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1. Single-cell multi-omics analysis of COVID-19 patients with pre-existing autoimmune diseases shows aberrant immune responses to infection

Author: Gates Cambridge Scholarships, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Chan Zuckerberg Biohub, Wellcome Sanger Institute, Josep Carreras Leukemia Foundation, Andrés-León, Eduardo [0000-0002-0621-9914], https://ror.org/02gfc7t72, Barmada, Anis, Handfield, Louis-François, Godoy-Tena, Gerard, de la Calle-Fabregat, Carlos, Ciudad, Laura, Arutyunyan, Anna, Andrés-León, Eduardo, Hoo, Regina, Porter, Tarryn, Oszlanczi, Agnes, Richardson, Laura, Calero-Nieto, Fernando J., Wilson, Nicola K., Marchese, Domenica, Sancho-Serra, Carmen, Carrillo, Jorge, Presas-Rodríguez, Silvia, Ramo-Tello, Cristina, Ruiz-Sanmartin, Adolfo, Ferrer, Ricard, Ruiz-Rodriguez, Juan Carlos, Martínez-Gallo, Mónica, Munera-Campos, Mónica, Carrascosa, Jose Manuel, Göttgens, Berthold, Heyn, Holger, Prigmore, Elena, Casafont-Solé, Ivette, Solanich, Xavier, Sánchez-Cerrillo, Ildefonso, González-Álvaro, Isidoro, Raimondo, Maria Gabriella, Ramming, Andreas, Martin, Javier, Martínez-Cáceres, Eva, Ballestar, Esteban, Vento-Tormo, Roser, Rodríguez-Ubreva, Javier, Gates Cambridge Scholarships, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Chan Zuckerberg Biohub, Wellcome Sanger Institute, Josep Carreras Leukemia Foundation, Andrés-León, Eduardo [0000-0002-0621-9914], https://ror.org/02gfc7t72, Barmada, Anis, Handfield, Louis-François, Godoy-Tena, Gerard, de la Calle-Fabregat, Carlos, Ciudad, Laura, Arutyunyan, Anna, Andrés-León, Eduardo, Hoo, Regina, Porter, Tarryn, Oszlanczi, Agnes, Richardson, Laura, Calero-Nieto, Fernando J., Wilson, Nicola K., Marchese, Domenica, Sancho-Serra, Carmen, Carrillo, Jorge, Presas-Rodríguez, Silvia, Ramo-Tello, Cristina, Ruiz-Sanmartin, Adolfo, Ferrer, Ricard, Ruiz-Rodriguez, Juan Carlos, Martínez-Gallo, Mónica, Munera-Campos, Mónica, Carrascosa, Jose Manuel, Göttgens, Berthold, Heyn, Holger, Prigmore, Elena, Casafont-Solé, Ivette, Solanich, Xavier, Sánchez-Cerrillo, Ildefonso, González-Álvaro, Isidoro, Raimondo, Maria Gabriella, Ramming, Andreas, Martin, Javier, Martínez-Cáceres, Eva, Ballestar, Esteban, Vento-Tormo, Roser, and Rodríguez-Ubreva, Javier
Abstract: In COVID-19, hyperinflammatory and dysregulated immune responses contribute to severity. Patients with pre-existing autoimmune conditions can therefore be at increased risk of severe COVID-19 and/or associated sequelae, yet SARS-CoV-2 infection in this group has been little studied. Here, we performed single-cell analysis of peripheral blood mononuclear cells from patients with three major autoimmune diseases (rheumatoid arthritis, psoriasis, or multiple sclerosis) during SARS-CoV-2 infection. We observed compositional differences between the autoimmune disease groups coupled with altered patterns of gene expression, transcription factor activity, and cell-cell communication that substantially shape the immune response under SARS-CoV-2 infection. While enrichment of HLA-DRlow CD14+ monocytes was observed in all three autoimmune disease groups, type-I interferon signaling as well as inflammatory T cell and monocyte responses varied widely between the three groups of patients. Our results reveal disturbed immune responses to SARS-CoV-2 in patients with pre-existing autoimmunity, highlighting important considerations for disease treatment and follow-up.
Published: 2024

2. ALPL-1 is a target for chimeric antigen receptor therapy in osteosarcoma

Author: Norwegian Research Council, Southern and Eastern Norway Regional Health Authority, Nova Southeastern University, Swedish Society for Medical Research, Fundación la Caixa, European Commission, Instituto de Salud Carlos III, European Institute of Innovation and Technology, Josep Carreras Leukemia Foundation, Centres de Recerca de Catalunya, Generalitat de Catalunya, Mensali, Nadia, Köksal, Hakan, Joaquina, Sandy, Wernhoff, Patrik, Casey, Nicholas P., Romecin, Paola, Panisello, Carla, Rodriguez, René, Vimeux, Lene, Juzeniene, Asta, Myhre, Marit R., Fåne, Anne, Castilla, Carolina, Maggadottir, Solrun Melkorka, Duru, Adil Doganay, Georgoudaki, Anna-Maria, Grad, Iwona, Maturana, Andrés Daniel, Gaudernack, Gustav, Kvalheim, Gunnar, Carcaboso, Ángel M., Álava, Enrique de, Donnadieu, Emmanuel, Bruland, Øyvind S., Menéndez, Pablo, Inderberg, Else Marit, Wälchli, Sébastien, Norwegian Research Council, Southern and Eastern Norway Regional Health Authority, Nova Southeastern University, Swedish Society for Medical Research, Fundación la Caixa, European Commission, Instituto de Salud Carlos III, European Institute of Innovation and Technology, Josep Carreras Leukemia Foundation, Centres de Recerca de Catalunya, Generalitat de Catalunya, Mensali, Nadia, Köksal, Hakan, Joaquina, Sandy, Wernhoff, Patrik, Casey, Nicholas P., Romecin, Paola, Panisello, Carla, Rodriguez, René, Vimeux, Lene, Juzeniene, Asta, Myhre, Marit R., Fåne, Anne, Castilla, Carolina, Maggadottir, Solrun Melkorka, Duru, Adil Doganay, Georgoudaki, Anna-Maria, Grad, Iwona, Maturana, Andrés Daniel, Gaudernack, Gustav, Kvalheim, Gunnar, Carcaboso, Ángel M., Álava, Enrique de, Donnadieu, Emmanuel, Bruland, Øyvind S., Menéndez, Pablo, Inderberg, Else Marit, and Wälchli, Sébastien
Abstract: Osteosarcoma (OS) remains a dismal malignancy in children and young adults, with poor outcome for metastatic and recurrent disease. Immunotherapies in OS are not as promising as in some other cancer types due to intra-tumor heterogeneity and considerable off-target expression of the potentially targetable proteins. Here we show that chimeric antigen receptor (CAR) T cells could successfully target an isoform of alkaline phosphatase, ALPL-1, which is highly and specifically expressed in primary and metastatic OS. The target recognition element of the second-generation CAR construct is based on two antibodies, previously shown to react against OS. T cells transduced with these CAR constructs mediate efficient and effective cytotoxicity against ALPL-positive cells in in vitro settings and in state-of-the-art in vivo orthotopic models of primary and metastatic OS, without unexpected toxicities against hematopoietic stem cells or healthy tissues. In summary, CAR-T cells targeting ALPL-1 show efficiency and specificity in treating OS in preclinical models, paving the path for clinical translation.
Published: 2023

3. Proposed European Competence Network on Mastocytosis—American Initiative in Mast Cell Diseases (ECNM-AIM) Response Criteria in Advanced Systemic Mastocytosis

Author: Charles and Ann Johnson Foundation, Josep Carreras Leukemia Foundation, National Institute of Allergy and Infectious Diseases (US), Gotlib, Jason, Schwaab, Juliana, Shomali, William, George, Tracy I., Radia, Deepti, Castells, Mariana, Carter, Melody C., Hartmann, Karin, Álvarez-Twos, Iván, Brockow, Knut, Bonadonna, Patrizia, Hermine, Olivier, Niedoszytko, Marek, Hoermann, Gregor, Sperr, Wolfgang R., Oude Elberink, Hanneke, Siebenhaar, Frank, Butterfield, Joseph H., Ustun, Celalettin, Zanotti, Roberta, Triggiani, Massimo, Schwartz, Lawrence B., Lyons, Jonathan J., Orfao, Alberto, Sotlar, Karl, Horny, Hans-Peter, Arock, Michel, Metcalfe, Dean D., Akin, Cem, Lübke, Johannes, Valent, Peter, Reiter, Andreas, Charles and Ann Johnson Foundation, Josep Carreras Leukemia Foundation, National Institute of Allergy and Infectious Diseases (US), Gotlib, Jason, Schwaab, Juliana, Shomali, William, George, Tracy I., Radia, Deepti, Castells, Mariana, Carter, Melody C., Hartmann, Karin, Álvarez-Twos, Iván, Brockow, Knut, Bonadonna, Patrizia, Hermine, Olivier, Niedoszytko, Marek, Hoermann, Gregor, Sperr, Wolfgang R., Oude Elberink, Hanneke, Siebenhaar, Frank, Butterfield, Joseph H., Ustun, Celalettin, Zanotti, Roberta, Triggiani, Massimo, Schwartz, Lawrence B., Lyons, Jonathan J., Orfao, Alberto, Sotlar, Karl, Horny, Hans-Peter, Arock, Michel, Metcalfe, Dean D., Akin, Cem, Lübke, Johannes, Valent, Peter, and Reiter, Andreas
Abstract: Advanced systemic mastocytosis (AdvSM) is characterized by the presence of KIT D816V and other somatic mutations (eg, in SRSF2, ASXL1, and RUNX1) in 95% and 60% to 70% of patients, respectively. The biological and clinical consequences of AdvSM include multilineage involvement (eg, associated hematologic neoplasm) in 60% to 80% of patients, variable infiltration and damage (C-findings) of predominantly bone marrow and visceral organs through affected mast cell (MC) and non-MC lineages, and elevated levels of serum tryptase. Recently, the treatment landscape has substantially changed with the introduction of the multikinase/KIT inhibitor midostaurin and the selective KIT D816V inhibitor avapritinib. In this review, we discuss the evolution of AdvSM response criteria that have been developed to better capture clinical benefit (eg, improved responses and progression-free and overall survival). We propose refined response criteria from European Competence Network on Mastocytosis and American Initiative in Mast Cell Diseases investigators that use a tiered approach to segregate the effects of histopathologic (eg, bone marrow MC burden, tryptase), molecular (eg, KIT D816V variant allele frequency), clinical (eg, C-findings), and symptom response on long-term outcomes. These response criteria require evaluation in future prospective clinical trials of selective KIT inhibitors and other novel agents.
Published: 2022

4. The HDAC7-TET2 epigenetic axis is essential during early B lymphocyte development

Author: Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Josep Carreras Leukemia Foundation, Asociación Española Contra el Cáncer, Fundación la Caixa, Instituto de Salud Carlos III, Azagra, Alba, Meler, Ainara, Barrios, Oriol de, Tomás-Daza, Laureano, Collazo, Olga, Monterde, Beatriz, Obiols, Mireia, Rovirosa, Llorenç, Vila-Casadesús, Maria, Cabrera-Pasadas, Mónica, Gusi-Vives, Mar, Graf, Thomas, Varela, Ignacio, Sardina, José Luis, Javierre, Biola M., Parra, Maribel, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Josep Carreras Leukemia Foundation, Asociación Española Contra el Cáncer, Fundación la Caixa, Instituto de Salud Carlos III, Azagra, Alba, Meler, Ainara, Barrios, Oriol de, Tomás-Daza, Laureano, Collazo, Olga, Monterde, Beatriz, Obiols, Mireia, Rovirosa, Llorenç, Vila-Casadesús, Maria, Cabrera-Pasadas, Mónica, Gusi-Vives, Mar, Graf, Thomas, Varela, Ignacio, Sardina, José Luis, Javierre, Biola M., and Parra, Maribel
Abstract: Correct B cell identity at each stage of cellular differentiation during B lymphocyte development is critically dependent on a tightly controlled epigenomic landscape. We previously identified HDAC7 as an essential regulator of early B cell development and its absence leads to a drastic block at the pro-B to pre-B cell transition. More recently, we demonstrated that HDAC7 loss in pro-B-ALL in infants associates with a worse prognosis. Here we delineate the molecular mechanisms by which HDAC7 modulates early B cell development. We find that HDAC7 deficiency drives global chromatin de-condensation, histone marks deposition and deregulates other epigenetic regulators and mobile elements. Specifically, the absence of HDAC7 induces TET2 expression, which promotes DNA 5-hydroxymethylation and chromatin de-condensation. HDAC7 deficiency also results in the aberrant expression of microRNAs and LINE-1 transposable elements. These findings shed light on the mechanisms by which HDAC7 loss or misregulation may lead to B cell-based hematological malignancies.
Published: 2022

5. Distinct roles for PARP-1 and PARP-2 in c-Myc-driven B-cell lymphoma in mice

Author: Ministerio de Industria y Competitividad (España), Ministerio de Ciencia e Innovación (España), Fundación Científica Asociación Española Contra el Cáncer, Medical Research Council (UK), Laboratory of Excellence of Biology for Psychiatry (France), Université de Strasbourg, Centre National de la Recherche Scientifique (France), Instituto de Salud Carlos III, European Commission, Generalitat de Catalunya, Centres de Recerca de Catalunya, Josep Carreras Leukemia Foundation, Fundación Unoentrecienmil, Marie Curie International Incoming Fellowship, Galindo-Campos, M. A., Lutfi, Nuria, Bonnin, S., Martínez, C., Velasco-Hernández, Talia, García-Hernández, V., Martín Caballero, Juan, Ampurdanés, Coral, Gimeno, R., Colomo, L., Roué, Gaël, Guilbaud, G., Dantzer, Françoise, Navarro Medrano, Pilar, Murga, Matilde, Fernández-Capetillo, Óscar, Bigas, A., Menéndez, Pablo, Sale; J. E., Ministerio de Industria y Competitividad (España), Ministerio de Ciencia e Innovación (España), Fundación Científica Asociación Española Contra el Cáncer, Medical Research Council (UK), Laboratory of Excellence of Biology for Psychiatry (France), Université de Strasbourg, Centre National de la Recherche Scientifique (France), Instituto de Salud Carlos III, European Commission, Generalitat de Catalunya, Centres de Recerca de Catalunya, Josep Carreras Leukemia Foundation, Fundación Unoentrecienmil, Marie Curie International Incoming Fellowship, Galindo-Campos, M. A., Lutfi, Nuria, Bonnin, S., Martínez, C., Velasco-Hernández, Talia, García-Hernández, V., Martín Caballero, Juan, Ampurdanés, Coral, Gimeno, R., Colomo, L., Roué, Gaël, Guilbaud, G., Dantzer, Françoise, Navarro Medrano, Pilar, Murga, Matilde, Fernández-Capetillo, Óscar, Bigas, A., Menéndez, Pablo, and Sale; J. E.
Abstract: Dysregulation of the c-Myc oncogene occurs in a wide variety of hematologic malignancies, and its overexpression has been linked with aggressive tumor progression. Here, we show that poly (ADP-ribose) polymerase 1 (PARP-1) and PARP-2 exert opposing influences on progression of c-Myc-driven B-cell lymphoma. PARP-1 and PARP-2 catalyze the synthesis and transfer of ADP-ribose units onto amino acid residues of acceptor proteins in response to DNA strand breaks, playing a central role in the response to DNA damage. Accordingly, PARP inhibitors have emerged as promising new cancer therapeutics. However, the inhibitors currently available for clinical use are not able to discriminate between individual PARP proteins. We found that genetic deletion of PARP-2 prevents c-Myc-driven B-cell lymphoma, whereas PARP-1 deficiency accelerates lymphomagenesis in the E¿-Myc mouse model of aggressive B-cell lymphoma. Loss of PARP-2 aggravates replication stress in preleukemic E¿-Myc B cells, resulting in accumulation of DNA damage and concomitant cell death that restricts the c-Myc-driven expansion of B cells, thereby providing protection against B-cell lymphoma. In contrast, PARP-1 deficiency induces a proinflammatory response and an increase in regulatory T cells, likely contributing to immune escape of B-cell lymphoma, resulting in an acceleration of lymphomagenesis. These findings pinpoint specific functions for PARP-1 and PARP-2 in c-Myc-driven lymphomagenesis with antagonistic consequences that may help inform the design of new PARP-centered therapeutic strategies, with selective PARP-2 inhibition potentially representing a new therapeutic approach for the treatment of c-Myc-driven tumors.
Published: 2022

6. HDAC7 is a major contributor in the pathogenesis of infant t(4;11) proB acute lymphoblastic leukemia

Author: Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Josep Carreras Leukemia Foundation, European Commission, Ministerio de Economía y Competitividad (España), Fundación Unoentrecienmil, Fundación Leo Messi, Asociación Española Contra el Cáncer, Instituto de Salud Carlos III, Barrios, Oriol de, Galaras, Alexandros, Trincado, Juan L., Azagra, Alba, Collazo, Olga, Meler, Ainara, Agraz-Doblas, Antonio, Bueno, Clara, Ballerini, Paola, Cazzaniga, Giovanni, Stam, Ronald W., Varela, Ignacio, Lorenzo, Paola De, Grazia Valsecchi, Maria, Hatzis, Pantelis, Menéndez, Pablo, Parra, Maribel, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Josep Carreras Leukemia Foundation, European Commission, Ministerio de Economía y Competitividad (España), Fundación Unoentrecienmil, Fundación Leo Messi, Asociación Española Contra el Cáncer, Instituto de Salud Carlos III, Barrios, Oriol de, Galaras, Alexandros, Trincado, Juan L., Azagra, Alba, Collazo, Olga, Meler, Ainara, Agraz-Doblas, Antonio, Bueno, Clara, Ballerini, Paola, Cazzaniga, Giovanni, Stam, Ronald W., Varela, Ignacio, Lorenzo, Paola De, Grazia Valsecchi, Maria, Hatzis, Pantelis, Menéndez, Pablo, and Parra, Maribel
Published: 2021

7. Leukemia Stem Cell Drug Discovery

Author: European Commission, Ministerio de Economía y Competitividad (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Junta de Castilla y León, Josep Carreras Leukemia Foundation, Fundación Unoentrecienmil, Cobaleda, César, Sánchez García, Isidro, European Commission, Ministerio de Economía y Competitividad (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Junta de Castilla y León, Josep Carreras Leukemia Foundation, Fundación Unoentrecienmil, Cobaleda, César, and Sánchez García, Isidro
Abstract: The relative survival of cancer patients, when considering the tumoral stage at diagnosis, has not changed significantly in the last three decades, in spite of our increasingly detailed knowledge of the molecular alterations occurring in human tumors. In parallel, despite a growing number of clinical trials being conducted, the absolute number of drugs that are effective in humans is declining, and many new drugs move into the market without having enough evidence of their benefit on survival or quality of life. In part, this failure is due to the discordance between the results from preclinical and clinical trial phases, therefore leading to a high percentage of apparently promising lead compounds being abandoned in the transfer to the clinic. This discordance is caused, to a large degree, by the use of inappropriate animal models in the first stages of drug development. In this chapter, we discuss how the development of cancer therapies needs to be redesigned in order to achieve cancer cure, and how this redesign must involve the generation of better animal models, based on the tenets of the cancer stem cell theory, and capable of recapitulating all the aspects of human cancer. The use of such improved models should increase the likelihood of success in drug development, reducing the number of agents that go into trial, and the amount of patients undergoing useless trials.
Published: 2021

8. Infectious triggers and novel therapeutic opportunities in childhood B cell leukaemia

Author: European Commission, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, CSIC-UAM - Centro de Biología Molecular Severo Ochoa (CBM), Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Fundación Unoentrecienmil, Josep Carreras Leukemia Foundation, Federal Office for Radiation Protection (Germany), Cobaleda, César, Vicente-Dueñas, Carolina, Sánchez García, Isidro, European Commission, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, CSIC-UAM - Centro de Biología Molecular Severo Ochoa (CBM), Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Fundación Unoentrecienmil, Josep Carreras Leukemia Foundation, Federal Office for Radiation Protection (Germany), Cobaleda, César, Vicente-Dueñas, Carolina, and Sánchez García, Isidro
Abstract: B cell acute lymphoblastic leukaemia (B-ALL) is the most common form of childhood cancer. Although treatment has advanced remarkably in the past 50 years, it still fails in ~20% of patients. Recent studies revealed that more than 5% of healthy newborns carry preleukaemic clones that originate in utero, but only a small percentage of these carriers will progress to overt B-ALL. The drivers of progression are unclear, but B-ALL incidence seems to be increasing in parallel with the adoption of modern lifestyles. Emerging evidence shows that a major driver for the conversion from the preleukaemic state to the B-ALL state is exposure to immune stressors, such as infection. Here, we discuss our current understanding of the environmental triggers and genetic predispositions that may lead to B-ALL, highlighting lessons from epidemiology, the clinic and animal models, and identifying priority areas for future research.
Published: 2021

9. Epigenome-wide association study of COVID-19 severity with respiratory failure

Author: Josep Carreras Leukemia Foundation, Fundació Privada Cellex, Generalitat de Catalunya, Castro de Moura, Manuel, Davalos, Veronica, Planas-Serra, Laura, Álvarez-Errico, Damiana, Arribas, Carles, Ruiz, Montserrat, Aguilera-Albesa, Sergio, Troya, Jesús, Valencia-Ramos, Juan, Vélez-Santamaría, Valentina, Rodríguez-Palmero, Agustí, Villar-García, Judit, Horcajada, Juan Pablo, Albu, Sergiu, Casasnovas, Carlos, Rull, Anna, Reverté, Laia, Dietl, Beatriz, Dalmau, David, Arranz, Maria J., Llucià-Carol, Laia, Planas, Anna M., Pérez-Tur, Jordi, Fernández-Cadenas, Israel, Villares, Paula, Tenorio, Jair, Colobran, Roger, Martin-Nalda, Andrea, Soler-Palacín, Pere, Vidal, Francesc, Pujol, Aurora, Esteller, Manel, Josep Carreras Leukemia Foundation, Fundació Privada Cellex, Generalitat de Catalunya, Castro de Moura, Manuel, Davalos, Veronica, Planas-Serra, Laura, Álvarez-Errico, Damiana, Arribas, Carles, Ruiz, Montserrat, Aguilera-Albesa, Sergio, Troya, Jesús, Valencia-Ramos, Juan, Vélez-Santamaría, Valentina, Rodríguez-Palmero, Agustí, Villar-García, Judit, Horcajada, Juan Pablo, Albu, Sergiu, Casasnovas, Carlos, Rull, Anna, Reverté, Laia, Dietl, Beatriz, Dalmau, David, Arranz, Maria J., Llucià-Carol, Laia, Planas, Anna M., Pérez-Tur, Jordi, Fernández-Cadenas, Israel, Villares, Paula, Tenorio, Jair, Colobran, Roger, Martin-Nalda, Andrea, Soler-Palacín, Pere, Vidal, Francesc, Pujol, Aurora, and Esteller, Manel
Abstract: Background: Patients infected with the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), responsible for the coronavirus disease 2019 (COVID-19), exhibit a wide spectrum of disease behaviour. Since DNA methylation has been implicated in the regulation of viral infections and the immune system, we performed an epigenome-wide association study (EWAS) to identify candidate loci regulated by this epigenetic mark that could be involved in the onset of COVID-19 in patients without comorbidities. Methods: Peripheral blood samples were obtained from 407 confirmed COVID-19 patients 61 years of age and without comorbidities, 194 (47.7%) of whom had mild symptomatology that did not involve hospitalization and 213 (52.3%) had a severe clinical course that required respiratory support. The set of cases was divided into discovery (n = 207) and validation (n = 200) cohorts, balanced for age and sex of individuals. We analysed the DNA methylation status of 850,000 CpG sites in these patients. Findings: The DNA methylation status of 44 CpG sites was associated with the clinical severity of COVID-19. Of these loci, 23 (52.3%) were located in 20 annotated coding genes. These genes, such as the inflammasome component Absent in Melanoma 2 (AIM2) and the Major Histocompatibility Complex, class I C (HLA-C) candidates, were mainly involved in the response of interferon to viral infection. We used the EWAS-identified sites to establish a DNA methylation signature (EPICOVID) that is associated with the severity of the disease. Interpretation: We identified DNA methylation sites as epigenetic susceptibility loci for respiratory failure in COVID-19 patients. These candidate biomarkers, combined with other clinical, cellular and genetic factors, could be useful in the clinical stratification and management of patients infected with the SARS-CoV-2.
Published: 2021

10. Targeting aberrant DNA methylation in mesenchymal stromal cells as a treatment for myeloma bone disease

Author: Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Multiple Myeloma Research Foundation, European Commission, Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, Fundació La Marató de TV3, Associazione Italiana per la Ricerca sul Cancro, Fundación Ramón Areces, García-Gómez, Antonio, Li, Tianlu, Rodríguez-Ubreva, Javier, Ciudad, Laura, Català-Moll, Francesc, Godoy-Tena, Gerard, Martín-Sánchez, Montserrat, San-Segundo, Laura, Muntión, Sandra, Morales, Xabier, Ortiz-de-Solorzano, Carlos, Oyarzabal, Julen, San José-Enériz, Edurne, Esteller, M., Agirre, Xavier, Prósper, Felipe, Garayoa, Mercedes, Ballestar, Esteban, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Multiple Myeloma Research Foundation, European Commission, Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, Fundació La Marató de TV3, Associazione Italiana per la Ricerca sul Cancro, Fundación Ramón Areces, García-Gómez, Antonio, Li, Tianlu, Rodríguez-Ubreva, Javier, Ciudad, Laura, Català-Moll, Francesc, Godoy-Tena, Gerard, Martín-Sánchez, Montserrat, San-Segundo, Laura, Muntión, Sandra, Morales, Xabier, Ortiz-de-Solorzano, Carlos, Oyarzabal, Julen, San José-Enériz, Edurne, Esteller, M., Agirre, Xavier, Prósper, Felipe, Garayoa, Mercedes, and Ballestar, Esteban
Abstract: Multiple myeloma (MM) progression and myeloma-associated bone disease (MBD) are highly dependent on bone marrow mesenchymal stromal cells (MSCs). MM-MSCs exhibit abnormal transcriptomes, suggesting the involvement of epigenetic mechanisms governing their tumor-promoting functions and prolonged osteoblast suppression. Here, we identify widespread DNA methylation alterations of bone marrow-isolated MSCs from distinct MM stages, particularly in Homeobox genes involved in osteogenic differentiation that associate with their aberrant expression. Moreover, these DNA methylation changes are recapitulated in vitro by exposing MSCs from healthy individuals to MM cells. Pharmacological targeting of DNMTs and G9a with dual inhibitor CM-272 reverts the expression of hypermethylated osteogenic regulators and promotes osteoblast differentiation of myeloma MSCs. Most importantly, CM-272 treatment prevents tumor-associated bone loss and reduces tumor burden in a murine myeloma model. Our results demonstrate that epigenetic aberrancies mediate the impairment of bone formation in MM, and its targeting by CM-272 is able to reverse MBD.
Published: 2021

11. Leukemia Stem Cells: Concept and Implications

Author: European Commission, Ministerio de Ciencia, Innovación y Universidades (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, Junta de Castilla y León, Josep Carreras Leukemia Foundation, Federal Office for Radiation Protection (Germany), Fundación Unoentrecienmil, Sánchez García, Isidro, Cobaleda, César, European Commission, Ministerio de Ciencia, Innovación y Universidades (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, Junta de Castilla y León, Josep Carreras Leukemia Foundation, Federal Office for Radiation Protection (Germany), Fundación Unoentrecienmil, Sánchez García, Isidro, and Cobaleda, César
Abstract: Only 10 years ago, the existence of cancer stem cells (CSCs) was still hotly debated. Even today, when their presence in most tumor types has been clearly demonstrated, all the consequences of their existence are far from being realized neither in the clinic nor, very often, in basic and translational cancer research. The existence of CSCs supposes a true change of paradigm in our understanding of cancer, but it will only have a real impact when we will properly assimilate its implications and apply these insights to both cancer research and cancer treatment. In this primer to the topic of leukemia stem cells (LSCs) our aim is to highlight with broad brushstrokes the most relevant of their properties, how these characteristics led to their identification, and the implications that the existence of LSCs has for the research and fight against leukemia.
Published: 2021

12. An immune window of opportunity to prevent childhood B cell leukemia

Author: Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Josep Carreras Leukemia Foundation, Fundación Unoentrecienmil, Federal Office for Radiation Protection (Germany), Cobaleda, César, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Josep Carreras Leukemia Foundation, Fundación Unoentrecienmil, Federal Office for Radiation Protection (Germany), Cobaleda, César, Vicente-Dueñas, Carolina, and Sánchez García, Isidro
Abstract: The prevalence of childhood B cell acute lymphoblastic leukemia (B-ALL) is increasing, particularly in developed countries. There is no clear explanation for this increment, but recent data suggest that, besides genetic predisposition, stress in the immune system (e.g., an infection) might have an important role in B-ALL leukemogenesis. Here, we speculate on how this knowledge might impact B-ALL prevention strategies.
Published: 2021

13. Integrative methylome-transcriptome analysis unravels cancer cell vulnerabilities in infant MLL-rearranged B cell acute lymphoblastic leukemia

Author: Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, European Research Council, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Asociación Española Contra el Cáncer, Fundación Unoentrecienmil, Principado de Asturias, Instituto de Salud Carlos III, Fundación General CSIC, Fundación Leo Messi, Obra Social Cajastur, Liberbank, Tejedor, Juan Ramón, Bueno, Clara, Vinyoles, Meritxell, Petazzi, Paolo, Agraz-Doblas, Antonio, Cobo, Isabel, Torres-Ruiz, Raúl, Bayón, Gustavo F., Pérez, Raúl F., López-Tamargo, Sara, Gutiérrez-Agüera, Francisco, Santamarina-Ojeda, Pablo, Ramírez-Orellana, Manuel, Bardini, Michela, Cazzaniga, Giovanni, Ballerini, Paola, Schneider, Paulina, Stam, Ronald W., Varela, Ignacio, Fraga, Mario F., Fernández, Agustín F., Menéndez, Pablo, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, European Research Council, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Asociación Española Contra el Cáncer, Fundación Unoentrecienmil, Principado de Asturias, Instituto de Salud Carlos III, Fundación General CSIC, Fundación Leo Messi, Obra Social Cajastur, Liberbank, Tejedor, Juan Ramón, Bueno, Clara, Vinyoles, Meritxell, Petazzi, Paolo, Agraz-Doblas, Antonio, Cobo, Isabel, Torres-Ruiz, Raúl, Bayón, Gustavo F., Pérez, Raúl F., López-Tamargo, Sara, Gutiérrez-Agüera, Francisco, Santamarina-Ojeda, Pablo, Ramírez-Orellana, Manuel, Bardini, Michela, Cazzaniga, Giovanni, Ballerini, Paola, Schneider, Paulina, Stam, Ronald W., Varela, Ignacio, Fraga, Mario F., Fernández, Agustín F., and Menéndez, Pablo
Abstract: B cell acute lymphoblastic leukemia (B-ALL) is the most common childhood cancer. As predicted by its prenatal origin, infant B-ALL (iB-ALL) shows an exceptionally silent DNA mutational landscape, suggesting that alternative epigenetic mechanisms may substantially contribute to its leukemogenesis. Here, we have integrated genome-wide DNA methylome and transcriptome data from 69 patients with de novo MLL-rearranged leukemia (MLLr) and non-MLLr iB-ALL leukemia uniformly treated according to the Interfant-99/06 protocol. iB-ALL methylome signatures display a plethora of common and specific alterations associated with chromatin states related to enhancer and transcriptional control in normal hematopoietic cells. DNA methylation, gene expression, and gene coexpression network analyses segregated MLLr away from non-MLLr iB-ALL and identified a coordinated and enriched expression of the AP-1 complex members FOS and JUN and RUNX factors in MLLr iB-ALL, consistent with the significant enrichment of hypomethylated CpGs in these genes. Integrative methylome-transcriptome analysis identified consistent cancer cell vulnerabilities, revealed a robust iB-ALL–specific gene expression–correlating dmCpG signature, and confirmed an epigenetic control of AP-1 and RUNX members in reshaping the molecular network of MLLr iB-ALL. Finally, pharmacological inhibition or functional ablation of AP-1 dramatically impaired MLLr-leukemic growth in vitro and in vivo using MLLr-iB-ALL patient–derived xenografts, providing rationale for new therapeutic avenues in MLLr-iB-ALL.
Published: 2021

14. An intact gut microbiome protects genetically predisposed mice against leukemia

Author: European Commission, Instituto de Salud Carlos III, German Cancer Aid, Josep Carreras Leukemia Foundation, German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Junta de Castilla y León, Heinrich Heine University Düsseldorf, Vicente-Dueñas, Carolina, Janssen, Stefan, Oldenburg, Marina, Auer, Franziska, González-Herrero, Inés, Casado-García, Ana, Isidro‑Hernández, Marta, Raboso-Gallego, Javier, Westhoff, Philipp, Pandyra, Aleksandra A., Hein, Daniel, Gössling, Katharina L., Alonso-López, D., Rivas, Javier de las, Bhatia, Sanil, García-Criado, Francisco Javier, García-Cenador, Begoña, Weber, Andreas P. M., Köhrer, Karl, Hauer, Julia, Fischer, Ute, Sánchez García, Isidro, Borkhardt, Arndt, European Commission, Instituto de Salud Carlos III, German Cancer Aid, Josep Carreras Leukemia Foundation, German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Junta de Castilla y León, Heinrich Heine University Düsseldorf, Vicente-Dueñas, Carolina, Janssen, Stefan, Oldenburg, Marina, Auer, Franziska, González-Herrero, Inés, Casado-García, Ana, Isidro‑Hernández, Marta, Raboso-Gallego, Javier, Westhoff, Philipp, Pandyra, Aleksandra A., Hein, Daniel, Gössling, Katharina L., Alonso-López, D., Rivas, Javier de las, Bhatia, Sanil, García-Criado, Francisco Javier, García-Cenador, Begoña, Weber, Andreas P. M., Köhrer, Karl, Hauer, Julia, Fischer, Ute, Sánchez García, Isidro, and Borkhardt, Arndt
Abstract: The majority of childhood leukemias are precursor B-cell acute lymphoblastic leukemias (pB-ALLs) caused by a combination of prenatal genetic predispositions and oncogenic events occurring after birth. Although genetic predispositions are frequent in children (>1% to 5%), fewer than 1% of genetically predisposed carriers will develop pB-ALL. Although infectious stimuli are believed to play a major role in leukemogenesis, the critical determinants are not well defined. Here, by using murine models of pB-ALL, we show that microbiome disturbances incurred by antibiotic treatment early in life were sufficient to induce leukemia in genetically predisposed mice, even in the absence of infectious stimuli and independent of T cells. By using V4 and full-length 16S ribosomal RNA sequencing of a series of fecal samples, we found that genetic predisposition to pB-ALL (Pax5 heterozygosity or ETV6-RUNX1 fusion) shaped a distinct gut microbiome. Machine learning accurately (96.8%) predicted genetic predisposition using 40 of 3983 amplicon sequence variants as proxies for bacterial species. Transplantation of either wild-type (WT) or Pax5+/– hematopoietic bone marrow cells into WT recipient mice revealed that the microbiome is shaped and determined in a donor genotype–specific manner. Gas chromatography-mass spectrometry (GC-MS) analyses of sera from WT and Pax5+/– mice demonstrated the presence of a genotype-specific distinct metabolomic profile. Taken together, our data indicate that it is a lack of commensal microbiota rather than the presence of specific bacteria that promotes leukemia in genetically predisposed mice. Future large-scale longitudinal studies are required to determine whether targeted microbiome modification in children predisposed to pB-ALL could become a successful prevention strategy.
Published: 2020

15. Inhibition of inflammatory signaling in Pax5 mutant cells mitigates B-cell leukemogenesis

Author: Associazione Italiana per la Ricerca sul Cancro, Fondazione Cariplo, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Josep Carreras Leukemia Foundation, Federal Office for Radiation Protection (Germany), Fundación Unoentrecienmil, Universidad de Salamanca, Isidro‑Hernández, Marta, Mayado, Andrea, Casado-García, Ana, Martínez‑Cano, Jorge, Palmi, Chiara, Fazio, Grazia, Orfao, Alberto, Ribera, Jordi, Ribera, Josep-Maria, Zamora, Lurdes, Raboso-Gallego, Javier, Blanco, Óscar, Alonso-López, D., Rivas, Javier de las, Jiménez, Rafael, García Criado, Francisco Javier, García-Cenador, Begoña, Ramírez‑Orellana, Manuel, Cazzaniga, Giovanni, Cobaleda, César, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Associazione Italiana per la Ricerca sul Cancro, Fondazione Cariplo, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Fundación Ramón Areces, Fundación Síndrome de Wolf-Hirschhorn, Banco Santander, European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Josep Carreras Leukemia Foundation, Federal Office for Radiation Protection (Germany), Fundación Unoentrecienmil, Universidad de Salamanca, Isidro‑Hernández, Marta, Mayado, Andrea, Casado-García, Ana, Martínez‑Cano, Jorge, Palmi, Chiara, Fazio, Grazia, Orfao, Alberto, Ribera, Jordi, Ribera, Josep-Maria, Zamora, Lurdes, Raboso-Gallego, Javier, Blanco, Óscar, Alonso-López, D., Rivas, Javier de las, Jiménez, Rafael, García Criado, Francisco Javier, García-Cenador, Begoña, Ramírez‑Orellana, Manuel, Cazzaniga, Giovanni, Cobaleda, César, Vicente-Dueñas, Carolina, and Sánchez García, Isidro
Abstract: PAX5 is one of the most frequently mutated genes in B-cell acute lymphoblastic leukemia (B-ALL), and children with inherited preleukemic PAX5 mutations are at a higher risk of developing the disease. Abnormal profiles of inflammatory markers have been detected in neonatal blood spot samples of children who later developed B-ALL. However, how inflammatory signals contribute to B-ALL development is unclear. Here, we demonstrate that Pax5 heterozygosis, in the presence of infections, results in the enhanced production of the inflammatory cytokine interleukin-6 (IL-6), which appears to act in an autocrine fashion to promote leukemia growth. Furthermore, in vivo genetic downregulation of IL-6 in these Pax5 heterozygous mice retards B-cell leukemogenesis, and in vivo pharmacologic inhibition of IL-6 with a neutralizing antibody in Pax5 mutant mice with B-ALL clears leukemic cells. Additionally, this novel IL–6 signaling paradigm identified in mice was also substantiated in humans. Altogether, our studies establish aberrant IL6 expression caused by Pax5 loss as a hallmark of Pax5-dependent B-ALL and the IL6 as a therapeutic vulnerability for B-ALL characterized by PAX5 loss.
Published: 2020

16. Bone marrow clonogenic myeloid progenitors from NPM1-mutated AML patients do not harbor the NPM1 mutation: Implication for the cell-of-origin of NPM1+ AML

Author: Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, Ministerio de Economía y Competitividad (España), Fundación Leo Messi, Fundación Banco Santander, Asociación Española Contra el Cáncer, Díaz de la Guardia, Rafael, González-Silva, Laura, López-Millán, Belén, Rodríguez-Sevilla, Juan José, Baroni, Matteo L., Bueno, Clara, Anguita, Eduardo, Vives, Susana, Palomo, Laura, Lapillonne, Helene, Varela, Ignacio, Menéndez, Pablo, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, Ministerio de Economía y Competitividad (España), Fundación Leo Messi, Fundación Banco Santander, Asociación Española Contra el Cáncer, Díaz de la Guardia, Rafael, González-Silva, Laura, López-Millán, Belén, Rodríguez-Sevilla, Juan José, Baroni, Matteo L., Bueno, Clara, Anguita, Eduardo, Vives, Susana, Palomo, Laura, Lapillonne, Helene, Varela, Ignacio, and Menéndez, Pablo
Abstract: The cell-of-origin of NPM1- and FLT3-mutated acute myeloid leukemia (AML) is still a matter of debate. Here, we combined in vitro clonogenic assays with targeted sequencing to gain further insights into the cell-of-origin of NPM1 and FLT3-ITD-mutated AML in diagnostic bone marrow (BM) from nine NPM1+/FLT3-ITD (+/−) AMLs. We reasoned that individually plucked colony forming units (CFUs) are clonal and reflect the progeny of a single stem/progenitor cell. NPM1 and FLT3-ITD mutations seen in the diagnostic blasts were found in only 2/95 and 1/57 individually plucked CFUs, suggesting that BM clonogenic myeloid progenitors in NPM1-mutated and NPM1/FLT3-ITD-mutated AML patients do not harbor such molecular lesions. This supports previous studies on NPM1 mutations as secondary mutations in AML, likely acquired in an expanded pool of committed myeloid progenitors, perhaps CD34−, in line with the CD34−/low phenotype of NPM1-mutated AMLs. This study has important implications on the cell-of-origin of NPM1+ AML, and reinforces that therapeutic targeting of either NPM1 or FLT3-ITD mutations might only have a transient clinical benefit in debulking the leukemia, but is unlikely to be curative since will not target the AML-initiating/preleukemic cells. The absence of NPM1 and FLT3-ITD mutations in normal clonogenic myeloid progenitors is in line with their absence in clonal hematopoiesis of indeterminate potential.
Published: 2020

17. Editorial: Epigenetic reprogramming and cancer development

Author: Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Junta de Castilla y León, European Commission, Josep Carreras Leukemia Foundation, Brown, Geoffrey, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Junta de Castilla y León, European Commission, Josep Carreras Leukemia Foundation, Brown, Geoffrey, Vicente-Dueñas, Carolina, and Sánchez García, Isidro
Published: 2020

18. A pediatric regimen for adolescents and young adults with Philadelphia chromosome‐negative acute lymphoblastic leukemia: Results of the ALLRE08 PETHEMA trial

Author: Josep Carreras Leukemia Foundation, Universidad Autónoma de Barcelona, CSIC-USAL - Instituto de Biología Molecular y Celular del Cancer de Salamanca (IBMCC), Ribera, Josep-Maria, Morgades, Mireia, Montesinos, Pau, Tormo, Mar, Martínez-Carballeira, Daniel, González-Campos, José A., Gil, Cristina, Barba, Pere, García-Boyero, Raimundo, Coll, Rosa, Pedreño, María A., Ribera, Jordi, Mercadal, Santiago, Vives, Susana, Novo, Andrés, Genescà, Eulàlia, Hernández, Jesús M., Bergua, Juan, Amigo, María Luz, Vall‐Llovera, Ferran, Martínez‐Sanchez, Pilar, Calbacho, M., García-Cadenas, Irene, Garcia-Guiñon, Antonio, Sánchez-Sánchez, María-José, Cervera, Marta, Feliu, Evarist, Orfao, Alberto, Josep Carreras Leukemia Foundation, Universidad Autónoma de Barcelona, CSIC-USAL - Instituto de Biología Molecular y Celular del Cancer de Salamanca (IBMCC), Ribera, Josep-Maria, Morgades, Mireia, Montesinos, Pau, Tormo, Mar, Martínez-Carballeira, Daniel, González-Campos, José A., Gil, Cristina, Barba, Pere, García-Boyero, Raimundo, Coll, Rosa, Pedreño, María A., Ribera, Jordi, Mercadal, Santiago, Vives, Susana, Novo, Andrés, Genescà, Eulàlia, Hernández, Jesús M., Bergua, Juan, Amigo, María Luz, Vall‐Llovera, Ferran, Martínez‐Sanchez, Pilar, Calbacho, M., García-Cadenas, Irene, Garcia-Guiñon, Antonio, Sánchez-Sánchez, María-José, Cervera, Marta, Feliu, Evarist, and Orfao, Alberto
Abstract: [Background]: Pediatric‐based or ‐inspired trials have improved the prognosis of adolescents and young adults (AYA) with Philadelphia chromosome‐negative (Ph‐neg) acute lymphoblastic leukemia (ALL)., [Methods]: This study reports the results of treatment of the ALLRE08 trial, a full pediatric trial for AYA aged 15‐30 years with standard‐risk (SR) ALL., [Results]: From 2008 to 2018, 89 patients (38 adolescents [15‐18 years] and 51 young adults [YA, 19‐30 years], median age: 20 [15‐29] years) were enrolled in the ALLRE08 trial. The complete response (CR) was 95%. Twenty‐two patients were transferred to a high‐risk (HR) protocol because of poor marrow response on day 14 (n = 20) or high‐level of end‐induction minimal residual response (MRD ≥ 0.25%, n = 2). Cumulative incidence of relapse (CIR) at 5 years was 35% (95%CI: 23%‐47%), with significant differences between adolescents and YA: 13% (4%‐28%) vs 52% (34%‐67%), P = .012. No treatment‐related mortality was observed in 66/66 patients following the ALLRE08 trial vs 3/23 patients moved to a HR trial. The estimated 5‐year overall survival (OS) was 74% (95%CI: 63%‐85%), with significantly higher rates for adolescents vs YA: 87% (95%CI: 74%‐100%) vs 63% (46%‐80%), P = .021. Although CIR or OS were lower in patients who were transferred to a HR trial, the differences were not statistically significant (CIR: 34% [21%‐47%] vs 37% [14%‐61%]; OS: 78% [66%‐90%] vs 61% [31%;91%])., [Conclusion]: A full pediatric trial is feasible and effective for AYA with Ph‐neg, SR‐ALL, with better results for adolescents than for YA. Outcome of patients with poor early response rescued with a HR trial was not significantly inferior.
Published: 2020

19. Epigenomics and transcriptomics of systemic sclerosis CD4+ T cells reveal long-range dysregulation of key inflammatory pathways mediated by disease-associated susceptibility loci

Author: Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Instituto de Salud Carlos III, European Commission, Li, Tianlu, Ortiz-Fernández, Lourdes, Andrés-León, Eduardo, Ciudad, Laura, Javierre, Biola M., López-Isac, Elena, Guillén del Castillo, Alfredo, Simeón, Carmen P., Ballestar, Estéban, Martín, Javier, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Instituto de Salud Carlos III, European Commission, Li, Tianlu, Ortiz-Fernández, Lourdes, Andrés-León, Eduardo, Ciudad, Laura, Javierre, Biola M., López-Isac, Elena, Guillén del Castillo, Alfredo, Simeón, Carmen P., Ballestar, Estéban, and Martín, Javier
Abstract: [Background]: Systemic sclerosis (SSc) is a genetically complex autoimmune disease mediated by the interplay between genetic and epigenetic factors in a multitude of immune cells, with CD4+ T lymphocytes as one of the principle drivers of pathogenesis., [Methods]: DNA samples exacted from CD4+ T cells of 48 SSc patients and 16 healthy controls were hybridized on MethylationEPIC BeadChip array. In parallel, gene expression was interrogated by hybridizing total RNA on Clariom™ S array. Downstream bioinformatics analyses were performed to identify correlating differentially methylated CpG positions (DMPs) and differentially expressed genes (DEGs), which were then confirmed utilizing previously published promoter capture Hi-C (PCHi-C) data., [Results]: We identified 9112 and 3929 DMPs and DEGs, respectively. These DMPs and DEGs are enriched in functional categories related to inflammation and T cell biology. Furthermore, correlation analysis identified 17,500 possible DMP-DEG interaction pairs within a window of 5 Mb, and utilizing PCHi-C data, we observed that 212 CD4+ T cell-specific pairs of DMP-DEG also formed part of three-dimensional promoter-enhancer networks, potentially involving CTCF. Finally, combining PCHi-C data with SSc GWAS data, we identified four important SSc-associated susceptibility loci, TNIP1 (rs3792783), GSDMB (rs9303277), IL12RB1 (rs2305743), and CSK (rs1378942), that could potentially interact with DMP-DEG pairs cg17239269-ANXA6, cg19458020-CCR7, cg10808810-JUND, and cg11062629-ULK3, respectively., [Conclusion]: Our study unveils a potential link between genetic, epigenetic, and transcriptional deregulation in CD4+ T cells of SSc patients, providing a novel integrated view of molecular components driving SSc pathogenesis.
Published: 2020

20. Infectious stimuli promote malignant B-cell acute lymphoblastic leukemia in the absence of AID

Author: Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), European Commission, German Cancer Aid, Josep Carreras Leukemia Foundation, European Research Council, Asociación Española Contra el Cáncer, Centro Nacional de Investigaciones Oncológicas (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), Junta de Castilla y León, Rodríguez-Hernández, Guillermo, Opitz, Friederike V., Delgado, Pilar, Walter, Carolin, Álvarez-Prado, Angel Francisco, González-Herrero, Inés, Auer, Franziska, Fischer, Ute, Janssen, Stefan, Bartenhagen, Christoph, Raboso-Gallego, Javier, Casado-García, Ana, Orfao, Alberto, Blanco, Óscar, Alonso-López, D., Rivas, Javier de las, González de Tena-Dávila, Sara, Müschen, Markus, Dugas, Martin, García-Criado, Francisco Javier, García-Cenador, Begoña, Vicente-Dueñas, Carolina, Hauer, Julia, Ramiro, Almudena R., Sánchez García, Isidro, Borkhardt, Arndt, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), European Commission, German Cancer Aid, Josep Carreras Leukemia Foundation, European Research Council, Asociación Española Contra el Cáncer, Centro Nacional de Investigaciones Oncológicas (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), Junta de Castilla y León, Rodríguez-Hernández, Guillermo, Opitz, Friederike V., Delgado, Pilar, Walter, Carolin, Álvarez-Prado, Angel Francisco, González-Herrero, Inés, Auer, Franziska, Fischer, Ute, Janssen, Stefan, Bartenhagen, Christoph, Raboso-Gallego, Javier, Casado-García, Ana, Orfao, Alberto, Blanco, Óscar, Alonso-López, D., Rivas, Javier de las, González de Tena-Dávila, Sara, Müschen, Markus, Dugas, Martin, García-Criado, Francisco Javier, García-Cenador, Begoña, Vicente-Dueñas, Carolina, Hauer, Julia, Ramiro, Almudena R., Sánchez García, Isidro, and Borkhardt, Arndt
Abstract: The prerequisite to prevent childhood B-cell acute lymphoblastic leukemia (B-ALL) is to decipher its etiology. The current model suggests that infection triggers B-ALL development through induction of activation-induced cytidine deaminase (AID; also known as AICDA) in precursor B-cells. This evidence has been largely acquired through the use of ex vivo functional studies. However, whether this mechanism governs native non-transplant B-ALL development is unknown. Here we show that, surprisingly, AID genetic deletion does not affect B-ALL development in Pax5-haploinsufficient mice prone to B-ALL upon natural infection exposure. We next test the effect of premature AID expression from earliest pro-B-cell stages in B-cell transformation. The generation of AID off-target mutagenic activity in precursor B-cells does not promote B-ALL. Likewise, known drivers of human B-ALL are not preferentially targeted by AID. Overall these results suggest that infections promote B-ALL through AID-independent mechanisms, providing evidence for a new model of childhood B-ALL development.
Published: 2019

21. Chromatin regulation by Histone H4 acetylation at Lysine 16 during cell death and differentiation in the myeloid compartment

Author: European Commission, Instituto de Salud Carlos III, Fundación Científica Asociación Española Contra el Cáncer, Ministerio de Economía y Competitividad (España), Fundación Ramón Areces, Principado de Asturias, German Research Foundation, European Research Council, Asociación Española Contra el Cáncer, Fundación Fero, Fundación la Caixa, Josep Carreras Leukemia Foundation, Generalitat de Catalunya, Obra Social Cajastur, Urdinguio, Rocío G., López, Virginia, Bayón, Gustavo F., Díaz de la Guardia, Rafael, Sierra, Marta I., García-Toraño, Estela, Pérez, Raúl F., García, María G., Carella, Antonella, Pruneda, Patricia C., Prieto López, Cristina, Dmitrijeva, Marija, Santamarina-Ojeda, Pablo, Belmonte, Thalia, Mangas, Cristina, Diaconu, Elena, Ferrero, Cecilia, Tejedor, Juan Ramón, Fernández-Morera, Juan L., Bravo, Cristina, Bueno, Clara, Sanjuan-Pla, Alejandra, Rodríguez López, Ramón María, Suárez-Álvarez, Beatriz, López-Larrea, Carlos, Bernal, Teresa, Colado, Enrique, Balbín, Milagros, García-Suarez, Olivia, Chiara, María-Dolores, Sáenz-de-Santa-María, Inés, Rodríguez Hernández, Francisco José, Pando-Sandoval, Ana, Rodrigo, Luis, Santos, Laura, Salas, Ana, Vallejo-Díaz, Jesús, Carrera, Ana C., Rico, Daniel, Hernández-López, Inmaculada, Vayá, Amparo, Ricart, José M., Seto, Edward, Sima-Teruel, Núria, Vaquero, Alejandro, Valledor, Luis, Cañal, María Jesús, Pisano, David, Graña-Castro, Osvaldo, Thomas, Tim, Voss, Anne K., Menéndez, Pablo, Villar-Garea, Ana, Deutzmann, Rainer, Fernández, Agustín F., Fraga, Mario F., European Commission, Instituto de Salud Carlos III, Fundación Científica Asociación Española Contra el Cáncer, Ministerio de Economía y Competitividad (España), Fundación Ramón Areces, Principado de Asturias, German Research Foundation, European Research Council, Asociación Española Contra el Cáncer, Fundación Fero, Fundación la Caixa, Josep Carreras Leukemia Foundation, Generalitat de Catalunya, Obra Social Cajastur, Urdinguio, Rocío G., López, Virginia, Bayón, Gustavo F., Díaz de la Guardia, Rafael, Sierra, Marta I., García-Toraño, Estela, Pérez, Raúl F., García, María G., Carella, Antonella, Pruneda, Patricia C., Prieto López, Cristina, Dmitrijeva, Marija, Santamarina-Ojeda, Pablo, Belmonte, Thalia, Mangas, Cristina, Diaconu, Elena, Ferrero, Cecilia, Tejedor, Juan Ramón, Fernández-Morera, Juan L., Bravo, Cristina, Bueno, Clara, Sanjuan-Pla, Alejandra, Rodríguez López, Ramón María, Suárez-Álvarez, Beatriz, López-Larrea, Carlos, Bernal, Teresa, Colado, Enrique, Balbín, Milagros, García-Suarez, Olivia, Chiara, María-Dolores, Sáenz-de-Santa-María, Inés, Rodríguez Hernández, Francisco José, Pando-Sandoval, Ana, Rodrigo, Luis, Santos, Laura, Salas, Ana, Vallejo-Díaz, Jesús, Carrera, Ana C., Rico, Daniel, Hernández-López, Inmaculada, Vayá, Amparo, Ricart, José M., Seto, Edward, Sima-Teruel, Núria, Vaquero, Alejandro, Valledor, Luis, Cañal, María Jesús, Pisano, David, Graña-Castro, Osvaldo, Thomas, Tim, Voss, Anne K., Menéndez, Pablo, Villar-Garea, Ana, Deutzmann, Rainer, Fernández, Agustín F., and Fraga, Mario F.
Abstract: Histone H4 acetylation at Lysine 16 (H4K16ac) is a key epigenetic mark involved in gene regulation, DNA repair and chromatin remodeling, and though it is known to be essential for embryonic development, its role during adult life is still poorly understood. Here we show that this lysine is massively hyperacetylated in peripheral neutrophils. Genome-wide mapping of H4K16ac in terminally differentiated blood cells, along with functional experiments, supported a role for this histone post-translational modification in the regulation of cell differentiation and apoptosis in the hematopoietic system. Furthermore, in neutrophils, H4K16ac was enriched at specific DNA repeats. These DNA regions presented an accessible chromatin conformation and were associated with the cleavage sites that generate the 50 kb DNA fragments during the first stages of programmed cell death. Our results thus suggest that H4K16ac plays a dual role in myeloid cells as it not only regulates differentiation and apoptosis, but it also exhibits a non-canonical structural role in poising chromatin for cleavage at an early stage of neutrophil cell death.
Published: 2019

22. Increased survival due to lower toxicity for high-risk T-cell acute lymphoblastic leukemia patients in two consecutive pediatric-inspired PETHEMA trials

Author: Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, Instituto de Salud Carlos III, Barba, Pere, Morgades, Mireia, Montesinos, Pau, Gil, Cristina, Fox, María‐Laura, Ciudad, Juana, Moreno, María José, González‐Campos, José, Genescà, Eulàlia, Martínez‐Carballeira, Daniel, Martino, Rodrigo, Vives, Susana, Guàrdia, Ramón, Mercadal, Santiago, Artola, María Teresa, Cladera, Antonia, Tormo, Mar, Esteve, Jordi, Bergua, Juan, Vall‐Llovera, Ferran, Ribera, Jordi, Martínez‐Sanchez, Pilar, Amigo, María Luz, Bermúdez, Arantxa, Calbacho, M., Hernández, Jesús M., Feliu, Evarist, Orfao, Alberto, Ribera, Josep-Maria, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, Instituto de Salud Carlos III, Barba, Pere, Morgades, Mireia, Montesinos, Pau, Gil, Cristina, Fox, María‐Laura, Ciudad, Juana, Moreno, María José, González‐Campos, José, Genescà, Eulàlia, Martínez‐Carballeira, Daniel, Martino, Rodrigo, Vives, Susana, Guàrdia, Ramón, Mercadal, Santiago, Artola, María Teresa, Cladera, Antonia, Tormo, Mar, Esteve, Jordi, Bergua, Juan, Vall‐Llovera, Ferran, Ribera, Jordi, Martínez‐Sanchez, Pilar, Amigo, María Luz, Bermúdez, Arantxa, Calbacho, M., Hernández, Jesús M., Feliu, Evarist, Orfao, Alberto, and Ribera, Josep-Maria
Abstract: [Objective and methods]: Pediatric‐inspired regimens have been adopted by several groups as the treatment strategy for adult patients with acute lymphoblastic leukemia (ALL). Whether subsequent modifications of these protocols have led to an improvement in the outcome of patients is uncertain, especially in T‐cell ALL. We analyzed 169 patients with high‐risk T‐cell ALL included in two consecutive trials of the PETHEMA Group (HR‐ALL03 [n = 104] and the more contemporary HR‐ALL11 [n = 65]). [Results]: Patients and disease characteristics were balanced between both groups. Regarding efficacy, we observed a similar complete remission (CR) rate, relapse and disease‐free survival (DFS) between both protocols. Patients included in the HR‐ALL11 trial had better 2‐year overall survival (OS) compared with the HR‐ALL03 (65% [95% CI 51%‐79%] vs 44% [95% CI 34%‐54%], P = 0.026). Regarding toxicity, we observed a better safety profile in the HR‐11 protocol. Irrespective of the protocol, patients with good measurable residual disease (MRD) clearance had a promising outcome without allogeneic hematopoietic stem cell transplantation (allo‐HSCT) in CR1, with 2‐year OS of 67%. [Conclusion]: Patients with T‐cell ALL included in the HR‐11 trial showed better OS than patients in the HR‐03, mostly driven by a reduction of NRM.
Published: 2019

23. Molecular profiling refines minimal residual disease-based prognostic assessment in adults with Philadelphia chromosome-negative B-cell precursor acute lymphoblastic leukemia

Author: Josep Carreras Leukemia Foundation, Generalitat de Catalunya, Instituto de Salud Carlos III, European Commission, Fundación la Caixa, Sociedad Española de Hematología y Hemoterapia, Ribera, Jordi, Zamora, Lurdes, Morgades, Mireia, Vives, Susana, Granada, Isabel, Montesinos, Pau, Gómez‐Seguí, Inés, Mercadal, Santiago, Guàrdia, Ramón, Nomdedéu, Josep F., Pratcorona, Marta, Tormo, Mar, Martínez‐Lopez, Joaquín, Hernández, Jesús M., Ciudad, Juana, Orfao, Alberto, González‐Campos, José, Barba, Pere, Escoda, Lourdes, Esteve, Jordi, Genescà, Eulàlia, Solé, Francesc, Feliu, Evarist, Ribera, Josep-Maria, Josep Carreras Leukemia Foundation, Generalitat de Catalunya, Instituto de Salud Carlos III, European Commission, Fundación la Caixa, Sociedad Española de Hematología y Hemoterapia, Ribera, Jordi, Zamora, Lurdes, Morgades, Mireia, Vives, Susana, Granada, Isabel, Montesinos, Pau, Gómez‐Seguí, Inés, Mercadal, Santiago, Guàrdia, Ramón, Nomdedéu, Josep F., Pratcorona, Marta, Tormo, Mar, Martínez‐Lopez, Joaquín, Hernández, Jesús M., Ciudad, Juana, Orfao, Alberto, González‐Campos, José, Barba, Pere, Escoda, Lourdes, Esteve, Jordi, Genescà, Eulàlia, Solé, Francesc, Feliu, Evarist, and Ribera, Josep-Maria
Abstract: Minimal residual disease (MRD) assessment is an essential tool in contemporary acute lymphoblastic leukemia (ALL) protocols, being used for therapeutic decisions such as hematopoietic stem cell transplantation in high‐risk patients. However, a significant proportion of adult ALL patients with negative MRD still relapse suggesting that other factors (ie, molecular alterations) must be considered in order to identify those patients with high risk of disease progression. We have identified partial IKZF1 gene deletions and CDKN2A/B deletions as markers of disease recurrence and poor survival in a series of uniformly treated adolescent and adult Philadelphia chromosome‐negative B‐cell progenitor ALL patients treated according to the Programa Español de Tratamientos en Hematología protocols. Importantly, CDKN2A/B deletions showed independent significance of MRD at the end of induction, which points out the need for treatment intensification in these patients despite being MRD‐negative after induction therapy.
Published: 2019

24. Fratricide-resistant CD1a-specific CAR T cells for the treatment of cortical T-cell acute lymphoblastic leukemia

Author: European Research Council, Agencia Estatal de Investigación (España), Ministerio de Economía y Competitividad (España), Generalitat de Catalunya, Asociación Española Contra el Cáncer, Instituto de Salud Carlos III, European Commission, Fundación la Caixa, Josep Carreras Leukemia Foundation, Sánchez-Martínez, Diego, Baroni, Matteo L., Gutierrez-Agüera, Francisco, Roca-Ho, Heleia, Blanch-Lombarte, Oscar, González-García, Sara, Torrebadell, Montserrat, Junca, Jordi, Ramírez-Orellana, Manuel, Velasco-Hernández, Talía, Bueno, Clara, Fuster, José Luís, Prado, Julia G., Calvo, Julien, Uzan, Benjamin, Cools, Jan, Camos, Mireia, Pflumio, Françoise, Toribio, María Luisa, Menéndez, Pablo, European Research Council, Agencia Estatal de Investigación (España), Ministerio de Economía y Competitividad (España), Generalitat de Catalunya, Asociación Española Contra el Cáncer, Instituto de Salud Carlos III, European Commission, Fundación la Caixa, Josep Carreras Leukemia Foundation, Sánchez-Martínez, Diego, Baroni, Matteo L., Gutierrez-Agüera, Francisco, Roca-Ho, Heleia, Blanch-Lombarte, Oscar, González-García, Sara, Torrebadell, Montserrat, Junca, Jordi, Ramírez-Orellana, Manuel, Velasco-Hernández, Talía, Bueno, Clara, Fuster, José Luís, Prado, Julia G., Calvo, Julien, Uzan, Benjamin, Cools, Jan, Camos, Mireia, Pflumio, Françoise, Toribio, María Luisa, and Menéndez, Pablo
Abstract: Relapsed/refractory T-cell acute lymphoblastic leukemia (T-ALL) has a dismal outcome, and no effective targeted immunotherapies for T-ALL exist. The extension of chimeric antigen receptor (CAR) T cells (CARTs) to T-ALL remains challenging because the shared expression of target antigens between CARTs and T-ALL blasts leads to CART fratricide. CD1a is exclusively expressed in cortical T-ALL (coT-ALL), a major subset of T-ALL, and retained at relapse. This article reports that the expression of CD1a is mainly restricted to developing cortical thymocytes, and neither CD34+ progenitors nor T cells express CD1a during ontogeny, confining the risk of on-target/off-tumor toxicity. We thus developed and preclinically validated a CD1a-specific CAR with robust and specific cytotoxicity in vitro and antileukemic activity in vivo in xenograft models of coT-ALL, using both cell lines and coT-ALL patient–derived primary blasts. CD1a-CARTs are fratricide resistant, persist long term in vivo (retaining antileukemic activity in re-challenge experiments), and respond to viral antigens. Our data support the therapeutic and safe use of fratricide-resistant CD1a-CARTs for relapsed/refractory coT-ALL.
Published: 2019

25. The making of leukemia

Author: European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Lady Tata Memorial Trust, Junta de Castilla y León, Josep Carreras Leukemia Foundation, González-Herrero, Inés, Rodríguez-Hernández, Guillermo, Luengas-Martínez, Andrea, Isidro‑Hernández, Marta, Jiménez, Rafael, García-Cenador, Begoña, García-Criado, Francisco Javier, Sánchez García, Isidro, Vicente-Dueñas, Carolina, European Commission, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Lady Tata Memorial Trust, Junta de Castilla y León, Josep Carreras Leukemia Foundation, González-Herrero, Inés, Rodríguez-Hernández, Guillermo, Luengas-Martínez, Andrea, Isidro‑Hernández, Marta, Jiménez, Rafael, García-Cenador, Begoña, García-Criado, Francisco Javier, Sánchez García, Isidro, and Vicente-Dueñas, Carolina
Abstract: Due to the clonal nature of human leukemia evolution, all leukemic cells carry the same leukemia-initiating genetic lesions, independently of the intrinsic tumoral cellular heterogeneity. However, the latest findings have shown that the mode of action of oncogenes is not homogeneous throughout the developmental history of leukemia. Studies on different types of hematopoietic tumors have shown that the contribution of oncogenes to leukemia is mainly mediated through the epigenetic reprogramming of the leukemia-initiating target cell. This driving of cancer by a malignant epigenetic stem cell rewiring is, however, not exclusive of the hematopoietic system, but rather represents a common tumoral mechanism that is also at work in epithelial tumors. Tumoral epigenetic reprogramming is therefore a new type of interaction between genes and their target cells, in which the action of the oncogene modifies the epigenome to prime leukemia development by establishing a new pathological tumoral cellular identity. This reprogramming may remain latent until it is triggered by either endogenous or environmental stimuli. This new view on the making of leukemia not only reveals a novel function for oncogenes, but also provides evidence for a previously unconsidered model of leukemogenesis, in which the programming of the leukemia cellular identity has already occurred at the level of stem cells, therefore showing a role for oncogenes in the timing of leukemia initiation
Published: 2018

26. T-cell leukemogenesis is an inappropriate lineage decision-making process: implications for precision oncology

Author: German Cancer Aid, Josep Carreras Leukemia Foundation, German Childhood Cancer Foundation, European Commission, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Instituto de Salud Carlos III, Lady Tata Memorial Trust, Rodríguez-Hernández, Guillermo, Bhatia, Sanil, Vicente-Dueñas, Carolina, Borkhardt, Arndt, Hauer, Julia, Sánchez García, Isidro, German Cancer Aid, Josep Carreras Leukemia Foundation, German Childhood Cancer Foundation, European Commission, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Instituto de Salud Carlos III, Lady Tata Memorial Trust, Rodríguez-Hernández, Guillermo, Bhatia, Sanil, Vicente-Dueñas, Carolina, Borkhardt, Arndt, Hauer, Julia, and Sánchez García, Isidro
Abstract: Genetic lineage tracing in cell type-specific mouse models of T-cell acute lymphoblastic leukemia (T-ALL) have revealed that tumor cell identity is imposed by expression of the oncogene Lim Domain Only 2 (LMO2), rather than by the target cell phenotype. This approach allowed to identify that secondary genomic alterations, like Notch1 mutations, appeared late and only took place within the thymus during T-ALL development. These concepts are therefore critical for the development of modern therapies aimed at curing T-ALL.
Published: 2018

27. Lmo2 expression defines tumor cell identity during T-cell leukemogenesis

Author: Josep Carreras Leukemia Foundation, University of Applied Sciences Bonn-Rhein-Sieg, German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), European Commission, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Inocente Inocente, García-Ramírez, Idoia, Bhatia, Sanil, Rodríguez-Hernández, Guillermo, González-Herrero, Inés, Walter, Carolin, González de Tena-Dávila, Sara, Parvin, Salma, Haas, Oskar, Woessmann, Wilhelm, Stanulla, Martin, Schrappe, Martin, Dugas, Martin, Natkunam, Yasodha, Orfao, Alberto, Domínguez, Verónica, Pintado, Belén, Blanco, Óscar, Alonso-López, D., Rivas, Javier de las, Martín-Lorenzo, Alberto, Jiménez, Rafael, García-Criado, Francisco Javier, García-Cenador, Begoña, Lossos, Izidore S., Vicente-Dueñas, Carolina, Borkhardt, Arndt, Hauer, Julia, Sánchez García, Isidro, Josep Carreras Leukemia Foundation, University of Applied Sciences Bonn-Rhein-Sieg, German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), European Commission, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Inocente Inocente, García-Ramírez, Idoia, Bhatia, Sanil, Rodríguez-Hernández, Guillermo, González-Herrero, Inés, Walter, Carolin, González de Tena-Dávila, Sara, Parvin, Salma, Haas, Oskar, Woessmann, Wilhelm, Stanulla, Martin, Schrappe, Martin, Dugas, Martin, Natkunam, Yasodha, Orfao, Alberto, Domínguez, Verónica, Pintado, Belén, Blanco, Óscar, Alonso-López, D., Rivas, Javier de las, Martín-Lorenzo, Alberto, Jiménez, Rafael, García-Criado, Francisco Javier, García-Cenador, Begoña, Lossos, Izidore S., Vicente-Dueñas, Carolina, Borkhardt, Arndt, Hauer, Julia, and Sánchez García, Isidro
Abstract: The impact of LMO2 expression on cell lineage decisions during T-cell leukemogenesis remains largely elusive. Using genetic lineage tracing, we have explored the potential of LMO2 in dictating a T-cell malignant phenotype. We first initiated LMO2 expression in hematopoietic stem/progenitor cells and maintained its expression in all hematopoietic cells. These mice develop exclusively aggressive human-like T-ALL. In order to uncover a potential exclusive reprogramming effect of LMO2 in murine hematopoietic stem/progenitor cells, we next showed that transient LMO2 expression is sufficient for oncogenic function and induction of T-ALL. The resulting T-ALLs lacked LMO2 and its target-gene expression, and histologically, transcriptionally, and genetically similar to human LMO2-driven T-ALL. We next found that during T-ALL development, secondary genomic alterations take place within the thymus. However, the permissiveness for development of T-ALL seems to be associated with wider windows of differentiation than previously appreciated. Restricted Cre-mediated activation of Lmo2 at different stages of B-cell development induces systematically and unexpectedly T-ALL that closely resembled those of their natural counterparts. Together, these results provide a novel paradigm for the generation of tumor T cells through reprogramming in vivo and could be relevant to improve the response of T-ALL to current therapies.
Published: 2018

28. Loss of Pax5 exploits sca1-BCR-ABLp190 susceptibility to confer the metabolic shift essential for pB-ALL

Author: German Cancer Aid, Josep Carreras Leukemia Foundation, National Institutes of Health (US), Wellcome Trust, German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), Junta de Castilla y León, Fundación Inocente Inocente, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, German Research Foundation, Martín-Lorenzo, Alberto, Auer, Franziska, Chan, Lai N., García-Ramírez, Idoia, González-Herrero, Inés, Rodríguez-Hernández, Guillermo, Bartenhagen, Christoph, Dugas, Martin, Gombert, Michael, Ginzel, Sebastian, Blanco, Óscar, Orfao, Alberto, Alonso-López, D., Rivas, Javier de las, García-Cenador, Begoña, García-Criado, Francisco Javier, Müschen, Markus, Sánchez García, Isidro, Borkhardt, Arndt, Vicente-Dueñas, Carolina, Hauer, Julia, German Cancer Aid, Josep Carreras Leukemia Foundation, National Institutes of Health (US), Wellcome Trust, German Childhood Cancer Foundation, Federal Ministry of Education and Research (Germany), Junta de Castilla y León, Fundación Inocente Inocente, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, German Research Foundation, Martín-Lorenzo, Alberto, Auer, Franziska, Chan, Lai N., García-Ramírez, Idoia, González-Herrero, Inés, Rodríguez-Hernández, Guillermo, Bartenhagen, Christoph, Dugas, Martin, Gombert, Michael, Ginzel, Sebastian, Blanco, Óscar, Orfao, Alberto, Alonso-López, D., Rivas, Javier de las, García-Cenador, Begoña, García-Criado, Francisco Javier, Müschen, Markus, Sánchez García, Isidro, Borkhardt, Arndt, Vicente-Dueñas, Carolina, and Hauer, Julia
Abstract: Preleukemic clones carrying BCR-ABLp190 oncogenic lesions are found in neonatal cord blood, where the majority of preleukemic carriers do not convert into precursor B-cell acute lymphoblastic leukemia (pB-ALL). However, the critical question of how these preleukemic cells transform into pB-ALL remains undefined. Here, we model a BCR-ABLp190 preleukemic state and show that limiting BCR-ABLp190 expression to hematopoietic stem/progenitor cells (HS/PC) in mice (Sca1-BCR-ABLp190) causes pB-ALL at low penetrance, which resembles the human disease. pB-ALL blast cells were BCR-ABL–negative and transcriptionally similar to pro-B/pre-B cells, suggesting disease onset upon reduced Pax5 functionality. Consistent with this, double Sca1-BCR-ABLp190+Pax5+/− mice developed pB-ALL with shorter latencies, 90% incidence, and accumulation of genomic alterations in the remaining wild-type Pax5 allele. Mechanistically, the Pax5-deficient leukemic pro-B cells exhibited a metabolic switch toward increased glucose utilization and energy metabolism. Transcriptome analysis revealed that metabolic genes (IDH1, G6PC3, GAPDH, PGK1, MYC, ENO1, ACO1) were upregulated in Pax5-deficient leukemic cells, and a similar metabolic signature could be observed in human leukemia. Our studies unveil the first in vivo evidence that the combination between Sca1-BCR-ABLp190 and metabolic reprogramming imposed by reduced Pax5 expression is sufficient for pB-ALL development. These findings might help to prevent conversion of BCR-ABLp190 preleukemic cells.
Published: 2018

29. Focal adhesion genes refine the intermediate-risk cytogenetic classification of acute myeloid leukemia

Author: Instituto de Salud Carlos III, European Commission, Fundació La Marató de TV3, Josep Carreras Leukemia Foundation, Asociación Española Contra el Cáncer, Generalitat de Catalunya, Sociedad Española de Hematología y Hemoterapia, Pallarès, Victor, Hoyos, Montserrat, Chillón, M. del Carmen, Barragán, Eva, Prieto-Conde, Isabel, Llop, Marta, Falgàs, Aïda, Céspedes, María Virtudes, Montesinos, Pau, Nomdedéu, Josep F., Brunet, Salut, Sanz, Miguel Ángel, González, Marcos, Sierra, Jorge, Mangues, Ramon, Casanova, Isolda, Instituto de Salud Carlos III, European Commission, Fundació La Marató de TV3, Josep Carreras Leukemia Foundation, Asociación Española Contra el Cáncer, Generalitat de Catalunya, Sociedad Española de Hematología y Hemoterapia, Pallarès, Victor, Hoyos, Montserrat, Chillón, M. del Carmen, Barragán, Eva, Prieto-Conde, Isabel, Llop, Marta, Falgàs, Aïda, Céspedes, María Virtudes, Montesinos, Pau, Nomdedéu, Josep F., Brunet, Salut, Sanz, Miguel Ángel, González, Marcos, Sierra, Jorge, Mangues, Ramon, and Casanova, Isolda
Abstract: In recent years, several attempts have been made to identify novel prognostic markers in patients with intermediate-risk acute myeloid leukemia (IR-AML), to implement risk-adapted strategies. The non-receptor tyrosine kinases are proteins involved in regulation of cell growth, adhesion, migration and apoptosis. They associate with metastatic dissemination in solid tumors and poor prognosis. However, their role in haematological malignancies has been scarcely studied. We hypothesized that PTK2/FAK, PTK2B/PYK2, LYN or SRC could be new prognostic markers in IR-AML. We assessed PTK2, PTK2B, LYN and SRC gene expression in a cohort of 324 patients, adults up to the age of 70, classified in the IR-AML cytogenetic group. Univariate and multivariate analyses showed that PTK2B, LYN and PTK2 gene expression are independent prognostic factors in IR-AML patients. PTK2B and LYN identify a patient subgroup with good prognosis within the cohort with non-favorable FLT3/NPM1 combined mutations. In contrast, PTK2 identifies a patient subgroup with poor prognosis within the worst prognosis cohort who display non-favorable FLT3/NPM1 combined mutations and underexpression of PTK2B or LYN. The combined use of these markers can refine the highly heterogeneous intermediate-risk subgroup of AML patients, and allow the development of risk-adapted post-remission chemotherapy protocols to improve their response to treatment.Pallarès, Victor
Published: 2018

30. CXCR7 expression in diffuse large B-cell lymphoma identifies a subgroup of CXCR4+ patients with good prognosis

Author: Instituto de Salud Carlos III, Centro de Investigación Biomédica en Red Cáncer (España), Generalitat de Catalunya, Fundació La Marató de TV3, Josep Carreras Leukemia Foundation, Junta de Castilla y León, Moreno, María José, Gallardo, Alberto, Novelli, Silvana, Mozos, Ana, Aragó, Marc, Pavón, Miguel A., Céspedes, María Virtudes, Pallarès, Victor, Falgàs, Aïda, Alcoceba, Miguel, Blanco, Óscar, Sierra, Jorge, Mangues, Ramon, Casanova, Isolda, Instituto de Salud Carlos III, Centro de Investigación Biomédica en Red Cáncer (España), Generalitat de Catalunya, Fundació La Marató de TV3, Josep Carreras Leukemia Foundation, Junta de Castilla y León, Moreno, María José, Gallardo, Alberto, Novelli, Silvana, Mozos, Ana, Aragó, Marc, Pavón, Miguel A., Céspedes, María Virtudes, Pallarès, Victor, Falgàs, Aïda, Alcoceba, Miguel, Blanco, Óscar, Sierra, Jorge, Mangues, Ramon, and Casanova, Isolda
Abstract: The CXCR4/CXCL12 axis has been extensively associated with different types of cancer correlating with higher aggressiveness and metastasis. In diffuse large B-cell lymphoma (DLBCL), the expression of the chemokine receptor CXCR4 is involved in the dissemination of malignant B cells and is a marker of poor prognosis. CXCR7 is a chemokine receptor that binds to the same ligand as CXCR4 and regulates de CXCR4-CXCL12 axis. These findings together with the report of CXCR7 prognostic value in several tumor types, led us to evaluate the expression of CXCR7 in diffuse large B-cell lymphoma biopsies. Here, we describe that CXCR7 receptor is an independent prognostic factor that associates with good clinical outcome. Moreover, the expression of CXCR7 associates with increased survival in CXCR4+ but not in CXCR4- DLBCL patients. Thus, the combined immunohistochemical evaluation of both CXCR7 and CXCR4 expression in DLBCL biopsies may improve their prognostic value as single markers. Finally, we show that CXCR7 overexpression in vitro is able to diminish DLBCL cell survival and increase their sensitivity to antitumor drugs. Hence, further studies on the CXCR7 receptor may establish its role in DLBCL and the molecular mechanisms that modulate CXCR4 activity.
Published: 2018

31. Lineage choice decisions in B-cell development and leukemia

Author: Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, European Commission, Josep Carreras Leukemia Foundation, Raboso-Gallego, Javier, Casado-García, Ana, Rodríguez-Hernández, Guillermo, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, European Commission, Josep Carreras Leukemia Foundation, Raboso-Gallego, Javier, Casado-García, Ana, Rodríguez-Hernández, Guillermo, Vicente-Dueñas, Carolina, and Sánchez García, Isidro
Abstract: Every tissue in the body is founded by a particular type of cell that is termed stem cell. These cells are generally presumed to be tissue-specific and, as such, are also responsible for maintenance of the tissue throughout the lifespan of an organism. There are two fundamental aspects to the regular behaviour of tissues during their genesis and thereafter. The offspring of stem cells divide in a manner that is controlled to the social benefit of the organism to generate/ensure the bulk of tissue that is required. These dividing cells mature: they acquire individual characteristics to enable them to perform a unique function within the tissue. Within cancer cells aspects of this normal physiology are distorted. This means the many strands to understanding of the behaviour of normal cells cannot be loosened from the strands of efforts to unravel what goes wrong in cancer.
Published: 2018

32. Phosphorylation of SOS1 on tyrosine 1196 promotes its RAC GEF activity and contributes to BCR-ABL leukemogenesis

Author: Asociación Española Contra el Cáncer, Ministry of Science, Research and Art Baden-Württemberg, European Commission, European Research Council, Josep Carreras Leukemia Foundation, Associazione Italiana per la Ricerca sul Cancro, Fondazione Cariplo, Association for International Cancer Research, Ministero dell'Istruzione, dell'Università e della Ricerca, Gerboth, S., Frittoli, E., Palamidessi, A., Baltanás, Fernando C., Salek, M., Rappsilber, J., Giuliani, C., Troglio, F., Rolland, Y., Pruneri, G., Kreutmair, S., Pallavicini, I., Zobel, M., Cinquanta, M., Minucci, S., Gómez, Carmela, Illert, A.L., Scita, G., Asociación Española Contra el Cáncer, Ministry of Science, Research and Art Baden-Württemberg, European Commission, European Research Council, Josep Carreras Leukemia Foundation, Associazione Italiana per la Ricerca sul Cancro, Fondazione Cariplo, Association for International Cancer Research, Ministero dell'Istruzione, dell'Università e della Ricerca, Gerboth, S., Frittoli, E., Palamidessi, A., Baltanás, Fernando C., Salek, M., Rappsilber, J., Giuliani, C., Troglio, F., Rolland, Y., Pruneri, G., Kreutmair, S., Pallavicini, I., Zobel, M., Cinquanta, M., Minucci, S., Gómez, Carmela, Illert, A.L., and Scita, G.
Abstract: Son of Sevenless 1 (SOS1) is a dual guanine nucleotide exchange factor (GEF) that activates the small GTPases RAC and RAS. Although the molecular mechanisms of RAS GEF catalysis have been unveiled, how SOS1 acquires RAC GEF activity and what is the physio-pathological relevance of this activity is much less understood. Here we show that SOS1 is tyrosine phosphorylated on Y1196 by ABL. Phosphorylation of Y1196 controls SOS1 inter-molecular interaction, is required to promote the exchange of nucleotides on RAC in vitro and for platelet-derived growth factor (PDGF) activation of RAC- and RAC-dependent actin remodeling and cell migration. SOS1 is also phosphorylated on Y1196 by BCR-ABL in chronic myelogenous leukemic cells. Importantly, in these cells, SOS1 is required for BCR-ABL-mediated activation of RAC, cell proliferation and transformation in vitro and in a xenograft mouse model. Finally, genetic removal of Sos1 in the bone marrow-derived cells (BMDCs) from Sos1 fl/fl mice and infected with BCR-ABL causes a significant delay in the onset of leukemogenesis once BMDCs are injected into recipient, lethally irradiated mice. Thus, SOS1 is required for full transformation and critically contribute to the leukemogenic potential of BCR-ABL.
Published: 2018

33. The actin-binding protein profilin 2 is a novel regulator of iron homeostasis

Author: Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, German Research Foundation, University of Applied Sciences Bonn-Rhein-Sieg, Ministerio de Economía y Competitividad (España), Luscieti, Sara, Galy, Bruno, Gutiérrez, Lucía, Reinke, Michael, Couso, Jorge, Shvartsman, Maya, Pascale, Antonio di, Witke, Walter, Hentze, Matthias W., Pilo Boyl, Pietro, Sanchez, Mayka, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, German Research Foundation, University of Applied Sciences Bonn-Rhein-Sieg, Ministerio de Economía y Competitividad (España), Luscieti, Sara, Galy, Bruno, Gutiérrez, Lucía, Reinke, Michael, Couso, Jorge, Shvartsman, Maya, Pascale, Antonio di, Witke, Walter, Hentze, Matthias W., Pilo Boyl, Pietro, and Sanchez, Mayka
Abstract: Cellular iron homeostasis is controlled by the iron regulatory proteins (IRPs) 1 and 2 that bind cis-regulatory iron-responsive elements (IRE) on target messenger RNAs (mRNA). We identified profilin 2 (Pfn2) mRNA, which encodes an actin-binding protein involved in endocytosis and neurotransmitter release, as a novel IRP-interacting transcript, and studied its role in iron metabolism. A combination of electrophoretic mobility shift assay experiments and bioinformatic analyses led to the identification of an atypical and conserved IRE in the 39 untranslated region of Pfn2 mRNA. Pfn2 mRNA levels were significantly reduced in duodenal samples from mice with intestinal IRP ablation, suggesting that IRPs exert a positive effect on Pfn2 mRNA expression in vivo. Overexpression of Pfn2 in HeLa and Hepa1-6 cells reduced their metabolically active iron pool. Importantly, Pfn2-deficient mice showed iron accumulation in discrete areas of the brain (olfactory bulb, hippocampus, and midbrain) and reduction of the hepatic iron store without anemia. Despite low liver iron levels, hepatic hepcidin expression remained high, likely because of compensatory activation of hepcidin by mild inflammation. Splenic ferroportin was increased probably to sustain hematopoiesis. Overall, our results indicate that Pfn2 expression is controlled by the IRPs in vivo and that Pfn2 contributes to maintaining iron homeostasis in cell lines and mice.
Published: 2017

34. Intratumoral heterogeneity and clonal evolution in blood malignancies and solid tumors

Author: Ministerio de Economía y Competitividad (España), Fundación Ramón Areces, European Research Council, Josep Carreras Leukemia Foundation, Fundación la Caixa, Generalitat de Catalunya, Varela, Ignacio, Menéndez, Pablo, Sanjuan-Pla, Alejandra, Ministerio de Economía y Competitividad (España), Fundación Ramón Areces, European Research Council, Josep Carreras Leukemia Foundation, Fundación la Caixa, Generalitat de Catalunya, Varela, Ignacio, Menéndez, Pablo, and Sanjuan-Pla, Alejandra
Abstract: This meeting held at the University of Barcelona in March 2017, brought together scientists and clinicians worldwide to discuss current and future clinico-biological implications of intratumoral heterogeneity (ITH) and subclonal evolution in cancer diagnosis, patient stratification, and treatment resistance in diagnosis, treatment and follow-up. There was consensus that both longitudinal and tumor multi-region studies in matched samples are needed to better understand the dynamics of ITH. The contribution of the epigenome and microenvironment to ITH and subclone evolution remains understudied. It was recommended to combine computational, pathology and imaging tools to study the role of the microenvironment in subclone selection/ evolution.
Published: 2017

35. Activation-induced cytidine deaminase prevents pro-B cell acute lymphoblastic leukemia by functioning as a negative regulator in Rag1 deficient pro-B cells

Author: Ministerio de Economía y Competitividad (España), Federal Ministry of Education and Research (Germany), Heinrich Heine University Düsseldorf, German Childhood Cancer Foundation, Instituto de Salud Carlos III, Junta de Castilla y León, Lady Tata Memorial Trust, Josep Carreras Leukemia Foundation, European Commission, Fundación Inocente Inocente, Auer, Franziska, Ingenhag, Deborah, Pinkert, Stefan, Kracker, Sven, Hacein-Bey-Abina, Salima, Cavazzana, Marina, Gombert, Michael, Martín-Lorenzo, Alberto, Lin, Min-Hui, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Borkhardt, Arndt, Hauer, Julia, Ministerio de Economía y Competitividad (España), Federal Ministry of Education and Research (Germany), Heinrich Heine University Düsseldorf, German Childhood Cancer Foundation, Instituto de Salud Carlos III, Junta de Castilla y León, Lady Tata Memorial Trust, Josep Carreras Leukemia Foundation, European Commission, Fundación Inocente Inocente, Auer, Franziska, Ingenhag, Deborah, Pinkert, Stefan, Kracker, Sven, Hacein-Bey-Abina, Salima, Cavazzana, Marina, Gombert, Michael, Martín-Lorenzo, Alberto, Lin, Min-Hui, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Borkhardt, Arndt, and Hauer, Julia
Abstract: Activation-induced cytidine deaminase (AID) is essential for somatic hypermutation and class switch recombination in mature B-cells, while AID was also shown to play a role in developing pre-BCR/BCR-positive B-cells of the bone marrow. To further elucidate a potential function of Aid in the bone marrow prior to V(D) J-recombination, we utilized an in vivo model which exerts a B-cell developmental arrest at the pro-B cell stage with low frequencies of pro-B cell acute lymphoblastic leukemia (pro-B ALL) development. Therefore, p19ArfRag1 (AR) mice were crossed with Aid-deficient mice (ARA). Surprisingly, loss of Aid expression in pro-B cells accelerated pro-B ALL incidence from 30% (AR) to 98% (ARA). This effect was Aid dose dependent, since Aid animals of the same background displayed a significantly lower incidence (83%). Furthermore, B-cell-specific Aid up-regulation was observed in Aid-competent pro-B ALLs. Additional whole exome/sanger sequencing of murine pro-B ALLs revealed an accumulation of recurrent somatic Jak3 (p. R653H, p. V670A) and Dnm2 (p. G397R) mutations, which highlights the importance of active IL7R signaling in the pro-B ALL blast cells. These findings were further supported by an enhanced proliferative potential of ARA pro-B cells compared to Aid-competent cells from the same genetic background. In summary, we show that both Aid and Rag1 act as a negative regulators in pro-B cells, preventing pro-B ALL.
Published: 2017

36. Infection exposure promotes ETV6-RUNX1 precursor B-cell leukemia via impaired H3K4 demethylases

Author: Wellcome Trust, National Institutes of Health (US), Federal Ministry of Education and Research (Germany), Ministerio de Economía y Competitividad (España), European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, Instituto de Investigación Biomédica de Salamanca, Fundación Inocente Inocente, Josep Carreras Leukemia Foundation, Lady Tata Memorial Trust, Leukemia & Lymphoma Society (US), Heinrich Heine University Düsseldorf, German Childhood Cancer Foundation, Rodríguez-Hernández, Guillermo, Hauer, Julia, Martín-Lorenzo, Alberto, Schäfer, Daniel, Bartenhagen, Christoph, García-Ramírez, Idoia, Auer, Franziska, González-Herrero, Inés, Ruiz-Roca, Lucía, Gombert, Michael, Okpanyi, Vera, Fischer, Ute, Chen, Cai, Dugas, Martin, Bhatia, Sanil, Martin Linka, René, García Suquía, Marta, Rascón-Trincado, María Victoria, García-Sánchez, Angel, Blanco, Óscar, García-Cenador, Begoña, García-Criado, Francisco Javier, Cobaleda, César, Alonso-López, D., De Las Rivas, Javier, Müschen, Markus, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Borkhardt, Arndt, Wellcome Trust, National Institutes of Health (US), Federal Ministry of Education and Research (Germany), Ministerio de Economía y Competitividad (España), European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, Instituto de Investigación Biomédica de Salamanca, Fundación Inocente Inocente, Josep Carreras Leukemia Foundation, Lady Tata Memorial Trust, Leukemia & Lymphoma Society (US), Heinrich Heine University Düsseldorf, German Childhood Cancer Foundation, Rodríguez-Hernández, Guillermo, Hauer, Julia, Martín-Lorenzo, Alberto, Schäfer, Daniel, Bartenhagen, Christoph, García-Ramírez, Idoia, Auer, Franziska, González-Herrero, Inés, Ruiz-Roca, Lucía, Gombert, Michael, Okpanyi, Vera, Fischer, Ute, Chen, Cai, Dugas, Martin, Bhatia, Sanil, Martin Linka, René, García Suquía, Marta, Rascón-Trincado, María Victoria, García-Sánchez, Angel, Blanco, Óscar, García-Cenador, Begoña, García-Criado, Francisco Javier, Cobaleda, César, Alonso-López, D., De Las Rivas, Javier, Müschen, Markus, Vicente-Dueñas, Carolina, Sánchez García, Isidro, and Borkhardt, Arndt
Abstract: ETV6-RUNX1 is associated with the most common subtype of childhood leukemia. As few ETV6-RUNX1 carriers develop precursor B-cell acute lymphocytic leukemia (pB-ALL), the underlying genetic basis for development of full-blown leukemia remains to be identified, but the appearance of leukemia cases in time-space clusters keeps infection as a potential causal factor. Here, we present in vivo genetic evidence mechanistically connecting preleukemic ETV6-RUNX1 expression in hematopoetic stem cells/precursor cells (HSC/PC) and postnatal infections for human-like pB-ALL. In our model, ETV6-RUNX1 conferred a low risk of developing pB-ALL after exposure to common pathogens, corroborating the low incidence observed in humans. Murine preleukemic ETV6-RUNX1 pro/preB cells showed high Rag1/2 expression, known for human ETV6-RUNX1 pB-ALL. Murine and human ETV6-RUNX1 pB-ALL revealed recurrent genomic alterations, with a relevant proportion affecting genes of the lysine demethylase (KDM) family. KDM5C loss of function resulted in increased levels of H3K4me3, which coprecipitated with RAG2 in a human cell line model, laying the molecular basis for recombination activity. We conclude that alterations of KDM family members represent a disease-driving mechanism and an explanation for RAG off-target cleavage observed in humans. Our results explain the genetic basis for clonal evolution of an ETV6-RUNX1 preleukemic clone to pB-ALL after infection exposure and offer the possibility of novel therapeutic approaches.
Published: 2017

37. Modeling the process of childhood ETV6-RUNX1 B-cell leukemias

Author: Junta de Castilla y León, Fundación Inocente Inocente, Josep Carreras Leukemia Foundation, European Commission, Lady Tata Memorial Trust, Agence Nationale de la Recherche (France), Federal Ministry of Education and Research (Germany), Heinrich Heine University Düsseldorf, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), German Childhood Cancer Foundation, Rodríguez-Hernández, Guillermo, Schäfer, Daniel, Gavilán, Ana, Vicente-Dueñas, Carolina, Hauer, Julia, Borkhardt, Arndt, Sánchez García, Isidro, Junta de Castilla y León, Fundación Inocente Inocente, Josep Carreras Leukemia Foundation, European Commission, Lady Tata Memorial Trust, Agence Nationale de la Recherche (France), Federal Ministry of Education and Research (Germany), Heinrich Heine University Düsseldorf, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), German Childhood Cancer Foundation, Rodríguez-Hernández, Guillermo, Schäfer, Daniel, Gavilán, Ana, Vicente-Dueñas, Carolina, Hauer, Julia, Borkhardt, Arndt, and Sánchez García, Isidro
Abstract: ETV6-RUNX1 is associated with the most common subtype of childhood leukemia. Pre-leukaemic clones carrying ETV6-RUNX1 oncogenic lesions are frequently found in neonatal cord blood, but only few ETV6-RUNX1 carriers develop pB-ALL. The highly demanding and pending challenge is to reveal the multistep natural history of ETV6-RUNX1 pB-ALL, because it can offer non-toxic prophylactic interventions to preleukemic carriers. However, the lack of a genetically engineered ETV6-RUNX1 mouse model mimicking the human pB-ALL has hampered our understanding of the pathogenesis of this disease. This rule has now been broken in a study of the effect of the ETV6-RUNX1 oncogene in cancer development in a mouse model in which oncogene expression is restricted to the stem cell compartment. In this article, we review the different attempts to model this disease, including the recent representative success stories and we discuss its potential application to both identify etiologic factors of childhood ETV6-RUNX1 pB-ALL and prevent the conversion of a preleukemic clone in an irreversible transformed state.
Published: 2017

38. NEDD 9 an independent good prognostic factor in intermediaterisk acute myeloid leukemia patients

Author: Josep Carreras Leukemia Foundation, Generalitat de Catalunya, Fundació La Marató de TV3, Fundació Privada Cellex, Instituto de Salud Carlos III, European Commission, Asociación Española Contra el Cáncer, Pallarès, Victor, Hoyos, Montserrat, Chillón, M. del Carmen, Barragán, Eva, Prieto-Conde, Isabel, Llop, Marta, Céspedes, María Virtudes, Nomdedéu, Josep F., Brunet, Salut, Sanz, Miguel Ángel, González, Marcos, Sierra, Jorge, Casanova, Isolda, Mangues, Ramon, Josep Carreras Leukemia Foundation, Generalitat de Catalunya, Fundació La Marató de TV3, Fundació Privada Cellex, Instituto de Salud Carlos III, European Commission, Asociación Española Contra el Cáncer, Pallarès, Victor, Hoyos, Montserrat, Chillón, M. del Carmen, Barragán, Eva, Prieto-Conde, Isabel, Llop, Marta, Céspedes, María Virtudes, Nomdedéu, Josep F., Brunet, Salut, Sanz, Miguel Ángel, González, Marcos, Sierra, Jorge, Casanova, Isolda, and Mangues, Ramon
Abstract: Intermediate-risk acute myeloid leukemia (IR-AML) is the largest subgroup of AML patients and is highly heterogeneous. Whereas adverse and favourable risk patients have well-established treatment protocols, IR-AML patients have not. It is, therefore, crucial to find novel factors that stratify this subgroup to implement risk-adapted strategies. The CAS (Crk-associated substrate) adaptor protein family regulates cell proliferation, survival, migration and adhesion. Despite its association with metastatic dissemination and prognosis of different solid tumors, the role of these proteins in hematological malignancies has been scarcely evaluated. Nevertheless, previous work has established an important role for the CAS family members NEDD9 or BCAR1 in the migratory and dissemination capacities of myeloid cells. On this basis, we hypothesized that NEDD9 or BCAR1 expression levels could associate with survival in IR-AML patients and become new prognostic markers. To that purpose, we assessed BCAR1 and NEDD9 gene expression in a cohort of 73 adult AML patients validating the results in an independent cohort (n = 206). We have identified NEDD9, but not BCAR1, as a new a marker for longer overall and disease-free survival, and for lower cumulative incidence of relapse. In summary, NEDD9 gene expression is an independent prognostic factor for favourable prognosis in IR-AML patients.
Published: 2017

39. Crebbp loss cooperates with Bcl2 overexpression to promote lymphoma in mice

Author: Nebraska Department of Health and Human Services, European Commission, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, National Cancer Institute (US), National Institutes of Health (US), Fundación Inocente Inocente, Instituto de Investigación Biomédica de Salamanca, Josep Carreras Leukemia Foundation, Centre National de la Recherche Scientifique (France), Région Ile-de-France, Université Paris Diderot, Institut National du Cancer (France), García-Ramírez, Idoia, Tadros, Saber, González-Herrero, Inés, Martín-Lorenzo, Alberto, Rodríguez-Hernández, Guillermo, Moore, Dalia, Ruiz-Roca, Lucía, Blanco, Óscar, Alonso-López, D., De Las Rivas, Javier, Hartert, Keenan, Duval, Romain, Klinkebiel, David, Bast, Martin, Vose, Julie, Lunning, Matthew, Fu, Kai, Greiner, Timothy, Rodrigues-Lima, Fernando, Jiménez, Rafael, García-Criado, Francisco Javier, García-Cenador, Begoña, Brindle, Paul, Vicente-Dueñas, Carolina, Alizadeh, Ash A., Sánchez García, Isidro, Green, Michael R., Nebraska Department of Health and Human Services, European Commission, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, National Cancer Institute (US), National Institutes of Health (US), Fundación Inocente Inocente, Instituto de Investigación Biomédica de Salamanca, Josep Carreras Leukemia Foundation, Centre National de la Recherche Scientifique (France), Région Ile-de-France, Université Paris Diderot, Institut National du Cancer (France), García-Ramírez, Idoia, Tadros, Saber, González-Herrero, Inés, Martín-Lorenzo, Alberto, Rodríguez-Hernández, Guillermo, Moore, Dalia, Ruiz-Roca, Lucía, Blanco, Óscar, Alonso-López, D., De Las Rivas, Javier, Hartert, Keenan, Duval, Romain, Klinkebiel, David, Bast, Martin, Vose, Julie, Lunning, Matthew, Fu, Kai, Greiner, Timothy, Rodrigues-Lima, Fernando, Jiménez, Rafael, García-Criado, Francisco Javier, García-Cenador, Begoña, Brindle, Paul, Vicente-Dueñas, Carolina, Alizadeh, Ash A., Sánchez García, Isidro, and Green, Michael R.
Abstract: CREBBP is targeted by inactivating mutations in follicular lymphoma (FL) and diffuse large B-cell lymphoma (DLBCL). Here, we provide evidence from transgenic mouse models that Crebbp deletion results in deficits in B-cell development and can cooperate with Bcl2 overexpression to promote B-cell lymphoma. Through transcriptional and epigenetic profiling of these B cells, we found that Crebbp inactivation was associated with broad transcriptional alterations, but no changes in the patterns of histone acetylation at the proximal regulatory regions of these genes. However, B cells with Crebbp inactivation showed high expression of Myc and patterns of altered histone acetylation that were localized to intragenic regions, enriched for Myc DNA binding motifs, andshowedMycbinding. Through the analysis ofCREBBPmutations from a large cohort of primary human FL and DLBCL, we show a significant difference in the spectrum of CREBBP mutations in these 2 diseases, with higher frequencies of nonsense/ frameshift mutations in DLBCL compared with FL. Together, our data therefore provide important links between Crebbp inactivation and Bcl2 dependence and show a role for Crebbp inactivation in the induction of Myc expression. We suggest this may parallel the role of CREBBP frameshift/nonsense mutations in DLBCL that result in loss of the protein, but may contrast the role of missense mutations in the lysine acetyltransferase domain that are more frequently observed in FL and yield an inactive protein.
Published: 2017

40. Metabolic gatekeeper function of B-lymphoid transcription factors

Author: Wellcome Trust, Melanoma Research Alliance (US), Howard Hughes Medical Institute, Josep Carreras Leukemia Foundation, American Cancer Society, National Institutes of Health (US), Federal Ministry of Education and Research (Germany), Chan, Lai N., Chen, Zhengshan, Braas, Daniel, Lee, Jae-Woong, Xiao, Gang, Huimin, Geng, Cosgun, Kadriye Nehir, Hurtz, Christian, Shojaee, Seyedmehdi, Cazzaniga, Valeria, Schjerven, Hilde, Ernst, Thomas, Hochhaus, Andreas, Kornblau, Steven M., Konopleva, Marina, Pufall, Miles A., Cazzaniga, Giovanni, Liu, Grace J., Milne, Thomas A., Koeffler, H. Philip, Ross, Theodora S., Sánchez García, Isidro, Borkhardt, Arndt, Yamamoto, Keith R., Dickins, Ross A., Graeber, Thomas G., Müschen, Markus, Wellcome Trust, Melanoma Research Alliance (US), Howard Hughes Medical Institute, Josep Carreras Leukemia Foundation, American Cancer Society, National Institutes of Health (US), Federal Ministry of Education and Research (Germany), Chan, Lai N., Chen, Zhengshan, Braas, Daniel, Lee, Jae-Woong, Xiao, Gang, Huimin, Geng, Cosgun, Kadriye Nehir, Hurtz, Christian, Shojaee, Seyedmehdi, Cazzaniga, Valeria, Schjerven, Hilde, Ernst, Thomas, Hochhaus, Andreas, Kornblau, Steven M., Konopleva, Marina, Pufall, Miles A., Cazzaniga, Giovanni, Liu, Grace J., Milne, Thomas A., Koeffler, H. Philip, Ross, Theodora S., Sánchez García, Isidro, Borkhardt, Arndt, Yamamoto, Keith R., Dickins, Ross A., Graeber, Thomas G., and Müschen, Markus
Abstract: B-lymphoid transcription factors, such as PAX5 and IKZF1, are critical for early B-cell development, yet lesions of the genes encoding these transcription factors occur in over 80% of cases of pre-B-cell acute lymphoblastic leukaemia (ALL). The importance of these lesions in ALL has, until now, remained unclear. Here, by combining studies using chromatin immunoprecipitation with sequencing and RNA sequencing, we identify a novel B-lymphoid program for transcriptional repression of glucose and energy supply. Our metabolic analyses revealed that PAX5 and IKZF1 enforce a state of chronic energy deprivation, resulting in constitutive activation of the energy-stress sensor AMPK. Dominant-negative mutants of PAX5 and IKZF1, however, relieved this glucose and energy restriction. In a transgenic pre-B ALL mouse model, the heterozygous deletion of Pax5 increased glucose uptake and ATP levels by more than 25-fold. Reconstitution of PAX5 and IKZF1 in samples from patients with pre-B ALL restored a non-permissive state and induced energy crisis and cell death. A CRISPR/Cas9-based screen of PAX5 and IKZF1 transcriptional targets identified the products of NR3C1 (encoding the glucocorticoid receptor), TXNIP (encoding a glucose-feedback sensor) and CNR2 (encoding a cannabinoid receptor) as central effectors of B-lymphoid restriction of glucose and energy supply. Notably, transport-independent lipophilic methyl-conjugates of pyruvate and tricarboxylic acid cycle metabolites bypassed the gatekeeper function of PAX5 and IKZF1 and readily enabled leukaemic transformation. Conversely, pharmacological TXNIP and CNR2 agonists and a small-molecule AMPK inhibitor strongly synergized with glucocorticoids, identifying TXNIP, CNR2 and AMPK as potential therapeutic targets. Furthermore, our results provide a mechanistic explanation for the empirical finding that glucocorticoids are effective in the treatment of B-lymphoid but not myeloid malignancies. Thus, B-lymphoid transcription factors fun
Published: 2017

41. Development refractoriness of MLL-rearranged human B cell acute leukemias to reprogramming into pluripotency

Author: Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, Asociación Española Contra el Cáncer, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, European Research Council, Muñoz-López, Alvaro, Prieto López, Cristina, Agraz-Doblas, Antonio, Varela, Ignacio, Menéndez, Pablo, Generalitat de Catalunya, Josep Carreras Leukemia Foundation, Fundación la Caixa, Asociación Española Contra el Cáncer, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, European Commission, European Research Council, Muñoz-López, Alvaro, Prieto López, Cristina, Agraz-Doblas, Antonio, Varela, Ignacio, and Menéndez, Pablo
Abstract: Induced pluripotent stem cells (iPSCs) are a powerful tool for disease modeling. They are routinely generated from healthy donors and patients from multiple cell types at different developmental stages. However, reprogramming leukemias is an extremely inefficient process. Few studies generated iPSCs from primary chronic myeloid leukemias, but iPSC generation from acute myeloid or lymphoid leukemias (ALL) has not been achieved. We attempted to generate iPSCs from different subtypes of B-ALL to address the developmental impact of leukemic fusion genes. OKSM(L)-expressing mono/polycistronic-, retroviral/lentiviral/episomal-, and Sendai virus vector-based reprogramming strategies failed to render iPSCs in vitro and in vivo. Addition of transcriptomic-epigenetic reprogramming “boosters” also failed to generate iPSCs from B cell blasts and B-ALL lines, and when iPSCs emerged they lacked leukemic fusion genes, demonstrating non-leukemic myeloid origin. Conversely, MLL-AF4-overexpressing hematopoietic stem cells/B progenitors were successfully reprogrammed, indicating that B cell origin and leukemic fusion gene were not reprogramming barriers. Global transcriptome/DNA methylome profiling suggested a developmental/differentiation refractoriness of MLL-rearranged B-ALL to reprogramming into pluripotency.
Published: 2016

42. Activated KRAS cooperates with MLLAF4 to promote extramedullary engraftment and migration of cord blood CD34+ HSPC but is insufficient to initiate leukemia

Author: Fundación la Caixa, Josep Carreras Leukemia Foundation, European Research Council, Instituto de Salud Carlos III, Federación Española de Enfermedades Raras, Ministerio de Economía y Competitividad (España), Asociación Española Contra el Cáncer, Fundación Inocente Inocente, Friends of José Carreras International Leukemia Foundation, Consejo Superior de Investigaciones Científicas (España), Prieto López, Cristina, Agraz-Doblas, Antonio, Varela, Ignacio, Menéndez, Pablo, Fundación la Caixa, Josep Carreras Leukemia Foundation, European Research Council, Instituto de Salud Carlos III, Federación Española de Enfermedades Raras, Ministerio de Economía y Competitividad (España), Asociación Española Contra el Cáncer, Fundación Inocente Inocente, Friends of José Carreras International Leukemia Foundation, Consejo Superior de Investigaciones Científicas (España), Prieto López, Cristina, Agraz-Doblas, Antonio, Varela, Ignacio, and Menéndez, Pablo
Abstract: The MLL-AF4 (MA4) fusion gene is the genetic hallmark of an aggressive infant pro-B-acute lymphoblastic leukemia (B-ALL). Our understanding of MA4-mediated transformation is very limited. Whole-genome sequencing studies revealed a silent mutational landscape, which contradicts the aggressive clinical outcome of this hematologic malignancy. Only RAS mutations were recurrently detected in patients and found to be associated with poorer outcome. The absence of MA4-driven B-ALL models further questions whether MA4 acts as a single oncogenic driver or requires cooperating mutations to manifest a malignant phenotype. We explored whether KRAS activation cooperates with MA4 to initiate leukemia in cord blood-derived CD34(+) hematopoietic stem/progenitor cells (HSPC). Clonogenic and differentiation/proliferation assays demonstrated that KRAS activation does not cooperate with MA4 to immortalize CD34(+) HSPCs. Intrabone marrow transplantation into immunodeficient mice further showed that MA4 and KRASG12V alone or in combination enhanced hematopoietic repopulation without impairing myeloid-lymphoid differentiation, and that mutated KRAS did not cooperate with MA4 to initiate leukemia. However, KRAS activation enhanced extramedullary hematopoiesis of MA4-expressing cell lines and CD34(+) HSPCs that was associated with leukocytosis and central nervous system infiltration, both hallmarks of infant t(4;11)(+) B-ALL. Transcriptional profiling of MA4-expressing patients supported a cell migration gene signature underlying the mutant KRAS-mediated phenotype. Collectively, our findings demonstrate that KRAS affects the homeostasis of MA4-expressing HSPCs, suggesting that KRAS activation in MA4(+) B-ALL is important for tumor maintenance rather than initiation.
Published: 2016

43. 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

44. GEMMs addressing Pax5 loss-of-function in childhood pB-ALL

Author: German Childhood Cancer Foundation, European Commission, Heinrich Heine University Düsseldorf, Federal Ministry of Education and Research (Germany), Josep Carreras Leukemia Foundation, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Inocente Inocente, Auer, Franziska, Ingenhag, Deborah, Bhatia, Sanil, Enczmann, Jürgen, Cobaleda, César, Sánchez García, Isidro, Borkhardt, Arndt, Hauer, Julia, German Childhood Cancer Foundation, European Commission, Heinrich Heine University Düsseldorf, Federal Ministry of Education and Research (Germany), Josep Carreras Leukemia Foundation, Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Junta de Castilla y León, Fundación Inocente Inocente, Auer, Franziska, Ingenhag, Deborah, Bhatia, Sanil, Enczmann, Jürgen, Cobaleda, César, Sánchez García, Isidro, Borkhardt, Arndt, and Hauer, Julia
Abstract: Germline mutations in transcription factors, which are implicated in hematopoiesis in general or specifically in B-cell differentiation have recently been described to confer an inherited risk to pB-ALL with often reduced penetrance. Predicting leukemia development, therapy response and long term follow up of mutation carriers is challenging because experience from large patient cohorts and their long term follow up are not available.Genetically Engineered Murine Models (GEMMs) represent a promising approach to create individualized and precise models reproducing the molecular makeup of the human disease. This review focuses on PAX5 loss-of-function and summarizes techniques of murine model generation, available GEMMs, which mimic Pax5 loss-of-function in leukemia development and discusses the challenges and drawbacks of these models. These aspects are discussed in the context of creating a robust model, which serves not only for validation of the relevance of a genomic alteration in pB-ALL but at the same time as a valid preclinical model.
Published: 2016

45. Arabinoxylan rice bran (MGN-3/Biobran) enhances natural killer cell-mediated cytotoxicity against neuroblastoma invitro and invivo

Author: Sociedad Española de Hematología y Oncología Pediátricas, Fundación CRIS contra el Cáncer, Fundación de la Sociedad Española de Hematología y Oncología Pediátricas, Instituto de Salud Carlos III, Josep Carreras Leukemia Foundation, German Childhood Cancer Foundation, Pérez-Martínez, Antonio, López-Collazo, Eduardo, Sociedad Española de Hematología y Oncología Pediátricas, Fundación CRIS contra el Cáncer, Fundación de la Sociedad Española de Hematología y Oncología Pediátricas, Instituto de Salud Carlos III, Josep Carreras Leukemia Foundation, German Childhood Cancer Foundation, Pérez-Martínez, Antonio, and López-Collazo, Eduardo
Abstract: [Background aims]: Natural killer cell (NK) cytotoxic activity plays a major role in natural immunologic defences against malignancies. NK cells are emerging as a tool for adoptive cancer immunotherapies. Arabinoxylan rice bran (MGN-3/Biobran) has been described as a biological response modifier that can enhance the cytotoxic activity of NK cells. This study evaluated the effect of MGN-3/Biobran on NK cell activation, expansion and cytotoxicity against neuroblastoma cells. [Methods]: NK cells were enriched with magnetic beads and stimulated with MGN-3/Biobran. NK cell activation was evaluated via analysis of their phenotype, and their expansion capability was tracked. The invitro cytotoxic ability of the activated NK cells was tested against K562, Jurkat, A673, NB1691, A-204, RD and RH-30 cell lines and the invivo cytotoxic ability against the NB1691 cell line. [Results]: MGN-3/Biobran stimulation of NK cells induced a higher expression of the activation-associated receptors CD25 and CD69 than in unstimulated cells (P< 0.05). The expression of NKG2D, DNAM, NCRs and TLRs remained unchanged. Overnight MGN-3/Biobran stimulation increased NK cell cytotoxic activity against all cell lines tested invitro and decelerated neuroblastoma growth invivo. The mechanism is not mediated by lipopolysaccharide contamination in MGN-3/Biobran. Furthermore, the addition of MGN-3/Biobran promoted NK cell expansion and decreased T cells invitro. Conclusions: Our data show that MGN-3/Biobran upregulates NK cell activation markers, stimulates NK cell cytotoxic activity against neuroblastoma invitro and invivo and selectively augments the expansion of NK cells. These results may be useful for future NK cell therapeutic strategies of the treatment of neuroblastoma.
Published: 2015

46. Infection exposure is a causal factor in B-cell precursor acute lymphoblastic leukemia as a result of Pax5-inherited susceptibility

Author: Fondation contre le Cancer, Federal Ministry of Education and Research (Germany), University of Applied Sciences Bonn-Rhein-Sieg, Heinrich Heine University Düsseldorf, German Childhood Cancer Foundation, Australian Research Council, Belgian Science Policy Office, European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, Ministerio de Economía y Competitividad (España), Fundación Inocente Inocente, Josep Carreras Leukemia Foundation, Martín-Lorenzo, Alberto, Hauer, Julia, Vicente-Dueñas, Carolina, González-Herrero, Inés, García-Ramírez, Idoia, Blanco, Óscar, Mayado, Andrea, Orfao, Alberto, De Las Rivas, Javier, Cobaleda, César, García-Cenador, Begoña, García-Criado, Francisco Javier, Sánchez García, Isidro, Borkhardt, Arndt, Fondation contre le Cancer, Federal Ministry of Education and Research (Germany), University of Applied Sciences Bonn-Rhein-Sieg, Heinrich Heine University Düsseldorf, German Childhood Cancer Foundation, Australian Research Council, Belgian Science Policy Office, European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, Ministerio de Economía y Competitividad (España), Fundación Inocente Inocente, Josep Carreras Leukemia Foundation, Martín-Lorenzo, Alberto, Hauer, Julia, Vicente-Dueñas, Carolina, González-Herrero, Inés, García-Ramírez, Idoia, Blanco, Óscar, Mayado, Andrea, Orfao, Alberto, De Las Rivas, Javier, Cobaleda, César, García-Cenador, Begoña, García-Criado, Francisco Javier, Sánchez García, Isidro, and Borkhardt, Arndt
Abstract: Earlier in the past century, infections were regarded as the most likely cause of childhood B-cell precursor acute lymphoblastic leukemia (pB-ALL). However, there is a lack of relevant biologic evidence supporting this hypothesis. We present in vivo genetic evidence mechanistically connecting inherited susceptibility to pB-ALL and postnatal infections by showing that pB-ALL was initiated in Pax5 heterozygous mice only when they were exposed to common pathogens. Strikingly, these murine pB-ALLs closely resemble the human disease. Tumor exome sequencing revealed activating somatic, nonsynonymous mutations of Jak3 as a second hit. Transplantation experiments and deep sequencing suggest that inactivating mutations in Pax5 promote leukemogenesis by creating an aberrant progenitor compartment that is susceptible to malignant transformation through accumulation of secondary Jak3 mutations. Thus, treatment of Pax5 leukemic cells with specific JAK1/3 inhibitors resulted in increased apoptosis. These results uncover the causal role of infection in pB-ALL development. [Significance]: These results demonstrate that delayed infection exposure is a causal factor in pB-ALL. Therefore, these findings have critical implications for the understanding of the pathogenesis of leukemia and for the development of novel therapies for this disease.
Published: 2015

47. CXCR4 expression enhances diffuse large B cell lymphoma dissemination and decreases patient survival

Author: Ministerio de Ciencia e Innovación (España), Instituto de Salud Carlos III, Centro de Investigación Biomédica en Red Bioingeniería, Biomateriales y Nanomedicina (España), Generalitat de Catalunya, Fundació La Marató de TV3, Josep Carreras Leukemia Foundation, Fundació Privada Cellex, Junta de Castilla y León, Moreno, María José, Alcoceba, Miguel, Blanco, Óscar, González, Marcos, Mangues, Ramon, Casanova, Isolda, Ministerio de Ciencia e Innovación (España), Instituto de Salud Carlos III, Centro de Investigación Biomédica en Red Bioingeniería, Biomateriales y Nanomedicina (España), Generalitat de Catalunya, Fundació La Marató de TV3, Josep Carreras Leukemia Foundation, Fundació Privada Cellex, Junta de Castilla y León, Moreno, María José, Alcoceba, Miguel, Blanco, Óscar, González, Marcos, Mangues, Ramon, and Casanova, Isolda
Abstract: The chemokine receptor CXCR4 has been implicated in the migration and trafficking of malignant B cells in several haematological malignancies. Over-expression of CXCR4 has been identified in haematological tumours, but data concerning the role of this receptor in diffuse large B cell lymphoma (DLBCL) are lacking. CXCR4 is a marker of poor prognosis in various neoplasms, correlating with metastatic disease and decreased survival of patients. We studied CXCR4 involvement in cell migration in vitro and dissemination in vivo. We also evaluated the prognostic significance of CXCR4 in 94 biopsies of DLBCL patients. We observed that the level of expression of CXCR4 in DLBCL cell lines correlated positively with in vitro migration. Expression of the receptor was also associated with increased engraftment and dissemination, and decreased survival time in NOD/SCID mice. Furthermore, administration of a specific CXCR4 antagonist, AMD3100, decreased dissemination of DLBCL cells in a xenograft mouse model. In addition, we found that CXCR4 expression is an independent prognostic factor for shorter overall survival and progression-free survival in DLBCL patients. These results show that CXCR4 mediates dissemination of DLBCL cells and define for the first time its value as an independent prognostic marker in DLBCL patients.
Published: 2015

48. Is lineage decision-making restricted during tumoral reprograming of haematopoietic stem cells?

Author: Josep Carreras Leukemia Foundation, Fundación Inocente Inocente, Junta de Castilla y León, Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), National Institutes of Health (US), Brown, Geoffrey, Sánchez García, Isidro, Josep Carreras Leukemia Foundation, Fundación Inocente Inocente, Junta de Castilla y León, Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), National Institutes of Health (US), Brown, Geoffrey, and Sánchez García, Isidro
Abstract: Within the past years there have been substantial changes to our understanding of haematopoiesis and cells that initiate and sustain leukemia. Recent studies have revealed that developing haematopoietic stem and progenitor cells are much more heterogeneous and versatile than has been previously thought. This versatility includes cells using more than one route to a fate and cells having progressed some way towards a cell type retaining other lineage options as clandestine. These notions impact substantially on our understanding of the origin and nature of leukemia. An important question is whether leukemia stem cells are as versatile as their cell of origin as an abundance of cells belonging to a lineage is often a feature of overt leukemia. In this regard, we examine the coming of age of the >leukemia stem cell> theory and the notion that leukemia, like normal haematopoiesis, is a hierarchically organized tissue. We examine evidence to support the notion that whilst cells that initiate leukemia have multi-lineage potential, leukemia stem cells are reprogrammed by further oncogenic insults to restrict their lineage decision-making. Accordingly, evolution of a sub-clone of lineage-restricted malignant cells is a key feature of overt leukemia.
Published: 2015

49. Early epigenetic cancer decisions

Author: Josep Carreras Leukemia Foundation, Junta de Castilla y León, National Institutes of Health (US), Ministerio de Ciencia e Innovación (España), European Commission, Martín-Lorenzo, Alberto, González-Herrero, Inés, Rodríguez-Hernández, Guillermo, García-Ramírez, Idoia, Vicente-Dueñas, Carolina, Sánchez García, Isidro, Josep Carreras Leukemia Foundation, Junta de Castilla y León, National Institutes of Health (US), Ministerio de Ciencia e Innovación (España), European Commission, Martín-Lorenzo, Alberto, González-Herrero, Inés, Rodríguez-Hernández, Guillermo, García-Ramírez, Idoia, Vicente-Dueñas, Carolina, and Sánchez García, Isidro
Abstract: A cancer dogma states that inactivation of oncogene(s) can cause cancer remission, implying that oncogenes are the Achilles' heel of cancers. This current model of cancer has kept oncogenes firmly in focus as therapeutic targets and is in agreement with the fact that in human cancers all cancerous cells, with independence of the cellular heterogeneity existing within the tumour, carry the same oncogenic genetic lesions. However, recent studies of the interactions between an oncogene and its target cell have shown that oncogenes contribute to cancer development via developmental reprogramming of the epigenome within the target cell. These results provide the first evidence that carcinogenesis can be initiated by epigenetic stem cell reprogramming, and uncover a new role for oncogenes in the origin of cancer. Here we analyse these evidences and discuss how this vision offers new avenues for developing novel anti-cancer interventions.
Published: 2014

50. Reprogramación tumoral en neoplasias linfoides

Author: Sánchez García, Isidro, European Commission, National Institutes of Health (US), Josep Carreras Leukemia Foundation, Ministerio de Educación, Cultura y Deporte (España), Junta de Castilla y León, Romero-Camarero, Isabel, Sánchez García, Isidro, European Commission, National Institutes of Health (US), Josep Carreras Leukemia Foundation, Ministerio de Educación, Cultura y Deporte (España), Junta de Castilla y León, and Romero-Camarero, Isabel
Abstract: El cáncer es un término genérico que designa un amplio grupo de enfermedades que pueden afectar a cualquier parte del organismo. En el año 2012, se cobró la vida de 8.000.000 personas, y es que, a pesar de todos los esfuerzos realizados a conocer la biología del cáncer, la supervivencia global no se ha visto incrementada de manera notoria y, en la mayoría de los casos se debe a una detección precoz de la enfermedad. Nuestro grupo de investigación está interesado en estudiar las etapas iniciales del cáncer, que van a convertir una célula pretumoral en una célula madre cancerígena. Una célula madre cancerígena es una célula neoplásica con características de célula madre, esto es, autorrenovación y capacidad de diferenciación, capaz de regenerar toda la diversidad celular presente en el tumor. La existencia de las células madre cancerígenas explicaría por qué algunos pacientes, tras un período de remisión inicial, sufren recaídas. Estas células madre cancerígenas serían las responsables de regenerar toda la masa tumoral de células. Sin embargo, no debemos confundir la célula madre cancerígena con la célula origen del cáncer, que es la célula donde va a tener lugar el primer evento oncogénico. En este contexto debemos hablar de la reprogramación tumoral, que es el proceso por el cual un evento oncogénico reprogramaría una célula, en este caso la célula origen del cáncer mediante alteraciones epigenéticas en su transcriptoma, estableciendo en ella un programa de diferenciación patológico que culminaría en el desarrollo de una masa tumoral, donde el oncogén ya no sería necesario ni para la progresión ni para el mantenimiento del cáncer. Nosotros quisimos estudiar la reprogramación tumoral en el contexto del linfoma difuso de células B grandes mediante la sobreexpresión de HGAL y en la génesis de leucemias linfoblásticas T tras la sobreexpresión de Lmo2.
Published: 2014

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