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1. Signaling pathways in CRC

Author: Sacristán Santos, Víctor, primary, Martínez Lago, Nieves, additional, Pazos García, Carla, additional, Pazos García, Alejandro, additional, and Antón Aparicio, Luis M., additional
Published: 2022
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2. Contributors

Author: Aguilar, José Francisco Noguera, primary, Alhayek-Aí, Mohammed, additional, Alonso Aguirre, Pedro A., additional, Álvarez-Chaver, Paula, additional, Alvarez-Gonzalez, Sara, additional, Álvarez-Santullano, Lucía, additional, Alvariño, Javier Castro, additional, Amigo, Jorge, additional, Antón Aparicio, Luis M., additional, Aptsiauri, Natalia, additional, Ares, María Sánchez, additional, Balea, Begoña Campos, additional, Balo, Paula Vieiro, additional, Barcia, Lucía, additional, Bou, Germán, additional, Barreiro, Vanesa Balboa, additional, Bendayán, Isaac Martínez, additional, Bernal, Mónica, additional, Briones, Pedro Carpintero, additional, Brozos-Vázquez, Elena, additional, Bueno, Begoña Bravo, additional, Burundarena, Alba, additional, Caamaño, Antonio Gómez, additional, Calviño, José Manuel Mera, additional, Calvo, Marcos, additional, Candamio-Folgar, Sonia, additional, Cardelle-Cobas, Alejandra, additional, Carracedo, Ángel, additional, Carrasco, Ainhoa, additional, Castro, Álvaro Gómez, additional, Castro, Ana María Carballo, additional, Cepeda, Alberto, additional, Cepeda-Emiliani, Alfonso, additional, Concha, Ángel, additional, Conde, Benito González, additional, Cordero, Oscar J., additional, Cortés, Alberto Centeno, additional, Cotoré, Jesús Paredes, additional, Crespo, Patricia Calvo, additional, de Castro, Alain García, additional, De Chiara, Loretta, additional, de la Ballina González, Enrique González, additional, de Llano, Sofía Rodríguez Martínez, additional, Deben, Manuel Núñez, additional, del Carmen Corujeira Rivera, M., additional, Díaz, Cristina Méndez, additional, Díaz, Sonia Pértega, additional, Diéguez, Leticia García, additional, D'Jesús, Antonio Rodríguez, additional, Dourado, Ramón Vázquez, additional, Dovigo, Alba Gómez, additional, Fajardo, Paloma Sosa, additional, Fernández, Nereida Fernández, additional, Fernández, Rafaela Soler, additional, Fernández, Rosalía, additional, Fernández, Sergio Manuel Estévez, additional, Fernandez-Lozano, Carlos, additional, Fernández-Rozadilla, Ceres, additional, Ferreiro, Raquel Sardina, additional, Ferreiro, Silvia Varela, additional, Figueiras, Roberto García, additional, Figueroa, Angélica, additional, Fontoira, Lydia Fraga, additional, Franco, Carlos M.N, additional, Gallardo-Gómez, María, additional, García, Concepción Crespo, additional, García, Esther Rodríguez, additional, García-López, Alba, additional, Garrido, Federico, additional, González, Javier Aguirrezabalaga, additional, González-Carreró, Joaquín, additional, Gonzalez-Rivas, Diego, additional, Graña-Suárez, Begoña, additional, Hernández, Vicent, additional, Higuero, Paula Peleteiro, additional, Iglesias, Héctor Lázare, additional, Lago, Orlando Fernández, additional, Lamas, Alexandre, additional, Liñares-Blanco, Jose, additional, Llanas, María Jose Martinez-Sapiña, additional, López, Fernando Fernández, additional, López, José Ramón Antúnez, additional, López-López, Rafael, additional, López-Novo, Anael, additional, Lorenzo, Carmen Álvarez, additional, Loureiro, Miguel Pereira, additional, Macenlle García, Ramiro Manuel, additional, Maldonado, Shirly Margarita Nieves, additional, Marcos, Sara Seijas, additional, Marqués, Eva Martí, additional, Martín, Cristina González, additional, Martínez, Arantza Germade, additional, Martínez Lago, Nieves, additional, Martínez-Bernal, Gala, additional, Martínez-Pérez, Julia, additional, Mato-Abad, Virginia, additional, Méndez, Silvia Louzao, additional, Montalvo, Manuel Bustamante, additional, Mosquera, Beatriz Romero, additional, Muñoz, Catuxa Celeiro, additional, Munteanu, Cristian R., additional, Nine, Ángel Concheiro, additional, Novoa, Alejandra García, additional, Oreiro, Martina Lema, additional, Osuna, Francisco Ruíz-Cabello, additional, Otero, María, additional, Otero Muinelo, Susana A., additional, Parada, Pilar Díaz, additional, Paredes Cotoré, Jesús P., additional, Pazos, Alejandro, additional, Pazos García, Alejandro, additional, Pazos García, Carla, additional, Pedreira, Nieves, additional, Pillado, María Teresa Seoane, additional, Piñeiro, Susana López, additional, Poza, Margarita, additional, Purriños, Natalia Cal, additional, Queipo, Francisco, additional, Regal, Patricia, additional, Reinquet, Fernando Zelaya, additional, Rey, María Teresa Vázquez, additional, Rivas, Andrés Dacal, additional, Rocha, José Luis Ulla, additional, Rodríguez, Alejandro Ledo, additional, Rodríguez, Francisco Javier González, additional, Rodríguez, Gerardo Baños, additional, Rodríguez, María Teresa García, additional, Rodríguez, Máximo Fraga, additional, Rojas, Miriam, additional, Rosés, Leopoldo López, additional, Rúa, Marta Covela, additional, Ruiz-Bañobre, Juan, additional, Ruiz-Ponte, Clara, additional, Saavedra, Francisco Javier Maestro, additional, Sacristán Santos, Víctor, additional, Said-Criado, Ismael, additional, Sánchez, Aliuska Duardo, additional, Santamaría, Paloma González, additional, Sardenberg, Rodrigo A.S., additional, Sieira, Antonio Jurjo, additional, Silva, Paulino Pais, additional, Suarez, Rosa Fungueiriño, additional, Taboada, Tatiana María Civeira, additional, Trillo, Adriana Barreiro, additional, Trillo, Rosa, additional, Vázquez-Tunas, M. Lidia, additional, Turnes, Alfonso Martínez, additional, Valladares, Begoña Taboada, additional, Valladares-Ayerbes, Manuel, additional, Varela, Vanesa Val, additional, Varela-Calviño, Rubén, additional, Vázquez, Beatriz I., additional, Vázquez, Carla Blanco, additional, Vázquez, Juan Turnes, additional, Vázquez, Pablo Parada, additional, Vázquez, Vanesa Vilanova, additional, Vázquez-Naya, José M., additional, Vázquez-Rivera, Francisca, additional, Veiga, Alberto, additional, Vidal-Ínsua, Yolanda, additional, Vilas, Alba María Arceo, additional, and Worner, Ignacio Couto, additional
Published: 2022
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3. MicroRNA Expression Profiling of Peripheral Blood Samples Predicts Resistance to First-line Sunitinib in Advanced Renal Cell Carcinoma Patients

Author: Gámez-Pozo, Angelo, Antón-Aparicio, Luis M., Bayona, Cristina, Borrega, Pablo, Gallegos Sancho, María I., García-Domínguez, Rocío, de Portugal, Teresa, Ramos-Vázquez, Manuel, Pérez-Carrión, Ramón, Bolós, María V., Madero, Rosario, Sánchez-Navarro, Iker, Fresno Vara, Juan A., and Arranz, Enrique Espinosa
Published: 2012
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4. Chapter 46 - Signaling pathways in CRC

Author: Sacristán Santos, Víctor, Martínez Lago, Nieves, Pazos García, Carla, Pazos García, Alejandro, and Antón Aparicio, Luis M.
Published: 2022
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5. Diagnostic accuracy of small breast epithelial mucin mRNA as a marker for bone marrow micrometastasis in breast cancer: a pilot study

Author: Valladares-Ayerbes, Manuel, Iglesias-Díaz, Pilar, Díaz-Prado, Silvia, Ayude, Daniel, Medina, Vanessa, Haz, Mar, Reboredo, Margarita, Antolín, Silvia, Calvo, Lourdes, and Antón-Aparicio, Luis M.
Published: 2009
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6. Comprehensive lung injury pathology induced by mTOR inhibitors

Author: Aparicio, Guadalupe, Calvo, Moisés B., Medina, Vanessa, Fernández, Ovidio, Jiménez, Paula, Lema, Martina, Figueroa, Angélica, and Antón Aparicio, Luis M.
Published: 2009
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7. Expression of Wnt gene family and frizzled receptors in head and neck squamous cell carcinomas

Author: Díaz Prado, Silvia Maria, Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Blanco Calvo, Moisés, López Cedrún, José Luis, Sironvalle Soliva, Sheila, Valladares Ayerbes, Manuel, García Campelo, Rosario, and Antón Aparicio, Luis M.
Published: 2009
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8. A Primary Signet Ring Cell Carcinoma of the Prostate With Bone Metastasis With Impressive Response to FOLFOX and Cetuximab

Author: Roldán, Ana Milena, Núñez, Natalia Fernández, Grande, Enrique, García, Augusto Álvarez, and Antón-Aparicio, Luis M.
Published: 2012
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9. A new scenario in metastatic renal cell carcinoma: a SOG‑GU consensus

Author: Vázquez Estévez, Sergio, Anido Herranz, Urbano, Lázaro Quintela, Martín, Fernández Calvo, Ovidio, Fernández-Núñez, Natalia, Dios Álvarez, N. de, Varela, V., Campos Balea, B., Agraso, S., Areses, M. C., Iglesias, L., Blanco, Moisés, Maciá, S., Antón-Aparicio, Luis M., Vázquez Estévez, Sergio, Anido Herranz, Urbano, Lázaro Quintela, Martín, Fernández Calvo, Ovidio, Fernández-Núñez, Natalia, Dios Álvarez, N. de, Varela, V., Campos Balea, B., Agraso, S., Areses, M. C., Iglesias, L., Blanco, Moisés, Maciá, S., and Antón-Aparicio, Luis M.
Abstract: [Abstract] Background This article describes and compares approved targeted therapies and the newer immunotherapy agents. Materials and methods This article especially performs an in-depth review of currently available data for tivozanib, explaining its mechanism of action, its safety profle and its role as an efcacy drug in the management of renal cancer. Results Despite the fact that the treatment of advanced RCC has been dramatically modifed in recent years, durable remissions are scarce and it remains a lethal disease. For frst- and second-line therapy, there is now growing evidence to guide the selection of the appropriate treatment. Conclusions Several TKIs are standard of care at diferent settings. Among those approved TKIs, tivozanib has similar efcacy than others with a better safety profle. The use of prognostic factors is critical to the selection of optimal therapy.
Published: 2020

10. Tyrosine kinase inhibitors reprogramming immunity in renal cell carcinoma: rethinking cancer immunotherapy

Author: Antón-Aparicio, Luis M., Peláez Fernández, Ignacio, Cassinello Espinosa, J., Antón-Aparicio, Luis M., Peláez Fernández, Ignacio, and Cassinello Espinosa, J.
Abstract: [Abstract] The immune system regulates angiogenesis in cancer by way of both pro- and antiangiogenic activities. A bidirectional link between angiogenesis and the immune system has been clearly demonstrated. Most antiangiogenic molecules do not inhibit only VEGF signaling pathways but also other pathways which may affect immune system. Understanding of the role of these pathways in the regulation of immunosuppressive mechanisms by way of specific inhibitors is growing. Renal cell carcinoma (RCC) is an immunogenic tumor in which angiogenesis and immunosuppression work hand in hand, and its growth is associated with impaired antitumor immunity. Given the antitumor activity of selected TKIs in metastatic RCC (mRCC), it seems relevant to assess their effect on the immune system. The confirmation that TKIs improve cell cytokine response in mRCC provides a basis for the rational combination and sequential treatment of TKIs and immunotherapy.
Published: 2017

11. Novel potential predictive markers of sunitinib outcomes in long-term responders versus primary refractory patients with metastatic clear-cell renal cell carcinoma

Author: Puente, Javier, Lainez, Nuria, Dueñas, Marta, Méndez-Vidal, María José, Esteban, Emilio, Castellano, Daniel, Martínez-Fernández, Mónica, Basterretxea, Laura, Juan-Fita, María José, Antón-Aparicio, Luis M., León, Luis, Lambea, Julio, Pérez-Valderrama, Begoña, Vázquez, Sergio, Suárez, Cristina, García del Muro, Xavier, Gallardo, Enrique, Maroto, José Pablo, Samaniego, M. Luz, Suárez-Paniagua, Beatriz, Sanz, Julián, Paramio, Jesús M., Puente, Javier, Lainez, Nuria, Dueñas, Marta, Méndez-Vidal, María José, Esteban, Emilio, Castellano, Daniel, Martínez-Fernández, Mónica, Basterretxea, Laura, Juan-Fita, María José, Antón-Aparicio, Luis M., León, Luis, Lambea, Julio, Pérez-Valderrama, Begoña, Vázquez, Sergio, Suárez, Cristina, García del Muro, Xavier, Gallardo, Enrique, Maroto, José Pablo, Samaniego, M. Luz, Suárez-Paniagua, Beatriz, Sanz, Julián, and Paramio, Jesús M.
Abstract: [Abstract] Background: Several potential predictive markers of efficacy of targeted agents in patients with metastatic renal cell carcinoma (mRCC) have been identified. Interindividual heterogeneity warrants further investigation. Patients and methods: Multicenter, observational, retrospective study in patients with clear-cell mRCC treated with sunitinib. Patients were classified in two groups: long-term responders (LR) (progression-free survival (PFS)≥22 months and at least stable disease), and primary refractory (PR) (progressive disease within 3-months of sunitinib onset). Objectives were to compare baseline clinical factors in both populations and to correlate tumor expression of selected signaling pathways components with sunitinib PFS. Results: 123 patients were analyzed (97 LR, 26 PR). In the LR cohort, overall response rate was 79% and median duration of best response was 30 months. Median PFS and overall survival were 43.2 (95% confidence intervals[CI]:37.2-49.3) and 63.5 months (95%CI:55.1-71.9), respectively. At baseline PR patients had a significantly lower proportion of nephrectomies, higher lactate dehydrogenase and platelets levels, lower hemoglobin, shorter time to and higher presence of metastases, and increased Fuhrman grade. Higher levels of HEYL, HEY and HES1 were observed in LR, although only HEYL discriminated populations significantly (AUC[ROC]=0.704; cut-off=34.85). Increased levels of hsa-miR-27b, hsa-miR-23b and hsa-miR-628-5p were also associated with prolonged survival. No statistical significant associations between hsa-miR-23b or hsa-miR-27b and the expression of c-Met were found. Conclusions: Certain mRCC patients treated with sunitinib achieve extremely long-term responses. Favorable baseline hematology values and longer time to metastasis may predict longer PFS. HEYL, hsa-miR-27b, hsa-miR-23b and hsa-miR-628-5p could be potentially used as biomarkers of sunitinib response.
Published: 2017

12. Role of taxanes in advanced prostate cancer

Author: Cassinello Espinosa, J., Carballido Rodríguez, J., Antón-Aparicio, Luis M., Cassinello Espinosa, J., Carballido Rodríguez, J., and Antón-Aparicio, Luis M.
Abstract: [Abstract] Advanced prostate cancer is an androgen-dependent disease for which the initial treatment is an androgen deprivation maneuver. However, some primary resistances to hormonal treatment occur with increasing incidence throughout the evolution of the disease. The taxanes, docetaxel and cabazitaxel, exert their action at multiple levels at the tumor cell: besides inhibiting the mitosis and inducing the cell death, they induce the nuclear accumulation of FOXO1, a potent nuclear factor that acts against the activation of androgen receptor inhibiting the transcription of AR-V7 variant associated with the development of resistances to abiraterone and enzalutamide. Docetaxel, as first-line therapy, and cabazitaxel, as second-line therapy, have demonstrated to increase the survival in castration-resistant prostate cancer. The results from last studies either on high-risk localized disease or on androgen-sensitive tumors demonstrate the increasing role of taxanes at earlier states of prostate cancer.
Published: 2016

13. Effect of a microtubule-targeting drug on cell–cell contacts in bladder epithelial tumour cells

Author: Antón-Aparicio, Luis M., Castosa, Raquel, Haz, Mar, Blanco, Moisés, Rodríguez, M., Valladares-Ayerbes, Manuel, and Figueroa, Angélica
Abstract: Póster
Published: 2014

14. Enzalutamide: a new prostate cancer targeted therapy against the androgen receptor

Author: Lázaro Quintela, Martín, León Mateos, Luis, Vázquez Estévez, Sergio, Fernández Calvo, Ovidio, Anido Herranz, Urbano, Afonso Afonso, Francisco Javier, Santomé, Lucía, Antón-Aparicio, Luis M., Lázaro Quintela, Martín, León Mateos, Luis, Vázquez Estévez, Sergio, Fernández Calvo, Ovidio, Anido Herranz, Urbano, Afonso Afonso, Francisco Javier, Santomé, Lucía, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Enzalutamide (MDV3100), an androgen receptor-signalling inhibitor, represents the most recent compound added to the therapeutic armamentarium for the treatment of metastatic castration-resistant prostate cancer (mCRPC) who progressed to docetaxel. The anti-tumour activity and safety of enzalutamide has been demonstrated in a phase III clinical trial, showing a benefit in overall survival, which was the primary endpoint. There are no head-to-head studies comparing the different treatment options in this subset of patients. In this article, most relevant data published in the literature have been reviewed, with special attention to the therapeutic alternatives currently available for postdocexatel mCRPC patients, emphasising the mechanisms of action of the different drugs, efficacy and quality of life-related aspects.
Published: 2015

15. Clinical implications of epithelial cell plasticity in cancer progression

Author: Antón-Aparicio, Luis M., Blanco, Moisés, Castosa, Raquel, Concha, Ángel, Valladares-Ayerbes, Manuel, Calvo, Lourdes, Figueroa, Angélica, Antón-Aparicio, Luis M., Blanco, Moisés, Castosa, Raquel, Concha, Ángel, Valladares-Ayerbes, Manuel, Calvo, Lourdes, and Figueroa, Angélica
Abstract: [Abstract] In the last few years, the role of epithelial cell plasticity in cancer biology research has gained increasing attention. This concept refers to the ability of the epithelial cells to dynamically switch between different phenotypic cellular states. This programme is particularly relevant during the epithelial-to-mesenchymal transition (EMT) in cancer progression. During colonization, epithelial cells first activate the EMT programme to disseminate from a primary tumour to reach a distant tissue site. During this process, cells are transported into the circulation and are able to escape the immune system of the host. Then, a reverse process called mesenchymal-to-epithelial transition (MET) occurs on cells that settle in the distant organs. Although epithelial cell plasticity has an important impact on tumour biology, the clinical relevance of this concept remains to be recapitulated. In this review, we will update the current state of epithelial cell plasticity in cancer progression and its clinical implications for the design of therapeutic strategies, the acquisition of multidrug resistance, and future perspectives for the management of cancer patients.
Published: 2015

16. Evaluation of the efficacy and safety of lanreotide in combination with targeted therapies in patients with neuroendocrine tumours in clinical practice: a retrospective cross-sectional analysis

Author: Capdevila, Jaume, Sevilla, Isabel, Alonso, Vicente, Antón-Aparicio, Luis M., Jiménez Fonseca, Paula, Grande, Enrique, Reina, Juan José, Manzano, José Luis, Alonso Lájara, Juan Domingo, Barriuso, Jorge, Castellano, Daniel, Medina, Javier, López, Carlos, Segura, Ángel, Carrera, Sergio, Crespo, Guillermo, Fuster, José, Munarriz, Javier, García Alfonso, Pilar, Capdevila, Jaume, Sevilla, Isabel, Alonso, Vicente, Antón-Aparicio, Luis M., Jiménez Fonseca, Paula, Grande, Enrique, Reina, Juan José, Manzano, José Luis, Alonso Lájara, Juan Domingo, Barriuso, Jorge, Castellano, Daniel, Medina, Javier, López, Carlos, Segura, Ángel, Carrera, Sergio, Crespo, Guillermo, Fuster, José, Munarriz, Javier, and García Alfonso, Pilar
Abstract: [Abstract] Background. Based on the mechanism of action, combining somatostatin analogues (SSAs) with mTOR inhibitors or antiangiogenic agents may provide synergistic effects for the treatment of patients with neuroendocrine tumours (NETs). Herein, we investigate the use of these treatment combinations in clinical practice. Methods. This retrospective cross-sectional analysis of patients with NETs treated with the SSA lanreotide and targeted therapies at 35 Spanish hospitals evaluated the efficacy and safety of lanreotide treatment combinations in clinical practice. The data of 159 treatment combinations with lanreotide in 133 patients was retrospectively collected. Results. Of the 133 patients, with a median age of 59.4 (16–83) years, 70 (52.6 %) patients were male, 64 (48.1 %) had pancreatic NET, 23 (17.3 %) had ECOG PS ≥2, 41 (30.8 %) had functioning tumours, 63 (47.7 %) underwent surgery of the primary tumour, 45 (33.8 %) had received prior chemotherapy, and 115 (86.5 %) had received prior SSAs. 115 patients received 1 lanreotide treatment combination and 18 patients received between 2 and 5 combinations. Lanreotide was mainly administered in combination with everolimus (73 combinations) or sunitinib (61 combinations). The probability of being progression-free was 78.5 % (6 months), 68.6 % (12 months) and 57.0 % (18 months) for patients who only received everolimus plus lanreotide (n = 57) and 89.3 % (6 months), 73.0 % (12 months), and 67.4 % (18 months) for patients who only received sunitinib and lanreotide (n = 50). In patients who only received everolimus plus lanreotide the median time-to-progression from the initiation of lanreotide combination treatment was 25.8 months (95 % CI, 11.3, 40.3) and it had not yet been reached among the subgroup of patients only receiving sunitinib plus lanreotide. The safety profile of the combination treatment was comparable to that of the targeted agent alone. Conclusions. The combination of lanreotide and targeted therapie
Published: 2015

17. Treatment of sunitinib-induced hypertension in solid tumor by nitric oxide donors

Author: León-Mateos, L., Mosquera, J., Antón-Aparicio, Luis M., León-Mateos, L., Mosquera, J., and Antón-Aparicio, Luis M.
Abstract: [Abstract] Vascular endothelial growth factor (VEGF) and its receptor (VEGFR) are overexpressed in the majority of renal cell carcinomas. This characteristic has supported the rationale of targeting VEGF-driven tumour vascularization, especially in clear cell RCC. VEGF-inhibiting strategies include the use of tyrosine kinase inhibitors (sunitinib, axitinib, pazopanib, and sorafenib) and neutralizing antibodies such as bevacizumab. Hypertension (HTN) is one of the most common adverse effects of angiogenesis inhibitors. HTN observed in clinical trials appears to correlate with the potency of VEGF kinase inhibitor against VEGFR-2: agents with higher potency are associated with a higher incidence of HTN. Although the exact mechanism by tyrosine kinase inhibitors induce HTN has not yet been completely clarified, two key hypotheses have been postulated. First, some studies have pointed to a VEGF inhibitors-induced decrease in nitric oxide synthase (NOS) and nitric oxide (NO) production, that can result in vasoconstriction and increased blood pressure. VEGF, mediated by PI3K/Akt and MAPK pathway, upregulates the endothelial nitric oxide synthase enzyme leading to up-regulation of NO production. So inhibition of signaling through the VEGF pathway would lead to a decrease in NO production, resulting in an increase in vascular resistance and blood pressure. Secondly a decrease in the number of microvascular endothelial cells and subsequent depletion of normal microvessel density (rarefaction) occurs upon VEGF signaling inhibition. NO donors could be successfully used not only for the treatment of developed angiogenesis-inhibitor-induced hypertension but also for preventive effects.
Published: 2015

18. Circulating miR-200c and miR-141 and outcomes in patients with breast cancer

Author: Antolín, Silvia, Calvo, Lourdes, Blanco, Moisés, Paz Santiago, María, Lorenzo-Patiño, María J., Haz, Mar, Santamarina, Isabel, Figueroa, Angélica, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Antolín, Silvia, Calvo, Lourdes, Blanco, Moisés, Paz Santiago, María, Lorenzo-Patiño, María J., Haz, Mar, Santamarina, Isabel, Figueroa, Angélica, Antón-Aparicio, Luis M., and Valladares-Ayerbes, Manuel
Abstract: [Abstract] Background. The deregulation of microRNAs in both tumours and blood has led to the search for microRNAs to indicate the presence of cancer and predict prognosis. We hypothesize the deregulation of miR-200c/miR-141 in the whole blood can identify breast cancer (BC), and could be developed into a prognostic signature. Methods. The expression of miR-200c and miR-141 were examined in bloods (57 stage I-IV BC patients and 20 age-matched controls) by quantitative reverse-transcription PCR. The associations of circulating microRNAs with clinic and pathological characteristics were analysed. Their effects on survival were analysed by the Kaplan-Meier method and Cox regressions. Results. MiR-200c was down regulated (P < 0.0001) in the blood of BC patients, yielded an area under the ROC curve of 0.79 (90% sensitivity, 70.2% specificity) in discriminating BC from controls. Circulating miR-141 was not discriminating. MiR-200c and miR-141 in the blood of BC patients were inversely correlated (P = 0.019). The miR-200c levels were numerically higher in stage IV and tumours with lower MIB-1. MiR-141 was significantly higher in the blood of patients with stage I-III, lymph node metastasis, and HER2 negative tumours. High blood expression of miR-200c and/or low expression of miR-141 was associated with unfavourable overall survival (hazard ratio, 3.89; [95% CI: 1.28-11.85]) and progression-free survival (3.79 [1.41–10.16]) independent of age, stage and hormonal receptors. Conclusions. Circulating miR-200c and miR-141 were deregulated in BC comparing with controls. Furthermore, miR-200c and miR-141 were independent prognostic factors and associated with distinct outcomes of BC patients.
Published: 2015

19. Circulating levels of GDF15, MMP7 and miR-200c as a poor prognostic signature in gastric cancer

Author: Blanco, Moisés, Tarrío, Nuria, Reboredo, Margarita, Haz, Mar, García, Jorge, Quindós-Varela, María, Figueroa, Angélica, Antón-Aparicio, Luis M., Calvo, Lourdes, Valladares-Ayerbes, Manuel, Blanco, Moisés, Tarrío, Nuria, Reboredo, Margarita, Haz, Mar, García, Jorge, Quindós-Varela, María, Figueroa, Angélica, Antón-Aparicio, Luis M., Calvo, Lourdes, and Valladares-Ayerbes, Manuel
Abstract: [Abstract] Aim: To analyze GDF15 and MMP7 serum levels as diagnostic biomarkers in gastric cancer (GC) patients. The prognostic value of GDF15 and MMP7 serum levels in combination with miR-200c blood expression was also analyzed. Patients & methods: Fifty-two GC and 23 control samples were included. Results: GDF15 and MMP7 proved to be powerful tools for GC diagnosis. Increased levels of GDF15 and MMP7 were associated with shorter progression-free survival and overall survival in univariate analysis. In multivariate analysis, the combination of high levels of GDF15, MMP7 and miR-200c was an independent predictor for death (p = 0.033). Conclusion: GDF15 and MMP7 serum levels have diagnostic value for GC. The combination marker formed by GDF15, MMP7 and miR-200c is indicative of adverse evolution in GC patients.
Published: 2014

20. Cabazitaxel for metastatic castration-resistant prostate cancer: safety data from the Spanish expanded access program

Author: Castellano, Daniel, Antón-Aparicio, Luis M., Esteban, Emilio, Sánchez-Hernández, Alfredo, Germá, José Ramón, Batista, Norberto, Maroto, Pablo, Pérez-Valderrama, Begoña, Luque, Raquel, Méndez-Vidal, María José, Castellano, Daniel, Antón-Aparicio, Luis M., Esteban, Emilio, Sánchez-Hernández, Alfredo, Germá, José Ramón, Batista, Norberto, Maroto, Pablo, Pérez-Valderrama, Begoña, Luque, Raquel, and Méndez-Vidal, María José
Abstract: [Abstract] BACKGROUND: Based on the TROPIC study results, cabazitaxel was approved for the management of metastatic castration-resistant prostate cancer (mCRPC) progressing on or after docetaxel. METHODS: This multi-centre program provided early access to cabazitaxel to patients with mCRPC before its commercialization. Safety data from 153 Spanish patients receiving cabazitaxel 25 mg/m(2) i.v. Q3W, plus oral prednisone/prednisolone 10 mg daily, are reported. RESULTS: Median age of patients was 70 years (26.8% ≥ 75 years), 94.1 and 26.8% had bone and visceral metastasis, respectively. Most had an Eastern Cooperative Oncology Group ≤ 1 (88.9%) and had received a median of 8.0 cycles of last docetaxel treatment. The median of cabazitaxel cycles and cumulative dose were 6.0 (Interquartile range [IQR]: 4.0; 8.0) and 148.9 (IQR: 98.2; 201.4) mg/m(2), respectively. Adverse events (AEs) possibly related to cabazitaxel occurred in 143 (93.5%) patients. The most frequent grade ≥ 3 AEs were neutropenia (n = 25, 16.3%) and asthenia (n = 17, 11.1%). Febrile neutropenia and grade ≥ 3 diarrhea occurred in 5.2% of the patients each. There were five (3.3%) possibly treatment-related deaths, mainly infection-related. G-CSFs were used in 114 (74.5%) patients, generally as prophylaxis (n = 107; 69.9%). Grade ≥ 3 peripheral neuropathy and nail disorders were uncommon. CONCLUSIONS: Cabazitaxel administration, in a real-world setting, is tolerated by Spanish patients with mCRPC, and the AEs are manageable.
Published: 2014

21. Role of the microtubule-targeting drug vinflunine on cell-cell adhesions in bladder epithelial tumour cells

Author: Antón-Aparicio, Luis M., Castosa, Raquel, Haz, Mar, Rodríguez, Marta, Blanco, Moisés, Valladares-Ayerbes, Manuel, Figueroa, Angélica, Antón-Aparicio, Luis M., Castosa, Raquel, Haz, Mar, Rodríguez, Marta, Blanco, Moisés, Valladares-Ayerbes, Manuel, and Figueroa, Angélica
Abstract: [Abstract] Background. Vinflunine (VFL) is a microtubule-targeting drug that suppresses microtubule dynamics, showing anti-metastatic properties both in vitro and in living cancer cells. An increasing body of evidence underlines the influence of the microtubules dynamics on the cadherin-dependent cell-cell adhesions. E-cadherin is a marker of epithelial-to-mesenchymal transition (EMT) and a tumour suppressor; its reduced levels in carcinoma are associated with poor prognosis. In this report, we investigate the role of VFL on cell-cell adhesions in bladder epithelial tumour cells. Methods. Human bladder epithelial tumour cell lines HT1376, 5637, SW780, T24 and UMUC3 were used to analyse cadherin-dependent cell-cell adhesions under VFL treatment. VFL effect on growth inhibition was measured by using a MTT colorimetric cell viability assay. Western blot, immunofluorescence and transmission electron microscopy analyses were performed to assess the roles of VFL effect on cell-cell adhesions, epithelial-to-mesenchymal markers and apoptosis. The role of the proteasome in controlling cell-cell adhesion was studied using the proteasome inhibitor MG132. Results. We show that VFL induces cell death in bladder cancer cells and activates epithelial differentiation of the remaining living cells, leading to an increase of E-cadherin-dependent cell-cell adhesion and a reduction of mesenchymal markers, such as N-cadherin or vimentin. Moreover, while E-cadherin is increased, the levels of Hakai, an E3 ubiquitin-ligase for E-cadherin, were significantly reduced in presence of VFL. In 5637, this reduction on Hakai expression was blocked by MG132 proteasome inhibitor, indicating that the proteasome pathway could be one of the molecular mechanisms involved in its degradation. Conclusions. Our findings underscore a critical function for VFL in cell-cell adhesions of epithelial bladder tumour cells, suggesting a novel molecular mechanism by which VFL may impact upon EMT and metastasis.
Published: 2014

22. MicroARN circulantes en sangre de pacientes con cáncer de próstata

Author: Medina Villaamil, Vanessa, Martínez-Breijo, S., Portela-Pereira, P., Quindós-Varela, María, Santamarina, Isabel, Antón-Aparicio, Luis M., Gómez Veiga, Francisco, Medina Villaamil, Vanessa, Martínez-Breijo, S., Portela-Pereira, P., Quindós-Varela, María, Santamarina, Isabel, Antón-Aparicio, Luis M., and Gómez Veiga, Francisco
Abstract: [Resumen] Introducción. Los microARN (miARN) son ARN reguladores de pequeño tamaño que no codifican para proteínas. La detección de células tumorales circulantes (CTC) proporcionaría información diagnóstica y pronóstica en los tumores de próstata (TP). En este sentido los miARN podrían constituir una nueva y prometedora clase de biomarcadores para la detección de CTC. Objetivos. Analizar miARN circulantes en sangre total como marcadores no invasivos en pacientes con cáncer de próstata localizado e individuos sanos. Material y métodos. Estudio preliminar con una N poblacional de 40 pacientes con una media de edad de 71 años y un PSA medio de 18, 9 ng/ml (rango). Respecto al grupo de riesgo (GR): un 33,3% bajo riesgo, un 30% riesgo intermedio y un 36,7% alto riesgo. Se realizó un estudio previo in silico que identificó 92 miARN candidatos seguido de otro in vivo para verificar los hallazgos del primero mediante tecnología de arrays de PCR a tiempo real. Resultados. El análisis estadístico de los resultados reveló 10 miARN candidatos con una expresión diferencial estadísticamente significativa entre los distintos grupos de riesgo y los controles sanos: hsa-miR-337-3p, hsa-miR-330-3p, hsa-miR-339-3p, hsa-miR-124, hsa-miR-218, hsa-miR-128, hsa-miR-10a, hsa-miR-199b-5p, hsa-miR-200b y hsa-miR-15b Conclusiones. Nuestros datos sugieren que los miARN circulantes pueden servir como biomarcadores para identificar grupos de riesgo en CaP., [Abstract] Introduction. MicroRNAs (miRNAs) are small regulatory RNAs that do not code for proteins. Detection of circulating tumor cells (CTC) would provide diagnostic and prognostic information in prostate tumors (PT). Thus, miRNAs could constitute a promising new class of biomarkers for CTC detection. Objectives. To analyze circulating microRNAs in whole blood as non-invasive markers in patients with localized prostate cancer and healthy individuals. Material and methods. A preliminary study including a population of 40 patients with mean age of 71 years and mean PSA of 18, 9ng/ml (range). Regarding the risk group (RG): 33.3% had low risk, 30% intermediate risk and 36.7% high risk. A previous in silico study identified 92 candidates and was followed by another in vivo to verify the findings of the former using array technology by real-time PCR. Results. Statistical analysis of the results revealed 10 microRNAs candidates with statistically significant differential expression between the different risk groups and healthy controls: hsa-miR-337-3p, hsa-miR-330-3p, hsa-miR-339-3p, hsa-miR-124, hsa-miR-218, hsa-miR-128, hsa-miR-10a, hsa-miR-199b-5p, hsa-miR-200b and hsa-miR-15b. Conclusions. Our data suggest that circulating microRNAs can act as biomarkers to identify risk groups in CaP.
Published: 2014

23. The role of PCA3 testing in a homogenenous population of patients with low and intermediate-risk prostate cancer treated with brachytherapy.

Author: Medina, Ana, primary, Losada, Raquel, additional, Mariño, Alfonso, additional, Candal Gómez, Arturo, additional, Diaz, Inmaculada, additional, Ramos Vazquez, Manuel, additional, Fernandez, Jose Luis, additional, Garcia, Sonia Aranzazu, additional, Mendez, Carlos, additional, Azpitarte, Cristina, additional, Paris, Lorena, additional, Chantada Abal, Venancio, additional, Martinez Breijo, Sara, additional, Antón Aparicio, Luis M., additional, and Olmos, David, additional
Published: 2014
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24. Metastatic castration-resistant prostate cancer

Author: Fernández, Ovidio, primary, Afonso, Javier, additional, Vázquez, Sergio, additional, Campos, Begoña, additional, Lázaro, Matín, additional, León, Luis, additional, and Antón Aparicio, Luis M., additional
Published: 2014
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25. Posttranscriptional regulation by RNA-binding proteins during epithelial-to-mesenchymal transition

Author: Antón-Aparicio, Luis M., Abella Cajigal, Vanessa, Valladares-Ayerbes, Manuel, Figueroa, Angélica, Antón-Aparicio, Luis M., Abella Cajigal, Vanessa, Valladares-Ayerbes, Manuel, and Figueroa, Angélica
Abstract: [Abstract] Epithelial-to-mesenchymal transition (EMT), one of the crucial steps for carcinoma cells to acquire invasive capacity, results from the disruption of cell–cell contacts and the acquisition of a motile mesenchymal phenotype. Although the transcriptional events controlling EMT have been extensively studied, in recent years, several posttranscriptional mechanisms have emerged as critical in the regulation of EMT during tumor progression. In this review, we highlight the regulation of posttranscriptional events in EMT by RNA-binding proteins (RBPs). RBPs are responsible for controlling pre-mRNA splicing, capping, and polyadenylation, as well as mRNA export, turnover, localization, and translation. We discuss the most relevant aspects of RBPs controlling the metabolism of EMT-related mRNAs, and describe the implication of novel posttranscriptional mechanisms regulating EMT in response to different signaling pathways. Novel insight into posttranscriptional regulation of EMT by RBPs is uncovering new therapeutic targets in cancer invasion and metastasis.
Published: 2013

26. Crossing paths in Human Renal Cell Carcinoma (hRCC)

Author: Aparicio Gallego, Guadalupe, Medina Villaamil, Vanessa, Grande Pulido, Enrique, Santamarina, Isabel, Antón-Aparicio, Luis M., Aparicio Gallego, Guadalupe, Medina Villaamil, Vanessa, Grande Pulido, Enrique, Santamarina, Isabel, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Historically, cell-signaling pathways have been studied as the compilation of isolated elements into a unique cascade that transmits extracellular stimuli to the tumor cell nucleus. Today, growing evidence supports the fact that intracellular drivers of tumor progression do not flow in a single linear pathway, but disseminate into multiple intracellular pathways. An improved understanding of the complexity of cancer depends on the elucidation of the underlying regulatory networks at the cellular and intercellular levels and in their temporal dimension. The high complexity of the intracellular cascades causes the complete inhibition of the growth of one tumor cell to be very unlikely, except in cases in which the so-called “oncogene addiction” is known to be a clear trigger for tumor catastrophe, such as in the case of gastrointestinal stromal tumors or chronic myeloid leukemia. In other words, the separation and isolation of the driver from the passengers is required to improve accuracy in cancer treatment. This review will summarize the signaling pathway crossroads that govern renal cell carcinoma proliferation and the emerging understanding of how these pathways facilitate tumor escape. We outline the available evidence supporting the putative links between different signaling pathways and how they may influence tumor proliferation, differentiation, apoptosis, angiogenesis, metabolism and invasiveness. The conclusion is that tumor cells may generate their own crossroads/crosstalk among signaling pathways, thereby reducing their dependence on stimulation of their physiologic pathways.
Published: 2012

27. Circulating miR-200c as a diagnostic and prognostic biomarker for gastric cancer

Author: Valladares-Ayerbes, Manuel, Reboredo, Margarita, Medina Villaamil, Vanessa, Iglesias-Díaz, Pilar, Lorenzo-Patiño, María J., Haz, Mar, Santamarina, Isabel, Blanco, Moisés, Fernández-Tajes, Juan, Quindós-Varela, María, Carral, Alberto, Figueroa, Angélica, Antón-Aparicio, Luis M., Calvo, Lourdes, Valladares-Ayerbes, Manuel, Reboredo, Margarita, Medina Villaamil, Vanessa, Iglesias-Díaz, Pilar, Lorenzo-Patiño, María J., Haz, Mar, Santamarina, Isabel, Blanco, Moisés, Fernández-Tajes, Juan, Quindós-Varela, María, Carral, Alberto, Figueroa, Angélica, Antón-Aparicio, Luis M., and Calvo, Lourdes
Abstract: [Abstract] Background. MicroRNAs are aberrantly expressed and correlate with tumourigenesis and the progression of solid tumours. The miR-200 family determines the epithelial phenotype of cancer cells and regulates invasiveness and migration. Thus, we hypothesised that the quantitative detection of the miR-200 family as epithelial-specific microRNAs in the blood could be a useful clinical biomarker for gastric cancer (GC). Methods. We initially validated the expression levels of miR-200a, 200b, 200c and 141 in GC cell lines (n = 2) and blood from healthy controls (n = 19) using real-time quantitative reverse transcription PCR (qRT-PCR). The microarray expression profiles of the miR-200 family in 160 paired samples of non-tumour gastric mucosae and GC were downloaded through ArrayExpress and analysed. MiR-200c was selected for clinical validation. The qRT-PCR prospective assessment of miR-200c was performed using 67 blood samples (52 stage I-IV GC patients and 15 controls); the area under the receiver operating characteristic curve (AUC-ROC) was estimated. The Kaplan-Meier and Breslow-Wilcoxon tests were used to assess the correlation of miR-200c with overall and progression-free survival (OS and PFS). Multivariate analyses were performed using the Cox model. Results. The miR-200c blood expression levels in GC patients were significantly higher than in normal controls (p = 0.018). The AUC-ROC was 0.715 (p = 0.012). The sensitivity, specificity and accuracy rates of 65.4%, 100% and 73.1%, respectively, were observed. The levels of miR-200c in the blood above the cutoff defined by the ROC curve was found in 17.6% of stage I-II GC patients, 20.6% of stage III patients and 67.7% of stage IV patients (p < 0.001). The miR-200c expression levels were not associated with clinical or pathological characteristics or recent surgical procedures. There was a correlation (p = 0.016) with the number of lymph node metastases and the increased expression levels of miR-200c in blood w
Published: 2012

28. miR-203 regulates cell proliferation through Its influence on Hakai expression

Author: Abella Cajigal, Vanessa, Valladares-Ayerbes, Manuel, Rodríguez, Teresa, Haz, Mar, Blanco, Moisés, Tarrío, Nuria, Iglesias, Pilar, Antón-Aparicio, Luis M., Figueroa, Angélica, Abella Cajigal, Vanessa, Valladares-Ayerbes, Manuel, Rodríguez, Teresa, Haz, Mar, Blanco, Moisés, Tarrío, Nuria, Iglesias, Pilar, Antón-Aparicio, Luis M., and Figueroa, Angélica
Abstract: Gene expression is potently regulated through the action of microRNAs (miRNAs). Here, we present evidence of a miRNA regulating Hakai protein. Hakai was discovered as an E3 ubiquitin-ligase that mediates the posttranslational downregulation of E-cadherin, a major component of adherens junctions in epithelial cells and a potent tumour suppressor. Recent data have provided evidence that Hakai affects cell proliferation in an E-cadherin-independent manner, thus revealing a role for Hakai in the early stages of tumour progression. Furthermore, Hakai is highly up-regulated in human colon adenocarcinomas compared to normal tissues. However, the molecular mechanisms that regulate Hakai abundance are unknown. We identified two putative sites of miR-203 interaction on the Hakai mRNA, in its 3′-untranslated region (UTR). In several human carcinoma cell lines tested, overexpression of a miR-203 precursor (Pre-miR-203) reduced Hakai abundance, while inhibiting miR-203 by using an antisense RNA (Anti-miR-203) elevated Hakai levels. The repressive influence of miR-203 on the Hakai 3′-UTR was confirmed using heterologous reporter constructs. In keeping with Hakai's proliferative influence, Anti-miR-203 significantly increased cell number and BrdU incorporation, while Pre-miR-203 reduced these parameters. Importantly, the growth-promoting effects of anti-miR-203 required the presence of Hakai, because downregulation of Hakai by siRNA suppressed its proliferative action. Finally, in situ hybridization showed that miR-203 expression is attenuated in colon tumour tissues compared to normal colon tissues, suggesting that miR-203 could be a potential new prognostic marker and therapeutic target to explore in colon cancer. In conclusion, our findings reveal, for the first time, a post-transcriptional regulator of Hakai expression. Furthermore, by lowering Hakai abundance, miR-203 also reduces Hakai-regulated-cell division.
Published: 2012

29. Biological influence of Hakai in cancer: a 10-year review

Author: Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Blanco, Moisés, Alonso, Guillermo, Figueroa, Angélica, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Blanco, Moisés, Alonso, Guillermo, and Figueroa, Angélica
Abstract: [Abstract] In order to metastasize, cancer cells must first detach from the primary tumor, migrate, invade through tissues, and attach to a second site. Hakai was discovered as an E3 ubiquitin-ligase that mediates the posttranslational downregulation of E-cadherin, a major component of adherens junctions in epithelial cells that is characterized as a potent tumor suppressor and is modulated during various processes including epithelial–mesenchymal transition. Recent data have provided evidences for novel biological functional role of Hakai during tumor progression and other diseases. Here, we will review the knowledge that has been accumulated since Hakai discovery 10 years ago and its implication in human cancer disease. We will highlight the different signaling pathways leading to the influence on Hakai and suggest its potential usefulness as therapeutic target for cancer.
Published: 2012

30. Circulating microRNAs: molecular microsensors in gastrointestinal cancer

Author: Blanco, Moisés, Calvo, Lourdes, Figueroa, Angélica, Haz, Mar, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Blanco, Moisés, Calvo, Lourdes, Figueroa, Angélica, Haz, Mar, Antón-Aparicio, Luis M., and Valladares-Ayerbes, Manuel
Abstract: [Abstract] MicroRNAs (miRNAs) are small molecules of single strand non-coding RNAs, which are able to regulate gene expression. miRNAs have been involved in multiple cellular processes, such as proliferation, apoptosis and differentiation, thus alterations in miRNA expression have been shown to be directly linked with the pathological origin of multiple diseases, including cancer. In this way, during last few years, an increasing number of exciting advances have contributed to the understanding of miRNA roles in cancer. Moreover, researchers have exploited the special characteristics of miRNAs, such as the tissue and disease specificity or miRNA presence in blood, to explore their use as non-invasive tumour markers. In the present review, we summarize the current data on the potential usefulness of circulating miRNAs as diagnostic and prognostic tools in gastrointestinal tumours.
Published: 2012

31. State of the art in silico tools for the study of signaling pathways in cancer

Author: Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Santamarina, Isabel, Valladares-Ayerbes, Manuel, Antón-Aparicio, Luis M., Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Santamarina, Isabel, Valladares-Ayerbes, Manuel, and Antón-Aparicio, Luis M.
Abstract: [Abstract] In the last several years, researchers have exhibited an intense interest in the evolutionarily conserved signaling pathways that have crucial roles during embryonic development. Interestingly, the malfunctioning of these signaling pathways leads to several human diseases, including cancer. The chemical and biophysical events that occur during cellular signaling, as well as the number of interactions within a signaling pathway, make these systems complex to study. In silico resources are tools used to aid the understanding of cellular signaling pathways. Systems approaches have provided a deeper knowledge of diverse biochemical processes, including individual metabolic pathways, signaling networks and genome-scale metabolic networks. In the future, these tools will be enormously valuable, if they continue to be developed in parallel with growing biological knowledge. In this study, an overview of the bioinformatics resources that are currently available for the analysis of biological networks is provided.
Published: 2012

32. Evaluation of the adenocarcinoma-associated gene AGR2 and the intestinal stem cell marker LGR5 as biomarkers in colorectal cancer

Author: Valladares-Ayerbes, Manuel, Blanco, Moisés, Reboredo, Margarita, Lorenzo-Patiño, María J., Iglesias-Díaz, Pilar, Haz, Mar, Díaz-Prado, Silvia, Medina, Vanessa, Santamarina, Isabel, Pértega-Díaz, Sonia, Figueroa, Angélica, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Blanco, Moisés, Reboredo, Margarita, Lorenzo-Patiño, María J., Iglesias-Díaz, Pilar, Haz, Mar, Díaz-Prado, Silvia, Medina, Vanessa, Santamarina, Isabel, Pértega-Díaz, Sonia, Figueroa, Angélica, and Antón-Aparicio, Luis M.
Abstract: [Abstract] We aim to estimate the diagnostic performances of anterior gradient homolog-2 (AGR2) and Leucine-rich repeat-containing-G-protein-coupled receptor 5 (LGR5) in peripheral blood (PB) as mRNA biomarkers in colorectal cancer (CRC) and to explore their prognostic significance. Real-time PCR was used to analyze AGR2 and LGR5 in 54 stages I-IV CRC patients and 19 controls. Both mRNAs were significantly increased in PB from CRC patients compared to controls. The area under the receiver-operating characteristic curves were 0.722 (p = 0.006), 0.376 (p = 0.123) and 0.767 (p = 0.001) for AGR2, LGR5 and combined AGR2/LGR5, respectively. The AGR2/LGR5 assay resulted in 67.4% sensitivity and 94.7% specificity. AGR2 correlated with pT3–pT4 and high-grade tumors. LGR5 correlated with metastasis, R2 resections and high-grade. The progression-free survival (PFS) of patients with high AGR2 was reduced (p = 0.037; HR, 2.32), also in the stage I-III subgroup (p = 0.046). LGR5 indicated a poor prognosis regarding both PFS (p = 0.007; HR, 1.013) and overall survival (p = 0.045; HR, 1.01). High AGR2/LGR5 was associated with poor PFS (p = 0.014; HR, 2.8) by multivariate analysis. Our findings indicate that the assessment of AGR2 and LGR5 in PB might reflect the presence of circulating tumor cells (CTC) and stem cell like CTC in CRC. Increased AGR2 and LGR5 are associated with poor outcomes.
Published: 2012

33. Relevant networks involving the p53 signalling pathway in renal cell carcinoma

Author: Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Santamarina, Isabel, Valbuena Ruvira, L., Valladares-Ayerbes, Manuel, Antón-Aparicio, Luis M., Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Santamarina, Isabel, Valbuena Ruvira, L., Valladares-Ayerbes, Manuel, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Introduction: Renal cell carcinoma is the most common type of kidney cancer. A better understanding of the critical pathways and interactions associated with alterations in renal function and renal tumour properties is required. Our final goal is to combine the knowledge provided by a regulatory network with experimental observations provided by the dataset. Methods: In this study, a systems biology approach was used, integrating immunohistochemistry protein expression profiles and protein interaction information with the STRING and MeV bioinformatics tools. A group consisting of 80 patients with renal cell carcinoma was studied. The expression of selected markers was assessed using tissue microarray technology on immunohistochemically stained slides. The immunohistochemical data of the molecular factors studied were analysed using a parametric statistical test, Pearson’s correlation coefficient test. Results: Bioinformatics analysis of tumour samples resulted in 2 protein networks. The first network consists of proteins involved in the angiogenesis pathway and the apoptosis suppressor, BCL2, and includes both positive and negative correlations. The second network shows a negative interaction between the p53 tumour suppressor protein and the glucose transporter type 4. Conclusion: The comprehensive pathway network will help us to realise the cooperative behaviours among pathways. Regulation of metabolic pathways is an important role of p53. The pathway involving the tumour suppressor gene p53 could regulate tumour angiogenesis. Further investigation of the proteins that interact with this pathway in this type of tumour may provide new strategies for cancer therapies to specifically inhibit the molecules that play crucial roles in tumour progression.
Published: 2011

34. Prognostic impact of disseminated tumor cells and microRNA-17-92 cluster deregulation in gastrointestinal cancer

Author: Valladares-Ayerbes, Manuel, Blanco, Moisés, Haz, Mar, Medina, Vanessa, Iglesias-Díaz, Pilar, Lorenzo-Patiño, María J., Reboredo, Margarita, Santamarina, Isabel, Figueroa, Angélica, Antón-Aparicio, Luis M., Calvo, Lourdes, Valladares-Ayerbes, Manuel, Blanco, Moisés, Haz, Mar, Medina, Vanessa, Iglesias-Díaz, Pilar, Lorenzo-Patiño, María J., Reboredo, Margarita, Santamarina, Isabel, Figueroa, Angélica, Antón-Aparicio, Luis M., and Calvo, Lourdes
Abstract: [Abstract] The presence of tumor cells in the bone marrow (BM) could be relevant to identifying high risk of disease progression and death in gastrointestinal cancer. However, the molecular profile associated with disseminated tumor cells (DTCs) homing to the BM has yet to be defined. MicroRNAs (miRNA) play key roles in cellular processes implicated in cancer. Thus, we investigated in 38 patients with colorectal, gastric or pancreatic cancer whether the presence of BM-DTCs is associated with a specific miRNA tumor profile and analyzed their potential prognostic impact. DTCs were detected by immunocytochemistry and anti-cytokeratin antibodies in 42.1% of the patients. miRNAs were isolated from formalin-fixed, paraffin-embedded tumors. qRT-PCR was used for miRNA profiling. No significant associations were found among DTC detection and miRNA deregulation. Kaplan-Meier curves demonstrated significantly reduced progression-free survival (PFS) and overall survival (OS) in the DTC-positive patients. Although miR-21 was upregulated in 90.6% of the tumors, no associations with outcomes were found. miR-17 and miR-20a (miRNA-17-92 cluster) were upregulated in 33.3 and 42.4%, respectively. Upregulation of both was correlated and found in 30.3%. Univariate analysis shows that increasing values for miR-20a were significantly associated with reduced PFS (HR 1.022; p=0.016) and OS (HR 1.027; p=0.003). In multivariate Cox models, DTC positivity (HR 4.07; p=0.005) and miR-17 overexpression (HR 2.11; p=0.003) were significantly associated with a higher risk of disease progression. The presence of DTCs in the BM (HR 3.98; p=0.010) and a miR-17 overexpression (HR 2.62; p<0.001) were also associated with a risk of death. Our study suggests that the presence of BM-DTCs and the upregulation of the miR-17-92 cluster in tumors are both significant but independent prognostic markers in gastrointestinal cancer patients.
Published: 2011

35. New insights into molecular mechanisms of sunitinib-associated side effects

Author: Aparicio Gallego, Guadalupe, Blanco, Moisés, Figueroa, Angélica, García-Campelo, Rosario, Valladares-Ayerbes, Manuel, Grande Pulido, Enrique, Antón-Aparicio, Luis M., Aparicio Gallego, Guadalupe, Blanco, Moisés, Figueroa, Angélica, García-Campelo, Rosario, Valladares-Ayerbes, Manuel, Grande Pulido, Enrique, and Antón-Aparicio, Luis M.
Abstract: [Abstract] The introduction of targeted therapy represents a major advance in the treatment of tumor progression. Targeted agents are a novel therapeutic approach developed to disrupt different cellular signaling pathways. The tyrosine kinase inhibitor sunitinib specifically blocks multiple tyrosine kinase receptors that are involved in the progression of many tumors. Sunitinib is the current standard of care in first-line treatment of advanced renal cell carcinoma, and it is approved in imatinib-intolerant and imatinib-refractory gastrointestinal stromal tumors. However, it is increasingly evident that sunitinib may display collateral effects on other proteins beyond its main target receptors, eliciting undesirable and unexpected adverse events. A better understanding of the molecular mechanisms underlying these undesirable sunitinib-associated side effects will help physicians to maximize efficacy of sunitinib and minimize adverse events. Here, we focus on new insights into molecular mechanisms that may mediate sunitinib-associated adverse events.
Published: 2011

36. Sunitinib-induced asthenia: from molecular basis to clinical relief

Author: Antón-Aparicio, Luis M., Grande Pulido, Enrique, Aparicio Gallego, Guadalupe, Antón-Aparicio, Luis M., Grande Pulido, Enrique, and Aparicio Gallego, Guadalupe
Abstract: [Abstract] Asthenia-fatigue syndrome (AFS) is defined as a persistent, subjective sense of tiredness related to cancer or its treatment and greatly impacts quality of life among cancer patients. All tyrosine kinase inhibitors, but especially sunitinib, may induce AFS. The reason for sunitinib-induced AFS is not yet well understood. Adverse events caused by sunitinib associated with AFS may include anemia, hypothyroidism, nausea and vomiting. However, AFS is also reported when active treatment with sunitinib is ongoing, and no other relevant adverse event can justify it. The molecular mechanisms by which sunitinib triggers AFS remain elusive. Sunitinib displays multiple off-target tyrosine-kinase interactions and competitively inhibits multiple proteins through the blockade of their ATP-binding sites. The broad spectrum of kinases inhibited may play a key role not only in terms of activity but also in terms of toxicity induced by sunitinib. This study considered different clinical observations and current metabolic and pharmacological knowledge, leading to hypotheses regarding which molecular mechanisms may be involved in sunitinib-induced AFS in cancer patients. Deeper knowledge of the molecular mode of action of sunitinib may lead to improved optimization of its clinical use.
Published: 2011

37. A novel procedure for protein extraction from formalin-fixed paraffin-embedded tissues

Author: Rodríguez-Rigueiro, Teresa, Valladares-Ayerbes, Manuel, Haz, Mar, Blanco, Moisés, Aparicio Gallego, Guadalupe, Fernández-Puente, Patricia, Blanco García, Francisco J, Lorenzo-Patiño, María J., Antón-Aparicio, Luis M., Figueroa, Angélica, Rodríguez-Rigueiro, Teresa, Valladares-Ayerbes, Manuel, Haz, Mar, Blanco, Moisés, Aparicio Gallego, Guadalupe, Fernández-Puente, Patricia, Blanco García, Francisco J, Lorenzo-Patiño, María J., Antón-Aparicio, Luis M., and Figueroa, Angélica
Abstract: [Abstract] Most of the archived pathological specimens in hospitals are kept as formalin-fixed paraffin-embedded tissues (FFPE) for long-term preservation. Up to now, these samples are only used for immunohistochemistry in a clinical routine as it is difficult to recover intact protein from these FFPE tissues. Here, we report a novel, short time-consuming and cost-effective method to extract full-length, non-degraded proteins from FFPE tissues. This procedure is combined with an effective and non-toxic deparaffinisation process and an extraction method based on antigen-retrieval, high concentration of SDS and high temperature. We have obtained enough intact protein to be detected by Western blotting analysis. This technique will allow utilising these stored FFPE tissues in several applications for protein analysis helping to advance the translational studies in cancer and other diseases.
Published: 2011

38. Hakai reduces cell-substratum adhesion and increases epithelial cell invasion

Author: Rodríguez-Rigueiro, Teresa, Valladares-Ayerbes, Manuel, Haz, Mar, Antón-Aparicio, Luis M., Figueroa, Angélica, Rodríguez-Rigueiro, Teresa, Valladares-Ayerbes, Manuel, Haz, Mar, Antón-Aparicio, Luis M., and Figueroa, Angélica
Abstract: [Abstract] Background. The dynamic regulation of cell-cell adhesions is crucial for developmental processes, including tissue formation, differentiation and motility. Adherens junctions are important components of the junctional complex between cells and are necessary for maintaining cell homeostasis and normal tissue architecture. E-cadherin is the prototype and best-characterized protein member of adherens junctions in mammalian epithelial cells. Regarded as a tumour suppressor, E-cadherin loss is associated with poor prognosis in carcinoma. The E3 ubiquitin-ligase Hakai was the first reported posttranslational regulator of the E-cadherin complex. Hakai specifically targetted E-cadherin for internalization and degradation and thereby lowered epithelial cell-cell contact. Hakai was also implicated in controlling proliferation, and promoted cancer-related gene expression by increasing the binding of RNA-binding protein PSF to RNAs encoding oncogenic proteins. We sought to investigate the possible implication of Hakai in cell-substratum adhesions and invasion in epithelial cells. Methods. Parental MDCK cells and MDCK cells stably overexpressing Hakai were used to analyse cell-substratum adhesion and invasion capabilities. Western blot and immunofluoresecence analyses were performed to assess the roles of Paxillin, FAK and Vinculin in cell-substratum adhesion. The role of the proteasome in controlling cell-substratum adhesion was studied using two proteasome inhibitors, lactacystin and MG132. To study the molecular mechanisms controlling Paxillin expression, MDCK cells expressing E-cadherin shRNA in a tetracycline-inducible manner was employed. Results. Here, we present evidence that implicate Hakai in reducing cell-substratum adhesion and increasing epithelial cell invasion, two hallmark features of cancer progression and metastasis. Paxillin, an important protein component of the cell-matrix adhesion, was completely absent from focal adhesions and focal contacts in
Published: 2011

39. Fructose transporter Glut5 expression in clear renal cell carcinoma

Author: Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Valbuena Ruvira, L., García Campelo, R., Valladares-Ayerbes, Manuel, Grande Pulido, Enrique, Bolós Fernández, Victoria, Santamarina, Isabel, Antón-Aparicio, Luis M., Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Valbuena Ruvira, L., García Campelo, R., Valladares-Ayerbes, Manuel, Grande Pulido, Enrique, Bolós Fernández, Victoria, Santamarina, Isabel, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Renal cell carcinomas (RCC) can be subclassified for general purposes into clear cell, papillary cell, chromophobe cell carcinomas and oncocytomas. Other tumours such as collecting duct, medullary, mucinous tubular and spindle cell and associated with Xp 11.2 translocations/TFE 3 gene fusion, are much less common. There is also a residual group of unclassified cases. Previous studies have shown that RCC has high glycolytic rates, and expresses GLUT transporters, but no distinction has been made among the different subtypes of renal cell tumours and their grades of malignancy. In clear renal cell carcinoma (cRCC) glycogen levels increase, glycolysis is activated and gluconeogenesis is reduced. The clear cell subtype of RCC is characterized histologically by a distinctive pale, glassy cytoplasm and this appearance of cRCC is due to abnormalities in carbohydrate and lipid metabolism, and this abnormality results in glycogen and sterol storage. Several isoforms of glucose carriers (GLUTs) have been identified. We show here in a panel of 80 cRCC samples a significant correlation between isoform 5 (GLUT5) and many pathological parameters such as grade of differentiation, pelvis invasion and breaking capsule. GLUT5 expression also appears to associate more strongly with the clear cell RCC subtype. These data suggest a role for the GLUT5 isoform in fructose uptake that takes place in cRCC cells and which subsequently leads to the malignant RCC progression.
Published: 2010

40. Glucose transporter expression and the potential role of fructose in renal cell carcinoma: a correlation with pathological parameters

Author: Antón-Aparicio, Luis M., Medina Villaamil, Vanessa, Blanco, Moisés, Valbuena Ruvira, L., Rois, José Manuel, Valladares-Ayerbes, Manuel, García Campelo, Rosario, Bolós Fernández, Victoria, Grande Pulido, Enrique, Antón-Aparicio, Luis M., Medina Villaamil, Vanessa, Blanco, Moisés, Valbuena Ruvira, L., Rois, José Manuel, Valladares-Ayerbes, Manuel, García Campelo, Rosario, Bolós Fernández, Victoria, and Grande Pulido, Enrique
Abstract: [Abstract] All mammalian cells contain one or more members of the facilitative glucose transporter (GLUT) gene family. Glucose transporter membrane proteins (GLUT) regulate the movement of glucose between the extracellular and intracellular compartments, maintaining a constant supply of glucose available for metabolism. Tumor cells are highly energy-dependent, therefore GLUT overexpression is often observed. In fact, overexpression of GLUT1 has been correlated with hypoxia markers in several tumor types, including renal cell carcinoma (RCC). We retrospectively analyzed 80 paraffin-embedded RCC samples. The pattern of GLUT1-5 expression in RCC specimens was evaluated using tissue-array technology and correlated with histological tumor characteristics. Pathological parameters included tumor location, renal pelvis, vein and lymph vessel invasion, capsule breakage, histological subtype, Furhman grade, hilar invasion and tumor stage at diagnosis. The expression of five facilitative glucose transporters, GLUT1 (erythrocyte type), GLUT2 (liver type), GLUT3 (brain type), GLUT4 (muscle/fat type) and GLUT5 (small intestinal type), was semi-quantitatively analyzed. In non-parametric, Mann-Whitney U and Kruskal-Wallis tests, a significant positive correlation was consistently found between moderately differentiated RCC tissues and the expression of GLUT5 (p=0.024). Patients who had pelvic invasion and capsule breakage at diagnosis also showed increased GLUT5 expression levels (p=0.039 and p=0.019, respectively). Moreover, GLUT5 showed statistical significance in those samples identified as being of clear cell histological type (p=0.001). A high expression of GLUT5 in human RCC was observed. GLUT5 appears to be correlated with grade II differentiation, locoregional invasion and aggressiveness, and may play a role in RCC development.
Published: 2010

41. Potential role of sugar transporters in cancer and their relationship with anticancer therapy

Author: Blanco, Moisés, Figueroa, Angélica, Grande Pulido, Enrique, García Campelo, Rosario, Antón-Aparicio, Luis M., Blanco, Moisés, Figueroa, Angélica, Grande Pulido, Enrique, García Campelo, Rosario, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Sugars, primarily glucose and fructose, are the main energy source of cells. Because of their hydrophilic nature, cells use a number of transporter proteins to introduce sugars through their plasma membrane. Cancer cells are well known to display an enhanced sugar uptake and consumption. In fact, sugar transporters are deregulated in cancer cells so they incorporate higher amounts of sugar than normal cells. In this paper, we compile the most significant data available about biochemical and biological properties of sugar transporters in normal tissues and we review the available information about sugar carrier expression in different types of cancer. Moreover, we describe the possible pharmacological interactions between drugs currently used in anticancer therapy and the expression or function of facilitative sugar transporters. Finally, we also go into the insights about the future design of drugs targeted against sugar utilization in cancer cells.
Published: 2010

42. Evaluation of Plakophilin-3 mRNA as a biomarker for detection of circulating tumor cells in gastrointestinal cancer patients

Author: Valladares-Ayerbes, Manuel, Díaz-Prado, Silvia, Reboredo, Margarita, Medina, Vanessa, Lorenzo-Patiño, María J., Iglesias-Díaz, Pilar, Haz, Mar, Pértega-Díaz, Sonia, Santamarina, Isabel, Blanco, Moisés, Quindós-Varela, María, Figueroa, Angélica, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Díaz-Prado, Silvia, Reboredo, Margarita, Medina, Vanessa, Lorenzo-Patiño, María J., Iglesias-Díaz, Pilar, Haz, Mar, Pértega-Díaz, Sonia, Santamarina, Isabel, Blanco, Moisés, Quindós-Varela, María, Figueroa, Angélica, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Background: This study aims to assess Plakophilin-3 (PKP3) as a surrogate biomarker of circulating tumor cells in patients with gastrointestinal cancer. Methods: The primary aim is to estimate the diagnostic accuracy of PKP3 real-time reverse transcriptase-PCR in blood. Receiver operating characteristic curves were constructed. Correlations between the blood PKP3 levels and the clinicopathologic features of the study subjects were analyzed. Logistic regression was used to predict outcomes based on PKP3. Results: Sixty-four patients with gastrointestinal cancer and 23 controls were included. The mean relative PKP3 mRNA expression was 48.45 in cancer patients and 2.8 in controls (P < 0.0001). Comparing the PKP3 levels in patients and controls, the area under the curve was 0.852 (95% confidence interval, 0.76-0.94; P < 0.0001) in receiver operating characteristic analysis. A higher blood level of PKP3 mRNA was associated with a more advanced stage (P = 0.025), pT3-4 tumors (P = 0.028), metastasis (P = 0.021), and residual (R2) disease (P = 0.037). Higher PKP3 mRNA was associated with the risk of cancer progression and death (odds ratio, 3.875; 95% confidence interval, 1.781-8.430; P = 0.001). Conclusions: Increased PKP3 mRNA was detected in the blood of gastrointestinal cancer patients. Significant correlations were found with advanced stage, pT3-4, metastatic disease, and the residual disease status. PKP3 mRNA in blood was associated with the risk of cancer progression and death.
Published: 2010

43. Evaluation of COX-2, EGFR, and p53 as biomarkers of non-dysplastic oral leukoplakias

Author: Díaz-Prado, Silvia, López Cedrún, José Luis, Luaces Rey, Ramón, Medina Villaamil, Vanessa, Álvarez García, Augusto, Valladares-Ayerbes, Manuel, Antón-Aparicio, Luis M., Díaz-Prado, Silvia, López Cedrún, José Luis, Luaces Rey, Ramón, Medina Villaamil, Vanessa, Álvarez García, Augusto, Valladares-Ayerbes, Manuel, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Objective. Identify candidate SEBs (surrogate endpoint biomarkers) for premalignant trends in head and neck mucosa. Study design. Study, by qPCR (quantitative real-time polymerase chain reaction), the expression of COX-2, EGFR and p53 in 24 biopsies of non-dysplastic oral leukoplakia and contra-lateral normal-appearing mucosa. Results. COX-2 was up-regulated in leukoplakia (79.2%); whereas EGFR and p53 were up-regulated (p > 0.05) in oral contra-lateral normal-appearing mucosa (60% and 46% respectively). Also, p53 expression was correlated with tobacco smoke habits and Spearman's rank correlation coefficient showed a positive linear correlation between p53 and EGFR mRNA expression levels. Conclusions. COX-2 would serve as SEB of oral leukoplakia. The results suggest that p53 appears to be one of the molecular targets of tobacco-related carcinogens in leukoplakia and that the co-expression of p53 and EGFR may play a role in this kind of oral pre-cancerous lesion. More detailed studies of EGFR and p53 should be continued in the future.
Published: 2010

44. Comprehensive lung injury pathology induced by mTOR inhibitors

Author: Aparicio Gallego, Guadalupe, Medina, Vanessa, Fernández, Ovidio, Jiménez, Paula, Lema, Martina, Figueroa, Angélica, Antón-Aparicio, Luis M., Aparicio Gallego, Guadalupe, Medina, Vanessa, Fernández, Ovidio, Jiménez, Paula, Lema, Martina, Figueroa, Angélica, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Interstitial lung disease is a rare side effect of temsirolimus treatment in renal cancer patients. Pulmonary fibrosis is characterised by the accumulation of extracellular matrix collagen, fibroblast proliferation and migration, and loss of alveolar gas exchange units. Previous studies of pulmonary fibrosis have mainly focused on the fibro-proliferative process in the lungs. However, the molecular mechanism by which sirolimus promotes lung fibrosis remains elusive. Here, we propose an overall cascade hypothesis of interstitial lung diseases that represents a common, partly underlying synergism among them as well as the lung pathogenesis side effects of mammalian target of rapamycin inhibitors.
Published: 2009

45. La ciclooxigenasa-2 (COX-2) y el factor de crecimiento epidérmico (EFG) en lesiones epiteliales orales premalignas

Author: Díaz-Prado, Silvia, Antón-Aparicio, Luis M., Gallego Guadalupe, A., López-Cedrún Cembranos, José Luis, Ferreras Granado, José, Díaz-Prado, Silvia, Antón-Aparicio, Luis M., Gallego Guadalupe, A., López-Cedrún Cembranos, José Luis, and Ferreras Granado, José
Abstract: [Resumen] Las lesiones premalignas orales incluyen eritroplasias (manchas rojas) y leucoplasias (manchas blancas), las cuales se desarrollan a lo largo de superficies epiteliales. Estas lesiones son considerados marcadores en la “car- cinogénesis de campo” ya que pacientes con lesiones premalignas orales pue- den desarrollar carcinoma de células escamosas (CCS) en el sitio de las lesio- nes, así como en otros lugares de tracto aerodigestivo superior. Se está hacien- do un gran esfuerzo para identificar nuevos biomarcadores SEBs (surrogate endpoint biomarkers) para el carcinoma de células escamosas de cabeza y cue- llo. Los SEBs candidatos para el carcinoma de células escamosas invasivo en el trato aerodigestivo superior deben ser detectables con los cambios molecu- lares celulares y tisulares que tienen lugar durante la formación del tumor. Entre los diferentes marcadores que se han propuesto hasta la actualidad, la ciclo- oxigenasa-2 (COX-2) y el receptor del factor de crecimiento epidérmico (EGFR) parecen ser los más prometedores. COX-2 se sobre expresa durante el pro- ceso tumoral, desde hiperplasia temprana a enfermedad metastásica. EGFR también está anormalmente activado en tumores epiteliales, pues las células de casi todas estas neoplasias expresan altos niveles de este receptor, una carac- terística asociada con un peor pronóstico clínico. En este sentido el tracto aero- digestivo superior proporciona un sistema o modelo único para el estudio de CCS y para la investigación de nuevos candidatos SEBs, [Abstract] Oral premalignant lesions include leukoplakia (white patch) and erythroplakia (red patch), which develop on epithelial surfaces. These lesions are markers for field cancerization because patients with oral premalignancy can develop squamous cell carcinoma at the site of the lesion(s) and at other sites in the upper aerodigestive tract. An effort is being made to identify surrogate endpoint biomarkers (SEBs) for head and neck squamous cell carcinoma (HNSCC). Candidate SEBs for invasive squamous cell carcinoma (SCC) of the upper aerodigestive tract are detectable molecular, cellular, and tissue changes that take place during tumorigenesis. Among the markers that have been proposed to date, cyclooxygenase-2 (COX-2) and the epidermal growth factor receptor (EGFR) seem to be the most promising. COX-2 is overexpressed during tumor transformation from early hyperplasia to metastasic disease. EGFR is also abnormally activated in epithelial tumors, since cells of almost all these kinds of neoplasm express high levels of this receptor, a characteristic associated with poor clinical outcome. The upper aerodigestive tract provides a unique model for studying the development of squamous cell carcinoma and for investigating candidate SEBs.
Published: 2009

46. Expression of Wnt gene family and frizzled receptors in head and neck squamous cell carcinomas

Author: Díaz-Prado, Silvia, Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Blanco, Moisés, López Cedrún, José Luis, Sironvalle Soliva, Sheila, Valladares-Ayerbes, Manuel, García Campelo, Rosario, Antón-Aparicio, Luis M., Díaz-Prado, Silvia, Medina Villaamil, Vanessa, Aparicio Gallego, Guadalupe, Blanco, Moisés, López Cedrún, José Luis, Sironvalle Soliva, Sheila, Valladares-Ayerbes, Manuel, García Campelo, Rosario, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Genes of the Wnt and Frizzled class, expressed in HNSCC tissue and cell lines, have an established role in cell morphogenesis and differentiation, and also they have oncogenic properties. We studied Wnt and Fz genes as potential tumor-associated markers in HNSCC by qPCR. Expression levels of Wnt and Fz genes in 22 unique frozen samples from HNSCC were measured. We also assessed possible correlation between the expression levels obtained in cancer samples in relation to clinicopathologic outcome. Wnt-1 was not expressed in the majority of the HNSCC studied, whereas Wnt-5A was the most strongly expressed by the malignant tumors. Wnt-10B expression levels were related with higher grade of undifferentiation. Related to Fz genes, Fz-5 showed more expression levels in no-affectation of regional lymph nodes. Kaplan–Meier survival analyses suggest a reduced time of survival for low and high expression of Wnt-7A and Fz-5 mRNA, respectively. qPCR demonstrated that HNSCC express Wnt and Fz members, and suggested that Wnt and Fz signaling is activated in HNSCC cells.
Published: 2009

47. Regional analysis of a cohort compassionate-use program (CUP) and early access program (EAP) with cabazitaxel (Cbz) plus prednisone (P; Cbz + P) in patients (pts) with metastatic castration-resistant prostate cancer (mCRPC) previously treated with docetaxel (D).

Author: Malik, Zafar, primary, di Lorenzo, Giuseppe, additional, Bracarda, Sergio, additional, Ardavanis, Alexandros, additional, Basaran, Mert, additional, Parente, Phillip, additional, de Schultz, Wito, additional, Saad, Fred, additional, van Oort, Inge, additional, Gerritsen, Winald R., additional, Antón Aparicio, Luis M., additional, Matus, Geoffrey, additional, Hitier, Simon, additional, Heidenreich, Axel, additional, and Bahl, Amit, additional
Published: 2014
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48. Cohort compassionate-use program (CUP) and early access program (EAP) with cabazitaxel (Cbz) plus prednisone (P; Cbz + P) in patients (pts) with metastatic castration-resistant prostate cancer (mCRPC) previously treated with docetaxel (D): Analysis by age group.

Author: Malik, Zafar, primary, di Lorenzo, Giuseppe, additional, Bracarda, Sergio, additional, Ardavanis, Alexandros, additional, Basaran, Mert, additional, Parente, Phillip, additional, de Schultz, Wito, additional, Saad, Fred, additional, van Oort, Inge, additional, Gerritsen, Winald R., additional, Antón Aparicio, Luis M., additional, Matus, Geoffrey, additional, Hitier, Simon, additional, Heidenreich, Axel, additional, and Bahl, Amit, additional
Published: 2014
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49. Origin of renal cell carcinomas

Author: Valladares-Ayerbes, Manuel, Aparicio Gallego, Guadalupe, Díaz-Prado, Silvia, Jiménez Fonseca, P., García Campelo, Rosario, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Aparicio Gallego, Guadalupe, Díaz-Prado, Silvia, Jiménez Fonseca, P., García Campelo, Rosario, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Cancer is a heritable disorder of somatic cells: environment and heredity are both important in the carcinogenic process. The primal force is the “two hits” of Knudson’s hypothesis, which has proved true for many tumours, including renal cell carcinoma. Knudson et al. [1, 2] recognised that familial forms of cancer might hold the key to the identification of important regulatory elements known as tumour-suppressor genes. Their observations (i.e., that retinoblastoma tend to be multifocal in familial cases and unifocal in sporadic presentation) led them to propose a two-hit theory of carcinogenesis. Furthermore, Knudson postulated that patients with the familial form of the cancer would be born with one mutant allele and that all cells in that organ or tissue would be at risk, accounting for early onset and the multifocal nature of the disease. In contrast, sporadic tumours would develop only if a mutation occurred in both alleles within the same cell, and, as each event would be expected to occur with low frequency, most tumours would develop late in life and in a unifocal manner [3, 4]. The kidney is affected in a variety of inherited cancer syndromes. For most of them, both the oncogene/tumour-suppressor gene involved and the respective germline mutations have been identified. Each of the inherited syndromes predisposes to distinct types of renal carcinoma. Families with hereditary predisposition to cancer continue to provide a unique opportunity for the identification and characterisation of genes involved in carcinogenesis. A surprising number of genetic syndromes predispose to the development of renal cell carcinoma, and genes associated with five of these syndromes have been already identified: VHL, MET, FH, BHD and HRPT2. Few cancers have as many different types of genetic predisposition as renal cancer, although to date only a small proportion of renal cell cancers can be explained by genetic predisposition.
Published: 2008

50. Bioinformatics approach to mRNA markers discovery for detection of circulating tumor cells in patients with gastrointestinal cancer

Author: Valladares-Ayerbes, Manuel, Díaz Prado, Silvia, Reboredo, Margarita, Medina Villaamil, Vanessa, Iglesias-Díaz, Pilar, Lorenzo-Patiño, María J., Campelo, Rosario G., Haz, Mar, Santamarina, Isabel, Antón-Aparicio, Luis M., Valladares-Ayerbes, Manuel, Díaz Prado, Silvia, Reboredo, Margarita, Medina Villaamil, Vanessa, Iglesias-Díaz, Pilar, Lorenzo-Patiño, María J., Campelo, Rosario G., Haz, Mar, Santamarina, Isabel, and Antón-Aparicio, Luis M.
Abstract: [Abstract] Background: Detection of tumor cells in the blood, or minimal deposits in distant organs as bone marrow, could be important to identify cancer patients at high risk of relapse or disease progression. Quantitative polymerase chain reaction (PCR) amplification of tissue or tumor selective mRNA is the most powerful tool for the detection of this circulating or occult metastatic cells. Our study aims to identify novel gastrointestinal cancer-specific markers for circulating tumor cell detection. Method: Phase I preclinical study was performed by means of computational tools for expression analysis. In silico data were used to identify and prioritize molecular markers highly expressed in gastrointestinal cancers but absent in hematopoietic-derived libraries. Selected genes were evaluated by means of qRT-PCR in gastrointestinal cancer and hematopoietic cell-lines, normal human bone marrows and bloods, tumor tissue, and blood from cancer patients. Results: Novel and known mRNA markers for circulating tumor cell detection in gastrointestinal cancer have been identified. Among all the genes assessed, PKP3, AGR2, S100A16, S100A6, LGALS4, and CLDN3 were selected and assays based on blood qRT-PCR were developed. Reliably qRT-PCR assays for the novel targets plakophilin 3 (PKP3) and anterior gradient-2 (AGR2) to identify blood-borne cells in cancer patients were developed. Conclusions: Novel and known gastrointestinal-specific mRNA markers for circulating tumor cells have been identified through in silico analysis and validated in clinical material. qRT-PCR assay targeted to PKP3 and AGR2 mRNAs might be helpful to detect circulating tumor cells in patients with gastrointestinal cancer.
Published: 2008

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