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Polymerase ribozyme efficiency increased by G/T-rich DNA oligonucleotides.

机译:富含G / T的DNA寡核苷酸可提高聚合酶核酶的效率。

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摘要

The RNA world hypothesis states that the early evolution of life went through a stage where RNA served as genome and as catalyst. The replication of RNA world organisms would have been facilitated by ribozymes that catalyze RNA polymerization. To recapitulate an RNA world in the laboratory, a series of RNA polymerase ribozymes was developed previously. However, these ribozymes have a polymerization efficiency that is too low for self-replication, and the most efficient ribozymes prefer one specific template sequence. The limiting factor for polymerization efficiency is the weak sequence-independent binding to its primer/template substrate. Most of the known polymerase ribozymes bind an RNA heptanucleotide to form the P2 duplex on the ribozyme. By modifying this heptanucleotide, we were able to significantly increase polymerization efficiency. Truncations at the 3'-terminus of this heptanucleotide increased full-length primer extension by 10-fold, on a specific template sequence. In contrast, polymerization on several different template sequences was improved dramatically by replacing the RNA heptanucleotide with DNA oligomers containing randomized sequences of 15 nt. The presence of G and T in the random sequences was sufficient for this effect, with an optimal composition of 60% G and 40% T. Our results indicate that these DNA sequences function by establishing many weak and nonspecific base-pairing interactions to the single-stranded portion of the template. Such low-specificity interactions could have had important functions in an RNA world.
机译:RNA世界假说指出,生命的早期进化经历了一个RNA充当基因组和催化剂的阶段。催化RNA聚合的核酶将促进RNA世界生物的复制。为了概括实验室中的RNA世界,以前开发了一系列RNA聚合酶核酶。然而,这些核酶的聚合效率对于自我复制而言太低,并且最有效的核酶更喜欢一种特定的模板序列。聚合效率的限制因素是与其引物/模板底物的弱序列依赖性结合。大多数已知的聚合酶核酶结合RNA七核苷酸以在核酶上形成P2双链体。通过修饰该七核苷酸,我们能够显着提高聚合效率。在特定模板序列上,此七核苷酸的3'端截断可将全长引物延伸增加10倍。相反,通过用包含15 nt随机序列的DNA寡聚物替代RNA七核苷酸,可以显着改善几种不同模板序列上的聚合。随机序列中G和T的存在足以达到这种效果,最佳组成为60%G和40%T。我们的结果表明,这些DNA序列通过与单个DNA建立许多弱的和非特异性的碱基配对相互作用而起作用模板的链部分。这样的低特异性相互作用可能在RNA世界中发挥了重要作用。

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