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The strength of the template effect attracting nucleotides to naked DNA

机译:模板效应的强度将核苷酸吸引到裸露的DNA

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The transmission of genetic information relies on Watson–Crick base pairing between nucleoside phosphates and template bases in template–primer complexes. Enzyme-free primer extension is the purest form of the transmission process, without any chaperon-like effect of polymerases. This simple form of copying of sequences is intimately linked to the origin of life and provides new opportunities for reading genetic information. Here, we report the dissociation constants for complexes between (deoxy)nucleotides and template–primer complexes, as determined by nuclear magnetic resonance and the inhibitory effect of unactivated nucleotides on enzyme-free primer extension. Depending on the sequence context, Kd′s range from 280 mM for thymidine monophosphate binding to a terminal adenine of a hairpin to 2 mM for a deoxyguanosine monophosphate binding in the interior of a sequence with a neighboring strand. Combined with rate constants for the chemical step of extension and hydrolytic inactivation, our quantitative theory explains why some enzyme-free copying reactions are incomplete while others are not. For example, for GMP binding to ribonucleic acid, inhibition is a significant factor in low-yielding reactions, whereas for amino-terminal DNA hydrolysis of monomers is critical. Our results thus provide a quantitative basis for enzyme-free copying.
机译:遗传信息的传递依赖于模板-引物复合物中核苷磷酸和模板碱基之间的沃森-克里克碱基配对。无酶引物延伸是传递过程中最纯净的形式,没有聚合酶的任何伴侣状作用。序列复制的这种简单形式与生命的起源紧密相关,并为阅读遗传信息提供了新的机会。在这里,我们报告了(脱氧)核苷酸和模板-引物复合物之间的复合解离常数,这是由核磁共振和未激活的核苷酸对无酶引物延伸的抑制作用所确定的。取决于序列的上下文,K d的范围为:在与内部发条相邻的序列中,胸腺嘧啶一磷酸结合到发夹的末端腺嘌呤的280 mM到脱氧鸟苷单磷酸结合的2 mM。 。结合用于化学延伸和水解灭活的速率常数,我们的定量理论解释了为什么一些无酶复制反应不完整而另一些则不是。例如,对于GMP与核糖核酸的结合,抑制是低产率反应中的重要因素,而对于氨基末端DNA的单体水解则至关重要。因此,我们的结果为无酶复制提供了定量基础。

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