Quantitative analysis of somatically acquired and constitutive uniparental disomy in gastrointestinal cancers

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RECERCAT Home > Universitat Autònoma de Barcelona > Articles escrits per personal UAB o publicats per la universitat > View document

Title:	Quantitative analysis of somatically acquired and constitutive uniparental disomy in gastrointestinal cancers
Author:	Torabi Asensio, Keyvan; Erola, Pau.; Alvarez Mora, María Isabel; Díaz-Gay, Marcos; Ferrer Menduiña, Queralt; Castells, Antoni; Castellví-Bel, Sergi; Milà, Montserrat; Lozano, Juan José; Miró, Rosa; Ried, Thomas; Ponsa Arjona, Immaculada; Camps, Jordi
Abstract:	Altres ajuts: GCB13131592CAST de la Fundación Cientíﬁca de la Asociación Española Contra el Cáncer; PERIS (SLT002/16/00398, Generalitat de Catalunya)
Abstract:	Somatically acquired uniparental disomies (aUPDs) are frequent events in solid tumors and have been associated with cancer-related genes. Studies assessing their functional consequences across several cancer types are therefore necessary. Here, we aimed at integrating aUPD profiles with the mutational status of cancer-related genes in a tumor-type specific manner. Using TCGA datasets for 1,032 gastrointestinal cancers, including colon (COAD), rectum (READ), stomach (STAD), esophageal adenocarcinoma (EAC) and esophageal squamous cell carcinoma (ESCC), we show a non-random distribution of aUPD, suggesting the existence of a cancer-specific landscape of aUPD events. Our analysis indicates that aUPD acts as a "second hit" in Knudson's model in order to achieve biallelic inactivation of tumor suppressor genes. In particular, APC , ARID1A and NOTCH1 were recurrently inactivated by the presence of homozygous mutation as a consequence of aUPD in COAD and READ, STAD and ESCC, respectively. Furthermore, while TP53 showed inactivation caused by aUPD at chromosome arm 17p across all tumor types, copy number losses at this genomic position were also frequent. By experimental and computationally inferring genome ploidy, we demonstrate that an increased number of aUPD events, both affecting the whole chromosome or segments of it, were present in highly aneuploid genomes compared to near-diploid tumors. Finally, the presence of mosaic UPD was detected at a higher frequency in DNA extracted from peripheral blood lymphocytes of patients with colorectal cancer compared to healthy individuals. In summary, our study defines specific profiles of aUPD in gastrointestinal cancers and provides unequivocal evidence of their relevance in cancer
Subject(s):	-Uniparental disomy -Copy-number alterations -Gastrointestinal cancers -Single nucleotide variants -Ploidy -Mosaicism
Rights:	open access Aquest document està subjecte a una llicència d'ús Creative Commons. Es permet la reproducció total o parcial, la distribució, la comunicació pública de l'obra i la creació d'obres derivades, sempre que no sigui amb finalitats comercials, i sempre que es reconegui l'autoria de l'obra original. https://creativecommons.org/licenses/by-nc/3.0/
Document type:	Article
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Uri:	https://ddd.uab.cat/record/223512

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