Identificador persistente para citar o vincular este elemento: http://hdl.handle.net/10553/42578
Título: Double strand break repair components are frequent targets of microsatellite instability in endometrial cancer
Autores/as: Bilbao, Cristina 
Ramírez, Raquel
Rodríguez, Germán
Falcón, Orlando
León, Laureano
Díaz-Chico, Nicolás 
Perucho, Manuel
Carlos Diaz-Chico, Juan 
Clasificación UNESCO: 320101 Oncología
Palabras clave: Endometrial cancer
Microsatellite instability
Fecha de publicación: 2010
Editor/a: 0959-8049
Publicación seriada: European Journal of Cancer 
Resumen: Aim: DNA double strand break (DSB) repair is a central cellular mechanism of the DNA damage response to maintain genomic stability. DSB components are frequently mutated in colorectal cancer with microsatellite instability (MSI). We investigated whether DSB repair is involved in endometrial cancer (EC) with MSI. Methods: Mononucleotide microsatellite tracts of 14 genes of the DSB repair system were analysed in a series of 41 EC with MSI. Among these genes, the microcephalin 1 (MCPH1/ BRIT1) has never been tested as target of MSI in tumour series. Results: The most frequently mutated gene was DNAPKcs (n = 14, 34%) followed by RAD50 (n = 7, 17%), MRE11, ATR and BRCA1 (n = 6, 15%), and by CtIP and MCPH1 (n = 5, 12%). While DSB biallelic mutations were infrequent, a high proportion of tumours (n = 30, 73%) presented mutations at some component of the DSB repair pathway, and almost half of them showed alterations at two or more components. Tumours with mutations in two or more genes were significantly associated with advanced grade (p = 0.03) and vascular invasion (p = 0.02) and marginally associated with advanced stage (p = 0.07). Conclusions: Our results suggest that in EC, the DSB repair is a relatively common mutational target of MSI and might contribute to tumour progression, and also that MCHP1 may be a novel target gene of MSI.
URI: http://hdl.handle.net/10553/42578
ISSN: 0959-8049
DOI: 10.1016/j.ejca.2010.06.116
Fuente: European Journal Of Cancer[ISSN 0959-8049],v. 46 (15), p. 2821-2827
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