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2. Predicting Survival after Allogeneic Hematopoietic Cell Transplantation in Myelofibrosis: Performance of the Myelofibrosis Transplant Scoring System (MTSS) and Development of a New Prognostic Model

Author

Hernández-Boluda, Juan-Carlos, Pereira, Arturo, Alvarez-Larran, Alberto, Martín, Ana-Africa, Benzaquen, Ana, Aguirre, Lourdes, Mora, Elvira, González, Pedro, Mora, Jorge, Dorado, Nieves, Sampol, Antonia, García-Gutiérrez, Valentín, López-Godino, Oriana, Fox, María-Laura, Reguera, Juan Luis, Pérez-Encinas, Manuel, Pascual, María-Jesús, Xicoy, Blanca, Parody, Rocío, González-Pinedo, Leslie, Español, Ignacio, Avendaño, Alejandro, Correa, Juan-Gonzalo, Vallejo, Carlos, Jurado, Manuel, García-Cadenas, Irene, Osorio, Santiago, Durán, María-Antonia, Sánchez-Guijo, Fermín, Cervantes, Francisco, and Piñana, José-Luis

Published
2020
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3. Next-generation sequencing and FISH studies reveal the appearance of gene mutations and chromosomal abnormalities in hematopoietic progenitors in chronic lymphocytic leukemia

Author

Quijada-Álamo, Miguel, Hernández Sánchez, María, Robledo, Cristina, Hernández-Sánchez, Jesús-María, Benito, Rocío, Montaño, Adrián, Rodríguez-Vicente, Ana E, Quwaider, Dalia, Martín, Ana-África, García-Álvarez, María, Vidal-Manceñido, María Jesús, Ferrer-Garrido, Gonzalo, Delgado-Beltrán, María-Pilar, Galende, Josefina, Rodríguez, Juan-Nicolás, Martín-Núñez, Guillermo, Alonso, José-María, García de Coca, Alfonso, Queizán, José A., Sierra, Magdalena, Aguilar, Carlos, Kohlmann, Alexander, Hernández,José-Ángel, González, Marcos, Hernández-Rivas, Jesús-María, Quijada-Álamo, Miguel, Hernández Sánchez, María, Robledo, Cristina, Hernández-Sánchez, Jesús-María, Benito, Rocío, Montaño, Adrián, Rodríguez-Vicente, Ana E, Quwaider, Dalia, Martín, Ana-África, García-Álvarez, María, Vidal-Manceñido, María Jesús, Ferrer-Garrido, Gonzalo, Delgado-Beltrán, María-Pilar, Galende, Josefina, Rodríguez, Juan-Nicolás, Martín-Núñez, Guillermo, Alonso, José-María, García de Coca, Alfonso, Queizán, José A., Sierra, Magdalena, Aguilar, Carlos, Kohlmann, Alexander, Hernández,José-Ángel, González, Marcos, and Hernández-Rivas, Jesús-María

Abstract

Background Chronic lymphocytic leukemia (CLL) is a highly genetically heterogeneous disease. Although CLL has been traditionally considered as a mature B cell leukemia, few independent studies have shown that the genetic alterations may appear in CD34+ hematopoietic progenitors. However, the presence of both chromosomal aberrations and gene mutations in CD34+ cells from the same patients has not been explored. Methods Amplicon-based deep next-generation sequencing (NGS) studies were carried out in magnetically activated-cell-sorting separated CD19+ mature B lymphocytes and CD34+ hematopoietic progenitors (n = 56) to study the mutational status of TP53, NOTCH1, SF3B1, FBXW7, MYD88, and XPO1 genes. In addition, ultra-deep NGS was performed in a subset of seven patients to determine the presence of mutations in flow-sorted CD34+CD19− early hematopoietic progenitors. Fluorescence in situ hybridization (FISH) studies were performed in the CD34+ cells from nine patients of the cohort to examine the presence of cytogenetic abnormalities. Results NGS studies revealed a total of 28 mutations in 24 CLL patients. Interestingly, 15 of them also showed the same mutations in their corresponding whole population of CD34+ progenitors. The majority of NOTCH1 (7/9) and XPO1 (4/4) mutations presented a similar mutational burden in both cell fractions; by contrast, mutations of TP53 (2/2), FBXW7 (2/2), and SF3B1 (3/4) showed lower mutational allele frequencies, or even none, in the CD34+ cells compared with the CD19+ population. Ultra-deep NGS confirmed the presence of FBXW7, MYD88, NOTCH1, and XPO1 mutations in the subpopulation of CD34+CD19− early hematopoietic progenitors (6/7). Furthermore, FISH studies showed the presence of 11q and 13q deletions (2/2 and 3/5, respectively) in CD34+ progenitors but the absence of IGH cytogenetic alterations (0/2) in the CD34+ cells. Combining all the results from NGS and FISH, a model of the appearance and expansion of genetic alterations in CLL w, Spanish Fondo de Investigaciones Sanitarias, Instituto de Salud Carlos III, European Regional Development Fund(ERDF) “Una manera de hacer Europa", Consejería de Educación, Junta de Castilla y León, Gerencia Regional de Salud de Castilla y León, Fundación Española de Hematología y Hemoterapia, Red Temática de Investigación Cooperativa en Cáncer, Spanish Ministry of Economy and Competitiveness, Fundación “Memoria Don Samuel Solórzano Barruso” 2016, European Union Seventh Framework Programme, Fondo Social Europeo, Depto. de Bioquímica y Biología Molecular, Fac. de Farmacia, TRUE, pub

Published
2024

5. CT-169 Cytokine Release Syndrome After Peripheral Blood Haploidentical Stem Cell Transplantation With Post-Transplant Cyclophosphamide: Time of Onset Matters

Author

Hernández-Sánchez, Alberto, Cabero, Almudena, Fonseca, Marta, Puertas, Borja, Gómez, Sandra, Alonso, David, Alejo, Elena, Puerta, Carlos, García, Pablo, Pablos, Alicia, Peña, Felipe, Cabrero, Mónica, Avendaño, Alejandro, Baile, Mónica, Martín, Ana África, Pérez, Estefanía, López, Miriam, Marcos, Sara, Prieto, Laura, Vázquez, Lourdes, Sánchez-Guijo, Fermín, Caballero, Ma Dolores, and López-Corral, Lucía

Published
2022
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6. CT-195 Predictive Value of ST2, REG3a, and MAGIC Algorithm in Haploidentical Transplantation With Post-Transplant Cyclophosphamide Outcomes

Author

Santos, Marta Fonseca, Alvarez, Maria Garcia, Sanchez, Luis Antonio Corchete, Sanchez, Alberto Hernandez, Martinez, Borja Puertas, Salinero, Manuela, Rodriguez, Angela, Martin, Ana Africa, Pita, Alejandro Avendaño, Gonzalez, Monica Baile, Cabero, Almudena, Lopez, Estefania Perez, Calvo, Monica Cabrero, Sanchez-Guijo, Fermin, Lopez, Lourdes Vazquez, Garcia-Sanz, Ramon, Barrigon, Maria Dolores Caballero, Alcoceba, Miguel, Lopez-Corral, Lucia, and de Hematología, Servicio

Published
2022
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8. CT-513 Pure Red Cell Aplasia in Major ABO-Incompatible Allogenic Stem Cell Transplantation: Retrospective Analysis From a Single-Center Experience

Author

Alonso, David, primary, Cabrero, Mónica, additional, Fonseca, Marta, additional, Alejo, Elena, additional, Navarro, José María, additional, Gómez, Sandra Patricia, additional, Puerta, Carlos, additional, Zapata, Evelyn, additional, García, Pablo, additional, Fuentes, Cristina Teresa, additional, Fernández, Adolfo, additional, Clavo, Diego, additional, Santos, Carmen, additional, Malaver, Rafael José, additional, Martín, Ana África, additional, Lopez, Miriam, additional, Martín-Mateos, Maria Luisa, additional, Pérez-López, Estefanía, additional, Puertas, Borja, additional, Hernadez, Alberto, additional, Baile, Mónica, additional, Cabero, Almudena, additional, Avendaño, Alejandro, additional, de Ramon, Cristina, additional, García-Bacelar, Ana, additional, Vázquez, Lourdes, additional, Sánchez-Guijo, Fermin, additional, López-Villar, Olga, additional, and López-Corral, Lucía, additional

Published
2023
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9. POSTER: CT-513 Pure Red Cell Aplasia in Major ABO-Incompatible Allogenic Stem Cell Transplantation: Retrospective Analysis From a Single-Center Experience

Author

Alonso, David, primary, Cabrero, Mónica, additional, Fonseca, Marta, additional, Alejo, Elena, additional, Navarro, José María, additional, Gómez, Sandra Patricia, additional, Puerta, Carlos, additional, Zapata, Evelyn, additional, García, Pablo, additional, Fuentes, Cristina Teresa, additional, Fernández, Adolfo, additional, Clavo, Diego, additional, Santos, Carmen, additional, Malaver, Rafael José, additional, Martín, Ana África, additional, Lopez, Miriam, additional, Martín-Mateos, Maria Luisa, additional, Pérez-López, Estefanía, additional, Puertas, Borja, additional, Hernadez, Alberto, additional, Baile, Mónica, additional, Cabero, Almudena, additional, Avendaño, Alejandro, additional, de Ramon, Cristina, additional, García-Bacelar, Ana, additional, Vázquez, Lourdes, additional, Sánchez-Guijo, Fermin, additional, López-Villar, Olga, additional, and López-Corral, Lucía, additional

Published
2023
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10. CLL cells cumulate genetic aberrations prior to the first therapy even in outwardly inactive disease phase

Author

Hernández-Sánchez, María, Kotaskova, Jana, Rodríguez, Ana E, Radova, Lenka, Tamborero, David, Abáigar, María, Plevova, Karla, Benito, Rocío, Tom, Nikola, Quijada-Álamo, Miguel, Bikos, Vasileos, Martín, Ana África, Pal, Karol, García de Coca, Alfonso, Doubek, Michael, López-Bigas, Nuria, Hernández-Rivas, Jesús-María, and Pospisilova, Sarka

Published
2019
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11. MiRNA expression profile of chronic lymphocytic leukemia patients with 13q deletion

Author

Hernández-Sánchez, María, Rodríguez-Vicente, Ana E., Hernández, José-Ángel, Lumbreras, Eva, Sarasquete, María-Eugenia, Martín, Ana-África, Benito, Rocío, Vicente-Gutiérrez, Carlos, Robledo, Cristina, Heras, Natalia de las, Rodríguez, Juan-Nicolás, Alcoceba, Miguel, Coca, Alfonso García de, Aguilar, Carlos, González, Marcos, and Hernández-Rivas, Jesús-María

Published
2016
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12. Poster: CT-169 Cytokine Release Syndrome After Peripheral Blood Haploidentical Stem Cell Transplantation With Post-Transplant Cyclophosphamide: Time of Onset Matters

Author

Hernández-Sánchez, Alberto, primary, Cabero, Almudena, additional, Fonseca, Marta, additional, Puertas, Borja, additional, Gómez, Sandra, additional, Alonso, David, additional, Alejo, Elena, additional, Puerta, Carlos, additional, García, Pablo, additional, Pablos, Alicia, additional, Peña, Felipe, additional, Cabrero, Mónica, additional, Avendaño, Alejandro, additional, Baile, Mónica, additional, Martín, Ana África, additional, Pérez, Estefanía, additional, López, Miriam, additional, Marcos, Sara, additional, Prieto, Laura, additional, Vázquez, Lourdes, additional, Sánchez-Guijo, Fermín, additional, Caballero, Ma Dolores, additional, and López-Corral, Lucía, additional

Published
2022
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14. Genome-wide transcriptomics leads to the identification of deregulated genes after deferasirox therapy in low-risk MDS patients

Author

Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Memoria de D. Samuel Solorzano Barruso, Fundacion de la Sociedad Española de Hematología y Hemoterapia, European Commission, Hernandez-Sánchez, Jesus M., Lumbreras, Eva, Díez-Campelo, María, González, Teresa, Alonso-López, D., Abáigar, María, Rey, Mónica del, Martín, Ana-África, Paz, Raquel de, Erquiaga, Sara, Arrizabalaga, Beatriz, Hernández, Jesús M., Rodríguez-Vicente, Ana Eugenia, Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Memoria de D. Samuel Solorzano Barruso, Fundacion de la Sociedad Española de Hematología y Hemoterapia, European Commission, Hernandez-Sánchez, Jesus M., Lumbreras, Eva, Díez-Campelo, María, González, Teresa, Alonso-López, D., Abáigar, María, Rey, Mónica del, Martín, Ana-África, Paz, Raquel de, Erquiaga, Sara, Arrizabalaga, Beatriz, Hernández, Jesús M., and Rodríguez-Vicente, Ana Eugenia

Abstract

The iron chelator deferasirox is widely used in patients with iron overload. Patients with low-grade myelodysplastic syndromes (MDS) get transfusion dependency and need to be treated with deferasirox to avoid iron overload. Moreover, in some patients an increase in both erythroid and platelets have been observed after deferasirox therapy. However, the mechanisms involved in these clinical findings are poorly understood. The aim of this work was to analyze, in patients treated with deferasirox, the changes in the gene-expression profile after receiving the treatment. A total of 15 patients with the diagnosis of low-grade MDS were studied. Microarrays were carried out in RNA from peripheral blood before and after 14 weeks of deferasirox therapy. Changes in 1457 genes and 54 miRNAs were observed: deferasirox induced the downregulation of genes related to the Nf kB pathway leading of an overall inactivation of this pathway. In addition, the iron chelator also downregulated gamma interferon. Altogether these changes could be related to the improvement of erythroid response observed in these patients after therapy. Moreover, the inhibition of NFE2L2/NRF2, which was predicted in silico, could be playing a critical role in the reduction of reactive oxygen species (ROS). Of note, miR-125b, overexpressed after deferasirox treatment, could be involved in the reduced inflammation and increased hematopoiesis observed in the patients after treatment. In summary this study shows, for the first time, the mechanisms that could be governing deferasirox impact in vivo.

Published
2020

15. Measures to maintain a SARS-CoV-2 negative inpatient hematological unit in the midst of the COVID-19 pandemic

Author

Cabero-Martínez, Almudena, Sánchez-Guijo, Fermín M., López-Corral, L., Pérez-López, Estefanía, Avendaño, Alejandro, Baile, Mónica, Cabrero, Mónica, Martín, Ana-África, Rodríguez, Ángela, Pérez, Balbina, Peña-Muñoz, Felipe, Román, Luz-Gema, Palomino, Danylo, López-Vázquez, Lourdes, Vidriales, Maria Belén, González, Marcos, Mateos, Maria Victoria, Caballero, Maria Dolores, Cabero-Martínez, Almudena, Sánchez-Guijo, Fermín M., López-Corral, L., Pérez-López, Estefanía, Avendaño, Alejandro, Baile, Mónica, Cabrero, Mónica, Martín, Ana-África, Rodríguez, Ángela, Pérez, Balbina, Peña-Muñoz, Felipe, Román, Luz-Gema, Palomino, Danylo, López-Vázquez, Lourdes, Vidriales, Maria Belén, González, Marcos, Mateos, Maria Victoria, and Caballero, Maria Dolores

Abstract

The University Hospital of Salamanca, in Spain, had its first COVID-19 case on March 1st and as of May 11th, we had 1,100 positive cases. Based on the vulnerability of patients with blood cancers, on March 9th, the Hematology Department developed a protocol, amended as the new information was available, to maintain the Hematology Unit as a “free COVID-19 island.” The protocol included symptom-based surveys and screening tests to patients, caregivers, and healthcare personnel to identify early potential positive cases and prevent its spread. Between March 9 and April 28, 32 asymptomatic patients and caregivers were tested and 68 rT-PCR diagnostic assays have been performed with two positive results. A 106 healthcare workers have been tested (208 rT-PCR) and seven of them were positive. In summary, the implementation of preemptive measures after the first case appeared allowed us to be able to provide treatment to our patients.

Published
2020

16. CLL cells cumulate genetic aberrations prior to the first therapy even in outwardly inactive disease phase

Author

European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Memoria de D. Samuel Solorzano Barruso, Red Temática de Investigación Cooperativa en Cáncer (España), Centro de Investigación Biomédica en Red Cáncer (España), Universidad de Salamanca, Sociedad Española de Hematología y Hemoterapia, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), Ministry of Education, Youth and Sports (Czech Republic), Hernández-Sánchez, María, Kotaskova, Jana, Rodríguez-Vicente, Ana Eugenia, Radova, Lenka, Tamborero, David, Abáigar, María, Plevova, Karla, Benito, Rocío, Tom, Nikola, Quijada-Álamo, Miguel, Bikos, Vasileos, Martín, Ana-África, Pal, Karol, García de Coca, Alfonso, Doubek, Michael, López-Bigas, Nuria, Hernández, Jesús M., Pospisilova, Sarka, European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Memoria de D. Samuel Solorzano Barruso, Red Temática de Investigación Cooperativa en Cáncer (España), Centro de Investigación Biomédica en Red Cáncer (España), Universidad de Salamanca, Sociedad Española de Hematología y Hemoterapia, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), Ministry of Education, Youth and Sports (Czech Republic), Hernández-Sánchez, María, Kotaskova, Jana, Rodríguez-Vicente, Ana Eugenia, Radova, Lenka, Tamborero, David, Abáigar, María, Plevova, Karla, Benito, Rocío, Tom, Nikola, Quijada-Álamo, Miguel, Bikos, Vasileos, Martín, Ana-África, Pal, Karol, García de Coca, Alfonso, Doubek, Michael, López-Bigas, Nuria, Hernández, Jesús M., and Pospisilova, Sarka

Abstract

Over the past few years, several large-scale studies using next-generation sequencing (NGS) of whole-genomes (WGS) and whole-exomes (WES) have defined the mutational landscape of chronic lymphocytic leukemia (CLL) [1,2,3,4]. NGS studies have also revealed the clonal heterogeneity in CLL and showed that clonal evolution contributes to the variability in clinical course among CLL patients [3]. Clonal evolution is considered a key condition in CLL progression and relapse after treatment. Most CLL cases are diagnosed during the inactive disease phase, genetic aberrations’ underlying progress in CLL activity leading to the need for therapy are poorly understood and should be explored. A large number of frequently mutated genes have been identified and several putative driver mutations likely to confer selective growth advantage to CLL tumor cells have been proposed [1,2,3]. In addition, clonal shifts between paired treatment-naïve and relapsed CLL samples have been reported due to pre-existing subclone expansion under therapeutic pressure, demonstrating that clonal evolution likely underlies CLL relapse [3, 5]. Nevertheless, there are still a limited amount of longitudinal WES studies analyzing consecutive CLL samples before treatment intervegntion [6]. The acquisition of driver mutations accompanied by selectively neutral passenger changes during disease prior to therapy influence is therefore poorly documented. Here, WES was performed on consecutive treatment-naïve samples of CLL patients from three groups with different disease course: Active disease (AD) group: patients with an active disease before the second analyzed time-point (TP2); Stable disease (SD) group: cases with a period of stable phase after diagnosis followed by progression within 3 years after; and Indolent disease (ID) group: those with a long-term stable indolent disease. Moreover, we applied a novel integrative bioinformatics tool called “Cancer Genome Interpreter” to identify driver mutations [7].

Published
2019

17. CLL cells cumulate genetic aberrations prior to the first therapy even in outwardly inactive disease phase

Author

Hernández-Sánchez, María, primary, Kotaskova, Jana, additional, Rodríguez, Ana E, additional, Radova, Lenka, additional, Tamborero, David, additional, Abáigar, María, additional, Plevova, Karla, additional, Benito, Rocío, additional, Tom, Nikola, additional, Quijada-Álamo, Miguel, additional, Bikos, Vasileos, additional, Martín, Ana África, additional, Pal, Karol, additional, García de Coca, Alfonso, additional, Doubek, Michael, additional, López-Bigas, Nuria, additional, Hernández-Rivas, Jesús-María, additional, and Pospisilova, Sarka, additional

Published
2018
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18. Next-generation sequencing and FISH studies reveal the appearance of gene mutations and chromosomal abnormalities in hematopoietic progenitors in chronic lymphocytic leukemia

Author

Quijada-Alamo, Miguel, Hernández Rivas, Jesús María, Robledo, Cristina, Benito Sánchez, Rocío, Montaño, Adrián, Rodríguez Vicente, Ana, Quwaider, Dalia, Martín, Ana África, García-Álvarez, María, Vidal-Manceñido, María Jesús, Ferrer-Garrido, Gonzalo, Delgado-Beltrán, María-Pilar, Galende, Josefina, Rodríguez, Juan-Nicolás, Martín-Núñez, Guillermo, Alonso, José-María, García de Coca, Alfonso, Queizán, José A., Sierra, Magdalena, Aguilar, Carlos, Kohlmann, Alexander, Hernández, José Ángel, and González, Marcos

Subjects
Hematopoietic progenitors, Next-generation sequencing, Chronic lymphocytic leukemia, Chromosomal abnormality, health care economics and organizations
Abstract

European Commision (EC). Funding FP7/SP1/HEALTH. Project Code: 306242

Published
2017

19. CT-177: Predictive Value of Early Measurement of ST2 and REG3α in the Outcome of Haploidentical Stem-Cell Transplantation with Post-Transplant Cyclophosphamide

Author

Fonseca-Santos, Marta, Garcia-Alvarez, Maria, Corchete-Sanchez, Luis Antonio, Rey-Bua, Beatriz, Azibeiro-Melchor, Raul, Roman-Molano, Luz Gema, Palomino-Mendoza, Danylo, Peña-Muñoz, Felipe, Gomez-Ubeda, Sandra Patricia, Hernandez-Sanchez, Alberto, Puertas-Martinez, Borja, Salinero, Manuela, Garcia-Blazquez, Marta, Martin, Ana Africa, Baile, Monica, Perez, Estefania, Cabrero, Monica, Sanchez-Guijo, Fermin, Vazquez, Lourdes, Caballero, Maria Dolores, Alcoceba, Miguel, and Lopez-Corral, Lucia

Published
2020
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20. Next-generation sequencing and FISH studies reveal the appearance of gene mutations and chromosomal abnormalities in hematopoietic progenitors in chronic lymphocytic leukemia

Author

Quijada-Álamo, Miguel, primary, Hernández-Sánchez, María, additional, Robledo, Cristina, additional, Hernández-Sánchez, Jesús-María, additional, Benito, Rocío, additional, Montaño, Adrián, additional, Rodríguez-Vicente, Ana E., additional, Quwaider, Dalia, additional, Martín, Ana-África, additional, García-Álvarez, María, additional, Vidal-Manceñido, María Jesús, additional, Ferrer-Garrido, Gonzalo, additional, Delgado-Beltrán, María-Pilar, additional, Galende, Josefina, additional, Rodríguez, Juan-Nicolás, additional, Martín-Núñez, Guillermo, additional, Alonso, José-María, additional, García de Coca, Alfonso, additional, Queizán, José A., additional, Sierra, Magdalena, additional, Aguilar, Carlos, additional, Kohlmann, Alexander, additional, Hernández, José-Ángel, additional, González, Marcos, additional, and Hernández-Rivas, Jesús-María, additional

Published
2017
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21. Next-generation sequencing and FISH studies reveal the appearance of gene mutations and chromosomal abnormalities in hematopoietic progenitors in chronic lymphocytic leukemia

Author

Fundación Memoria de D. Samuel Solorzano Barruso, Fundacion de la Sociedad Española de Hematología y Hemoterapia, Ministerio de Economía y Competitividad (España), Red Temática de Investigación Cooperativa en Cáncer (España), Junta de Castilla y León, Instituto de Salud Carlos III, European Commission, Quijada-Álamo, Miguel, Hernández-Sánchez, María, Robledo, Cristina, Hernandez-Sánchez, Jesus M., Benito, Rocío, Montaño, Adrián, Rodríguez-Vicente, Ana Eugenia, Quwaider, Dalia, Martín, Ana-África, García-Alvarez, María, Vidal-Manceñido, María Jesús, Ferrer-Garrido, Gonzalo, Delgado-Beltrán, María-Pilar, Galende, Josefina, Rodríguez, Juan-Nicolas, Martín-Núñez, Guillermo, Alonso, José M., García de Coca, Alfonso, Queizán, José-Antonio, Sierra, Magdalena, Aguilar, Carlos, Kohlmann, Alexander, Hernández, José Ángel, González, Marcos, Hernández, Jesús M., Fundación Memoria de D. Samuel Solorzano Barruso, Fundacion de la Sociedad Española de Hematología y Hemoterapia, Ministerio de Economía y Competitividad (España), Red Temática de Investigación Cooperativa en Cáncer (España), Junta de Castilla y León, Instituto de Salud Carlos III, European Commission, Quijada-Álamo, Miguel, Hernández-Sánchez, María, Robledo, Cristina, Hernandez-Sánchez, Jesus M., Benito, Rocío, Montaño, Adrián, Rodríguez-Vicente, Ana Eugenia, Quwaider, Dalia, Martín, Ana-África, García-Alvarez, María, Vidal-Manceñido, María Jesús, Ferrer-Garrido, Gonzalo, Delgado-Beltrán, María-Pilar, Galende, Josefina, Rodríguez, Juan-Nicolas, Martín-Núñez, Guillermo, Alonso, José M., García de Coca, Alfonso, Queizán, José-Antonio, Sierra, Magdalena, Aguilar, Carlos, Kohlmann, Alexander, Hernández, José Ángel, González, Marcos, and Hernández, Jesús M.

Abstract

[Background]: Chronic lymphocytic leukemia (CLL) is a highly genetically heterogeneous disease. Although CLL has been traditionally considered as a mature B cell leukemia, few independent studies have shown that the genetic alterations may appear in CD34+ hematopoietic progenitors. However, the presence of both chromosomal aberrations and gene mutations in CD34+ cells from the same patients has not been explored. [Methods]: Amplicon-based deep next-generation sequencing (NGS) studies were carried out in magnetically activated-cell-sorting separated CD19+ mature B lymphocytes and CD34+ hematopoietic progenitors (n = 56) to study the mutational status of TP53, NOTCH1, SF3B1, FBXW7, MYD88, and XPO1 genes. In addition, ultra-deep NGS was performed in a subset of seven patients to determine the presence of mutations in flow-sorted CD34+CD19− early hematopoietic progenitors. Fluorescence in situ hybridization (FISH) studies were performed in the CD34+ cells from nine patients of the cohort to examine the presence of cytogenetic abnormalities. [Results]: NGS studies revealed a total of 28 mutations in 24 CLL patients. Interestingly, 15 of them also showed the same mutations in their corresponding whole population of CD34+ progenitors. The majority of NOTCH1 (7/9) and XPO1 (4/4) mutations presented a similar mutational burden in both cell fractions; by contrast, mutations of TP53 (2/2), FBXW7 (2/2), and SF3B1 (3/4) showed lower mutational allele frequencies, or even none, in the CD34+ cells compared with the CD19+ population. Ultra-deep NGS confirmed the presence of FBXW7, MYD88, NOTCH1, and XPO1 mutations in the subpopulation of CD34+CD19− early hematopoietic progenitors (6/7). Furthermore, FISH studies showed the presence of 11q and 13q deletions (2/2 and 3/5, respectively) in CD34+ progenitors but the absence of IGH cytogenetic alterations (0/2) in the CD34+ cells. Combining all the results from NGS and FISH, a model of the appearance and expansion of genetic alterations

Published
2017

22. Hyperdiploidy as a rare event that accompanies poor prognosis markers in CLL

Author

Fundación Ramón Areces, Ministerio de Economía y Competitividad (España), Red Temática de Investigación Cooperativa en Cáncer (España), Sociedad Española de Hematología y Hemoterapia, Junta de Castilla y León, Fundación Memoria de D. Samuel Solorzano Barruso, European Commission, Instituto de Salud Carlos III, González-Gascón y Marín, Isabel, Martín, Ana-África, Hernandez-Sánchez, Jesus M., Robledo, Cristina, Hermosín, Lourdes, Heras, Natalia de las, Lacalle, Laura, Galende, Josefina, Arriba, Felipe de, Rodríguez-Vicente, Ana Eugenia, Hernández, José Ángel, Hernández, Jesús M., Fundación Ramón Areces, Ministerio de Economía y Competitividad (España), Red Temática de Investigación Cooperativa en Cáncer (España), Sociedad Española de Hematología y Hemoterapia, Junta de Castilla y León, Fundación Memoria de D. Samuel Solorzano Barruso, European Commission, Instituto de Salud Carlos III, González-Gascón y Marín, Isabel, Martín, Ana-África, Hernandez-Sánchez, Jesus M., Robledo, Cristina, Hermosín, Lourdes, Heras, Natalia de las, Lacalle, Laura, Galende, Josefina, Arriba, Felipe de, Rodríguez-Vicente, Ana Eugenia, Hernández, José Ángel, and Hernández, Jesús M.

Abstract

The presence of chromosomal gains other than trisomy 12 in chronic lymphocytic leukaemia (CLL) is unusual. However, some patients may show gains on several chromosomes simultaneously suggesting a hyperdiploid karyotype. Objective: The objective of this study was to analyse by FISH the frequency and prognostic impact of hyperdiploidy in CLL. Method: A review of 1359 consecutive cases diagnosed with CLL referred for FISH analysis to a unique institution was carried out. Hyperdiploidy was considered when a gain of at least three of the five FISH probes used was observed. Results: Seven cases (0.51%) with hyperdiploidy were found, confirming that it is a rare event in this disease. Although most patients presented with early Binet stages at diagnosis, six of seven (86%) shortly progressed. The median of time to the first therapy (TTFT) and overall survival (OS) for the patients with hyperdiploidy were short (1.4 months and 20 months, respectively). Moreover, comparing them with a control group of patients (non-hyperdiploid) with completed follow-up data, TTFT and OS of the patients with hyperdiploidy were significantly shorter than the control group. Conclusion: The presence of hyperdiploidy is uncommon and probably associated with poor prognostic markers in CLL.

Published
2017

23. MiRNA expression profile of chronic lymphocytic leukemia patients with 13q deletion

Author

Red Temática de Investigación Cooperativa en Cáncer (España), Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Sociedad Española de Hematología y Hemoterapia, European Commission, Hernández-Sánchez, María, Rodríguez-Vicente, Ana Eugenia, Hernández, José Ángel, Lumbreras, Eva, Sarasquete, María Eugenia, Martín, Ana-África, Benito, Rocío, Vicente-Gutiérrez, Carlos, Robledo, Cristina, Heras, Natalia de las, Rodríguez, Juan-Nicolas, Alcoceba, Miguel, García de Coca, Alfonso, Aguilar, Carlos, González, Marcos, Hernández, Jesús M., Red Temática de Investigación Cooperativa en Cáncer (España), Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Sociedad Española de Hematología y Hemoterapia, European Commission, Hernández-Sánchez, María, Rodríguez-Vicente, Ana Eugenia, Hernández, José Ángel, Lumbreras, Eva, Sarasquete, María Eugenia, Martín, Ana-África, Benito, Rocío, Vicente-Gutiérrez, Carlos, Robledo, Cristina, Heras, Natalia de las, Rodríguez, Juan-Nicolas, Alcoceba, Miguel, García de Coca, Alfonso, Aguilar, Carlos, González, Marcos, and Hernández, Jesús M.

Abstract

Deletion 13q (13q-) is the most common cytogenetic aberration in chronic lymphocytic leukemia (CLL) and is associated with the most favorable prognosis as the sole cytogenetic abnormality. However, it is heterogeneous whereby CLL patients with higher percentages of 13q- cells (13q-H) have a more aggressive clinical course and a distinct gene expression profile. The microRNA (miRNA) expression profile of CLL gives additional biological and prognostic information, but its expression in 13q- CLL has not been examined in detail. The miRNA expression of clonal B cell lymphocytes (CD19+ cells) of 38 CLL patients and normal B cells of six healthy donors was analyzed. CLL patients with higher percentages of 13q- cells (≥80%) showed a different level of miRNA expression from patients with lower percentages (<80%). Interestingly, miR-143 was downregulated and miR-155 was overexpressed in 13q-H. This deregulation affected important validated target genes involved in apoptosis (BCL2, MDM2, TP53INP1) and proliferation (KRAS, PI3K-AKT signaling), that could lead to decreased apoptosis and increased proliferation in 13q-H patients. This study provides new evidence about the heterogeneity of the 13q deletion in CLL patients, showing that miRNA regulation could be involved in several significant pathways deregulated in CLL patients with a high number of losses in 13q.

Published
2016

24. Post-transcriptional modifications contribuye to the overexpression of cyclin D2 in multiple myeloma

Author

Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, Junta de Castilla y León, Grupo Español de Mieloma, Ministerio de Economía y Competitividad (España), European Commission, Josep Carreras Leukemia Foundation, Fundación Inocente Inocente, Misiewicz-Krzeminska, Irena, Sarasquete, María Eugenia, Vicente-Dueñas, Carolina, Krzemiński, Patryk, Wiktorska, Katarzyna, Corchete, Luis A., Quwaider, Dalia, Rojas, Elizabeta A., Corral, Rocío, Martín, Ana-África, Escalante, Fernando, Bárez, Abelardo, García, Juan L., Sánchez García, Isidro, García-Sanz, Ramón, San Miguel, Jesús F., Gutiérrez, Norma Carmen, Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, Junta de Castilla y León, Grupo Español de Mieloma, Ministerio de Economía y Competitividad (España), European Commission, Josep Carreras Leukemia Foundation, Fundación Inocente Inocente, Misiewicz-Krzeminska, Irena, Sarasquete, María Eugenia, Vicente-Dueñas, Carolina, Krzemiński, Patryk, Wiktorska, Katarzyna, Corchete, Luis A., Quwaider, Dalia, Rojas, Elizabeta A., Corral, Rocío, Martín, Ana-África, Escalante, Fernando, Bárez, Abelardo, García, Juan L., Sánchez García, Isidro, García-Sanz, Ramón, San Miguel, Jesús F., and Gutiérrez, Norma Carmen

Abstract

[Purpose]: Dysregulation of one of the three D-cyclin genes has been observed in virtually all multiple myeloma tumors. The mechanisms by which CCND2 is upregulated in a set of multiple myeloma are not completely deciphered. We investigated the role of post-transcriptional regulation through the interaction between miRNAs and their binding sites at 3′UTR in CCND2 overexpression in multiple myeloma. [Experimental Design]: Eleven myeloma cell lines and 45 primary myeloma samples were included in the study. Interactions between miRNAs deregulated in multiple myeloma and mRNA targets were analyzed by 3′UTR-luciferase plasmid assay. The presence of CCND2 mRNA isoforms different in length was explored using qRT-PCR, Northern blot, mRNA FISH, and 3′ rapid amplification of cDNA ends (RACE)-PCR. [Results]: We detected the presence of short CCND2 mRNA, both in the multiple myeloma cell lines and primary cells. The results obtained by 3′RACE experiments revealed that changes in CCND2 3′UTR length are explained by alternative polyadenylation. The luciferase assays using plasmids harboring the truncated CCND2 mRNA strongly confirmed the loss of miRNA sites in the shorter CCND2 mRNA isoform. Those multiple myelomas with greater abundance of the shorter 3′UTR isoform were associated with significant higher level of total CCND2 mRNA expression. Furthermore, functional analysis showed significant CCND2 mRNA shortening after CCND1 silencing and an increased relative expression of longer isoform after CCND1 and CCND3 overexpression, suggesting that cyclin D1 and D3 could regulate CCND2 levels through modifications in polyadenylation-cleavage reaction. [Conclusions]: Overall, these results highlight the impact of CCND2 3′UTR shortening on miRNA-dependent regulation of CCND2 in multiple myeloma.

Published
2016

25. Genome-wide DNA copy number analysis of acute lymphoblastic leukemia identifies new genetic markers associated with clinical outcome

Author

Instituto de Salud Carlos III, Sociedad Española de Hematología y Hemoterapia, European Commission, Universidad Pedagógica y Tecnológica de Colombia, Junta de Castilla y León, Fundación Castellano Leonesa de Hematología y Hemoterapia, Ministerio de Economía y Competitividad (España), Forero-Castro, Maribel, Robledo, Cristina, Benito, Rocío, Abáigar, María, Martín, Ana-África, Arefi, Maryam, Fuster, José Luis, Heras, Natalia de las, Rodríguez, Juan-Nicolas, Quintero, Jonathan, Riesco, Susana, Hermosín, Lourdes, Fuente, Ignacio de la, Recio, Isabel, Ribera, Jordi, Labrador, Jorge, Alonso, José M., Olivier, Carmen, Sierra, Magdalena, Megido, Marta, Corchete, Luis A., Ciudad, Juana, García, Juan L., Ribera, Josep-Maria, Hernández, Jesús M., Instituto de Salud Carlos III, Sociedad Española de Hematología y Hemoterapia, European Commission, Universidad Pedagógica y Tecnológica de Colombia, Junta de Castilla y León, Fundación Castellano Leonesa de Hematología y Hemoterapia, Ministerio de Economía y Competitividad (España), Forero-Castro, Maribel, Robledo, Cristina, Benito, Rocío, Abáigar, María, Martín, Ana-África, Arefi, Maryam, Fuster, José Luis, Heras, Natalia de las, Rodríguez, Juan-Nicolas, Quintero, Jonathan, Riesco, Susana, Hermosín, Lourdes, Fuente, Ignacio de la, Recio, Isabel, Ribera, Jordi, Labrador, Jorge, Alonso, José M., Olivier, Carmen, Sierra, Magdalena, Megido, Marta, Corchete, Luis A., Ciudad, Juana, García, Juan L., Ribera, Josep-Maria, and Hernández, Jesús M.

Abstract

Identifying additional genetic alterations associated with poor prognosis in acute lymphoblastic leukemia (ALL) is still a challenge. Aims: To characterize the presence of additional DNA copy number alterations (CNAs) in children and adults with ALL by whole-genome oligonucleotide array (aCGH) analysis, and to identify their associations with clinical features and outcome. Array-CGH was carried out in 265 newly diagnosed ALLs (142 children and 123 adults). The NimbleGen CGH 12x135K array (Roche) was used to analyze genetic gains and losses. CNAs were analyzed with GISTIC and aCGHweb software. Clinical and biological variables were analyzed. Three of the patients showed chromothripsis (cth6, cth14q and cth15q). CNAs were associated with age, phenotype, genetic subtype and overall survival (OS). In the whole cohort of children, the losses on 14q32.33 (p = 0.019) and 15q13.2 (p = 0.04) were related to shorter OS. In the group of children without good- or poor-risk cytogenetics, the gain on 1p36.11 was a prognostic marker independently associated with shorter OS. In adults, the gains on 19q13.2 (p = 0.001) and Xp21.1 (p = 0.029), and the loss of 17p (p = 0.014) were independent markers of poor prognosis with respect to OS. In summary, CNAs are frequent in ALL and are associated with clinical parameters and survival. Genome-wide DNA copy number analysis allows the identification of genetic markers that predict clinical outcome, suggesting that detection of these genetic lesions will be useful in the management of patients newly diagnosed with ALL.

Published
2016

26. Integrative analysis of DNA copy number, DNA methylation and gene expression in multiple myeloma reveals alterations related to relapse

Author

Asociación Española Contra el Cáncer, Instituto de Salud Carlos III, Junta de Castilla y León, European Commission, Grupo Español de Mieloma, Krzemiński, Patryk, Corchete, Luis A., García, Juan L., López-Corral, L., Fermiñán, Encarnación, García García, Eva María, Martín, Ana-África, Hernández, Jesús M., García-Sanz, Ramón, San Miguel, Jesús F., Gutiérrez, Norma Carmen, Asociación Española Contra el Cáncer, Instituto de Salud Carlos III, Junta de Castilla y León, European Commission, Grupo Español de Mieloma, Krzemiński, Patryk, Corchete, Luis A., García, Juan L., López-Corral, L., Fermiñán, Encarnación, García García, Eva María, Martín, Ana-África, Hernández, Jesús M., García-Sanz, Ramón, San Miguel, Jesús F., and Gutiérrez, Norma Carmen

Abstract

Multiple myeloma (MM) remains incurable despite the introduction of novel agents, and a relapsing course is observed in most patients. Although the development of genomic technologies has greatly improved our understanding of MM pathogenesis, the mechanisms underlying relapse have been less thoroughly investigated. In this study, an integrative analysis of DNA copy number, DNA methylation and gene expression was conducted in matched diagnosis and relapse samples from MM patients. Overall, the acquisition of abnormalities at relapse was much more frequent than the loss of lesions present at diagnosis, and DNA losses were significantly more frequent in relapse than in diagnosis samples. Interestingly, copy number abnormalities involving more than 100 Mb of DNA at relapse significantly affect the gene expression of these samples, provoking a particular deregulation of the IL-8 pathway. On the other hand, no significant modifications of gene expression were observed in those samples with less than 100 Mb affected by chromosomal changes. Although several statistical approaches were used to identify genes whose abnormal expression at relapse was regulated by methylation, only two genes that were significantly deregulated in relapse samples (SORL1 and GLT1D1) showed a negative correlation between methylation and expression. Further analysis revealed that DNA methylation was involved in regulating SORL1 expression in MM. Finally, relevant changes in gene expression observed in relapse samples, such us downregulation of CD27 and P2RY8, were most likely not preceded by alterations in the corresponding DNA. Taken together, these results suggest that the genomic heterogeneity described at diagnosis remains at relapse.

Published
2016

27. Chromothripsis is a recurrent genomic abnormality in high-risk myelodysplastic syndromes

Author

AstraZeneca, Sociedad Española de Hematología y Hemoterapia, Consejo Superior de Investigaciones Científicas (España), European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Abáigar, María, Robledo, Cristina, Benito, Rocío, Ramos, Fernando, Díez-Campelo, María, Hermosín, Lourdes, Sánchez-del-Real, Javier, Alonso, José M., Cuello, Rebeca, Megido, Marta, Rodríguez, Juan-Nicolas, Martín-Núñez, Guillermo, Aguilar, Carlos, Vargas, Manuel, Martín, Ana-África, García, Juan L., Kohlmann, Alexander, Cañizo, María Consuelo del, Hernández, Jesús M., AstraZeneca, Sociedad Española de Hematología y Hemoterapia, Consejo Superior de Investigaciones Científicas (España), European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Abáigar, María, Robledo, Cristina, Benito, Rocío, Ramos, Fernando, Díez-Campelo, María, Hermosín, Lourdes, Sánchez-del-Real, Javier, Alonso, José M., Cuello, Rebeca, Megido, Marta, Rodríguez, Juan-Nicolas, Martín-Núñez, Guillermo, Aguilar, Carlos, Vargas, Manuel, Martín, Ana-África, García, Juan L., Kohlmann, Alexander, Cañizo, María Consuelo del, and Hernández, Jesús M.

Abstract

To explore novel genetic abnormalities occurring in myelodysplastic syndromes (MDS) through an integrative study combining array-based comparative genomic hybridization (aCGH) and next-generation sequencing (NGS) in a series of MDS and MDS/myeloproliferative neoplasms (MPN) patients. 301 patients diagnosed with MDS (n = 240) or MDS/MPN (n = 61) were studied at the time of diagnosis. A genome-wide analysis of DNA copy number abnormalities was performed. In addition, a mutational analysis of DNMT3A, TET2, RUNX1, TP53 and BCOR genes was performed by NGS in selected cases. 285 abnormalities were identified in 71 patients (23.6%). Three high-risk MDS cases (1.2%) displayed chromothripsis involving exclusively chromosome 13 and affecting some cancer genes: FLT3, BRCA2 and RB1. All three cases carried TP53 mutations as revealed by NGS. Moreover, in the whole series, the integrative analysis of aCGH and NGS enabled the identification of cryptic recurrent deletions in 2p23.3 (DNMT3A; n = 2.8%), 4q24 (TET2; n = 10%) 17p13 (TP53; n = 8.5%), 21q22 (RUNX1; n = 7%), and Xp11.4 (BCOR; n = 2.8%), while mutations in the non-deleted allele where found only in DNMT3A (n = 1), TET2 (n = 3), and TP53 (n = 4). These cryptic abnormalities were detected mainly in patients with normal (45%) or non-informative (15%) karyotype by conventional cytogenetics, except for those with TP53 deletion and mutation (15%), which had a complex karyotype. In addition to wellknown copy number defects, the presence of chromothripsis involving chromosome 13 was a novel recurrent change in high-risk MDS patients. Array CGH analysis revealed thepresence of cryptic abnormalities in genomic regions where MDS-related genes, such as TET2, DNMT3A, RUNX1 and BCOR, are located.

Published
2016

28. Analysis of Clonal Evolution in Chronic Lymphocytic Leukemia from Inactive to Symptomatic Disease Prior Treatment Using Whole-Exome Sequencing

Author

Hernández-Sánchez, María, primary, Radova, Lenka, additional, Kotaskova, Jana, additional, Tamborero, David, additional, Rodriguez, Ana E, additional, Plevova, Karla, additional, Abáigar, María, additional, Bikos, Vasileios, additional, Benito, Rocío, additional, Takacova, Sylvia, additional, Quijada, Miguel, additional, Martín, Ana África, additional, Alcoceba, Miguel, additional, García de Coca, Alfonso, additional, Doubek, Michael, additional, González, Marcos, additional, Lopez-Bigas, Nuria, additional, Pospisilova, Sarka, additional, and Hernández-Rivas, Jesús María, additional

Published
2016
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29. Hyperdiploidy as a rare event that accompanies poor prognosis markers in CLL

Author

González‐Gascón y Marín, Isabel, primary, Martín, Ana África, additional, Hernández‐Sanchez, María, additional, Robledo, Cristina, additional, Hermosín, María Lourdes, additional, de las Heras, Natalia, additional, Lacalle, Laura, additional, Galende, Josefina, additional, de Arriba, Felipe, additional, Rodríguez‐Vicente, Ana Eugenia, additional, Hernández, José‐Ángel, additional, and Hernández‐Rivas, Jesús María, additional

Published
2016
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30. Poster: CT-195 Predictive Value of ST2, REG3a, and MAGIC Algorithm in Haploidentical Transplantation With Post-Transplant Cyclophosphamide Outcomes

Author

Santos, Marta Fonseca, Alvarez, Maria Garcia, Sanchez, Luis Antonio Corchete, Sanchez, Alberto Hernandez, Martinez, Borja Puertas, Salinero, Manuela, Rodriguez, Angela, Martin, Ana Africa, Pita, Alejandro Avendaño, Gonzalez, Monica Baile, Cabero, Almudena, Lopez, Estefania Perez, Calvo, Monica Cabrero, Sanchez-Guijo, Fermin, Lopez, Lourdes Vazquez, Garcia-Sanz, Ramon, Barrigon, Maria Dolores Caballero, Alcoceba, Miguel, and Lopez-Corral, Lucia

Published
2022
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31. Insights into epigenetic regulation of microRNA-155 expression in multiple myeloma

Author

Instituto de Salud Carlos III, Junta de Castilla y León, Grupo Español de Mieloma, Asociación Española Contra el Cáncer, Krzemiński, Patryk, Sarasquete, María Eugenia, Misiewicz-Krzeminska, Irena, Corral, Rocío, Corchete, Luis A., Martín, Ana-África, García-Sanz, Ramón, San Miguel, Jesús F., Gutiérrez, Norma Carmen, Instituto de Salud Carlos III, Junta de Castilla y León, Grupo Español de Mieloma, Asociación Española Contra el Cáncer, Krzemiński, Patryk, Sarasquete, María Eugenia, Misiewicz-Krzeminska, Irena, Corral, Rocío, Corchete, Luis A., Martín, Ana-África, García-Sanz, Ramón, San Miguel, Jesús F., and Gutiérrez, Norma Carmen

Abstract

[Context]: MiR-155 plays a critical role in the development of B-cell malignancies. Previous studies have shown a deregulation of miR-155 in specific cytogenetic subtypes of multiple myeloma (MM). However, the mechanisms that regulate miR-155 expression in MM are not fully understood. [Objective]: In the present study, we explored the regulation of miRNA-155 in MM by DNA methylation mechanisms and the impact of miR-155 expression in survival of MM patients. [Method]: Primary samples were obtained from 95 patients with newly diagnosed myeloma. Methylation was analyzed by Methylation Specific PCR, sequencing of bisulfite treated DNA and luciferase assay. [Results]: qRT-PCR analysis revealed that miR-155 was differentially expressed in MM and its upregulation was associated with longer survival. DNA methylation of CpG island present in the first exon of miR-155 host gene was associated with its low expression in MM cell lines and patient samples. Our results showed for the first time that in vitro methylation of part of the promoter and first exon abrogated the miR-155 expression. We further showed that miR-155 expression in MM cell lines was increased by demethylating 5-aza-dC treatment and decreased by RNA-directed DNA methylation. Additionally, we found that LPS >immunological challenge> was insufficient to induce miR-155 expression in MM cell lines with methylated DNA around transcription start site (TSS). [Conclusion]: This study provides evidence that DNA methylation contributes to miR-155 expression in myeloma cells. Interestingly, the survival data showed an association between miR-155 expression and outcome of MM.

Published
2015

32. Hyperdiploidy as a rare event that accompanies poor prognosis markers in CLL.

Author

González‐Gascón y Marín, Isabel, Martín, Ana África, Hernández‐Sanchez, María, Robledo, Cristina, Hermosín, María Lourdes, Heras, Natalia, Lacalle, Laura, Galende, Josefina, Arriba, Felipe, Rodríguez‐Vicente, Ana Eugenia, Hernández, José‐Ángel, and Hernández‐Rivas, Jesús María

Subjects
*LYMPHOCYTIC leukemia, *TRISOMY, *BIOMARKERS, *CHROMOSOMES, *DIPLOIDY, *PROGNOSIS
Abstract

The presence of chromosomal gains other than trisomy 12 in chronic lymphocytic leukaemia ( CLL) is unusual. However, some patients may show gains on several chromosomes simultaneously suggesting a hyperdiploid karyotype. Objective The objective of this study was to analyse by FISH the frequency and prognostic impact of hyperdiploidy in CLL. Method A review of 1359 consecutive cases diagnosed with CLL referred for FISH analysis to a unique institution was carried out. Hyperdiploidy was considered when a gain of at least three of the five FISH probes used was observed. Results Seven cases (0.51%) with hyperdiploidy were found, confirming that it is a rare event in this disease. Although most patients presented with early Binet stages at diagnosis, six of seven (86%) shortly progressed. The median of time to the first therapy ( TTFT) and overall survival ( OS) for the patients with hyperdiploidy were short (1.4 months and 20 months, respectively). Moreover, comparing them with a control group of patients (non-hyperdiploid) with completed follow-up data, TTFT and OS of the patients with hyperdiploidy were significantly shorter than the control group. Conclusion The presence of hyperdiploidy is uncommon and probably associated with poor prognostic markers in CLL. [ABSTRACT FROM AUTHOR]

Published
2017
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33. An Analysis of Prognostic Markers and the Performance of Scoring Systems in 1837 Patients with Therapy-Related Myelodysplastic Syndrome - a Study of the International Working Group (IWG-PM) for Myelodysplastic Syndromes (MDS)

Author

Kuendgen, Andrea, Tuechler, Heinz, Nomdedeu, Meritxell, Garcia-Manero, Guillermo, Komrokji, Rami S., Sekeres, Mikkael A., Della Porta, Matteo Giovanni, List, Alan F, Cazzola, Mario, DeZern, Amy E., Roboz, Gail J., Steensma, David P., van de Loosdrecht, Arjan A, Schlenk, Richard F., Calvo, Xavier, Blum, Sabine, Pereira, Arturo, Valent, Peter, Costa, Dolors, Giagounidis, Aristoteles, Benlloch, Luis, Platzbecker, Uwe, Pedro, Carmen, Lübbert, Michael, Cedena, Maria Teresa, Machherndl-Spandl, Sigrid, Lopez-Pavia, Maria, Haase, Detlef, Martin, Ana Africa, Baldus, Claudia D, Martínez de Sola, Montserrat, Stauder, Reinhard, Merchan, Brayan, Mende, Claudia, Ardanaz, María Teresa, Ganster, Christina, Cobo, Francesc, Schroeder, Thomas, Esteve, Jordi, Haas, Rainer, Benet, Nomdedeu, Greenberg, Peter L., Germing, Ulrich, and Sanz, Guillermo

Published
2015
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34. A Low Frequency of Losses in 11q Chromosome Is Associated with Better Outcome and Lower Rate of Genomic Mutations in Patients with Chronic Lymphocytic Leukemia.

Author

Hernández, José Ángel, Hernández-Sánchez, María, Rodríguez-Vicente, Ana Eugenia, Grossmann, Vera, Collado, Rosa, Heras, Cecilia, Puiggros, Anna, Martín, Ana África, Puig, Noemí, Benito, Rocío, Robledo, Cristina, Delgado, Julio, González, Teresa, Queizán, José Antonio, Galende, Josefina, de la Fuente, Ignacio, Martín-Núñez, Guillermo, Alonso, José María, Abrisqueta, Pau, and Luño, Elisa

Subjects
CHROMOSOMES, GENETIC mutation, CHRONIC lymphocytic leukemia, FLUORESCENCE in situ hybridization, LYMPHADENITIS, NUCLEOTIDE sequence
Abstract

To analyze the impact of the 11q deleted (11q-) cells in CLL patients on the time to first therapy (TFT) and overall survival (OS), 2,493 patients with CLL were studied. 242 patients (9.7%) had 11q-. Fluorescence in situ hybridization (FISH) studies showed a threshold of 40% of deleted cells to be optimal for showing that clinical differences in terms of TFT and OS within 11q- CLLs. In patients with ≥40% of losses in 11q (11q-H) (74%), the median TFT was 19 months compared with 44 months in CLL patients with <40% del(11q) (11q-L) (P<0.0001). In the multivariate analysis, only the presence of 11q-L, mutated IGHV status, early Binet stage and absence of extended lymphadenopathy were associated with longer TFT. Patients with 11q-H had an OS of 90 months, while in the 11q-L group the OS was not reached (P = 0.008). The absence of splenomegaly (P = 0.02), low LDH (P = 0.018) or β2M (P = 0.006), and the presence of 11q-L (P = 0.003) were associated with a longer OS. In addition, to detect the presence of mutations in the ATM, TP53, NOTCH1, SF3B1, MYD88, FBXW7, XPO1 and BIRC3 genes, a select cohort of CLL patients with losses in 11q was sequenced by next-generation sequencing of amplicons. Eighty % of CLLs with 11q- showed mutations and fewer patients with low frequencies of 11q- had mutations among genes examined (50% vs 94.1%, P = 0.023). In summary, CLL patients with <40% of 11q- had a long TFT and OS that could be associated with the presence of fewer mutated genes. [ABSTRACT FROM AUTHOR]

Published
2015
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35. Clinical Features and Prognostic Assessment in 233 Patients with Therapy-Related Myelodysplastic Syndromes: The IPSS-R Is a Powerful Predictor of Outcome

Author

Nomdedeu, Meritxell, Calvo, Xavier, Pereira, Arturo, Costa, Dolors, Pedro, Carmen, Cedena, Maria Teresa, López-Pavía, María, Martín, Ana Africa, Martínez de Sola, Montserrat, Merchan, Brayan Marcel, Ardanaz, Maria Teresa, Esteve, Jordi, Cobo, Francesc, Sanz, Guillermo F., and Nomdedeu, Benet

Published
2014
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