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Tissue- and development-stage–specific mRNA and heterogeneous CNV signatures of human ribosomal proteins in normal and cancer samples

机译:正常和癌症样品中人核糖体蛋白的组织和发育阶段特异性mRNA和异质CNV特征

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摘要

We give results from a detailed analysis of human Ribosomal Protein (RP) levels in normal and cancer samples and cell lines from large mRNA, copy number variation and ribosome profiling datasets. After normalizing total RP mRNA levels per sample, we find highly consistent tissue specific RP mRNA signatures in normal and tumor samples. Multiple RP mRNA-subtypes exist in several cancers, with significant survival and genomic differences. Some RP mRNA variations among subtypes correlate with copy number loss of RP genes. In kidney cancer, RP subtypes map to molecular subtypes related to cell-of-origin. Pan-cancer analysis of TCGA data showed widespread single/double copy loss of RP genes, without significantly affecting survival. In several cancer cell lines, CRISPR-Cas9 knockout of RP genes did not affect cell viability. Matched RP ribosome profiling and mRNA data in humans and rodents stratified by tissue and development stage and were strongly correlated, showing that RP translation rates were proportional to mRNA levels. In a small dataset of human adult and fetal tissues, RP protein levels showed development stage and tissue specific heterogeneity of RP levels. Our results suggest that heterogeneous RP levels play a significant functional role in cellular physiology, in both normal and disease states.
机译:我们给出了对正常和癌症样品以及大mRNA,拷贝数变异和核糖体谱数据集中的细胞系中人核糖体蛋白(RP)水平进行详细分析的结果。在将每个样品的总RP mRNA水平标准化后,我们在正常和肿瘤样品中发现高度一致的组织特异性RP mRNA特征。多种癌症中存在多种RP mRNA亚型,具有明显的生存率和基因组差异。亚型之间的一些RP mRNA变化与RP基因的拷贝数丢失有关。在肾癌中,RP亚型映射到与起源细胞相关的分子亚型。 TCGA数据的全癌分析表明,RP基因普遍存在单/双拷贝丢失,而没有显着影响生存率。在几种癌细胞系中,RP-基因的CRISPR-Cas9敲除并不影响细胞活力。人体和啮齿类动物按组织和发育阶段分层的匹配的RP核糖体图谱和mRNA数据,并具有很强的相关性,表明RP的翻译率与mRNA水平成正比。在人类成人和胎儿组织的小型数据集中,RP蛋白水平显示了RP水平的发育阶段和组织特异性异质性。我们的结果表明,在正常和疾病状态下,异质RP水平在细胞生理中均起着重要的作用。

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