4.5 Article

Integrative analyses of the RNA modification machinery reveal tissue- and cancer-specific signatures

期刊

GENOME BIOLOGY
卷 21, 期 1, 页码 -

出版社

BMC
DOI: 10.1186/s13059-020-02009-z

关键词

RNA modifications; Epitranscriptomics; Tissue specificity; Dysregulation in cancer

资金

  1. UNSW International PhD fellowship
  2. FPI Severo Ochoa PhD fellowship from the Spanish Ministry of Economy, Industry and Competitiveness (MEIC)
  3. Discovery Early Career Researcher Award from the Australian Research Council [DE170100506]
  4. CRG Severo Ochoa Funding
  5. Australian Research Council [DP180103571]
  6. Spanish Ministry of Economy, Industry and Competitiveness [PGC2018-098152-A-100]
  7. NHMRC funds [APP1070631]
  8. Spanish Ministry of Economy, Industry and Competitiveness (MEIC)
  9. CERCA Programme/Generalitat de Catalunya
  10. Australian Research Council [DE170100506] Funding Source: Australian Research Council

向作者/读者索取更多资源

Background RNA modifications play central roles in cellular fate and differentiation. However, the machinery responsible for placing, removing, and recognizing more than 170 RNA modifications remains largely uncharacterized and poorly annotated, and we currently lack integrative studies that identify which RNA modification-related proteins (RMPs) may be dysregulated in each cancer type. Results Here, we perform a comprehensive annotation and evolutionary analysis of human RMPs, as well as an integrative analysis of their expression patterns across 32 tissues, 10 species, and 13,358 paired tumor-normal human samples. Our analysis reveals an unanticipated heterogeneity of RMP expression patterns across mammalian tissues, with a vast proportion of duplicated enzymes displaying testis-specific expression, suggesting a key role for RNA modifications in sperm formation and possibly intergenerational inheritance. We uncover many RMPs that are dysregulated in various types of cancer, and whose expression levels are predictive of cancer progression. Surprisingly, we find that several commonly studied RNA modification enzymes such as METTL3 or FTO are not significantly upregulated in most cancer types, whereas several less-characterized RMPs, such as LAGE3 and HENMT1, are dysregulated in many cancers. Conclusions Our analyses reveal an unanticipated heterogeneity in the expression patterns of RMPs across mammalian tissues and uncover a large proportion of dysregulated RMPs in multiple cancer types. We provide novel targets for future cancer research studies targeting the human epitranscriptome, as well as foundations to understand cell type-specific behaviors that are orchestrated by RNA modifications.

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