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底物结构对II组内含子体外核酶活性的影响。

Influence of substrate structure on in vitro ribozyme activity of a group II intron.

作者信息

Nolte A, Chanfreau G, Jacquier A

机构信息

CNRS (URA 1300), Département des Biotechnologies, Institut Pasteur, Paris, France.

出版信息

RNA. 1998 Jun;4(6):694-708. doi: 10.1017/s1355838298980165.

Abstract

Substrate sequences surrounding catalytic RNAs but not involved in specific, conserved interactions can severely interfere with in vitro ribozyme activity. Using model group II intron precursor transcripts with truncated or randomized exon sequences, we show that unspecific sequences within the 5' exon are particularly prone to inhibit both the forward and the reverse first splicing step (branching). Using in vitro selection, we selected efficient 5' exons for the reverse branching reaction. Precursor RNAs carrying these selected 5' exons reacted more homogeneously and faster than usual model precursor transcripts. This suggests that unfavorable structures induced by the 5' exon can introduce a folding step that limits the rate of in vitro self-splicing. These results stress how critical is the choice of the sequences retained or discarded when isolating folding domains from their natural sequence environments. Moreover, they suggest that exon sequences not involved in specific interactions are more evolutionarily constrained with respect to splicing than previously envisioned.

摘要

围绕催化性RNA但不参与特定保守相互作用的底物序列,可能会严重干扰体外核酶活性。使用具有截短或随机化外显子序列的II组内含子前体转录本模型,我们发现5'外显子内的非特异性序列特别容易抑制正向和反向的第一步剪接反应(分支反应)。通过体外筛选,我们为反向分支反应选择了高效的5'外显子。携带这些选定5'外显子的前体RNA比通常的模型前体转录本反应更均匀、更快。这表明5'外显子诱导的不利结构会引入一个折叠步骤,从而限制体外自我剪接的速率。这些结果强调了从其天然序列环境中分离折叠结构域时,保留或丢弃的序列选择有多关键。此外,它们表明不参与特定相互作用的外显子序列在剪接方面比以前设想的受到更多的进化限制。

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