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小 RNA 驱动的前馈环:通过 sRNA 介导的串扰精细调控蛋白质合成。

Small RNA-driven feed-forward loop: fine-tuning of protein synthesis through sRNA-mediated crosstalk.

机构信息

Protein Chemistry and Technology, Central Food Technological Research Institute, Mysore, Karnataka, 570 020, India.

Mathematical and Physical Sciences Division, School of Arts and Sciences, Ahmedabad University, Navrangpura, Ahmedabad, 380009, India.

出版信息

Eur Phys J E Soft Matter. 2021 Apr 19;44(4):55. doi: 10.1140/epje/s10189-021-00013-0.

Abstract

Often in bacterial regulatory networks, small non-coding RNAs (sRNA) interact with several mRNA species. The competition among mRNAs for binding to the common pool of sRNA might lead to crosstalk between the mRNAs. This is similar to the competing endogenous RNA effect that leads to complex gene regulation with stabilized gene expression in Eukaryotes. Here, we study an sRNA-driven feed-forward loop (sFFL) where the top-tier regulator, an sRNA, translationally activates the target protein (TP) as well as a transcriptional activator of the TP through binding to the respective mRNAs. We show that the sRNA-mediated crosstalk between the two mRNA species enables the sFFL to function in three different regimes depending on the synthesis rate of the transcriptional activator mRNA. Of these three regimes, there exists a sensitive regime where the TP level shows interesting features depending on the precise mechanism of target translation. In the case of translation entirely from sRNA-mRNA bound complexes, the TP level becomes maximum around the sensitive regime. Through stochastic analysis and simulations, we show that relative fluctuations in the TP level is minimized here. For translation both from mRNA and sRNA-mRNA bound complexes, the target expression shows a threshold response across the sensitive regime.

摘要

在细菌调控网络中,小分子非编码 RNA(sRNA)通常与几种 mRNA 相互作用。mRNA 与 sRNA 结合的竞争可能导致 mRNA 之间的串扰。这类似于竞争内源性 RNA 效应,导致真核生物中复杂的基因调控和稳定的基因表达。在这里,我们研究了一个由 sRNA 驱动的前馈环(sFFL),其中顶层调节剂 sRNA 通过与相应的 mRNA 结合,翻译激活靶蛋白(TP)以及 TP 的转录激活剂。我们表明,两种 mRNA 之间的 sRNA 介导的串扰使 sFFL 能够在三种不同的状态下发挥作用,具体取决于转录激活剂 mRNA 的合成速率。在这三种状态中,存在一个敏感状态,TP 水平根据靶翻译的精确机制表现出有趣的特征。在完全从 sRNA-mRNA 结合复合物翻译的情况下,TP 水平在敏感状态下达到最大值。通过随机分析和模拟,我们表明这里可以最小化 TP 水平的相对波动。对于同时从 mRNA 和 sRNA-mRNA 结合复合物翻译的情况,目标表达在敏感状态下呈现出阈值响应。

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