Autor según el artículo: Martín A; Epifano C; Vilaplana-Marti B; Hernández I; Macías RIR; Martínez-Ramírez Á; Cerezo A; Cabezas-Sainz P; Garranzo-Asensio M; Amarilla-Quintana S; Gómez-Domínguez D; Caleiras E; Camps J; Gómez-López G; Gómez de Cedrón M; Ramírez de Molina A; Barderas R; Sánchez L; Velasco-Miguel S; Pérez de Castro I
Departamento: Medicina i Cirurgia
Autor/es de la URV: Camps Andreu, Jorge
Palabras clave: Translation Multidrug-resistance Methylome Metastasis Mechanisms Integration Gene-expression Chromosomal instability Autophagy Adaptation
Resumen: Despite being frequently observed in cancer cells, chromosomal instability (CIN) and its immediate consequence, aneuploidy, trigger adverse effects on cellular homeostasis that need to be overcome by anti-stress mechanisms. As such, these safeguard responses represent a tumor-specific Achilles heel, since CIN and aneuploidy are rarely observed in normal cells. Recent data have revealed that epitranscriptomic marks catalyzed by RNA-modifying enzymes change under various stress insults. However, whether aneuploidy is associated with such RNA modifying pathways remains to be determined. Through an in silico search for aneuploidy biomarkers in cancer cells, we found TRMT61B, a mitochondrial RNA methyltransferase enzyme, to be associated with high levels of aneuploidy. Accordingly, TRMT61B protein levels are increased in tumor cell lines with an imbalanced karyotype as well as in different tumor types when compared to control tissues. Interestingly, while TRMT61B depletion induces senescence in melanoma cell lines with low levels of aneuploidy, it leads to apoptosis in cells with high levels. The therapeutic potential of these results was further validated by targeting TRMT61B in transwell and xenografts assays. We show that TRM61B depletion reduces the expression of several mitochondrial encoded proteins and limits mitochondrial function. Taken together, these results identify a new biomarker of aneuploidy in cancer cells that could potentially be used to selectively target highly aneuploid tumors.
Áreas temáticas: Molecular biology Medicina ii Medicina i Ciências biológicas iii Ciências biológicas ii Ciências biológicas i Cell biology Biotecnología Biochemistry & molecular biology
Acceso a la licencia de uso: https://creativecommons.org/licenses/by/3.0/es/
Direcció de correo del autor: jorge.camps@urv.cat
Identificador del autor: 0000-0002-3165-3640
Fecha de alta del registro: 2024-08-03
Versión del articulo depositado: info:eu-repo/semantics/submittedVersion
Enlace a la fuente original: https://www.nature.com/articles/s41418-022-01044-6
URL Documento de licencia: https://repositori.urv.cat/ca/proteccio-de-dades/
Referencia al articulo segun fuente origial: Cell Death And Differentiation.
Referencia de l'ítem segons les normes APA: Martín A; Epifano C; Vilaplana-Marti B; Hernández I; Macías RIR; Martínez-Ramírez Á; Cerezo A; Cabezas-Sainz P; Garranzo-Asensio M; Amarilla-Quintana (2023). Mitochondrial RNA methyltransferase TRMT61B is a new, potential biomarker and therapeutic target for highly aneuploid cancers. Cell Death And Differentiation, (), -. DOI: 10.1038/s41418-022-01044-6
DOI del artículo: 10.1038/s41418-022-01044-6
Entidad: Universitat Rovira i Virgili
Año de publicación de la revista: 2023
Tipo de publicación: Journal Publications
Repositori URV