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    Título
    Telomere Length as a New Risk Marker of Early-Onset Colorectal Cancer
    Autor(es)
    Martel Martel, Abel Jesús
    Corchete Sánchez, Luis Antonio
    Martí, Marc
    Vidal Tocino, María del Rosario
    Hurtado, Elena
    Álvaro, Edurne
    Jiménez, Fernando
    Jiménez-Toscano, Marta
    Balaguer, Francesc
    Sanz, Gonzalo
    López, Irene
    Hernández-Villafranca, Sergio
    Ballestero, Araceli
    Vivas, Alfredo
    Melone, Sirio
    Pastor, Carlos
    Brandáriz, Lorena
    Gómez Marcos, Manuel ÁngelAutoridad USAL
    Cruz Hernández, Juan JesúsAutoridad USAL
    Perea García, José
    González Sarmiento, RogelioAutoridad USAL
    Palabras clave
    Early onset colorectal cancer
    EOCRC
    Telomere
    Fecha de publicación
    2023-02-09
    Editor
    Martel-Martel, A., Corchete, L. A., Martí, M., Vidal-Tocino, R., Hurtado, E., Álvaro, E., Jiménez, F., Jiménez-Toscano, M., Balaguer, F., Sanz, G., López, I., Hernández-Villafranca, S., Ballestero, A., Vivas, A., Melone, S., Pastor, C., Brandáriz, L., Gómez-Marcos, M. A., Cruz-Hernández, J. J., et al. (2023). Telomere Length as a New Risk Marker of Early-Onset Colorectal Cancer. International Journal of Molecular Sciences, 24(4). https://doi.org/10.3390/IJMS24043526
    Resumen
    [EN]Early-onset colorectal cancer (EOCRC; age younger than 50 years) incidence has been steadily increasing in recent decades worldwide. The need for new biomarkers for EOCRC prevention strategies is undeniable. In this study, we aimed to explore whether an aging factor, such as telomere length (TL), could be a useful tool in EOCRC screening. The absolute leukocyte TL from 87 microsatellite stable EOCRC patients and 109 healthy controls (HC) with the same range of age, was quantified by Real Time Quantitative PCR (RT-qPCR). Then, leukocyte whole-exome sequencing (WES) was performed to study the status of the genes involved in TL maintenance (hTERT, TERC, DKC1, TERF1, TERF2, TERF2IP, TINF2, ACD, and POT1) in 70 sporadic EOCRC cases from the original cohort. We observed that TL was significantly shorter in EOCRC patients than in healthy individuals (EOCRC mean: 122 kb vs. HC mean: 296 kb; p < 0.001), suggesting that telomeric shortening could be associated with EOCRC susceptibility. In addition, we found a significant association between several SNPs of hTERT (rs79662648), POT1 (rs76436625, rs10263573, rs3815221, rs7794637, rs7784168, rs4383910, and rs7782354), TERF2 (rs251796 and rs344152214), and TERF2IP (rs7205764) genes and the risk of developing EOCRC. We consider that the measurement of germline TL and the status analysis of telomere maintenance related genes polymorphisms at early ages could be non-invasive methods that could facilitate the early identification of individuals at risk of developing EOCRC.
    URI
    http://hdl.handle.net/10366/164475
    DOI
    10.3390/ijms24043526
    Versión del editor
    https://www.mdpi.com/1422-0067/24/4/3526
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