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核糖体干扰、密码子使用和出口隧道相互作用对翻译延伸速率变化的影响。

The impact of ribosomal interference, codon usage, and exit tunnel interactions on translation elongation rate variation.

机构信息

Computer Science Division, University of California Berkeley, Berkeley, California, United States of America.

Department of Statistics, University of California Berkeley, Berkeley, California, United States of America.

出版信息

PLoS Genet. 2018 Jan 16;14(1):e1007166. doi: 10.1371/journal.pgen.1007166. eCollection 2018 Jan.

Abstract

Previous studies have shown that translation elongation is regulated by multiple factors, but the observed heterogeneity remains only partially explained. To dissect quantitatively the different determinants of elongation speed, we use probabilistic modeling to estimate initiation and local elongation rates from ribosome profiling data. This model-based approach allows us to quantify the extent of interference between ribosomes on the same transcript. We show that neither interference nor the distribution of slow codons is sufficient to explain the observed heterogeneity. Instead, we find that electrostatic interactions between the ribosomal exit tunnel and specific parts of the nascent polypeptide govern the elongation rate variation as the polypeptide makes its initial pass through the tunnel. Once the N-terminus has escaped the tunnel, the hydropathy of the nascent polypeptide within the ribosome plays a major role in modulating the speed. We show that our results are consistent with the biophysical properties of the tunnel.

摘要

先前的研究表明,翻译延伸受到多种因素的调节,但观察到的异质性仍然只能部分解释。为了定量剖析延伸速度的不同决定因素,我们使用概率建模从核糖体分析数据中估计起始和局部延伸速度。这种基于模型的方法使我们能够量化同一转录物上核糖体之间的干扰程度。我们发现,干扰或慢速密码子的分布都不足以解释观察到的异质性。相反,我们发现,核糖体出口隧道与新生多肽特定部分之间的静电相互作用控制着延伸速度的变化,因为多肽最初穿过隧道。一旦 N 端逃离隧道,核糖体中新生多肽的亲水性在调节速度方面起着重要作用。我们表明,我们的结果与隧道的物理性质一致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0e8b/5786338/199175a958e2/pgen.1007166.g001.jpg

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