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对核糖体中密码子与反密码子相互作用的分析为密码子解读和遗传密码结构提供了新的见解。

Analysis of codon:anticodon interactions within the ribosome provides new insights into codon reading and the genetic code structure.

作者信息

Lim V I, Curran J F

机构信息

Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, Moscow.

出版信息

RNA. 2001 Jul;7(7):942-57. doi: 10.1017/s135583820100214x.

Abstract

Although the decoding rules have been largely elucidated, the physical-chemical reasons for the "correctness" of codon:anticodon duplexes have never been clear. In this work, on the basis of the available data, we propose that the correct codon:anticodon duplexes are those whose formation and interaction with the ribosomal decoding center are not accompanied by uncompensated losses of hydrogen and ionic bonds. Other factors such as proofreading, base-base stacking and aminoacyl-tRNA concentration contribute to the efficiency and accuracy of aminoacyl-tRNA selection, and certainly these factors are important; but we suggest that analyses of hydrogen and ionic bonding alone provides a robust first-order approximation of decoding accuracy. Thus our model can simplify predictions about decoding accuracy and error. The model can be refined with data, but is already powerful enough to explain all of the available data on decoding accuracy. Here we predict which duplexes should be considered correct, which duplexes are responsible for virtually all misreading, and we suggest an evolutionary scheme that gave rise to the mixed boxes of the genetic code.

摘要

尽管解码规则已基本阐明,但密码子:反密码子双链体“正确性”的物理化学原因一直不清楚。在这项工作中,基于现有数据,我们提出正确的密码子:反密码子双链体是那些其形成以及与核糖体解码中心的相互作用不会伴随着氢键和离子键的无补偿损失的双链体。其他因素,如校对、碱基堆积和氨酰 - tRNA浓度,对氨酰 - tRNA选择的效率和准确性有影响,当然这些因素很重要;但我们认为仅对氢键和离子键的分析就能提供解码准确性的可靠一阶近似值。因此,我们的模型可以简化关于解码准确性和错误的预测。该模型可以用数据进行完善,但已经强大到足以解释所有关于解码准确性的现有数据。在此,我们预测哪些双链体应被视为正确的,哪些双链体几乎导致了所有的错读,并且我们提出了一种进化方案,该方案产生了遗传密码的混合密码子框。

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