes Medical Institute, Broad Institute of Harvard and MIT, 7 Cambridge Center, Cambridge, MA 02142, USA.

出版信息

J Mol Evol. 2007 Aug;65(2):186-96. doi: 10.1007/s00239-007-0013-x. Epub 2007 Aug 7.

DOI:10.1007/s00239-007-0013-x
PMID:17684697
Abstract

The "cognate bias hypothesis" states that early in evolutionary history the biosynthetic enzymes for amino acid x gradually lost residues of x, thereby reducing the threshold for deleterious effects of x scarcity. The resulting reduction in cognate amino acid composition of the enzymes comprising a particular amino acid biosynthetic pathway is predicted to confer a selective growth advantage on cells. Bioinformatic evidence from protein-sequence data of two bacterial species previously demonstrated reduced cognate bias in amino acid biosynthetic pathways. Here we show that cognate bias in amino acid biosynthesis is present in the other domains of life-Archaebacteria and Eukaryota. We also observe evolutionarily conserved underrepresentations (e.g., glycine in methionine biosynthesis) and overrepresentations (e.g., tryptophan in asparagine biosynthesis) of amino acids in noncognate biosynthetic pathways, which can be explained by secondary amino acid metabolism. Additionally, we experimentally validate the cognate bias hypothesis using the yeast Saccharomyces cerevisiae. Specifically, we show that the degree to which growth declines following amino acid deprivation is negatively correlated with the degree to which an amino acid is underrepresented in the enzymes that comprise its cognate biosynthetic pathway. Moreover, we demonstrate that cognate fold representation is more predictive of growth advantage than a host of other potential growth-limiting factors, including an amino acid's metabolic cost or its intracellular concentration and compartmental distribution.

摘要

“同源偏好假说”指出,在进化历史早期,用于合成氨基酸x的生物合成酶逐渐失去x的残基,从而降低了x稀缺时有害影响的阈值。预计构成特定氨基酸生物合成途径的酶的同源氨基酸组成的这种减少会赋予细胞选择性生长优势。先前来自两种细菌物种蛋白质序列数据的生物信息学证据表明,氨基酸生物合成途径中的同源偏好降低。在这里,我们表明氨基酸生物合成中的同源偏好在生命的其他领域——古细菌和真核生物中也存在。我们还观察到非同源生物合成途径中氨基酸在进化上保守的低丰度(例如,甲硫氨酸生物合成中的甘氨酸)和高丰度(例如,天冬酰胺生物合成中的色氨酸),这可以用次级氨基酸代谢来解释。此外,我们使用酿酒酵母通过实验验证了同源偏好假说。具体来说,我们表明氨基酸剥夺后生长下降的程度与该氨基酸在其同源生物合成途径的酶中低丰度的程度呈负相关。此外,我们证明同源折叠丰度比许多其他潜在的生长限制因素更能预测生长优势,这些因素包括氨基酸的代谢成本或其细胞内浓度和区室分布。

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Evolutionarily conserved optimization of amino acid biosynthesis.氨基酸生物合成的进化保守优化
J Mol Evol. 2007 Aug;65(2):186-96. doi: 10.1007/s00239-007-0013-x. Epub 2007 Aug 7.
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Evolution of a genome-encoded bias in amino acid biosynthetic pathways is a potential indicator of amino acid dynamics in the environment.氨基酸生物合成途径中基因组编码偏好性的演变是环境中氨基酸动态变化的一个潜在指标。
Mol Biol Evol. 2014 Nov;31(11):2865-78. doi: 10.1093/molbev/msu225. Epub 2014 Aug 12.
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本文引用的文献

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Persistent biases in the amino acid composition of prokaryotic proteins.原核生物蛋白质氨基酸组成中的持续偏差。
Bioessays. 2006 Jul;28(7):726-38. doi: 10.1002/bies.20431.
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氨基酸代谢与蛋白质多样性相互冲突。
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