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Directed Evolution of a Model Primordial Enzyme Provides Insights into the Development of the Genetic Code

机译:模型原始酶的定向进化为遗传密码的发展提供了见识

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摘要

The contemporary proteinogenic repertoire contains 20 amino acids with diverse functional groups and side chain geometries. Primordial proteins, in contrast, were presumably constructed from a subset of these building blocks. Subsequent expansion of the proteinogenic alphabet would have enhanced their capabilities, fostering the metabolic prowess and organismal fitness of early living systems. While the addition of amino acids bearing innovative functional groups directly enhances the chemical repertoire of proteomes, the inclusion of chemically redundant monomers is difficult to rationalize. Here, we studied how a simplified chorismate mutase evolves upon expanding its amino acid alphabet from nine to potentially 20 letters. Continuous evolution provided an enhanced enzyme variant that has only two point mutations, both of which extend the alphabet and jointly improve protein stability by >4 kcal/mol and catalytic activity tenfold. The same, seemingly innocuous substitutions (Ile→Thr, Leu→Val) occurred in several independent evolutionary trajectories. The increase in fitness they confer indicates that building blocks with very similar side chain structures are highly beneficial for fine-tuning protein structure and function.
机译:当代的蛋白质库包含20个氨基酸,具有不同的官能团和侧链几何形状。相比之下,原始蛋白质大概是由这些构件的一个子集构建而成的。蛋白原字母的后续扩展将增强其功能,促进早期生命系统的代谢能力和机体适应性。尽管添加带有创新功能基团的氨基酸可以直接增强蛋白质组的化学组成,但是很难合理地包含化学上多余的单体。在这里,我们研究了简化的分支酸盐变位酶如何将其氨基酸字母从9个字母扩展到20个。持续进化提供了一种增强的酶变体,该变体仅具有两个点突变,这两个突变均扩展了字母并共同将蛋白质稳定性提高了> 4 kcal / mol,催化活性提高了十倍。相同的看似无害的取代(Ile→Thr,Leu→Val)发生在几个独立的进化轨迹中。他们赋予的适应性提高表明,具有非常相似的侧链结构的结构单元对于微调蛋白质结构和功能非常有益。

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