TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer

In colorectal cancer (CRC), an inherited susceptibility risk affects about 35% of patients, whereas high-penetrance germline mutations account for <6% of cases. A considerable proportion of sporadic tumors could be explained by the coinheritance of multiple low-penetrance variants, some of which...

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Autores principales: Martinez-Canto, Ana, Castillejo, Adela, Mata-Balaguer, Trinidad, Castillejo, Maria-Isabel, Hernandez-Illan, Eva, Irles, Esperanza, Barbera, Victor Manuel, Egoavil, Cecilia, Guarinos, Carla, Alenda, Cristina, Ochoa, Enrique, Lazaro, Rafael, Fajardo, Silvia, Lacueva, Javier, Calpena, Rafael, Soto, Jose Luis
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3264637/
https://www.ncbi.nlm.nih.gov/pubmed/22292045
http://dx.doi.org/10.1371/journal.pone.0030812
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author Martinez-Canto, Ana
Castillejo, Adela
Mata-Balaguer, Trinidad
Castillejo, Maria-Isabel
Hernandez-Illan, Eva
Irles, Esperanza
Barbera, Victor Manuel
Egoavil, Cecilia
Guarinos, Carla
Alenda, Cristina
Ochoa, Enrique
Lazaro, Rafael
Fajardo, Silvia
Lacueva, Javier
Calpena, Rafael
Soto, Jose Luis
author_facet Martinez-Canto, Ana
Castillejo, Adela
Mata-Balaguer, Trinidad
Castillejo, Maria-Isabel
Hernandez-Illan, Eva
Irles, Esperanza
Barbera, Victor Manuel
Egoavil, Cecilia
Guarinos, Carla
Alenda, Cristina
Ochoa, Enrique
Lazaro, Rafael
Fajardo, Silvia
Lacueva, Javier
Calpena, Rafael
Soto, Jose Luis
author_sort Martinez-Canto, Ana
collection PubMed
description In colorectal cancer (CRC), an inherited susceptibility risk affects about 35% of patients, whereas high-penetrance germline mutations account for <6% of cases. A considerable proportion of sporadic tumors could be explained by the coinheritance of multiple low-penetrance variants, some of which are common. We assessed the susceptibility to CRC conferred by genetic variants at the TGFBR1 locus. We analyzed 14 polymorphisms and the allele-specific expression (ASE) of TGFBR1 in 1025 individuals from the Spanish population. A case-control study was undertaken with 504 controls and 521 patients with sporadic CRC. Fourteen polymorphisms located at the TGFBR1 locus were genotyped with the iPLEX Gold (MassARRAY-Sequenom) technology. Descriptive analyses of the polymorphisms and haplotypes and association studies were performed with the SNPator workpackage. No relevant associations were detected between individual polymorphisms or haplotypes and the risk of CRC. The TGFBR1*9A/6A polymorphism was used for the ASE analysis. Heterozygous individuals were analyzed for ASE by fragment analysis using cDNA from normal tissue. The relative level of allelic expression was extrapolated from a standard curve. The cutoff value was calculated with Youden's index. ASE was found in 25.4% of patients and 16.4% of controls. Considering both bimodal and continuous types of distribution, no significant differences between the ASE values of patients and controls were identified. Interestingly, a combined analysis of the polymorphisms and ASE for the association with CRC occurrence revealed that ASE-positive individuals carrying one of the most common haplotypes (H2: 20.7%) showed remarkable susceptibility to CRC (RR: 5.25; 95% CI: 2.547–5.250; p<0.001) with a synergy factor of 3.7. In our study, 54.1% of sporadic CRC cases were attributable to the coinheritance of the H2 haplotype and TGFBR1 ASE. These results support the hypothesis that the allelic architecture of cancer genes, rather than individual polymorphisms, more accurately defines the CRC risk.
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spelling pubmed-32646372012-01-30 TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer Martinez-Canto, Ana Castillejo, Adela Mata-Balaguer, Trinidad Castillejo, Maria-Isabel Hernandez-Illan, Eva Irles, Esperanza Barbera, Victor Manuel Egoavil, Cecilia Guarinos, Carla Alenda, Cristina Ochoa, Enrique Lazaro, Rafael Fajardo, Silvia Lacueva, Javier Calpena, Rafael Soto, Jose Luis PLoS One Research Article In colorectal cancer (CRC), an inherited susceptibility risk affects about 35% of patients, whereas high-penetrance germline mutations account for <6% of cases. A considerable proportion of sporadic tumors could be explained by the coinheritance of multiple low-penetrance variants, some of which are common. We assessed the susceptibility to CRC conferred by genetic variants at the TGFBR1 locus. We analyzed 14 polymorphisms and the allele-specific expression (ASE) of TGFBR1 in 1025 individuals from the Spanish population. A case-control study was undertaken with 504 controls and 521 patients with sporadic CRC. Fourteen polymorphisms located at the TGFBR1 locus were genotyped with the iPLEX Gold (MassARRAY-Sequenom) technology. Descriptive analyses of the polymorphisms and haplotypes and association studies were performed with the SNPator workpackage. No relevant associations were detected between individual polymorphisms or haplotypes and the risk of CRC. The TGFBR1*9A/6A polymorphism was used for the ASE analysis. Heterozygous individuals were analyzed for ASE by fragment analysis using cDNA from normal tissue. The relative level of allelic expression was extrapolated from a standard curve. The cutoff value was calculated with Youden's index. ASE was found in 25.4% of patients and 16.4% of controls. Considering both bimodal and continuous types of distribution, no significant differences between the ASE values of patients and controls were identified. Interestingly, a combined analysis of the polymorphisms and ASE for the association with CRC occurrence revealed that ASE-positive individuals carrying one of the most common haplotypes (H2: 20.7%) showed remarkable susceptibility to CRC (RR: 5.25; 95% CI: 2.547–5.250; p<0.001) with a synergy factor of 3.7. In our study, 54.1% of sporadic CRC cases were attributable to the coinheritance of the H2 haplotype and TGFBR1 ASE. These results support the hypothesis that the allelic architecture of cancer genes, rather than individual polymorphisms, more accurately defines the CRC risk. Public Library of Science 2012-01-23 /pmc/articles/PMC3264637/ /pubmed/22292045 http://dx.doi.org/10.1371/journal.pone.0030812 Text en Martinez-Canto et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Martinez-Canto, Ana
Castillejo, Adela
Mata-Balaguer, Trinidad
Castillejo, Maria-Isabel
Hernandez-Illan, Eva
Irles, Esperanza
Barbera, Victor Manuel
Egoavil, Cecilia
Guarinos, Carla
Alenda, Cristina
Ochoa, Enrique
Lazaro, Rafael
Fajardo, Silvia
Lacueva, Javier
Calpena, Rafael
Soto, Jose Luis
TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer
title TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer
title_full TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer
title_fullStr TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer
title_full_unstemmed TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer
title_short TGFBR1 Intralocus Epistatic Interaction as a Risk Factor for Colorectal Cancer
title_sort tgfbr1 intralocus epistatic interaction as a risk factor for colorectal cancer
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3264637/
https://www.ncbi.nlm.nih.gov/pubmed/22292045
http://dx.doi.org/10.1371/journal.pone.0030812
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