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2'-脱氧核糖嘌呤底物对非酶促RNA模板指导的引物延伸的影响

Impact of 2'-deoxyribo-purine substrates on nonenzymatic RNA template-directed primer extension.

作者信息

Fang Ziyuan, Acikgoz Orhan, Jia Xiwen, Essex Jahmyl, Wen Ruby, Szostak Jack W

机构信息

Howard Hughes Medical Institute, Department of Chemistry, The University of Chicago, Chicago, IL 60637, USA.

Department of Chemistry and Chemical Biology, Harvard University, 12 Oxford Street, Cambridge, MA 02138, USA.

出版信息

bioRxiv. 2025 Aug 29:2025.08.29.673048. doi: 10.1101/2025.08.29.673048.

Abstract

The composition of the primordial genetic material remains uncertain. Studies of duplex structure and stability, and of nonenzymatic template copying chemistry, provide insight into the viability of potentially primordial genetic polymers. Recent work suggests that 2'-deoxyribo-purine nucleotides may have been generated together with ribonucleotides on the early Earth. Since DNA/RNA duplexes are known to be less stable than RNA/RNA duplexes, we have examined the impact of dA, dI, and dG substitutions on RNA structure and nonenzymatic template copying. We find that single 2'-deoxyribo-purine substitutions reduce RNA duplex stability, as expected. Crystallographic studies show that such substitutions lead to minimal structural changes but point to diminished solvation as a likely reason for duplex destabilization. Kinetic studies show that dI and dG substrates exhibit slightly weaker template binding and slower rates of template-directed primer extension than the corresponding ribo-purine substrates. In contrast, dA substrates exhibit much slower reaction kinetics but higher template affinity than rA substrates. Our results suggest that a mixed RNA/DNA primordial genetic polymer would have suffered from moderately slower rates of template copying, but that this could have been offset by an advantage due to more facile strand separation or exchange.

摘要

原始遗传物质的组成仍然不确定。对双链结构与稳定性以及非酶模板复制化学的研究,为潜在的原始遗传聚合物的可行性提供了见解。最近的研究表明,2'-脱氧核糖嘌呤核苷酸可能与核糖核苷酸在早期地球上同时产生。由于已知DNA/RNA双链体比RNA/RNA双链体更不稳定,我们研究了dA、dI和dG取代对RNA结构和非酶模板复制的影响。我们发现,如预期的那样,单个2'-脱氧核糖嘌呤取代会降低RNA双链体的稳定性。晶体学研究表明,此类取代导致的结构变化最小,但指出溶剂化作用减弱可能是双链体不稳定的原因。动力学研究表明,与相应的核糖嘌呤底物相比,dI和dG底物表现出稍弱的模板结合能力和较慢的模板指导引物延伸速率。相比之下,dA底物表现出慢得多的反应动力学,但比rA底物具有更高的模板亲和力。我们的结果表明,混合的RNA/DNA原始遗传聚合物的模板复制速率可能会适度降低,但这可能会被更易进行的链分离或交换所带来的优势所抵消。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/64e6/12407904/edc90a760e35/nihpp-2025.08.29.673048v1-f0001.jpg

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