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Dual DNA rulers reveal an 'mRNA looping' intermediate state during ribosome translocation

机译:双DNA统治者在核糖体易位期间揭示了“mRNA循环”中间状态

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摘要

The precise 3-nucleotide movement of mRNA is critical for translation fidelity. One mRNA translocation error propagates to all of the following codons, which is detrimental to the cell. However, none of the current methods can reveal the mRNA dynamics near the ribosome entry site, which limits the understanding of this important issue. We have developed an assay of dual DNA rulers that provides such capability. By uniquely probing both the 3MODIFIER LETTER PRIME- and 5MODIFIER LETTER PRIME-ends of mRNA, we observed an antibiotic-trapped intermediate state that is consistent with a ribosomal conformation containing mRNA asymmetric partial displacements at its entry and exit sites. Based on the available ribosome structures and computational simulations, we proposed a 'looped' mRNA conformation, which suggested a stepwise 'inchworm' mechanism for ribosomal translocation. The same 'looped' intermediate state identified with the dual rulers persists with a '-1' frameshifting motif, indicating that the branching point of normal and frameshifting translocations occurs at a later stage of translocation.
机译:mRNA的精确3核苷酸运动对于翻译保真度至关重要。一个mRNA易位误差传播到所有以下密码子,这对细胞不利。然而,目前的方法都不可以揭示核糖体入口场所附近的mRNA动力学,这限制了对这一重要问题的理解。我们开发了一种提供这种能力的双DNA统治者的测定。通过唯一探测MRNA的3种过型字母素和5modifier字母末端,我们观察到抗生素被捕获的中间状态,这与含有MRNA不对称部分位移的核糖体构象一致,其进入和出口位点。基于可用的核糖体结构和计算模拟,我们提出了“环状”mRNA构象,这表明核糖体易位的逐步“九虫”机制。使用双尺寸标识的相同“环路”中间状态持续与'-1'rameshifting图案,表明正常和越来越的易位的分支点发生在易位的稍后阶段。

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