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2. Cancer Nano-Immunotherapy: The Novel and Promising Weapon to Fight Cancer

Author

Junta de Andalucía, Instituto de Salud Carlos III, Universidad de Sevilla, García-Domínguez, D. J. [0000-0001-8150-2747], López-Enríquez, Soledad [0000-0003-3727-1843], Flores-Campos, Rocío [0000-0002-2563-4136], Hontecillas-Prieto, Lourdes [0000-0002-0582-3386], Consejo Superior de Investigaciones Científicas [https://ror.org/02gfc7t72], García-Domínguez, D. J., López-Enríquez, Soledad, Alba, Gonzalo, Garnacho-Montero, Carmen, Jiménez-Cortegana, Carlos, Flores-Campos, Rocío, Cruz-Merino, Luis de la, Hajji, Nabil, Sánchez-Margalet, Víctor, Hontecillas-Prieto, Lourdes, Junta de Andalucía, Instituto de Salud Carlos III, Universidad de Sevilla, García-Domínguez, D. J. [0000-0001-8150-2747], López-Enríquez, Soledad [0000-0003-3727-1843], Flores-Campos, Rocío [0000-0002-2563-4136], Hontecillas-Prieto, Lourdes [0000-0002-0582-3386], Consejo Superior de Investigaciones Científicas [https://ror.org/02gfc7t72], García-Domínguez, D. J., López-Enríquez, Soledad, Alba, Gonzalo, Garnacho-Montero, Carmen, Jiménez-Cortegana, Carlos, Flores-Campos, Rocío, Cruz-Merino, Luis de la, Hajji, Nabil, Sánchez-Margalet, Víctor, and Hontecillas-Prieto, Lourdes

Abstract

Cancer is a complex disease that, despite advances in treatment and the greater understanding of the tumor biology until today, continues to be a prevalent and lethal disease. Chemotherapy, radiotherapy, and surgery are the conventional treatments, which have increased the survival for cancer patients. However, the complexity of this disease together with the persistent problems due to tumor progression and recurrence, drug resistance, or side effects of therapy make it necessary to explore new strategies that address the challenges to obtain a positive response. One important point is that tumor cells can interact with the microenvironment, promoting proliferation, dissemination, and immune evasion. Therefore, immunotherapy has emerged as a novel therapy based on the modulation of the immune system for combating cancer, as reflected in the promising results both in preclinical studies and clinical trials obtained. In order to enhance the immune response, the combination of immunotherapy with nanoparticles has been conducted, improving the access of immune cells to the tumor, antigen presentation, as well as the induction of persistent immune responses. Therefore, nanomedicine holds an enormous potential to enhance the efficacy of cancer immunotherapy. Here, we review the most recent advances in specific molecular and cellular immunotherapy and in nano-immunotherapy against cancer in the light of the latest published preclinical studies and clinical trials.

Published
2024

3. DataSheet_1_CD8+ NKs as a potential biomarker of complete response and survival with lenalidomide plus R-GDP in the R2-GDP-GOTEL trial in recurrent/refractory diffuse large B cell lymphoma.pdf

Author

Hontecillas-Prieto, Lourdes [0000-0002-0582-3386], García-Domínguez, D. J. [0000-0001-8150-2747], Flores-Campos, Rocío [0000-0002-2563-4136], Hontecillas-Prieto, Lourdes, García-Domínguez, D. J., Palazón-Carrión, Natalia, Martín García-Sancho, Alejandro, Nogales Fernández, Esteban, Jiménez-Cortegana, Carlos, Sánchez-León, María L., Silva-Romeiro, Silvia, Flores-Campos, Rocío, Carnicero-González, Fernando, Rios-Herranz, Eduardo, Cruz-Vicente, Fátima de la, Rodríguez-García, Guillermo, Fernández-Álvarez, Rubén, Martínez-Banaclocha, Natividad, Gumà-Padrò, Josep, Gómez Codina, José, Salar-Silvestre, Antonio, Rodríguez-Abreu, Delvys, Gálvez-Carvajal, Laura, Labrador, Jorge, Guirado-Risueño, María, Provencio, Mariano, Sánchez-Beato, Margarita, Marylene, Lejeune, Álvaro Naranjo, Tomás, Casanova-Espinosa, María, Rueda-Domínguez, Antonio, Sánchez-Margalet, Víctor, Cruz-Merino, Luis de la, Hontecillas-Prieto, Lourdes [0000-0002-0582-3386], García-Domínguez, D. J. [0000-0001-8150-2747], Flores-Campos, Rocío [0000-0002-2563-4136], Hontecillas-Prieto, Lourdes, García-Domínguez, D. J., Palazón-Carrión, Natalia, Martín García-Sancho, Alejandro, Nogales Fernández, Esteban, Jiménez-Cortegana, Carlos, Sánchez-León, María L., Silva-Romeiro, Silvia, Flores-Campos, Rocío, Carnicero-González, Fernando, Rios-Herranz, Eduardo, Cruz-Vicente, Fátima de la, Rodríguez-García, Guillermo, Fernández-Álvarez, Rubén, Martínez-Banaclocha, Natividad, Gumà-Padrò, Josep, Gómez Codina, José, Salar-Silvestre, Antonio, Rodríguez-Abreu, Delvys, Gálvez-Carvajal, Laura, Labrador, Jorge, Guirado-Risueño, María, Provencio, Mariano, Sánchez-Beato, Margarita, Marylene, Lejeune, Álvaro Naranjo, Tomás, Casanova-Espinosa, María, Rueda-Domínguez, Antonio, Sánchez-Margalet, Víctor, and Cruz-Merino, Luis de la

Abstract

[Background] Diffuse large B cell lymphoma (DLBCL) is the most common non-Hodgkin lymphoma worldwide. DLBCL is an aggressive disease that can be cured with upfront standard chemoimmunotherapy schedules. However, in approximately 35-40% of the patients DLBCL relapses, and therefore, especially in this setting, the search for new prognostic and predictive biomarkers is an urgent need. Natural killer (NK) are effector cells characterized by playing an important role in antitumor immunity due to their cytotoxic capacity and a subset of circulating NK that express CD8 have a higher cytotoxic function. In this substudy of the R2-GDP-GOTEL trial, we have evaluated blood CD8+ NK cells as a predictor of treatment response and survival in relapsed/refractory (R/R) DLBCL patients., [Methods] 78 patients received the R2-GDP schedule in the phase II trial. Blood samples were analyzed by flow cytometry. Statistical analyses were carried out in order to identify the prognostic potential of CD8+ NKs at baseline in R/R DLBCL patients., [Results] Our results showed that the number of circulating CD8+ NKs in R/R DLBCL patients were lower than in healthy donors, and it did not change during and after treatment. Nevertheless, the level of blood CD8+ NKs at baseline was associated with complete responses in patients with R/R DLBCL. In addition, we also demonstrated that CD8+ NKs levels have potential prognostic value in terms of overall survival in R/R DLBCL patients., [Conclusion] CD8+ NKs represent a new biomarker with prediction and prognosis potential to be considered in the clinical management of patients with R/R DLBCL., [Clinical trial registration] https://www.clinicaltrialsregister.eu/ctr-search/search?query=2014-001620-29 EudraCT, ID:2014-001620-29.

Published
2024

4. Selective histone methyltransferase G9a inhibition reduces metastatic development of Ewing sarcoma through the epigenetic regulation of NEU1

Author

García-Domínguez, Daniel J., Hajji, Nabil, López-Alemany, Roser, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, Morón Civanto, Francisco J., Rello-Varona, Santiago, Andrés-León, Eduardo, Benito, Adrián, Keun, Hector C., Mora, Jaume, Tirado, Óscar M., de Álava, Enrique, and Hontecillas-Prieto, Lourdes

Published
2022
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5. Supplementary data for the biological age linked to oxidative stress modifies breast cancer aggressiveness

Author

del Mar Sáez-Freire, María, Blanco-Gómez, Adrián, Castillo-Lluva, Sonia, Gómez-Vecino, Aurora, Galvis-Jiménez, Julie Milena, Martín-Seisdedos, Carmen, Isidoro-García, María, Hontecillas-Prieto, Lourdes, García-Cenador, María Begoña, García-Criado, Francisco Javier, Patino-Alonso, María Carmen, Galindo-Villardón, Purificación, Mao, Jian-Hua, Prieto, Carlos, Castellanos-Martín, Andrés, Kaderali, Lars, and Pérez-Losada, Jesús

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Women's Health, Breast Cancer, Cancer, Aging, 2.1 Biological and endogenous factors, Good Health and Well Being, Biochemistry and Cell Biology, Genetics, Data management and data science
Abstract

The data presented in this article are related to the research paper entitled "The biological age linked to oxidative stress modifies breast cancer aggressiveness" (M.M. Sáez-Freire, A. Blanco-Gómez, S. Castillo-Lluva, A. Gómez-Vecino, J.M. Galvis-Jiménez, C. Martín-Seisdedos, M. Isidoro-García, L. Hontecillas-Prieto, M.B. García-Cenador, F.J. García-Criado, M.C. Patino-Alonso, P. Galindo-Villardón, J.H. Mao, C. Prieto, A. Castellanos-Martín, L. Kaderali, J. Pérez-Losada). The data shown were obtained from a population of transgenic mice, MMTV-Erbb2/Neu, with different susceptibility to breast cancer and a mixed genetic background generated by backcrossing. It was observed that the aggressiveness of breast cancer negatively correlates with age, being lower in chronologically old mice, similar to what occurs in humans. Given that oxidative stress is associated with tumour susceptibility and the degree of aging, the association between the aggressiveness of breast cancer and multiple intermediate phenotypes directly or indirectly related to oxidative stress was studied. Using a mathematical model, we defined biological age and the degree of aging as the difference between biological and chronological ages. As a result, we observed that biologically old mice predominated among those that developed the disease early on, that is, those that were chronologically young. We then identified the specific and common genetic components of Quantitative Trait loci or QTL associated with different evolution of breast cancer, the intermediate phenotypes related to oxidative stress studied, the biological age and the degree of aging. Lastly, we showed that the expression pattern in the livers of biologically old mice were enriched in signalling pathways related to inflammation and response to infections; whereas the biologically young mice exhibited enriched pathways related to mitochondrial activity. For the explanation and discussion of these data refer to the research article cited above.

Published
2018

6. Supplementary data for the biological age linked to oxidative stress modifies breast cancer aggressiveness.

Author

Sáez-Freire, María Del Mar, Blanco-Gómez, Adrián, Castillo-Lluva, Sonia, Gómez-Vecino, Aurora, Galvis-Jiménez, Julie Milena, Martín-Seisdedos, Carmen, Isidoro-García, María, Hontecillas-Prieto, Lourdes, García-Cenador, María Begoña, García-Criado, Francisco Javier, Patino-Alonso, María Carmen, Galindo-Villardón, Purificación, Mao, Jian-Hua, Prieto, Carlos, Castellanos-Martín, Andrés, Kaderali, Lars, and Pérez-Losada, Jesús

Abstract

The data presented in this article are related to the research paper entitled "The biological age linked to oxidative stress modifies breast cancer aggressiveness" (M.M. Sáez-Freire, A. Blanco-Gómez, S. Castillo-Lluva, A. Gómez-Vecino, J.M. Galvis-Jiménez, C. Martín-Seisdedos, M. Isidoro-García, L. Hontecillas-Prieto, M.B. García-Cenador, F.J. García-Criado, M.C. Patino-Alonso, P. Galindo-Villardón, J.H. Mao, C. Prieto, A. Castellanos-Martín, L. Kaderali, J. Pérez-Losada). The data shown were obtained from a population of transgenic mice, MMTV-Erbb2/Neu, with different susceptibility to breast cancer and a mixed genetic background generated by backcrossing. It was observed that the aggressiveness of breast cancer negatively correlates with age, being lower in chronologically old mice, similar to what occurs in humans. Given that oxidative stress is associated with tumour susceptibility and the degree of aging, the association between the aggressiveness of breast cancer and multiple intermediate phenotypes directly or indirectly related to oxidative stress was studied. Using a mathematical model, we defined biological age and the degree of aging as the difference between biological and chronological ages. As a result, we observed that biologically old mice predominated among those that developed the disease early on, that is, those that were chronologically young. We then identified the specific and common genetic components of Quantitative Trait loci or QTL associated with different evolution of breast cancer, the intermediate phenotypes related to oxidative stress studied, the biological age and the degree of aging. Lastly, we showed that the expression pattern in the livers of biologically old mice were enriched in signalling pathways related to inflammation and response to infections; whereas the biologically young mice exhibited enriched pathways related to mitochondrial activity. For the explanation and discussion of these data refer to the research article cited above.

Published
2018

7. The biological age linked to oxidative stress modifies breast cancer aggressiveness

Author

Sáez-Freire, María Del Mar, Blanco-Gómez, Adrián, Castillo-Lluva, Sonia, Gómez-Vecino, Aurora, Galvis-Jiménez, Julie Milena, Martín-Seisdedos, Carmen, Isidoro-García, María, Hontecillas-Prieto, Lourdes, García-Cenador, María Begoña, García-Criado, Francisco Javier, Patino-Alonso, María Carmen, Galindo-Villardón, Purificación, Mao, Jian-Hua, Prieto, Carlos, Castellanos-Martín, Andrés, Kaderali, Lars, and Pérez-Losada, Jesús

Subjects
Genetics, Digestive Diseases, Cancer, Aging, Women's Health, Breast Cancer, 2.1 Biological and endogenous factors, 1.1 Normal biological development and functioning, Animals, Breast Neoplasms, Female, Genes, erbB-2, Glutathione, Inflammation, Liver, Mice, Mice, Inbred C57BL, Mice, Transgenic, Models, Theoretical, Oxidative Stress, Proto-Oncogene Proteins c-akt, Quantitative Trait Loci, Receptor, ErbB-2, Transcriptome, Breast cancer, Biological age, Mouse genetics, Oxidative stress, Subphenotypes, Receptor, erbB-2, Medicinal and Biomolecular Chemistry, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics
Abstract

The incidence of breast cancer increases with age until menopause, and breast cancer is more aggressive in younger women. The existence of epidemiological links between breast cancer and aging indicates that both processes share some common mechanisms of development. Oxidative stress is associated with both cancer susceptibility and aging. Here we observed that ERBB2-positive breast cancer, which developed in genetically heterogeneous ERBB2-positive transgenic mice generated by a backcross, is more aggressive in chronologically younger than in older mice (differentiated by the median survival of the cohort that was 79 weeks), similar to what occurs in humans. In this cohort, we estimated the oxidative biological age using a mathematical model that integrated several subphenotypes directly or indirectly related to oxidative stress. The model selected the serum levels of HDL-cholesterol and magnesium and total AKT1 and glutathione concentrations in the liver. The grade of aging was calculated as the difference between the predicted biological age and the chronological age. This comparison permitted the identification of biologically younger and older mice compared with their chronological age. Interestingly, biologically older mice developed more aggressive breast cancer than the biologically younger mice. Genomic regions on chromosomes 2 and 15 linked to the grade of oxidative aging were identified. The levels of expression of Zbp1 located on chromosome 2, a gene related to necroptosis and inflammation, positively correlated with the grade of aging and tumour aggressiveness. Moreover, the pattern of gene expression of genes linked to the inflammation and the response to infection pathways was enriched in the livers of biologically old mice. This study shows part of the complex interactions between breast cancer and aging.

Published
2018

8. Integrin alpha9 emerges as a key therapeutic target to reduce metastasis in rhabdomyosarcoma and neuroblastoma

Author

Navarro, Natalia, Molist, Carla, Sansa-Girona, Júlia, Zarzosa, Patricia, Gallo-Oller, Gabriel, Pons, Guillem, Magdaleno, Ainara, Guillén, Gabriela, Hladun, Raquel, Garrido, Marta, Segura, Miguel F., Hontecillas-Prieto, Lourdes, de Álava, Enrique, Ponsati, Berta, Fernández-Carneado, Jimena, Almazán-Moga, Ana, Vallès-Miret, Mariona, Farrera-Sinfreu, Josep, de Toledo, Josep Sánchez, Moreno, Lucas, Gallego, Soledad, and Roma, Josep

Published
2022
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9. Selective inhibition of HDAC6 regulates expression of the oncogenic driver EWSR1-FLI1 through the EWSR1 promoter in Ewing sarcoma

Author

García-Domínguez, Daniel J., Hajji, Nabil, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, de Pablos, Rocío M., Espinosa-Oliva, Ana M., Andrés-León, Eduardo, Terrón-Camero, Laura Carmen, Flores-Campos, Rocío, Pascual-Pasto, Guillem, Robles, María José, Machado, Isidro, Llombart-Bosch, Antonio, Magagnoli, Giovanna, Scotlandi, Katia, Carcaboso, Ángel M., Mora, Jaume, de Álava, Enrique, and Hontecillas-Prieto, Lourdes

Published
2021
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10. Treatment-driven selection of chemoresistant Ewing sarcoma tumors with limited drug distribution

Author

Castillo-Ecija, Helena, Monterrubio, Carles, Pascual-Pasto, Guillem, Gomez-Gonzalez, Soledad, Garcia-Dominguez, Daniel J., Hontecillas-Prieto, Lourdes, Resa-Pares, Claudia, Burgueño, Victor, Paco, Sonia, Olaciregui, Nagore G., Vila-Ubach, Monica, Restrepo-Perdomo, Camilo, Cuadrado-Vilanova, Maria, Balaguer-Lluna, Leire, Perez-Jaume, Sara, Castañeda, Alicia, Santa-Maria, Vicente, Roldan, Monica, Suñol, Mariona, de Alava, Enrique, Mora, Jaume, Lavarino, Cinzia, and Carcaboso, Angel M.

Published
2020
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11. Missing heritability of complex diseases: Enlightenment by genetic variants from intermediate phenotypes

Author

Blanco-Gómez, Adrián, Castillo-Lluva, Sonia, Del Mar Sáez-Freire, María, Hontecillas-Prieto, Lourdes, Mao, Jian Hua, Castellanos-Martín, Andrés, and Pérez-Losada, Jesus

Subjects
Biological Sciences, Genetics, Human Genome, 2.1 Biological and endogenous factors, Generic health relevance, Animals, Genetic Diseases, Inborn, Genetic Predisposition to Disease, Genetic Variation, Genetics, Medical, Humans, Models, Genetic, Phenotype, complex diseases, heritability, intermediate phenotype or endophenotype, missing heritability, Medical and Health Sciences, Psychology and Cognitive Sciences, Developmental Biology, Biological sciences
Abstract

Diseases of complex origin have a component of quantitative genetics that contributes to their susceptibility and phenotypic variability. However, after several studies, a major part of the genetic component of complex phenotypes has still not been found, a situation known as "missing heritability." Although there have been many hypotheses put forward to explain the reasons for the missing heritability, its definitive causes remain unknown. Complex diseases are caused by multiple intermediate phenotypes involved in their pathogenesis and, very often, each one of these intermediate phenotypes also has a component of quantitative inheritance. Here we propose that at least part of the missing heritability can be explained by the genetic component of intermediate phenotypes that is not detectable at the level of the main complex trait. At the same time, the identification of the genetic component of intermediate phenotypes provides an opportunity to identify part of the missing heritability of complex diseases.

Published
2016

12. Cancer nano-immunotherapy: the novel and promising weapon to fight cancer

Author

Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Universidad de Sevilla. Departamento de Medicina, García-Domínguez, Daniel J., López Enriquez, Soledad, Alba Jiménez, Gonzalo, Garnacho Montero, Carmen, Jiménez Cortegana, Carlos, Flores-Campos, Rocío, Cruz Merino, Luis de la, Hajji, Nabil, Sánchez Margalet, Víctor, Hontecillas-Prieto, Lourdes, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Universidad de Sevilla. Departamento de Medicina, García-Domínguez, Daniel J., López Enriquez, Soledad, Alba Jiménez, Gonzalo, Garnacho Montero, Carmen, Jiménez Cortegana, Carlos, Flores-Campos, Rocío, Cruz Merino, Luis de la, Hajji, Nabil, Sánchez Margalet, Víctor, and Hontecillas-Prieto, Lourdes

Abstract

Cancer is a complex disease that, despite advances in treatment and the greater understanding of the tumor biology until today, continues to be a prevalent and lethal disease. Chemotherapy, radiotherapy, and surgery are the conventional treatments, which have increased the survival for cancer patients. However, the complexity of this disease together with the persistent problems due to tumor progression and recurrence, drug resistance, or side effects of therapy make it necessary to explore new strategies that address the challenges to obtain a positive response. One important point is that tumor cells can interact with the microenvironment, promoting proliferation, dissemination, and immune evasion. Therefore, immunotherapy has emerged as a novel therapy based on the modulation of the immune system for combating cancer, as reflected in the promising results both in preclinical studies and clinical trials obtained. In order to enhance the immune response, the combination of immunotherapy with nanoparticles has been conducted, improving the access of immune cells to the tumor, antigen presentation, as well as the induction of persistent immune responses. Therefore, nanomedicine holds an enormous potential to enhance the efficacy of cancer immunotherapy. Here, we review the most recent advances in specific molecular and cellular immunotherapy and in nano immunotherapy against cancer in the light of the latest published preclinical studies and clinical trials.

Published
2024

13. CD8+ NKs as a potential biomarker of complete response and survival with lenalidomide plus R-GDP in the R2-GDP-GOTEL trial in recurrent/refractory diffuse large B cell lymphoma

Author

Instituto de Salud Carlos III, Universidad de Sevilla, Celgene, Junta de Andalucía, Hontecillas-Prieto, Lourdes, García-Domínguez, D. J., Palazón-Carrión, Natalia, Martín García-Sancho, Alejandro, Nogales Fernández, Esteban, Jiménez-Cortegana, Carlos, Sánchez-León, María L., Silva-Romeiro, Silvia, Flores-Campos, Rocío, Carnicero-González, Fernando, Rios-Herranz, Eduardo, Cruz-Vicente, Fátima de la, Rodríguez-García, Guillermo, Fernández-Álvarez, Rubén, Martínez-Banaclocha, Natividad, Gumà-Padrò, Josep, Gómez Codina, José, Salar-Silvestre, Antonio, Rodríguez-Abreu, Delvys, Gálvez-Carvajal, Laura, Labrador, Jorge, Guirado-Risueño, María, Provencio, Mariano, Sánchez-Beato, Margarita, Marylene, Lejeune, Álvaro Naranjo, Tomás, Casanova-Espinosa, María, Rueda-Domínguez, Antonio, Sánchez-Margalet, Víctor, Cruz-Merino, Luis de la, Instituto de Salud Carlos III, Universidad de Sevilla, Celgene, Junta de Andalucía, Hontecillas-Prieto, Lourdes, García-Domínguez, D. J., Palazón-Carrión, Natalia, Martín García-Sancho, Alejandro, Nogales Fernández, Esteban, Jiménez-Cortegana, Carlos, Sánchez-León, María L., Silva-Romeiro, Silvia, Flores-Campos, Rocío, Carnicero-González, Fernando, Rios-Herranz, Eduardo, Cruz-Vicente, Fátima de la, Rodríguez-García, Guillermo, Fernández-Álvarez, Rubén, Martínez-Banaclocha, Natividad, Gumà-Padrò, Josep, Gómez Codina, José, Salar-Silvestre, Antonio, Rodríguez-Abreu, Delvys, Gálvez-Carvajal, Laura, Labrador, Jorge, Guirado-Risueño, María, Provencio, Mariano, Sánchez-Beato, Margarita, Marylene, Lejeune, Álvaro Naranjo, Tomás, Casanova-Espinosa, María, Rueda-Domínguez, Antonio, Sánchez-Margalet, Víctor, and Cruz-Merino, Luis de la

Abstract

Diffuse large B cell lymphoma (DLBCL) is the most common non-Hodgkin lymphoma worldwide. DLBCL is an aggressive disease that can be cured with upfront standard chemoimmunotherapy schedules. However, in approximately 35-40% of the patients DLBCL relapses, and therefore, especially in this setting, the search for new prognostic and predictive biomarkers is an urgent need. Natural killer (NK) are effector cells characterized by playing an important role in antitumor immunity due to their cytotoxic capacity and a subset of circulating NK that express CD8 have a higher cytotoxic function. In this substudy of the R2-GDP-GOTEL trial, we have evaluated blood CD8+ NK cells as a predictor of treatment response and survival in relapsed/refractory (R/R) DLBCL patients.

Published
2024

14. Unraveling heterogeneous susceptibility and the evolution of breast cancer using a systems biology approach.

Author

Castellanos-Martín, Andrés, Castillo-Lluva, Sonia, Sáez-Freire, María Del Mar, Blanco-Gómez, Adrián, Hontecillas-Prieto, Lourdes, Patino-Alonso, Carmen, Galindo-Villardon, Purificación, Pérez Del Villar, Luis, Martín-Seisdedos, Carmen, Isidoro-Garcia, María, Abad-Hernández, María Del Mar, Cruz-Hernández, Juan Jesús, Rodríguez-Sánchez, César Augusto, González-Sarmiento, Rogelio, Alonso-López, Diego, De Las Rivas, Javier, García-Cenador, Begoña, García-Criado, Javier, Lee, Do Yup, Bowen, Benjamin, Reindl, Wolfgang, Northen, Trent, Mao, Jian-Hua, and Pérez-Losada, Jesús

Subjects
Animals, Humans, Mice, Breast Neoplasms, Neoplasm Metastasis, Disease Progression, Receptor, erbB-2, Systems Biology, MAP Kinase Signaling System, Gene Expression Regulation, Neoplastic, Models, Genetic, Female, Proto-Oncogene Proteins c-akt, Receptor, ErbB-2, Receptor, erbB-2, Gene Expression Regulation, Neoplastic, Models, Genetic, ErbB-2, Breast Cancer, Cancer, Digestive Diseases, Genetics, 2.1 Biological and endogenous factors, Bioinformatics, Environmental Sciences, Biological Sciences, Information and Computing Sciences
Abstract

BackgroundAn essential question in cancer is why individuals with the same disease have different clinical outcomes. Progress toward a more personalized medicine in cancer patients requires taking into account the underlying heterogeneity at different molecular levels.ResultsHere, we present a model in which there are complex interactions at different cellular and systemic levels that account for the heterogeneity of susceptibility to and evolution of ERBB2-positive breast cancers. Our model is based on our analyses of a cohort of mice that are characterized by heterogeneous susceptibility to ERBB2-positive breast cancers. Our analysis reveals that there are similarities between ERBB2 tumors in humans and those of backcross mice at clinical, genomic, expression, and signaling levels. We also show that mice that have tumors with intrinsically high levels of active AKT and ERK are more resistant to tumor metastasis. Our findings suggest for the first time that a site-specific phosphorylation at the serine 473 residue of AKT1 modifies the capacity for tumors to disseminate. Finally, we present two predictive models that can explain the heterogeneous behavior of the disease in the mouse population when we consider simultaneously certain genetic markers, liver cell signaling and serum biomarkers that are identified before the onset of the disease.ConclusionsConsidering simultaneously tumor pathophenotypes and several molecular levels, we show the heterogeneous behavior of ERBB2-positive breast cancer in terms of disease progression. This and similar studies should help to better understand disease variability in patient populations.

Published
2015

15. Cancer Nano-Immunotherapy: The Novel and Promising Weapon to Fight Cancer

Author

García-Domínguez, Daniel J., primary, López-Enríquez, Soledad, additional, Alba, Gonzalo, additional, Garnacho, Carmen, additional, Jiménez-Cortegana, Carlos, additional, Flores-Campos, Rocío, additional, de la Cruz-Merino, Luis, additional, Hajji, Nabil, additional, Sánchez-Margalet, Víctor, additional, and Hontecillas-Prieto, Lourdes, additional

Published
2024
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16. DNA methylation profiling identifies PTRF/Cavin-1 as a novel tumor suppressor in Ewing sarcoma when co-expressed with caveolin-1

Author

Huertas-Martínez, Juan, Court, Franck, Rello-Varona, Santiago, Herrero-Martín, David, Almacellas-Rabaiget, Olga, Sáinz-Jaspeado, Miguel, Garcia-Monclús, Silvia, Lagares-Tena, Laura, Buj, Raquel, Hontecillas-Prieto, Lourdes, Sastre, Ana, Azorin, Daniel, Sanjuan, Xavier, López-Alemany, Roser, Moran, Sebastian, Roma, Josep, Gallego, Soledad, Mora, Jaume, García del Muro, Xavier, Giangrande, Paloma H., Peinado, Miquel A., Alonso, Javier, de Alava, Enrique, Monk, Dave, Esteller, Manel, and Tirado, Oscar M.

Published
2017
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17. CD8+ NKs as a potential biomarker of complete response and survival with lenalidomide plus R-GDP in the R2-GDPGOTEL trial in recurrent/refractory diffuse large B cell lymphoma.

Author

Hontecillas-Prieto, Lourdes, García-Domínguez, Daniel J., Palazón-Carrión, Natalia, García-Sancho, Alejandro Martín, Nogales-Fernández, Esteban, Jiménez-Cortegana, Carlos, Sánchez-León, María L., Silva-Romeiro, Silvia, Flores-Campos, Rocío, Carnicero-González, Fernando, Ríos-Herranz, Eduardo, de la Cruz-Vicente, Fátima, Rodríguez-García, Guillermo, Fernández-Álvarez, Rubén, Martínez-Banaclocha, Natividad, Gumà-Padrò, Josep, Gómez-Codina, José, Salar-Silvestre, Antonio, Rodríguez-Abreu, Delvys, and Gálvez-Carvajal, Laura

Subjects
B cell lymphoma, DIFFUSE large B-cell lymphomas, CD8 antigen, LENALIDOMIDE, BIOMARKERS, KILLER cells
Abstract

Background: Diffuse large B cell lymphoma (DLBCL) is the most common non-Hodgkin lymphoma worldwide. DLBCL is an aggressive disease that can be cured with upfront standard chemoimmunotherapy schedules. However, in approximately 35-40% of the patients DLBCL relapses, and therefore, especially in this setting, the search for new prognostic and predictive biomarkers is an urgent need. Natural killer (NK) are effector cells characterized by playing an important role in antitumor immunity due to their cytotoxic capacity and a subset of circulating NK that express CD8 have a higher cytotoxic function. In this substudy of the R2-GDPGOTEL trial, we have evaluated blood CD8+ NK cells as a predictor of treatment response and survival in relapsed/refractory (R/R) DLBCL patients. Methods: 78 patients received the R2-GDP schedule in the phase II trial. Blood samples were analyzed by flow cytometry. Statistical analyses were carried out in order to identify the prognostic potential of CD8+ NKs at baseline in R/R DLBCL patients. Results: Our results showed that the number of circulating CD8+ NKs in R/R DLBCL patients were lower than in healthy donors, and it did not change during and after treatment. Nevertheless, the level of blood CD8+ NKs at baseline was associated with complete responses in patients with R/R DLBCL. In addition, we also demonstrated that CD8+ NKs levels have potential prognostic value in terms of overall survival in R/R DLBCL patients. Conclusion: CD8+ NKs represent a new biomarker with prediction and prognosis potential to be considered in the clinical management of patients with R/R DLBCL. [ABSTRACT FROM AUTHOR]

Published
2024
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19. Defining the Emergence of New Immunotherapy Approaches in Breast Cancer: Role of Myeloid-Derived Suppressor Cells

Author

Universidad de Sevilla. Departamento de Medicina, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Sánchez León, María Luisa, Jiménez Cortegana, Carlos, Silva Romeiro, Silvia, Garnacho Montero, Carmen, Cruz Merino, Luis de la, García-Domínguez, Daniel J., Hontecillas-Prieto, Lourdes, Sánchez Margalet, Víctor, Universidad de Sevilla. Departamento de Medicina, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Sánchez León, María Luisa, Jiménez Cortegana, Carlos, Silva Romeiro, Silvia, Garnacho Montero, Carmen, Cruz Merino, Luis de la, García-Domínguez, Daniel J., Hontecillas-Prieto, Lourdes, and Sánchez Margalet, Víctor

Abstract

Breast cancer (BC) continues to be the most diagnosed tumor in women and a very heterogeneous disease both inter- and intratumoral, mainly given by the variety of molecular profiles with different biological and clinical characteristics. Despite the advancements in early detection and therapeutic strategies, the survival rate is low in patients who develop metastatic disease. Therefore, it is mandatory to explore new approaches to achieve better responses. In this regard, immunotherapy arose as a promising alternative to conventional treatments due to its ability to modulate the immune system, which may play a dual role in this disease since the relationship between the immune system and BC cells depends on several factors: the tumor histology and size, as well as the involvement of lymph nodes, immune cells, and molecules that are part of the tumor microenvironment. Particularly, myeloid-derived suppressor cell (MDSC) expansion is one of the major immunosuppressive mechanisms used by breast tumors since it has been associated with worse clinical stage, metastatic burden, and poor efficacy of immunotherapies. This review focuses on the new immunotherapies in BC in the last five years. Additionally, the role of MDSC as a therapeutic target in breast cancer will be described.

Published
2023

20. Supplementary Data from Stromal SNAI2 Is Required for ERBB2 Breast Cancer Progression

Author

Blanco-Gómez, Adrián, primary, Hontecillas-Prieto, Lourdes, primary, Corchado-Cobos, Roberto, primary, García-Sancha, Natalia, primary, Salvador, Nélida, primary, Castellanos-Martín, Andrés, primary, Sáez-Freire, María del Mar, primary, Mendiburu-Eliçabe, Marina, primary, Alonso-López, Diego, primary, De Las Rivas, Javier, primary, Lorente, Mar, primary, García-Casas, Ana, primary, Del Carmen, Sofía, primary, Abad-Hernández, María del Mar, primary, Cruz-Hernández, Juan Jesús, primary, Rodríguez-Sánchez, César Augusto, primary, Claros-Ampuero, Juncal, primary, García-Cenador, Begoña, primary, García-Criado, Javier, primary, Orimo, Akira, primary, Gridley, Thomas, primary, Pérez-Losada, Jesús, primary, and Castillo-Lluva, Sonia, primary

Published
2023
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21. Supplementary Data from Lenalidomide plus R-GDP (R2-GDP) in Relapsed/Refractory Diffuse Large B-Cell Lymphoma: Final Results of the R2-GDP-GOTEL Trial and Immune Biomarker Subanalysis

Author

Palazón-Carrión, Natalia, primary, Martín García-Sancho, Alejandro, primary, Nogales-Fernández, Esteban, primary, Jiménez-Cortegana, Carlos, primary, Carnicero-González, Fernando, primary, Ríos-Herranz, Eduardo, primary, de la Cruz-Vicente, Fátima, primary, Rodríguez-García, Guillermo, primary, Fernández-Álvarez, Rubén, primary, Martínez-Banaclocha, Natividad, primary, Gumà-Padrò, Josep, primary, Gómez-Codina, José, primary, Salar-Silvestre, Antonio, primary, Rodríguez-Abreu, Delvys, primary, Gálvez-Carvajal, Laura, primary, Labrador, Jorge, primary, Guirado-Risueño, María, primary, García-Domínguez, Daniel J., primary, Hontecillas-Prieto, Lourdes, primary, Espejo-García, Pablo, primary, Fernández-Román, Isabel, primary, Provencio-Pulla, Mariano, primary, Sánchez-Beato, Margarita, primary, Navarro, Marta, primary, Marylene, Lejeune, primary, Álvaro-Naranjo, Tomás, primary, Casanova-Espinosa, Maria, primary, Sánchez-Margalet, Victor, primary, Rueda-Domínguez, Antonio, primary, and de la Cruz-Merino, Luis, primary

Published
2023
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23. Obesity and Risk for Lymphoma: Possible Role of Leptin

Author

Jiménez-Cortegana, Carlos, primary, Hontecillas-Prieto, Lourdes, additional, García-Domínguez, Daniel J., additional, Zapata, Fernando, additional, Palazón-Carrión, Natalia, additional, Sánchez-León, María L., additional, Tami, Malika, additional, Pérez-Pérez, Antonio, additional, Sánchez-Jiménez, Flora, additional, Vilariño-García, Teresa, additional, de la Cruz-Merino, Luis, additional, and Sánchez-Margalet, Víctor, additional

Published
2022
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26. Lenalidomide plus R-GDP (R2-GDP) in Relapsed/Refractory Diffuse Large B-Cell Lymphoma: Final Results of the R2-GDP-GOTEL Trial and Immune Biomarker Subanalysis

Author

Palazón-Carrión, Natalia, primary, Martín García-Sancho, Alejandro, additional, Nogales-Fernández, Esteban, additional, Jiménez-Cortegana, Carlos, additional, Carnicero-González, Fernando, additional, Ríos-Herranz, Eduardo, additional, de la Cruz-Vicente, Fátima, additional, Rodríguez-García, Guillermo, additional, Fernández-Álvarez, Rubén, additional, Martínez-Banaclocha, Natividad, additional, Gumà-Padrò, Josep, additional, Gómez-Codina, José, additional, Salar-Silvestre, Antonio, additional, Rodríguez-Abreu, Delvys, additional, Gálvez-Carvajal, Laura, additional, Labrador, Jorge, additional, Guirado-Risueño, María, additional, García-Domínguez, Daniel J., additional, Hontecillas-Prieto, Lourdes, additional, Espejo-García, Pablo, additional, Fernández-Román, Isabel, additional, Provencio-Pulla, Mariano, additional, Sánchez-Beato, Margarita, additional, Navarro, Marta, additional, Marylene, Lejeune, additional, Álvaro-Naranjo, Tomás, additional, Casanova-Espinosa, Maria, additional, Sánchez-Margalet, Victor, additional, Rueda-Domínguez, Antonio, additional, and de la Cruz-Merino, Luis, additional

Published
2022
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27. Tumor Immune Microenvironment in Lymphoma: Focus on Epigenetics

Author

Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Medicina, García Domínguez, Daniel, Hontecillas Prieto, Lourdes, Palazón Carrión, Natalia, Jiménez Cortegana, Carlos, Sánchez Margalet, Víctor, Cruz Merino, Luis de la, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Medicina, García Domínguez, Daniel, Hontecillas Prieto, Lourdes, Palazón Carrión, Natalia, Jiménez Cortegana, Carlos, Sánchez Margalet, Víctor, and Cruz Merino, Luis de la

Abstract

Lymphoma is a neoplasm arising from B or T lymphocytes or natural killer cells characterized by clonal lymphoproliferation. This tumor comprises a diverse and heterogeneous group of malignancies with distinct clinical, histopathological, and molecular characteristics. Despite advances in lymphoma treatment, clinical outcomes of patients with relapsed or refractory disease remain poor. Thus, a deeper understanding of molecular pathogenesis and tumor progression of lymphoma is required. Epigenetic alterations contribute to cancer initiation, progression, and drug resistance. In fact, over the past decade, dysregulation of epigenetic mechanisms has been identified in lymphomas, and the knowledge of the epigenetic aberrations has led to the emergence of the promising epigenetic therapy field in lymphoma tumors. However, epigenetic aberrations in lymphoma not only have been found in tumor cells, but also in cells from the tumor microenvironment, such as immune cells. Whereas the epigenetic dysregulation in lymphoma cells is being intensively investigated, there are limited studies regarding the epigenetic mechanisms that affect the functions of immune cells from the tumor microenvironment in lymphoma. Therefore, this review tries to provide a general overview of epigenetic alterations that affect both lymphoma cells and infiltrating immune cells within the tumor, as well as the epigenetic cross-talk between them.

Published
2022

28. Selective histone methyltransferase G9a inhibition reduces metastatic development of Ewing sarcoma through the epigenetic regulation of NEU1

Author

Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Ministerio de Economía y Competitividad (MINECO). España, European Commission (EC). Fondo Europeo de Desarrollo Regional (FEDER), Consejería de Salud, Junta de Andalucía, García Domínguez, Daniel, Hajji, Nabil, López Alemany, Roser, Sánchez Molina, Sara, Figuerola Bou, Elisabet, Morón Civanto, Francisco Jesús, Álava Casado, Enrique de, Hontecillas Prieto, Lourdes, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Ministerio de Economía y Competitividad (MINECO). España, European Commission (EC). Fondo Europeo de Desarrollo Regional (FEDER), Consejería de Salud, Junta de Andalucía, García Domínguez, Daniel, Hajji, Nabil, López Alemany, Roser, Sánchez Molina, Sara, Figuerola Bou, Elisabet, Morón Civanto, Francisco Jesús, Álava Casado, Enrique de, and Hontecillas Prieto, Lourdes

Abstract

Ewing sarcoma (EWS) is an aggressive bone and soft tissue tumor with high susceptibility to metastasize. The underlying molecular mechanisms leading to EWS metastases remain poorly understood. Epigenetic changes have been implicated in EWS tumor growth and progression. Linking epigenetics and metastases may provide insight into novel molecular targets in EWS and improve its treatment. Here, we evaluated the effects of a selective G9a histone methyltransferase inhibitor (BIX01294) on EWS metastatic process. Our results showed that overexpression of G9a in tumors from EWS patients correlates with poor prognosis. Moreover, we observe a significantly higher expression of G9a in metastatic EWS tumor as compared to either primary or recurrent tumor. Using functional assays, we demonstrate that pharmacological G9a inhibition using BIX01294 disrupts several metastatic steps in vitro, such as migration, invasion, adhesion, colony formation and vasculogenic mimicry. Moreover, BIX01294 reduces tumor growth and metastases in two spontaneous metastases mouse models. We further identified the sialidase NEU1 as a direct target and effector of G9a in the metastatic process in EWS. NEU1 overexpression impairs migration, invasion and clonogenic capacity of EWS cell lines. Overall, G9a inhibition impairs metastases in vitro and in vivo through the overexpression of NEU1. G9a has strong potential as a prognostic marker and may be a promising therapeutic target for EWS patients.

Published
2022

29. Obesity and Risk for Lymphoma: Possible Role of Leptin

Author

Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Medicina, Plan Andaluz de Investigación, Desarrollo e Innovación. Junta de Andalucía, Jiménez Cortegana, Carlos, Hontecillas Prieto, Lourdes, García-Domínguez, Daniel J., Zapata, Fernando, Palazón Carrión, Natalia, Sánchez León, María Luisa, Tami, Malika, Pérez Pérez, Antonio, Sánchez Jiménez, Flora, Vilariño García, Teresa, Cruz Merino, Luis de la, Sánchez Margalet, Víctor, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Medicina, Plan Andaluz de Investigación, Desarrollo e Innovación. Junta de Andalucía, Jiménez Cortegana, Carlos, Hontecillas Prieto, Lourdes, García-Domínguez, Daniel J., Zapata, Fernando, Palazón Carrión, Natalia, Sánchez León, María Luisa, Tami, Malika, Pérez Pérez, Antonio, Sánchez Jiménez, Flora, Vilariño García, Teresa, Cruz Merino, Luis de la, and Sánchez Margalet, Víctor

Abstract

Obesity, which is considered a pandemic due to its high prevalence, is a risk factor for many types of cancers, including lymphoma, through a variety of mechanisms by promoting an inflammatory state. Specifically, over the last few decades, obesity has been suggested not only to increase the risk of lymphoma but also to be associated with poor clinical outcomes and worse responses to different treatments for those diseases. Within the extensive range of proinflammatory mediators that adipose tissue releases, leptin has been demonstrated to be a key adipokine due to its pleotropic effects in many physiological systems and diseases. In this sense, different studies have analyzed leptin levels and leptin/leptin receptor expressions as a probable bridge between obesity and lymphomas. Since both obesity and lymphomas are prevalent pathophysiological conditions worldwide and their incidences have increased over the last few years, here we review the possible role of leptin as a promising proinflammatory mediator promoting lymphomas.

Published
2022

30. Ewing Sarcoma Meets Epigenetics, Immunology and Nanomedicine: Moving Forward into Novel Therapeutic Strategies

Author

Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Medicina, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Junta de Andalucía. Consejeria de Salud y Familias, FIS-FEDER, Sánchez Molina, Sara, Figuerola Bou, Elisabet, Sánchez Margalet, Víctor, Cruz Merino, Luis de la, Mora, Jaume, Álava Casado, Enrique de, García-Domínguez, Daniel J., Hontecillas Prieto, Lourdes, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Medicina, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Junta de Andalucía. Consejeria de Salud y Familias, FIS-FEDER, Sánchez Molina, Sara, Figuerola Bou, Elisabet, Sánchez Margalet, Víctor, Cruz Merino, Luis de la, Mora, Jaume, Álava Casado, Enrique de, García-Domínguez, Daniel J., and Hontecillas Prieto, Lourdes

Abstract

Ewing Sarcoma (EWS) is an aggressive bone and soft tissue tumor that mainly affects children, adolescents, and young adults. The standard therapy, including chemotherapy, surgery, and radiotherapy, has substantially improved the survival of EWS patients with localized disease. Unfortunately, this multimodal treatment remains elusive in clinics for those patients with recurrent or metastatic disease who have an unfavorable prognosis. Consistently, there is an urgent need to find new strategies for patients that fail to respond to standard therapies. In this regard, in the last decade, treatments targeting epigenetic dependencies in tumor cells and the immune system have emerged into the clinical scenario. Additionally, recent advances in nanomedicine provide novel delivery drug systems, which may address challenges such as side effects and toxicity. Therefore, therapeutic strategies stemming from epigenetics, immunology, and nanomedicine yield promising alternatives for treating these patients. In this review, we highlight the most relevant EWS preclinical and clinical studies in epigenetics, immunotherapy, and nanotherapy conducted in the last five years.

Published
2022

31. Selective histone methyltransferase G9a inhibition reduces metastatic development of Ewing sarcoma through the epigenetic regulation of NEU1

Author

Asociación Española Contra el Cáncer, Ministerio de Economía y Competitividad (España), European Commission, Centro de Investigación Biomédica en Red Cáncer (España), Junta de Andalucía, Fundación Alba Pérez, Agència de Gestió d'Ajuts Universitaris i de Recerca, García-Domínguez, D. J., Hajji, Nabil, López-Alemany, Roser, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, Morón, Francisco J., Rello-Varona, Santiago, Andrés-León, Eduardo, Benito, Adrián, Keun, Hector C., Mora, Jaume, Tirado, Óscar M., Álava, Enrique de, Hontecillas-Prieto, Lourdes, Asociación Española Contra el Cáncer, Ministerio de Economía y Competitividad (España), European Commission, Centro de Investigación Biomédica en Red Cáncer (España), Junta de Andalucía, Fundación Alba Pérez, Agència de Gestió d'Ajuts Universitaris i de Recerca, García-Domínguez, D. J., Hajji, Nabil, López-Alemany, Roser, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, Morón, Francisco J., Rello-Varona, Santiago, Andrés-León, Eduardo, Benito, Adrián, Keun, Hector C., Mora, Jaume, Tirado, Óscar M., Álava, Enrique de, and Hontecillas-Prieto, Lourdes

Abstract

Ewing sarcoma (EWS) is an aggressive bone and soft tissue tumor with high susceptibility to metastasize. The underlying molecular mechanisms leading to EWS metastases remain poorly understood. Epigenetic changes have been implicated in EWS tumor growth and progression. Linking epigenetics and metastases may provide insight into novel molecular targets in EWS and improve its treatment. Here, we evaluated the effects of a selective G9a histone methyltransferase inhibitor (BIX01294) on EWS metastatic process. Our results showed that overexpression of G9a in tumors from EWS patients correlates with poor prognosis. Moreover, we observe a significantly higher expression of G9a in metastatic EWS tumor as compared to either primary or recurrent tumor. Using functional assays, we demonstrate that pharmacological G9a inhibition using BIX01294 disrupts several metastatic steps in vitro, such as migration, invasion, adhesion, colony formation and vasculogenic mimicry. Moreover, BIX01294 reduces tumor growth and metastases in two spontaneous metastases mouse models. We further identified the sialidase NEU1 as a direct target and effector of G9a in the metastatic process in EWS. NEU1 overexpression impairs migration, invasion and clonogenic capacity of EWS cell lines. Overall, G9a inhibition impairs metastases in vitro and in vivo through the overexpression of NEU1. G9a has strong potential as a prognostic marker and may be a promising therapeutic target for EWS patients.

Published
2022

32. Ewing Sarcoma Meets Epigenetics, Immunology and Nanomedicine: Moving Forward into Novel Therapeutic Strategies

Author

Instituto de Salud Carlos III, European Commission, Junta de Andalucía, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, Sánchez-Margalet, Víctor, Cruz Merino, L. de la, Mora, Jaume, Álava, Enrique de, García-Domínguez, D. J., Hontecillas-Prieto, Lourdes, Instituto de Salud Carlos III, European Commission, Junta de Andalucía, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, Sánchez-Margalet, Víctor, Cruz Merino, L. de la, Mora, Jaume, Álava, Enrique de, García-Domínguez, D. J., and Hontecillas-Prieto, Lourdes

Abstract

Ewing Sarcoma (EWS) is an aggressive bone and soft tissue tumor that mainly affects children, adolescents, and young adults. The standard therapy, including chemotherapy, surgery, and radiotherapy, has substantially improved the survival of EWS patients with localized disease. Unfortunately, this multimodal treatment remains elusive in clinics for those patients with recurrent or metastatic disease who have an unfavorable prognosis. Consistently, there is an urgent need to find new strategies for patients that fail to respond to standard therapies. In this regard, in the last decade, treatments targeting epigenetic dependencies in tumor cells and the immune system have emerged into the clinical scenario. Additionally, recent advances in nanomedicine provide novel delivery drug systems, which may address challenges such as side effects and toxicity. Therefore, therapeutic strategies stemming from epigenetics, immunology, and nanomedicine yield promising alternatives for treating these patients. In this review, we highlight the most relevant EWS preclinical and clinical studies in epigenetics, immunotherapy, and nanotherapy conducted in the last five years.

Published
2022

33. Integrin alpha9 emerges as a key therapeutic target to reduce metastasis in rhabdomyosarcoma and neuroblastoma

Author

Institut Català d'Oncologia, Instituto de Salud Carlos III, Generalitat de Catalunya, Fundació La Marató de TV3, Fundació A. Bosch, Rotary Foundation, Abidal Foundation, Del Hospital a la Catedral, Mi Compañero de Viaje, Navarro, Natalia [0000-0002-2160-6656], Roma, Josep [0000-0001-7692-6123], Navarro, Natalia, Molist, Carla, Sansa-Girona, Júlia, Zarzosa, Patricia, Gallo-Oller, Gabriel, Pons, Guillem, Magdaleno, Ainara, Guillén, Gabriela, Hladun, Raquel, Garrido, Marta, Segura, Miguel F., Hontecillas-Prieto, Lourdes, Álava, Enrique de, Ponsati, Berta, Fernández-Carneado, Jimena, Almazán-Moga, Ana, Vallès-Miret, Mariona, Farrera-Sinfreu, Josep, Sánchez de Toledo, Josep, Moreno, Lucas, Gallego, Soledad, Roma, Josep, Institut Català d'Oncologia, Instituto de Salud Carlos III, Generalitat de Catalunya, Fundació La Marató de TV3, Fundació A. Bosch, Rotary Foundation, Abidal Foundation, Del Hospital a la Catedral, Mi Compañero de Viaje, Navarro, Natalia [0000-0002-2160-6656], Roma, Josep [0000-0001-7692-6123], Navarro, Natalia, Molist, Carla, Sansa-Girona, Júlia, Zarzosa, Patricia, Gallo-Oller, Gabriel, Pons, Guillem, Magdaleno, Ainara, Guillén, Gabriela, Hladun, Raquel, Garrido, Marta, Segura, Miguel F., Hontecillas-Prieto, Lourdes, Álava, Enrique de, Ponsati, Berta, Fernández-Carneado, Jimena, Almazán-Moga, Ana, Vallès-Miret, Mariona, Farrera-Sinfreu, Josep, Sánchez de Toledo, Josep, Moreno, Lucas, Gallego, Soledad, and Roma, Josep

Abstract

The majority of current cancer therapies are aimed at reducing tumour growth, but there is lack of viable pharmacological options to reduce the formation of metastasis. This is a paradox, since more than 90% of cancer deaths are attributable to metastatic progression. Integrin alpha9 (ITGA9) has been previously described as playing an essential role in metastasis; however, little is known about the mechanism that links this protein to this process, being one of the less studied integrins. We have now deciphered the importance of ITGA9 in metastasis and provide evidence demonstrating its essentiality for metastatic dissemination in rhabdomyosarcoma and neuroblastoma. However, the most translational advance of this study is to reveal, for the first time, the possibility of reducing metastasis by pharmacological inhibition of ITGA9 with a synthetic peptide simulating a key interaction domain of ADAM proteins, in experimental metastasis models, not only in childhood cancers but also in a breast cancer model.

Published
2022

35. The bitter side of epigenetics: variability and resistance to chemotherapy

Author

Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Hajji, Nabil, García-Domínguez, Daniel J., Hontecillas Prieto, Lourdes, O'Neill, Kevin, Álava Casado, Enrique de, Syed, Nelofer, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Hajji, Nabil, García-Domínguez, Daniel J., Hontecillas Prieto, Lourdes, O'Neill, Kevin, Álava Casado, Enrique de, and Syed, Nelofer

Abstract

One of the major obstacles to the development of effective new cancer treatments and the main factor for the increasing number of clinical trial failures appears to be the paucity of accurate, reproducible and robust drug resistance testing methods. Most research assessing the resistance of cancers to chemotherapy has concentrated on genetic-based molecular mechanisms, while the role of epigenetics in drug resistance has been generally overlooked. This is rather surprising given that an increasing body of evidence pointing to the fact that epigenetic mechanism alterations appear to play a pivotal role in cancer initiation, progression and development of chemoresistance. This resulted in a series of clinical trials involving epi-drug as single treatment or combined with cancer conventional drugs. In this review, we provided the main mechanisms by which the epigenetic regulators control the resistance to cancer drugs.

Published
2021

36. Selective inhibition of HDAC6 regulates expression of the oncogenic driver EWSR1-FLI1 through the EWSR1 promoter in Ewing sarcoma

Author

Universidad de Sevilla. Departamento de Bioquímica y Biología Molecular, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Ministerio de Ciencia e Innovación (MICIN). España, Junta de Andalucía, García Domínguez, Daniel, Hajji, Nabil, Sánchez Molina, Sara, Figuerola Bou, Elisabet, Martínez de Pablos, Rocío, Espinosa Oliva, Ana María, Flores Campos, Rocío, Robles Frías, María José, Álava Casado, Enrique de, Hontecillas Prieto, Lourdes, Universidad de Sevilla. Departamento de Bioquímica y Biología Molecular, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Ministerio de Ciencia e Innovación (MICIN). España, Junta de Andalucía, García Domínguez, Daniel, Hajji, Nabil, Sánchez Molina, Sara, Figuerola Bou, Elisabet, Martínez de Pablos, Rocío, Espinosa Oliva, Ana María, Flores Campos, Rocío, Robles Frías, María José, Álava Casado, Enrique de, and Hontecillas Prieto, Lourdes

Abstract

Ewing sarcoma (EWS) is an aggressive bone and soft tissue tumor of children and young adults in which the principal driver is a fusion gene, EWSR1-FLI1. Although the essential role of EWSR1-FLI1 protein in the regulation of oncogenesis, survival, and tumor progression processes has been described in-depth, little is known about the regulation of chimeric fusion-gene expression. Here, we demonstrate that the active nuclear HDAC6 in EWS modulates the acetylation status of specificity protein 1 (SP1), consequently regulating the SP1/P300 activator complex binding to EWSR1 and EWSR1-FLI1 promoters. Selective inhibition of HDAC6 impairs binding of the activator complex SP1/P300, thereby inducing EWSR1-FLI1 downregulation and significantly reducing its oncogenic functions. In addition, sensitivity of EWS cell lines to HDAC6 inhibition is higher than other tumor or non-tumor cell lines. High expression of HDAC6 in primary EWS tumor samples from patients correlates with a poor prognosis in two independent series accounting 279 patients. Notably, a combination treatment of a selective HDAC6 and doxorubicin (a DNA damage agent used as a standard therapy of EWS patients) dramatically inhibits tumor growth in two EWS murine xenograft models. These results could lead to suitable and promising therapeutic alternatives for patients with EWS.

Published
2021

37. Selective inhibition of HDAC6 regulates expression of the oncogenic driver EWSR1-FLI1 through the EWSR1 promoter in Ewing sarcoma

Author

Asociación Española Contra el Cáncer, Ministerio de Ciencia, Innovación y Universidades (España), Junta de Andalucía, European Commission, García-Domínguez, D. J., Hajji, Nabil, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, de Pablos, Rocío M., Espinosa-Oliva, Ana M., Andrés-León, Eduardo, Terrón-Camero, Laura Carmen, Flores-Campos, Rocío, Pascual-Pasto, Guillem, Robles-Frías, María José, Machado, Isidro, Llombart-Bosch, Antonio, Magagnoli, Giovanna, Scotlandi, Katia, Carcaboso, Ángel M., Mora, Jaume, Álava, Enrique de, Hontecillas-Prieto, Lourdes, Asociación Española Contra el Cáncer, Ministerio de Ciencia, Innovación y Universidades (España), Junta de Andalucía, European Commission, García-Domínguez, D. J., Hajji, Nabil, Sánchez-Molina, Sara, Figuerola-Bou, Elisabet, de Pablos, Rocío M., Espinosa-Oliva, Ana M., Andrés-León, Eduardo, Terrón-Camero, Laura Carmen, Flores-Campos, Rocío, Pascual-Pasto, Guillem, Robles-Frías, María José, Machado, Isidro, Llombart-Bosch, Antonio, Magagnoli, Giovanna, Scotlandi, Katia, Carcaboso, Ángel M., Mora, Jaume, Álava, Enrique de, and Hontecillas-Prieto, Lourdes

Abstract

Ewing sarcoma (EWS) is an aggressive bone and soft tissue tumor of children and young adults in which the principal driver is a fusion gene, EWSR1-FLI1. Although the essential role of EWSR1-FLI1 protein in the regulation of oncogenesis, survival, and tumor progression processes has been described in-depth, little is known about the regulation of chimeric fusion-gene expression. Here, we demonstrate that the active nuclear HDAC6 in EWS modulates the acetylation status of specificity protein 1 (SP1), consequently regulating the SP1/P300 activator complex binding to EWSR1 and EWSR1-FLI1 promoters. Selective inhibition of HDAC6 impairs binding of the activator complex SP1/P300, thereby inducing EWSR1-FLI1 downregulation and significantly reducing its oncogenic functions. In addition, sensitivity of EWS cell lines to HDAC6 inhibition is higher than other tumor or non-tumor cell lines. High expression of HDAC6 in primary EWS tumor samples from patients correlates with a poor prognosis in two independent series accounting 279 patients. Notably, a combination treatment of a selective HDAC6 and doxorubicin (a DNA damage agent used as a standard therapy of EWS patients) dramatically inhibits tumor growth in two EWS murine xenograft models. These results could lead to suitable and promising therapeutic alternatives for patients with EWS.

Published
2021

39. Impact of obesity-associated myeloid-derived suppressor cells on cancer risk and progression (Review).

Author

Jiménez-Cortegana, Carlos, Gutiérrez-García, Cristian, Sánchez-Jiménez, Flora, Vilariño-García, Teresa, Flores-Campos, Rocio, Pérez-Pérez, Antonio, Garnacho, Carmen, Sánchez-León, Maria L., García-Domínguez, Daniel J., Hontecillas-Prieto, Lourdes, Palazón-Carrión, Natalia, De La Cruz-Merino, Luis, and Sánchez-Margalet, Víctor

Published
2024
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40. HDAC6 regulates expression of the oncogenic driver EWSR1-FLI1 through the EWSR1 promoter in Ewing sarcoma

Author

García-Domínguez, Daniel J., primary, Hajji, Nabil, additional, Sánchez-Molina, Sara, additional, Figuerola-Bou, Elisabet, additional, de Pablos, Rocío M., additional, Espinosa-Oliva, Ana M., additional, Andrés-León, Eduardo, additional, Terrón-Camero, Laura Carmen, additional, Flores-Campos, Rocío, additional, Pascual-Pasto, Guillem, additional, Robles, María José, additional, Carcaboso, Ángel M., additional, Mora, Jaume, additional, de Álava, Enrique, additional, and Hontecillas-Prieto, Lourdes, additional

Published
2021
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41. Stromal SNAI2 Is Required for ERBB2 Breast Cancer Progression

Author

Blanco-Gómez, Adrián, primary, Hontecillas-Prieto, Lourdes, additional, Corchado-Cobos, Roberto, additional, García-Sancha, Natalia, additional, Salvador, Nélida, additional, Castellanos-Martín, Andrés, additional, Sáez-Freire, María del Mar, additional, Mendiburu-Eliçabe, Marina, additional, Alonso-López, Diego, additional, De Las Rivas, Javier, additional, Lorente, Mar, additional, García-Casas, Ana, additional, Del Carmen, Sofía, additional, Abad-Hernández, María del Mar, additional, Cruz-Hernández, Juan Jesús, additional, Rodríguez-Sánchez, César Augusto, additional, Claros-Ampuero, Juncal, additional, García-Cenador, Begoña, additional, García-Criado, Javier, additional, Orimo, Akira, additional, Gridley, Thomas, additional, Pérez-Losada, Jesús, additional, and Castillo-Lluva, Sonia, additional

Published
2020
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42. Novel nuclear role of HDAC6 in prognosis and therapeutic target for colorectal cancer

Author

García-Domínguez, Daniel J., primary, Hontecillas-Prieto, Lourdes, additional, Kaliszczak, Maciej, additional, He, Miaomiao, additional, Burguillos, Miguel Angel, additional, Bekay, Rajaa, additional, Abdul-Salam, Vahitha B., additional, Khozoie, Combiz, additional, Shah, Khalid, additional, O’Neill, Kevin, additional, de Álava, Enrique, additional, Silver, Andrew, additional, Syed, Nelofer, additional, Aboagye, Eric O., additional, and Hajji, Nabil, additional

Published
2020
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43. RING1B recruits EWSR1-FLI1 and cooperates in the remodeling of chromatin necessary for Ewing sarcoma tumorigenesis

Author

Sánchez-Molina, Sara, primary, Figuerola-Bou, Elisabet, additional, Blanco, Enrique, additional, Sánchez-Jiménez, María, additional, Táboas, Pablo, additional, Gómez, Soledad, additional, Ballaré, Cecilia, additional, García-Domínguez, Daniel J., additional, Prada, Estela, additional, Hontecillas-Prieto, Lourdes, additional, M. Carcaboso, Ángel, additional, Tirado, Óscar M., additional, Hernández-Muñoz, Inmaculada, additional, de Álava, Enrique, additional, Lavarino, Cinzia, additional, Di Croce, Luciano, additional, and Mora, Jaume, additional

Published
2020
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46. Synergistic Enhancement of Cancer Therapy Using HDAC Inhibitors: Opportunity for Clinical Trials

Author

Hontecillas-Prieto, Lourdes, Flores-Campos, Rocío, Silver, Andrew, Álava, Enrique de, Hajji, Nabil, García-Domínguez, D. J., Instituto de Salud Carlos III, European Commission, Fundación María García Estrada, and Junta de Andalucía

Subjects
Clinical trials, Histone deacetylases, Combination treatment, Preclinical studies, HDAC inhibitors (HDACis), Cancer
Abstract

Chemotherapy is one of the most established and effective treatments for almost all types of cancer. However, the elevated toxicity due to the non-tumor-associated effects, development of secondary malignancies, infertility, radiation-induced fibrosis and resistance to treatment limit the effectiveness and safety of treatment. In addition, these multiple factors significantly impact quality of life. Over the last decades, our increased understanding of cancer epigenetics has led to new therapeutic approaches and the promise of improved patient outcomes. Epigenetic alterations are commonly found in cancer, especially the increased expression and activity of histone deacetylases (HDACs). Dysregulation of HDACs are critical to the development and progression of the majority of tumors. Hence, HDACs inhibitors (HDACis) were developed and now represent a very promising treatment strategy. The use of HDACis as monotherapy has shown very positive pre-clinical results, but clinical trials have had only limited success. However, combinatorial regimens with other cancer drugs have shown synergistic effects both in pre-clinical and clinical studies. At the same time, these combinations have enhanced the efficacy, reduced the toxicity and tumor resistance to therapy. In this review, we will examine examples of HDACis used in combination with other cancer drugs and highlight the synergistic effects observed in recent preclinical and clinical studies. This work was supported by Instituto de Salud Carlos III_FEDER (PI17/00464 and CB16/12/00361), by the Consejería de Salud, Junta de Andalucía (PI-0013-2018), and by Fundación María García Estrada.

Published
2020

47. Stromal SNAI2 is required for ERBB2 breast cancer progression

Author

Blanco Gómez, Adrián, Hontecillas Prieto, Lourdes, Corchado Cobos, Roberto, García Sancha, Natalia, Salvador Tormo, Nélida, Castellanos Martín, Andrés, Sáez Freire, María del Mar, Mendiburu-Eliçabe Garganta, Marina, Alonso López, Diego, De Las Rivas Sanz, Javier, Lorente Pérez, María Del Mar, García Casas, Ana, Del Carmen Martínez, Sofía, Abad Hernández, María del Mar, Cruz Hernández, Juan Jesús, Rodríguez Sánchez, César Augusto, Claros Ampuero, Juncal, García Cenador, Begoña, García Criado, Javier, Orimo, Akira, Gridley, Thomas, Pérez Losada, Jesús, Castillo Lluva, Sonia, Blanco Gómez, Adrián, Hontecillas Prieto, Lourdes, Corchado Cobos, Roberto, García Sancha, Natalia, Salvador Tormo, Nélida, Castellanos Martín, Andrés, Sáez Freire, María del Mar, Mendiburu-Eliçabe Garganta, Marina, Alonso López, Diego, De Las Rivas Sanz, Javier, Lorente Pérez, María Del Mar, García Casas, Ana, Del Carmen Martínez, Sofía, Abad Hernández, María del Mar, Cruz Hernández, Juan Jesús, Rodríguez Sánchez, César Augusto, Claros Ampuero, Juncal, García Cenador, Begoña, García Criado, Javier, Orimo, Akira, Gridley, Thomas, Pérez Losada, Jesús, and Castillo Lluva, Sonia

Abstract

SNAI2 overexpression appears to be associated with poor prognosis in breast cancer, yet it remains unclear in which breast cancer subtypes this occurs. Here we show that excess SNAI2 is associated with a poor prognosis of luminal B HER2+/ERBB2+ breast cancers in which SNAI2 expression in the stroma but not the epithelium correlates with tumor proliferation. To determine how stromal SNAI2 might influence HER2+ tumor behavior, Snai2-deficient mice were crossed with a mouse line carrying the ErbB2/Neu protooncogene to generate HER2+/ERBB2+ breast cancer. Tumors generated in this model expressed SNAI2 in the stroma but not the epithelium, allowing for the role of stromal SNAI2 to be studied without interference from the epithelial compartment. The absence of SNAI2 in the stroma of HER2+/ERBB2+ tumors is associated with: (i) lower levels of cyclin D1 (CCND1) and reduced tumor epithelium proliferation; (ii) higher levels of AKT and a lower incidence of metastasis; (iii) lower levels of angiopoietin-2 (ANGPT2), and more necrosis. Together, these results indicate that the loss of SNAI2 in cancer-associated fibroblasts limits the production of some cytokines, which influences AKT/ERK tumor signaling and subsequent proliferative and metastatic capacity of ERBB2+ breast cancer cells. Accordingly, SNAI2 expression in the stroma enhanced the tumorigenicity of luminal B HER2+/ERBB2+ breast cancers. This work emphasizes the importance of stromal SNAI2 in breast cancer progression and patients' prognosis., Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, National Institutes of Health, Sandra Ibarra Foundation for Solidarity against Cancer, “We can be heroes” Foundation, Federación Española de Enfermedades Raras, Sección Deptal. de Bioquímica y Biología Molecular (Biológicas), Depto. de Bioquímica y Biología Molecular, Fac. de Ciencias Biológicas, Fac. de Ciencias Químicas, TRUE, pub

Published
2020

48. An inducible ectopic expression system of EWSR1-FLI1 as a tool for understanding Ewing sarcoma oncogénesis

Author

Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Asociacion Espanola Contra el Cancer (AECC), CIBERONC, Consejeria de Salud, Junta de Andalucia, European Commission (FP7HEALTH-2011-two-stage), Ministry of Economy and Competitiveness of Spain-FEDER (CIBERONC), García-Domínguez, Daniel J., Hontecillas-Prieto, Lourdes, Andrés León, Eduardo, Sánchez-Molina, Sara, Rodríguez-Núñez, Pablo, Morón, Francisco J., Hajji, Nabil, Mackintosh, Carlos, Álava Casado, Enrique de, Universidad de Sevilla. Departamento de Bioquímica Médica y Biología Molecular e Inmunología, Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Asociacion Espanola Contra el Cancer (AECC), CIBERONC, Consejeria de Salud, Junta de Andalucia, European Commission (FP7HEALTH-2011-two-stage), Ministry of Economy and Competitiveness of Spain-FEDER (CIBERONC), García-Domínguez, Daniel J., Hontecillas-Prieto, Lourdes, Andrés León, Eduardo, Sánchez-Molina, Sara, Rodríguez-Núñez, Pablo, Morón, Francisco J., Hajji, Nabil, Mackintosh, Carlos, and Álava Casado, Enrique de

Abstract

The presence of the chimeric EWSR1-FLI1 oncoprotein is the main and initiating event defining Ewing sarcoma (ES). The dysregulation of epigenomic and proteomic homeostasis induced by the oncoprotein contributes to a wide variety of events involved in oncogenesis and tumor progression. Attempts at studying the effects of EWSR1-FLI1 in non-tumor cells to understand the mechanisms underlying sarcomagenesis have been unsuccessful to date, as ectopic expression of EWSR1-FLI1 blocks cell cycle progression and induces apoptosis in the tested cell lines. Therefore, it is essential to find a permissive cell type for EWSR1-FLI1 expression that allows its endogenous molecular functions to be studied. Here we have demonstrated that HeLa cell lines are permissive to EWSR1-FLI1 ectopic expression, and that our model substantially recapitulates the endogenous activity of the EWSR1-FLI1 fusion protein. This model could contribute to better understanding ES sarcomagenesis by helping to understand the molecular mechanisms induced by the EWSR1-FLI1 oncoprotein.

Published
2020

49. Synergistic Enhancement of Cancer Therapy Using HDAC Inhibitors: Opportunity for Clinical Trials

Author

Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Universidad de Sevilla. CTS1035: Patología Molecular del Cáncer Sólido, Hontecillas Prieto, Lourdes, Flores Campos, Rocío, Silver, Andrew, Álava Casado, Enrique de, Hajji, Nabil, García-Domínguez, Daniel J., Universidad de Sevilla. Departamento de Citología e Histología Normal y Patológica, Universidad de Sevilla. CTS1035: Patología Molecular del Cáncer Sólido, Hontecillas Prieto, Lourdes, Flores Campos, Rocío, Silver, Andrew, Álava Casado, Enrique de, Hajji, Nabil, and García-Domínguez, Daniel J.

Abstract

Chemotherapy is one of the most established and effective treatments for almost all types of cancer. However, the elevated toxicity due to the non-tumor-associated effects, development of secondary malignancies, infertility, radiation-induced fibrosis and resistance to treatment limit the effectiveness and safety of treatment. In addition, these multiple factors significantly impact quality of life. Over the last decades, our increased understanding of cancer epigenetics has led to new therapeutic approaches and the promise of improved patient outcomes. Epigenetic alterations are commonly found in cancer, especially the increased expression and activity of histone deacetylases (HDACs). Dysregulation of HDACs are critical to the development and progression of the majority of tumors. Hence, HDACs inhibitors (HDACis) were developed and now represent a very promising treatment strategy. The use of HDACis as monotherapy has shown very positive pre-clinical results, but clinical trials have had only limited success. However, combinatorial regimens with other cancer drugs have shown synergistic effects both in pre-clinical and clinical studies. At the same time, these combinations have enhanced the efficacy, reduced the toxicity and tumor resistance to therapy. In this review, we will examine examples of HDACis used in combination with other cancer drugs and highlight the synergistic effects observed in recent preclinical and clinical studies.

Published
2020

50. Treatment-driven selection of chemoresistant Ewing sarcoma tumors with limited drug distribution

Author

Fundación Científica Asociación Española Contra el Cáncer, European Commission, Instituto de Salud Carlos III, Centro de Investigación Biomédica en Red Cáncer (España), Asociación Pablo Ugarte, Fundación María García Estrada, Ministerio de Economía y Competitividad (España), Fundación BBVA, Castillo-Écija, Helena, Monterrubio, Carles, Pascual-Pasto, Guillem, Gómez, Soledad, García-Domínguez, D. J., Hontecillas-Prieto, Lourdes, Resa-Pares, Claudia, Burgueño, Víctor, Paco, Sonia, Olaciregui, Nagore G., Vila-Ubach, Mónica, Restrepo-Perdomo, Camilo, Cuadrado-Vilanova, María, Balaguer-Lluna, Leire, Pérez-Jaume, Sara, Castañeda, Alicia, Santamaría, Vicente, Roldán, Mónica, Suñol, Mariona, Álava, Enrique de, Mora, Jaume, Lavarino, Cinzia, Carcaboso, Ángel M., Fundación Científica Asociación Española Contra el Cáncer, European Commission, Instituto de Salud Carlos III, Centro de Investigación Biomédica en Red Cáncer (España), Asociación Pablo Ugarte, Fundación María García Estrada, Ministerio de Economía y Competitividad (España), Fundación BBVA, Castillo-Écija, Helena, Monterrubio, Carles, Pascual-Pasto, Guillem, Gómez, Soledad, García-Domínguez, D. J., Hontecillas-Prieto, Lourdes, Resa-Pares, Claudia, Burgueño, Víctor, Paco, Sonia, Olaciregui, Nagore G., Vila-Ubach, Mónica, Restrepo-Perdomo, Camilo, Cuadrado-Vilanova, María, Balaguer-Lluna, Leire, Pérez-Jaume, Sara, Castañeda, Alicia, Santamaría, Vicente, Roldán, Mónica, Suñol, Mariona, Álava, Enrique de, Mora, Jaume, Lavarino, Cinzia, and Carcaboso, Ángel M.

Abstract

Ewing sarcoma is a bone and soft tissue tumor predominantly affecting adolescents and young adults. To characterize changes in anticancer drug activity and intratumor drug distribution during the evolution of Ewing sarcomas, we used immunodeficient mice to establish pairs of patient-derived xenografts (PDX) at early (initial diagnosis) and late (relapse or refractory progression) stages of the disease from three patients. Analysis of copy number alterations (CNA) in early passage PDX tissues showed that two tumor pairs established from patients which responded initially to therapy and relapsed more than one year later displayed similar CNAs at early and late stages. For these two patients, PDX established from late tumors were more resistant to chemotherapy (irinotecan) than early counterparts. In contrast, the tumor pair established at refractory progression showed highly dissimilar CNA profiles, and the pattern of response to chemotherapy was discordant with those of relapsed cases. In mice receiving irinotecan infusions, the level of SN-38 (active metabolite of irinotecan) in the intracellular tumor compartment was reduced in tumors at later stages compared to earlier tumors for those pairs bearing similar CNAs, suggesting that distribution of anticancer drug shifted toward the extracellular compartment during clonal tumor evolution. Overexpression of the drug transporter P-glycoprotein in late tumor was likely responsible for this shift in drug distribution in one of the cases.

Published
2020

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