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Are proposed early genetic codes capable of encoding viable proteins?

机译:建议的早期遗传密码是否能够编码有活力的蛋白质?

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摘要

Proteins are elaborate biopolymers balancing between contradicting intrinsic propensities to fold, aggregate or remain disordered. Assessing their primary structural preferences observable without evolutionary optimization has been reinforced by the recent identification of de novo proteins that have emerged from previously non-coding sequences. In this paper we investigate structural preferences of hypothetical proteins translated from random DNA segments using the standard genetic code and three of its proposed evolutionarily predecessor models encoding 10, 6 and 4 amino acids, respectively. Our only main assumption is that the disorder, aggregation and transmembrane helix predictions used are able to reflect the differences in the trends of the protein sets investigated. We found that the 10-residue code encodes proteins that resemble modern proteins in their predicted structural properties. All of the investigated early genetic codes give rise to proteins with enhanced disorder and diminished aggregation propensities. Our results suggest that an ancestral genetic code similar to the proposed 10-residue one is capable of encoding functionally diverse proteins but these might have existed under conditions different from today's common physiological ones. The existence of a protein functional repertoire for the investigated earlier stages which is quite distinct as it is today can be deduced from the presented results.
机译:蛋白质是精心设计的生物聚合物,可以在相互矛盾的固有倾向之间进行折叠,聚集或保持无序状态。最近鉴定了从以前的非编码序列中出现的从头蛋白质,从而加强了评估其无需进化优化即可观察到的主要结构偏好的能力。在本文中,我们研究了使用标准遗传密码及其拟议的进化前体模型(分别编码10、6和4个氨基酸)从随机DNA片段翻译而来的假设蛋白质的结构偏好。我们唯一的主要假设是,所使用的无序,聚集和跨膜螺旋预测能够反映所研究蛋白质组趋势的差异。我们发现10个残基的代码编码的蛋白质在预测的结构特性方面类似于现代蛋白质。所有已研究的早期遗传密码均会导致蛋白质紊乱和聚集倾向降低。我们的结果表明,与拟议的10个残基相似的祖先遗传密码能够编码功能多样的蛋白质,但这些蛋白质可能存在于不同于当今常见生理条件的条件下。可以从提出的结果中推论出所研究的早期阶段的蛋白质功能库的存在,这与今天非常不同。

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