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系统研究细胞社会中 mRNA 和蛋白质之间的全球协调。

Systematic investigation of global coordination among mRNA and protein in cellular society.

机构信息

School of Life Science and Technology, Tongji University, Shanghai 200092, China.

出版信息

BMC Genomics. 2010 Jun 9;11:364. doi: 10.1186/1471-2164-11-364.

Abstract

BACKGROUND

Cell functions depend on molecules organized in the cellular society. Two basic components are mRNA molecules and proteins. The interactions within and between those two components are crucial for carrying out sophisticated cell functions. The interplay can be analyzed by comparing expression levels of mRNA and proteins. This is critical for understanding the molecular interactions, (post-) transcriptional regulations and conservation of co-expression between mRNAs and proteins. By using high-throughput transcriptome and proteome data, this study aims to systematically investigate the general picture of such expression correlations. We analyze four groups of correlations: (i) transcript levels of different genes, (ii) protein levels of different genes, (iii) mRNA levels with protein levels of different genes and (iv) mRNA levels with protein levels of same genes. This helps to obtain global insights into the stability and variability of co-expression and correlation of mRNA and protein levels.

RESULTS

Analysis of the simultaneous co-expression of mRNAs and proteins yields mainly weak correlations. Therefore we introduce the concept of time-delayed co-expression patterns. Based on a time-course dataset, we obtain a high fraction of time-delayed correlations. In group (i), 67% of different transcripts are significantly correlated. At the protein level (ii), 68% of different proteins are significantly correlated. Comparison of the different molecular levels results in a 74% fraction of correlated transcript and protein levels of different genes (iii) and 56% for the same genes (iv). Furthermore, a higher fraction of protein levels (simultaneously 20% and short time-delayed 29%) is correlated than at the transcript level (10% and 18% respectively). Analysis of the dynamics of the correlation shows that correlation at the transcript level is largely passed to the protein level. In contrast, specific co-expression patterns are changed in multiple ways.

CONCLUSIONS

Our analysis reveals that the regulation of transcription and translation contains a time-delayed component. The correlation at the protein level is more synchronous or delayed by shorter time than those at the transcript level. This supports the hypothesis that a higher degree of direct physical interactions require a higher synchronicity between the interacting partners. The conservation of correlation between the transcript level (i) and the protein level (ii) sheds light on the processes underlying transcription, translation and regulation. A future investigation of the conditions of conservation will give comprehensive insights in the complexity of the regulatory mechanisms.

摘要

背景

细胞功能依赖于细胞社会中组织的分子。两个基本组成部分是 mRNA 分子和蛋白质。这两个组成部分内部和之间的相互作用对于执行复杂的细胞功能至关重要。这种相互作用可以通过比较 mRNA 和蛋白质的表达水平来分析。这对于理解分子相互作用、(转录后)调控以及 mRNA 和蛋白质之间的共表达的保守性至关重要。本研究利用高通量转录组和蛋白质组数据,系统地研究了这种表达相关性的一般情况。我们分析了四组相关性:(i)不同基因的转录本水平,(ii)不同基因的蛋白质水平,(iii)不同基因的 mRNA 水平与蛋白质水平,以及(iv)相同基因的 mRNA 水平与蛋白质水平。这有助于全面了解 mRNA 和蛋白质水平的共表达和相关性的稳定性和可变性。

结果

对 mRNA 和蛋白质的同时共表达分析主要产生较弱的相关性。因此,我们引入了时滞共表达模式的概念。基于时间序列数据集,我们获得了高比例的时滞相关性。在组(i)中,67%的不同转录本显著相关。在蛋白质水平(ii)中,68%的不同蛋白质显著相关。不同分子水平的比较导致不同基因的转录本和蛋白质水平(iii)的相关性分数为 74%,相同基因(iv)的相关性分数为 56%。此外,蛋白质水平的相关性比例(同时为 20%和短时间延迟为 29%)高于转录本水平(分别为 10%和 18%)。对相关性的动态分析表明,转录本水平的相关性在很大程度上传递到蛋白质水平。相反,特定的共表达模式以多种方式发生变化。

结论

我们的分析表明,转录和翻译的调控包含一个时滞成分。蛋白质水平的相关性比转录本水平更同步或延迟更短的时间。这支持了这样一种假设,即更高程度的直接物理相互作用需要相互作用的伙伴之间更高的同步性。转录本水平(i)和蛋白质水平(ii)之间相关性的保守性揭示了转录、翻译和调控背后的过程。对保守性条件的进一步研究将全面了解调控机制的复杂性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f86/2900266/a16397f2fe63/1471-2164-11-364-1.jpg

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