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Si us plau utilitzeu sempre aquest identificador per citar o enllaçar aquest document: https://hdl.handle.net/2445/224858
Gene-Specific Detection Rate of Adenomas and Advanced Adenomas in Lynch Syndrome
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Background & Aims
Colonoscopy is expected to reduce colorectal cancer (CRC) incidence in Lynch syndrome (LS) by detecting and removing adenomas. The existence of gene-specific differences in adenoma detection has been proposed yet remains insufficiently explored. This study aims to elucidate gene-specific adenoma detection rates and their association with post-colonoscopy CRC (PCCRC), which stands as an important issue in LS surveillance.
Methods
In this multicenter study, we analyzed 1072 LS carriers without prior CRC undergoing surveillance colonoscopy, evaluating adenoma and advanced adenoma (AA) detection rates by gene. The primary outcome was to compare adenoma detection rates in individuals without prior CRC carrying pathogenic variants in MLH1/MSH2 vs MSH6/PMS2. Subgroup analysis was performed to assess the intermediate risk profile in MSH6 carriers relative to MLH1/MSH2 and PMS2 carriers. We compared overall adenoma detection rates, adenoma burden, age at first adenoma occurrence, and 10-year cumulative detection rates. Risk factors for AA and PCCRC were also identified. Multiple testing and multivariate analyses were performed.
Results
The adenoma detection rates were similar across the 4 genes. However, MLH1/MSH2 carriers had a higher overall AA detection rate compared with MSH6/PMS2 carriers (14.5% vs 11.9%; P = .04) and showed higher cumulative AA detection rates over 10 years (21.6% vs 19.7%; P = .04). Subgroup analysis indicated that MSH6 carriers had an intermediate AA detection rate positioned between MLH1/MSH2 carriers and PMS2 carriers. Multivariate analysis indicated that AAs (odds ratio, 2.12; 95% confidence interval, 1.08–4.17; P=.03) and repeated AA detection (odds ratio, 4.62; 95% confidence interval, 1.70–12.57; P < .01) were independent risk factors for PCCRC.
Conclusions
Carriers of MLH1/MSH2 pathogenic variants are at a higher risk of developing AAs compared with those with MSH6/PMS2 mutations, with MSH6 carriers exhibiting an intermediate risk profile. AAs are an independent risk factor for PCCRC. LS patients with AAs should be identified as high risk and undergo enhanced colonoscopy surveillance.
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SÁNCHEZ BRUALLA, Alicia, CASTILLO ITURRA, Joaquín, BALMAÑA, Judith, BRUNET, Joan, CASTELLS SÁNCHEZ, Alba, CAPELLÁ, G. (gabriel), LADABAUM, Uri, DEKKER, Evelien, MOREIRA, Luciana, PELLISÉ, M., BALAGUER PRUNÉS, Francesc, LÓPEZ FERNÁNDEZ, Adrià, SALCES, Inmaculada, PICÓ, María dolores, RIVAS, Laura, BUJANDA, Luis, GARZON, Marta, PIZARRO, Angeles, MARTINEZ DE CASTRO, Eva, ROOS, V.h., DUEÑAS, Nuria, PINEDA RIU, Marta, MORENO CALLE, Lorena, RODRÍGUEZ ALONSO, Lorena, RAMON Y CAJAL, Teresa, LLORT, Gemma, PIÑOL, Virginia, LÓPEZ ARIAS, María .jesús, POVES, Carmen, GARAU, Catalina, RODRÍGUEZ ALCALDE, Daniel, HERRAIZ, Maite, ÁLVAREZ URRUTIA, Cristina, DACAL, Andrés, CARRILLO PALAU, Marta, CID, Lucía, PONCE, Marta, BARREIRO ALONSO, Eva, SAPERAS, Esteban, AGUIRRE, Elena, BASTIAANSEN, B., OCAÑA, Teresa, CARBALLAL, Sabela, RIVERO SÁNCHEZ, Liseth, ORTIZ, Oswaldo, DACA ÁLVAREZ, María, PRAT GALITO, Ricard, BESSA, Xavier, CUBIELLA, Joaquin, JOVER, Rodrigo, RODRÍGUEZ MORANTA, Francisco. Gene-Specific Detection Rate of Adenomas and Advanced Adenomas in Lynch Syndrome. _Gastroenterology_. 2025. Vol. 169, núm. 4, pàgs. 663-675. [consulta: 9 de gener de 2026]. ISSN: 0016-5085. [Disponible a: https://hdl.handle.net/2445/224858]