Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing

INTRODUCTION: Altered splicing landscape is an emerging cancer hallmark; however, the dysregulation and implication of the cellular machinery controlling this process (spliceosome components and splicing factors) in hepatocellular carcinoma (HCC) is poorly known. This study aimed to comprehensively...

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Autores principales: López‐Cánovas, Juan L., Hermán‐Sánchez, Natalia, Moreno‐Montilla, Maria Trinidad, del Rio‐Moreno, Mercedes, Alors‐Perez, Emilia, Sánchez‐Frias, Marina E., Amado, Víctor, Ciria, Rubén, Briceño, Javier, de la Mata, Manuel, Castaño, Justo P., Rodriguez‐Perálvarez, Manuel, Luque, Raúl M., Gahete, Manuel D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2022
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9684617/
https://www.ncbi.nlm.nih.gov/pubmed/36419260
http://dx.doi.org/10.1002/ctm2.1102
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author López‐Cánovas, Juan L.
Hermán‐Sánchez, Natalia
Moreno‐Montilla, Maria Trinidad
del Rio‐Moreno, Mercedes
Alors‐Perez, Emilia
Sánchez‐Frias, Marina E.
Amado, Víctor
Ciria, Rubén
Briceño, Javier
de la Mata, Manuel
Castaño, Justo P.
Rodriguez‐Perálvarez, Manuel
Luque, Raúl M.
Gahete, Manuel D.
author_facet López‐Cánovas, Juan L.
Hermán‐Sánchez, Natalia
Moreno‐Montilla, Maria Trinidad
del Rio‐Moreno, Mercedes
Alors‐Perez, Emilia
Sánchez‐Frias, Marina E.
Amado, Víctor
Ciria, Rubén
Briceño, Javier
de la Mata, Manuel
Castaño, Justo P.
Rodriguez‐Perálvarez, Manuel
Luque, Raúl M.
Gahete, Manuel D.
author_sort López‐Cánovas, Juan L.
collection PubMed
description INTRODUCTION: Altered splicing landscape is an emerging cancer hallmark; however, the dysregulation and implication of the cellular machinery controlling this process (spliceosome components and splicing factors) in hepatocellular carcinoma (HCC) is poorly known. This study aimed to comprehensively characterize the spliceosomal profile and explore its role in HCC. METHODS: Expression levels of 70 selected spliceosome components and splicing factors and clinical implications were evaluated in two retrospective and six in silico HCC cohorts. Functional, molecular and mechanistic studies were implemented in three cell lines (HepG2, Hep3B and SNU‐387) and preclinical Hep3B‐induced xenograft tumours. RESULTS: Spliceosomal dysregulations were consistently found in retrospective and in silico cohorts. EIF4A3, RBM3, ESRP2 and SRPK1 were the most dysregulated spliceosome elements in HCC. EIF4A3 expression was associated with decreased survival and greater recurrence. Plasma EIF4A3 levels were significantly elevated in HCC patients. In vitro EIF4A3‐silencing (or pharmacological inhibition) resulted in reduced aggressiveness, and hindered xenograft‐tumours growth in vivo, whereas EIF4A3 overexpression increased tumour aggressiveness. EIF4A3‐silencing altered the expression and splicing of key HCC‐related genes, specially FGFR4. EIF4A3‐silencing blocked the cellular response to the natural ligand of FGFR4, FGF19. Functional consequences of EIF4A3‐silencing were mediated by FGFR4 splicing as the restoration of non‐spliced FGFR4 full‐length version blunted these effects, and FGFR4 inhibition did not exert further effects in EIF4A3‐silenced cells. CONCLUSIONS: Splicing machinery is strongly dysregulated in HCC, providing a source of new diagnostic, prognostic and therapeutic options in HCC. EIF4A3 is consistently elevated in HCC patients and associated with tumour aggressiveness and mortality, through the modulation of FGFR4 splicing.
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spelling pubmed-96846172022-11-25 Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing López‐Cánovas, Juan L. Hermán‐Sánchez, Natalia Moreno‐Montilla, Maria Trinidad del Rio‐Moreno, Mercedes Alors‐Perez, Emilia Sánchez‐Frias, Marina E. Amado, Víctor Ciria, Rubén Briceño, Javier de la Mata, Manuel Castaño, Justo P. Rodriguez‐Perálvarez, Manuel Luque, Raúl M. Gahete, Manuel D. Clin Transl Med Research Articles INTRODUCTION: Altered splicing landscape is an emerging cancer hallmark; however, the dysregulation and implication of the cellular machinery controlling this process (spliceosome components and splicing factors) in hepatocellular carcinoma (HCC) is poorly known. This study aimed to comprehensively characterize the spliceosomal profile and explore its role in HCC. METHODS: Expression levels of 70 selected spliceosome components and splicing factors and clinical implications were evaluated in two retrospective and six in silico HCC cohorts. Functional, molecular and mechanistic studies were implemented in three cell lines (HepG2, Hep3B and SNU‐387) and preclinical Hep3B‐induced xenograft tumours. RESULTS: Spliceosomal dysregulations were consistently found in retrospective and in silico cohorts. EIF4A3, RBM3, ESRP2 and SRPK1 were the most dysregulated spliceosome elements in HCC. EIF4A3 expression was associated with decreased survival and greater recurrence. Plasma EIF4A3 levels were significantly elevated in HCC patients. In vitro EIF4A3‐silencing (or pharmacological inhibition) resulted in reduced aggressiveness, and hindered xenograft‐tumours growth in vivo, whereas EIF4A3 overexpression increased tumour aggressiveness. EIF4A3‐silencing altered the expression and splicing of key HCC‐related genes, specially FGFR4. EIF4A3‐silencing blocked the cellular response to the natural ligand of FGFR4, FGF19. Functional consequences of EIF4A3‐silencing were mediated by FGFR4 splicing as the restoration of non‐spliced FGFR4 full‐length version blunted these effects, and FGFR4 inhibition did not exert further effects in EIF4A3‐silenced cells. CONCLUSIONS: Splicing machinery is strongly dysregulated in HCC, providing a source of new diagnostic, prognostic and therapeutic options in HCC. EIF4A3 is consistently elevated in HCC patients and associated with tumour aggressiveness and mortality, through the modulation of FGFR4 splicing. John Wiley and Sons Inc. 2022-11-23 /pmc/articles/PMC9684617/ /pubmed/36419260 http://dx.doi.org/10.1002/ctm2.1102 Text en © 2022 The Authors. Clinical and Translational Medicine published by John Wiley & Sons Australia, Ltd on behalf of Shanghai Institute of Clinical Bioinformatics. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Articles
López‐Cánovas, Juan L.
Hermán‐Sánchez, Natalia
Moreno‐Montilla, Maria Trinidad
del Rio‐Moreno, Mercedes
Alors‐Perez, Emilia
Sánchez‐Frias, Marina E.
Amado, Víctor
Ciria, Rubén
Briceño, Javier
de la Mata, Manuel
Castaño, Justo P.
Rodriguez‐Perálvarez, Manuel
Luque, Raúl M.
Gahete, Manuel D.
Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing
title Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing
title_full Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing
title_fullStr Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing
title_full_unstemmed Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing
title_short Spliceosomal profiling identifies EIF4A3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of FGFR4 splicing
title_sort spliceosomal profiling identifies eif4a3 as a novel oncogene in hepatocellular carcinoma acting through the modulation of fgfr4 splicing
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9684617/
https://www.ncbi.nlm.nih.gov/pubmed/36419260
http://dx.doi.org/10.1002/ctm2.1102
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