A concurrent canonical and modified miRNAome pan-cancer study on TCGA and TARGET cohorts leads to an enhanced resolution in cancer

Author:

Distefano RosarioORCID,Tomasello LuisaORCID,Vinciguerra Gian Luca RampioniORCID,Gasparini PierluigiORCID,Xiang Yujia,Bagnoli MarinaORCID,Marceca Gioacchino PaoloORCID,Fadda Paolo,Lagana AlessandroORCID,Acunzo Mario,Ma QinORCID,Nigita GiovanniORCID,Croce Carlo MORCID

Abstract

MiRNA Epitranscriptomics has placed a new layer of complexity in the cancer field. Despite the fastgrowing interest in miRNA editing and shifted miRNA isoforms, a simultaneous study of both modifications in cancer is still missing. Here, we concurrently profiled multiple miRNA modifications, including A-to-I RNA editing and shifted miRNA isoforms, in >13K adult and pediatric tumor samples across 38 distinct cancer cohorts from The Cancer Genome Atlas and The Therapeutically Applicable Research to Generate Effective Treatments datasets. We investigated the differences among canonical miRNAs and the wider miRNAome in terms of expression, clustering, dysregulation, and prognostic standpoint. The combination of canonical miRNAs/miRNA isoforms boosted the quality of clustering results, outlining unique cohorts' clinical-pathological features. We described modified miRNAs showing opposite dysregulation with respect to their canonical counterparts in cancer, potentially impacting their targetome and function. The abundance of expressed miRNA isoforms directly impacted the activation/deactivation of critical carcinogenesis pathways. Finally, we experimentally validated unique targeting for a shifted and edited miRNA isoform. Our findings outlined once more the importance of going beyond the well-established paradigm of one-mature-miRNA per miRNA arm to elucidate novel mechanisms related to cancer progression.

Publisher

Cold Spring Harbor Laboratory

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