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    Por favor, use este identificador para citar o enlazar este ítem:https://uvadoc.uva.es/handle/10324/75142

    Título
    Genomics review of selective RET inhibitors sensitivity in thyroid cancer clinical trials
    Autor
    Gil Bernabé, SaraAutoridad UVA Orcid
    García de la Fuente, Lucía
    García Álvarez, Alejandro
    García-Rostán y Pérez, Ginesa MaríaAutoridad UVA Orcid
    Capdevilla, Jaume
    Hernando, Jorge
    Año del Documento
    2025
    Editorial
    Wiley
    Descripción
    Producción Científica
    Documento Fuente
    American Journal of Medical Genetics Part C:Seminars in Medical Genetics, [Early view]
    Resumen
    RET gene is a driver of thyroid cancer (TC) tumorigenesis. The incidence of TC has increased worldwide in the last few decades, both in medullary and follicular-derived subtypes. Several drugs, including multikinase and selective inhibitors, have been explored. Selpercatinib and pralsetinib are selective RET inhibitors that have shown clear clinical benefits for patients in the LIBRETTO and ARROW trials, respectively. Currently, their development and application in clinical practice are ongoing. However, its efficacy in different RET pathogenic variants has not yet been well established. Although selpercatinib and pralsetinib achieved a high ORR, no data are available regarding the differences in tumor responses of both TC groups according to RET pathogenic variants. Clinical trials and literature have analyzed the efficacy of selective RET inhibitors with a special interest in the most common variants. A review of LIBRETTO and ARROW trials was made regarding the change in tumor size depending on the pathogenic variants. M918T pathogenic variant resulted in a higher complete response rate. Patients who underwent fusion had the highest ORR (objective response rate). MKi-treated patients did not exhibit significant differences from untreated patients. Different RET pathogenic variants are not biomarkers of RETi response in TC. Selpercatinib showed a tendency to achieve a complete response. All patients with RET pathogenic variants should receive treatment with selpercatinib or pralsetinib at any moment of the therapeutic schedule owing to off-target inhibition and toxicity. Therefore, new targets for drug sensitivity and resistance should be explored.
    Materias Unesco
    32 Ciencias Médicas
    Palabras Clave
    medullary thyroid cancer
    oncogenes
    papillary thyroid cancer
    Pralsetinib
    Selpercatinib
    targeted therapy
    ISSN
    1552-4868
    Revisión por pares
    SI
    DOI
    10.1002/ajmg.c.32127
    Version del Editor
    https://onlinelibrary.wiley.com/doi/10.1002/ajmg.c.32127
    Propietario de los Derechos
    © 2025 The Author(s)
    Idioma
    eng
    URI
    https://uvadoc.uva.es/handle/10324/75142
    Tipo de versión
    info:eu-repo/semantics/publishedVersion
    Derechos
    openAccess
    Aparece en las colecciones
    • DEP03 - Artículos de revista [102]
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    Attribution-NonCommercial-NoDerivatives 4.0 InternacionalLa licencia del ítem se describe como Attribution-NonCommercial-NoDerivatives 4.0 Internacional

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