Your search keyword '"Riesco, Susana"' showing total 48 results

1. Immune stress suppresses innate immune signaling in preleukemic precursor B-cells to provoke leukemia in predisposed mice

Author

Isidro-Hernández, Marta, Casado-García, Ana, Oak, Ninad, Alemán-Arteaga, Silvia, Ruiz-Corzo, Belén, Martínez-Cano, Jorge, Mayado, Andrea, Sánchez, Elena G., Blanco, Oscar, Gaspar, Ma Luisa, Orfao, Alberto, Alonso-López, Diego, De Las Rivas, Javier, Riesco, Susana, Prieto-Matos, Pablo, González-Murillo, África, Criado, Francisco Javier García, Cenador, María Begoña García, Ramírez-Orellana, Manuel, de Andrés, Belén, Vicente-Dueñas, Carolina, Cobaleda, César, Nichols, Kim E., and Sánchez-García, Isidro

Published

2023

2. Outcome of haematopoietic cell transplantation in children with lysosomal acid lipase deficiency: a study on behalf of the EBMT Inborn Errors Working Party

Author

Lum, Su Han, Minkov, Milen, Jones, Simon A., Hazelaar, Sheree, Sirait, Tiarlan, Potter, Jane E., Stepensky, Polina, Garban, Frederic, Pichler, Herbert, Stein, Jerry, Kaya, Zuhre, Schulz, Ansgar, Mellgren, Karin, Diaz de Heredia, Cristina, Pochon, Cecile, Riesco, Susana, Diaz, Miguel Angel, Michel, Gérard, Lindemans, Caroline, Gruhn, Bernd, Albert, Michael H., Lankester, Arjan C., Neven, Bénédicte, and Wynn, Robert

Published

2023

3. Mutually-Exclusive Pathways between IKZF1 plus and RAS Mutations and TP53 double-Hit Alterations Lead Relapse in B-Other, Ph-like and Hyperdiploidy Genetic Groups in Adult B-Cell Acute Lymphoblastic Leukemia

Author

Navas Acosta, Josgrey Del Valle Del Valle, primary, González, Teresa, additional, Serramito-Gómez, Inmaculada, additional, Villaverde Ramiro, Angela, additional, Miguel-García, Cristina, additional, Santos-Mínguez, Sandra, additional, Ribera, Jordi, additional, Granada, Isabel, additional, Morgades, Mireia, additional, Sanchez, Ricardo, additional, Such, Esperanza, additional, Barrera, Susana, additional, Ciudad, Juana, additional, Orfao, Alberto, additional, Valls, Julio Davila, additional, De Las Heras, Natalia, additional, Fuster, José, additional, Garcia de Coca, Alfonso, additional, Labrador, Jorge, additional, Queizan Hernandez, Jose Antonio, additional, Mendoza, María Carmen, additional, Riesco, Susana, additional, Martín, Sandra, additional, Ribera, Josep-Maria, additional, Benito Sanchez, Maria Rocio, additional, and Hernández-Rivas, Jesús María, additional

Published

2023

4. Lessons from mouse models in the impact of risk factors on the genesis of childhood B-cell leukemia

Author

Casado-García, Ana, primary, Isidro-Hernández, Marta, additional, Alemán-Arteaga, Silvia, additional, Ruiz-Corzo, Belén, additional, Riesco, Susana, additional, Prieto-Matos, Pablo, additional, Sánchez, Lucía, additional, Sánchez-García, Isidro, additional, and Vicente-Dueñas, Carolina, additional

Published

2023

5. P343: MUTATIONS IN GENES RELATED TO EPIGENETIC REGULATION, TREATMENT RESISTANCE AND IKZF1 PLUS PROFILE IDENTIFY RELAPSE PROFILES IN B-ALL.

Author

del Valle Navas Acosta, Josgrey, primary, Gonzalez, Teresa, additional, Serramito, Inmaculada, additional, Miguel, Cristina, additional, Santos, Sandra, additional, Villaverde, Angela, additional, Ribera, Jordi, additional, Granada, Isabel, additional, Morgades, Mireia, additional, Sánchez, Ricardo, additional, Such, Esperanza, additional, Barrera, Susana, additional, Ciudad, Juana, additional, Orfao, Alberto, additional, Maria Ribera, Josep, additional, Dávila Valls, Julio, additional, De Las Heras Rodriguez, Natalia, additional, Luis Fuster, José, additional, García de Coca, Alfonso, additional, Labrador, Jorge, additional, Antonio Queizan, Jose, additional, Carmen Mendoza, Mª, additional, Riesco, Susana, additional, Benito, Rocío, additional, and Hernández Rivas, Jesus, additional

Published

2023

6. Supplementary Data from Transient Inhibition of the JAK/STAT Pathway Prevents B-ALL Development in Genetically Predisposed Mice

Author

Casado-García, Ana, primary, Isidro-Hernández, Marta, primary, Oak, Ninad, primary, Mayado, Andrea, primary, Mann-Ran, Christine, primary, Raboso-Gallego, Javier, primary, Alemán-Arteaga, Silvia, primary, Buhles, Alexandra, primary, Sterker, Dario, primary, Sánchez, Elena G., primary, Martínez-Cano, Jorge, primary, Blanco, Oscar, primary, Orfao, Alberto, primary, Alonso-López, Diego, primary, De Las Rivas, Javier, primary, Riesco, Susana, primary, Prieto-Matos, Pablo, primary, González-Murillo, África, primary, García Criado, Francisco Javier, primary, García Cenador, María Begoña, primary, Radimerski, Thomas, primary, Ramírez-Orellana, Manuel, primary, Cobaleda, César, primary, Yang, Jun J., primary, Vicente-Dueñas, Carolina, primary, Weiss, Andreas, primary, Nichols, Kim E., primary, and Sánchez-García, Isidro, primary

Published

2023

7. Data from Transient Inhibition of the JAK/STAT Pathway Prevents B-ALL Development in Genetically Predisposed Mice

Author

Casado-García, Ana, primary, Isidro-Hernández, Marta, primary, Oak, Ninad, primary, Mayado, Andrea, primary, Mann-Ran, Christine, primary, Raboso-Gallego, Javier, primary, Alemán-Arteaga, Silvia, primary, Buhles, Alexandra, primary, Sterker, Dario, primary, Sánchez, Elena G., primary, Martínez-Cano, Jorge, primary, Blanco, Oscar, primary, Orfao, Alberto, primary, Alonso-López, Diego, primary, De Las Rivas, Javier, primary, Riesco, Susana, primary, Prieto-Matos, Pablo, primary, González-Murillo, África, primary, García Criado, Francisco Javier, primary, García Cenador, María Begoña, primary, Radimerski, Thomas, primary, Ramírez-Orellana, Manuel, primary, Cobaleda, César, primary, Yang, Jun J., primary, Vicente-Dueñas, Carolina, primary, Weiss, Andreas, primary, Nichols, Kim E., primary, and Sánchez-García, Isidro, primary

Published

2023

8. Lessons from mouse models in the impact of risk factors on the genesis of childhood B-cell leukemia

Author

Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia e Innovación (España), Junta de Castilla y León, Fundación Unoentrecienmil, Fundación Científica Asociación Española Contra el Cáncer, Universidad de Salamanca, Banco Santander, Casado-García, Ana, Isidro‑Hernández, Marta, Alemán-Arteaga, Silvia, Ruiz-Corzo, Belén, Riesco, Susana, Prieto-Matos, Pablo, Sánchez, Lucía, Sánchez-García, Isidro, Vicente-Dueñas, Carolina, Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia e Innovación (España), Junta de Castilla y León, Fundación Unoentrecienmil, Fundación Científica Asociación Española Contra el Cáncer, Universidad de Salamanca, Banco Santander, Casado-García, Ana, Isidro‑Hernández, Marta, Alemán-Arteaga, Silvia, Ruiz-Corzo, Belén, Riesco, Susana, Prieto-Matos, Pablo, Sánchez, Lucía, Sánchez-García, Isidro, and Vicente-Dueñas, Carolina

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) stands as the primary contributor to childhood cancer-related mortality on a global scale. The development of the most conventional forms of this disease has been proposed to be conducted by two different steps influenced by different types of risk factors. The first step is led by a genetic insult that is presumably acquired before birth that transforms a healthy cell into a preleukemic one, which is maintained untransformed until the second step takes place. This necessary next step to leukemia development will be triggered by different risk factors to which children are exposed after birth. Murine models that recap the stepwise progression of B-ALL have been instrumental in identifying environmental and genetic factors that contribute to disease risk. Recent evidence from these models has demonstrated that specific environmental risk factors, such as common infections or gut microbiome dysbiosis, induce immune stress, driving the transformation of preleukemic cells, and harboring genetic alterations, into fully transformed leukemic cells. Such models serve as valuable tools for investigating the mechanisms underlying preleukemic events and can aid in the development of preventive approaches for leukemia in child. Here, we discuss the existing knowledge, learned from mouse models, of the impact of genetic and environmental risk factors on childhood B-ALL evolution and how B-ALL prevention could be reached by interfering with preleukemic cells.

Published

2023

9. Immune stress suppresses innate immune signaling in preleukemic precursor B-cells to provoke leukemia in predisposed mice

Author

Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Fundación Ramón Areces, Banco Santander, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Asociación Española Contra el Cáncer, Isidro‑Hernández, Marta, Casado-García, Ana, Oak, Ninad, Alemán-Arteaga, Silvia, Ruiz-Corzo, Belén, Martínez-Cano, Jorge, Mayado, Andrea, Sánchez, Elena G, Blanco, Oscar, Gaspar, Ma Luisa, Orfao, Alberto, Alonso-López, Diego, De Las Rivas, Javier, Riesco, Susana, Prieto-Matos, Pablo, González-Murillo, África, Criado, Francisco Javier García, Cenador, María Begoña García, Ramírez-Orellana, Manuel, de Andrés, Belén, Vicente-Dueñas, Carolina, Cobaleda, César, Nichols, Kim E, Sánchez García, Isidro, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), European Commission, Fundación Ramón Areces, Banco Santander, Instituto de Salud Carlos III, Ministerio de Economía y Competitividad (España), Junta de Castilla y León, Asociación Española Contra el Cáncer, Isidro‑Hernández, Marta, Casado-García, Ana, Oak, Ninad, Alemán-Arteaga, Silvia, Ruiz-Corzo, Belén, Martínez-Cano, Jorge, Mayado, Andrea, Sánchez, Elena G, Blanco, Oscar, Gaspar, Ma Luisa, Orfao, Alberto, Alonso-López, Diego, De Las Rivas, Javier, Riesco, Susana, Prieto-Matos, Pablo, González-Murillo, África, Criado, Francisco Javier García, Cenador, María Begoña García, Ramírez-Orellana, Manuel, de Andrés, Belén, Vicente-Dueñas, Carolina, Cobaleda, César, Nichols, Kim E, and Sánchez García, Isidro

Abstract

The initial steps of B-cell acute lymphoblastic leukemia (B-ALL) development usually pass unnoticed in children. Several preclinical studies have shown that exposure to immune stressors triggers the transformation of preleukemic B cells to full-blown B-ALL, but how this takes place is still a longstanding and unsolved challenge. Here we show that dysregulation of innate immunity plays a driving role in the clonal evolution of pre-malignant Pax5 B-cell precursors toward leukemia. Transcriptional profiling reveals that Myd88 is downregulated in immune-stressed pre-malignant B-cell precursors and in leukemic cells. Genetic reduction of Myd88 expression leads to a significant increase in leukemia incidence in Pax5 Myd88 mice through an inflammation-dependent mechanism. Early induction of Myd88-independent Toll-like receptor 3 signaling results in a significant delay of leukemia development in Pax5 mice. Altogether, these findings identify a role for innate immunity dysregulation in leukemia, with important implications for understanding and therapeutic targeting of the preleukemic state in children.

Published

2023

10. Outcomes of patients undergoing allogeneic haematopoietic stem cell transplantation for congenital amegakaryocytic thrombocytopenia; a study on behalf of the PDWP of the EBMT

Author

Aldebert, Clémence, Fahd, Mony, Galimard, Jacques-Emmanuel, Ghemlas, Ibrahim A., Zecca, Marco, Silva, Juliana, Mohseny, Alexander, Kupesiz, Alphan, Hamladji, Rose-Marie, Miranda, Nuno, Güngör, Tayfun, Wynn, Robert F., Merli, Pietro, Sundin, Mikael, Faraci, Maura, Diaz-de-Heredia, Cristina, Burkhardt, Birgit, Bordon, Victoria, Angoso, Marie, Bader, Peter, Ifversen, Marianne, Herrera Arroyo, Concepcion, Maximova, Natalia, Riesco, Susana, Stein, Jerry, Dalissier, Arnaud, Locatelli, Franco, Kalwak, Krzysztof, Dalle, Jean-Hugues, and Corbacioglu, Selim

Abstract

Congenital amegakaryocytic thrombocytopenia is a rare, inherited bone marrow failure syndrome. Allogeneic haematopoietic stem cell transplantation (allo-HSCT) is currently the only curative treatment. In this retrospective study, we analysed 66 patients with allo-HSCT, reported in the European Society for Blood and Marrow Transplantation (EBMT) registry. Bone marrow (BM) was the most widely used stem cell source (n= 40; 61%) followed by peripheral blood (PB) (n= 18; 27%), and unrelated umbilical cord blood (UCB) (n= 8; 12%). Most frequently was a HLA-matched graft from related (n= 26; 39%) and unrelated (n= 15; 23%) donors after a myeloablative busulfan-based conditioning regimen. GvHD prophylaxis was mostly cyclosporine and methotrexate (53%). The 6-year cumulative incidence of graft-failure and second transplant were 25% and 17%, respectively. The 6-year disease-free survival (DFS) and overall survival (OS) were 66.9% and 85.6%, respectively. The 6-year transplant-related mortality (TRM) was 8.0%. In conclusion, most patients with CAMT benefit from allo-HSCT, but with many graft failures.

Published

2024

11. Outcomes of Allogeneic Hematopoietic Stem Cell Transplantation for Congenital Amegakaryocytic Thrombocytopenia, a PDWP/EBMT Study

Author

Aldebert, Clemence, primary, Fahd, Mony, additional, Galimard, Jacques-Emmanuel, additional, Ghemlas, Ibrahim A., additional, Zecca, Marco, additional, Silva, Juliana, additional, Mohseny, Alexander, additional, Kupesiz, Alphan, additional, Hamladji, Rose-Marie, additional, Miranda, Nuno, additional, Gungor, Tayfun, additional, Wynn, Robert F, additional, Merli, Pietro, additional, Sundin, Mikael, additional, Faraci, Maura, additional, Díaz-de-Heredia, Cristina, additional, Burkhardt, Birgit, additional, Bordon, Victoria, additional, Jubert, Charlotte, additional, Bader, Peter, additional, Ifversen, Marianne, additional, Herrera Arroyo, Concepcion, additional, Maximova, Natalia, additional, Riesco, Susana, additional, Stein, Jerry, additional, Dalissier, Arnaud, additional, Locatelli, Franco, additional, Kalwak, Krzysztof, additional, Dalle, Jean-Hugues, additional, and Corbacioglu, Selim, additional

Published

2022

12. Childhood B-Cell Preleukemia Mouse Modeling

Author

Isidro-Hernández, Marta, primary, Alemán-Arteaga, Silvia, additional, Casado-García, Ana, additional, Ruiz-Corzo, Belén, additional, Riesco, Susana, additional, Prieto-Matos, Pablo, additional, Martínez-Cano, Jorge, additional, Sánchez, Lucía, additional, Cobaleda, César, additional, Sánchez-García, Isidro, additional, and Vicente-Dueñas, Carolina, additional

Published

2022

13. Transient inhibition of the JAK/STAT pathway prevents B-ALL development in genetically predisposed mice

Author

European Commission, Instituto de Salud Carlos III, American Lebanese Syrian Associated Charities, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Junta de Castilla y León, Fundación Unoentrecienmil, Asociación Española Contra el Cáncer, Universidad de Salamanca, Banco Santander, Casado-García, Ana, Isidro‑Hernández, Marta, Oak, Ninad, Mayado, Andrea, Mann-Ran, Christine, Raboso-Gallego, Javier, Alemán-Arteaga, Silvia, Buhles, Alexandra, Sterker, Dario, Sánchez, Elena G., Martínez-Cano, Jorge, Blanco, Óscar, Orfao, Alberto, Alonso-López, D., De Las Rivas, Javier, Riesco, Susana, Prieto-Matos, Pablo, González-Murillo, África, García-Criado, Francisco Javier, García-Cenador, Begoña, Radimerski, Thomas, Ramírez‑Orellana, Manuel, Cobaleda, César, Yang, Jun J., Vicente-Dueñas, Carolina, Weiss, Andreas, Nichols, Kim E., Sánchez García, Isidro, European Commission, Instituto de Salud Carlos III, American Lebanese Syrian Associated Charities, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Junta de Castilla y León, Fundación Unoentrecienmil, Asociación Española Contra el Cáncer, Universidad de Salamanca, Banco Santander, Casado-García, Ana, Isidro‑Hernández, Marta, Oak, Ninad, Mayado, Andrea, Mann-Ran, Christine, Raboso-Gallego, Javier, Alemán-Arteaga, Silvia, Buhles, Alexandra, Sterker, Dario, Sánchez, Elena G., Martínez-Cano, Jorge, Blanco, Óscar, Orfao, Alberto, Alonso-López, D., De Las Rivas, Javier, Riesco, Susana, Prieto-Matos, Pablo, González-Murillo, África, García-Criado, Francisco Javier, García-Cenador, Begoña, Radimerski, Thomas, Ramírez‑Orellana, Manuel, Cobaleda, César, Yang, Jun J., Vicente-Dueñas, Carolina, Weiss, Andreas, Nichols, Kim E., and Sánchez García, Isidro

Abstract

Preventing development of childhood B-cell acute lymphoblastic leukemia (B-ALL), a disease with devastating effects, is a longstanding and unsolved challenge. Heterozygous germline alterations in the PAX5 gene can lead to B-ALL upon accumulation of secondary mutations affecting the JAK/STAT signaling pathway. Preclinical studies have shown that this malignant transformation occurs only under immune stress such as exposure to infectious pathogens. Here we show in Pax5+/− mice that transient, early-life administration of clinically relevant doses of ruxolitinib, a JAK1/2 inhibitor, significantly mitigates the risk of B-ALL following exposure to infection; 1 of 29 animals treated with ruxolitinib developed B-ALL versus 8 of 34 untreated mice. Ruxolitinib treatment preferentially targeted Pax5+/− versus wild-type B-cell progenitors and exerted unique effects on the Pax5+/− B-cell progenitor transcriptional program. These findings provide the first in vivo evidence for a potential strategy to prevent B-ALL development.

Published

2022

14. Childhood B-Cell Preleukemia Mouse Modeling

Author

Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Junta de Castilla y León, Fundación Unoentrecienmil, Asociación Española Contra el Cáncer, Ministerio de Ciencia e Innovación (España), Fundación Ramón Areces, Banco Santander, Asociación Española del Síndrome de Wolf-Hirschhorn, Universidad de Salamanca, Isidro‑Hernández, Marta, Alemán-Arteaga, Silvia, Casado-García, Ana, Ruiz-Corzo, Belén, Riesco, Susana, Prieto-Matos, Pablo, Martínez-Cano, Jorge, Sánchez, Lucía, Cobaleda, César, Sánchez García, Isidro, Vicente-Dueñas, Carolina, Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Junta de Castilla y León, Fundación Unoentrecienmil, Asociación Española Contra el Cáncer, Ministerio de Ciencia e Innovación (España), Fundación Ramón Areces, Banco Santander, Asociación Española del Síndrome de Wolf-Hirschhorn, Universidad de Salamanca, Isidro‑Hernández, Marta, Alemán-Arteaga, Silvia, Casado-García, Ana, Ruiz-Corzo, Belén, Riesco, Susana, Prieto-Matos, Pablo, Martínez-Cano, Jorge, Sánchez, Lucía, Cobaleda, César, Sánchez García, Isidro, and Vicente-Dueñas, Carolina

Abstract

Leukemia is the most usual childhood cancer, and B-cell acute lymphoblastic leukemia (B-ALL) is its most common presentation. It has been proposed that pediatric leukemogenesis occurs through a “multi-step” or “multi-hit” mechanism that includes both in utero and postnatal steps. Many childhood leukemia-initiating events, such as chromosomal translocations, originate in utero, and studies so far suggest that these “first-hits” occur at a far higher frequency than the incidence of childhood leukemia itself. The reason why only a small percentage of the children born with such preleukemic “hits” will develop full-blown leukemia is still a mystery. In order to better understand childhood leukemia, mouse modeling is essential, but only if the multistage process of leukemia can be recapitulated in the model. Therefore, mouse models naturally reproducing the “multi-step” process of childhood B-ALL will be essential to identify environmental or other factors that are directly linked to increased risk of disease.

Published

2022

15. Pancitopenia: valoración clínica y diagnóstica

Author

Rubio Aparicio, Pedro M. and Riesco, Susana Riesco

Published

2012

16. Transient Inhibition of the JAK/STAT Pathway Prevents B-ALL Development in Genetically Predisposed Mice

Author

Casado-García, Ana, primary, Isidro-Hernández, Marta, additional, Oak, Ninad, additional, Mayado, Andrea, additional, Mann-Ran, Christine, additional, Raboso-Gallego, Javier, additional, Alemán-Arteaga, Silvia, additional, Buhles, Alexandra, additional, Sterker, Dario, additional, Sánchez, Elena G., additional, Martínez-Cano, Jorge, additional, Blanco, Oscar, additional, Orfao, Alberto, additional, Alonso-López, Diego, additional, De Las Rivas, Javier, additional, Riesco, Susana, additional, Prieto-Matos, Pablo, additional, González-Murillo, África, additional, García Criado, Francisco Javier, additional, García Cenador, María Begoña, additional, Radimerski, Thomas, additional, Ramírez-Orellana, Manuel, additional, Cobaleda, César, additional, Yang, Jun J., additional, Vicente-Dueñas, Carolina, additional, Weiss, Andreas, additional, Nichols, Kim E., additional, and Sánchez-García, Isidro, additional

Published

2022

17. Cáncer de tiroides en pediatría

Author

Prieto-Matos, Pablo, primary, Martín-Hernández, Diana, additional, Martín-Alonso, Montserrat, additional, Bajo-Delgado, Ana Fe, additional, Riesco-Riesco, Susana, additional, and Prieto-Matos, Carlos, additional

Published

2021

18. The Second Oncogenic Hit Determines the Cell Fate of ETV6-RUNX1 Positive Leukemia

Author

Rodríguez-Hernández, Guillermo, primary, Casado-García, Ana, additional, Isidro-Hernández, Marta, additional, Picard, Daniel, additional, Raboso-Gallego, Javier, additional, Alemán-Arteaga, Silvia, additional, Orfao, Alberto, additional, Blanco, Oscar, additional, Riesco, Susana, additional, Prieto-Matos, Pablo, additional, García Criado, Francisco Javier, additional, García Cenador, María Begoña, additional, Hock, Hanno, additional, Enver, Tariq, additional, Sanchez-Garcia, Isidro, additional, and Vicente-Dueñas, Carolina, additional

Published

2021

19. Cáncer de tiroides en pediatría

Author

Prieto Matos, Pablo, Martín, Diana, Martin Alonso, María Montserrat, Bajo Delgado, Ana Fe, Riesco Riesco, Susana, Prieto Matos, Carlos, Prieto Matos, Pablo, Martín, Diana, Martin Alonso, María Montserrat, Bajo Delgado, Ana Fe, Riesco Riesco, Susana, and Prieto Matos, Carlos

Abstract

Thyroid cancer is a rare disease in pediatric age; however it is increasing in the last few years, mainly in adolescent women. Although children and adult thyroid cancer are similar, they have some particular differences. The aim of this report is to analyze those differences, emphasizing the particularities of thyroid cáncer in pediatric age. The development of molecular genetic testing has allowed a deeper understanding of genetic predisposition síndromes, such as MEN2A, which has led to a significant increase in prophylactic thyroidectomies. The most frequent histological group is differentiated cáncer, specifically papilar type. At the time of diagnosis in children thyroid cancer presents a greater size and extensión, and more probabilities of multifocality and metastasis than in adults. The short-term prognosis is excellent; however in the long-term there are a significant number of recurrences and second tumors. It is important to carry out a personalized medicine, and to create diagnostic protocols. A Deep tumor characterization and the prognosis stratification will be essential to choose the correct treatment for each case, also to achieve maximum effectiveness, survival and to minimize side effects., Introducción y objetivo: El cáncer de tiroides es una enfermedad rara en la edad pediátrica que está aumentando en los últimos años, principalmente en mujeres adolescentes. Aunque guarda similitudes con el cáncer tiroideo del adulto tiene una serie de peculiaridades que lo diferencian. Nuestro objetivo es mostrar estas diferencias, resaltando las particularidades de esta enfermedad en la edad pediátrica frente a la del adulto. Los avances en las técnicas diagnósticas de genética molecular han permitido nuevos descubrimientos acerca de la génesis de tumores tiroideos en edades tempranas. También han supuesto un incremento de los diagnósticos de síndromes de predisposición genética, principalmente MEN2A, que ha producido un aumento significativo de tiroidectomías profilácticas. Los tipos histológicos más frecuentes son los cánceres diferenciados, principalmente el papilar. Al diagnóstico en edad pediátrica, suelen presentar un mayor tamaño, extensión, y probabilidades de multifocalidad y metástasis que en el adulto. A corto plazo el pronóstico es excelente; sin embargo, a largo plazo existe un número importante de recaídas y de aparición de segundos tumores. Para su tratamiento y seguimiento son necesarias unidades de alta especialización pediátrica que incluyan cirujanos expertos en tiroides. Se debe tender a la medicina personalizada estableciendo protocolos diagnósticos que caractericen correctamente el tumor y estratifiquen el pronóstico, adaptando la cirugía, la administración de yodo-131 y los nuevos tratamientos farmacológicos para buscar la máxima efectividad y supervivencia y minimicen los efectos secundarios.

Published

2021

20. The Second Oncogenic Hit Determines the Cell Fate of ETV6-RUNX1 Positive Leukemia

Author

Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Junta de Castilla y León, Fundación Unoentrecienmil, Hyundai Hope On Wheels, Universidad de Salamanca, Banco Santander, Rodríguez-Hernández, Guillermo, Casado-García, Ana, Isidro‑Hernández, Marta, Picard, Daniel, Raboso-Gallego, Javier, Alemán-Arteaga, Silvia, Orfao, Alberto, Blanco, Óscar, Riesco, Susana, Prieto-Matos, Pablo, García-Criado, Francisco Javier, García-Cenador, Begoña, Hock, Hanno, Enver, Tariq, Sánchez García, Isidro, Vicente-Dueñas, Carolina, Instituto de Salud Carlos III, European Commission, Ministerio de Economía y Competitividad (España), Agencia Estatal de Investigación (España), Ministerio de Ciencia, Innovación y Universidades (España), Junta de Castilla y León, Fundación Unoentrecienmil, Hyundai Hope On Wheels, Universidad de Salamanca, Banco Santander, Rodríguez-Hernández, Guillermo, Casado-García, Ana, Isidro‑Hernández, Marta, Picard, Daniel, Raboso-Gallego, Javier, Alemán-Arteaga, Silvia, Orfao, Alberto, Blanco, Óscar, Riesco, Susana, Prieto-Matos, Pablo, García-Criado, Francisco Javier, García-Cenador, Begoña, Hock, Hanno, Enver, Tariq, Sánchez García, Isidro, and Vicente-Dueñas, Carolina

Abstract

ETV6-RUNX1 is almost exclusively associated with childhood B-cell acute lymphoblastic leukemia (B-ALL), but the consequences of ETV6-RUNX1 expression on cell lineage decisions during B-cell leukemogenesis are completely unknown. Clinically silent ETV6-RUNX1 preleukemic clones are frequently found in neonatal cord blood, but few carriers develop B-ALL as a result of secondary genetic alterations. The understanding of the mechanisms underlying the first transforming steps could greatly advance the development of non-toxic prophylactic interventions. Using genetic lineage tracing, we examined the capacity of ETV6-RUNX1 to instruct a malignant phenotype in the hematopoietic lineage by cell-specific Cre-mediated activation of ETV6-RUNX1 from the endogenous Etv6 gene locus. Here we show that, while ETV6-RUNX1 has the propensity to trigger both T- and B-lymphoid malignancies, it is the second hit that determines tumor cell identity. To instigate leukemia, both oncogenic hits must place early in the development of hematopoietic/precursor cells, not in already committed B-cells. Depending on the nature of the second hit, the resulting B-ALLs presented distinct entities that were clearly separable based on their gene expression profiles. Our findings give a novel mechanistic insight into the early steps of ETV6-RUNX1+ B-ALL development and might have major implications for the potential development of ETV6-RUNX1+ B-ALL prevention strategies.

Published

2021

21. Mutually-Exclusive Pathways between IKZF1plus and RAS Mutations and TP53 double-Hit Alterations Lead Relapse in B-Other, Ph-like and Hyperdiploidy Genetic Groups in Adult B-Cell Acute Lymphoblastic Leukemia

Author

Navas Acosta, Josgrey Del Valle Del Valle, González, Teresa, Serramito-Gómez, Inmaculada, Villaverde Ramiro, Angela, Miguel-García, Cristina, Santos-Mínguez, Sandra, Ribera, Jordi, Granada, Isabel, Morgades, Mireia, Sanchez, Ricardo, Such, Esperanza, Barrera, Susana, Ciudad, Juana, Orfao, Alberto, Valls, Julio Davila, De Las Heras, Natalia, Fuster, José, Garcia de Coca, Alfonso, Labrador, Jorge, Queizan Hernandez, Jose Antonio, Mendoza, María Carmen, Riesco, Susana, Martín, Sandra, Ribera, Josep-Maria, Benito Sanchez, Maria Rocio, and Hernández-Rivas, Jesús María

Published

2023

22. Juvenile myelomonocytic leukemia in CBL syndrome associated with germline splice‐site mutations: Two case reports and a literature review

Author

Cardoso, Leila, primary, Galán‐Gómez, Víctor, additional, Corral‐Sánchez, María Dolores, additional, Pérez‐Martínez, Antonio, additional, Riesco, Susana, additional, Isidoro‐García, María, additional, and Escudero, Adela, additional

Published

2021

23. Helpful Criteria When Implementing NGS Panels in Childhood Lymphoblastic Leukemia

Author

Vega-Garcia, Nerea, Benito, Rocío, Esperanza-Cebollada, Elena, Llop, Marta, Robledo, Cristina, Vicente-Garcés, Clara, Alonso, Javier, Barragán, Eva, Fernández, Guerau, Hernández-Sánchez, Jesús M., Martín-Izquierdo, Marta, Maynou, Joan, Minguela, Alfredo, Montaño, Adrián, Ortega, Margarita, Torrebadell, Montserrat, Cervera, José, Sánchez, Joaquín, Jiménez-Velasco, Antonio, Riesco, Susana, Hernández-Rivas, Jesús M., Lassaletta, Álvaro, Fernández, José María, Rives, Susana, Dapena, José Luis, Ramírez, Manuel, Camós, Mireia, Universitat Autònoma de Barcelona, Vega-Garcia, Nerea, Benito, Rocío, Esperanza-Cebollada, Elena, Llop, Marta, Robledo, Cristina, Vicente-Garcés, Clara, Alonso, Javier, Barragán, Eva, Fernández, Guerau, Hernández-Sánchez, Jesús M., Martín-Izquierdo, Marta, Maynou, Joan, Minguela, Alfredo, Montaño, Adrián, Ortega, Margarita, Torrebadell, Montserrat, Cervera, José, Sánchez, Joaquín, Jiménez-Velasco, Antonio, Riesco, Susana, Hernández-Rivas, Jesús M., Lassaletta, Álvaro, Fernández, José María, Rives, Susana, Dapena, José Luis, Ramírez, Manuel, Camós, Mireia, and Universitat Autònoma de Barcelona

Abstract

The development of Next-Generation Sequencing (NGS) has provided useful diagnostic, prognostic, and therapeutic strategies for individualized management of B-cell precursor acute lymphoblastic leukemia (BCP-ALL) patients. Consequently, NGS is rapidly being established in clinical practice. However, the technology's complexity, bioinformatics analysis, and the different available options difficult a broad consensus between different laboratories in its daily routine introduction. This collaborative study among Spanish centers was aimed to assess the feasibility, pros, and cons of our customized panel and other commercial alternatives of NGS-targeted approaches. The custom panel was tested in three different sequencing centers. We used the same samples to assess other commercial panels (Oncomine TM Childhood Cancer Research Assay; Archer ® FusionPlex ® ALL, and Human Comprehensive Cancer Panel GeneRead Panel v2 ®). Overall, the panels showed a good performance in different centers and platforms, but each NGS approach presented some issues, as well as pros and cons. Moreover, a previous consensus on the analysis and reporting following international guidelines would be preferable to improve the concordance in results among centers. Our study shows the challenges posed by NGS methodology and the need to consider several aspects of the chosen NGS-targeted approach and reach a consensus before implementing it in daily practice

Published

2020

24. Hipoxemia como única manifestación de hemoglobinopatía estructural

Author

Sánchez Magdaleno, Mariana, Mendoza Sánchez, Mª del Carmen, Gaboli, Mirella, González Prieto, Almudena, and Riesco Riesco, Susana

Subjects

Hypoxemia, Pulse oximetry, Hipoxemia, Pulsioximetría, Hemoglobinopatía, Hemoglobinopathy

Abstract

Resumen Las hemoglobinopatías son resultado de mutaciones en los genes responsables de la estructura molecular de la hemoglobina. Tienen una expresividad clínica muy variable: desde mínimamente sintomáticas a patología grave. Presentamos el caso de un niño de tres años ingresado por una neumonía atípica con hipoxemia que, tras 11 días de ingreso, mantiene saturaciones periféricas de oxígeno (SpO) de 92-94% sin otra sintomatología, exploración física y estudio cardiopulmonar normal. En el seguimiento ambulatorio persiste la desaturación periférica con gasometría y cooximetría arterial normal. El padre del paciente presenta los mismos hallazgos tanto en la pulsioximetría como en la gasometría arterial. Ante la sospecha de una hemoglobinopatía estructural se realiza estudio genético y electroforético detectándose la presencia de hemoglobina Arta. Abstract Structural hemoglobinopathies are the result of gene mutations that cause alterations in the molecular structure of hemoglobin. They have a very variable clinical expression: from minimally symptomatic to severe pathology. We present the case of a 3-year-old boy admitted for atypical pneumonia with hypoxemia who, after 11 days of admission, maintained peripheral oxygen saturations (SpO) of 92-94% without other symptoms, physical examination and normal cardiopulmonary study. In outpatient follow-up, peripheral desaturation persists with gasometry and normal arterial co-oxymetry. Patient's father with the same findings in pulse oximetry as in arterial blood gases. When a structural hemoglobinopathy was suspected, a genetic and electrophoretic study was performed, detecting the presence of hemoglobin Arta.

Published

2019

25. Initial report on Spanish pediatric oncologic, hematologic, and post stem cell transplantation patients during SARS‐CoV‐2 pandemic

Author

Faura, Anna, primary, Rives, Susana, additional, Lassaletta, Álvaro, additional, Sebastián, Elena, additional, Madero, Luis, additional, Huerta, Jorge, additional, García‐Morín, Marina, additional, Martínez, Antonio Pérez, additional, Sisinni, Luisa, additional, Astigarraga, Itziar, additional, Velasco, Pablo, additional, Gros, Luis, additional, Moreno, Lucas, additional, Carboné, Ana, additional, Rodríguez‐Vigil, Carmen, additional, Riesco, Susana, additional, Mendoza, María del Carmen, additional, Macias, Elena García, additional, Trabazo, Maria, additional, Torrent, Montse, additional, Badell, Isabel, additional, Fuster, José Luis, additional, Dominguez‐Pinilla, Nerea, additional, Juan Ribelles, Antonio, additional, Pérez‐Alonso, Vanesa, additional, Fernández Sanmartín, Manuel, additional, Baragaño, Marta, additional, Gorostegui, Maite, additional, Perez‐Jaume, Sara, additional, Fernández‐Teijeiro, Ana, additional, Morales La Madrid, Andrés, additional, and Dapena, José Luis, additional

Published

2020

26. INITIAL REPORT ON SPANISH PEDIATRIC ONCOLOGIC, HEMATOLOGIC AND POST STEM CELL TRANSPLANTATION PATIENTS DURING SARS-COV-2 PANDEMIC

Author

Morros, Anna Faura, primary, Sol, Susana Rives, additional, LASSALETTA, ALVARO, additional, n, Elena Sebasti, additional, Madero, Luis, additional, s, Jorge Huerta Aragon, additional, Morin, Marina Garc a, additional, Martinez, Antonio Perez, additional, Sisinni, Luisa, additional, Astigarraga, Itziar, additional, Velasco, Pablo, additional, Gros, Luis, additional, Moreno, Lucas, additional, Carbon, Ana, additional, Vigil, Carmen Rodriguez, additional, Riesco, Susana, additional, Sanchez, Maria del Carmen Mendoza, additional, Macias, Elena Garcia, additional, Trabazo, Maria, additional, Torrent, Montserrat, additional, Badell, Isabel, additional, Soler, Jos Luis Fuster, additional, Pinilla, Nerea Dom nguez, additional, Ribelles, Antonio Juan, additional, Alonso, Vanesa P rez, additional, Sanmartin, Manuel Fern ndez, additional, o, Marta Baraga, additional, Gorostegui, Maite, additional, Jaume, Sara Perez, additional, Teijeiro, Ana Fern ndez, additional, Madrid, Andres Morales La, additional, and Dapena, Jose Luis, additional

Published

2020

27. Hipoxemia como única manifestación de hemoglobinopatía estructural

Author

Sánchez Magdaleno,Mariana, Mendoza Sánchez,Mª del Carmen, Gaboli,Mirella, González Prieto,Almudena, and Riesco Riesco,Susana

Subjects

Hipoxemia, Pulsioximetría, Hemoglobinopatía

Abstract

Resumen Las hemoglobinopatías son resultado de mutaciones en los genes responsables de la estructura molecular de la hemoglobina. Tienen una expresividad clínica muy variable: desde mínimamente sintomáticas a patología grave. Presentamos el caso de un niño de tres años ingresado por una neumonía atípica con hipoxemia que, tras 11 días de ingreso, mantiene saturaciones periféricas de oxígeno (SpO) de 92-94% sin otra sintomatología, exploración física y estudio cardiopulmonar normal. En el seguimiento ambulatorio persiste la desaturación periférica con gasometría y cooximetría arterial normal. El padre del paciente presenta los mismos hallazgos tanto en la pulsioximetría como en la gasometría arterial. Ante la sospecha de una hemoglobinopatía estructural se realiza estudio genético y electroforético detectándose la presencia de hemoglobina Arta.

Published

2019

28. Introducing high-throughput sequencing into mainstream genetic diagnosis practice in inherited platelet disorders

Author

Fundación Séneca, Sociedad Española de Trombosis y Hemostasia, European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, British Heart Foundation, Bastida, José María, Lozano, María L., Benito, Rocío, Janusz, Kamila, Palma-Barqueros, Verónica, Rey, Mónica del, Hernandez-Sánchez, Jesus M., Riesco, Susana, Bermejo, Nuria, González-García, Hermenegildo, Rodriguez-Alén, Agustín, Aguilar, Carlos, Sevivas, Teresa, López-Fernández, María F., Marneth, Anna E., Reijden, Bert A. van der, Morgan, Neil V., Watson, Steve P., Vicente, Vicente, Hernández, Jesús M., Rivera, José, González-Porras, José R., Fundación Séneca, Sociedad Española de Trombosis y Hemostasia, European Commission, Instituto de Salud Carlos III, Junta de Castilla y León, British Heart Foundation, Bastida, José María, Lozano, María L., Benito, Rocío, Janusz, Kamila, Palma-Barqueros, Verónica, Rey, Mónica del, Hernandez-Sánchez, Jesus M., Riesco, Susana, Bermejo, Nuria, González-García, Hermenegildo, Rodriguez-Alén, Agustín, Aguilar, Carlos, Sevivas, Teresa, López-Fernández, María F., Marneth, Anna E., Reijden, Bert A. van der, Morgan, Neil V., Watson, Steve P., Vicente, Vicente, Hernández, Jesús M., Rivera, José, and González-Porras, José R.

Abstract

Inherited platelet disorders are a heterogeneous group of rare diseases, caused by inherited defects in platelet production and/or function. Their genetic diagnosis would benefit clinical care, prognosis and preventative treatments. Until recently, this diagnosis has usually been performed via Sanger sequencing of a limited number of candidate genes. High-throughput sequencing is revolutionizing the genetic diagnosis of diseases, including bleeding disorders. We have designed a novel high-throughput sequencing platform to investigate the unknown molecular pathology in a cohort of 82 patients with inherited platelet disorders. Thirty-four (41.5%) patients presented with a phenotype strongly indicative of a particular type of platelet disorder. The other patients had clinical bleeding indicative of platelet dysfunction, but with no identifiable features. The high-throughput sequencing test enabled a molecular diagnosis in 70% of these patients. This sensitivity increased to 90% among patients suspected of having a defined platelet disorder. We found 57 different candidate variants in 28 genes, of which 70% had not previously been described. Following consensus guidelines, we qualified 68.4% and 26.3% of the candidate variants as being pathogenic and likely pathogenic, respectively. In addition to establishing definitive diagnoses of well-known inherited platelet disorders, high-throughput sequencing also identified rarer disorders such as sitosterolemia, filamin and actinin deficiencies, and G protein-coupled receptor defects. This included disease-causing variants in DIAPH1 (n=2) and RASGRP2 (n=3). Our study reinforces the feasibility of introducing high-throughput sequencing technology into the mainstream laboratory for the genetic diagnostic practice in inherited platelet disorders.

Published

2018

29. Mutations in TP53 and JAK2 are independent prognostic biomarkers in B-cell precursor acute lymphoblastic leukaemia

Author

Forero-Castro, Maribel, Robledo, Cristina, Benito Sánchez, Rocío, Bodega-Mayor, Irene, Rapado, Inmaculada, Hernández Rivas, Jesús María, Abáigar, María, Quijada-Alamo, Miguel, Sánchez-Pina, José M, Sala-Valdés, Mónica, Araujo-Silva, Fernanda, Kohlmann, Alexander, Fuster, José Luis, Arefi, Maryam, Heras, Natalia de las, Riesco, Susana, Rodríguez, Juan-Nicolás, Hermosín, Lourdes, Ribera, Jordi, Camos Guijosa, Mireia, Ramírez, Manuel, Díaz de Heredia Rubio, Cristina, Barragán, Eva, Martínez, Joaquín, Ribera, Jose M., and Fernández-Ruiz, Elena

Subjects

JAK2, Next-generation sequencing (NGS), Mutation, TP53, Acute lymphoblastic leukemia

Abstract

[EN]Background: In B-cell precursor acute lymphoblastic leukaemia (B-ALL), the identification of additional genetic alterations associated with poor prognosis is still of importance. We determined the frequency and prognostic impact of somatic mutations in children and adult cases with B-ALL treated with Spanish PETHEMA and SEHOP protocols. Methods: Mutational status of hotspot regions of TP53, JAK2, PAX5, LEF1, CRLF2 and IL7R genes was determined by next-generation deep sequencing in 340 B-ALL patients (211 children and 129 adults). The associations between mutation status and clinicopathological features at the time of diagnosis, treatment outcome and survival were assessed. Univariate and multivariate survival analyses were performed to identify independent prognostic factors associated with overall survival (OS), event-free survival (EFS) and relapse rate (RR). Results: A mutation rate of 12.4% was identified. The frequency of adult mutations was higher (20.2% vs 7.6%, P=0.001). TP53 was the most frequently mutated gene (4.1%), followed by JAK2 (3.8%), CRLF2 (2.9%), PAX5 (2.4%), LEF1 (0.6%) and IL7R (0.3%). All mutations were observed in B-ALL without ETV6-RUNX1 (P=0.047) or BCR-ABL1 fusions (P, European Commision (EC). Funding FP7/SP1/HEALTH. Project Code: 306242

Published

2017

30. Mutations in TP53 and JAK2 are independent prognostic biomarkers in B-cell precursor acute lymphoblastic leukaemia

Author

Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Red Temática de Investigación Cooperativa en Cáncer (España), Universidad Pedagógica y Tecnológica de Colombia, Junta de Castilla y León, European Commission, Forero-Castro, Maribel, Robledo, Cristina, Benito, Rocío, Bodega-Mayor, Irene, Rapado, Inmaculada, Hernández-Sánchez, María, Abáigar, María, Hernandez-Sánchez, Jesus M., Quijada-Álamo, Miguel, Sánchez-Pina, José María, Sala-Valdés, Mónica, Araujo-Silva, Fernando, Kohlmann, Alexander, Fuster, José Luis, Arefi, Maryam, Heras, Natalia de las, Riesco, Susana, Rodríguez, Juan-Nicolas, Hermosín, Lourdes, Ribera, Jordi, Camos Guijosa, Mireia, Ramírez, Manuel, Díaz de Heredia, Cristina, Barragán, Eva, Martínez-López, Joaquín, Ribera, Josep-Maria, Fernández-Ruiz, Elena, Hernández, Jesús M., Ministerio de Economía y Competitividad (España), Instituto de Salud Carlos III, Red Temática de Investigación Cooperativa en Cáncer (España), Universidad Pedagógica y Tecnológica de Colombia, Junta de Castilla y León, European Commission, Forero-Castro, Maribel, Robledo, Cristina, Benito, Rocío, Bodega-Mayor, Irene, Rapado, Inmaculada, Hernández-Sánchez, María, Abáigar, María, Hernandez-Sánchez, Jesus M., Quijada-Álamo, Miguel, Sánchez-Pina, José María, Sala-Valdés, Mónica, Araujo-Silva, Fernando, Kohlmann, Alexander, Fuster, José Luis, Arefi, Maryam, Heras, Natalia de las, Riesco, Susana, Rodríguez, Juan-Nicolas, Hermosín, Lourdes, Ribera, Jordi, Camos Guijosa, Mireia, Ramírez, Manuel, Díaz de Heredia, Cristina, Barragán, Eva, Martínez-López, Joaquín, Ribera, Josep-Maria, Fernández-Ruiz, Elena, and Hernández, Jesús M.

Abstract

[Background]: In B-cell precursor acute lymphoblastic leukaemia (B-ALL), the identification of additional genetic alterations associated with poor prognosis is still of importance. We determined the frequency and prognostic impact of somatic mutations in children and adult cases with B-ALL treated with Spanish PETHEMA and SEHOP protocols. [Methods]: Mutational status of hotspot regions of TP53, JAK2, PAX5, LEF1, CRLF2 and IL7R genes was determined by next-generation deep sequencing in 340 B-ALL patients (211 children and 129 adults). The associations between mutation status and clinicopathological features at the time of diagnosis, treatment outcome and survival were assessed. Univariate and multivariate survival analyses were performed to identify independent prognostic factors associated with overall survival (OS), event-free survival (EFS) and relapse rate (RR). [Results]: A mutation rate of 12.4% was identified. The frequency of adult mutations was higher (20.2% vs 7.6%, P=0.001). TP53 was the most frequently mutated gene (4.1%), followed by JAK2 (3.8%), CRLF2 (2.9%), PAX5 (2.4%), LEF1 (0.6%) and IL7R (0.3%). All mutations were observed in B-ALL without ETV6-RUNX1 (P=0.047) or BCR-ABL1 fusions (P<0.0001). In children, TP53mut was associated with lower OS (5-year OS: 50% vs 86%, P=0.002) and EFS rates (5-year EFS: 50% vs 78.3%, P=0.009) and higher RR (5-year RR: 33.3% vs 18.6% P=0.037), and was independently associated with higher RR (hazard ratio (HR)=4.5; P=0.04). In adults, TP53mut was associated with a lower OS (5-year OS: 0% vs 43.3%, P=0.019) and a higher RR (5-year RR: 100% vs 61.4%, P=0.029), whereas JAK2mut was associated with a lower EFS (5-year EFS: 0% vs 30.6%, P=0.035) and a higher RR (5-year RR: 100% vs 60.4%, P=0.002). TP53mut was an independent risk factor for shorter OS (HR=2.3; P=0.035) and, together with JAK2mut, also were independent markers of poor prognosis for RR (TP53mut: HR=5.9; P=0.027 and JAK2mut: HR=5.6; P=0.036). [Conclusions]: TP53mu

Published

2017

31. Wiskott–Aldrich syndrome in a child presenting with macrothrombocytopenia

Author

Bastida, José María, Rey, Mónica del, Revilla, Nuria, Benito, Rocío, Pérez-Andrés, Martin, González, Berta, Riesco, Susana, Janusz, Kamila, Padilla, Jose, Hortal Benito-Sendin, Ana, Bueno, David, Blanco, Elena, Hernández, Jesús M., Vicente, Vicente, Rivera, José, González-Porras, José R., Lozano, María L., Bastida, José María, Rey, Mónica del, Revilla, Nuria, Benito, Rocío, Pérez-Andrés, Martin, González, Berta, Riesco, Susana, Janusz, Kamila, Padilla, Jose, Hortal Benito-Sendin, Ana, Bueno, David, Blanco, Elena, Hernández, Jesús M., Vicente, Vicente, Rivera, José, González-Porras, José R., and Lozano, María L.

Abstract

Wiskott–Aldrich syndrome (WAS) is a rare X-linked recessive disease resulting from variants in the WAS gene, characterized by a triad of immunodeficiency, eczema, and thrombocytopenia. Despite the fact that WAS is traditionally differentiated from immune thrombocytopenia (ITP) by small size of WAS platelets, in practice, microthrombocytopenia may occasionally not be present, and in certain cases, WAS patients exhibit some parallelism to ITP patients. We characterized one patient presenting with the classic form of the disease but increased mean platelet volume. Molecular studies revealed a novel hemizygous 1-bp deletion in WAS gene, c.802delC, leading to a frameshift and stop codon at amino acid 308 (p.Arg268Glyfs*40). Next-generation sequencing of a total of 70 additional genes known to harbor variants implicated in inherited platelet disorders did not identify additional defects. The pathogenesis of macrothrombocytopenia in this case is not known, but probably the coexistence of a still unidentified additional genetic variant might be involved.

Published

2017

32. Introducing high-throughput sequencing into mainstream genetic diagnosis practice in inherited platelet disorders

Author

Bastida, José M., primary, Lozano, María L., additional, Benito, Rocío, additional, Janusz, Kamila, additional, Palma-Barqueros, Verónica, additional, Del Rey, Mónica, additional, Hernández-Sánchez, Jesús M., additional, Riesco, Susana, additional, Bermejo, Nuria, additional, González-García, Hermenegildo, additional, Rodriguez-Alén, Agustín, additional, Aguilar, Carlos, additional, Sevivas, Teresa, additional, López-Fernández, María F., additional, Marneth, Anna E., additional, van der Reijden, Bert A., additional, Morgan, Neil V., additional, Watson, Steve P., additional, Vicente, Vicente, additional, Hernández-Rivas, Jesús M., additional, Rivera, José, additional, and González-Porras, José R., additional

Published

2017

33. Mutations in TP53 and JAK2 are independent prognostic biomarkers in B-cell precursor acute lymphoblastic leukaemia

Author

Forero-Castro, Maribel, primary, Robledo, Cristina, additional, Benito, Rocío, additional, Bodega-Mayor, Irene, additional, Rapado, Inmaculada, additional, Hernández-Sánchez, María, additional, Abáigar, María, additional, Maria Hernández-Sánchez, Jesús, additional, Quijada-Álamo, Miguel, additional, María Sánchez-Pina, José, additional, Sala-Valdés, Mónica, additional, Araujo-Silva, Fernanda, additional, Kohlmann, Alexander, additional, Luis Fuster, José, additional, Arefi, Maryam, additional, de las Heras, Natalia, additional, Riesco, Susana, additional, Rodríguez, Juan N, additional, Hermosín, Lourdes, additional, Ribera, Jordi, additional, Camos Guijosa, Mireia, additional, Ramírez, Manuel, additional, de Heredia Rubio, Cristina Díaz, additional, Barragán, Eva, additional, Martínez, Joaquín, additional, Ribera, José M, additional, Fernández-Ruiz, Elena, additional, and Hernández-Rivas, Jesús-María, additional

Published

2017

34. Application of a molecular diagnostic algorithm for haemophilia A and B using next-generation sequencing of entire F8, F9 and VWF genes

Author

González-Porras, Jose, primary, Jiménez, Cristina, primary, Benito, Rocio, primary, Ordoñez, Gonzalo R., primary, Álvarez-Román, Maria, primary, Fontecha, M. Elena, primary, Janusz, Kamila, primary, Castillo, David, primary, Fisac, Rosa, primary, García-Frade, Luis, primary, Aguilar, Carlos, primary, Martínez, Paz, primary, Bermejo, Nuria, primary, Herrero, Sonia, primary, Balanzategui, Ana, primary, Martin-Antorán, Jose, primary, Ramos, Rafael, primary, Cebeiro, Maria, primary, Pardal, Emilia, primary, Aguilera, Carmen, primary, Pérez-Gutierrez, Belen, primary, Prieto, Manuel, primary, Riesco, Susana, primary, Mendoza, Maria, primary, Benito, Ana, primary, Benito-Sendin, Ana, primary, Jimenez-Yuste, Victor, primary, Hernández-Rivas, Jesus, primary, García-Sanz, Ramon, primary, González-Díaz, Marcos, primary, Sarasquete, Maria, primary, and Bastida, Jose, additional

Published

2017

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

Author

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

Abstract

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

Published

2016

36. Design and application of a 23-gene panel by next-generation sequencing for inherited coagulation bleeding disorders

Author

Bastida, José María, Rey, Mónica del, Lozano, María L., Sarasquete, María Eugenia, Benito, Rocío, Fontecha, M. E., Fisac, R., García-Frade, L. J., Aguilar, Carlos, Martínez, M. P., Pardal, Emilia, Aguilera-Sanz, C., Pérez, B., Ramos, Rafael, Cardesa, M. R., Martin-Antorán, J. M., Silvestre, L. A., Cebeira, M. J., Bermejo, Nuria, Riesco, Susana, Mendoza, M. C., García-Sanz, Ramón, González, Marcos, Hernández, Jesús M., González-Porras, José R., Bastida, José María, Rey, Mónica del, Lozano, María L., Sarasquete, María Eugenia, Benito, Rocío, Fontecha, M. E., Fisac, R., García-Frade, L. J., Aguilar, Carlos, Martínez, M. P., Pardal, Emilia, Aguilera-Sanz, C., Pérez, B., Ramos, Rafael, Cardesa, M. R., Martin-Antorán, J. M., Silvestre, L. A., Cebeira, M. J., Bermejo, Nuria, Riesco, Susana, Mendoza, M. C., García-Sanz, Ramón, González, Marcos, Hernández, Jesús M., and González-Porras, José R.

Abstract

[Introduction]: Molecular testing of Inherited bleeding coagulation disorders (IBCDs) not only offers confirmation of diagnosis but also aids in genetic counselling, prenatal diagnosis and in certain cases genotype–phenotype correlations are important for predicting the clinical course of the disease and to allow tailor-made follow-up of individuals. Until recently, genotyping has been mainly performed by Sanger sequencing, a technique known to be time consuming and expensive. Currently, next-generation sequencing (NGS) offers a new potential approach that enables the simultaneous investigation of multiple genes at manageable cost. [Aim]: The aim of this study was to design and to analyse the applicability of a 23-gene NGS panel in the molecular diagnosis of patients with IBCDs. [Methods]: A custom target enrichment library was designed to capture 31 genes known to be associated with IBCDs. Probes were generated for 296 targets to cover 86.3 kb regions (all exons and flanking regions) of these genes. Twenty patients with an IBCDs phenotype were studied using NGS technology. [Results]: In all patients, our NGS approach detected causative mutations. Twenty-one pathogenic variants were found; while most of them were missense (18), three deletions were also identified. Six novel mutations affecting F8, FGA, F11, F10 and VWF genes, and 15 previously reported variants were detected. NGS and Sanger sequencing were 100% concordant. Conclusion: Our results demonstrate that this approach could be an accurate, reproducible and reliable tool in the rapid genetic diagnosis of IBCDs.

Published

2016

37. Wiskott–Aldrich syndrome in a child presenting with macrothrombocytopenia

Author

Bastida, Jose Maria, primary, Del Rey, Monica, additional, Revilla, Nuria, additional, Benito, Rocio, additional, Perez-Andrés, Martin, additional, González, Berta, additional, Riesco, Susana, additional, Janusz, Kamila, additional, Padilla, Jose, additional, Hortal Benito-Sendin, Ana, additional, Bueno, David, additional, Blanco, Elena, additional, Hernández-Rivas, Maria, additional, Vicente, Vicente, additional, Rivera, Jose, additional, González-Porras, Ramon, additional, and Lozano, Maria Luisa, additional

Published

2016

38. Genome-Wide DNA Copy Number Analysis of Acute Lymphoblastic Leukemia Identifies New Genetic Markers Associated with Clinical Outcome

Author

Forero-Castro, Maribel, primary, Robledo, Cristina, additional, Benito, Rocío, additional, Abáigar, María, additional, África Martín, Ana, additional, Arefi, Maryam, additional, Fuster, José Luis, additional, de las Heras, Natalia, additional, Rodríguez, Juan N., additional, Quintero, Jonathan, additional, Riesco, Susana, additional, Hermosín, Lourdes, additional, de la Fuente, Ignacio, additional, Recio, Isabel, additional, Ribera, Jordi, additional, Labrador, Jorge, additional, Alonso, José M., additional, Olivier, Carmen, additional, Sierra, Magdalena, additional, Megido, Marta, additional, Corchete-Sánchez, Luis A., additional, Ciudad Pizarro, Juana, additional, García, Juan Luis, additional, Ribera, José M., additional, and Hernández-Rivas, Jesús M., additional

Published

2016

39. Mutually-Exclusive Pathways between IKZF1plusand RAS Mutations and TP53double-Hit Alterations Lead Relapse in B-Other, Ph-like and Hyperdiploidy Genetic Groups in Adult B-Cell Acute Lymphoblastic Leukemia

Author

Navas Acosta, Josgrey Del Valle Del Valle, González, Teresa, Serramito-Gómez, Inmaculada, Villaverde Ramiro, Angela, Miguel-García, Cristina, Santos-Mínguez, Sandra, Ribera, Jordi, Granada, Isabel, Morgades, Mireia, Sanchez, Ricardo, Such, Esperanza, Barrera, Susana, Ciudad, Juana, Orfao, Alberto, Valls, Julio Davila, De Las Heras, Natalia, Fuster, José, Garcia de Coca, Alfonso, Labrador, Jorge, Queizan Hernandez, Jose Antonio, Mendoza, María Carmen, Riesco, Susana, Martín, Sandra, Ribera, Josep-Maria, Benito Sanchez, Maria Rocio, and Hernández-Rivas, Jesús María

Abstract

Introduction:Adult B-cell precursor acute lymphoblastic leukemia (BCP-ALL) is a hematologic malignancy characterized by a high genetic heterogeneity and high relapse rate. Despite treatment advances have led to high cure rates in pediatric BCP-ALL (90%), improving survival in adults remains a challenge. Identification of genetic alterations driving relapse and both new prognostic and therapeutic biomarkers are important to improve survival in adults with BCP-ALL.

Published

2023

40. Design and Validate of Next-Generation Sequencing Panel for Inherited Platelet Disorders

Author

Bastida, Jose Maria, primary, del Rey, Mónica, additional, Benito, Rocío, additional, Sanchez-Guiu, Isabel, additional, Riesco, Susana, additional, Peñarrubia, Maria Jesús, additional, Fisac, Rosa, additional, García Frade, Javier, additional, Aguilar, Carlos, additional, Cebeiro, Maria Jose, additional, Martinez-Badás, Paz, additional, Pardal, Emilia, additional, Aguilera, Carmen, additional, Fontecha, Elena, additional, Perez, Beatriz, additional, Llinares, Esther, additional, Fuster, Jose Luis, additional, Rivera, Jose, additional, Lozano, Maria Luisa, additional, Vicente, Vicente, additional, Del Canizo, Consuelo, additional, Hernandez, Jesus Maria, additional, and Gonzalez, José Ramón, additional

Published

2014

41. Hidden DNA Copy Number Alterations and Mutations in IKZF1, TP53, CRLF2 and JAK2 Genes Are Associated with a Poor Prognosis in B-Progenitor Acute Lymphoblastic Leukemia

Author

Hernández-Rivas, Jesús María, primary, Forero, Maribel, additional, Robledo, Cristina, additional, Benito, Rocio, additional, Hernández, María, additional, Abáigar, María, additional, Rodríguez, Ana, additional, Corchete, Luis A., additional, Martín, Ana, additional, Riesco-Riesco, Susana, additional, García-de-Coca, A, additional, Fuster, José L., additional, De-las-Heras, Natalia, additional, Rodríguez, Juan N., additional, De-la-Fuente, I, additional, Ribera, Josep-Maria, additional, Ribera, Jordi, additional, Labrador, Jorge, additional, Alonso, Jose M., additional, García, Juan L., additional, and Del Cañizo, Consuelo, additional

Published

2014

42. Application of a molecular diagnostic algorithm for haemophilia A and B using next-generation sequencing of entire F8, F9 and VWF genes

Author

Bastida, Jose Maria, González-Porras, Jose Ramon, Jiménez, Cristina, Benito, Rocio, Ordoñez, Gonzalo R., Álvarez-Román, Maria Teresa, Fontecha, M. Elena, Janusz, Kamila, Castillo, David, Fisac, Rosa Maria, García-Frade, Luis Javier, Aguilar, Carlos, Martínez, Paz Maria, Bermejo, Nuria, Herrero, Sonia, Balanzategui, Ana, Martin-Antorán, Jose Manuel, Ramos, Rafael, Cebeiro, Maria Jose, Pardal, Emilia, Aguilera, Carmen, Pérez-Gutierrez, Belen, Prieto, Manuel, Riesco, Susana, Mendoza, Maria Carmen, Benito, Ana, Benito-Sendin, Ana Hortal, Jimenez-Yuste, Victor, Hernández-Rivas, Jesus Maria, García-Sanz, Ramon, González-Díaz, Marcos, and Sarasquete, Maria Eugenia

Published

2017

43. Increasing Incidence of Invasive Aspergillosis in Pediatric Hematology Oncology Patients Over the Last Decade

Author

Rubio, Pedro M., primary, Sevilla, Julián, additional, González-Vicent, Marta, additional, Lassaletta, Alvaro, additional, Cuenca-Estrella, Manuel, additional, Díaz, Miguel A., additional, Riesco, Susana, additional, and Madero, Luis, additional

Published

2009

44. Heterogeneous Landscape of RUNX1Related Disorder: Four Families with Inherited Thrombocytopenias and Novel Genetic Variants in RUNX1Associated to Relevant Clinical Complications

Author

Bastida, Jose Maria, Benito, Rocio, Hernández-Sánchez, Jesus M, Lozano, Maria L, Janusz, Kamila, Lumbreras, Eva, Lassaletta, Alvaro, Riesco, Susana, Huerta, Jorge, Palma-Barqueros, Veronica, Hortal, Ana, Díez-Campelo, Maria, Prieto-Conde, Maria Isabel, Chillon, Maria Carmen, Del Cañizo, Consuelo, Hernández-Rivas, Jesús M, Rivera, Jose, and González-Porras, Jose Ramon

Abstract

Background

Published

2017

45. Hidden DNA Copy Number Alterations and Mutations in IKZF1, TP53, CRLF2and JAK2Genes Are Associated with a Poor Prognosis in B-Progenitor Acute Lymphoblastic Leukemia

Author

Hernández-Rivas, Jesús María, Forero, Maribel, Robledo, Cristina, Benito, Rocio, Hernández, María, Abáigar, María, Rodríguez, Ana, Corchete, Luis A., Martín, Ana, Riesco-Riesco, Susana, García-de-Coca, A, Fuster, José L., De-las-Heras, Natalia, Rodríguez, Juan N., De-la-Fuente, I, Ribera, Josep-Maria, Ribera, Jordi, Labrador, Jorge, Alonso, Jose M., García, Juan L., and Del Cañizo, Consuelo

Abstract

Background:In B-progenitor acute lymphoblastic leukemia (B-ALL) the identification of additional genetic alterations associated with treatment failure is still a challenge.

Published

2014

46. Helpful Criteria When Implementing NGS Panels in Childhood Lymphoblastic Leukemia.

Author

Vega-Garcia N, Benito R, Esperanza-Cebollada E, Llop M, Robledo C, Vicente-Garcés C, Alonso J, Barragán E, Fernández G, Hernández-Sánchez JM, Martín-Izquierdo M, Maynou J, Minguela A, Montaño A, Ortega M, Torrebadell M, Cervera J, Sánchez J, Jiménez-Velasco A, Riesco S, Hernández-Rivas JM, Lassaletta Á, Fernández JM, Rives S, Dapena JL, Ramírez M, Camós M, and On Behalf Of The Group Of Leukemia Of The Spanish Society Of Pediatric Hematology And Oncology Sehop

Abstract

The development of Next-Generation Sequencing (NGS) has provided useful diagnostic, prognostic, and therapeutic strategies for individualized management of B-cell precursor acute lymphoblastic leukemia (BCP-ALL) patients. Consequently, NGS is rapidly being established in clinical practice. However, the technology's complexity, bioinformatics analysis, and the different available options difficult a broad consensus between different laboratories in its daily routine introduction. This collaborative study among Spanish centers was aimed to assess the feasibility, pros, and cons of our customized panel and other commercial alternatives of NGS-targeted approaches. The custom panel was tested in three different sequencing centers. We used the same samples to assess other commercial panels (Oncomine TM Childhood Cancer Research Assay; Archer ® FusionPlex ® ALL, and Human Comprehensive Cancer Panel GeneRead Panel v2 ® ). Overall, the panels showed a good performance in different centers and platforms, but each NGS approach presented some issues, as well as pros and cons. Moreover, a previous consensus on the analysis and reporting following international guidelines would be preferable to improve the concordance in results among centers. Our study shows the challenges posed by NGS methodology and the need to consider several aspects of the chosen NGS-targeted approach and reach a consensus before implementing it in daily practice.

Published

2020

47. Introducing high-throughput sequencing into mainstream genetic diagnosis practice in inherited platelet disorders.

Author

Bastida JM, Lozano ML, Benito R, Janusz K, Palma-Barqueros V, Del Rey M, Hernández-Sánchez JM, Riesco S, Bermejo N, González-García H, Rodriguez-Alén A, Aguilar C, Sevivas T, López-Fernández MF, Marneth AE, van der Reijden BA, Morgan NV, Watson SP, Vicente V, Hernández-Rivas JM, Rivera J, and González-Porras JR

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Blood Platelets metabolism, Child, Child, Preschool, Female, Genetic Association Studies, Genetic Predisposition to Disease, Humans, Infant, Male, Middle Aged, Phenotype, Reproducibility of Results, Sequence Analysis, DNA, Young Adult, Blood Platelet Disorders diagnosis, Blood Platelet Disorders genetics, Genetic Diseases, Inborn diagnosis, Genetic Diseases, Inborn genetics, Genetic Testing methods, High-Throughput Nucleotide Sequencing

Abstract

Inherited platelet disorders are a heterogeneous group of rare diseases, caused by inherited defects in platelet production and/or function. Their genetic diagnosis would benefit clinical care, prognosis and preventative treatments. Until recently, this diagnosis has usually been performed via Sanger sequencing of a limited number of candidate genes. High-throughput sequencing is revolutionizing the genetic diagnosis of diseases, including bleeding disorders. We have designed a novel high-throughput sequencing platform to investigate the unknown molecular pathology in a cohort of 82 patients with inherited platelet disorders. Thirty-four (41.5%) patients presented with a phenotype strongly indicative of a particular type of platelet disorder. The other patients had clinical bleeding indicative of platelet dysfunction, but with no identifiable features. The high-throughput sequencing test enabled a molecular diagnosis in 70% of these patients. This sensitivity increased to 90% among patients suspected of having a defined platelet disorder. We found 57 different candidate variants in 28 genes, of which 70% had not previously been described. Following consensus guidelines, we qualified 68.4% and 26.3% of the candidate variants as being pathogenic and likely pathogenic, respectively. In addition to establishing definitive diagnoses of well-known inherited platelet disorders, high-throughput sequencing also identified rarer disorders such as sitosterolemia, filamin and actinin deficiencies, and G protein-coupled receptor defects. This included disease-causing variants in DIAPH1 (n=2) and RASGRP2 (n=3). Our study reinforces the feasibility of introducing high-throughput sequencing technology into the mainstream laboratory for the genetic diagnostic practice in inherited platelet disorders., (Copyright© 2018 Ferrata Storti Foundation.)

Published

2018

48. Wiskott-Aldrich syndrome in a child presenting with macrothrombocytopenia.

Author

Bastida JM, Del Rey M, Revilla N, Benito R, Perez-Andrés M, González B, Riesco S, Janusz K, Padilla J, Hortal Benito-Sendin A, Bueno D, Blanco E, Hernández-Rivas M, Vicente V, Rivera J, González-Porras R, and Lozano ML

Subjects

Child, Preschool, Humans, Male, Thrombocytopenia genetics, Wiskott-Aldrich Syndrome

Abstract

Wiskott-Aldrich syndrome (WAS) is a rare X-linked recessive disease resulting from variants in the WAS gene, characterized by a triad of immunodeficiency, eczema, and thrombocytopenia. Despite the fact that WAS is traditionally differentiated from immune thrombocytopenia (ITP) by small size of WAS platelets, in practice, microthrombocytopenia may occasionally not be present, and in certain cases, WAS patients exhibit some parallelism to ITP patients. We characterized one patient presenting with the classic form of the disease but increased mean platelet volume. Molecular studies revealed a novel hemizygous 1-bp deletion in WAS gene, c.802delC, leading to a frameshift and stop codon at amino acid 308 (p.Arg268Glyfs*40). Next-generation sequencing of a total of 70 additional genes known to harbor variants implicated in inherited platelet disorders did not identify additional defects. The pathogenesis of macrothrombocytopenia in this case is not known, but probably the coexistence of a still unidentified additional genetic variant might be involved.

Published

2017