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1. Clonal heterogeneity and rates of specific chromosome gains are risk predictors in childhood high-hyperdiploid B-cell acute lymphoblastic leukemia

Author

Ramos-Muntada, M, Trincado, J, Blanco, J, Bueno, C, Rodriguez-Cortez, V, Bataller, A, Lopez-Millan, B, Schwab, C, Ortega, M, Velasco, P, Blanco, M, Nomdedeu, J, Ramirez-Orellana, M, Minguela, A, Fuster, J, Cuatrecasas, E, Camos, M, Ballerini, P, Escherich, G, Boer, J, Denboer, M, Hernandez-Rivas, J, Calasanz, M, Cazzaniga, G, Harrison, C, Menendez, P, Molina, O, Ramos-Muntada M., Trincado J. L., Blanco J., Bueno C., Rodriguez-Cortez V. C., Bataller A., Lopez-Millan B., Schwab C., Ortega M., Velasco P., Blanco M. L., Nomdedeu J., Ramirez-Orellana M., Minguela A., Fuster J. L., Cuatrecasas E., Camos M., Ballerini P., Escherich G., Boer J., DenBoer M., Hernandez-Rivas J. M., Calasanz M. J., Cazzaniga G., Harrison C. J., Menendez P., Molina O., Ramos-Muntada, M, Trincado, J, Blanco, J, Bueno, C, Rodriguez-Cortez, V, Bataller, A, Lopez-Millan, B, Schwab, C, Ortega, M, Velasco, P, Blanco, M, Nomdedeu, J, Ramirez-Orellana, M, Minguela, A, Fuster, J, Cuatrecasas, E, Camos, M, Ballerini, P, Escherich, G, Boer, J, Denboer, M, Hernandez-Rivas, J, Calasanz, M, Cazzaniga, G, Harrison, C, Menendez, P, Molina, O, Ramos-Muntada M., Trincado J. L., Blanco J., Bueno C., Rodriguez-Cortez V. C., Bataller A., Lopez-Millan B., Schwab C., Ortega M., Velasco P., Blanco M. L., Nomdedeu J., Ramirez-Orellana M., Minguela A., Fuster J. L., Cuatrecasas E., Camos M., Ballerini P., Escherich G., Boer J., DenBoer M., Hernandez-Rivas J. M., Calasanz M. J., Cazzaniga G., Harrison C. J., Menendez P., and Molina O.

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) is the commonest childhood cancer. High hyperdiploidy (HHD) identifies the most frequent cytogenetic subgroup in childhood B-ALL. Although hyperdiploidy represents an important prognostic factor in childhood B-ALL, the specific chromosome gains with prognostic value in HHD-B-ALL remain controversial, and the current knowledge about the hierarchy of chromosome gains, clonal heterogeneity and chromosomal instability in HHD-B-ALL remains very limited. We applied automated sequential-iFISH coupled with single-cell computational modeling to identify the specific chromosomal gains of the eight typically gained chromosomes in a large cohort of 72 primary diagnostic (DX, n = 62) and matched relapse (REL, n = 10) samples from HHD-B-ALL patients with either favorable or unfavorable clinical outcome in order to characterize the clonal heterogeneity, specific chromosome gains and clonal evolution. Our data show a high degree of clonal heterogeneity and a hierarchical order of chromosome gains in DX samples of HHD-B-ALL. The rates of specific chromosome gains and clonal heterogeneity found in DX samples differ between HHD-B-ALL patients with favorable or unfavorable clinical outcome. In fact, our comprehensive analyses at DX using a computationally defined risk predictor revealed low levels of trisomies +18+10 and low levels of clonal heterogeneity as robust relapse risk factors in minimal residual disease (MRD)-negative childhood HHD-B-ALL patients: relapse-free survival beyond 5 years: 22.1% versus 87.9%, P < 0.0001 and 33.3% versus 80%, P < 0.0001, respectively. Moreover, longitudinal analysis of matched DX-REL HHD-B-ALL samples revealed distinct patterns of clonal evolution at relapse. Our study offers a reliable prognostic sub-stratification of pediatric MRD-negative HHD-B-ALL patients.

Published
2022

2. Clonal dynamics in pediatric B-cell precursor acute lymphoblastic leukemia with very early relapse

Author

Antic, Z, Yu, J, Bornhauser, B, Lelieveld, S, van der Ham, C, van Reijmersdal, S, Morgado, L, Elitzur, S, Bourquin, J, Cazzaniga, G, Eckert, C, Camos, M, Sutton, R, Cave, H, Moorman, A, Sonneveld, E, Geurts van Kessel, A, van Leeuwen, F, Hoogerbrugge, P, Waanders, E, Kuiper, R, Antic Z., Yu J., Bornhauser B. C., Lelieveld S. H., van der Ham C. G., van Reijmersdal S. V., Morgado L., Elitzur S., Bourquin J. -P., Cazzaniga G., Eckert C., Camos M., Sutton R., Cave H., Moorman A. V., Sonneveld E., Geurts van Kessel A., van Leeuwen F. N., Hoogerbrugge P. M., Waanders E., Kuiper R. P., Antic, Z, Yu, J, Bornhauser, B, Lelieveld, S, van der Ham, C, van Reijmersdal, S, Morgado, L, Elitzur, S, Bourquin, J, Cazzaniga, G, Eckert, C, Camos, M, Sutton, R, Cave, H, Moorman, A, Sonneveld, E, Geurts van Kessel, A, van Leeuwen, F, Hoogerbrugge, P, Waanders, E, Kuiper, R, Antic Z., Yu J., Bornhauser B. C., Lelieveld S. H., van der Ham C. G., van Reijmersdal S. V., Morgado L., Elitzur S., Bourquin J. -P., Cazzaniga G., Eckert C., Camos M., Sutton R., Cave H., Moorman A. V., Sonneveld E., Geurts van Kessel A., van Leeuwen F. N., Hoogerbrugge P. M., Waanders E., and Kuiper R. P.

Abstract

Introduction: One-quarter of the relapses in children with B-cell precursor acute lymphoblastic leukemia (BCP-ALL) occur very early (within 18 months, before completion of treatment), and prognosis in these patients is worse compared to cases that relapse after treatment has ended. Methods: In this study, we performed a genomic analysis of diagnosis–relapse pairs of 12 children who relapsed very early, followed by a deep-sequencing validation of all identified mutations. In addition, we included one case with a good initial treatment response and on-treatment relapse at the end of upfront therapy. Results: We observed a dynamic clonal evolution in all cases, with relapse almost exclusively originating from a subclone at diagnosis. We identified several driver mutations that may have influenced the outgrowth of a minor clone at diagnosis to become the major clone at relapse. For example, a minimal residual disease (MRD)-based standard-risk patient with ETV6-RUNX1-positive leukemia developed a relapse from a TP53-mutated subclone after loss of the wildtype allele. Furthermore, two patients with TCF3-PBX1-positive leukemia that developed a very early relapse carried E1099K WHSC1 mutations at diagnosis, a hotspot mutation that was recurrently encountered in other very early TCF3-PBX1-positive leukemia relapses as well. In addition to alterations in known relapse drivers, we found two cases with truncating mutations in the cohesin gene RAD21. Conclusion: Comprehensive genomic characterization of diagnosis–relapse pairs shows that very early relapses in BCP-ALL frequently arise from minor subclones at diagnosis. A detailed understanding of the therapeutic pressure driving these events may aid the development of improved therapies.

Published
2022

6. Chromosome structure and mitotic defects are major pathogenic mechanisms in hyperdiploid childhood B-ALL

Author

Molina, O, additional, Bueno, C, additional, Bosch, A, additional, Granada, I, additional, Roca-Ho, H, additional, Gutierrez-Agüera, F, additional, Tirados, S, additional, Pal, D, additional, Ballerini, P, additional, deBoer, M, additional, Plensa, I, additional, Calasanz, MJ, additional, Rodríguez, R, additional, Camos, M, additional, Calvo, M, additional, and Menendez, P, additional

Published
2019
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8. Chromosome segregation defects as early underlying pathogenic mechanism in hyperdiploid childhood B-cell acute lymphoblastic leukaemia

Author

Molina, O, additional, Agraz-Doblas, A, additional, Roca-Ho, H, additional, Pal, D, additional, Granada, I, additional, Rodríguez-Perales, S, additional, Ballerini, P, additional, Camos, M, additional, Perez-Iribarne, MM, additional, Plensa, I, additional, Islam, A, additional, Calasanz, MJ, additional, Bueno, C, additional, and Menendez, P, additional

Published
2018
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9. Longer follow-up confirms major improvement in outcome in children and adolescents with Philadelphia chromosome acute lymphoblastic leukaemia treated with continuous imatinib and haematopoietic stem cell transplantation. Results from the Spanish Cooperative Study SHOP/ALL-2005

Author

Rives, S, Camos, M, Estella, J, Gomez, P, Moreno, MJ, Vivanco, JL, Melo, M, Fernandez-Delgado, R, Verdeguer, A, Fernandez-Teijeiro, A, Lendinez, F, Lopez-Almaraz, R, Uriz, JJ, and Badell, I

Subjects
tyrosine kinase inhibitor, acute lymphoblastic leukaemia, children, imatinib, Philadelphia chromosome
Published
2013

12. Prognostic value of FLT3 mutations in patients with acute promyelocytic leukemia treated with all-trans retinoic acid and anthracycline monochemotherapy

Author

Barragan, E, Montesinos, P, Camos, M, Gonzalez, M, Calasanz, MJ, Roman-Gomez, J, Gomez-Casares, MT, Ayala, R, Lopez, J, Fuster, O, Colomer, D, Chillon, C, Larrayoz, MJ, Sanchez-Godoy, P, Gonzalez-Campos, J, Manso, F, Amador, ML, Vellenga, E, Löwenberg, Bob, Sanz, MA, Barragan, E, Montesinos, P, Camos, M, Gonzalez, M, Calasanz, MJ, Roman-Gomez, J, Gomez-Casares, MT, Ayala, R, Lopez, J, Fuster, O, Colomer, D, Chillon, C, Larrayoz, MJ, Sanchez-Godoy, P, Gonzalez-Campos, J, Manso, F, Amador, ML, Vellenga, E, Löwenberg, Bob, and Sanz, MA

Abstract

Background Fms-like tyrosine kinase-3 (FLT3) gene mutations are frequent in acute promyelocytic leukemia but their prognostic value is not well established. Design and Methods We evaluated FLT3-internal tandem duplication and FLT3-D835 mutations in patients treated with all-trans retinoic acid and anthracycline-based chemotherapy enrolled in two subsequent trials of the Programa de Estudio y Tratamiento de las Hemopatias Malignas (PETHEMA) and Hemato-Oncologie voor Volwassenen Nederland (HOVON) groups between 1996 and 2005. Results FLT3-internal tandem duplication and FLT3-D835 mutation status was available for 306 (41%) and 213 (29%) patients, respectively. Sixty-eight (22%) and 20 (9%) patients had internal tandem duplication and D835 mutations, respectively. Internal tandem duplication was correlated with higher white blood cell and blast counts, lactate dehydrogenase, relapse-risk score, fever, hemorrhage, coagulopathy, BCR3 isoform, M3 variant subtype, and expression of CD2, CD34, human leukocyte antigen-DR, and CD11b surface antigens. The FLT3-D835 mutation was not significantly associated with any clinical or biological characteristic. Univariate analysis showed higher relapse and lower survival rates in patients with a FLT3-internal tandem duplication, while no impact was observed in relation to FLT3-D835. The prognostic value of the FLT3-internal tandem duplication was not retained in the multivariate analysis. Conclusions FLT3-internal tandem duplication mutations are associated with several hematologic features in acute promyelocytic leukemia, in particular with high white blood cell counts, but we were unable to demonstrate an independent prognostic value in patients with acute promyelocytic leukemia treated with all-trans retinoic acid and anthracycline-based regimens.

Published
2011

13. Expanded and highly active proliferation centers identify a histological subtype of chronic lymphocytic leukemia ("accelerated" chronic lymphocytic leukemia) with aggressive clinical behavior

Author

Gine, E., primary, Martinez, A., additional, Villamor, N., additional, Lopez-Guillermo, A., additional, Camos, M., additional, Martinez, D., additional, Esteve, J., additional, Calvo, X., additional, Muntanola, A., additional, Abrisqueta, P., additional, Rozman, M., additional, Rozman, C., additional, Bosch, F., additional, Campo, E., additional, and Montserrat, E., additional

Published
2010
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16. Clonal dynamics in pediatric B-cell precursor acute lymphoblastic leukemia with very early relapse

Author

Lionel Morgado, Jean-Pierre Bourquin, Mireia Camós, Hélène Cavé, Cedric G. van der Ham, Esmé Waanders, Peter M. Hoogerbrugge, Simon V. van Reijmersdal, Roland P. Kuiper, Cornelia Eckert, Željko Antić, Ad Geurts van Kessel, Beat Bornhauser, Anthony V. Moorman, Rosemary Sutton, Giovanni Cazzaniga, Frank N. van Leeuwen, Sarah Elitzur, Edwin Sonneveld, Stefan H. Lelieveld, Jiangyan Yu, Antic, Z, Yu, J, Bornhauser, B, Lelieveld, S, van der Ham, C, van Reijmersdal, S, Morgado, L, Elitzur, S, Bourquin, J, Cazzaniga, G, Eckert, C, Camos, M, Sutton, R, Cave, H, Moorman, A, Sonneveld, E, Geurts van Kessel, A, van Leeuwen, F, Hoogerbrugge, P, Waanders, E, Kuiper, R, University of Zurich, and Kuiper, Roland P

Subjects
Oncology, medicine.medical_specialty, Lymphoblastic Leukemia, 2720 Hematology, Clone (cell biology), lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Graft vs Host Disease, 610 Medicine & health, pediatric acute lymphoblastic leukemia, clonal dynamics, Somatic evolution in cancer, very early relapse, Clonal Evolution, Recurrence, Internal medicine, medicine, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Humans, 2735 Pediatrics, Perinatology and Child Health, TP53, Allele, RAD21, Child, WHSC1, B cell, business.industry, Wild type, Hematology, Genomics, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Prognosis, Minimal residual disease, Leukemia, medicine.anatomical_structure, 10036 Medical Clinic, Pediatrics, Perinatology and Child Health, 2730 Oncology, business, clonal dynamic
Abstract

Contains fulltext : 248362.pdf (Publisher’s version ) (Open Access) INTRODUCTION: One-quarter of the relapses in children with B-cell precursor acute lymphoblastic leukemia (BCP-ALL) occur very early (within 18 months, before completion of treatment), and prognosis in these patients is worse compared to cases that relapse after treatment has ended. METHODS: In this study, we performed a genomic analysis of diagnosis-relapse pairs of 12 children who relapsed very early, followed by a deep-sequencing validation of all identified mutations. In addition, we included one case with a good initial treatment response and on-treatment relapse at the end of upfront therapy. RESULTS: We observed a dynamic clonal evolution in all cases, with relapse almost exclusively originating from a subclone at diagnosis. We identified several driver mutations that may have influenced the outgrowth of a minor clone at diagnosis to become the major clone at relapse. For example, a minimal residual disease (MRD)-based standard-risk patient with ETV6-RUNX1-positive leukemia developed a relapse from a TP53-mutated subclone after loss of the wildtype allele. Furthermore, two patients with TCF3-PBX1-positive leukemia that developed a very early relapse carried E1099K WHSC1 mutations at diagnosis, a hotspot mutation that was recurrently encountered in other very early TCF3-PBX1-positive leukemia relapses as well. In addition to alterations in known relapse drivers, we found two cases with truncating mutations in the cohesin gene RAD21. CONCLUSION: Comprehensive genomic characterization of diagnosis-relapse pairs shows that very early relapses in BCP-ALL frequently arise from minor subclones at diagnosis. A detailed understanding of the therapeutic pressure driving these events may aid the development of improved therapies.

Published
2022

17. CircRNAome of Childhood Acute Lymphoblastic Leukemia: Deciphering Subtype-Specific Expression Profiles and Involvement in TCF3::PBX1 ALL.

Author

Gutierrez-Camino A, Caron M, Richer C, Fuchs C, Illarregi U, Poncelet L, St-Onge P, Bataille AR, Tremblay-Dauphinais P, Lopez-Lopez E, Camos M, Ramirez-Orellana M, Astigarraga I, Lécuyer É, Bourque G, Martin-Guerrero I, and Sinnett D

Subjects
Humans, Basic Helix-Loop-Helix Transcription Factors genetics, Oncogene Proteins, Fusion genetics, MicroRNAs, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma metabolism, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, RNA, Circular genetics
Abstract

Childhood B-cell acute lymphoblastic leukemia (B-ALL) is a heterogeneous disease comprising multiple molecular subgroups with subtype-specific expression profiles. Recently, a new type of ncRNA, termed circular RNA (circRNA), has emerged as a promising biomarker in cancer, but little is known about their role in childhood B-ALL. Here, through RNA-seq analysis in 105 childhood B-ALL patients comprising six genetic subtypes and seven B-cell controls from two independent cohorts we demonstrated that circRNAs properly stratified B-ALL subtypes. By differential expression analysis of each subtype vs. controls, 156 overexpressed and 134 underexpressed circRNAs were identified consistently in at least one subtype, most of them with subtype-specific expression. TCF3::PBX1 subtype was the one with the highest number of unique and overexpressed circRNAs, and the circRNA signature could effectively discriminate new patients with TCF3::PBX1 subtype from others. Our results indicated that NUDT21 , an RNA-binding protein (RBP) involved in circRNA biogenesis, may contribute to this circRNA enrichment in TCF3::PBX1 ALL. Further functional characterization using the CRISPR-Cas13d system demonstrated that circBARD1 , overexpressed in TCF3::PBX1 patients and regulated by NUDT21 , might be involved in leukemogenesis through the activation of p38 via hsa-miR-153-5p . Our results suggest that circRNAs could play a role in the pathogenesis of childhood B-ALL.

Published
2024
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18. Maternal Lifestyle and Prenatal Risk Factors for Childhood Leukemia: A Review of the Existing Evidence.

Author

Benítez L, Castro-Barquero S, Crispi F, Youssef L, Crovetto F, Fischer U, Kameri E, Bueno C, Camos M, Menéndez P, Heinäniemi M, Borkhardt A, and Gratacós E

Subjects
Humans, Pregnancy, Risk Factors, Female, Child, Child, Preschool, Life Style, Prenatal Exposure Delayed Effects epidemiology, Leukemia epidemiology, Leukemia etiology
Abstract

Background: Acute leukemia is the most common pediatric cancer, with an incidence peak at 2-5 years of age. Despite the medical advances improving survival rates, children suffer from significant side effects of treatments as well as its high social and economic impact. The frequent prenatal origin of this developmental disease follows the two-hit carcinogenesis model established in the 70s: a first hit in prenatal life with the creation of genetic fusion lesions or aneuploidy in hematopoietic progenitor/stem cells, and usually a second hit in the pediatric age that converts the preleukemic clone into clinical leukemia. Previous research has mostly focused on postnatal environmental factors triggering the second hit., Summary: There is scarce evidence on prenatal risk factors associated with the first hit. Mainly retrospective case-control studies suggested several environmental and lifestyle determinants as risk factors. If these associations could be confirmed, interventions focused on modifying prenatal factors might influence the subsequent risk of leukemia during childhood and reveal unexplored research avenues for the future. In this review, we aim to comprehensively summarize the currently available evidence on prenatal risk factors for the development of childhood leukemia. According to the findings of this review, parental age, ethnicity, maternal diet, folate intake, alcohol consumption, X-ray exposure, pesticides, perinatal infections, and fetal growth may have a significant role in the appearance of preleukemic lesions during fetal life. Other factors such as socioeconomic status, consumption of caffeinated beverages, and smoking consumption have been suggested with inconclusive evidence. Additionally, investigating the association between prenatal factors and genetic lesions associated with childhood leukemia at birth is crucial. Prospective studies evaluating the link between lifestyle factors and genetic alterations could provide indirect evidence supporting new research avenues for leukemia prevention. Maternal diet and lifestyle factors are modifiable determinants associated with adverse perinatal outcomes that could be also related to preleukemic lesions., Key Messages: Parental age, ethnicity, maternal diet, folate intake, alcohol consumption, X-ray exposure, pesticides, perinatal infections, and fetal growth may have a significant role in the appearance of preleukemic lesions during fetal life. Dedicating efforts to studying maternal lifestyle during pregnancy and its association with genetic lesions leading to childhood leukemia could lead to novel prevention strategies., (© 2024 S. Karger AG, Basel.)

Published
2024
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19. Fratricide-resistant CD1a-specific CAR T cells for the treatment of cortical T-cell acute lymphoblastic leukemia.

Author

Sánchez-Martínez D, Baroni ML, Gutierrez-Agüera F, Roca-Ho H, Blanch-Lombarte O, González-García S, Torrebadell M, Junca J, Ramírez-Orellana M, Velasco-Hernández T, Bueno C, Fuster JL, Prado JG, Calvo J, Uzan B, Cools J, Camos M, Pflumio F, Toribio ML, and Menéndez P

Subjects
Animals, Humans, Jurkat Cells, Mice, Xenograft Model Antitumor Assays, Antigens, CD1 immunology, Drug Resistance, Neoplasm immunology, Immunotherapy, Adoptive, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma immunology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma pathology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma therapy, Receptors, Chimeric Antigen immunology
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., (© 2019 by The American Society of Hematology.)

Published
2019
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20. Activated KRAS Cooperates with MLL-AF4 to Promote Extramedullary Engraftment and Migration of Cord Blood CD34+ HSPC But Is Insufficient to Initiate Leukemia.

Author

Prieto C, Stam RW, Agraz-Doblas A, Ballerini P, Camos M, Castaño J, Marschalek R, Bursen A, Varela I, Bueno C, and Menendez P

Subjects
Animals, Heterografts, Humans, Leukemia pathology, Mice, Antigens, CD34 blood, DNA-Binding Proteins metabolism, Fetal Blood immunology, Genes, ras, Hematopoietic Stem Cells pathology, Leukemia genetics, Myeloid-Lymphoid Leukemia Protein metabolism, Transcriptional Elongation Factors metabolism
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 KRAS(G12V) 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. Cancer Res; 76(8); 2478-89. ©2016 AACR., (©2016 American Association for Cancer Research.)

Published
2016
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21. Prognostic value of FLT3 mutations in patients with acute promyelocytic leukemia treated with all-trans retinoic acid and anthracycline monochemotherapy.

Author

Barragán E, Montesinos P, Camos M, González M, Calasanz MJ, Román-Gómez J, Gómez-Casares MT, Ayala R, López J, Fuster Ó, Colomer D, Chillón C, Larrayoz MJ, Sánchez-Godoy P, González-Campos J, Manso F, Amador ML, Vellenga E, Lowenberg B, and Sanz MA

Subjects
Adolescent, Adult, Aged, Child, Female, Humans, Leukemia, Promyelocytic, Acute genetics, Leukemia, Promyelocytic, Acute mortality, Male, Middle Aged, Prognosis, Remission Induction, Survival Analysis, Treatment Outcome, Young Adult, Anthracyclines therapeutic use, Antineoplastic Agents therapeutic use, Leukemia, Promyelocytic, Acute drug therapy, Mutation, Tretinoin therapeutic use, fms-Like Tyrosine Kinase 3 genetics
Abstract

Background: Fms-like tyrosine kinase-3 (FLT3) gene mutations are frequent in acute promyelocytic leukemia but their prognostic value is not well established., Design and Methods: We evaluated FLT3-internal tandem duplication and FLT3-D835 mutations in patients treated with all-trans retinoic acid and anthracycline-based chemotherapy enrolled in two subsequent trials of the Programa de Estudio y Tratamiento de las Hemopatías Malignas (PETHEMA) and Hemato-Oncologie voor Volwassenen Nederland (HOVON) groups between 1996 and 2005., Results: FLT3-internal tandem duplication and FLT3-D835 mutation status was available for 306 (41%) and 213 (29%) patients, respectively. Sixty-eight (22%) and 20 (9%) patients had internal tandem duplication and D835 mutations, respectively. Internal tandem duplication was correlated with higher white blood cell and blast counts, lactate dehydrogenase, relapse-risk score, fever, hemorrhage, coagulopathy, BCR3 isoform, M3 variant subtype, and expression of CD2, CD34, human leukocyte antigen-DR, and CD11b surface antigens. The FLT3-D835 mutation was not significantly associated with any clinical or biological characteristic. Univariate analysis showed higher relapse and lower survival rates in patients with a FLT3-internal tandem duplication, while no impact was observed in relation to FLT3-D835. The prognostic value of the FLT3-internal tandem duplication was not retained in the multivariate analysis., Conclusions: FLT3-internal tandem duplication mutations are associated with several hematologic features in acute promyelocytic leukemia, in particular with high white blood cell counts, but we were unable to demonstrate an independent prognostic value in patients with acute promyelocytic leukemia treated with all-trans retinoic acid and anthracycline-based regimens.

Published
2011
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22. Clonally related follicular lymphomas and histiocytic/dendritic cell sarcomas: evidence for transdifferentiation of the follicular lymphoma clone.

Author

Feldman AL, Arber DA, Pittaluga S, Martinez A, Burke JS, Raffeld M, Camos M, Warnke R, and Jaffe ES

Subjects
Adult, Aged, Cell Differentiation, Cell Lineage, Cell Transdifferentiation, Dendritic Cells, Follicular pathology, Dendritic Cells, Follicular physiology, Female, Gene Expression Regulation, Neoplastic, Gene Rearrangement, Humans, Immunohistochemistry, Immunophenotyping, In Situ Hybridization, Fluorescence, Male, Middle Aged, Neoplasms, Second Primary genetics, Neoplasms, Second Primary pathology, Polymerase Chain Reaction, Dendritic Cell Sarcoma, Follicular genetics, Dendritic Cell Sarcoma, Follicular pathology, Histiocytic Sarcoma genetics, Histiocytic Sarcoma pathology, Lymphoma, Follicular genetics, Lymphoma, Follicular pathology
Abstract

Rare cases of histiocytic and dendritic cell (H/DC) neoplasms have been reported in patients with follicular lymphoma (FL), but the biologic relationship between the 2 neoplasms is unknown. We studied 8 patients with both FL and H/DC neoplasms using immunohistochemistry, fluorescence in situ hybridization (FISH) for t(14;18), and polymerase chain reaction (PCR)/sequencing of BCL2 and IGH rearrangements. There were 5 men and 3 women (median age, 59 years). All cases of FL were positive for t(14;18). The H/DC tumors included 7 histiocytic sarcomas, 5 of which showed evidence of dendritic differentiation, and 1 interdigitating cell sarcoma. Five H/DC tumors were metachronous, following FL by 2 months to 12 years; tumors were synchronous in 3. All 8 H/DC tumors showed presence of the t(14;18) either by FISH, or in 2 cases by PCR with the major breakpoint region (MBR) probe. PCR and sequencing identified identical IGH gene rearrangements or BCL2 gene breakpoints in all patients tested. All H/DC tumors lacked PAX5, and up-regulation of CEBPbeta and PU.1 was seen in all cases tested. These results provide evidence for a common clonal origin of FL and H/DC neoplasms when occurring in the same patient, and suggest that lineage plasticity may occur in mature lymphoid neoplasms.

Published
2008
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