MicroRNA-27a-3p targets FoxO signalling to induce tumour-like phenotypes in bile duct cells

Background & Aims: Cholangiocarcinoma (CCA) is a heterogeneous and lethal malignancy, the molecular origins of which remain poorly understood. MicroRNAs (miRs) target diverse signalling pathways, functioning as potent epigenetic regulators of tran-scriptional output. We aimed to characterise miR...

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Autores: Duwe, L. (Lea)|||/items/1df65fa7-63f1-4c57-bb9d-7d33879e5cdb, Munoz-Garrido, P. (Patricia)|||/items/5791e618-3b5a-4fee-935b-e4ef9a792005, Lewinska, M. (Monika)|||/items/1e033557-9622-4746-982f-0fee929aabef, Lafuente-Barquero, J. (Juan)|||/items/b8c028e6-0270-432b-bf89-151996164af3, Satriano, L. (Letizia)|||/items/4dadbe44-845d-4b04-a853-fb105958c197, Hogdall, D. (Dan)|||/items/6081a4f3-817c-46c2-8701-082f39fbe2f4, Taranta, A. (Andrzej)|||/items/23baccb4-878a-41c7-afca-aaae4f253ff0, Nielsen, B.S. (Boye S.)|||/items/5954aa2e-711c-40f5-8fa3-613b29e0d6b8, Ghazal, A. (Awaisa)|||/items/cd460a86-08d7-4735-b982-ab350ffaaeda, Matter, M.S. (Matthias S.)|||/items/47ce053d-852a-4a42-866d-5ddff37ff20b, Banales, J.M. (Jesús M.)|||/items/0c1309ae-e4e4-4e85-b2f1-567a388889d5, Aldana, B.I. (Blanca I.)|||/items/d025dc42-f502-4b2b-8960-428adf46c3ff, Gao, Y.T. (Yu-Tang)|||/items/1309d47b-b519-4f60-96de-558e08f9d0f5, Marquardt, J.U. (Jens U.)|||/items/8893339b-8329-4877-b932-062ad496013c, Roberts, L.R. (Lewis R.)|||/items/53e58801-8eb8-49f9-9fd2-46b93d01e35b, Oliveira, R.C. (Rui C.)|||/items/c1955700-d117-489f-8f07-10e795024300, Koshiol, J. (Jill)|||/items/33448410-bb90-4f8f-89fd-896df187081d, O’Rourke, C.J. (Colm J.)|||/items/087eb514-d64b-470f-92a8-64ed5518c11f, Andersen, J.B. (Jesper B.)|||/items/30522278-e252-4feb-9558-84b5c027103a
Tipo de recurso: artículo
Fecha de publicación:2023
País:España
Institución:Universidad de Navarra
Repositorio:Dadun. Depósito Académico Digital de la Universidad de Navarra
Idioma:inglés
OAI Identifier:oai:dadun.unav.edu:10171/65979
Acceso en línea:https://hdl.handle.net/10171/65979
Access Level:acceso abierto
Palabra clave:Cholangiocarcinoma
Cholangiocytes
FoxO1
microRNAs
Proliferation
Descripción
Sumario:Background & Aims: Cholangiocarcinoma (CCA) is a heterogeneous and lethal malignancy, the molecular origins of which remain poorly understood. MicroRNAs (miRs) target diverse signalling pathways, functioning as potent epigenetic regulators of tran-scriptional output. We aimed to characterise miRNome dysregulation in CCA, including its impact on transcriptome homeostasis and cell behaviour.Methods: Small RNA sequencing was performed on 119 resected CCAs, 63 surrounding liver tissues, and 22 normal livers. High -throughput miR mimic screens were performed in three primary human cholangiocyte cultures. Integration of patient tran-scriptomes and miRseq together with miR screening data identified an oncogenic miR for characterization. MiR-mRNA in-teractions were investigated by a luciferase assay. MiR-CRISPR knockout cells were generated and phenotypically characterized in vitro (proliferation, migration, colony, mitochondrial function, glycolysis) and in vivo using subcutaneous xenografts.Results: In total, 13% (140/1,049) of detected miRs were differentially expressed between CCA and surrounding liver tissues, including 135 that were upregulated in tumours. CCA tissues were characterised by higher miRNome heterogeneity and miR biogenesis pathway expression. Unsupervised hierarchical clustering of tumour miRNomes identified three subgroups, including distal CCA-enriched and IDH1 mutant-enriched subgroups. High-throughput screening of miR mimics uncovered 71 miRs that consistently increased proliferation of three primary cholangiocyte models and were upregulated in CCA tissues regardless of anatomical location, among which only miR-27a-3p had consistently increased expression and activity in several cohorts. FoxO signalling was predominantly downregulated by miR-27a-3p in CCA, partially through targeting of FOXO1. MiR-27a knockout increased FOXO1 levels in vitro and in vivo, impeding tumour behaviour and growth.Conclusions: The miRNomes of CCA tissues are highly remodelled, impacting transcriptome homeostasis in part through regulation of transcription factors like FOXO1. MiR-27a-3p arises as an oncogenic vulnerability in CCA.