Search

Your search keyword '"Ruiz-Ponte, Clara"' showing total 371 results
Start Over Author "Ruiz-Ponte, Clara"
371 results on '"Ruiz-Ponte, Clara"'

102. A Colorectal Cancer Susceptibility New Variant at 4q26 in the Spanish Population Identified by Genome-Wide Association Analysis

Author

Real, Luis M., primary, Ruiz, Agustín, additional, Gayán, Javier, additional, González-Pérez, Antonio, additional, Sáez, María E., additional, Ramírez-Lorca, Reposo, additional, Morón, Francisco J., additional, Velasco, Juan, additional, Marginet-Flinch, Ruth, additional, Musulén, Eva, additional, Carrasco, José M., additional, Moreno-Rey, Concha, additional, Vázquez, Enrique, additional, Chaves-Conde, Manuel, additional, Moreno-Nogueira, Jose A., additional, Hidalgo-Pascual, Manuel, additional, Ferrero-Herrero, Eduardo, additional, Castellví-Bel, Sergi, additional, Castells, Antoni, additional, Fernandez-Rozadilla, Ceres, additional, Ruiz-Ponte, Clara, additional, Carracedo, Angel, additional, González, Beatriz, additional, Alonso, Sergio, additional, and Perucho, Manuel, additional

Published
2014
Full Text
View/download PDF

104. A candidate gene study of capecitabine-related toxicity in colorectal cancer identifies new toxicity variants atDPYDand a putative role forENOSF1rather thanTYMS

Author

Rosmarin, Dan, primary, Palles, Claire, additional, Pagnamenta, Alistair, additional, Kaur, Kulvinder, additional, Pita, Guillermo, additional, Martin, Miguel, additional, Domingo, Enric, additional, Jones, Angela, additional, Howarth, Kimberley, additional, Freeman-Mills, Luke, additional, Johnstone, Elaine, additional, Wang, Haitao, additional, Love, Sharon, additional, Scudder, Claire, additional, Julier, Patrick, additional, Fernández-Rozadilla, Ceres, additional, Ruiz-Ponte, Clara, additional, Carracedo, Angel, additional, Castellvi-Bel, Sergi, additional, Castells, Antoni, additional, Gonzalez-Neira, Anna, additional, Taylor, Jenny, additional, Kerr, Rachel, additional, Kerr, David, additional, and Tomlinson, Ian, additional

Published
2014
Full Text
View/download PDF

105. Cumulative impact of 10 common genetic variants on colorectal cancer risk in 42,333 individuals from eight populations

Author

Dunlop, Malcolm G, Tenesa, Albert, Farrington, Susan M, Ballereau, Stephane, Brewster, David H, Koessler, Thibaud, Pharoah, Paul, Schafmayer, Clemens, Hampe, Jochen, Voelzke, Henry, Chang-Claude, Jenny, Hoffmeister, Michael, Brenner, Hermann, von Holst, Susanna, Picelli, Simone, Lindblom, Annika, Jenkins, Mark A, Hopper, John L, Casey, Graham, Duggan, David J, Newcomb, Polly A, Abuli, Anna, Bessa, Xavier, Ruiz-Ponte, Clara, Castellvi-Bel, Sergi, Niittymaeki, Iina, Tuupanen, Sari, Karhu, Auli, Aaltonen, Lauri A, Zanke, Brent, Hudson, Tom, Gallinger, Steven, Barclay, Ella, Martin, Lynn, Gorman, Maggie, Carvajal-Carmona, Luis G, Walther, Axel, Kerr, David J, Lubbe, Steven, Broderick, Peter, Chandler, Ian, Pittman, Alan, Penegar, Steven, Campbell, Harry, Tomlinson, Ian, Houlston, Richard S, Dunlop, Malcolm G, Tenesa, Albert, Farrington, Susan M, Ballereau, Stephane, Brewster, David H, Koessler, Thibaud, Pharoah, Paul, Schafmayer, Clemens, Hampe, Jochen, Voelzke, Henry, Chang-Claude, Jenny, Hoffmeister, Michael, Brenner, Hermann, von Holst, Susanna, Picelli, Simone, Lindblom, Annika, Jenkins, Mark A, Hopper, John L, Casey, Graham, Duggan, David J, Newcomb, Polly A, Abuli, Anna, Bessa, Xavier, Ruiz-Ponte, Clara, Castellvi-Bel, Sergi, Niittymaeki, Iina, Tuupanen, Sari, Karhu, Auli, Aaltonen, Lauri A, Zanke, Brent, Hudson, Tom, Gallinger, Steven, Barclay, Ella, Martin, Lynn, Gorman, Maggie, Carvajal-Carmona, Luis G, Walther, Axel, Kerr, David J, Lubbe, Steven, Broderick, Peter, Chandler, Ian, Pittman, Alan, Penegar, Steven, Campbell, Harry, Tomlinson, Ian, and Houlston, Richard S

Abstract

OBJECTIVE: Colorectal cancer (CRC) has a substantial heritable component. Common genetic variation has been shown to contribute to CRC risk. A study was conducted in a large multi-population study to assess the feasibility of CRC risk prediction using common genetic variant data combined with other risk factors. A risk prediction model was built and applied to the Scottish population using available data. DESIGN: Nine populations of European descent were studied to develop and validate CRC risk prediction models. Binary logistic regression was used to assess the combined effect of age, gender, family history (FH) and genotypes at 10 susceptibility loci that individually only modestly influence CRC risk. Risk models were generated from case-control data incorporating genotypes alone (n=39 266) and in combination with gender, age and FH (n=11 324). Model discriminatory performance was assessed using 10-fold internal cross-validation and externally using 4187 independent samples. The 10-year absolute risk was estimated by modelling genotype and FH with age- and gender-specific population risks. RESULTS: The median number of risk alleles was greater in cases than controls (10 vs 9, p<2.2×10(-16)), confirmed in external validation sets (Sweden p=1.2×10(-6), Finland p=2×10(-5)). The mean per-allele increase in risk was 9% (OR 1.09; 95% CI 1.05 to 1.13). Discriminative performance was poor across the risk spectrum (area under curve for genotypes alone 0.57; area under curve for genotype/age/gender/FH 0.59). However, modelling genotype data, FH, age and gender with Scottish population data shows the practicalities of identifying a subgroup with >5% predicted 10-year absolute risk. CONCLUSION: Genotype data provide additional information that complements age, gender and FH as risk factors, but individualised genetic risk prediction is not currently feasible. Nonetheless, the modelling exercise suggests public health potential since it is possible to stratify the population i

Published
2013

106. A colorectal cancer genome-wide association study in a Spanish cohort identifies two variants associated with colorectal cancer risk at 1p33 and 8p12

Author

Medicina, Medikuntza, Fernández Rozadilla, Ceres, Cazier, Jean-Baptiste, Tomlinson, Ian P., Carvajal Carmona, Luis G., Palles, Claire, Lamas, María J., Baiget, Montserrat, López Fernández, Luis A., Brea Fernández, Alejandro, Abulí, Anna, Bujanda Fernández de Pierola, Luis, Clofent, Juan, González, Dolors, Xicola, Rosa, Andreu, Montserrat, Bessa, Xavier, Jover, Rodrigo, Llor, Xavier, Moreno, Víctor, Castells, Antoni, Carracedo, Angel, Castellví-Bel, Sergi, Ruiz Ponte, Clara, EPICOLON Consortium, Medicina, Medikuntza, Fernández Rozadilla, Ceres, Cazier, Jean-Baptiste, Tomlinson, Ian P., Carvajal Carmona, Luis G., Palles, Claire, Lamas, María J., Baiget, Montserrat, López Fernández, Luis A., Brea Fernández, Alejandro, Abulí, Anna, Bujanda Fernández de Pierola, Luis, Clofent, Juan, González, Dolors, Xicola, Rosa, Andreu, Montserrat, Bessa, Xavier, Jover, Rodrigo, Llor, Xavier, Moreno, Víctor, Castells, Antoni, Carracedo, Angel, Castellví-Bel, Sergi, Ruiz Ponte, Clara, and EPICOLON Consortium

Abstract

Background: Colorectal cancer (CRC) is a disease of complex aetiology, with much of the expected inherited risk being due to several common low risk variants. Genome-Wide Association Studies (GWAS) have identified 20 CRC risk variants. Nevertheless, these have only been able to explain part of the missing heritability. Moreover, these signals have only been inspected in populations of Northern European origin. Results: Thus, we followed the same approach in a Spanish cohort of 881 cases and 667 controls. Sixty-four variants at 24 loci were found to be associated with CRC at p-values <10-5. We therefore evaluated the 24 loci in another Spanish replication cohort (1481 cases and 1850 controls). Two of these SNPs, rs12080929 at 1p33 (P-replication=0.042; P-pooled=5.523x10(-03); OR (CI95%)=0.866(0.782-0.959)) and rs11987193 at 8p12 (P-replication=0.039; P-pooled=6.985x10(-5); OR (CI95%)=0.786(0.705-0.878)) were replicated in the second Phase, although they did not reach genome-wide statistical significance. Conclusions: We have performed the first CRC GWAS in a Southern European population and by these means we were able to identify two new susceptibility variants at 1p33 and 8p12 loci. These two SNPs are located near the SLC5A9 and DUSP4 loci, respectively, which could be good functional candidates for the association signals. We therefore believe that these two markers constitute good candidates for CRC susceptibility loci and should be further evaluated in other larger datasets. Moreover, we highlight that were these two SNPs true susceptibility variants, they would constitute a decrease in the CRC missing heritability fraction.

Published
2013

107. Risk of Cancer in Cases of Suspected Lynch Syndrome Without Germline Mutation

Author

Universidad de Alicante. Departamento de Biotecnología, Rodríguez-Soler, María, Pérez-Carbonell, Lucía, Guarinos, Carla, Zapater, Pedro, Castillejo, Adela, Barberá, Víctor Manuel, Juárez, Miriam, Bessa, Xavier, Xicola, Rosa M., Clofent, Juan, Bujanda, Luis, Balaguer, Francesc, Reñé, Josep-Maria, Castro, Luisa de, Marín-Gabriel, José C., Lanas, Ángel, Cubiella, Joaquín, Nicolás-Pérez, David, Brea-Fernández, Alejandro, Castellví-Bel, Sergi, Alenda, Cristina, Ruiz-Ponte, Clara, Carracedo, Ángel, Castells, Antoni, Andreu, Montserrat, Llor, Xavier, Soto, José Luis, Payá, Artemio, Universidad de Alicante. Departamento de Biotecnología, Rodríguez-Soler, María, Pérez-Carbonell, Lucía, Guarinos, Carla, Zapater, Pedro, Castillejo, Adela, Barberá, Víctor Manuel, Juárez, Miriam, Bessa, Xavier, Xicola, Rosa M., Clofent, Juan, Bujanda, Luis, Balaguer, Francesc, Reñé, Josep-Maria, Castro, Luisa de, Marín-Gabriel, José C., Lanas, Ángel, Cubiella, Joaquín, Nicolás-Pérez, David, Brea-Fernández, Alejandro, Castellví-Bel, Sergi, Alenda, Cristina, Ruiz-Ponte, Clara, Carracedo, Ángel, Castells, Antoni, Andreu, Montserrat, Llor, Xavier, Soto, José Luis, and Payá, Artemio

Abstract

Background & Aims: Colorectal cancers (CRCs) with microsatellite instability (MSI) and a mismatch repair (MMR) immunohistochemical deficit without hypermethylation of the MLH1 promoter are likely to be caused by Lynch syndrome. Some patients with these cancers have not been found to have pathogenic germline mutations and are considered to have Lynch-like syndrome (LLS). The aim of this study was to determine the risk of cancer in families of patients with LLS. Methods: We studied a population-based cohort of 1705 consecutive patients, performing MSI tests and immunohistochemical analyses of MMR proteins. Patients were diagnosed with Lynch syndrome when they were found to have pathogenic germline mutations. Patients with MSI and loss of MSH2 and/or MSH6 expression, isolated loss of PMS2 or loss of MLH1 without MLH1 promoter hypermethylation, and no pathogenic mutation were considered to have LLS. The clinical characteristics of patients and the age- and sex-adjusted standardized incidence ratios (SIRs) of cancer in families were compared between groups. Results: The incidence of CRC was significantly lower in families of patients with LLS than in families with confirmed cases of Lynch syndrome (SIR for Lynch syndrome, 6.04; 95% confidence interval [CI], 3.58–9.54; SIR for LLS, 2.12; 95% CI, 1.16–3.56; P < .001). However, the incidence of CRC was higher in families of patients with LLS than in families with sporadic CRC (SIR for sporadic CRC, 0.48; 95% CI, 0.27–0.79; P < .001). Conclusions: The risk of cancer in families with LLS is lower that of families with Lynch syndrome but higher than that of families with sporadic CRC. These results confirm the need for special screening and surveillance strategies for these patients and their relatives.

Published
2013

108. Genomics and pharmacogenomics of colorectal cancer

Author

Carracedo Álvarez, Ángel, Ruiz Ponte, Clara M., Universidade de Santiago de Compostela. Facultade de Medicina e Odontoloxía, Universidade de Santiago de Compostela. Departamento de Anatomía Patolóxica e Ciencias Forenses, Fernández Rozadilla, Ceres, Carracedo Álvarez, Ángel, Ruiz Ponte, Clara M., Universidade de Santiago de Compostela. Facultade de Medicina e Odontoloxía, Universidade de Santiago de Compostela. Departamento de Anatomía Patolóxica e Ciencias Forenses, and Fernández Rozadilla, Ceres

Abstract

Se ha estimado que la heredabilidad asociada al cáncer colorrectal (CCR) es de alrededor de un 35%. A pesar de que cerca de un 5% de esta proporción es explicable a través de mutaciones raras de alta penetrancia, y un 7% adicional es debido a la presencia de combinaciones de algunos de los 16 loci de susceptibilidad descritos, existe aún una fracción de esta susceptibilidad genética que no ha podido ser explicada. Por otro lado, existe también una importante variabilidad en la forma en la que los pacientes de CCR responden al tratamiento con quimioterapia. Además, el hecho de que la mayoría de fármacos usados en quimioterapia presentan rangos terapéuticos restringidos resulta en la frecuente aparición de reacciones adversas a fármacos (ADRs). Por ello, la identificación de la variación genética que modula esta respuesta es indispensable a la hora de ofrecer tratamientos personalizados que sean más efectivos, produzcan menos efectos secundarios y se optimicen los costes sanitarios. En este contexto, el trabajo presentado en esta Tesis Doctoral ha tenido dos objetivos principales: en primer lugar, la búsqueda de nuevas variantes de susceptibilidad al CCR. En segundo, el análisis de la variación genética subyacente a las diferencias en las respuestas tóxicas de pacientes de CCR tratados con quimioterapia.

Published
2012

110. Evidence for classification of c.1852_1853AA > GC in MLH1 as a neutral variant for Lynch syndrome

Author

Medicina, Medikuntza, Castillejo, Adela, Guarinos, Carla, Martínez Canto, Ana, Barberá, Víctor Manuel, Egoavil, Cecilia, Castillejo, María Isabel, Pérez Carbonell, Lucía, Sánchez Heras, Ana Beatriz, Segura, Angel, Ochoa, Enrique, Lázaro, Rafael, Ruiz Ponte, Clara, Bujanda Fernández de Pierola, Luis, Andreu, Montserrat, Castells, Antoni, Carracedo, Angel, Llor, Xavier, Clofent, Juan, Alenda, Cristina, Paya, Artemio, Jover, Rodrigo, Soto, José Luis, Medicina, Medikuntza, Castillejo, Adela, Guarinos, Carla, Martínez Canto, Ana, Barberá, Víctor Manuel, Egoavil, Cecilia, Castillejo, María Isabel, Pérez Carbonell, Lucía, Sánchez Heras, Ana Beatriz, Segura, Angel, Ochoa, Enrique, Lázaro, Rafael, Ruiz Ponte, Clara, Bujanda Fernández de Pierola, Luis, Andreu, Montserrat, Castells, Antoni, Carracedo, Angel, Llor, Xavier, Clofent, Juan, Alenda, Cristina, Paya, Artemio, Jover, Rodrigo, and Soto, José Luis

Abstract

Background: Lynch syndrome (LS) is an autosomal dominant inherited cancer syndrome characterized by early onset cancers of the colorectum, endometrium and other tumours. A significant proportion of DNA variants in LS patients are unclassified. Reports on the pathogenicity of the c.1852_1853AA>GC (p.Lys618Ala) variant of the MLH1 gene are conflicting. In this study, we provide new evidence indicating that this variant has no significant implications for LS. Methods: The following approach was used to assess the clinical significance of the p.Lys618Ala variant: frequency in a control population, case-control comparison, co-occurrence of the p.Lys618Ala variant with a pathogenic mutation, co-segregation with the disease and microsatellite instability in tumours from carriers of the variant. We genotyped p.Lys618Ala in 1034 individuals (373 sporadic colorectal cancer [CRC] patients, 250 index subjects from families suspected of having LS [revised Bethesda guidelines] and 411 controls). Three well-characterized LS families that fulfilled the Amsterdam II Criteria and consisted of members with the p.Lys618Ala variant were included to assess co-occurrence and co-segregation. A subset of colorectal tumour DNA samples from 17 patients carrying the p.Lys618Ala variant was screened for microsatellite instability using five mononucleotide markers. Results: Twenty-seven individuals were heterozygous for the p.Lys618Ala variant; nine had sporadic CRC (2.41%), seven were suspected of having hereditary CRC (2.8%) and 11 were controls (2.68%). There were no significant associations in the case-control and case-case studies. The p.Lys618Ala variant was co-existent with pathogenic mutations in two unrelated LS families. In one family, the allele distribution of the pathogenic and unclassified variant was in trans, in the other family the pathogenic variant was detected in the MSH6 gene and only the deleterious variant co-segregated with the disease in both families. Only two positive

Published
2011

111. Comparison between universal molecular screening for Lynch syndrome and revised Bethesda guidelines in a large population-based cohort of patients with colorectal cancer

Author

Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, Pérez-Carbonell, Lucía, Ruiz-Ponte, Clara, Guarinos, Carla, Alenda, Cristina, Payá, Artemio, Brea-Fernández, Alejandro, Egoavil, Cecilia, Castillejo, Adela, Barberá, Víctor Manuel, Bessa, Xavier, Xicola, Rosa M., Rodríguez-Soler, María, Sánchez-Fortún, Cristina, Acame, Nuria, Castellví-Bel, Sergi, Piñol, Virgínia, Balaguer, Francesc, Bujanda, Luis, Castro, Luisa de, Llor, Xavier, Andreu, Montserrat, Carracedo, Ángel, Soto, José Luis, Castells, Antoni, Jover, Rodrigo, Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, Pérez-Carbonell, Lucía, Ruiz-Ponte, Clara, Guarinos, Carla, Alenda, Cristina, Payá, Artemio, Brea-Fernández, Alejandro, Egoavil, Cecilia, Castillejo, Adela, Barberá, Víctor Manuel, Bessa, Xavier, Xicola, Rosa M., Rodríguez-Soler, María, Sánchez-Fortún, Cristina, Acame, Nuria, Castellví-Bel, Sergi, Piñol, Virgínia, Balaguer, Francesc, Bujanda, Luis, Castro, Luisa de, Llor, Xavier, Andreu, Montserrat, Carracedo, Ángel, Soto, José Luis, Castells, Antoni, and Jover, Rodrigo

Abstract

Background: The selection of patients for genetic testing to rule out Lynch syndrome is currently based on fulfilment of at least one of the revised Bethesda criteria followed by mismatch repair (MMR) status analysis. A study was undertaken to compare the present approach with universal MMR study-based strategies to detect Lynch syndrome in a large series of patients with colorectal cancer (CRC). Methods: 2093 patients with CRC from the EPICOLON I and II cohorts were included. Immunohistochemistry for MMR proteins and/or microsatellite instability (MSI) analysis was performed in tumour tissue. Germline MLH1 and MSH2 mutation analysis was performed in patients whose tumours showed loss of MLH1 or MSH2 staining, respectively. MSH6 genetic testing was done in patients whose tumours showed lack of MSH6 expression or a combined lack of MSH2 and MSH6 expression but did not have MSH2 mutations. PMS2 genetic testing was performed in patients showing isolated loss of PMS2 expression. In patients with MSI tumours and normal or not available MMR protein expression, all four MMR genes were studied. Results: A total of 180 patients (8.6%) showed loss of expression of some of the MMR proteins and/or MSI. Four hundred and eighty-six patients (23.2%) met some of the revised Bethesda criteria. Of the 14 (0.7%) patients who had a MMR gene mutation, 12 fulfilled at least one of the revised Bethesda criteria and two (14.3%) did not. Conclusions: Routine molecular screening of patients with CRC for Lynch syndrome using immunohistochemistry or MSI has better sensitivity for detecting mutation carriers than the Bethesda guidelines.

Published
2011

112. Evidence for classification of c.1852_1853AA>GC in MLH1 as a neutral variant for Lynch syndrome

Author

Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, Castillejo, Adela, Guarinos, Carla, Martínez-Cantó, Ana, Barberá, Víctor Manuel, Egoavil, Cecilia, Castillejo, María Isabel, Pérez-Carbonell, Lucía, Sánchez-Heras, Ana Beatriz, Segura, Ángel, Ochoa, Enrique, Lázaro, Rafael, Ruiz-Ponte, Clara, Bujanda, Luis, Andreu, Montserrat, Castells, Antoni, Carracedo, Ángel, Llor, Xavier, Clofent, Juan, Alenda, Cristina, Payá, Artemio, Jover, Rodrigo, Soto, José Luis, Universidad de Alicante. Departamento de Fisiología, Genética y Microbiología, Castillejo, Adela, Guarinos, Carla, Martínez-Cantó, Ana, Barberá, Víctor Manuel, Egoavil, Cecilia, Castillejo, María Isabel, Pérez-Carbonell, Lucía, Sánchez-Heras, Ana Beatriz, Segura, Ángel, Ochoa, Enrique, Lázaro, Rafael, Ruiz-Ponte, Clara, Bujanda, Luis, Andreu, Montserrat, Castells, Antoni, Carracedo, Ángel, Llor, Xavier, Clofent, Juan, Alenda, Cristina, Payá, Artemio, Jover, Rodrigo, and Soto, José Luis

Abstract

Background: Lynch syndrome (LS) is an autosomal dominant inherited cancer syndrome characterized by early onset cancers of the colorectum, endometrium and other tumours. A significant proportion of DNA variants in LS patients are unclassified. Reports on the pathogenicity of the c.1852_1853AA>GC (p.Lys618Ala) variant of the MLH1 gene are conflicting. In this study, we provide new evidence indicating that this variant has no significant implications for LS. Methods: The following approach was used to assess the clinical significance of the p.Lys618Ala variant: frequency in a control population, case-control comparison, co-occurrence of the p.Lys618Ala variant with a pathogenic mutation, co-segregation with the disease and microsatellite instability in tumours from carriers of the variant. We genotyped p.Lys618Ala in 1034 individuals (373 sporadic colorectal cancer [CRC] patients, 250 index subjects from families suspected of having LS [revised Bethesda guidelines] and 411 controls). Three well-characterized LS families that fulfilled the Amsterdam II Criteria and consisted of members with the p.Lys618Ala variant were included to assess co-occurrence and co-segregation. A subset of colorectal tumour DNA samples from 17 patients carrying the p.Lys618Ala variant was screened for microsatellite instability using five mononucleotide markers. Results: Twenty-seven individuals were heterozygous for the p.Lys618Ala variant; nine had sporadic CRC (2.41%), seven were suspected of having hereditary CRC (2.8%) and 11 were controls (2.68%). There were no significant associations in the case-control and case-case studies. The p.Lys618Ala variant was co-existent with pathogenic mutations in two unrelated LS families. In one family, the allele distribution of the pathogenic and unclassified variant was in trans, in the other family the pathogenic variant was detected in the MSH6 gene and only the deleterious variant co-segregated with the disease in both families. Only two positive

Published
2011

113. Evidence for classification of c.1852_1853AA>GC in MLH1 as a neutral variant for Lynch syndrome

Author

Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Castillejo, Adela, Guarinos, Carla, Martínez Canto, Ana, Barbera, Víctor Manuel, Egoavil, Cecilia, Castillejo, María Isabel, Pérez Carbonell, Lucía, Sánchez Heras, Ana Beatriz, Segura, Ángel, Ochoa, Enrique, Lázaro, Rafael, Ruiz Ponte, Clara, Bujanda, Luis, Andreu, Montserrat, Castells, Antoni, Carracedo Álvarez, Ángel María, Llor, Xavier, Clofent, Juan, Alenda, Cristina, Paya, Artemio, Jover, Rodrigo, Soto, José Luis, Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Castillejo, Adela, Guarinos, Carla, Martínez Canto, Ana, Barbera, Víctor Manuel, Egoavil, Cecilia, Castillejo, María Isabel, Pérez Carbonell, Lucía, Sánchez Heras, Ana Beatriz, Segura, Ángel, Ochoa, Enrique, Lázaro, Rafael, Ruiz Ponte, Clara, Bujanda, Luis, Andreu, Montserrat, Castells, Antoni, Carracedo Álvarez, Ángel María, Llor, Xavier, Clofent, Juan, Alenda, Cristina, Paya, Artemio, Jover, Rodrigo, and Soto, José Luis

Abstract

Background Lynch syndrome (LS) is an autosomal dominant inherited cancer syndrome characterized by early onset cancers of the colorectum, endometrium and other tumours. A significant proportion of DNA variants in LS patients are unclassified. Reports on the pathogenicity of the c.1852_1853AA>GC (p.Lys618Ala) variant of the MLH1 gene are conflicting. In this study, we provide new evidence indicating that this variant has no significant implications for LS. Methods The following approach was used to assess the clinical significance of the p.Lys618Ala variant: frequency in a control population, case-control comparison, co-occurrence of the p.Lys618Ala variant with a pathogenic mutation, co-segregation with the disease and microsatellite instability in tumours from carriers of the variant. We genotyped p.Lys618Ala in 1034 individuals (373 sporadic colorectal cancer [CRC] patients, 250 index subjects from families suspected of having LS [revised Bethesda guidelines] and 411 controls). Three well-characterized LS families that fulfilled the Amsterdam II Criteria and consisted of members with the p.Lys618Ala variant were included to assess co-occurrence and co-segregation. A subset of colorectal tumour DNA samples from 17 patients carrying the p.Lys618Ala variant was screened for microsatellite instability using five mononucleotide markers. Results Twenty-seven individuals were heterozygous for the p.Lys618Ala variant; nine had sporadic CRC (2.41%), seven were suspected of having hereditary CRC (2.8%) and 11 were controls (2.68%). There were no significant associations in the case-control and case-case studies. The p.Lys618Ala variant was co-existent with pathogenic mutations in two unrelated LS families. In one family, the allele distribution of the pathogenic and unclassified variant was in trans, in the other family the pathogenic variant was detected in the MSH6 gene and only the deleterious variant co-segregated with the disease in both families. Only two positive cas

Published
2011

114. Common variants at 2q37.3, 8q24.21, 15q21.3 and 16q24.1 influence chronic lymphocytic leukemia risk

Author

Crowther-Swanepoel, Dalemari, Broderick, Peter, Di Bernardo, Maria Chiara, Dobbins, Sara E., Torres, Maria, Mansouri, Mahmoud, Ruiz-Ponte, Clara, Enjuanes, Anna, Rosenquist, Richard, Carracedo, Angel, Jurlander, Jesper, Campo, Elias, Juliusson, Gunnar, Montserrat, Emilio, Smedby, Karin E., Dyer, Martin J. S., Matutes, Estella, Dearden, Claire, Sunter, Nicola J., Hall, Andrew G., Mainou-Fowler, Tryfonia, Jackson, Graham H., Summerfield, Geoffrey, Harris, Robert J., Pettitt, Andrew R., Allsup, David J., Bailey, James R., Pratt, Guy, Pepper, Chris, Fegan, Chris, Parker, Anton, Oscier, David, Allan, James M., Catovsky, Daniel, Houlston, Richard S., Crowther-Swanepoel, Dalemari, Broderick, Peter, Di Bernardo, Maria Chiara, Dobbins, Sara E., Torres, Maria, Mansouri, Mahmoud, Ruiz-Ponte, Clara, Enjuanes, Anna, Rosenquist, Richard, Carracedo, Angel, Jurlander, Jesper, Campo, Elias, Juliusson, Gunnar, Montserrat, Emilio, Smedby, Karin E., Dyer, Martin J. S., Matutes, Estella, Dearden, Claire, Sunter, Nicola J., Hall, Andrew G., Mainou-Fowler, Tryfonia, Jackson, Graham H., Summerfield, Geoffrey, Harris, Robert J., Pettitt, Andrew R., Allsup, David J., Bailey, James R., Pratt, Guy, Pepper, Chris, Fegan, Chris, Parker, Anton, Oscier, David, Allan, James M., Catovsky, Daniel, and Houlston, Richard S.

Abstract

To identify new risk variants for chronic lymphocytic leukemia (CLL), we conducted a genome-wide association study of 299,983 tagging SNPs, with validation in four additional series totaling 2,503 cases and 5,789 controls. We identified four new risk loci for CLL at 2q37.3 (rs757978, FARP2; odds ratio (OR) = 1.39; P = 2.11 x 10(-9)), 8q24.21 (rs2456449; OR = 1.26; P = 7.84 x 10(-10)), 15q21.3 (rs7169431; OR = 1.36; P = 4.74 x 10(-7)) and 16q24.1 (rs305061; OR = 1.22; P = 3.60 x 10(-7)). We also found evidence for risk loci at 15q25.2 (rs783540, CPEB1; OR = 1.18; P = 3.67 x 10(-6)) and 18q21.1 (rs1036935; OR = 1.22; P = 2.28 x 10(-6)). These data provide further evidence for genetic susceptibility to this B-cell hematological malignancy.

Published
2010
Full Text
View/download PDF

115. Single Nucleotide Polymorphisms in the Wnt and BMP Pathways and Colorectal Cancer Risk in a Spanish Cohort

Author

Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Fernández Rozadilla, Ceres, Castro, Luisa de, Clofent, Juan, Brea Fernández, Alejandro José, Bessa, Xavier, Abulı, Anna, Andreu, Montserrat, Jover, Rodrigo, Xicola, Rosa, Llor, Xavier, Castells, Antoni, Castellví Bel, Sergi, Carracedo Álvarez, Ángel María, Ruiz Ponte, Clara, Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Fernández Rozadilla, Ceres, Castro, Luisa de, Clofent, Juan, Brea Fernández, Alejandro José, Bessa, Xavier, Abulı, Anna, Andreu, Montserrat, Jover, Rodrigo, Xicola, Rosa, Llor, Xavier, Castells, Antoni, Castellví Bel, Sergi, Carracedo Álvarez, Ángel María, and Ruiz Ponte, Clara

Abstract

Background: Colorectal cancer (CRC) is considered a complex disease, and thus the majority of the genetic susceptibility is thought to lie in the form of low-penetrance variants following a polygenic model of inheritance. Candidate-gene studies have so far been one of the basic approaches taken to identify these susceptibility variants. The consistent involvement of some signaling routes in carcinogenesis provided support for pathway-based studies as a natural strategy to select genes that could potentially harbour new susceptibility loci. Methodology/Principal Findings: We selected two main carcinogenesis-related pathways: Wnt and BMP, in order to screen the implicated genes for new risk variants. We then conducted a case-control association study in 933 CRC cases and 969 controls based on coding and regulatory SNPs. We also included rs4444235 and rs9929218, which did not fulfill our selection criteria but belonged to two genes in the BMP pathway and had consistently been linked to CRC in previous studies. Neither allelic, nor genotypic or haplotypic analyses showed any signs of association between the 37 screened variants and CRC risk. Adjustments for sex and age, and stratified analysis between sporadic and control groups did not yield any positive results either. Conclusions/Significance: Despite the relevance of both pathways in the pathogenesis of the disease, and the fact that this is indeed the first study that considers these pathways as a candidate-gene selection approach, our study does not present any evidence of the presence of low-penetrance variants for the selected markers in any of the considered genes in our cohort.

Published
2010

116. Molecular analysis of the APC and MUTYH genes in Galician and Catalonian FAP families: a different spectrum of mutations?

Author

Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Gómez Fernández, Nuria, Castellví Bel, Sergi, Fernández Rozadilla, Ceres, Balaguer, Francesc, Muñoz, Jenifer, Madrigal, Irene, Milà, Montserrat, Graña Suárez, Begoña, Vega Gliemmo, Ana Paula, Castells, Antoni, Carracedo Álvarez, Ángel María, Ruiz Ponte, Clara, Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Gómez Fernández, Nuria, Castellví Bel, Sergi, Fernández Rozadilla, Ceres, Balaguer, Francesc, Muñoz, Jenifer, Madrigal, Irene, Milà, Montserrat, Graña Suárez, Begoña, Vega Gliemmo, Ana Paula, Castells, Antoni, Carracedo Álvarez, Ángel María, and Ruiz Ponte, Clara

Abstract

Background: Familial adenomatous polyposis (FAP) is an autosomal dominant-inherited colorectal cancer syndrome, caused by germline mutations in the APC gene. Recently, biallelic mutations in MUTYH have also been identified in patients with multiple colorectal adenomas and in APC-negative patients with FAP. The aim of this work is therefore to determine the frequency of APC and MUTYH mutations among FAP families from two Spanish populations. Methods: Eighty-two unrelated patients with classical or attenuated FAP were screened for APC germline mutations. MUTYH analysis was then conducted in those APC-negative families and in 9 additional patients from a previous study. Direct sequencing, SSCP analysis and TaqMan genotyping were used to identify point and frameshift mutations, meanwhile large rearrangements in the APC gene were screened by multiplex ligation-dependent probe amplification (MLPA). Results: APC germline mutations were found in 39% of the patients and, despite the great number of genetic variants described so far in this gene, seven new mutations were identified. The two hotspots at codons 1061 and 1309 of the APC gene accounted for 9,4% of the APC-positive families, although they were underrepresented in Galician samples. The deletion at codon 1061 was not found in 19 APC-positive Galician patients but represented 23% of the Catalonian positive families (p = 0,058). The same trend was observed at codon 1309, even though statistical analysis showed no significance between populations. Twenty-four percent of the APC-negative patients carried biallelic MUTYH germline mutations, and showed an attenuated polyposis phenotype generally without extracolonic manifestations. New genetic variants were found, as well as the two hotspots already reported (p.Tyr165Cys and p.Gly382Asp).

Published
2009

118. 106 Implication of the 3′Utr Region of TGFβR1 With MSS HNPCC and Sporadic Colorectal Cancer

Author

Xicola, Rosa M, primary, Doyle, Brian J., additional, Rawson, Jamie, additional, Garre, Pilar, additional, Abulí, Anna, additional, Murugappan, Sathyaraj, additional, Lee, Ji Yeon, additional, Bessa, Xavier, additional, Clofent, Juan, additional, Bujanda, Luis, additional, Balaguer, Francesc, additional, Castellvi-Bel, Sergi, additional, Alenda, Cristina, additional, Jover, Rodrigo, additional, Ruiz-Ponte, Clara, additional, Syngal, Sapna, additional, Andreu, Montserrat, additional, Carracedo, Angel, additional, Castells, Antoni, additional, Ellis, Nathan A., additional, Caldes, Trinidad, additional, and Llor, Xavier, additional

Published
2013
Full Text
View/download PDF

119. Risk of Cancer in Cases of Suspected Lynch Syndrome Without Germline Mutation

Author

Rodríguez–Soler, María, primary, Pérez–Carbonell, Lucía, additional, Guarinos, Carla, additional, Zapater, Pedro, additional, Castillejo, Adela, additional, Barberá, Victor M., additional, Juárez, Miriam, additional, Bessa, Xavier, additional, Xicola, Rosa M., additional, Clofent, Juan, additional, Bujanda, Luis, additional, Balaguer, Francesc, additional, Reñé, Josep–Maria, additional, de–Castro, Luisa, additional, Marín–Gabriel, José C., additional, Lanas, Angel, additional, Cubiella, Joaquín, additional, Nicolás–Pérez, David, additional, Brea–Fernández, Alejandro, additional, Castellví–Bel, Sergi, additional, Alenda, Cristina, additional, Ruiz–Ponte, Clara, additional, Carracedo, Angel, additional, Castells, Antoni, additional, Andreu, Montserrat, additional, Llor, Xavier, additional, Soto, José L., additional, Payá, Artemio, additional, and Jover, Rodrigo, additional

Published
2013
Full Text
View/download PDF

120. Abstract 1334: Implication of the 3′UTR region of TGFβR1 with MSS HNPCC and sporadic colorectal cancer.

Author

Munoz Xicola, Rosa M., primary, Doyle, Brian, additional, Rawson, Jamie, additional, Garre, Pilar, additional, Abuli, Anna, additional, Lee, Esther, additional, Murugappan, Sathyaraj, additional, Bessa, Xavier, additional, Bujanda, Luis, additional, Balaguer, Francesc, additional, Castellvi-Bel, Sergi, additional, Clofent, Juan, additional, Alenda, Cristina, additional, Jover, Rodrigo, additional, Ruiz-Ponte, Clara, additional, Singal, Sapna, additional, Andreu, Montserrat, additional, Carracedo, Angel, additional, Castells, Antoni, additional, Ellis, Nathan, additional, Caldes, Trinidad, additional, and LLor, Xavier, additional

Published
2013
Full Text
View/download PDF

121. Association of a let-7 miRNA binding region of TGFBR1 with hereditary mismatch repair proficient colorectal cancer (MSS HNPCC).

Author

Xicola, Rosa M., Bontu, Sneha, Doyle, Brian J., Rawson, Jamie, Garre, Pilar, Lee, Esther, de la Hoya, Miguel, Bessa, Xavier, Clofent, Joan, Bujanda, Luis, Balaguer, Francesc, Castellví-Bel, Sergi, Alenda, Cristina, Jover, Rodrigo, Ruiz-Ponte, Clara, Syngal, Sapna, Andreu, Montserrat, Carracedo, Angel, Castells, Antoni, and Newcomb, Polly A.

Subjects
MICRORNA, RNA-binding proteins, GENETIC disorders, COLON cancer, HUMAN genetic variation, LUCIFERASES
Abstract

The purpose of this study was to identify novel colorectal cancer (CRC)-causing alleles in unexplained familial CRC cases. In order to do so, coding regions in five candidate genes (MGMT, AXIN2, CTNNB1, TGFBR1 and TGFBR2) were sequenced in 11 unrelated microsatellite-stable hereditary non-polyposis CRC (MSS HNPCC) cases. Selected genetic variants were genotyped in a discovery set of 27 MSS HNPCC cases and 85 controls. One genetic variant, rs67687202, in TGFBR1 emerged as significant (P = 0.002), and it was genotyped in a replication set of 87 additional MSS HNPCC-like cases and 338 controls where it was also significantly associated with MSS HNPCC cases (P = 0.041). In the combined genotype data, rs67687202 was associated with a moderate increase in CRC risk (OR = 1.68; 95% CI = 1.13.2.50; P = 0.010). We tested a highly correlated SNP rs868 in 723 non-familial CRC cases compared with 629 controls, and it was not significantly associated with CRC risk (P = 0.370). rs868 is contained in a let-7 miRNA binding site in the 3ŒUTR of TGFBR1, which might provide a functional basis for the association in MSS HNPCC. In luciferase assays, the risk-associated allele for rs868 was associated with half the luciferase expression in the presence of miRNA let-7b-5p compared with protective allele, suggesting more binding of let-7b-5p and less TGFBR1 expression. Thus, rs868 potentially is a CRC risk-causing allele. Our results support the concept that rs868 is associated with lower TGFBR1 expression thereby increasing CRC risk. [ABSTRACT FROM AUTHOR]

Published
2016
Full Text
View/download PDF

122. BMP2 / BMP4 colorectal cancer susceptibility loci in northern and southern European populations

Author

Fernandez-Rozadilla, Ceres, primary, Palles, Claire, additional, Carvajal-Carmona, Luis, additional, Peterlongo, Paolo, additional, Nici, Carmela, additional, Veneroni, Silvia, additional, Pinheiro, Manuela, additional, Teixeira, Manuel R., additional, Moreno, Victor, additional, Lamas, Maria-Jesus, additional, Baiget, Montserrat, additional, Lopez-Fernandez, LA, additional, Gonzalez, Dolors, additional, Brea-Fernandez, Alejandro, additional, Clofent, Juan, additional, Bujanda, Luis, additional, Bessa, Xavier, additional, Andreu, Montserrat, additional, Xicola, Rosa, additional, Llor, Xavier, additional, Jover, Rodrigo, additional, Castells, Antoni, additional, Castellvi-Bel, Sergi, additional, Carracedo, Angel, additional, Tomlinson, Ian, additional, and Ruiz-Ponte, Clara, additional

Published
2012
Full Text
View/download PDF

123. Sa1774 Prevalence of MLH1 Constitutional Epimutations as a Cause of Lynch Syndrome in Unselected Consecutive Cases of Colorectal Cancer

Author

Rodriguez-Soler, Maria, primary, Pérez-Carbonell, Lucia, additional, Guarinos, Carla, additional, Castillejo, Adela, additional, Egoavil, Cecilia, additional, Barberà, Victor M., additional, Martinez-Dueńas, Eduardo, additional, Castillejo, Maria-Isabel, additional, Martinez-Canto, Ana, additional, Sanchez-Heras, Ana B., additional, Ruiz-Ponte, Clara, additional, Brea, Alejandro, additional, Alenda, Cristina, additional, Paya, Artemio, additional, Sanchez-Fortun, Cristina, additional, Juarez-Quesada, Miriam, additional, Bujanda, Luis, additional, Clofent, Juan, additional, Llor, Xavier, additional, Andreu, Montserrat, additional, Castells, Antoni, additional, Carracedo, Angel, additional, Soto, José-Luis, additional, and Jover, Rodrigo, additional

Published
2012
Full Text
View/download PDF

124. Su1813 Susceptibility Genetic Variants Associated With Early-Onset Colorectal Cancer

Author

Giráldez, María Dolores, primary, López-Dóriga, Adriana, additional, Bujanda, Luis, additional, Abulí, Anna, additional, Bessa, Xavier, additional, Fernandez-Rozadilla, Ceres, additional, Munoz, Jenifer, additional, Cuatrecasas, Miriam, additional, Jover, Rodrigo, additional, Xicola, Rosa M, additional, Llor, Xavier, additional, Piqué, Josep M, additional, Carracedo, Angel, additional, Ruiz-Ponte, Clara, additional, Cosme, Angel, additional, Enriquez-Navascués, José M., additional, Moreno, Victor, additional, Andreu, Montserrat, additional, Castells, Antoni, additional, Balaguer, Francesc, additional, and Castellvi-Bel, Sergi, additional

Published
2012
Full Text
View/download PDF

125. Cumulative impact of common genetic variants and other risk factors on colorectal cancer risk in 42 103 individuals

Author

Dunlop, Malcolm G, primary, Tenesa, Albert, additional, Farrington, Susan M, additional, Ballereau, Stephane, additional, Brewster, David H, additional, Koessler, Thibaud, additional, Pharoah, Paul, additional, Schafmayer, Clemens, additional, Hampe, Jochen, additional, Völzke, Henry, additional, Chang-Claude, Jenny, additional, Hoffmeister, Michael, additional, Brenner, Hermann, additional, von Holst, Susanna, additional, Picelli, Simone, additional, Lindblom, Annika, additional, Jenkins, Mark A, additional, Hopper, John L, additional, Casey, Graham, additional, Duggan, David, additional, Newcomb, Polly A, additional, Abulí, Anna, additional, Bessa, Xavier, additional, Ruiz-Ponte, Clara, additional, Castellví-Bel, Sergi, additional, Niittymäki, Iina, additional, Tuupanen, Sari, additional, Karhu, Auli, additional, Aaltonen, Lauri, additional, Zanke, Brent, additional, Hudson, Tom, additional, Gallinger, Steven, additional, Barclay, Ella, additional, Martin, Lynn, additional, Gorman, Maggie, additional, Carvajal-Carmona, Luis, additional, Walther, Axel, additional, Kerr, David, additional, Lubbe, Steven, additional, Broderick, Peter, additional, Chandler, Ian, additional, Pittman, Alan, additional, Penegar, Steven, additional, Campbell, Harry, additional, Tomlinson, Ian, additional, and Houlston, Richard S, additional

Published
2012
Full Text
View/download PDF

126. Refinement of the associations between risk of colorectal cancer and polymorphisms on chromosomes 1q41 and 12q13.13

Author

Spain, Sarah L., primary, Carvajal-Carmona, Luis G., additional, Howarth, Kimberley M., additional, Jones, Angela M., additional, Su, Zhan, additional, Cazier, Jean-Baptiste, additional, Williams, Jennet, additional, Aaltonen, Lauri A., additional, Pharoah, Paul, additional, Kerr, David J., additional, Cheadle, Jeremy, additional, Li, Li, additional, Casey, Graham, additional, Vodicka, Pavel, additional, Sieber, Oliver, additional, Lipton, Lara, additional, Gibbs, Peter, additional, Martin, Nicholas G., additional, Montgomery, Grant W., additional, Young, Joanne, additional, Baird, Paul N., additional, Morreau, Hans, additional, van Wezel, Tom, additional, Ruiz-Ponte, Clara, additional, Fernandez-Rozadilla, Ceres, additional, Carracedo, Angel, additional, Castells, Antoni, additional, Castellvi-Bel, Sergi, additional, Dunlop, Malcolm, additional, Houlston, Richard S., additional, and Tomlinson, Ian P.M., additional

Published
2011
Full Text
View/download PDF

127. Genetic Associations in the Vitamin D Receptor and Colorectal Cancer in African Americans and Caucasians

Author

Kupfer, Sonia S., primary, Anderson, Jeffrey R., additional, Ludvik, Anton E., additional, Hooker, Stanley, additional, Skol, Andrew, additional, Kittles, Rick A., additional, Keku, Temitope O., additional, Sandler, Robert S., additional, Ruiz-Ponte, Clara, additional, Castellvi-Bel, Sergi, additional, Castells, Antoni, additional, Carracedo, Angel, additional, and Ellis, Nathan A., additional

Published
2011
Full Text
View/download PDF

128. Comparison between universal molecular screening for Lynch syndrome and revised Bethesda guidelines in a large population-based cohort of patients with colorectal cancer

Author

Pérez-Carbonell, Lucía, primary, Ruiz-Ponte, Clara, additional, Guarinos, Carla, additional, Alenda, Cristina, additional, Payá, Artemio, additional, Brea, Alejandro, additional, Egoavil, Cecilia M, additional, Castillejo, Adela, additional, Barberá, Victor M, additional, Bessa, Xavier, additional, Xicola, Rosa M, additional, Rodríguez-Soler, María, additional, Sánchez-Fortún, Cristina, additional, Acame, Nuria, additional, Castellví-Bel, Sergi, additional, Piñol, Virgínia, additional, Balaguer, Francesc, additional, Bujanda, Luis, additional, De-Castro, María-Luisa, additional, Llor, Xavier, additional, Andreu, Montserrat, additional, Carracedo, Angel, additional, Soto, José-Luis, additional, Castells, Antoni, additional, and Jover, Rodrigo, additional

Published
2011
Full Text
View/download PDF

130. Differential Features of Colorectal Cancer (CRC) in Patients With Probable Non-Sporadic Mismatch Repair Deficiency Without Germline Mutation

Author

Rodríguez Soler, María, primary, Pérez-Carbonell, Lucía, additional, Guarinos, Carla, additional, Ruiz-Ponte, Clara, additional, Brea, Alejandro, additional, Castillejo, Adela, additional, Barberá, Victor M., additional, Sanchez-Fortun, Cristina, additional, Sempere-Robles, Laura, additional, Bujanda, Luis, additional, Clofent, Joan, additional, Llor, Xavier, additional, Andreu, Montserrat, additional, Castells, Antoni, additional, Carracedo, Angel, additional, Soto, José-Luis, additional, Payá, Artemio, additional, Alenda, Cristina, additional, and Jover, Rodrigo, additional

Published
2011
Full Text
View/download PDF

131. Comparison Between Universal Immunohistochemistry for Mismatch Repair Proteins Versus Revised Bethesda Guidelines in the Detection of Patients With Lynch Syndrome

Author

Pérez-Carbonell, Lucía, primary, Guarinos, Carla, additional, Rodríguez Soler, María, additional, Sanchez-Fortun, Cristina, additional, Sempere-Robles, Laura, additional, Ruiz-Ponte, Clara, additional, Castillejo, Adela, additional, Brea, Alejandro, additional, Carracedo, Angel, additional, Barberá, Victor M., additional, Rojas, Estefanía, additional, Bujanda, Luis, additional, Clofent, Joan, additional, Andreu, Montserrat, additional, Llor, Xavier, additional, Castells, Antoni, additional, Soto, José-Luis, additional, and Jover, Rodrigo, additional

Published
2011
Full Text
View/download PDF

132. Evidence for classification of c.1852_1853AA>GC in MLH1 as a neutral variant for Lynch syndrome

Author

Castillejo, Adela, primary, Guarinos, Carla, additional, Martinez-Canto, Ana, additional, Barbera, Victor-Manuel, additional, Egoavil, Cecilia, additional, Castillejo, Maria-Isabel, additional, Perez-Carbonell, Lucia, additional, Sanchez-Heras, Ana-Beatriz, additional, Segura, Angel, additional, Ochoa, Enrique, additional, Lazaro, Rafael, additional, Ruiz-Ponte, Clara, additional, Bujanda, Luis, additional, Andreu, Montserrat, additional, Castells, Antoni, additional, Carracedo, Angel, additional, Llor, Xavier, additional, Clofent, Juan, additional, Alenda, Cristina, additional, Paya, Artemio, additional, Jover, Rodrigo, additional, and Soto, Jose-Luis, additional

Published
2011
Full Text
View/download PDF

133. S1984 Case-Control Genetic Association Study of Candidates Genes for Genetic Susceptibility to Colorectal Cancer

Author

Abulí, Anna, primary, Fernandez-Rozadilla, Ceres, additional, Alonso-Espinaco, Virginia, additional, Giráldez, María Dolores, additional, Muñoz, Jenifer, additional, Bessa, Xavier, additional, Llor, Xavier, additional, Jover, Rodrigo, additional, Carvajal-Carmona, Luís, additional, Tomlinson, Ian, additional, Moreno, Victor, additional, Carracedo, Angel, additional, Castells, Antoni, additional, Andreu, Montserrat, additional, Ruiz-Ponte, Clara, additional, and Castellvi-Bel, Sergi, additional

Published
2010
Full Text
View/download PDF

134. S1993 Comparison Between Routine Immunohistochemistry for Mismatch Repair Proteins Versus Revised Bethesda Guidelines in the Diagnosis of Lynch Syndrome in a Non-Selected Population of Colorectal Cancer Patients

Author

Pérez-Carbonell, Lucía, primary, Ruiz-Ponte, Clara, additional, Bessa, Xavier, additional, Soto, José-Luis, additional, Castillejo, Adela, additional, Barberá, Victor, additional, Brea, Alejandro, additional, Sempere, Laura, additional, Sánchez-Fortún, Cristina, additional, Castellvi-Bel, Sergi, additional, Balaguer, Francesc, additional, Xicola, Rosa M, additional, Llor, Xavier, additional, Abulí, Anna, additional, Andreu, Montserrat, additional, Alenda, Cristina, additional, Payá, Artemio, additional, Carracedo, Angel, additional, Castells, Antoni, additional, and Jover, Rodrigo, additional

Published
2010
Full Text
View/download PDF

135. Common variants at 2q37.3, 8q24.21, 15q21.3 and 16q24.1 influence chronic lymphocytic leukemia risk

Author

Crowther-Swanepoel, Dalemari, primary, Broderick, Peter, additional, Di Bernardo, Maria Chiara, additional, Dobbins, Sara E, additional, Torres, María, additional, Mansouri, Mahmoud, additional, Ruiz-Ponte, Clara, additional, Enjuanes, Anna, additional, Rosenquist, Richard, additional, Carracedo, Angel, additional, Jurlander, Jesper, additional, Campo, Elias, additional, Juliusson, Gunnar, additional, Montserrat, Emilio, additional, Smedby, Karin E, additional, Dyer, Martin J S, additional, Matutes, Estella, additional, Dearden, Claire, additional, Sunter, Nicola J, additional, Hall, Andrew G, additional, Mainou-Fowler, Tryfonia, additional, Jackson, Graham H, additional, Summerfield, Geoffrey, additional, Harris, Robert J, additional, Pettitt, Andrew R, additional, Allsup, David J, additional, Bailey, James R, additional, Pratt, Guy, additional, Pepper, Chris, additional, Fegan, Chris, additional, Parker, Anton, additional, Oscier, David, additional, Allan, James M, additional, Catovsky, Daniel, additional, and Houlston, Richard S, additional

Published
2010
Full Text
View/download PDF

136. 767 Genotype-Phenotype Correlation of Genetic Susceptibility Variants Identified Through Genome-Wide Association Studies for Colorectal Cancer

Author

Abulí, Anna, primary, Bessa, Xavier, additional, Ruiz-Ponte, Clara, additional, Fernandez-Rozadilla, Ceres, additional, Carracedo, Angel, additional, Ilzarbe, Lucas, additional, Llor, Xavier, additional, Jover, Rodrigo, additional, Muñoz, Jenifer, additional, Castells, Antoni, additional, Castellvi-Bel, Sergi, additional, and Andreu, Montserrat, additional

Published
2009
Full Text
View/download PDF

139. A New Set of in SilicoTools to Support the Interpretation of ATMMissense Variants Using Graphical Analysis

Author

Porras, Luz-Marina, Padilla, Natàlia, Moles-Fernández, Alejandro, Feliubadaló, Lidia, Santamariña-Pena, Marta, Sánchez, Alysson T., López-Novo, Anael, Blanco, Ana, de la Hoya, Miguel, Molina, Ignacio J., Osorio, Ana, Pineda, Marta, Rueda, Daniel, Ruiz-Ponte, Clara, Vega, Ana, Lázaro, Conxi, Díez, Orland, Gutiérrez-Enríquez, Sara, and de la Cruz, Xavier

Abstract

Establishing the pathogenic nature of variants in ATM, a gene associated with breast cancer and other hereditary cancers, is crucial for providing patients with adequate care. Unfortunately, achieving good variant classification is still difficult. To address this challenge, we extended the range of in silicotools with a series of graphical tools devised for the analysis of computational evidence by health care professionals. We propose a family of fast and easy-to-use graphical representations in which the impact of a variant is considered relative to other pathogenic and benign variants. To illustrate their value, the representations are applied to three problems in variant interpretation. The assessment of computational pathogenicity predictions showed that the graphics provide an intuitive view of prediction reliability, complementing and extending conventional numerical reliability indexes. When applied to variant of unknown significance populations, the representations shed light on the nature of these variants and can be used to prioritize variants of unknown significance for further studies. In a third application, the graphics were used to compare the two versions of the ATM-adapted American College of Medical Genetics and Genomics and Association for Molecular Pathology guidelines, obtaining valuable information on their relative virtues and weaknesses. Finally, a server [ATMision (ATM missense in silicointerpretation online)] was generated for users to apply these representations in their variant interpretation problems, to check the ATM-adapted guidelines' criteria for computational evidence on their variant(s) and access different sources of information.

Published
2023
Full Text
View/download PDF

140. Uso de paneles de genes en pacientes con alto riesgo de cáncer digestivo hereditario: documento de posicionamiento de la AEG, SEOM, AEGH y consorcio IMPaCT-GENÓMICA

Author

Carballal, Sabela, Balaguer, Francesc, Bujanda, Luis, Capellá, Gabriel, González Santiago, Santiago, Jover, Rodrigo, Moreira, Leticia, Pineda, Marta, Ruiz-Ponte, Clara, Sánchez Heras, Ana Beatriz, Serrano Blanch, Raquel, Soto, José Luis, Vidal Tocino, Rosario, and Cubiella, Joaquín

Abstract

Este documento de posicionamiento, auspiciado por la Asociación Española de Gastroenterología, la Sociedad Española de Oncología Médica, la Asociación Española de Genética Humana y el consorcio IMPaCT-Genómica, tiene como objetivo realizar recomendaciones para el uso de paneles de genes en la evaluación de individuos con alto riesgo de cáncer digestivo hereditario. Para medir la calidad de la evidencia y los niveles de recomendación se ha utilizado la metodología basada en el sistema Grading of Recommendations Assessment, Development and Evaluation(GRADE). Se obtuvo el consenso entre expertos mediante un método Delphi. El documento incluye recomendaciones sobre escenarios clínicos en los que se recomienda el uso de paneles de genes en cáncer colorrectal, síndromes polipósicos, cáncer gástrico y pancreático, así como los genes de los paneles a ser considerados en cada una de estas situaciones clínicas. También se establecen recomendaciones sobre la evaluación de mosaicismos, las estrategias de asesoramiento ante la ausencia de sujeto índice y, finalmente, el análisis constitucional tras identificación de variantes patogénicas tumorales.

Published
2023
Full Text
View/download PDF

141. Genotyping SNPs With the LightCycler.

Author

Walker, John M., Carracedo, Angel, Lareu, Mará Victoria, and Ruiz-Ponte, Clara

Abstract

Here, a single nucleotide polymorphism typing methodology is described based on polymerase chain reaction monitoring, in real time, of fluorescently labeled amplified products using the LightCycler. The main advantages of the system are the time required for the analysis (about 20 min), combined with the robustness, accuracy, and the sensitivity of the method. [ABSTRACT FROM AUTHOR]

Published
2005
Full Text
View/download PDF

146. The Fanconi anemia DNA damage repair pathway in the spotlight for germline predisposition to colorectal cancer

Author

Esteban-Jurado, Clara, Franch-Expósito, Sebastià, Muñoz, Jenifer, Ocaña, Teresa, Carballal, Sabela, López-Cerón, Maria, Cuatrecasas, Miriam, Vila-Casadesús, Maria, Lozano, Juan José, Serra, Enric, Beltran, Sergi, Brea-Fernández, Alejandro, Ruiz-Ponte, Clara, Castells, Antoni, Bujanda, Luis, Garre, Pilar, Caldés, Trinidad, Cubiella, Joaquín, Balaguer, Francesc, and Castellví-Bel, Sergi

Abstract

Colorectal cancer (CRC) is one of the most common neoplasms in the world. Fanconi anemia (FA) is a very rare genetic disease causing bone marrow failure, congenital growth abnormalities and cancer predisposition. The comprehensive FA DNA damage repair pathway requires the collaboration of 53 proteins and it is necessary to restore genome integrity by efficiently repairing damaged DNA. A link between FA genes in breast and ovarian cancer germline predisposition has been previously suggested. We selected 74 CRC patients from 40 unrelated Spanish families with strong CRC aggregation compatible with an autosomal dominant pattern of inheritance and without mutations in known hereditary CRC genes and performed germline DNA whole-exome sequencing with the aim of finding new candidate germline predisposition variants. After sequencing and data analysis, variant prioritization selected only those very rare alterations, producing a putative loss of function and located in genes with a role compatible with cancer. We detected an enrichment for variants in FA DNA damage repair pathway genes in our familial CRC cohort as 6 families carried heterozygous, rare, potentially pathogenic variants located in BRCA2/FANCD1, BRIP1/FANCJ, FANCC, FANCE and REV3L/POLZ. In conclusion, the FA DNA damage repair pathway may play an important role in the inherited predisposition to CRC.

Published
2016
Full Text
View/download PDF

148. Diagnostic criteria for constitutional mismatch repair deficiency syndrome: suggestions of the European consortium 'Care for CMMRD' (C4CMMRD).

Author

Wimmer, Katharina, Kratz, Christian P., Vasen, Hans F. A., Caron, Olivier, Colas, Chrystelle, Entz-Werle, Natacha, Gerdes, Anne-Marie, Goldberg, Yael, Ilencikova, Denisa, Muleris, Martine, Duval, Alex, Lavoine, Noémie, Ruiz-Ponte, Clara, Slavc, Irene, Burkhardt, Brigit, and Brugieres, Laurence

Subjects
CYSTS (Pathology), ONCOLOGY, TUMORS, BRAIN diseases
Abstract

Constitutional mismatch repair deficiency (CMMRD) syndrome is a distinct childhood cancer predisposition syndrome that results from biallelic germline mutations in one of the four MMR genes, MLH1, MSH2, MSH6 or PMS2. The tumour spectrum is very broad, including mainly haematological, brain and intestinal tract tumours. Patients show a variety of non-malignant features that are indicative of CMMRD. However, currently no criteria that should entail diagnostic evaluation of CMMRD exist. We present a three-point scoring system for the suspected diagnosis CMMRD in a paediatric/young adult cancer patient. Tumours highly specific for CMMRD syndrome are assigned three points, malignancies overrepresented in CMMRD two points and all other malignancies one point. According to their specificity for CMMRD and their frequency in the general population, additional features are weighted with 1-2 points. They include multiple hyperpigmented and hypopigmented skin areas, brain malformations, pilomatricomas, a second childhood malignancy, a Lynch syndrome (LS)-associated tumour in a relative and parental consanguinity. According to the scoring system, CMMRD should be suspected in any cancer patient who reaches a minimum of three points by adding the points of the malignancy and the additional features. The diagnostic steps to confirm or refute the suspected diagnosis are outlined. We expect that application of the suggested strategy for CMMRD diagnosis will increase the number of patients being identified at the time when they develop their first tumour. This will allow adjustment of the treatment modalities, offering surveillance strategies for second malignancies and appropriate counselling of the entire family. [ABSTRACT FROM AUTHOR]

Published
2014
Full Text
View/download PDF

149. Multiple Sporadic Colorectal Cancers Display a Unique Methylation Phenotype.

Author

Gonzalo, Victoria, Lozano, Juan Jose, Alonso-Espinaco, Virginia, Moreira, Leticia, Muñoz, Jenifer, Pellisé, Maria, Castellví-Bel, Sergi, Bessa, Xavier, Andreu, Montserrat, Xicola, Rosa M., Llor, Xavier, Ruiz-Ponte, Clara, Carracedo, Angel, Jover, Rodrigo, Castells, Antoni, and Balaguer, Francesc

Subjects
COLON cancer patients, DNA methylation, PHENOTYPES, CARCINOGENESIS, EPIGENETICS, BIOLOGICAL assay, FUNCTIONAL analysis
Abstract

Epigenetics are thought to play a major role in the carcinogenesis of multiple sporadic colorectal cancers (CRC). Previous studies have suggested concordant DNA hypermethylation between tumor pairs. However, only a few methylation markers have been analyzed. This study was aimed at describing the epigenetic signature of multiple CRC using a genome-scale DNA methylation profiling. We analyzed 12 patients with synchronous CRC and 29 age-, sex-, and tumor location-paired patients with solitary tumors from the EPICOLON II cohort. DNA methylation profiling was performed using the Illumina Infinium HM27 DNA methylation assay. The most significant results were validated by Methylight. Tumors samples were also analyzed for the CpG Island Methylator Phenotype (CIMP); KRAS and BRAF mutations and mismatch repair deficiency status. Functional annotation clustering was performed. We identified 102 CpG sites that showed significant DNA hypermethylation in multiple tumors with respect to the solitary counterparts (difference in β value ≥0.1). Methylight assays validated the results for 4 selected genes (p = 0.0002). Eight out of 12(66.6%) multiple tumors were classified as CIMP-high, as compared to 5 out of 29(17.2%) solitary tumors (p = 0.004). Interestingly, 76 out of the 102 (74.5%) hypermethylated CpG sites found in multiple tumors were also seen in CIMP-high tumors. Functional analysis of hypermethylated genes found in multiple tumors showed enrichment of genes involved in different tumorigenic functions. In conclusion, multiple CRC are associated with a distinct methylation phenotype, with a close association between tumor multiplicity and CIMP-high. Our results may be important to unravel the underlying mechanism of tumor multiplicity. [ABSTRACT FROM AUTHOR]

Published
2014
Full Text
View/download PDF

150. Association between CASP8 –652 6N Del Polymorphism (rs3834129) and Colorectal Cancer Risk: Results from a Multi-Centric Study.

Author

Pardini, Barbara, Verderio, Paolo, Pizzamiglio, Sara, Nici, Carmela, Maiorana, Maria Valeria, Naccarati, Alessio, Vodickova, Ludmila, Vymetalkova, Veronika, Veneroni, Silvia, Daidone, Maria Grazia, Ravagnani, Fernando, Bianchi, Tiziana, Bujanda, Luis, Carracedo, Angel, Castells, Antoni, Ruiz-Ponte, Clara, Morreau, Hans, Howarth, Kimberley, Jones, Angela, and Castellví-Bel, Sergi

Subjects
COLON cancer risk factors, GENETIC polymorphisms, GENE frequency, CASE-control method, ROBUST control, GENETICS of colon cancer, HUMAN genetic variation
Abstract

The common −652 6N del variant in the CASP8 promoter (rs3834129) has been described as a putative low-penetrance risk factor for different cancer types. In particular, some studies suggested that the deleted allele (del) was inversely associated with CRC risk while other analyses failed to confirm this. Hence, to better understand the role of this variant in the risk of developing CRC, we performed a multi-centric case-control study. In the study, the variant −652 6N del was genotyped in a total of 6,733 CRC cases and 7,576 controls recruited by six different centers located in Spain, Italy, USA, England, Czech Republic and the Netherlands collaborating to the international consortium COGENT (COlorectal cancer GENeTics). Our analysis indicated that rs3834129 was not associated with CRC risk in the full data set. However, the del allele was under-represented in one set of cases with a family history of CRC (per allele model OR = 0.79, 95% CI = 0.69–0.90) suggesting this allele might be a protective factor versus familial CRC. Since this multi-centric case-control study was performed on a very large sample size, it provided robust clarification of the effect of rs3834129 on the risk of developing CRC in Caucasians. [ABSTRACT FROM AUTHOR]

Published
2014
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results