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从前生物催化剂到生物催化剂的肽。

Peptides En Route from Prebiotic to Biotic Catalysis.

机构信息

Department of Cell Biology, Faculty of Science, Charles University, Prague 12800, Czech Republic.

Institute of Organic Chemistry and Biochemistry, Czech Academy of Sciences, Prague 16610, Czech Republic.

出版信息

Acc Chem Res. 2024 Aug 6;57(15):2027-2037. doi: 10.1021/acs.accounts.4c00137. Epub 2024 Jul 17.

Abstract

ConspectusIn the quest to understand prebiotic catalysis, different molecular entities, mainly minerals, metal ions, organic cofactors, and ribozymes, have been implied as key players. Of these, inorganic and organic cofactors have gained attention for their ability to catalyze a wide array of reactions central to modern metabolism and frequently participate in these reactions within modern enzymes. Nevertheless, bridging the gap between prebiotic and modern metabolism remains a fundamental question in the origins of life.In this Account, peptides are investigated as a potential bridge linking prebiotic catalysis by minerals/cofactors to enzymes that dominate modern life's chemical reactions. Before ribosomal synthesis emerged, peptides of random sequences were plausible on early Earth. This was made possible by different sources of amino acid delivery and synthesis, as well as their condensation under a variety of conditions. Early peptides and proteins probably exhibited distinct compositions, enriched in small aliphatic and acidic residues. An increase in abundance of amino acids with larger side chains and canonical basic groups was most likely dependent on the emergence of their more challenging (bio)synthesis. Pressing questions thus arise: how did this composition influence the early peptide properties, and to what extent could they contribute to early metabolism?Recent research from our group and colleagues shows that highly acidic peptides/proteins comprising only the presumably "early" amino acids are in fact competent at secondary structure formation and even possess adaptive folding characteristics such as spontaneous refoldability and chaperone independence to achieve soluble structures. Moreover, we showed that highly acidic proteins of presumably "early" composition can still bind RNA by utilizing metal ions as cofactors to bridge carboxylate and phosphoester functional groups. And finally, ancient organic cofactors were shown to be capable of binding to sequences from amino acids considered prebiotically plausible, supporting their folding properties and providing functional groups, which would nominate them as catalytic hubs of great prebiotic relevance.These findings underscore the biochemical plausibility of an early peptide/protein world devoid of more complex amino acids yet collaborating with other catalytic species. Drawing from the mechanistic properties of protein-cofactor catalysis, it is speculated here that the early peptide/protein-cofactor ensemble could facilitate a similar range of chemical reactions, albeit with lower catalytic rates. This hypothesis invites a systematic experimental test.Nonetheless, this Account does not exclude other scenarios of prebiotic-to-biotic catalysis or prioritize any specific pathways of prebiotic syntheses. The objective is to examine peptide availability, composition, and functional potential among the various factors involved in the emergence of early life.

摘要

概述

在探索前生物催化的过程中,不同的分子实体,主要是矿物质、金属离子、有机辅因子和核酶,都被认为是关键因素。在这些因素中,无机和有机辅因子因其能够催化现代代谢中广泛的反应而受到关注,并且经常在现代酶中参与这些反应。然而,将前生物和现代代谢之间的差距联系起来仍然是生命起源的一个基本问题。

在本报告中,研究了肽作为连接矿物质/辅因子的前生物催化与主导现代生命化学反应的酶的潜在桥梁。核糖体合成出现之前,早期地球上可能存在随机序列的肽。这是通过不同的氨基酸输送和合成来源以及在各种条件下它们的缩合来实现的。早期的肽和蛋白质可能表现出不同的组成,富含小的脂族和酸性残基。具有更大侧链和典型碱性基团的氨基酸的丰度增加很可能取决于它们更具挑战性的(生物)合成的出现。因此,出现了紧迫的问题:这种组成如何影响早期肽的性质,以及它们在多大程度上可以促进早期代谢?

我们小组和同事的最新研究表明,仅由假定的“早期”氨基酸组成的高度酸性的肽/蛋白质实际上能够形成二级结构,甚至具有自适应折叠特性,例如自发折叠和不需要伴侣蛋白就能实现可溶性结构。此外,我们表明,具有假定的“早期”组成的高度酸性蛋白质仍然可以通过利用金属离子作为辅因子来结合 RNA,以桥接羧酸盐和磷酸酯官能团。最后,古老的有机辅因子被证明能够与被认为具有前生物合理性的氨基酸序列结合,支持它们的折叠特性并提供功能基团,这将使它们成为具有重要前生物相关性的催化中心。

这些发现强调了缺乏更复杂氨基酸的早期肽/蛋白质世界的生化可行性,但同时也与其他催化物种合作。借鉴蛋白-辅因子催化的机制特性,这里推测早期的肽/蛋白-辅因子组合可以促进类似范围的化学反应,尽管催化速率较低。这个假设邀请了一个系统的实验测试。

然而,本报告并不排除其他前生物到生物催化的情景,也不优先考虑任何特定的前生物合成途径。目的是检查早期生命出现过程中涉及的各种因素中的肽可用性、组成和功能潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c16e/11308367/1377414e3a70/ar4c00137_0001.jpg

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