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前生物条件下底物导向的小型生物催化剂的形成。

Substrate-directed formation of small biocatalysts under prebiotic conditions.

作者信息

Kochavi E, Bar-Nun A, Fleminger G

机构信息

Department of Geophysics and Planetary Sciences, Tel Aviv University, Israel.

出版信息

J Mol Evol. 1997 Oct;45(4):342-51. doi: 10.1007/pl00006239.

Abstract

One of the most debated issues concerning the origin of life, is how enzymes which are essential for existence of any living organism, evolved. It is clear that, regardless of the exact mechanism, the process should have been specific and reproducible, involving interactions between different molecules. We propose that substrate templating played a crucial role in maintaining reproducible and specific formation of prebiotic catalysts. This work demonstrates experimentally, for the first time, substrate-directed formation of an oligopeptide that possesses a specific catalytic activity toward the substrate on which it was formed. In our experiments we used the substrate O-nitrophenol-beta-D-galactopyranoside (ONPG) as a molecular template for the synthesis of a specific catalyst that is capable of cleaving the same substrate. This was achieved by incubation of the substrate with free amino acids and a condensing agent (dicyandiamide) at elevated temperatures. A linear increase with time of the reaction rate (d[product]/d2t), pointed to an acceleration regime, where the substrate generates the formation of the catalyst. The purified catalyst, produced by a substrate-directed mechanism, was analyzed, and identified as Cys2-Fe+2. The mechanism of substrate-directed formation of prebiotic catalysts provides a solution to both the specificity and the reproducibility requirements from any prebiotic system which should evolve into the biological world.

摘要

关于生命起源最具争议的问题之一,是任何生物体生存所必需的酶是如何进化的。很明显,无论确切的机制如何,这个过程都应该是特定且可重复的,涉及不同分子之间的相互作用。我们认为底物模板化在维持益生元催化剂的可重复和特异性形成中起着关键作用。这项工作首次通过实验证明了底物导向形成的一种寡肽,它对其形成时所基于的底物具有特定的催化活性。在我们的实验中,我们使用底物邻硝基苯酚-β-D-吡喃半乳糖苷(ONPG)作为分子模板来合成一种能够裂解相同底物的特异性催化剂。这是通过在高温下将底物与游离氨基酸和缩合剂(双氰胺)一起孵育来实现的。反应速率(d[产物]/dt²)随时间呈线性增加,表明存在加速阶段,即底物促使催化剂形成。对通过底物导向机制产生的纯化催化剂进行了分析,并鉴定为Cys2-Fe+2。益生元催化剂底物导向形成的机制为任何应进化为生物世界的益生元系统的特异性和可重复性要求都提供了解决方案。

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