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癌症非整倍体和正常组织的蛋白质基因组分析揭示了细胞通路中基因调控的不同模式。

Proteogenomic analysis of cancer aneuploidy and normal tissues reveals divergent modes of gene regulation across cellular pathways.

机构信息

Institute for Systems Genetics and Department of Biochemistry and Molecular Pharmacology, NYU School of Medicine, New York, United States.

Moores Cancer Center, University of California San Diego, La Jolla, United States.

出版信息

Elife. 2022 Sep 21;11:e75227. doi: 10.7554/eLife.75227.

Abstract

How cells control gene expression is a fundamental question. The relative contribution of protein-level and RNA-level regulation to this process remains unclear. Here, we perform a proteogenomic analysis of tumors and untransformed cells containing somatic copy number alterations (SCNAs). By revealing how cells regulate RNA and protein abundances of genes with SCNAs, we provide insights into the rules of gene regulation. Protein complex genes have a strong protein-level regulation while non-complex genes have a strong RNA-level regulation. Notable exceptions are plasma membrane protein complex genes, which show a weak protein-level regulation and a stronger RNA-level regulation. Strikingly, we find a strong negative association between the degree of RNA-level and protein-level regulation across genes and cellular pathways. Moreover, genes participating in the same pathway show a similar degree of RNA- and protein-level regulation. Pathways including translation, splicing, RNA processing, and mitochondrial function show a stronger protein-level regulation while cell adhesion and migration pathways show a stronger RNA-level regulation. These results suggest that the evolution of gene regulation is shaped by functional constraints and that many cellular pathways tend to evolve one predominant mechanism of gene regulation at the protein level or at the RNA level.

摘要

细胞如何控制基因表达是一个基本问题。蛋白质水平和 RNA 水平调节对这一过程的相对贡献仍不清楚。在这里,我们对含有体细胞拷贝数改变 (SCNAs) 的肿瘤和未转化细胞进行了蛋白质基因组分析。通过揭示细胞如何调节具有 SCNAs 的基因的 RNA 和蛋白质丰度,我们深入了解了基因调控的规则。蛋白质复合物基因具有很强的蛋白质水平调节,而非复合物基因具有很强的 RNA 水平调节。值得注意的例外是质膜蛋白复合物基因,它们表现出较弱的蛋白质水平调节和较强的 RNA 水平调节。引人注目的是,我们发现基因之间以及细胞途径中 RNA 水平和蛋白质水平调节的程度之间存在强烈的负相关。此外,参与相同途径的基因表现出相似程度的 RNA 和蛋白质水平调节。包括翻译、剪接、RNA 加工和线粒体功能在内的途径表现出更强的蛋白质水平调节,而细胞黏附和迁移途径则表现出更强的 RNA 水平调节。这些结果表明,基因调控的进化受到功能限制的影响,许多细胞途径往往倾向于在蛋白质水平或 RNA 水平上进化出一种主要的基因调控机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/387f/9491860/b9844fdd7e21/elife-75227-fig1.jpg

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