Your search keyword '"Poves, Carmen"' showing total 30 results

1. Quality of Colonoscopy Is Associated With Adenoma Detection and Postcolonoscopy Colorectal Cancer Prevention in Lynch Syndrome

Author

Sánchez, Ariadna, Roos, Victorine H., Navarro, Matilde, Pineda, Marta, Caballol, Berta, Moreno, Lorena, Carballal, Sabela, Rodríguez-Alonso, Lorena, Ramon y Cajal, Teresa, Llort, Gemma, Piñol, Virginia, López-Fernández, Adrià, Salces, Inmaculada, Picó, Maria Dolores, Rivas, Laura, Bujanda, Luis, Garzon, Marta, Pizarro, Angeles, Martinez de Castro, Eva, López-Arias, Maria Jesus, Poves, Carmen, Garau, Catalina, Rodriguez-Alcalde, Daniel, Herraiz, Maite, Alvarez-Urrutia, Cristina, Dacal, Andres, Carrillo-Palau, Marta, Cid, Lucia, Ponce, Marta, Barreiro-Alonso, Eva, Saperas, Esteban, Aguirre, Elena, Romero, Cristina, Bastiaansen, Barbara, Gonzalez-Acosta, Maribel, Morales-Romero, Blai, Ocaña, Teresa, Rivero-Sánchez, Liseth, Jung, Gerhard, Bessa, Xavier, Cubiella, Joaquin, Jover, Rodrigo, Rodríguez-Moranta, Francisco, Balmaña, Judith, Brunet, Joan, Castells, Antoni, Dekker, Evelien, Capella, Gabriel, Serra-Burriel, Miquel, Moreira, Leticia, Pellise, Maria, and Balaguer, Francesc

Published

2022

2. Multiplexed Biosensing Diagnostic Platforms Detecting Autoantibodies to Tumor-Associated Antigens from Exosomes Released by CRC Cells and Tissue Samples Showed High Diagnostic Ability for Colorectal Cancer

Author

Montero-Calle, Ana, Aranguren-Abeigon, Itziar, Garranzo-Asensio, María, Poves, Carmen, Fernández-Aceñero, María Jesús, Martínez-Useros, Javier, Sanz, Rodrigo, Dziaková, Jana, Rodriguez-Cobos, Javier, Solís-Fernández, Guillermo, Povedano, Eloy, Gamella, Maria, Torrente-Rodríguez, Rebeca Magnolia, Alonso-Navarro, Miren, de los Ríos, Vivian, Casal, J. Ignacio, Domínguez, Gemma, Guzman-Aranguez, Ana, Peláez-García, Alberto, Pingarrón, José Manuel, Campuzano, Susana, and Barderas, Rodrigo

Published

2021

3. Identification of tumor-associated antigens with diagnostic ability of colorectal cancer by in-depth immunomic and seroproteomic analysis

Author

Garranzo-Asensio, María, San Segundo-Acosta, Pablo, Povés, Carmen, Fernández-Aceñero, María Jesús, Martínez-Useros, Javier, Montero-Calle, Ana, Solís-Fernández, Guillermo, Sanchez-Martinez, Maricruz, Rodríguez, Nuria, Cerón, María Ángeles, Fernandez-Diez, Servando, Domínguez, Gemma, de los Ríos, Vivian, Peláez-García, Alberto, Guzmán-Aránguez, Ana, and Barderas, Rodrigo

Published

2020

4. Clinical and Pathological Characterization of Lynch-Like Syndrome

Author

Picó, María Dolores, Castillejo, Adela, Murcia, Óscar, Giner-Calabuig, Mar, Alustiza, Miren, Sánchez, Ariadna, Moreira, Leticia, Pellise, María, Castells, Antoni, Carrillo-Palau, Marta, Ramon y Cajal, Teresa, Gisbert-Beamud, Alexandra, Llort, Gemma, Yagüe, Carmen, López-Fernández, Adriá, Alvarez-Urturi, Cristina, Cubiella, Joaquin, Rivas, Laura, Rodríguez-Alcalde, Daniel, Herraiz, Maite, Garau, Catalina, Dolz, Carlos, Bujanda, Luis, Cid, Lucia, Povés, Carmen, Garzon, Marta, Salces, Inmaculada, Ponce, Marta, Hernández-Villalba, Luís, Alenda, Cristina, Balaguer, Francesc, Soto, Jose-Luis, and Jover, Rodrigo

Published

2020

5. Impact of age- and gender-specific cut-off values for the fecal immunochemical test for hemoglobin in colorectal cancer screening

Author

Lanas, Angel, Gonzalez-Rubio, Francisca, Moya-Calvo, Alberto, Polo-Tomas, Mónica, Pilar Roncales, Maria, Sebastian-Martínez, Pilar, Valencia-Doblas, María Ángeles, Valero-Capilla, Nieves, Bujanda, Luis, Alkiza, María E., Altzibar, Jone, Amiano, Pilar, Arenas, Juan, Artiñano, Edurne, Cosme, Angel, Egitegi, Isabel, Elorriaga, Kepa, Elósegui, Jose L., Enriquez-Navascués, José M., Erce, Cristina, Gil, Inés, Gutiérrez-Stampa, María A., Herreros, Marta, Hijona, Elizabeth, Jaúregui, Mariluz, Laredo, Eva, Martínez, Roberto, Mitxelena, Maria J., Montalvo, Isabel, Placer, Carlos, Portillo, Isabel, Quintero, Enrique, Alarcón, Onofre, Alonso-Abreu, Inmaculada, Carrillo-Palau, Marta, de la Vega-Prieto, Mariola, Díez-Fuentes, María Luisa, Gimeno-García, Antonio, González-Méndez, Yanira, Hernández-Guerra, Manuel, Linertová, Renata, Nicolás-Perez, David, Reyes-Melián, Juana María, Andreu, Montserrat, Álvarez, Cristina, Augé, Josep M., Balaguer, Francesc, Barau, Mercè, Bessa, Xavier, Bory, Felipe, Burón, Andrea, Castells, Antoni, Castells, Xavier, Comas, Mercè, Cuatrecasas, Míriam, Estrada, Maria, Ferrer, Olga, Garrell, Imma, Grau, Jaume, Guayta, Rafael, Hernández, Cristina, López-Cerón, María, Macià, Francesc, Moreira, Leticia, Ocaña, Teresa, Pellisé, Maria, Piracés, Mercè, Polbach, Sandra, Puigvehí, Marc, Rodríguez, Cristina, Sala, Maria, Seoane, Agustín, Serradesanferm, Anna, Sivilla, Judith, Cubiella, Joaquín, Belén Aguado, Mª, Aldecoa, Susana, Almazán, Raquel, Alonso, Ana, Castro, Inés, Cid, Estela, Cid, Lucía, Clofent, Joan, de Castro, Mª Luisa, Estévez, Pamela, Fernández, Ana Belén, Dolores González, Mª, González, Simoneta, Carmen González-Mao, Mª, Hernández, Vicent, Iglesias, Begoña, Iglesias, Felipe, Iglesias, Pilar, López-Martínez, Ángeles, Macenlle, Ramiro, Martínez, Alfonso, Martínez, David, Menéndez, Carlos, Méndez, Carmen, Hermo, José Antonio, Pérez, Isabel, Portasany, Carmen, Rionda, Mar, Rivera, Concepción, Rodríguez, Benito, Rodríguez, Rosa, Rubio, Manuel, Santiago, María Isolina, Vázquez, Miriam, Vázquez, José Ángel, Vega, Pablo, Carmen Vidal, Mª, Zubizarreta, Raquel, Diego Morillas, Juan, Abreu, Luís, Javier Amador, Francisco, Arroyo, Manuel, Bandrés, Fernando, Barba, Margarita, Blanco, José Manuel, Cacho, Guillermo, Cantero, José, Carrasco, Juan, Carrascosa, Beatriz, Castellano, Gregorio, Colina, Francisco, Chaparro, María, Díaz-Rubio, Manuel, Díaz-Tasende, José, Esteban, José Miguel, Fernández, Conrado, Fernández-Díez, Servando, Fernández-Gil, Marta, Ferrándiz, Juan, Franco, Alejandro, García-Álvarez, Gabriela, Garrido, Aurelio, Garrido, Sofía, Gisbert, Javier P., Gómez-Haba, Mariano, Gómez-Molíns, Inés, González-Navarro, Andrés, González, María José, Herranz, Belén, Herránz, Pilar, Herreros, Alberto, Iglesias, Rosario, Izquierdo, Sonia, López, Carlos, López-Rubio, María Aranzazu, Marín, Alicia, Marín, José Carlos, Martín, María Carmen, Martínez, José Luis, Martínez, Raquel, Moliner, Carmen, Moreno, José Manuel, Moreno, Ricardo, Nogueiras, Amelia, Pérez, María Teresa, Píriz, Rafael, Plaza, Carmen, Polentinos, Elena, Povés, Carmen, Ruíz, Pedro, Salces, Inmaculada, Sánchez-Ceballos, Francisco, Santander, Cecilio, Sastre, Rocío, Valentín, Vicente, Carballo, Fernando, Alajarín, Miriam, Alberca, Fernando, Bermejo, Juan, Carrillo, Joaquín, Cruzado, José, López, Purificación, Martínez, Mariano, Navarro, María Dolores, Ono, Akiko, Parra, Soledad, Pérez-Riquelme, Francisco, Salas, Dolores, Andrés, Mercedes, Calvo, Consuelo, Jimenez, Montserrat, Málaga, Araceli, Pérez, Elena, Peris, Antonio, Ponce, Marta, Jover, Rodrigo, Sala, Teresa, Teruel, Gloria, Alvarez-Urturi, Cristina, Hernandez, Cristina, Perez-Riquelme, Francisco, Cruzado, Jose, Hernandez, Vicent, Mao, Carmen Gonzalez, Perez, Elena, Sarasqueta, Cristina, Morillas, Juan Diego, Sostres, Carlos, and Augé, Josep Maria

Published

2016

6. Contribution of New Adenomatous Polyposis Predisposition Genes in an Unexplained Attenuated Spanish Cohort by Multigene Panel Testing

Author

Lorca, Víctor, Rueda, Daniel, Martín-Morales, Lorena, Fernández-Aceñero, María Jesús, Grolleman, Judith, Poves, Carmen, Llovet, Patricia, Tapial, Sandra, García-Barberán, Vanesa, Sanz, Julián, Pérez-Segura, Pedro, de Voer, Richarda M., Díaz-Rubio, Eduardo, de la Hoya, Miguel, Caldés, Trinidad, and Garre, Pilar

Published

2019

7. p53 and p63 Proteoforms Derived from Alternative Splicing Possess Differential Seroreactivity in Colorectal Cancer with Distinct Diagnostic Ability from the Canonical Proteins.

Author

Montero-Calle, Ana, Garranzo-Asensio, María, Torrente-Rodríguez, Rebeca M., Ruiz-Valdepeñas Montiel, Víctor, Poves, Carmen, Dziaková, Jana, Sanz, Rodrigo, Díaz del Arco, Cristina, Pingarrón, José Manuel, Fernández-Aceñero, María Jesús, Campuzano, Susana, and Barderas, Rodrigo

Subjects

PROTEIN metabolism, AUTOANTIBODIES, BIOSENSORS, BIOMARKERS, EXPERIMENTAL design, COLORECTAL cancer, IMMUNOASSAY, RESEARCH funding, POLYMERASE chain reaction, RECEIVER operating characteristic curves, BODY fluid examination, EARLY diagnosis

Abstract

Simple Summary: The humoral immune response in cancer has been demonstrated to be useful for distinguishing patients from healthy individuals using serum or plasma. Our study aimed to assess whether p53 and p63 proteoforms derived from alternative splicing could have a differential seroreactivity and higher diagnostic value than canonical proteins in colorectal cancer. Using luminescence assays and biosensing approaches with the proteoforms expressed in vitro fused to HaloTag, we demonstrate the appearance of a differential seroreactivity among the proteoforms in colorectal cancer patients. Our findings reveal increased complexity of the humoral immune response in cancer against specific autoantigens, since specific seroreactivity and different diagnostic values were observed among the p53 and p63 proteoforms and the canonical proteins. Colorectal cancer (CRC) is the third most common cancer and the second most frequent cause of cancer-related death worldwide. The detection in plasma samples of autoantibodies against specific tumor-associated antigens has been demonstrated to be useful for the early diagnosis of CRC by liquid biopsy. However, new studies related to the humoral immune response in cancer are needed to enable blood-based diagnosis of the disease. Here, our aim was to characterize the humoral immune response associated with the different p53 and p63 proteoforms derived from alternative splicing and previously described as aberrantly expressed in CRC. Thus, here we investigated the diagnostic ability of the twelve p53 proteoforms and the eight p63 proteoforms described to date, and their specific N-terminal and C-terminal end peptides, by means of luminescence HaloTag beads immunoassays. Full-length proteoforms or specific peptides were cloned as HaloTag fusion proteins and their seroreactivity analyzed using plasma from CRC patients at stages I-IV (n = 31), individuals with premalignant lesions (n = 31), and healthy individuals (n = 48). p53γ, Δ40p53β, Δ40p53γ, Δ133p53γ, Δ160p53γ, TAp63α, TAp63δ, ΔNp63α, and ΔNp63δ, together with the specific C-terminal end α and δ p63 peptides, were found to be more seroreactive against plasma from CRC patients and/or individuals with premalignant lesions than from healthy individuals. In addition, ROC (receiver operating characteristic) curves revealed a high diagnostic ability of those p53 and p63 proteoforms to detect CRC and premalignant individuals (AUC higher than 85%). Finally, electrochemical biosensing platforms were employed in POC-like devices to investigate their usefulness for CRC detection using selected p53 and p63 proteoforms. Our results demonstrate not only the potential of these biosensors for the simultaneous analysis of proteoforms' seroreactivity, but also their convenience and versatility for the clinical detection of CRC by liquid biopsy. In conclusion, we here show that p53 and p63 proteoforms possess differential seroreactivity in CRC patients in comparison to controls, distinctive from canonical proteins, which should improve the diagnostic panels for obtaining a blood-based biomarker signature for CRC detection. [ABSTRACT FROM AUTHOR]

Published

2023

8. In-depth proteomics characterization of ΔNp73 effectors identifies key proteins with diagnostic potential implicated in lymphangiogenesis, vasculogenesis and metastasis in colorectal cancer.

Author

Garranzo-Asensio, María, Rodríguez-Cobos, Javier, San Millán, Coral, Poves, Carmen, Fernández-Aceñero, María Jesús, Pastor-Morate, Daniel, Viñal, David, Montero-Calle, Ana, Solís-Fernández, Guillermo, Ceron, María-Ángeles, Gámez-Chiachio, Manuel, Rodríguez, Nuria, Guzmán-Aránguez, Ana, Barderas, Rodrigo, and Domínguez, Gemma

Abstract

Colorectal cancer (CRC) is the third most common cancer and the second leading cause of cancer-related death worldwide. Alterations in proteins of the p53-family are a common event in CRC. ΔNp73, a p53-family member, shows oncogenic properties and its effectors are largely unknown. We performed an in-depth proteomics characterization of transcriptional control by ΔNp73 of the secretome of human colon cancer cells and validated its clinical potential. The secretome was analyzed using high-density antibody microarrays and stable isotopic metabolic labeling. Validation was performed by semiquantitative PCR, ELISA, dot-blot and western blot analysis. Evaluation of selected effectors was carried out using 60 plasma samples from CRC patients, individuals carrying premalignant colorectal lesions and colonoscopy-negative controls. In total, 51 dysregulated proteins were observed showing at least 1.5-foldchange in expression. We found an important association between the overexpression of ΔNp73 and effectors related to lymphangiogenesis, vasculogenesis and metastasis, such as brain-derived neurotrophic factor (BDNF) and the putative aminoacyl tRNA synthase complex-interacting multifunctional protein 1 (EMAP-II)- vascular endothelial growth factor C-vascular endothelial growth factor receptor 3 axis. We further demonstrated the usefulness of BDNF as a potential CRC biomarker able to discriminate between CRC patients and premalignant individuals from controls with high sensitivity and specificity. [ABSTRACT FROM AUTHOR]

Published

2022

9. Mo1151 COLORECTAL ADENOMA PREVALENCE AND INCIDENCE IN LYNCH SYNDROME BY GENE

Author

Sanchez, Ariadna, Castillo, Joaquin, Roos, Victorine, Navarro, Matilde, Pineda, Marta, Oliva, Berta Caballol, Calle, Lorena Moreno, Carballal, Sabela, Rodriguez-Alonso, Lorena, Cajal, Teresa Ramon Y, Llort, Gemma, Piñol, Virginia, Lopez-Fernandez, Adrià, Salces, Inmaculada, Picó, Maria Dolores, Rivas, Laura, Bujanda, Luis, Garzon-Benavides, Marta, Pizarro, Angeles, De Castro, Eva M., Lopez-Arias, Maria Jesús, Poves, Carmen F., Garau, Catalina, Rodríguez-Alcalde, Daniel, Herraiz, Maite, Alvarez, Cristina, Rivas, Andres Dacal, Carrillo-Palau, Marta, Cid, Lucía, Ponce, Marta, Barreiro-Alonso, Eva, Saperas, Esteban, Aguirre, Elena, Ocaña, Teresa, Rivero, Liseth, Bessa, Xavier, Cubiella, Joaquin, Jover, Rodrigo, Rodriguez-Moranta, Francisco, Balmaña, Judit, Brunet, Joan, Castells, Antoni, Dekker, Evelien, Capella, Gabriel, Moreira, Leticia, Pellise, Maria, and Balaguer, Francesc

Published

2023

10. Mo1154 IS GASTRIC CANCER SCREENING NECESSARY IN LYNCH SYNDROME?

Author

Sanchez, Ariadna, Arango, Andres, Moreta, Maria Jose, Llach, Joan, Centeno, Mireia Diaz, Lopez-Fernandez, Adrià, Aguilera, Lara, Salces, Inmaculada, Llort, Gemma, Bujanda, Luis, Carrillo-Palau, Marta, Hernández, Goretti, Rodríguez-Alcalde, Daniel, Picó, Maria Dolores, Jover, Rodrigo, Poves, Carmen F., Barreiro-Alonso, Eva, Rivas, Andres Dacal, Herraiz, Maite, Cubiella, Joaquin, Piñol, Virginia, Peñas, Beatriz, Calle, Lorena Moreno, Rivero, Liseth, Ocaña, Teresa, Carballal, Sabela, Castells, Antoni, Pellise, Maria, Balaguer, Francesc, and Moreira, Leticia

Published

2023

11. 163 - ¿ES NECESARIO EL CRIBADO DE CÁNCER GÁSTRICO EN EL SÍNDROME DE LYNCH?

Author

Sánchez, Ariadna, Arango, Andres, Moreta, Maria José, Llach, Joan, Centeno, Mireia Diaz, Fernández, Adrià López, Salces, Inmaculada, Llort, Gemma, de Piérola, Luis Bujanda Fernández, Carrillo-Palau, Marta, Mesa, Goretti Hernández, Rodríguez-Alcalde, Daniel, Sala, Maria Dolores Pico, Jover, Rodrigo, Poves, Carmen, Barreiro-Alonso, Eva, Rivas, Andres Dacal, Bayod, Maite Herraiz, Cubiella, Joaquin, Piñol, Virginia, Peñas, Beatriz, Moreno, Lorena, Sánchez, Liseth Rivero, Ocaña, Teresa, Carballal, Sabela, Castells, Antoni, Urquiza, María Pellisé, Balaguer, Francesc, and Ruiz, Leticia Moreira

Published

2023

12. INCIDENCIA, TASA DE DETECCIÓN DE ADENOMAS Y FACTORES DE RIESGO DE CRC SEGÚN EL GEN AFECTO EN EL SÍNDROME DE LYNCH

Author

Sánchez, Ariadna, Castillo, Joaquin, Roos, Victorine H., Dueñas, Núria, Pineda, Marta, Caballol, Berta, Moreno, Lorena, Carballal, Sabela, Rodríguez-Alonso, Lorena, Cajal, Teresa Ramón y, Llort, Gemma, Piñol, Virginia, Fernández, Adrià López, Salces, Inmaculada, Picó, Maria Dolores, Rivas, Laura, Bujanda, Luis, Garzón, Marta, Pizarro, Angeles, de Castro, Eva Martínez, López-Arias, Maria Jesus, Poves, Carmen, Garau, Catalina, Alcalde, Daniel Rodríguez, Herraiz, Maite, Alvarez-Urrutia, Cristina, Dacal, Andrés, Carrillo-Palau, Marta, Cid, Lucia, Ponce, Marta, Barreiro-Alonso, Eva, Saperas, Esteban, Aguirre, Elena, Ocaña, Teresa, Sánchez, Liseth Rivero, Bessa, Xavier, Cubiella, Joaquin, Jover, Rodrigo, Rodríguez-Moranta, Francisco, Balmaña, Judith, Brunet, Joan, Castells, Antoni, Dekker, Evelien, Capella, Gabriel, Moreira, Leticia, Pellise, Maria, and Balaguer, Francesc

Published

2023

13. Colonoscopy versus Fecal Immunochemical Testing in Colorectal-Cancer Screening

Author

Quintero, Enrique, Castells, Antoni, Bujanda, Luis, Cubiella, Joaquín, Salas, Dolores, Lanas, Ángel, Andreu, Montserrat, Carballo, Fernando, Morillas, Juan Diego, Hernández, Cristina, Jover, Rodrigo, Montalvo, Isabel, Arenas, Juan, Laredo, Eva, Hernández, Vicent, Iglesias, Felipe, Cid, Estela, Zubizarreta, Raquel, Sala, Teresa, Ponce, Marta, Andrés, Mercedes, Teruel, Gloria, Peris, Antonio, Roncales, María-Pilar, Polo-Tomás, Mónica, Bessa, Xavier, Ferrer-Armengou, Olga, Grau, Jaume, Serradesanferm, Anna, Ono, Akiko, Cruzado, José, Pérez-Riquelme, Francisco, Alonso-Abreu, Inmaculada, de la Vega-Prieto, Mariola, Reyes-Melian, Juana Maria, Cacho, Guillermo, Díaz-Tasende, José, Herreros-de-Tejada, Alberto, Poves, Carmen, Santander, Cecilio, and González-Navarro, Andrés

Published

2012

14. 598 POST-COLONOSCOPY COLORECTAL CANCER IN LYNCH SYNDROME IS ASSOCIATED WITH QUALITY ISSUES DURING SURVEILLANCE

Author

Garcia, Ariadna Sanchez, Navarro, Matilde, Roos, Victorine, Pineda, Marta, Caballol, Berta, Moreno, Lorena, Ocaña, Teresa, Rodriguez-Moranta, Francisco, Rodriguez-Alonso, Lorena, Cajal, Teresa Ramon y, Llort, Gemma, Picó, Maria Dolores, Jover, Rodrigo, Fernandez, Adrià Lopez, de Castro, Eva Martinez, Lopez-Arias, Maria Jesús, Alvarez, Cristina, Bessa, Xavier, Rivas, Laura, Cubiella, Joaquin, Rodríguez-Alcalde, Daniel, Dacal, Andres, Herraiz, Maite, Garau, Catalina, Bujanda, Luis, Cid, Lucía, Povés, Carmen, Garzon, Marta, Pizarro, Angeles, Salces, Inmaculada, Ponce, Marta, Carrillo-Palau, Marta, Aguirre, Elena, Saperas, Esteban, Suarez, Adolfo, Piñol, Virginia, Carballal, Sabela, Rivero, Liseth, Balmaña, Judit, Brunet, Joan, Castells, Antoni, Dekker, Evelien, Pellise, Maria, Capella, Gabriel, Serra, Miquel, Moreira, Leticia, and Balaguer, Francesc

Published

2020

15. High incidence of advanced colorectal neoplasia during endoscopic surveillance in serrated polyposis syndrome.

Author

Rodríguez-Alcalde, Daniel, Carballal, Sabela, Moreira, Leticia, Hernández, Luis, Rodríguez-Alonso, Lorena, Rodríguez-Moranta, Francisco, Gonzalo, Victoria, Bujanda, Luis, Bessa, Xavier, Poves, Carmen, Cubiella, Joaquín, Castro, Inés, González, Mariano, Moya, Eloísa, Oquiñena, Susana, Clofent, Joan, Quintero, Enrique, Esteban, Pilar, Piñol, Virginia, and Fernández, Francisco Javier

Subjects

COLON cancer, COLONOSCOPY, COLECTOMY

Abstract

Background Serrated polyposis syndrome (SPS) has been associated with an increased risk of colorectal cancer (CRC). Accordingly, intensive surveillance with annual colonoscopy is advised. The aim of this multicenter study was to describe the risk of advanced lesions in SPS patients undergoing surveillance, and to identify risk factors that could guide the prevention strategy. Methods From March 2013 to April 2015, 296 patients who fulfilled criteria I and/or III for SPS were retrospectively recruited at 18 centers. We selected patients in whom successful clearing colonoscopy had been performed and who underwent subsequent endoscopic surveillance. Advanced neoplasia was defined as CRC, advanced adenoma, or advanced serrated lesion that were = 10mm and/or with dysplasia. Cumulative incidence of advanced neoplasia was calculated and independent predictors of advanced neoplasia development were identified. Results In 152 SPS patients a total of 315 surveillance colonoscopies were performed (median 2, range 1 - 7). The 3-year cumulative incidence of CRC and advanced neoplasia were 3.1% (95% confidence interval [CI] 0 - 6.9) and 42.0% (95%CI 32.4 - 51.7), respectively. Fulfilling both I + III criteria and the presence of advanced serrated lesions at baseline colonoscopy were independent predictors of advanced neoplasia development (odds ratio [OR] 1.85, 95 %CI 1.03 - 3.33, P = 0.04 and OR 2.62, 95 %CI 1.18 - 5.81, P = 0.02, respectively). During follow-up, nine patients (5.9 %) were referred for surgery for invasive CRC (n = 4, 2.6 %) or because of polyp burden (n = 5, 3.3 %). After total colectomy, 17.9% patients developed advanced neoplasia in the retained rectum. Conclusions Patients with SPS have a substantial risk of developing advanced neoplasia under endoscopic surveillance, whereas CRC incidence is low. Personalized endoscopic surveillance based on polyp burden and advanced serrated histology could help to optimize prevention in patients with SPS. [ABSTRACT FROM AUTHOR]

Published

2019

16. Mo1736 - Identification of Clinical, Genetic and Endoscopic Predictors of Incident Colorectal Cancer in Lynch Syndrome

Author

Sanchez, Ariadna, Navarro, Matilde, Moreno, Lorena, Ocaña, Teresa, Pineda, Marta, Rodriguez-Moranta, Francisco, Rodriguez-Alonso, Lorena, Cajal, Teresa Ramon y, llort, Gemma, Yagüe, Carme, Picó, Maria Dolores, Jover, Rodrigo, Fernandez, Adrià Lopez, de Castro, Eva Martinez, Alvarez, Cristina, Bessa, Xavier, Rivas, Laura, Cubiella, Joaquin, Rodríguez-Alcalde, Daniel, Dacal, Andres, Herraiz, Maite, Garau, Catalina, Bujanda, Luis, Cid, Lucía, Povés, Carmen, Garzon, Marta, Pizarro, Angeles, Salces, Inmaculada, Ponce, Marta, Carrillo-Palau, Marta, Aguirre, Elena, Saperas, Esteban, Suarez, Adolfo, Piñol, Virginia, Gisbert-Beamud, Alexandra, Carballal, Sabela, Rivero, Liseth, Pellise, Maria, Balmaña, Judit, Brunet, Joan, Castells, Antoni, Capellà, Gabriel, Moreira, Leticia, Serra-Burriel, Miquel, and Balaguer, Francesc

Published

2018

17. 1071 - Clinical and Molecular Characterization of Lynch-Like Syndrome

Author

Picó, Maria Dolores, Jover, Rodrigo, Murcia, Oscar, Giner-Calabuig, Mar, Alustiza, Miren, Soto, Jose Luis, Castillejo, Adela, Sánchez, Ana Beatriz, Sanchez, Ariadna, Balaguer, Francesc, Moreira, Leticia, Castells, Antoni, Pellise, Maria, Carrillo-Palau, Marta, Gisbert-Beamud, Alexandra, Cajal, Teresa Ramon y, llort, Gemma, Yagüe, Carme, Fernandez, Adrià Lopez, Balmaña, Judit, de Castro, Eva Martinez, Alvarez, Cristina, Bessa, Xavier, Cubiella, Joaquin, Rivas, Laura, Rodríguez-Alcalde, Daniel, Dacal, Andres, Herraiz, Maite, Garau, Catalina, Bujanda, Luis, Cid, Lucía, Povés, Carmen, Garzon, Marta, Pizarro, Angeles, Salces, Inmaculada, Ponce, Marta, Aguirre, Elena, Saperas, Esteban, and Piñol, Virginia

Published

2018

18. Carcinoid tumor and patent foramen ovale

Author

Ramos-Leví, Ana María, Díaz-Pérez, José A., Poves, Carmen, and Bover, Ramón

Published

2011

19. Su1768 - Colorectal Cancer Incidence in Lynch Syndrome Patients: First Report of a Multicenter Nation-Wide Study

Author

Sanchez, Ariadna, Navarro, Matilde, Ocaña, Teresa, Pineda, Marta, Rodriguez-Moranta, Francisco, Soriano, Antonio, Cajal, Teresa Ramon y, llort, Gemma, Yagüe, Carme, Picó, Maria Dolores, Jover, Rodrigo, Fernandez, Adrià Lopez, de Castro, Eva Martinez, Alvarez, Cristina, Bessa, Xavier, Rivas, Laura, Rodríguez-Alcalde, Daniel, Dacal, Andres, Herraiz, Maite, Garau, Catalina, Bujanda, Luis, Cid, Lucia, Povés, Carmen, Garzon, Marta, Pizarro, Angeles, Gomez, Antonio, Salces, Inmaculada, Ponce, Marta, Carrillo-Palau, Marta, Aguirre, Elena, Saperas, Esteve, Marnrique, Anna Virgili, Masferrer, David Fisas, Piñol, Virginia, Carballal, Sabela, Rivero, Liseth, Pellise, Maria, Serra, Miquel, Balmaña, Judit, Capellà, Gabriel, Brunet, Joan, Castells, Antoni, Moreira, Leticia, and Balaguer, Francesc

Published

2017

20. Role of GALNT12 in the genetic predisposition to attenuated adenomatous polyposis syndrome.

Author

Lorca, Víctor, Rueda, Daniel, Martín-Morales, Lorena, Poves, Carmen, Fernández-Aceñero, María Jesús, Ruiz-Ponte, Clara, Llovet, Patricia, Marrupe, David, García-Barberán, Vanesa, García-Paredes, Beatriz, Pérez-Segura, Pedro, de la Hoya, Miguel, Díaz-Rubio, Eduardo, Caldés, Trinidad, and Garre, Pilar

Subjects

COLON cancer, ADENOMATOUS polyposis coli, PHENOTYPES, GLYCOMICS, GERM cells, NUCLEOTIDE sequencing

Abstract

The involvement of GALNT12 in colorectal carcinogenesis has been demonstrated but it is not clear to what extent it is implicated in familial CRC susceptibility. Partially inactivating variant, NM_024642.4:c.907G>A, p.(D303N), has been previously detected in familial CRC and proposed as the causative risk allele. Since phenotypes of the described carrier families showed not only CRC but also a polyp history, we hypothesized that GALNT12 could be involved in adenoma predisposition and consequently, in hereditary polyposis CRC syndromes. For that purpose, we have screened the GALNT12 gene in germline DNA from 183 unrelated attenuated polyposis patients. c.907G>A, p.(D303N) was detected in 4 cases (MAF = 1.1%) and no other candidate variants were found. After segregation studies, LOH analyses, glycosylation pattern tests and case-control studies, our results did not support the role of c.907G>A, p.(D303N) as a high-penetrance risk allele for polyposis CRC. [ABSTRACT FROM AUTHOR]

Published

2017

21. 1065 Incidence of Colonic Neoplasia in Patients With Serrated Polyposis Syndrome Who Undergo Endoscopic Surveillance: A Multicenter Study

Author

Carballal, Sabela, Rodríguez-Alcalde, Daniel, Moreira, Leticia, Hernández, Luis, Rodríguez, Lorena, Rodriguez-Moranta, Francisco, Gonzalo, Victoria, Bujanda, Luis, Bessa, Xavier, Poves, Carmen, Cubiella, Joaquín, Castro, Ines, Gonzalez, Mariano, Moya, Eloisa, Oquiñena, Susana, Clofent, Joan, Quintero, Enrique, Esteban, Pilar, Piñol, Virginia, Fernandez, Francisco Javier, Jover, Rodrigo, Cid, Lucía, Saperas, Esteve, Cuatrecasas, Miriam, Lopez-Ceron, Maria, López-Vicente, Jorge, Leoz, María Liz, Sanchez, Liseth Rivero, Castells, Antoni, Pellise, Maria, and Balaguer, Francesc

Published

2016

22. Colorectal cancer risk factors in patients with serrated polyposis syndrome: a large multicentre study.

Author

Carballal, Sabela, Rodríguez-Alcalde, Daniel, Moreira, Leticia, Hernández, Luis, Rodríguez, Lorena, Rodríguez-Moranta, Francisco, Gonzalo, Victoria, Bujanda, Luis, Bessa, Xavier, Poves, Carmen, Cubiella, Joaquin, Castro, Inés, González, Mariano, Moya, Eloísa, Oquiñena, Susana, Clofent, Joan, Quintero, Enrique, Esteban, Pilar, Piñol, Virginia, and Fernández, Francisco Javier

Subjects

COLON cancer risk factors, LARGE intestine diseases, COLON cancer prevention, HISTOPATHOLOGY, FOLLOW-up studies (Medicine)

Published

2016

23. ΔNp73, TAp73 and Δ133p53 Extracellular Vesicle Cargo as Early Diagnosis Markers in Colorectal Cancer.

Author

Rodríguez-Cobos, Javier, Viñal, David, Poves, Carmen, Fernández-Aceñero, María J., Peinado, Héctor, Pastor-Morate, Daniel, Prieto, Mª Isabel, Barderas, Rodrigo, Rodríguez-Salas, Nuria, Domínguez, Gemma, Bourdon, Jean-Christophe, and Slade, Neda

Subjects

COLON tumors, BLOOD plasma, RECTUM tumors, EARLY detection of cancer, CANCER patients, MESSENGER RNA, EXTRACELLULAR space, TUMOR markers, TUMOR antigens, BODY fluid examination, PRECANCEROUS conditions, EARLY diagnosis

Abstract

Simple Summary: The survival of colorectal cancer patients largely relies on the stage at diagnosis. The identification of early and non-invasive biomarkers to be used in screening programs for the diagnosis of the disease at the premalignant stage is mandatory. The aim of this study is to validate in plasma-derived extracellular vesicles secreted by malignant cells the diagnostic potential of well-known tumor-associated genes, ΔNp73, TAp73, and Δ133p53, in healthy subjects (n = 29), individuals with premalignant lesions (n = 49), and colorectal cancer patients (n = 42). Our data support ΔNp73 levels contained in extracellular vesicles as such a non-invasive and premature biomarker for the early diagnosis of colorectal cancer. The early diagnosis of colorectal cancer is a key factor in the overall survival of the patients. The actual screening programs include different approaches with significant limitations such as unspecificity, high invasiveness, and detection at late stages of the disease. The specific content of extracellular vesicles derived from malignant cells may represent a non-invasive technique for the early detection of colorectal cancer. Here, we studied the mRNA levels of ΔNp73, TAp73, and Δ133p53 in plasma-derived extracellular vesicles from healthy subjects (n = 29), individuals with premalignant lesions (n = 49), and colorectal cancer patients (n = 42). Extracellular vesicles' ΔNp73 levels were already significantly high in subjects with premalignant lesions. Δ133p53 levels were statistically increased in colorectal cancer patients compared to the other two groups and were associated with patients' survival. Remarkably, TAp73 mRNA was not detected in any of the individuals. The evaluation of ΔNp73, Δ133p53 and CEA sensitivity, specificity and AUC values supports ΔNp73 as a better early diagnosis biomarker and CEA as the best to identify advanced stages. Thus, low levels of CEA and a high content of ΔNp73 may identify in screening programs those individuals at higher risk of presenting a premalignant lesion. In addition, Δ133p53 emerges as a potential prognosis biomarker in colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2021

24. High incidence of advanced colorectal neoplasia during endoscopic surveillance in serrated polyposis syndrome.

Author

Rodríguez-Alcalde, Daniel, Carballal, Sabela, Moreira, Leticia, Hernández, Luis, Rodríguez-Alonso, Lorena, Rodríguez-Moranta, Francisco, Gonzalo, Victoria, Bujanda, Luis, Bessa, Xavier, Poves, Carmen, Cubiella, Joaquín, Castro, Inés, González, Mariano, Moya, Eloísa, Oquiñena, Susana, Clofent, Joan, Quintero, Enrique, Esteban, Pilar, Piñol, Virginia, and Fernández, Francisco Javier

Abstract

Background: Serrated polyposis syndrome (SPS) has been associated with an increased risk of colorectal cancer (CRC). Accordingly, intensive surveillance with annual colonoscopy is advised. The aim of this multicenter study was to describe the risk of advanced lesions in SPS patients undergoing surveillance, and to identify risk factors that could guide the prevention strategy.Methods: From March 2013 to April 2015, 296 patients who fulfilled criteria I and/or III for SPS were retrospectively recruited at 18 centers. We selected patients in whom successful clearing colonoscopy had been performed and who underwent subsequent endoscopic surveillance. Advanced neoplasia was defined as CRC, advanced adenoma, or advanced serrated lesion that were ≥ 10 mm and/or with dysplasia. Cumulative incidence of advanced neoplasia was calculated and independent predictors of advanced neoplasia development were identified.Results: In 152 SPS patients a total of 315 surveillance colonoscopies were performed (median 2, range 1 - 7). The 3-year cumulative incidence of CRC and advanced neoplasia were 3.1 % (95 % confidence interval [CI] 0 - 6.9) and 42.0 % (95 %CI 32.4 - 51.7), respectively. Fulfilling both I + III criteria and the presence of advanced serrated lesions at baseline colonoscopy were independent predictors of advanced neoplasia development (odds ratio [OR] 1.85, 95 %CI 1.03 - 3.33, P  = 0.04 and OR 2.62, 95 %CI 1.18 - 5.81, P  = 0.02, respectively). During follow-up, nine patients (5.9 %) were referred for surgery for invasive CRC (n = 4, 2.6 %) or because of polyp burden (n = 5, 3.3 %). After total colectomy, 17.9 % patients developed advanced neoplasia in the retained rectum.Conclusions: Patients with SPS have a substantial risk of developing advanced neoplasia under endoscopic surveillance, whereas CRC incidence is low. Personalized endoscopic surveillance based on polyp burden and advanced serrated histology could help to optimize prevention in patients with SPS. [ABSTRACT FROM AUTHOR]

Published

2018

25. In-Depth Proteomic Analysis of Paraffin-Embedded Tissue Samples from Colorectal Cancer Patients Revealed TXNDC17 and SLC8A1 as Key Proteins Associated with the Disease.

Author

Montero-Calle A, Garranzo-Asensio M, Poves C, Sanz R, Dziakova J, Peláez-García A, de Los Ríos V, Martinez-Useros J, Fernández-Aceñero MJ, and Barderas R

Subjects

Aged, Animals, Female, Humans, Male, Middle Aged, Adenocarcinoma metabolism, Adenocarcinoma pathology, Adenoma pathology, Adenoma metabolism, Cell Line, Tumor, Gene Expression Regulation, Neoplastic, Paraffin Embedding, Biomarkers, Tumor metabolism, Colorectal Neoplasms pathology, Colorectal Neoplasms metabolism, Proteomics methods, Thioredoxins metabolism, Sodium-Calcium Exchanger metabolism

Abstract

A deeper understanding of colorectal cancer (CRC) biology would help to identify specific early diagnostic markers. Here, we conducted quantitative proteomics on FFPE healthy, adenoma, and adenocarcinoma tissue samples from six stage I sporadic CRC patients to identify dysregulated proteins during early CRC development. Two independent quantitative 10-plex TMT experiments were separately performed. After protein extraction, trypsin digestion, and labeling, proteins were identified and quantified by using a Q Exactive mass spectrometer. A total of 2681 proteins were identified and quantified after data analysis and bioinformatics with MaxQuant and the R program. Among them, 284 and 280 proteins showed significant upregulation and downregulation (expression ratio ≥1.5 or ≤0.67, p -value ≤0.05), respectively, in adenoma and/or adenocarcinoma compared to healthy tissue. Ten dysregulated proteins were selected to study their role in CRC by WB, IHC, TMA, and ELISA using tissue and plasma samples from CRC patients, individuals with premalignant colorectal lesions (adenomas), and healthy individuals. In vitro loss-of-function cell-based assays and in vivo experiments using three CRC cell lines with different metastatic properties assessed the important roles of SLC8A1 and TXNDC17 in CRC and liver metastasis. Additionally, SLC8A1 and TXNDC17 protein levels in plasma possessed the diagnostic ability of early CRC stages.

Published

2024

26. Fecal occult blood and calprotectin testing to prioritize primary care patients for colonoscopy referral: The advantage study.

Author

Lanas Á, Balaguer F, Sánchez-Luengo M, Hijos-Mallada G, Hernández-Mesa G, Piñero M, Castillo J, Ocaña T, Cubiella J, Crespo A, Iglesias Á, Medeiros I, Cacho G, Jover-Martínez R, Alustiza M, Diaz-Tasende J, Poves C, Macedo G, and Quintero E

Subjects

Humans, Prospective Studies, Leukocyte L1 Antigen Complex, Referral and Consultation, Primary Health Care, Occult Blood, Colonoscopy

Abstract

Background: Colonoscopy is the gold standard for colorectal cancer (CRC) diagnosis and screening, but endoscopy services are usually overburdened. This study aims to investigate the usefulness of fecal hemoglobin (fHb) and calprotectin (FC) for the identification of patients with high probability of CRC who need urgent referral., Methods: In a multicenter prospective study, we enrolled symptomatic patients referred from primary care for colonoscopy. Prior to bowel preparation, fHb and FC quantitative tests were performed. The diagnostic performance was estimated for each biomarker/combination. We built a multivariable predictive model based on logistic regression, translated to a nomogram and a risk calculator to assist clinicians in the decision-making process., Results: The study included 1224 patients, of whom 69 (5.6%) had CRC. At the fHb cut-offs of >0 and 10 μg/g, the negative predictive values for CRC were 98.8% (95% confidence interval 97.8%-99.3%) and 98.6% (95%CI 97.7%-99.1%), and the sensitivities were 85.5% (95%CI 75.0%-92.8%) and 79.7% (95%CI 68.3%-88.4%), respectively. When we added the cut-off of 150 μg/g of FC to both fHb thresholds, the sensitivity of fecal tests improved. In the multivariate logistic regression model, the concentration of fHb was an independent predictor for CRC; age and gender were also independently associated with CRC., Conclusions: fHb and FC are useful as part of a triage tool to identify those symptomatic patients with high probability of CRC. This can be easily applied by physicians to prioritize high-risk patients for urgent colonoscopy., (© 2023 The Authors. United European Gastroenterology Journal published by Wiley Periodicals LLC on behalf of United European Gastroenterology.)

Published

2023

27. In-depth proteomics characterization of ∆Np73 effectors identifies key proteins with diagnostic potential implicated in lymphangiogenesis, vasculogenesis and metastasis in colorectal cancer.

Author

Garranzo-Asensio M, Rodríguez-Cobos J, San Millán C, Poves C, Fernández-Aceñero MJ, Pastor-Morate D, Viñal D, Montero-Calle A, Solís-Fernández G, Ceron MÁ, Gámez-Chiachio M, Rodríguez N, Guzmán-Aránguez A, Barderas R, and Domínguez G

Subjects

Brain-Derived Neurotrophic Factor metabolism, Humans, Proteomics, Tumor Suppressor Protein p53, Vascular Endothelial Growth Factor A metabolism, Vascular Endothelial Growth Factor C metabolism, Colorectal Neoplasms genetics, Lymphangiogenesis

Abstract

Colorectal cancer (CRC) is the third most common cancer and the second leading cause of cancer-related death worldwide. Alterations in proteins of the p53-family are a common event in CRC. ΔNp73, a p53-family member, shows oncogenic properties and its effectors are largely unknown. We performed an in-depth proteomics characterization of transcriptional control by ∆Np73 of the secretome of human colon cancer cells and validated its clinical potential. The secretome was analyzed using high-density antibody microarrays and stable isotopic metabolic labeling. Validation was performed by semiquantitative PCR, ELISA, dot-blot and western blot analysis. Evaluation of selected effectors was carried out using 60 plasma samples from CRC patients, individuals carrying premalignant colorectal lesions and colonoscopy-negative controls. In total, 51 dysregulated proteins were observed showing at least 1.5-foldchange in expression. We found an important association between the overexpression of ∆Np73 and effectors related to lymphangiogenesis, vasculogenesis and metastasis, such as brain-derived neurotrophic factor (BDNF) and the putative aminoacyl tRNA synthase complex-interacting multifunctional protein 1 (EMAP-II)-vascular endothelial growth factor C-vascular endothelial growth factor receptor 3 axis. We further demonstrated the usefulness of BDNF as a potential CRC biomarker able to discriminate between CRC patients and premalignant individuals from controls with high sensitivity and specificity., (© 2022 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published

2022

28. Multiplexed monitoring of a novel autoantibody diagnostic signature of colorectal cancer using HaloTag technology-based electrochemical immunosensing platform.

Author

Garranzo-Asensio M, Guzmán-Aránguez A, Povedano E, Ruiz-Valdepeñas Montiel V, Poves C, Fernandez-Aceñero MJ, Montero-Calle A, Solís-Fernández G, Fernandez-Diez S, Camps J, Arenas M, Rodríguez-Tomàs E, Joven J, Sanchez-Martinez M, Rodriguez N, Dominguez G, Yáñez-Sedeño P, Pingarrón JM, Campuzano S, and Barderas R

Subjects

Antibody Specificity, Antigens, Neoplasm immunology, Area Under Curve, Asymptomatic Diseases, Biomarkers, Tumor, Breast Neoplasms blood, Colorectal Neoplasms blood, Colorectal Neoplasms immunology, Electrochemical Techniques instrumentation, Electrodes, Female, Humans, Hydroquinones, Immobilized Proteins immunology, Lung Neoplasms blood, Male, ROC Curve, Recombinant Fusion Proteins immunology, Sensitivity and Specificity, Antibodies, Neoplasm blood, Autoantibodies blood, Biosensing Techniques, Colorectal Neoplasms diagnosis, Electrochemical Techniques methods

Abstract

Background and Purpose : The humoral immune response in cancer patients can be used for early detection of the disease. Autoantibodies raised against tumor-associated antigens (TAAs) are promising clinical biomarkers for reliable cancer diagnosis, prognosis, and therapy monitoring. In this study, an electrochemical disposable multiplexed immunosensing platform able to integrate difficult- and easy-to-express colorectal cancer (CRC) TAAs is reported for the sensitive determination of eight CRC-specific autoantibodies. Methods : The electrochemical immunosensing approach involves the use of magnetic microcarriers (MBs) as solid supports modified with covalently immobilized HaloTag fusion proteins for the selective capture of specific autoantibodies. After magnetic capture of the modified MBs onto screen-printed carbon working electrodes, the amperometric responses measured using the hydroquinone (HQ)/H 2 O 2 system were related to the levels of autoantibodies in plasma. Results : The biosensing platform was applied to the analysis of autoantibodies against 8 TAAs described for the first time in this work in plasma samples from healthy asymptomatic individuals (n=3), and patients with high-risk of developing CRC (n=3), and from patients already diagnosed with colorectal (n=3), lung (n=2) or breast (n=2) cancer. The developed bioplatform demonstrated an improved discrimination between CRC patients and controls (asymptomatic healthy individuals and breast and lung cancer patients) compared to an ELISA-like luminescence test. Conclusions : The proposed methodology uses a just-in-time produced protein in a simpler protocol, with low sample volume, and involves cost-effective instrumentation, which could be used in a high-throughput manner for reliable population screening to facilitate the detection of early CRC patients at affordable cost., Competing Interests: Competing Interests: The authors have declared that no competing interest exists., (© The author(s).)

Published

2020

29. Relationship of colonoscopy-detected serrated polyps with synchronous advanced neoplasia in average-risk individuals.

Author

Álvarez C, Andreu M, Castells A, Quintero E, Bujanda L, Cubiella J, Salas D, Lanas Á, Carballo F, Morillas JD, Hernández C, Jover R, Sarasqueta C, Enriquéz-Navascués JM, Hernández V, Estévez P, Macenlle R, Sala T, Balaguer F, Pellisé M, Moreira L, Gil I, Peris A, González-Rubio F, Ferrández A, Poves C, Ponce M, Grau J, Serradesanferm A, Ono A, Cruzado J, Pérez-Riquelme F, Alonso-Abreu I, Carrillo-Palau M, Santander C, Díaz Tasende J, Herreros A, Cacho G, Barranco LE, and Bessa X

Subjects

Adenoma pathology, Aged, Carcinoma pathology, Colonic Neoplasms diagnosis, Colonic Neoplasms pathology, Colonic Polyps pathology, Colonoscopy, Colorectal Neoplasms pathology, Female, Humans, Male, Mass Screening, Middle Aged, Neoplasms, Multiple Primary pathology, Risk Factors, Sex Factors, Adenoma diagnosis, Carcinoma diagnosis, Colonic Polyps diagnosis, Colorectal Neoplasms diagnosis, Neoplasms, Multiple Primary diagnosis

Abstract

Background: Serrated cancers account for 10% to 20% of all colorectal cancers (CRC) and more than 30% of interval cancers. The presence of proximal serrated polyps and large (≥10 mm) serrated polyps (LSP) has been correlated with colorectal neoplasia., Objective: To evaluate the prevalence of serrated polyps and their association with synchronous advanced neoplasia in a cohort of average-risk population and to assess the efficacy of one-time colonoscopy and a biennial fecal immunochemical test for reducing CRC-related mortality. This study focused on the sample of 5059 individuals belonging to the colonoscopy arm., Design: Multicenter, randomized, controlled trial., Setting: The ColonPrev study, a population-based, multicenter, nationwide, randomized, controlled trial., Patients: A total of 5059 asymptomatic men and women aged 50 to 69 years., Intervention: Colonoscopy., Main Outcome Measurements: Prevalence of serrated polyps and their association with synchronous advanced neoplasia., Results: Advanced neoplasia was detected in 520 individuals (10.3%) (CRC was detected in 27 [0.5%] and advanced adenomas in 493 [9.7%]). Serrated polyps were found in 1054 individuals (20.8%). A total of 329 individuals (6.5%) had proximal serrated polyps, and 90 (1.8%) had LSPs. Proximal serrated polyps or LSPs were associated with male sex (odds ratio [OR] 2.08, 95% confidence interval [CI], 1.76-4.45 and OR 1.65, 95% CI, 1.31-2.07, respectively). Also, LSPs were associated with advanced neoplasia (OR 2.49, 95% CI, 1.47-4.198), regardless of their proximal (OR 4.15, 95% CI, 1.69-10.15) or distal (OR 2.61, 95% CI, 1.48-4.58) locations. When we analyzed subtypes of serrated polyps, proximal hyperplasic polyps were related to advanced neoplasia (OR 1.61, 95% CI, 1.13-2.28), although no correlation with the location of the advanced neoplasia was observed., Limitations: Pathology criteria for the diagnosis of serrated polyps were not centrally reviewed. The morphology of the hyperplasic polyps (protruded or flat) was not recorded. Finally, because of the characteristics of a population-based study carried out in average-risk patients, the proportion of patients with CRC was relatively small., Conclusion: LSPs, but not proximal serrated polyps, are associated with the presence of synchronous advanced neoplasia. Further studies are needed to determine the risk of proximal hyperplastic polyps., (Copyright © 2013 American Society for Gastrointestinal Endoscopy. Published by Mosby, Inc. All rights reserved.)

Published

2013

30. [Carcinoid tumor and patent foramen ovale].

Author

Ramos-Leví AM, Díaz-Pérez JA, Poves C, and Bover R

Subjects

Aged, Antineoplastic Agents, Hormonal therapeutic use, Capsule Endoscopy, Carcinoid Tumor diagnosis, Carcinoid Tumor diagnostic imaging, Carcinoid Tumor drug therapy, Carcinoid Tumor secondary, Foramen Ovale, Patent diagnosis, Foramen Ovale, Patent diagnostic imaging, Foramen Ovale, Patent surgery, Heart Valve Prosthesis Implantation, Humans, Jejunal Neoplasms diagnosis, Liver Neoplasms diagnostic imaging, Liver Neoplasms secondary, Male, Malignant Carcinoid Syndrome etiology, Pulmonary Edema prevention & control, Somatostatin analogs & derivatives, Somatostatin therapeutic use, Tomography, Emission-Computed, Single-Photon, Tricuspid Valve Insufficiency diagnostic imaging, Tricuspid Valve Insufficiency surgery, Ultrasonography, Carcinoid Tumor complications, Dyspnea etiology, Endomyocardial Fibrosis etiology, Foramen Ovale, Patent complications, Jejunal Neoplasms complications, Tricuspid Valve Insufficiency etiology

Published

2011