Your search keyword '"Hasle, Henrik"' showing total 282 results

1. A multidimensional analysis reveals distinct immune phenotypes and the composition of immune aggregates in pediatric acute myeloid leukemia

Author

Koedijk, Joost B., van der Werf, Inge, Penter, Livius, Vermeulen, Marijn A., Barneh, Farnaz, Perzolli, Alicia, Meesters-Ensing, Joyce I., Metselaar, Dennis S., Margaritis, Thanasis, Fiocco, Marta, de Groot-Kruseman, Hester A., Moeniralam, Rubina, Bang Christensen, Kristina, Porter, Billie, Pfaff, Kathleen, Garcia, Jacqueline S., Rodig, Scott J., Wu, Catherine J., Hasle, Henrik, Nierkens, Stefan, Belderbos, Mirjam E., Zwaan, C. Michel, and Heidenreich, Olaf

Abstract

Because of the low mutational burden and consequently, fewer potential neoantigens, children with acute myeloid leukemia (AML) are thought to have a T cell-depleted or ‘cold’ tumor microenvironment and may have a low likelihood of response to T cell-directed immunotherapies. Understanding the composition, phenotype, and spatial organization of T cells and other microenvironmental populations in the pediatric AML bone marrow (BM) is essential for informing future immunotherapeutic trials about targetable immune-evasion mechanisms specific to pediatric AML. Here, we conducted a multidimensional analysis of the tumor immune microenvironment in pediatric AML and non-leukemic controls. We demonstrated that nearly one-third of pediatric AML cases has an immune-infiltrated BM, which is characterized by a decreased ratio of M2- to M1-like macrophages. Furthermore, we detected the presence of large T cell networks, both with and without colocalizing B cells, in the BM and dissected the cellular composition of T- and B cell-rich aggregates using spatial transcriptomics. These analyses revealed that these aggregates are hotspots of CD8+T cells, memory B cells, plasma cells and/or plasmablasts, and M1-like macrophages. Collectively, our study provides a multidimensional characterization of the BM immune microenvironment in pediatric AML and indicates starting points for further investigations into immunomodulatory mechanisms in this devastating disease.

Published

2024

2. ATMgerm line pathogenic variants affect outcomes in children with ataxia-telangiectasia and hematological malignancies

Author

Elitzur, Sarah, Shiloh, Ruth, Loeffen, Jan L. C., Pastorczak, Agata, Takagi, Masatoshi, Bomken, Simon, Baruchel, Andre, Lehrnbecher, Thomas, Tasian, Sarah K., Abla, Oussama, Arad-Cohen, Nira, Astigarraga, Itziar, Ben-Harosh, Miriam, Bodmer, Nicole, Brozou, Triantafyllia, Ceppi, Francesco, Chugaeva, Liliia, Dalla Pozza, Luciano, Ducassou, Stephane, Escherich, Gabriele, Farah, Roula, Gibson, Amber, Hasle, Henrik, Hoveyan, Julieta, Jacoby, Elad, Jazbec, Janez, Junk, Stefanie, Kolenova, Alexandra, Lazic, Jelena, Lo Nigro, Luca, Mahlaoui, Nizar, Miller, Lane, Papadakis, Vassilios, Pecheux, Lucie, Pillon, Marta, Sarouk, Ifat, Stary, Jan, Stiakaki, Eftichia, Strullu, Marion, Tran, Thai Hoa, Ussowicz, Marek, Verdu-Amoros, Jaime, Wakulinska, Anna, Zawitkowska, Joanna, Stoppa-Lyonnet, Dominique, Taylor, A. Malcolm, Shiloh, Yosef, Izraeli, Shai, Minard-Colin, Veronique, Schmiegelow, Kjeld, Nirel, Ronit, Attarbaschi, Andishe, and Borkhardt, Arndt

Abstract

•The major cause of death in patients with ataxia-telangiectasia and hematological malignancies is treatment-related toxicity.•The germ line ATMpathogenic variant functional class is a robust outcome predictor, which can be applied to therapy stratification.

Published

2024

3. Mitoxantrone Versus Liposomal Daunorubicin in Induction of Pediatric AML With Risk Stratification Based on Flow Cytometry Measurement of Residual Disease.

Author

Tierens, Anne, Arad-Cohen, Nira, Cheuk, Daniel, De Moerloose, Barbara, Fernandez Navarro, Jose Maria, Hasle, Henrik, Jahnukainen, Kirsi, Juul-Dam, Kristian Løvvik, Kaspers, Gertjan, Kovalova, Zanna, Lausen, Birgitte, Norén-Nyström, Ulrika, Palle, Josefine, Pasauliene, Ramune, Jan Pronk, Cornelis, Saks, Kadri, Zeller, Bernward, and Abrahamsson, Jonas

Published

2024

4. Efficacy of T-cell assays for the diagnosis of primary defects in cytotoxic lymphocyte exocytosis

Author

Chiang, Samuel C. C., Covill, Laura E., Tesi, Bianca, Campbell, Tessa M., Schlums, Heinrich, Nejati-Zendegani, Jelve, Mördrup, Karina, Wood, Stephanie, Theorell, Jakob, Sekine, Takuya, Al-Herz, Waleed, Akar, Himmet Haluk, Belen, Fatma Burcu, Chan, Mei Yoke, Devecioglu, Omer, Aksu, Tekin, Ifversen, Marianne, Malinowska, Iwona, Sabel, Magnus, Unal, Ekrem, Unal, Sule, Introne, Wendy J., Krzewski, Konrad, Gilmour, Kimberly C., Ehl, Stephan, Abboud, Miguel R, Aytac, Sevkiye Selin, Bosse, Franziskus Johannes, Choo, Sharon, Drabko, Katarzyna, Onkologii, Klinika, Elfeky, Reem, El-Ghoneimy, Dalia Helmy, Fadoo, Zehra, Greenwood, Tatiana, Gustafsson, Britt, Hagelberg, Stefan, Hasle, Henrik, Hästbacka, Johanna, Jadrešin, Oleg, Jädersten, Martin, Kaya, Zuhre, Lecumberri, Ranon, Marques, Laura, Mushtaq, Naureen, Naqvi, Ahmed, Neves, João Farela, Nunes, Susana, Paucar, Martin, Payne, Jeanette H., Rascon, Jelena, Ruuska, Terhi Susanna, Saribeyoglu, Ebru Tugrul, Sundin, Mikael C., Svedenkrans, Jenny, Świderska, Natalia, Tedgård, Ulf, Tvedt, Tor Henrik, Ünüvar, Ayşegül, Van Laar, Jan A. M., Weitzman, Sheila, Winiarski, Jacek, Yaseen, Muhamma Zohaib, Yildiz, Mehmet, Zantomio, Daniela, Øra, Ingrid, Øverland, Torstein, Ljunggren, Hans-Gustaf, Nordenskjöld, Magnus, Horne, AnnaCarin, Henter, Jan-Inge, Meeths, Marie, and Bryceson, Yenan T.

Abstract

•TCR-triggered T-cell and Fc receptor–triggered NK-cell assays are most accurate for diagnosing defective cytotoxic lymphocyte exocytosis.•The standard K562 cell assay has high interindividual variability and is affected by expanded NK-cell subsets and transportation stress.

Published

2024

5. Optimized cytogenetic risk-group stratification of KMT2A-rearranged pediatric acute myeloid leukemia

Author

van Weelderen, Romy E., Harrison, Christine J., Klein, Kim, Jiang, Yilin, Abrahamsson, Jonas, Alonzo, Todd, Aplenc, Richard, Arad-Cohen, Nira, Bart-Delabesse, Emmanuelle, Buldini, Barbara, De Moerloose, Barbara, Dworzak, Michael N., Elitzur, Sarah, Fernández Navarro, José M., Gamis, Alan, Gerbing, Robert B., Goemans, Bianca F., de Groot-Kruseman, Hester A., Guest, Erin, Ha, Shau-Yin, Hasle, Henrik, Kelaidi, Charikleia, Lapillonne, Hélène, Leverger, Guy, Locatelli, Franco, Miyamura, Takako, Norén-Nyström, Ulrika, Polychronopoulou, Sophia, Rasche, Mareike, Rubnitz, Jeffrey E., Stary, Jan, Tierens, Anne, Tomizawa, Daisuke, Zwaan, C. Michel, and Kaspers, Gertjan J. L.

Abstract

•We clinically characterized 3 additional, recurring KMT2A-r groups and identified specific ACAs of independent prognostic significance.•We present an optimized, fusion-based risk-group stratification of KMT2A-r pediatric AML.

Published

2024

6. Measurable Residual Disease and Fusion Partner Independently Predict Survival and Relapse Risk in Childhood KMT2A -Rearranged Acute Myeloid Leukemia: A Study by the International Berlin-Frankfurt-Münster Study Group.

Author

van Weelderen, Romy E., Klein, Kim, Harrison, Christine J., Jiang, Yilin, Abrahamsson, Jonas, Arad-Cohen, Nira, Bart-Delabesse, Emmanuelle, Buldini, Barbara, De Moerloose, Barbara, Dworzak, Michael N., Elitzur, Sarah, Fernández Navarro, José M., Gerbing, Robert B., Goemans, Bianca F., de Groot-Kruseman, Hester A., Guest, Erin, Ha, Shau-Yin, Hasle, Henrik, Kelaidi, Charikleia, and Lapillonne, Hélène

Published

2023

7. Survival outcomes of children with relapsed or refractory myeloid leukemia associated with Down syndrome

Author

Raghuram, Nikhil, Hasegawa, Daisuke, Nakashima, Kentaro, Rahman, Syaza, Antoniou, Evangelia, Skajaa, Torjus, Merli, Pietro, Verma, Anupam, Rabin, Karen R., Aftandilian, Catherine, Kotecha, Rishi S., Cheuk, Daniel, Jahnukainen, Kirsi, Kolenova, Alexandra, Balwierz, Walentyna, Norton, Alice, O’Brien, Maureen, Cellot, Sonia, Chopek, Ashley, Arad-Cohen, Nira, Goemans, Bianca, Rojas-Vasquez, Marta, Ariffin, Hany, Bartram, Jack, Kolb, E. Anders, Locatelli, Franco, Klusmann, Jan-Henning, Hasle, Henrik, McGuire, Bryan, Hasnain, Afia, Sung, Lillian, and Hitzler, Johann

Abstract

•Treatment outcomes for relapsed or refractory ML-DS remain dismal in a contemporary treatment period (3-year OS 22%).•Patients who had a long duration of first remission, achieved a second remission and underwent HSCT were most likely to survive.

Published

2023

8. Hypodiploidy has unfavorable impact on survival in pediatric acute myeloid leukemia: an I-BFM Study Group collaboration

Author

Hammer, Anne Sofie Borg, Juul-Dam, Kristian Løvvik, Sandahl, Julie Damgaard, Abrahamsson, Jonas, Czogala, Malgorzata, Delabesse, Emmanuelle, Haltrich, Iren, Jahnukainen, Kirsi, Kolb, E. Anders, Kovács, Gábor, Leverger, Guy, Locatelli, Franco, Masetti, Riccardo, Noren-Nyström, Ulrika, Raimondi, Susana C., Rasche, Mareike, Reinhardt, Dirk, Taki, Tomohiko, Tomizawa, Daisuke, Zeller, Bernward, Hasle, Henrik, and Kjeldsen, Eigil

Abstract

Hypodiploidy, defined as modal numbers (MNs) 45 or lower, has not been independently investigated in pediatric acute myeloid leukemia (AML) but is a well-described high-risk factor in pediatric acute lymphoblastic leukemia. We aimed to characterize and study the prognostic impact of hypodiploidy in pediatric AML. In this retrospective cohort study, we included children below 18 years of age with de novo AML and a hypodiploid karyotype diagnosed from 2000 to 2015 in 14 childhood AML groups from the International Berlin-Frankfurt-Münster (I-BFM) framework. Exclusion criteria comprised constitutional hypodiploidy, monosomy 7, composite karyotype, and t(8;21) with concurring sex chromosome loss. Hypodiploidy occurred in 81 patients (1.3%) with MNs, 45 (n = 66); 44 (n = 10) and 43 (n = 5). The most frequently lost chromosomes were chromosome 9 and sex chromosomes. Five-year event-free survival (EFS) and overall survival (OS) were 34% and 52%, respectively, for the hypodiploid cohort. Children with MN≤44 (n = 15) had inferior EFS (21%) and OS (33%) compared with children with MN = 45 (n = 66; EFS, 37%; OS, 56%). Adjusted hazard ratios (HRs) were 4.9 (P = .001) and 6.1 (P = .003). Monosomal karyotype or monosomy 9 had particular poor OS (43% and 15%, respectively). Allogeneic stem cell transplantation (SCT) in first complete remission (CR1) (n = 18) did not mitigate the unfavorable outcome of hypodiploidy (adjusted HR for OS was 1.5; P = .42). We identified pediatric hypodiploid AML as a rare subgroup with an inferior prognosis even in the patients treated with SCT in CR1.

Published

2023

9. Hypodiploidy has unfavorable impact on survival in pediatric acute myeloid leukemia: an I-BFM Study Group collaboration

Author

Hammer, Anne Sofie Borg, Juul-Dam, Kristian Løvvik, Sandahl, Julie Damgaard, Abrahamsson, Jonas, Czogala, Malgorzata, Delabesse, Emmanuelle, Haltrich, Iren, Jahnukainen, Kirsi, Kolb, E. Anders, Kovács, Gábor, Leverger, Guy, Locatelli, Franco, Masetti, Riccardo, Noren-Nyström, Ulrika, Raimondi, Susana C., Rasche, Mareike, Reinhardt, Dirk, Taki, Tomohiko, Tomizawa, Daisuke, Zeller, Bernward, Hasle, Henrik, and Kjeldsen, Eigil

Abstract

•Hypodiploidy is found in <2% of pediatric AML. No patient had modal number below 43.•Poor survival is observed in hypodiploid AML with aggravating prognosis in patients with modal number 43 to 44.

Published

2023

10. Glucocorticosteroid and Silicone Gel During Patch Application Without Clinical Scar Improvement After Central Venous Catheter Removal: A Randomized Trial

Author

Nissen, Ida Bo, Handrup, Mette Møller, Bang, Karen, and Hasle, Henrik

Published

2022

11. Abdominal Complications During Treatment for Pediatric Acute Myeloid Leukemia

Author

Borgstedt-Bendixen, Sofie E., Abrahamsson, Jonas, Ha, Shau-Yin, Koskenvuo, Minna, Lausen, Birgitte, Palle, Josefine, Zeller, Bernward, Hasle, Henrik, and Løhmann, Ditte J.A.

Abstract

Acute myeloid leukemia (AML) accounts for 15% to 20% of childhood leukemias. Because of high-intensive therapy, up to 5% of patients suffer from treatment-related mortality (TRM). Abdominal complications are frequent, however, literature on this subject is sparse. We aimed to characterize severe abdominal pain (AP) and hyperbilirubinemia experienced by pediatric AML patients treated according to the Nordic Society of Pediatric Hematology and Oncology (NOPHO)-AML 2004 protocol (n=313). Patients were censored at hematopoietic stem cell transplantation and relapse. Toxicity information was collected prospectively. Additional information was requested retrospectively from the treating centers. Sixteen episodes of hyperbilirubinemia and 107 episodes of AP were reported. The treating centers deemed infection (30%) and typhlitis (18%) as the most frequent causes of AP. Six patients developed appendicitis (2%). Patients experiencing concurrent AP and sepsis had a high risk of TRM (36%, n=4). Eighty percent of episodes with hyperbilirubinemia fulfilled the European Society for Bone and Marrow Transplantation criteria for sinusoidal obstruction syndrome. In conclusion, abdominal complications were frequent with infection considered the predominate cause. Most patients with hyperbilirubinemia fulfilled the criteria for sinusoidal obstruction syndrome. AML treatment might be associated with appendicitis. Patients suffering from concurrent AP and sepsis had a high risk of TRM indicating that high awareness of abdominal complications is essential to reduce mortality, especially during sepsis.

Published

2022

12. Second allogeneic stem cell transplantation can rescue a significant proportion of patients with JMML relapsing after first allograft

Author

Vinci, Luca, Flotho, Christian, Noellke, Peter, Lebrecht, Dirk, Masetti, Riccardo, de Haas, Valerie, De Moerloose, Barbara, Dworzak, Michael, Hasle, Henrik, Güngör, Tayfun, Starý, Jan, Turkiewicz, Dominik, Ussowicz, Marek, de Heredia, Cristina Diaz, Buechner, Jochen, Jahnukainen, Kirsi, Kallay, Krisztian, Bodova, Ivana, Smith, Owen P., Zecca, Marco, Bresters, Dorine, Lang, Peter, Masmas, Tania Nicole, Meisel, Roland, Pichler, Herbert, Erlacher, Miriam, Göhring, Gudrun, Locatelli, Franco, Strahm, Brigitte, Niemeyer, Charlotte M., and Yoshimi, Ayami

Published

2023

13. Germline GATA1s-generating mutations predispose to leukemia with acquired trisomy 21 and Down syndrome-like phenotype

Author

Hasle, Henrik, Kline, Ronald M., Kjeldsen, Eigil, Nik-Abdul-Rashid, Nik F., Bhojwani, Deepa, Verboon, Jeffrey M., DiTroia, Stephanie P., Chao, Katherine R., Raaschou-Jensen, Klas, Palle, Josefine, Zwaan, C. Michel, Nyvold, Charlotte Guldborg, Sankaran, Vijay G., and Cantor, Alan B.

Abstract

Individuals with Down syndrome are at increased risk of myeloid leukemia in early childhood, which is associated with acquisition of GATA1 mutations that generate a short GATA1 isoform called GATA1s. Germline GATA1s-generating mutations result in congenital anemia in males. We report on 2 unrelated families that harbor germline GATA1s-generating mutations in which several members developed acute megakaryoblastic leukemia in early childhood. All evaluable leukemias had acquired trisomy 21 or tetrasomy 21. The leukemia characteristics overlapped with those of myeloid leukemia associated with Down syndrome, including age of onset at younger than 4 years, unique immunophenotype, complex karyotype, gene expression patterns, and drug sensitivity. These findings demonstrate that the combination of trisomy 21 and GATA1s-generating mutations results in a unique myeloid leukemia independent of whether the GATA1 mutation or trisomy 21 is the primary or secondary event and suggest that there is a unique functional cooperation between GATA1s and trisomy 21 in leukemogenesis. The family histories also indicate that germline GATA1s-generating mutations should be included among those associated with familial predisposition for myelodysplastic syndrome and leukemia.

Published

2022

14. M-ficolin: a valuable biomarker to identify leukaemia from juvenile idiopathic arthritis

Author

Brix, Ninna, Glerup, Mia, Thiel, Steffen, Mistegaard, Clara Elbæk, Skals, Regitze Gyldenholm, Berntson, Lillemor, Fasth, Anders, Nielsen, Susan Mary, Nordal, Ellen, Rygg, Marite, Hasle, Henrik, Albertsen, Birgitte Klug, and Herlin, Troels

Abstract

ObjectiveDistinction on clinical grounds between acute lymphoblastic leukaemia presenting with arthropathy (ALLarthropathy) and juvenile idiopathic arthritis (JIA) is difficult, as the clinical and paraclinical signs of leukaemia may be vague. The primary aim was to examine the use of lectin complement pathway proteins as markers to differentiate ALLarthropathyfrom JIA. The secondary aims were to compare the protein levels at baseline and follow-up in a paired number of children with ALL and to examine the correlation with haematology counts, erythrocyte sedimentation reaction (ESR), C-reactive protein (CRP), blasts, relapse and death.Study designIn this observational study, we measured M-ficolin, CL-K1 and MASP-3 in serum from children with ALL (n=151) and JIA (n=238) by time-resolved immunofluorometric assays. Logistic regression was used for predictions of ALL risk, considering the markers as the respective exposures. We performed internal validation using repeated ‘10-fold cross-validation’ with 100 repetitions computing the area under the curve (AUC) as well as positive and negative predictive values in order to evaluate the predictive performance.ResultsThe level of M-ficolin was higher in JIA than ALLtotaland the ALLarthropathysubgroup. The M-ficolin level normalised after remission of ALL. M-ficolin could differentiate ALL from JIA with an AUC of 94% and positive predictive value (PPV) of 95%, exceeding CRP and haemoglobin. In a dichotomised predictive model with optimal cut-offs for M-ficolin, platelets and haemoglobin, AUC was 99% and PPV 98% in detecting ALL from JIA.ConclusionM-ficolin is a valuable marker to differentiate the child with ALL from JIA.

Published

2022

15. Psychiatric disorders in childhood cancer survivors in Denmark, Finland, and Sweden: a register-based cohort study from the SALiCCS research programme

Author

Frederiksen, Line Elmerdahl, Erdmann, Friederike, Mader, Luzius, Mogensen, Hanna, Pedersen, Camilla, Kenborg, Line, Bautz, Andrea, Talbäck, Mats, Hirvonen, Elli, Nielsen, Thomas Tjørnelund, Andersen, Elisabeth Anne Wreford, Holmqvist, Anna Sällfors, Jørgensen, Ole Sylvester, Jepsen, Jens Richardt Møllegaard, Malila, Nea, Hasle, Henrik, Madanat-Harjuoja, Laura, Feychting, Maria, and Winther, Jeanette Falck

Abstract

A childhood cancer diagnosis and treatment-induced somatic late effects can affect the long-term mental health of survivors. We aimed to explore whether childhood cancer survivors are at higher risk of psychiatric disorders later in life than their siblings and the general population.

Published

2022

16. Association of unbalanced translocation der(1;7) with germline GATA2 mutations

Author

Kozyra, Emilia J., Göhring, Gudrun, Hickstein, Dennis D., Calvo, Katherine R., DiNardo, Courtney D., Dworzak, Michael, de Haas, Valerie, Starý, Jan, Hasle, Henrik, Shimamura, Akiko, Fleming, Mark D., Inaba, Hiroto, Lewis, Sara, Hsu, Amy P., Holland, Steven M., Arnold, Danielle E., Mecucci, Cristina, Keel, Siobán B., Bertuch, Alison A., Tawana, Kiran, Barzilai, Shlomit, Hirabayashi, Shinsuke, Onozawa, Masahiro, Lei, Shaohua, Alaiz, Helena, Andrikovics, Hajnalka, Betts, David, Beverloo, Berna H., Buechner, Jochen, Čermák, Martin, Cervera, José, Haus, Olga, Jahnukainen, Kirsi, Manola, Kalliopi N., Nebral, Karin, Pasquali, Francesco, Tchinda, Joelle, Turkiewicz, Dominik, Van Roy, Nadine, Zemanova, Zuzana, Pastor, Victor B., Strahm, Brigitte, Noellke, Peter, Niemeyer, Charlotte M., Schlegelberger, Brigitte, Yoshimi, Ayami, and Wlodarski, Marcin W.

Published

2021

17. Hematopoietic stem cell transplantation in children and adolescents with GATA2-related myelodysplastic syndrome

Author

Bortnick, Rachel, Wlodarski, Marcin, de Haas, Valerie, De Moerloose, Barbara, Dworzak, Michael, Hasle, Henrik, Masetti, Riccardo, Starý, Jan, Turkiewicz, Dominik, Ussowicz, Marek, Kozyra, Emilia, Albert, Michael, Bader, Peter, Bordon, Victoria, Cario, Gunnar, Beier, Rita, Schulte, Johannes, Bresters, Dorine, Müller, Ingo, Pichler, Herbert, Sedlacek, Petr, Sauer, Martin G., Zecca, Marco, Göhring, Gudrun, Yoshimi, Ayami, Noellke, Peter, Erlacher, Miriam, Locatelli, Franco, Niemeyer, Charlotte M., and Strahm, Brigitte

Abstract

GATA2 deficiency is a heterogeneous multi-system disorder characterized by a high risk of developing myelodysplastic syndrome (MDS) and myeloid leukemia. We analyzed the outcome of 65 patients reported to the registry of the European Working Group (EWOG) of MDS in childhood carrying a germline GATA2mutation (GATA2mut) who had undergone hematopoietic stem cell transplantation (HSCT). At 5 years the probability of overall survival and disease-free survival (DFS) was 75% and 70%, respectively. Non-relapse mortality and relapse equally contributed to treatment failure. There was no evidence of increased incidence of graft-versus-host-disease or excessive rates of infections or organ toxicities. Advanced disease and monosomy 7 (−7) were associated with worse outcome. Patients with refractory cytopenia of childhood (RCC) and normal karyotype showed an excellent outcome (DFS 90%) compared to RCC and −7 (DFS 67%). Comparing outcome of GATA2mutwith GATA2wtpatients, there was no difference in DFS in patients with RCC and normal karyotype. The same was true for patients with −7 across morphological subtypes. We demonstrate that HSCT outcome is independent of GATA2germline mutations in pediatric MDS suggesting the application of standard MDS algorithms and protocols. Our data support considering HSCT early in the course of GATA2 deficiency in young individuals.

Published

2021

18. Clinical evolution, genetic landscape and trajectories of clonal hematopoiesis in SAMD9/SAMD9L syndromes

Author

Sahoo, Sushree S., Pastor, Victor B., Goodings, Charnise, Voss, Rebecca K., Kozyra, Emilia J., Szvetnik, Amina, Noellke, Peter, Dworzak, Michael, Starý, Jan, Locatelli, Franco, Masetti, Riccardo, Schmugge, Markus, De Moerloose, Barbara, Catala, Albert, Kállay, Krisztián, Turkiewicz, Dominik, Hasle, Henrik, Buechner, Jochen, Jahnukainen, Kirsi, Ussowicz, Marek, Polychronopoulou, Sophia, Smith, Owen P., Fabri, Oksana, Barzilai, Shlomit, de Haas, Valerie, Baumann, Irith, Schwarz-Furlan, Stephan, Niewisch, Marena R., Sauer, Martin G., Burkhardt, Birgit, Lang, Peter, Bader, Peter, Beier, Rita, Müller, Ingo, Albert, Michael H., Meisel, Roland, Schulz, Ansgar, Cario, Gunnar, Panda, Pritam K., Wehrle, Julius, Hirabayashi, Shinsuke, Derecka, Marta, Durruthy-Durruthy, Robert, Göhring, Gudrun, Yoshimi-Noellke, Ayami, Ku, Manching, Lebrecht, Dirk, Erlacher, Miriam, Flotho, Christian, Strahm, Brigitte, Niemeyer, Charlotte M., and Wlodarski, Marcin W.

Abstract

Germline SAMD9and SAMD9Lmutations (SAMD9/9Lmut) predispose to myelodysplastic syndromes (MDS) with propensity for somatic rescue. In this study, we investigated a clinically annotated pediatric MDS cohort (n= 669) to define the prevalence, genetic landscape, phenotype, therapy outcome and clonal architecture of SAMD9/9L syndromes. In consecutively diagnosed MDS, germline SAMD9/9Lmutaccounted for 8% and were mutually exclusive with GATA2mutations present in 7% of the cohort. Among SAMD9/9Lmutcases, refractory cytopenia was the most prevalent MDS subtype (90%); acquired monosomy 7 was present in 38%; constitutional abnormalities were noted in 57%; and immune dysfunction was present in 28%. The clinical outcome was independent of germline mutations. In total, 67 patients had 58 distinct germline SAMD9/9Lmutclustering to protein middle regions. Despite inconclusive in silico prediction, 94% of SAMD9/9Lmutsuppressed HEK293 cell growth, and mutations expressed in CD34+cells induced overt cell death. Furthermore, we found that 61% of SAMD9/9Lmutpatients underwent somatic genetic rescue (SGR) resulting in clonal hematopoiesis, of which 95% was maladaptive (monosomy 7 ± cancer mutations), and 51% had adaptive nature (revertant UPD7q, somatic SAMD9/9Lmut). Finally, bone marrow single-cell DNA sequencing revealed multiple competing SGR events in individual patients. Our findings demonstrate that SGR is common in SAMD9/9LmutMDS and exemplify the exceptional plasticity of hematopoiesis in children.

Published

2021

19. Synonymous GATA2mutations result in selective loss of mutated RNA and are common in patients with GATA2 deficiency

Author

Kozyra, Emilia J., Pastor, Victor B., Lefkopoulos, Stylianos, Sahoo, Sushree S., Busch, Hauke, Voss, Rebecca K., Erlacher, Miriam, Lebrecht, Dirk, Szvetnik, Enikoe A., Hirabayashi, Shinsuke, Pasaulienė, Ramunė, Pedace, Lucia, Tartaglia, Marco, Klemann, Christian, Metzger, Patrick, Boerries, Melanie, Catala, Albert, Hasle, Henrik, de Haas, Valerie, Kállay, Krisztián, Masetti, Riccardo, De Moerloose, Barbara, Dworzak, Michael, Schmugge, Markus, Smith, Owen, Starý, Jan, Mejstrikova, Ester, Ussowicz, Marek, Morris, Emma, Singh, Preeti, Collin, Matthew, Derecka, Marta, Göhring, Gudrun, Flotho, Christian, Strahm, Brigitte, Locatelli, Franco, Niemeyer, Charlotte M., Trompouki, Eirini, and Wlodarski, Marcin W.

Abstract

Deficiency of the transcription factor GATA2 is a highly penetrant genetic disorder predisposing to myelodysplastic syndromes (MDS) and immunodeficiency. It has been recognized as the most common cause underlying primary MDS in children. Triggered by the discovery of a recurrent synonymous GATA2variant, we systematically investigated 911 patients with phenotype of pediatric MDS or cellular deficiencies for the presence of synonymous alterations in GATA2. In total, we identified nine individuals with five heterozygous synonymous mutations: c.351C>G, p.T117T (N= 4); c.649C>T, p.L217L; c.981G>A, p.G327G; c.1023C>T, p.A341A; and c.1416G>A, p.P472P (N= 2). They accounted for 8.2% (9/110) of cases with GATA2 deficiency in our cohort and resulted in selective loss of mutant RNA. While for the hotspot mutation (c.351C>G) a splicing error leading to RNA and protein reduction was identified, severe, likely late stage RNA loss without splicing disruption was found for other mutations. Finally, the synonymous mutations did not alter protein function or stability. In summary, synonymous GATA2substitutions are a new common cause of GATA2 deficiency. These findings have broad implications for genetic counseling and pathogenic variant discovery in Mendelian disorders.

Published

2020

20. Genetic variation of cisplatin-induced ototoxicity in non-cranial-irradiated pediatric patients using a candidate gene approach: The International PanCareLIFE Study

Author

Clemens, Eva, Broer, Linda, Langer, Thorsten, Uitterlinden, André G., de Vries, Andrica C. H., van Grotel, Martine, Pluijm, Saskia F. M., Binder, Harald, Byrne, Julianne, Broeder, Eline van Dulmen-den, Crocco, Marco, Grabow, Desiree, Kaatsch, Peter, Kaiser, Melanie, Kenborg, Line, Winther, Jeanette F., Rechnitzer, Catherine, Hasle, Henrik, Kepak, Tomas, van der Kooi, Anne-Lotte F., Kremer, Leontien C., Kruseova, Jarmila, Kuehni, Claudia E., van der Pal, Heleen, Parfitt, Ross, Deuster, Dirk, Matulat, Peter, Spix, Claudia, Tillmanns, Amelie, Tissing, Wim J. E., Maier, Lara, am Zehnhoff-Dinnesen, Antoinette, Zolk, Oliver, and van den Heuvel-Eibrink, Marry M.

Abstract

Ototoxicity is a common side effect of platinum treatment and manifests as irreversible, high-frequency sensorineural hearing loss. Genetic association studies have suggested a role for SNPs in genes related to the disposition of cisplatin or deafness. In this study, 429 pediatric patients that were treated with cisplatin were genotyped for 10 candidate SNPs. Logistic regression analyses revealed that younger age at treatment (≤5 years vs >15 years: OR: 9.1; 95% CI: 3.8–21.5; P= 5.6 × 10−7) and higher cumulative dose of cisplatin (>450 vs ≤300 mg/m2: OR: 2.4; 95% CI: 1.3–4.6; P= 0.007) confer a significant risk of ototoxicity. Of the SNPs investigated, none of them were significantly associated with an increase of ototoxicity. In the meta-analysis, ACYP2rs1872328 (OR: 3.94; 95% CI: 1.04–14.03; P= 0.04) and SLC22A2rs316019 (OR: 1.46; 95% CI: 1.07–2.00; P= 0.02) were associated with ototoxicity. In order to increase the understanding of the association between SNPs and ototoxicity, we propose a polygenic model, which takes into account multiple interacting genes of the cisplatin pathway that together confer an increased risk of ototoxicity.

Published

2020

21. A phase 3 randomized trial of mavorixafor, a CXCR4 antagonist, for WHIM syndrome

Author

Badolato, Raffaele, Alsina, Laia, Azar, Antoine, Bertrand, Yves, Bolyard, Audrey A., Dale, David, Deyà-Martínez, Angela, Dickerson, Kathryn E., Ezra, Navid, Hasle, Henrik, Kang, Hyoung Jin, Kiani-Alikhan, Sorena, Kuijpers, Taco W., Kulagin, Alexander, Langguth, Daman, Levin, Carina, Neth, Olaf, Olbrich, Peter, Peake, Jane, Rodina, Yulia, Rutten, Caroline E., Shcherbina, Anna, Tarrant, Teresa K., Vossen, Matthias G., Wysocki, Christian A., Belschner, Andrea, Bridger, Gary J., Chen, Kelly, Dubuc, Susan, Hu, Yanping, Jiang, Honghua, Li, Sunny, MacLeod, Rick, Stewart, Murray, Taveras, Arthur G., Yan, Tina, and Donadieu, Jean

Abstract

•Treatment with the oral CXCR4 antagonist mavorixafor resulted in increased levels of absolute neutrophil and lymphocyte counts vs placebo.•Infection frequency, severity, and duration were decreased with mavorixafor treatment vs placebo. Mavorixafor was well tolerated.

Published

2024

22. Long-term health outcomes in survivors of childhood AML treated with allogeneic HSCT: a NOPHO–AML Study

Author

Wilhelmsson, Mari, Glosli, Heidi, Ifversen, Marianne, Abrahamsson, Jonas, Winiarski, Jacek, Jahnukainen, Kirsi, and Hasle, Henrik

Abstract

Allogeneic hematopoietic stem cell transplantation (allo-HSCT) improves event-free survival in acute myeloid leukemia (AML); however, the burden of late effects may be increased. We compared health-related outcomes in childhood AML survivors treated according to the NOPHO-AML protocols either with or without allo-HSCT at age < 21 years. Out of the 147 eligible AML survivors treated with allo-HSCT, 95 (65%) and 53 (75%) of their eligible siblings completed a questionnaire. Their data were compared to corresponding data collected previously from NOPHO-AML survivors treated with chemotherapy only (CT) (n= 101). The median follow-up was 12 (range 2–28) years after allo-HSCT and 47% had received total body irradiation (TBI)-based conditioning. Allo-HSCT survivors reported significantly more physical health limitations (39% vs 7%, p< 0.005), medications for cardiovascular disease (10% vs 1%, p< 0.05) and use of analgesics (32% vs 11%, p< 0.01) than CT survivors. Health problems prevented 16% of the allo-HSCT survivors from attending school or managing a job vs. 3% among CT survivors (p< 0.05). Among 73 allo-HSCT survivors (age ≥ 15 years), seven females reported natural pregnancies and three males reported unassisted conceptions in partners. Survivors of childhood AML treated with allo-HSCT experienced more physical health limitations and used more medications than the survivors treated with chemotherapy only.

Published

2019

23. Disease-specific Hospitalizations Among 5-Year Survivors of Hepatoblastoma: A Nordic Population-based Cohort Study

Author

Bonnesen, Trine G., Asdahl, Peter H., de Fine Licht, Sofie, Gudmundsdottir, Thorgerdur, Holmqvist, Anna S., Madanat-Harjuoja, Laura-Maria, Tryggvadottir, Laufey, Winther, Jeanette F., and Hasle, Henrik

Abstract

Supplemental Digital Content is available in the text.

Published

2019

24. Hearing Status in Survivors of Childhood Acute Myeloid Leukemia Treated With Chemotherapy Only: A NOPHO-AML Study

Author

Skou, Anne-Sofie, Olsen, Steen Ø., Nielsen, Lars H., Glosli, Heidi, Jahnukainen, Kirsi, Jarfelt, Marianne, Jónmundsson, Guðmundur K., Malmros, Johan, Nysom, Karsten, and Hasle, Henrik

Published

2019

25. Inflammatory Biomarkers Can Differentiate Acute Lymphoblastic Leukemia with Arthropathy from Juvenile Idiopathic Arthritis Better Than Standard Blood Tests.

Author

Brix, Ninna, Glerup, Mia, Foell, Dirk, Kessel, Christoph, Wittkowski, Helmut, Berntson, Lillemor, Fasth, Anders, Nielsen, Susan, Nordal, Ellen, Rygg, Marite, Hasle, Henrik, and Herlin, Troels

Published

2023

26. Early Peripheral Blood Blast Clearance As a Prognostic Marker for Early Treatment Response in Pediatric Acute Myeloid Leukemia

Author

Wijnen, Noa E., de Boer, Bianca, Klein, Kim, Abrahamsson, Jonas, De Moerloose, Barbara, Zeller, Bernward, Hasle, Henrik, Kovalova, Zhanna, Arad-Cohen, Nira, and Kaspers, Gertjan J.L.

Abstract

Background and Significance

Published

2023

27. ATMGermline Pathogenic Variants Affect Treatment Outcomes in Children with Acute Lymphoblastic Leukemia/Lymphoma and Ataxia Telangiectasia

Author

Elitzur, Sarah, Shiloh, Ruth, Loeffen, Jan, Pastorczak, Agata, Takagi, Masatoshi, Bomken, Simon, Baruchel, Andre, Ducassou, Stephane, Mahlaoui, Nizar, Strullu, Marion, Lehrnbecher, Thomas, Schmiegelow, Kjeld, Abla, Oussama, Anderzhanova, Liliia, Arad-Cohen, Nira, Astigarraga, Itziar, Ben-Harosh, Miriam, Ceppi, Francesco, Bodmer, Nicole, Brozou, Triantafyllia, Dalla-Pozza, Luciano, Escherich, Gabriele, Farah, Roula, Gibson, Amber, Hasle, Henrik, Hoveyan, Julieta, Jacoby, Elad, Jazbec, Janez, Kolenova, Alexandra, Lazic, Jelena, Lo Nigro, Luca, Miller, Lane, Papadakis, Vassilios, Pecheux, Lucie, Pillon, Marta, Sarouk, Ifat, Stary, Jan, Stiakaki, Eftichia, Tasian, Sarah K., Tran, Thai Hoa, Ussowicz, Marek, Verdu-Amoros, Jose Jaime, Wakulinska, Anna, Zawitkowska, Joanna, Stoppa-Lyonnet, Dominique, Taylor, Malcolm, Shiloh, Yosef, Izraeli, Shai, Nirel, Ronit, Minard-Colin, Veronique, Attarbaschi, Andishe, and Borkhardt, Arndt

Abstract

IntroductionAtaxia telangiectasia (A-T) is a multisystem disorder caused by biallelic germline pathogenic variants (PV) in the ATM gene. An important feature of A-T is an increased predisposition to cancer with a reported incidence of 25%, primarily attributed to hematological malignancies. Patients with A-T and cancer are usually excluded from therapeutic clinical trials, limited information thus exists concerning their treatment outcomes and toxicity profiles and consequently, optimal management strategies are unclear and an unmet need. In this multinational study, we aimed to investigate the characteristics and outcomes of leukemia and lymphoma in a large cohort of children with A-T and to determine risk factors which impact treatment outcome in order to generate consensus and data-based prospective treatment recommendations.

Published

2023

28. Management of Hyperleukocytosis in Pediatric Acute Myeloid Leukemia Using Immediate Chemotherapy without Leukapheresis, in Protocol NOPHO-DBH AML-2012

Author

Zeller, Bernward, Arad-Cohen, Nira, Cheuk, Daniel, De Moerloose, Barbara, Fernandez Navarro, Jose Maria, Hasle, Henrik, Kirsi, Jahnukainen, Juul-Dam, Kristian, Kaspers, Gertjan J.L., Kovalova, Zhanna, Lausen, Birgitte, Munthe-Kaas, Monica C., Norén-Nyström, Ulrika, Palle, Josefine, Pasauliene, Ramune, Pronk, Cornelis Jan, Saks, Kadri, Tierens, Anne Maria, and Abrahamsson, Jonas

Abstract

Introduction: Hyperleukocytosis (HL) in pediatric acute myeloid leukemia (AML) is associated with severe complications and inferior outcome. Initial management is subject to debate, and the role of invasive methods such as leukapheresis (LA) and exchange transfusion (ET) has been questioned. We report the results on HL patients included in the NOPHO-DBH AML 2012 study.

Published

2023

29. Chip-AML22 Master Protocol: An Open-Label Clinical Trial in Newly Diagnosed Pediatric De Novo Acute Myeloid Leukemia (AML) Patients Including a Linked Phase II Trial with Quizartinib in FLT3-ITD/ NPM1wt Patients - a Study By the NOPHO-DB-SHIP Consortium

Author

Kaspers, Gertjan J.L., Wijnen, Noa E., Koedijk, Joost B., Ishimaru, Sae, Benedictus, Renske, Van Opstal, Ellen C., Van Tinteren, Harm, Zwaan, C. Michel, Biserna, Noha, Downs, Pamela, Duong, Yvonne, Kamel, Yasser Mostafa, Abrahamsson, Jonas, Arad-Cohen, Nira, Bodmer, Nicole, Castillo, Luis, Cheuk, Daniel, Costa, Vitor, De Moerloose, Barbara, Fernandez Navarro, Jose Maria, Fogelstrand, Linda, Goemans, Bianca F., Hasle, Henrik, Jonsson, Olafur G., Kovalova, Zhanna, Munthe-Kaas, Monica C., Norén-Nyström, Ulrika, Palmu, Sauli, Pasauliene, Ramune, Saks, Kadri, Tierens, Anne Maria, Turkiewicz, Dominik, and Pronk, Cornelis Jan

Abstract

Background and SignificancePediatric AML is a heterogeneous disease with current rates for event-free survival (EFS) of 50-60% and for overall survival (OS) of 70-80%, for newly diagnosed patients. In patients with refractory and relapsed disease, and in subsets as defined by AML biology and treatment response, prognosis is dismal. To further improve EFS, the NOPHO-DB-SHIP consortium has initiated trial CHIP-AML22. Building on the successes achieved by the recent trial from this consortium (NOPHO-DBH AML-2012, preliminary data as per June 2023, n=878: 5-years pEFS 63%, 5-years pOS 78%), CHIP-AML22 will incorporate innovative elements, mainly the FLT3-inhibitor quizartinib (Vanflyta®) that was recently approved by the FDA and PMDA in combination with chemotherapy for the treatment of newly diagnosed adult AML patients with FLT3-ITD mutations, and gemtuzumab ozogamicin (GO, Mylotarg ®) that improved outcome in adult and pediatric AML when added to chemotherapy. CHIP-AML22 will maintain the approach of treatment-response driven risk-adapted treatment, intensified induction treatment for patients with ≥5% AML cells in the bone marrow (BM) after course 1, and consolidation with allogeneic stem cell transplantation (allo-SCT) for high-risk patients after the first consolidation course HAM.

Published

2023

30. Treatment of Molecular Relapses in Pediatric AML Saves Toxicities Prior to Hematopoietic Stem Cell Transplantation (HSCT) - Results of AMoRe2017 Trial

Author

Polutta, Amelie, Reinhardt, Dirk, Baruchel, Andre, Hasle, Henrik, Locatelli, Franco, Zwaan, C. Michel, Frühwald, Michael, Westphal, Silke, Dworzak, Michael, Boztug, Heidrun, Escherich, Gabriele, Lehrnbecher, Thomas, Goemans, Bianca F., Strahm, Brigitte, Schneider, Markus, Hoffmeister, Lina, and Waack, Katharina

Abstract

Introduction

Published

2023

31. Nucleophosmin (NPM1) Type D Genotype Is Associated with Distinct Outcome in Acute Myeloid Leukemia - an AIEOP-BFM and COG-SWOG Intergroup Collaboration

Author

Pigazzi, Martina, Tregnago, Claudia, Ries, Rhonda E, Benetton, Maddalena, Alonzo, Todd A., Duployez, Nicolas, Sonneveld, Edwin, Abrahamsson, Jonas, Fogelstrand, Linda, Von Neuhoff, Nils, Hasle, Henrik, Reinhardt, Dirk, Locatelli, Franco, and Meshinchi, Soheil

Abstract

Background:Nucleophosmin (NPM1) is a nucleo-cytoplasmic shuttling protein, predominantly located in the nucleolus that regulates a multiplicity of different biological processes. NPM1 localization in the cell is finely tuned by the nuclear export signal domain, where two tryptophan residues (Trp) are essential for the nucleolar localization. In acute myeloid leukemia (AML), several genomic subsets of NPM1frameshift mutations of 4 base pair insertions have been identified, with the type A variant (insertion of TCTG) being the most common, followed by type B (CATG) and D (CCTG). More recently, a series of different and rarer frameshifts have been found in adult and pediatric AML. We collected and studied the NPM1insertion genotypes in a large cohort of children with de novoAML enrolled in the AIEOP, BFM, ELAM02, NOPHO, DCOG, COG trials.

Published

2023

32. A Randomized Comparison of Liposomal Daunorubicin/Daunorubicin Combined with Low-Dose Cytarabine and Etoposide or High-Dose Cytarabine and Fludarabine in Induction Treatment of Pediatric AML Using MRD-Based Risk Stratification in the NOPHO-DBH AML 2012 Protocol

Author

De Moerloose, Barbara, Arad-Cohen, Nira, Cheuk, Daniel, Fernandez Navarro, Jose Maria, Hasle, Henrik, Jahnukainen, Kirsi, Kaspers, Gertjan J.L., Kovalova, Zhanna, Lausen, Birgitte, Norén-Nyström, Ulrika, Palle, Josefine, Pasauliene, Ramune, Pronk, Cornelis Jan, Saks, Kadri, Tierens, Anne Maria, Zeller, Bernward, and Abrahamsson, Jonas

Abstract

Background: In pediatric acute myeloid leukemia (AML), measurable residual disease (MRD) by flow cytometry (FCM) after induction therapy has emerged as one of the strongest prognostic factors. We designed a phase III study (NOPHO-DBH AML2012) using an intensified response-guided induction with mainly MRD based risk stratification. All high-risk patients were treated with allogeneic stem cell transplantation (SCT). The study contained two randomized questions: 1) a randomized comparison of mitoxantrone and liposomal daunorubicin (DNX) in first induction which is reported elsewhere and 2) the comparison of AD(x)E (low dose cytarabine, DNX, etoposide) and FLAD(x) (fludarabine, high dose cytarabine, DNX [60 mg/m 2x III]) which was proven effective in refractory/relapsed AML in the second induction course

Published

2023

33. Heterogeneous Gene Fusion Transcripts Found in t(7;12)(q36;p13) Acute Myeloid Leukemia but with Similar Gene Expression Profile

Author

Östlund, Anders, Staffas, Anna, Norén-Nyström, Ulrika, Hasle, Henrik, Fogelstrand, Linda, Abrahamsson, Jonas, and Palmqvist, Lars

Abstract

Cytogenetic aberrations are often involved in acute myeloid leukemia (AML) and can serve as diagnostic markers, prognosis predictors and impact the choice of therapy. A translocation t(7;12)(q36;p13) is reported in up to 20-30% of AML patients typically diagnosed before 24 months of age (Beverloo, Panagopoulos et al. 2001, Cancer Res 61(14): 5374-5377). However, in a retrospective survey of the Nordic Organization of Pediatric Hematology and Oncology (NOPHO) registry, only 4% of reported AML diagnosed before 24 months of age had t(7;12) (Espersen, Noren-Nystrom et al. 2018, Genes Chromosomes Cancer 57(7): 359-365). The t(7;12) is difficult to identify with conventional karyotyping, why the true frequency of t(7;12) may be underestimated. Similarly, the reported prognosis for t(7;12) patients has varied ranging from good (Espersen, Noren-Nystrom et al. 2018) to dismal (von Bergh, van Drunen et al. 2006, Genes Chromosomes Cancer 45(8): 731-739). The translocation has been reported to give rise to an in-frame fusion transcript, MNX1::ETV6. However, detection of this fusion is reported only in 50% of cases in contrast to high expression of MNX1in 100% (von Bergh, van Drunen et al. 2006). The aim of this study was to determine the frequency of the t(7;12) in pediatric AML patients in the NOPHO AML-2004/2012 protocols, their event-free and overall survival and to investigate the presence of additional genetic alterations.

Published

2023

34. Spatial Technologies Reveal the Immune Landscape of Pediatric Acute Myeloid Leukemia

Author

Koedijk, Joost B., Van Der Werf, Inge, Vermeulen, Marijn A., Perzolli, Alicia, Fiocco, Marta F., de Groot-Kruseman, Hester A., Moeniralam, Rubina, Christensen, Kristina B., Hasle, Henrik, Nierkens, Stefan, Belderbos, Mirjam E., Zwaan, Michel C., and Heidenreich, Olaf

Abstract

Pediatric acute myeloid leukemia (AML) is a cancer with a particularly low mutational burden in comparison to other pediatric and adult cancers and therefore, thought to be a poor candidate for T cell-engaging immunotherapies (Gröbner et al., 2018; Pfister et al., 2022). However, little is known about the composition and function of T cells in the bone marrow (BM) of pediatric AML patients. Insight into the frequency and function of BM T cells in children with AML is relevant for naturally occurring AML immune defenses, as well as for T cell-engaging immunotherapies (Koedijk et al., 2021). Here, we performed a multidimensional characterization of the tumor immune microenvironment in children with newly diagnosed AML.

Published

2023

35. Classification of rare pediatric myeloid neoplasia—Quo vadis?

Author

Niemeyer, Charlotte M., Rudelius, Martina, Shimamura, Akiko, Flotho, Christian, Hasle, Henrik, Stieglitz, Elliot, Strahm, Brigitte, Godley, Lucy A., Weinberg, Olga K., Orazi, Attilio, and Calvo, Katherine R.

Published

2022

36. Prognostic impact of t(16;21)(p11;q22) and t(16;21)(q24;q22) in pediatric AML: a retrospective study by the I-BFM Study Group

Author

Noort, Sanne, Zimmermann, Martin, Reinhardt, Dirk, Cuccuini, Wendy, Pigazzi, Martina, Smith, Jenny, Ries, Rhonda E., Alonzo, Todd A., Hirsch, Betsy, Tomizawa, Daisuke, Locatelli, Franco, Gruber, Tanja A., Raimondi, Susana, Sonneveld, Edwin, Cheuk, Daniel K., Dworzak, Michael, Stary, Jan, Abrahamsson, Jonas, Arad-Cohen, Nira, Czogala, Malgorzata, De Moerloose, Barbara, Hasle, Henrik, Meshinchi, Soheil, van den Heuvel-Eibrink, Marry, and Zwaan, C. Michel

Abstract

To study the prognostic relevance of rare genetic aberrations in acute myeloid leukemia (AML), such as t(16;21), international collaboration is required. Two different types of t(16;21) translocations can be distinguished: t(16;21)(p11;q22), resulting in the FUS-ERG fusion gene; and t(16;21)(q24;q22), resulting in RUNX1-core binding factor (CBFA2T3). We collected data on clinical and biological characteristics of 54 pediatric AML cases with t(16;21) rearrangements from 14 international collaborative study groups participating in the international Berlin-Frankfurt-Münster (I-BFM) AML study group. The AML-BFM cohort diagnosed between 1997 and 2013 was used as a reference cohort. RUNX1-CBFA2T3 (n = 23) had significantly lower median white blood cell count (12.5 × 109/L, P = .03) compared with the reference cohort. FUS-ERG rearranged AML (n = 31) had no predominant French-American-British (FAB) type, whereas 76% of RUNX1-CBFA2T3 had an M1/M2 FAB type (M1, M2), significantly different from the reference cohort (P = .004). Four-year event-free survival (EFS) of patients with FUS-ERG was 7% (standard error [SE] = 5%), significantly lower compared with the reference cohort (51%, SE = 1%, P < .001). Four-year EFS of RUNX1-CBFA2T3 was 77% (SE = 8%, P = .06), significantly higher compared with the reference cohort. Cumulative incidence of relapse was 74% (SE = 8%) in FUS-ERG, 0% (SE = 0%) in RUNX1-CBFA2T3, compared with 32% (SE = 1%) in the reference cohort (P < .001). Multivariate analysis identified both FUS-ERG and RUNX1-CBFA2T3 as independent risk factors with hazard ratios of 1.9 (P < .0001) and 0.3 (P = .025), respectively. These results describe 2 clinically relevant distinct subtypes of pediatric AML. Similarly to other core-binding factor AMLs, patients with RUNX1-CBFA2T3 rearranged AML may benefit from stratification in the standard risk treatment, whereas patients with FUS-ERG rearranged AML should be considered high-risk.

Published

2018

37. Prognostic impact of t(16;21)(p11;q22) and t(16;21)(q24;q22) in pediatric AML: a retrospective study by the I-BFM Study Group

Author

Noort, Sanne, Zimmermann, Martin, Reinhardt, Dirk, Cuccuini, Wendy, Pigazzi, Martina, Smith, Jenny, Ries, Rhonda E., Alonzo, Todd A., Hirsch, Betsy, Tomizawa, Daisuke, Locatelli, Franco, Gruber, Tanja A., Raimondi, Susana, Sonneveld, Edwin, Cheuk, Daniel K., Dworzak, Michael, Stary, Jan, Abrahamsson, Jonas, Arad-Cohen, Nira, Czogala, Malgorzata, De Moerloose, Barbara, Hasle, Henrik, Meshinchi, Soheil, van den Heuvel-Eibrink, Marry, and Zwaan, C. Michel

Abstract

To study the prognostic relevance of rare genetic aberrations in acute myeloid leukemia (AML), such as t(16;21), international collaboration is required. Two different types of t(16;21) translocations can be distinguished: t(16;21)(p11;q22), resulting in the FUS-ERGfusion gene; and t(16;21)(q24;q22), resulting in RUNX1-core binding factor (CBFA2T3). We collected data on clinical and biological characteristics of 54 pediatric AML cases with t(16;21) rearrangements from 14 international collaborative study groups participating in the international Berlin-Frankfurt-Münster (I-BFM) AML study group. The AML-BFM cohort diagnosed between 1997 and 2013 was used as a reference cohort. RUNX1-CBFA2T3(n = 23) had significantly lower median white blood cell count (12.5 × 109/L, P= .03) compared with the reference cohort. FUS-ERGrearranged AML (n = 31) had no predominant French-American-British (FAB) type, whereas 76% of RUNX1-CBFA2T3had an M1/M2 FAB type (M1, M2), significantly different from the reference cohort (P= .004). Four-year event-free survival (EFS) of patients with FUS-ERGwas 7% (standard error [SE] = 5%), significantly lower compared with the reference cohort (51%, SE = 1%, P< .001). Four-year EFS of RUNX1-CBFA2T3was 77% (SE = 8%, P= .06), significantly higher compared with the reference cohort. Cumulative incidence of relapse was 74% (SE = 8%) in FUS-ERG, 0% (SE = 0%) in RUNX1-CBFA2T3,compared with 32% (SE = 1%) in the reference cohort (P< .001). Multivariate analysis identified both FUS-ERGand RUNX1-CBFA2T3as independent risk factors with hazard ratios of 1.9 (P< .0001) and 0.3 (P= .025), respectively. These results describe 2 clinically relevant distinct subtypes of pediatric AML. Similarly to other core-binding factor AMLs, patients with RUNX1-CBFA2T3 rearranged AML may benefit from stratification in the standard risk treatment, whereas patients with FUS-ERG rearranged AML should be considered high-risk.

Published

2018

38. Risk-adapted treatment of acute promyelocytic leukemia: results from the International Consortium for Childhood APL

Author

Testi, Anna Maria, Pession, Andrea, Diverio, Daniela, Grimwade, David, Gibson, Brenda, de Azevedo, Amilcar Cardoso, Moran, Lorena, Leverger, Guy, Elitzur, Sarah, Hasle, Henrik, ten Bosch, Jutte van der Werff, Smith, Owen, De Rosa, Marisa, Piciocchi, Alfonso, Lo Coco, Francesco, Foà, Robin, Locatelli, Franco, and Kaspers, Gertjan J. L.

Abstract

Pediatric acute promyelocytic leukemia (APL) can be cured with all-trans retinoic acid (ATRA) and anthracycline. However, most published trials have employed high cumulative doses of anthracyclines. Here, we report the outcome of newly diagnosed APL patients enrolled in the International Consortium for Childhood APL (ICC-APL-01) trial, which reduced anthracycline exposure but extended that of ATRA. The study recruited 258 children/adolescents with molecularly/cytogenetically proven APL. Patients were stratified into standard-risk (SR) and high-risk (HR) groups according to baseline white blood cell counts (<10 × 109/L or ≥10 × 109/L); both groups received identical induction treatment with ATRA and 3 doses of idarubicin. Two or 3 blocks of consolidation therapy were administered to SR and HR patients, respectively, while maintenance therapy with low-dose chemotherapy and ATRA cycles was given to all patients for 2 years. The cumulative dose of daunorubicin equivalent anthracyclines in SR and HR patients was lower than that of previous studies (355 mg/m2 and 405 mg/m2, respectively). Hematologic remission was obtained in 97% of patients; 8 children died of intracranial hemorrhage in the first 2 weeks following diagnosis. Five-year overall and event-free survival for the whole cohort were 94.6% and 79.9%, respectively; they were 98.4% and 89.4% in SR patients and 84.3% and 74.2% in HR patients (P = .002 and P = .043, respectively). These data demonstrate that extended use of ATRA coupled to a risk-adapted consolidation can achieve high cure rates in childhood APL and limit anthracycline exposure. The trial was registered at www.clinicaltrials.gov as EudractCT 2008-002311-40.

Published

2018

39. Risk-adapted treatment of acute promyelocytic leukemia: results from the International Consortium for Childhood APL

Author

Testi, Anna Maria, Pession, Andrea, Diverio, Daniela, Grimwade, David, Gibson, Brenda, de Azevedo, Amilcar Cardoso, Moran, Lorena, Leverger, Guy, Elitzur, Sarah, Hasle, Henrik, ten Bosch, Jutte van der Werff, Smith, Owen, De Rosa, Marisa, Piciocchi, Alfonso, Lo Coco, Francesco, Foà, Robin, Locatelli, Franco, and Kaspers, Gertjan J.L.

Abstract

Pediatric acute promyelocytic leukemia (APL) can be cured with all-transretinoic acid (ATRA) and anthracycline. However, most published trials have employed high cumulative doses of anthracyclines. Here, we report the outcome of newly diagnosed APL patients enrolled in the International Consortium for Childhood APL (ICC-APL-01) trial, which reduced anthracycline exposure but extended that of ATRA. The study recruited 258 children/adolescents with molecularly/cytogenetically proven APL. Patients were stratified into standard-risk (SR) and high-risk (HR) groups according to baseline white blood cell counts (<10 × 109/L or ≥10 × 109/L); both groups received identical induction treatment with ATRA and 3 doses of idarubicin. Two or 3 blocks of consolidation therapy were administered to SR and HR patients, respectively, while maintenance therapy with low-dose chemotherapy and ATRA cycles was given to all patients for 2 years. The cumulative dose of daunorubicin equivalent anthracyclines in SR and HR patients was lower than that of previous studies (355 mg/m2and 405 mg/m2, respectively). Hematologic remission was obtained in 97% of patients; 8 children died of intracranial hemorrhage in the first 2 weeks following diagnosis. Five-year overall and event-free survival for the whole cohort were 94.6% and 79.9%, respectively; they were 98.4% and 89.4% in SR patients and 84.3% and 74.2% in HR patients (P= .002 and P= .043, respectively). These data demonstrate that extended use of ATRA coupled to a risk-adapted consolidation can achieve high cure rates in childhood APL and limit anthracycline exposure. The trial was registered at www.clinicaltrials.govas EudractCT 2008-002311-40.

Published

2018

40. Giant cell tumour of bone in os sacrum of a prepubertal girl – Surgical and medical treatment with zoledronate and denosumab

Author

Beck-Nielsen, Signe Sparre, Hasle, Henrik, Safwat, Akmal, Valancius, Kestutis, Langdahl, Bente, and Hansen, Ebbe Stender

Abstract

A giant cell tumour of bone presented in the os sacrum of a prepubertal girl. Surgery with reconstruction was performed, but total resection was impossible. Zoledronate failed to avoid tumour regrowth, and treatment was changed to denosumab, despite not being recommended for use in growing children. Denosumab treatment for 21 months reduced and stabilized tumour size, the girl became pain free with asymptomatic side effects as mild hypocalcemia, hypophosphatemia and sclerosis of newly formed bone.

Published

2023

41. UBTF tandem Duplications Account for a Third of Advanced Pediatric MDS without Genetic Predisposition to Myeloid Neoplasia

Author

Erlacher, Miriam, Stasik, Sebastian, Yoshimi, Ayami, Georgi, Julia-Annabell, Göhring, Gudrun, Rudelius, Martina, Baumann, Irith, Schwarz-Furlan, Stephan, De Moerloose, Barbara, Hasle, Henrik, Masetti, Riccardo, Barzilai-Birenboim, Shlomit, Stary, Jan, Wlodarski, Marcin W., Rotari, Natalia, Ramamoorthy, Senthilkumar, Lebrecht, Dirk, Noellke, Peter, Strahm, Brigitte, Niemeyer, Charlotte M., and Thiede, Christian

Published

2022

42. Association between Fc-Gamma Receptor Polymorphisms and Autoimmune Neutropenia in Early Childhood in Danish Patients

Author

Kløve-Mogensen, Kirstine, Steffensen, Rudi, Masmas, Tania Nicole, Hoglund, Petter, Glenthøj, Andreas, Haunstrup, Thure, Ratcliffe, Paul, Hasle, Henrik, and Nielsen, Kaspar Rene

Published

2022

43. Treatment Outcomes of Childhood Picalm:MLLT10+ Acute Leukemias: An International Retrospective Study

Author

Mark, Catherine, Kolb, Edward A., Goemans, Bianca F., Meshinchi, Soheil, Gibson, Brenda, Bergmann, Anke K., Harrison, Christine J., Pronk, Cornelis Jan, Lapillonne, Hélène, Leverger, Guy, Antoniou, Evangelia, Attarbaschi, Andishe, Dworzak, Michael, Stary, Jan, Tomizawa, Daisuke, Lejman, Monika, Schmiegelow, Kjeld, Hasle, Henrik, Joyce, Brooklyn, Schneider, Markus, and Abla, Oussama

Published

2022

44. Association between Fc-Gamma Receptor Polymorphisms and Autoimmune Neutropenia in Early Childhood in Danish Patients

Author

Kløve-Mogensen, Kirstine, Steffensen, Rudi, Masmas, Tania Nicole, Hoglund, Petter, Glenthøj, Andreas, Haunstrup, Thure, Ratcliffe, Paul, Hasle, Henrik, and Nielsen, Kaspar Rene

Published

2022

45. Treatment Outcomes of Childhood Picalm:MLLT10+Acute Leukemias: An International Retrospective Study

Author

Mark, Catherine, Kolb, Edward A., Goemans, Bianca F., Meshinchi, Soheil, Gibson, Brenda, Bergmann, Anke K., Harrison, Christine J., Pronk, Cornelis Jan, Lapillonne, Hélène, Leverger, Guy, Antoniou, Evangelia, Attarbaschi, Andishe, Dworzak, Michael, Stary, Jan, Tomizawa, Daisuke, Lejman, Monika, Schmiegelow, Kjeld, Hasle, Henrik, Joyce, Brooklyn, Schneider, Markus, and Abla, Oussama

Published

2022

46. UBTFtandem Duplications Account for a Third of Advanced Pediatric MDS without Genetic Predisposition to Myeloid Neoplasia

Author

Erlacher, Miriam, Stasik, Sebastian, Yoshimi, Ayami, Georgi, Julia-Annabell, Göhring, Gudrun, Rudelius, Martina, Baumann, Irith, Schwarz-Furlan, Stephan, De Moerloose, Barbara, Hasle, Henrik, Masetti, Riccardo, Barzilai-Birenboim, Shlomit, Stary, Jan, Wlodarski, Marcin W., Rotari, Natalia, Ramamoorthy, Senthilkumar, Lebrecht, Dirk, Noellke, Peter, Strahm, Brigitte, Niemeyer, Charlotte M., and Thiede, Christian

Published

2022

47. Therapy reduction in patients with Down syndrome and myeloid leukemia: the international ML-DS 2006 trial

Author

Uffmann, Madita, Rasche, Mareike, Zimmermann, Martin, von Neuhoff, Christine, Creutzig, Ursula, Dworzak, Michael, Scheffers, Lenie, Hasle, Henrik, Zwaan, C. Michel, Reinhardt, Dirk, and Klusmann, Jan-Henning

Abstract

Children with myeloid leukemia associated with Down syndrome (ML-DS) have superior outcome compared with non-DS patients, but suffer from higher constitutional cytotoxic drug susceptibility. We analyzed the outcome of 170 pediatric patients with ML-DS enrolled in the prospective, multicenter, open-label, nonrandomized ML-DS 2006 trial by Nordic Society for Pediatric Hematology and Oncology (NOPHO), Dutch Childhood Oncology Group (DCOG), and Acute Myeloid Leukemia–Berlin-Frankfurt-Münster (AML-BFM) study group. Compared with the historical control arm (reduced-intensity protocol for ML-DS patients from the AML-BFM 98 trial), treatment intensity was reduced by lowering the cumulative dose of etoposide (950 to 450 mg/m2) and intrathecal central nervous system prophylaxis while omitting maintenance therapy. Still, 5-year overall survival (89% ± 3% vs 90% ± 4%; Plog-rank = .64), event-free survival (EFS; 87% ± 3% vs 89% ± 4%; Plog-rank = .71), and cumulative incidence of relapse/nonresponse (CIR/NR; 6% ± 3% vs 6% ± 2%; PGray = .03) did not significantly differ between the ML-DS 2006 trial and the historical control arm. Poor early treatment response (5-year EFS, 58% ± 16% vs 88% ± 3%; Plog rank = .0008) and gain of chromosome 8 (CIR/NR, 16% ± 7% vs 3% ± 2%, PGray = .02; 5-year EFS, 73% ± 8% vs 91% ± 4%, Plog rank = .018) were identified as independent prognostic factors predicting a worse EFS. Five of 7 relapsed patients (71%) with cytogenetic data had trisomy 8. Our study reveals prognostic markers for children with ML-DS and illustrates that reducing therapy did not impair excellent outcome. The trial was registered at EudraCT as #2007-006219-2.

Published

2017

48. Therapy reduction in patients with Down syndrome and myeloid leukemia: the international ML-DS 2006 trial

Author

Uffmann, Madita, Rasche, Mareike, Zimmermann, Martin, von Neuhoff, Christine, Creutzig, Ursula, Dworzak, Michael, Scheffers, Lenie, Hasle, Henrik, Zwaan, C.Michel, Reinhardt, Dirk, and Klusmann, Jan-Henning

Abstract

Children with myeloid leukemia associated with Down syndrome (ML-DS) have superior outcome compared with non-DS patients, but suffer from higher constitutional cytotoxic drug susceptibility. We analyzed the outcome of 170 pediatric patients with ML-DS enrolled in the prospective, multicenter, open-label, nonrandomized ML-DS 2006 trial by Nordic Society for Pediatric Hematology and Oncology (NOPHO), Dutch Childhood Oncology Group (DCOG), and Acute Myeloid Leukemia–Berlin-Frankfurt-Münster (AML-BFM) study group. Compared with the historical control arm (reduced-intensity protocol for ML-DS patients from the AML-BFM 98 trial), treatment intensity was reduced by lowering the cumulative dose of etoposide (950 to 450 mg/m2) and intrathecal central nervous system prophylaxis while omitting maintenance therapy. Still, 5-year overall survival (89% ± 3% vs 90% ± 4%; Plog-rank= .64), event-free survival (EFS; 87% ± 3% vs 89% ± 4%; Plog-rank= .71), and cumulative incidence of relapse/nonresponse (CIR/NR; 6% ± 3% vs 6% ± 2%; PGray= .03) did not significantly differ between the ML-DS 2006 trial and the historical control arm. Poor early treatment response (5-year EFS, 58% ± 16% vs 88% ± 3%; Plog rank= .0008) and gain of chromosome 8 (CIR/NR, 16% ± 7% vs 3% ± 2%, PGray= .02; 5-year EFS, 73% ± 8% vs 91% ± 4%, Plog rank= .018) were identified as independent prognostic factors predicting a worse EFS. Five of 7 relapsed patients (71%) with cytogenetic data had trisomy 8. Our study reveals prognostic markers for children with ML-DS and illustrates that reducing therapy did not impair excellent outcome. The trial was registered at EudraCT as #2007-006219-2.

Published

2017

49. Myelodysplastic and myeloproliferative disorders of childhood

Author

Hasle, Henrik

Abstract

Myelodysplastic syndrome (MDS) and myeloproliferative disorders are rare in children; they are divided into low-grade MDS (refractory cytopenia of childhood [RCC]), advanced MDS (refractory anemia with excess blasts in transformation), and juvenile myelomonocytic leukemia (JMML), each with different characteristics and management strategies. Underlying genetic predisposition is recognized in an increasing number of patients. Germ line GATA2 mutation is found in 70% of adolescents with MDS and monosomy 7. It is challenging to distinguish RCC from aplastic anemia, inherited bone marrow failure, and reactive conditions. RCC is often hypoplastic and may respond to immunosuppressive therapy. In case of immunosuppressive therapy failure, hypercellular RCC, or RCC with monosomy 7, hematopoietic stem cell transplantation (HSCT) using reduced-intensity conditioning regimens is indicated. Almost all patients with refractory anemia with excess blasts are candidates for HSCT; children age 12 years or older have a higher risk of treatment-related death, and the conditioning regimens should be adjusted accordingly. Unraveling the genetics of JMML has demonstrated that JMML in patients with germ line PTPN11 and CBL mutations often regresses spontaneously, and therapy is seldom indicated. Conversely, patients with JMML and neurofibromatosis type 1, somatic PTPN11, KRAS, and most of those with NRAS mutations have a rapidly progressive disease, and early HSCT is indicated. The risk of relapse after HSCT is high, and prophylaxis for graft-versus-host disease and monitoring should be adapted to this risk.

Published

2016

50. Treatment of Molecular Relapse by Cessation of Immunosuppression After Hematopoietic Stem Cell Transplantation in Pediatric FLT3-ITD AML Monitored by WT1Expression in Peripheral Blood

Author

Løvvik Juul-Dam, Kristian, Ifversen, Marianne, Guldborg Nyvold, Charlotte, Hansen, Maria, and Hasle, Henrik

Abstract

Relapse after hematopoietic stem cell transplantation in pediatric acute myeloid leukemia is a fatal event in the majority of cases. Immunotherapy may prevent an impending relapse if instituted at first molecular evidence of disease recurrence. Wilms tumor gene 1 (WT1) is overexpressed in the majority of children and may constitute a useful molecular marker of measurable residual disease applicable for disease monitoring in peripheral blood where the background amplification from healthy hematopoiesis is less prevalent compared with bone marrow. We report the measurable residual disease kinetics from a child with FLT3-internal tandem duplication acute myeloid leukemia where sequential WT1monitoring in peripheral blood-guided withdrawal of immunosuppression.

Published

2019