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通过研究mRNA与蛋白质丰度之间的特定关系来鉴定应激反应基因。

Identification of stress responsive genes by studying specific relationships between mRNA and protein abundance.

作者信息

Morimoto Shimpei, Yahara Koji

机构信息

Division of Biostatistics, Kurume University School of Medicine, Fukuoka, Japan.

Antimicrobial Resistance Research Center, National Institute of Infectious Diseases, Tokyo, Japan.

出版信息

Heliyon. 2018 Mar 8;4(3):e00558. doi: 10.1016/j.heliyon.2018.e00558. eCollection 2018 Mar.

Abstract

Protein expression is regulated by the production and degradation of mRNAs and proteins but the specifics of their relationship are controversial. Although technological advances have enabled genome-wide and time-series surveys of mRNA and protein abundance, recent studies have shown paradoxical results, with most statistical analyses being limited to linear correlation, or analysis of variance applied separately to mRNA and protein datasets. Here, using recently analyzed genome-wide time-series data, we have developed a statistical analysis framework for identifying which types of genes or biological gene groups have significant correlation between mRNA and protein abundance after accounting for potential time delays. Our framework stratifies all genes in terms of the extent of time delay, conducts gene clustering in each stratum, and performs a non-parametric statistical test of the correlation between mRNA and protein abundance in a gene cluster. Consequently, we revealed stronger correlations than previously reported between mRNA and protein abundance in two metabolic pathways. Moreover, we identified a pair of stress responsive genes ( and ) that showed a highly similar time series of mRNA and protein abundance. Furthermore, we confirmed robustness of the analysis framework by applying it to another genome-wide time-series data and identifying a cytoskeleton-related gene cluster (keratin 18, keratin 17, and mitotic spindle positioning) that shows similar correlation. The significant correlation and highly similar changes of mRNA and protein abundance suggests a concerted role of these genes in cellular stress response, which we consider provides an answer to the question of the specific relationships between mRNA and protein in a cell. In addition, our framework for studying the relationship between mRNAs and proteins in a cell will provide a basis for studying specific relationships between mRNA and protein abundance after accounting for potential time delays.

摘要

蛋白质表达受mRNA和蛋白质的产生与降解调控,但其关系的具体细节存在争议。尽管技术进步使得能够对mRNA和蛋白质丰度进行全基因组和时间序列调查,但最近的研究显示出矛盾的结果,大多数统计分析仅限于线性相关性,或分别应用于mRNA和蛋白质数据集的方差分析。在这里,我们使用最近分析的全基因组时间序列数据,开发了一个统计分析框架,用于识别在考虑潜在时间延迟后,哪些类型的基因或生物基因组在mRNA和蛋白质丰度之间具有显著相关性。我们的框架根据时间延迟程度对所有基因进行分层,在每个层中进行基因聚类,并对基因簇中mRNA和蛋白质丰度之间的相关性进行非参数统计检验。因此,我们揭示了两条代谢途径中mRNA和蛋白质丰度之间比先前报道更强的相关性。此外,我们鉴定出一对应激反应基因(和),它们显示出高度相似的mRNA和蛋白质丰度时间序列。此外,我们通过将其应用于另一个全基因组时间序列数据并识别出一个显示相似相关性的细胞骨架相关基因簇(角蛋白18、角蛋白17和有丝分裂纺锤体定位),证实了该分析框架的稳健性。mRNA和蛋白质丰度的显著相关性以及高度相似的变化表明这些基因在细胞应激反应中协同发挥作用,我们认为这为细胞中mRNA和蛋白质之间的特定关系问题提供了答案。此外,我们用于研究细胞中mRNA和蛋白质之间关系的框架将为在考虑潜在时间延迟后研究mRNA和蛋白质丰度之间的特定关系提供基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/111f/5857721/938cd8c83332/gr1.jpg

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