Your search keyword '"Esmé Waanders"' showing total 94 results

1. Upfront Treatment Influences the Composition of Genetic Alterations in Relapsed Pediatric B-Cell Precursor Acute Lymphoblastic Leukemia

Author

Jiangyan Yu, Esmé Waanders, Simon V. van Reijmersdal, Željko Antić, Charlotte M. van Bosbeek, Edwin Sonneveld, Hester de Groot, Marta Fiocco, Ad Geurts van Kessel, Frank N. van Leeuwen, Rob Pieters, Peter M. Hoogerbrugge, and Roland P. Kuiper

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Abstract. Genomic alterations in relapsed B-cell precursor acute lymphoblastic leukemia (BCP-ALL) may provide insight into the role of specific genomic events in relapse development. Along this line, comparisons between the spectrum of alterations in relapses that arise in different upfront treatment protocols may provide valuable information on the association between the tumor genome, protocol components and outcome. Here, we performed a comprehensive characterization of relapsed BCP-ALL cases that developed in the context of 3 completed Dutch upfront studies, ALL8, ALL9, and ALL10. In total, 123 pediatric BCP-ALL relapses and 77 paired samples from primary diagnosis were analyzed for alterations in 22 recurrently affected genes. We found pronounced differences in relapse alterations between the 3 studies. Specifically, CREBBP mutations were observed predominantly in relapses after treatment with ALL8 and ALL10 which, in the latter group, were all detected in medium risk-treated patients. IKZF1 alterations were enriched 2.2-fold (p = 0.01) and 2.9-fold (p

Published

2020

2. Intragenic amplification of PAX5: a novel subgroup in B-cell precursor acute lymphoblastic leukemia?

Author

Claire Schwab, Karin Nebral, Lucy Chilton, Cristina Leschi, Esmé Waanders, Judith M. Boer, Markéta Žaliová, Rosemary Sutton, Ingegerd Ivanov Öfverholm, Kentaro Ohki, Yuka Yamashita, Stefanie Groeneveld-Krentz, Eva Froňková, Marleen Bakkus, Joelle Tchinda, Thayana da Conceição Barbosa, Grazia Fazio, Wojciech Mlynarski, Agata Pastorczak, Giovanni Cazzaniga, Maria S. Pombo-de-Oliveira, Jan Trka, Renate Kirschner-Schwabe, Toshihiko Imamura, Gisela Barbany, Martin Stanulla, Andishe Attarbaschi, Renate Panzer-Grümayer, Roland P. Kuiper, Monique L. den Boer, Hélène Cavé, Anthony V. Moorman, Christine J. Harrison, and Sabine Strehl

Subjects

Specialties of internal medicine, RC581-951

Published

2017

3. Tumor suppressors BTG1 and IKZF1 cooperate during mouse leukemia development and increase relapse risk in B-cell precursor acute lymphoblastic leukemia patients

Author

Blanca Scheijen, Judith M. Boer, René Marke, Esther Tijchon, Dorette van Ingen Schenau, Esmé Waanders, Liesbeth van Emst, Laurens T. van der Meer, Rob Pieters, Gabriele Escherich, Martin A. Horstmann, Edwin Sonneveld, Nicola Venn, Rosemary Sutton, Luciano Dalla-Pozza, Roland P. Kuiper, Peter M. Hoogerbrugge, Monique L. den Boer, and Frank N. van Leeuwen

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Deletions and mutations affecting lymphoid transcription factor IKZF1 (IKAROS) are associated with an increased relapse risk and poor outcome in B-cell precursor acute lymphoblastic leukemia. However, additional genetic events may either enhance or negate the effects of IKZF1 deletions on prognosis. In a large discovery cohort of 533 childhood B-cell precursor acute lymphoblastic leukemia patients, we observed that single-copy losses of BTG1 were significantly enriched in IKZF1-deleted B-cell precursor acute lymphoblastic leukemia (P=0.007). While BTG1 deletions alone had no impact on prognosis, the combined presence of BTG1 and IKZF1 deletions was associated with a significantly lower 5-year event-free survival (P=0.0003) and a higher 5-year cumulative incidence of relapse (P=0.005), when compared with IKZF1-deleted cases without BTG1 aberrations. In contrast, other copy number losses commonly observed in B-cell precursor acute lymphoblastic leukemia, such as CDKN2A/B, PAX5, EBF1 or RB1, did not affect the outcome of IKZF1-deleted acute lymphoblastic leukemia patients. To establish whether the combined loss of IKZF1 and BTG1 function cooperate in leukemogenesis, Btg1-deficient mice were crossed onto an Ikzf1 heterozygous background. We observed that loss of Btg1 increased the tumor incidence of Ikzf1+/− mice in a dose-dependent manner. Moreover, murine B cells deficient for Btg1 and Ikzf1+/− displayed increased resistance to glucocorticoids, but not to other chemotherapeutic drugs. Together, our results identify BTG1 as a tumor suppressor in leukemia that, when deleted, strongly enhances the risk of relapse in IKZF1-deleted B-cell precursor acute lymphoblastic leukemia, and augments the glucocorticoid resistance phenotype mediated by the loss of IKZF1 function.

Published

2017

4. The origin and nature of tightly clustered BTG1 deletions in precursor B-cell acute lymphoblastic leukemia support a model of multiclonal evolution.

Author

Esmé Waanders, Blanca Scheijen, Laurens T van der Meer, Simon V van Reijmersdal, Liesbeth van Emst, Yvet Kroeze, Edwin Sonneveld, Peter M Hoogerbrugge, Ad Geurts van Kessel, Frank N van Leeuwen, and Roland P Kuiper

Subjects

Genetics, QH426-470

Abstract

Recurrent submicroscopic deletions in genes affecting key cellular pathways are a hallmark of pediatric acute lymphoblastic leukemia (ALL). To gain more insight into the mechanism underlying these deletions, we have studied the occurrence and nature of abnormalities in one of these genes, the B-cell translocation gene 1 (BTG1), in a large cohort of pediatric ALL cases. BTG1 was found to be exclusively affected by genomic deletions, which were detected in 65 out of 722 B-cell precursor ALL (BCP-ALL) patient samples (9%), but not in 109 T-ALL cases. Eight different deletion sizes were identified, which all clustered at the telomeric site in a hotspot region within the second (and last) exon of the BTG1 gene, resulting in the expression of truncated BTG1 read-through transcripts. The presence of V(D)J recombination signal sequences at both sites of virtually all deletions strongly suggests illegitimate RAG1/RAG2-mediated recombination as the responsible mechanism. Moreover, high levels of histone H3 lysine 4 trimethylation (H3K4me3), which is known to tether the RAG enzyme complex to DNA, were found within the BTG1 gene body in BCP-ALL cells, but not T-ALL cells. BTG1 deletions were rarely found in hyperdiploid BCP-ALLs, but were predominant in other cytogenetic subgroups, including the ETV6-RUNX1 and BCR-ABL1 positive BCP-ALL subgroups. Through sensitive PCR-based screening, we identified multiple additional BTG1 deletions at the subclonal level in BCP-ALL, with equal cytogenetic distribution which, in some cases, grew out into the major clone at relapse. Taken together, our results indicate that BTG1 deletions may act as "drivers" of leukemogenesis in specific BCP-ALL subgroups, in which they can arise independently in multiple subclones at sites that are prone to aberrant RAG1/RAG2-mediated recombination events. These findings provide further evidence for a complex and multiclonal evolution of ALL.

Published

2012

5. Heterozygosity for bisphosphoglycerate mutase deficiency expressing clinically as congenital erythrocytosis: A case series and literature review

Author

Myrthe J. van Dijk, Brigitte A. van Oirschot, Manon C. Stam‐Slob, Esmé Waanders, Bert van der Zwaag, Eduard J. van Beers, Judith J. M. Jans, Peter Willem van der Linden, Jose M. Torregrosa Diaz, Betty Gardie, François Girodon, Rik Schots, Noortje Thielen, Richard van Wijk, Clinical sciences, and Hematology

Subjects

bisphosphoglycerate mutase deficiency, Congenital, Heterozygosity, Internal Medicine, red blood cell mass, Hematology, Erythrocytosis, clinical

Abstract

Erythrocytosis is associated with increased red blood cell mass and can be either congenital or acquired. Congenital secondary causes are rare and include germline variants increasing haemoglobin (Hb)-oxygen affinity (e.g., Hb or bisphosphoglycerate mutase (BPGM) variants) or affecting oxygen-sensing pathway proteins. Here, we describe five adults from three kindreds with erythrocytosis associated with heterozygosity for BPGM variants, including one novel. Functional analyses showed partial BPGM deficiency, reduced 2,3-bisphosphoglycerate levels and/or increased Hb-oxygen affinity. We also review currently known BPGM variants. This study contributes to raising awareness of BPGM variants, and in particular that heterozygosity for BPGM deficiency may already manifest clinically.

Published

2022

6. Supplementary Table S3 from Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

Author

John E. Dick, Charles G. Mullighan, Quaid Morris, Mark D. Minden, Jinghui Zhang, Jayne S. Danska, Cynthia J. Guidos, John Easton, Gary Bader, Steven M. Chan, Geoffrey Neale, Scott R. Olsen, Ying Shao, Michael Rusch, Pankaj Gupta, Sagi Abelson, Mohsen Hosseini, Stephanie Z. Xie, Michelle Chan-Seng-Yue, Veronique Voisin, Yiping Fan, Xiaotu Ma, Michael N. Edmonson, Debbie Payne-Turner, Ildiko Grandal, Olga I. Gan, Jessica McLeod, Zhaohui Gu, Esmé Waanders, Jeffrey Wintersinger, Robert J. Vanner, Laura García-Prat, and Stephanie M. Dobson

Abstract

Targeted-sequencing analysis of PDX and PairTree predicted mutational population clusters

Published

2023

7. Data from Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

Author

John E. Dick, Charles G. Mullighan, Quaid Morris, Mark D. Minden, Jinghui Zhang, Jayne S. Danska, Cynthia J. Guidos, John Easton, Gary Bader, Steven M. Chan, Geoffrey Neale, Scott R. Olsen, Ying Shao, Michael Rusch, Pankaj Gupta, Sagi Abelson, Mohsen Hosseini, Stephanie Z. Xie, Michelle Chan-Seng-Yue, Veronique Voisin, Yiping Fan, Xiaotu Ma, Michael N. Edmonson, Debbie Payne-Turner, Ildiko Grandal, Olga I. Gan, Jessica McLeod, Zhaohui Gu, Esmé Waanders, Jeffrey Wintersinger, Robert J. Vanner, Laura García-Prat, and Stephanie M. Dobson

Abstract

Disease recurrence causes significant mortality in B-progenitor acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples shows relapse often arising from minor diagnosis subclones. However, why therapy eradicates some subclones while others survive and progress to relapse remains obscure. Elucidation of mechanisms underlying these differing fates requires functional analysis of isolated subclones. Here, large-scale limiting dilution xenografting of diagnosis and relapse samples, combined with targeted sequencing, identified and isolated minor diagnosis subclones that initiate an evolutionary trajectory toward relapse [termed diagnosis Relapse Initiating clones (dRI)]. Compared with other diagnosis subclones, dRIs were drug-tolerant with distinct engraftment and metabolic properties. Transcriptionally, dRIs displayed enrichment for chromatin remodeling, mitochondrial metabolism, proteostasis programs, and an increase in stemness pathways. The isolation and characterization of dRI subclones reveals new avenues for eradicating dRI cells by targeting their distinct metabolic and transcriptional pathways before further evolution renders them fully therapy-resistant.Significance:Isolation and characterization of subclones from diagnosis samples of patients with B-ALL who relapsed showed that relapse-fated subclones had increased drug tolerance and distinct metabolic and survival transcriptional programs compared with other diagnosis subclones. This study provides strategies to identify and target clinically relevant subclones before further evolution toward relapse.See related video: https://vimeo.com/442838617See related article by E. Waanders et al.

Published

2023

8. Data from High Yield of Pathogenic Germline Mutations Causative or Likely Causative of the Cancer Phenotype in Selected Children with Cancer

Author

Marjolijn C. Jongmans, Nicoline Hoogerbrugge, Roland P. Kuiper, Arjen R. Mensenkamp, Anja Wagner, Jan Loeffen, Eveline S. de Bont, Thatjana Gardeitchik, Anneke Vulto- van Silfhout, Denisa Ilencikova, Wojciech Mlynarski, Agata Pastorczak, Antonis Kattamis, Elizabeth Thompson, Lesley McGregor, Dylan Mordaunt, Martine J. van Belzen, Gijs W. Santen, Carlo Marcelis, David A. Koolen, Erica H. Gerkes, Maran J. Olderode-Berends, Saskia Hopman, Peter M. Hoogerbrugge, Eveline J. Kamping, Diede A.G. van Bladel, Marjolijn J. Ligtenberg, Esmé Waanders, and Illja J. Diets

Abstract

Purpose: In many children with cancer and characteristics suggestive of a genetic predisposition syndrome, the genetic cause is still unknown. We studied the yield of pathogenic mutations by applying whole-exome sequencing on a selected cohort of children with cancer.Experimental Design: To identify mutations in known and novel cancer-predisposing genes, we performed trio-based whole-exome sequencing on germline DNA of 40 selected children and their parents. These children were diagnosed with cancer and had at least one of the following features: (1) intellectual disability and/or congenital anomalies, (2) multiple malignancies, (3) family history of cancer, or (4) an adult type of cancer. We first analyzed the sequence data for germline mutations in 146 known cancer-predisposing genes. If no causative mutation was found, the analysis was extended to the whole exome.Results: Four patients carried causative mutations in a known cancer-predisposing gene: TP53 and DICER1 (n = 3). In another 4 patients, exome sequencing revealed mutations causing syndromes that might have contributed to the malignancy (EP300-based Rubinstein–Taybi syndrome, ARID1A-based Coffin–Siris syndrome, ACTB-based Baraitser–Winter syndrome, and EZH2-based Weaver syndrome). In addition, we identified two genes, KDM3B and TYK2, which are possibly involved in genetic cancer predisposition.Conclusions: In our selected cohort of patients, pathogenic germline mutations causative or likely causative of the cancer phenotype were found in 8 patients, and two possible novel cancer-predisposing genes were identified. Therewith, our study shows the added value of sequencing beyond a cancer gene panel in selected patients, to recognize childhood cancer predisposition. Clin Cancer Res; 24(7); 1594–603. ©2018 AACR.

Published

2023

9. Supplementary Appendix 1 from High Yield of Pathogenic Germline Mutations Causative or Likely Causative of the Cancer Phenotype in Selected Children with Cancer

Author

Marjolijn C. Jongmans, Nicoline Hoogerbrugge, Roland P. Kuiper, Arjen R. Mensenkamp, Anja Wagner, Jan Loeffen, Eveline S. de Bont, Thatjana Gardeitchik, Anneke Vulto- van Silfhout, Denisa Ilencikova, Wojciech Mlynarski, Agata Pastorczak, Antonis Kattamis, Elizabeth Thompson, Lesley McGregor, Dylan Mordaunt, Martine J. van Belzen, Gijs W. Santen, Carlo Marcelis, David A. Koolen, Erica H. Gerkes, Maran J. Olderode-Berends, Saskia Hopman, Peter M. Hoogerbrugge, Eveline J. Kamping, Diede A.G. van Bladel, Marjolijn J. Ligtenberg, Esmé Waanders, and Illja J. Diets

Abstract

Supplementary Table S1 - Cancer gene panel Supplementary Table S2 - Patients with multiple malignancies Supplementary Table S3 - Tumor types of index patients Supplementary Table S4 - Candidate genes Supplementary Table S5 - Overview of clinical features and mutations found in category 1 (ID and/or congenital anomalies) Supplementary Table S6 - Overview of clinical features and mutations found in category 2 (cancer twice) Supplementary Table S7 - Overview of clinical features and mutations found in category 3 (family history) Supplementary Table S8 - Overview of clinical features and mutations found in category 4 (adult type of cancer) Supplementary Table S9 - Overview of clinical features and mutations found in category 5 (multiple reasons for inclusion) Supplementary Figure S1 - Detection of mosaic mutation in ARID1A Supplementary Figure S2 - Family tree of case #04 Supplementary Figure S3 - Family tree of case #05 Supplementary Figure S4 - Family tree of case #07 Supplementary Figure S5 - Family tree of case #10 Supplementary Figure S6 - Family tree of case #12 Supplementary Figure S7 - Family tree of case #17 Supplementary Figure S8 - Family tree of case #21 Supplementary Figure S9 - Family tree of case #22 Supplementary Figure S10 - Family tree of case #24 Supplementary Figure S11 - Family tree of case #27 Supplementary Figure S12 - Family tree of case #28 Supplementary Figure S13 - Family tree of case #29 Supplementary Figure S14 - Family tree of case #34 Supplementary Figure S15 - Family tree of case #36 Supplementary Figure S16 - Family tree of case #39

Published

2023

10. Supplementary Appendix 2 from High Yield of Pathogenic Germline Mutations Causative or Likely Causative of the Cancer Phenotype in Selected Children with Cancer

Author

Marjolijn C. Jongmans, Nicoline Hoogerbrugge, Roland P. Kuiper, Arjen R. Mensenkamp, Anja Wagner, Jan Loeffen, Eveline S. de Bont, Thatjana Gardeitchik, Anneke Vulto- van Silfhout, Denisa Ilencikova, Wojciech Mlynarski, Agata Pastorczak, Antonis Kattamis, Elizabeth Thompson, Lesley McGregor, Dylan Mordaunt, Martine J. van Belzen, Gijs W. Santen, Carlo Marcelis, David A. Koolen, Erica H. Gerkes, Maran J. Olderode-Berends, Saskia Hopman, Peter M. Hoogerbrugge, Eveline J. Kamping, Diede A.G. van Bladel, Marjolijn J. Ligtenberg, Esmé Waanders, and Illja J. Diets

Abstract

This file contains all mutations identified in all patients.

Published

2023

11. Constitutional 2p16.3 deletion including MSH6 and FBXO11 in a boy with developmental delay and diffuse large B-cell lymphoma

Author

Roland P. Kuiper, M A Vermeulen, N van Engelen, Jan Loeffen, Esmé Waanders, Marjolijn C.J. Jongmans, F van Dijk, and Arjan Buijs

Subjects

Male, 0301 basic medicine, Protein-Arginine N-Methyltransferases, Cancer Research, Developmental delay, Somatic cell, BCL6, FBXO11, Biology, Germline, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, Genetics (clinical), B cell, F-Box Proteins, Germinal center, MSH6, Germinal Center, medicine.disease, Lymphoma, DLBCL (diffuse large B-cell lymphoma), 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cancer research, Original Article, Lymphoma, Large B-Cell, Diffuse, Diffuse large B-cell lymphoma

Abstract

We describe a case of a boy with neurodevelopmental delay and a diffuse large B-cell lymphoma (DLBCL) in whom we discovered a germline de novo 2p16.3 deletion including MSH6 and part of the FBXO11 gene. A causative role for MSH6 in cancer development was excluded based on tumor characteristics. The constitutional FBXO11 deletion explains the neurodevelopmental delay in the patient. The FBXO11 protein is involved in BCL-6 ubiquitination and BCL-6 is required for the germinal center reaction resulting in B cell differentiation. Somatic loss of function alterations of FBXO11 result in BCL-6 overexpression which is a known driver in DLBCL. We therefore consider that a causative relationship between the germline FBXO11 deletion and the development of DLBCL in this boy is conceivable.

Published

2021

12. Prevalence of (Epi)genetic Predisposing Factors in a 5-Year Unselected National Wilms Tumor Cohort: A Comprehensive Clinical and Genomic Characterization

Author

Janna A. Hol, Roland P. Kuiper, Freerk van Dijk, Esmé Waanders, Sophie E. van Peer, Marco J. Koudijs, Reno Bladergroen, Simon V. van Reijmersdal, Lionel M. Morgado, Jet Bliek, Maria Paola Lombardi, Saskia Hopman, Jarno Drost, Ronald R. de Krijger, Marry M. van den Heuvel-Eibrink, Marjolijn C.J. Jongmans, Human Genetics, ARD - Amsterdam Reproduction and Development, and ACS - Pulmonary hypertension & thrombosis

Subjects

Adult, Causality, Cancer Research, Beckwith-Wiedemann Syndrome, Oncology, Prevalence, Humans, Genetic Predisposition to Disease, Genomics, Child, Wilms Tumor, Germ-Line Mutation, Kidney Neoplasms

Abstract

PURPOSE Wilms tumor (WT) is associated with (epi)genetic predisposing factors affecting a growing number of WT predisposing genes and loci, including those causing Beckwith-Wiedemann spectrum (BWSp) or WT1-related syndromes. To guide genetic counseling and testing, we need insight into the prevalence of WT predisposing (epi)genetic factors. PATIENTS AND METHODS All children diagnosed with WT in the Netherlands between 2015 and 2020 were referred to a clinical geneticist. Phenotypic data, disease characteristics, and diagnostic test results were collected. If no genetic predisposition was identified by targeted diagnostic testing, germline (trio-)whole-exome sequencing and BWSp testing on normal kidney-derived DNA were offered. RESULTS A total of 126 cases were analyzed of 128 identified patients. (Epi)genetic predisposing factors were present in 42 of 126 patients (33.3%) on the basis of a molecular diagnosis in blood-derived DNA (n = 26), normal kidney-derived DNA (n = 12), or solely a clinical diagnosis of BWSp (n = 4). Constitutional, heterozygous DIS3L2 variants were identified as a recurrent predisposing factor in five patients (4%), with a second somatic hit in 4 of 5 tumors. Twenty patients (16%) were diagnosed with BWSp while four additional patients without BWSp features harbored chromosome 11p15 methylation defects in normal kidney tissue. Remaining findings included WT1-related syndromes (n = 10), Fanconi anemia (n = 1), neurofibromatosis type 1 (n = 1), and a pathogenic REST variant (n = 1). In addition, (likely) pathogenic variants in adult-onset cancer predisposition genes ( BRCA2, PMS2, CHEK2, and MUTYH) were identified in 5 of 56 (8.9%) patients with available whole-exome sequencing data. Several candidate WT predisposition genes were identified, which require further validation. CONCLUSION (Epi)genetic WT predisposing factors, including mosaic aberrations and recurrent heterozygous DIS3L2 variants, were present in at least 33.3% of patients with WT. On the basis of these results, we encourage standard genetic testing after counseling by a clinical geneticist.

Published

2022

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

Author

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

Subjects

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

Abstract

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

Published

2022

14. Characteristics of white blood cell count in acute lymphoblastic leukemia: A COST LEGEND phenotype–genotype study

Author

Marianne Helenius, Goda Vaitkeviciene, Jonas Abrahamsson, Ólafur Gisli Jonsson, Bendik Lund, Arja Harila‐Saari, Kim Vettenranta, Sirje Mikkel, Martin Stanulla, Elixabet Lopez‐Lopez, Esmé Waanders, Hans O. Madsen, Hanne Vibeke Marquart, Signe Modvig, Ramneek Gupta, Kjeld Schmiegelow, Rikke Linnemann Nielsen, University of Helsinki, Clinicum, Children's Hospital, Lastentautien yksikkö, and HUS Children and Adolescents

Subjects

Genotype, 3122 Cancers, ASSIGNMENT, BIOLOGY, CHILDREN, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, white blood cell count (WBC), PERCENTAGE, Leukocyte Count, AGE, acute lymphoblastic leukemia (ALL), spline functions, 3123 Gynaecology and paediatrics, hemic and lymphatic diseases, genome-wide association studies (GWAS), Humans, Hematologi, GENOME-WIDE ASSOCIATION, Precursor Cell Lymphoblastic Leukemia-Lymphoma/genetics, POPULATION, genotype, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, espline functions, Prognosis, Phenotype, Oncology, DISCOVERY, RISK CLASSIFICATION, Pediatrics, Perinatology and Child Health, HOX GENES, Genome-Wide Association Study

Abstract

[EN] Background White blood cell count (WBC) as a measure of extramedullary leukemic cell survival is a well-known prognostic factor in acute lymphoblastic leukemia (ALL), but its biology, including impact of host genome variants, is poorly understood. Methods We included patients treated with the Nordic Society of Paediatric Haematology and Oncology (NOPHO) ALL-2008 protocol (N = 2347, 72% were genotyped by Illumina Omni2.5exome-8-Bead chip) aged 1-45 years, diagnosed with B-cell precursor (BCP-) or T-cell ALL (T-ALL) to investigate the variation in WBC. Spline functions of WBC were fitted correcting for association with age across ALL subgroups of immunophenotypes and karyotypes. The residuals between spline WBC and actual WBC were used to identify WBC-associated germline genetic variants in a genome-wide association study (GWAS) while adjusting for age and ALL subtype associations. Results We observed an overall inverse correlation between age and WBC, which was stronger for the selected patient subgroups of immunophenotype and karyotypes (rho(BCP-ALL )= -.17, rho(T-ALL )= -.19; p < 3 x 10(-4)). Spline functions fitted to age, immunophenotype, and karyotype explained WBC variation better than age alone (rho = .43, p << 2 x 10(-6)). However, when the spline-adjusted WBC residuals were used as phenotype, no GWAS significant associations were found. Based on available annotation, the top 50 genetic variants suggested effects on signal transduction, translation initiation, cell development, and proliferation. Conclusion These results indicate that host genome variants do not strongly influence WBC across ALL subsets, and future studies of why some patients are more prone to hyperleukocytosis should be performed within specific ALL subsets that apply more complex analyses to capture potential germline variant interactions and impact on WBC. Ingenior Otto Christensens Fond; Kirsten and Freddy Johansen Foundation; Kraeftens Bekaempelse, Grant/Award Number: R-257-A14720; Novo Nordisk Fonden; the Nordic Cancer Union; European Cooperation in Science and Technology, Grant/Award Number: Lekemia gene discovery by data sharing, mining and collaboration, CA16223; Barncancerfonden; Bornecancerfonden, Grant/Award Numbers: 2018-3755, 2019-5934; University Hospital Rigshospitalet; Interreg Oresund-Kattegat-Skagerak European Regional Development Fund, Grant: The interregional childhood oncology precision medicine exploration (iCOPE) project

Published

2022

15. Mutational landscape and patterns of clonal evolution in relapsed pediatric acute lymphoblastic leukemia

Author

Željko Antić, Xin Zhou, Michael Rusch, Zhaohui Gu, Yiping Fan, Michael N. Edmonson, William E. Evans, Ruben van Boxtel, Ching-Hon Pui, Roland P. Kuiper, John E. Dick, Jian Wang, Francis Blokzijl, Mary V. Relling, Kelly McCastlain, Jiangyan Yu, Debbie Payne-Turner, Ilaria Iacobucci, Charles G. Mullighan, Jinghui Zhang, Jeremy Chase Crawford, Deqing Pei, Ji Wen, Jing Ma, Gang Wu, Xiaotu Ma, Geoffrey Neale, Irina McGuire, Stephanie M. Dobson, Kathryn G. Roberts, Guangchun Song, Cheng Cheng, Kim E. Nichols, Esmé Waanders, Lei Shi, Paul G. Thomas, Ying Shao, John Easton, Scott R. Olsen, Marjolijn C.J. Jongmans, Jun J. Yang, Maartje van der Vorst, and Stanley Pounds

Subjects

Genetics, Mutation, Lineage (genetic), Clone (cell biology), Somatic hypermutation, Genomics, General Medicine, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Biology, medicine.disease, medicine.disease_cause, Somatic evolution in cancer, Clonal Evolution, Leukemia, Recurrence, medicine, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Humans, Digital polymerase chain reaction, Child

Abstract

Relapse of acute lymphoblastic leukemia (ALL) remains a leading cause of childhood cancer-related death. Prior studies have shown clonal mutations at relapse often arise from relapse-fated subclones that exist at diagnosis. However, the genomic landscape, evolutionary trajectories, and mutational mechanisms driving relapse are incompletely understood. In an analysis of 92 cases of relapsed childhood ALL incorporating multimodal DNA and RNA sequencing, deep digital mutational tracking, and xenografting to formally define clonal structure, we identified 50 significant targets of mutation with distinct patterns of mutational acquisition or enrichment. CREBBP, NOTCH1, and RAS signaling mutations arose from diagnosis subclones, whereas variants in NCOR2, USH2A, and NT5C2 were exclusively observed at relapse. Evolutionary modeling and xenografting demonstrated that relapse-fated clones were minor (50%), major (27%), or multiclonal (18%) at diagnosis. Putative second leukemias, including those with lineage shift, were shown to most commonly represent relapse from an ancestral clone rather than a truly independent second primary leukemia. A subset of leukemias prone to repeated relapse exhibited hypermutation driven by at least three distinct mutational processes, resulting in heightened neoepitope burden and potential vulnerability to immunotherapy. Finally, relapse-driving sequence mutations were detected prior to relapse using droplet digital PCR at levels comparable with orthogonal approaches to monitor levels of measurable residual disease. These results provide a genomic framework to anticipate and circumvent relapse by earlier detection and targeting of relapse-fated clones. Significance: This study defines the landscape of mutations that preexist and arise after commencement of ALL therapy and shows that relapse may be propagated from ancestral, major, or minor clones at initial diagnosis. A subset of cases exhibits hypermutation that results in expression of neoepitopes that may be substrates for immunotherapeutic intervention. See related video: https://vimeo.com/442838617 See related commentary by Ogawa, p. 21. See related article by S. Dobson et al . This article is highlighted in the In This Issue feature, p. 5

Published

2020

16. De Novo and Inherited Pathogenic Variants in KDM3B Cause Intellectual Disability, Short Stature, and Facial Dysmorphism

Author

Laurence Perrin, Marjolijn C.J. Jongmans, Isabelle Thiffault, Han G. Brunner, Bethany Peri, Sarah K. Bartz, Alexandra Afenjar, Kristina Baltrunaite, Esmé Waanders, Jayne Y. Hehir-Kwa, Illja J. Diets, Boris Keren, Alexander J. M. Dingemans, Gea Beunders, Roland P. Kuiper, Anneke T. Vulto-van Silfhout, Laurens Wiel, Bert Callewaert, Andrew Dauber, Margot R.F. Reijnders, Tjitske Kleefstra, Vivian Hwa, Caroline Nava, Matias Wagner, Matthias Griese, Lina Huerta-Saenz, Roos van der Donk, Rolph Pfundt, Nicoline Hoogerbrugge, Christian Gilissen, Maxime Cadieux-Dion, Julia Vodopiutz, Koen L.I. van Gassen, Annekatrien Boel, Julien Thevenon, Nienke E. Verbeek, Bert B.A. de Vries, Vassiliki Konstantopoulou, Human genetics, MUMC+: DA KG Polikliniek (9), MUMC+: DA Klinische Genetica (5), Klinische Genetica, and RS: GROW - R4 - Reproductive and Perinatal Medicine

Subjects

0301 basic medicine, Male, Jumonji Domain-Containing Histone Demethylases, Developmental Disabilities, WEAVER SYNDROME, PROTEIN, Haploinsufficiency, Craniofacial Abnormalities, Histones, 0302 clinical medicine, Intellectual disability, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Missense mutation, DEMETHYLASE KDM3B, Exome, Child, Genetics (clinical), Exome sequencing, Genetics, RUBINSTEIN-TAYBI SYNDROME, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Phenotype, 030220 oncology & carcinogenesis, Female, medicine.symptom, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Joint hypermobility, GENETICS, JMJD1C, Mutation, Missense, Dwarfism, Biology, Short stature, Kdm3b, Cancer Predisposition, Developmental Delay, Facial Recognition, Intellectual Disability, Leukemia, Lymphoma, Short Stature, 03 medical and health sciences, Report, medicine, Humans, MYELOID-LEUKEMIA, Genetic Association Studies, Germ-Line Mutation, Weaver syndrome, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Rubinstein–Taybi syndrome, MUTATIONS, DELETION, Genetic Variation, medicine.disease, Body Height, Musculoskeletal Abnormalities, INDIVIDUALS, 030104 developmental biology, Face, Nanomedicine Radboud Institute for Molecular Life Sciences [Radboudumc 19]

Abstract

Contains fulltext : 202646.pdf (Publisher’s version ) (Open Access) By using exome sequencing and a gene matching approach, we identified de novo and inherited pathogenic variants in KDM3B in 14 unrelated individuals and three affected parents with varying degrees of intellectual disability (ID) or developmental delay (DD) and short stature. The individuals share additional phenotypic features that include feeding difficulties in infancy, joint hypermobility, and characteristic facial features such as a wide mouth, a pointed chin, long ears, and a low columella. Notably, two individuals developed cancer, acute myeloid leukemia and Hodgkin lymphoma, in childhood. KDM3B encodes for a histone demethylase and is involved in H3K9 demethylation, a crucial part of chromatin modification required for transcriptional regulation. We identified missense and truncating variants, suggesting that KDM3B haploinsufficiency is the underlying mechanism for this syndrome. By using a hybrid facial-recognition model, we show that individuals with a pathogenic variant in KDM3B have a facial gestalt, and that they show significant facial similarity compared to control individuals with ID. In conclusion, pathogenic variants in KDM3B cause a syndrome characterized by ID, short stature, and facial dysmorphism.

Published

2019

17. Optical genome mapping identifies a germline retrotransposon insertion in SMARCB1 in two siblings with atypical teratoid rhabdoid tumors

Author

Alexander Hoischen, Michael Kwint, Jayne Y. Hehir-Kwa, Madalena Tropa Martins, Roland P. Kuiper, Kornelia Neveling, Freerk van Dijk, Marjolijn C.J. Jongmans, Mariangela Sabatella, Arjen R. Mensenkamp, Jacklyn A. Biegel, Marcel R. Nelen, Tuomo Mantere, Benno Küsters, Esmé Waanders, Maarten H. Lequin, Ronnie Derks, Pieter Wesseling, Luke O’Gorman, Corrie Gidding, Pathology, CCA - Cancer biology and immunology, and CCA - Imaging and biomarkers

Subjects

Retroelements, rhabdoid tumors, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], SMARCB1, Locus (genetics), Biology, Germline, Pathology and Forensic Medicine, Structural variation, optical imaging, Germline mutation, Gene mapping, medicine, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Humans, Exome, Germ-Line Mutation, Rhabdoid Tumor, Genetics, Whole genome sequencing, Original Paper, Women's cancers Radboud Institute for Molecular Life Sciences [Radboudumc 17], Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Siblings, Other Research Radboud Institute for Health Sciences [Radboudumc 0], retrotransposon, Infant, Newborn, Teratoma, Chromosome Mapping, SMARCB1 Protein, medicine.disease, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Original Papers, childhood cancer predisposition, Atypical teratoid rhabdoid tumor, Female

Abstract

Contains fulltext : 237894.pdf (Publisher’s version ) (Open Access) In a subset of pediatric cancers, a germline cancer predisposition is highly suspected based on clinical and pathological findings, but genetic evidence is lacking, which hampers genetic counseling and predictive testing in the families involved. We describe a family with two siblings born from healthy parents who were both neonatally diagnosed with atypical teratoid rhabdoid tumor (ATRT). This rare and aggressive pediatric tumor is associated with biallelic inactivation of SMARCB1, and in 30% of the cases, a predisposing germline mutation is involved. Whereas the tumors of both siblings showed loss of expression of SMARCB1 and acquired homozygosity of the locus, whole exome and whole genome sequencing failed to identify germline or somatic SMARCB1 pathogenic mutations. We therefore hypothesized that the insertion of a pathogenic repeat-rich structure might hamper its detection, and we performed optical genome mapping (OGM) as an alternative strategy to identify structural variation in this locus. Using this approach, an insertion of ~2.8 kb within intron 2 of SMARCB1 was detected. Long-range PCR covering this region remained unsuccessful, but PacBio HiFi genome sequencing identified this insertion to be a SINE-VNTR-Alu, subfamily E (SVA-E) retrotransposon element, which was present in a mosaic state in the mother. This SVA-E insertion disrupts correct splicing of the gene, resulting in loss of a functional allele. This case demonstrates the power of OGM and long-read sequencing to identify genomic variations in high-risk cancer-predisposing genes that are refractory to detection with standard techniques, thereby completing the clinical and molecular diagnosis of such complex cases and greatly improving counseling and surveillance of the families involved. © 2021 The Authors. The Journal of Pathology published by John Wiley & Sons, Ltd. on behalf of The Pathological Society of Great Britain and Ireland.

Published

2021

18. Accurate detection of low-level mosaic mutations in pediatric acute lymphoblastic leukemia using single molecule tagging and deep-sequencing

Author

Simon V. van Reijmersdal, Roland P. Kuiper, Željko Antić, Edwin Sonneveld, Alexander Hoischen, Esmé Waanders, and Jiangyan Yu

Subjects

0301 basic medicine, Cancer Research, DNA Mutational Analysis, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Biology, Deep sequencing, 03 medical and health sciences, All institutes and research themes of the Radboud University Medical Center, Pediatric Acute Lymphoblastic Leukemia, Biomarkers, Tumor, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Humans, Child, Allele frequency, Gene, Alleles, Genetics, Mosaicism, Detection threshold, High-Throughput Nucleotide Sequencing, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Single Molecule Imaging, Ras pathway, 030104 developmental biology, Oncology, Chromosome Inversion, Mutation, Risk stratification, DNA Probes

Abstract

Pathogenic mutations in relapse-associated genes in pediatric acute lymphoblastic leukemia may improve risk stratification when detected at subclonal levels at primary diagnosis. However, to detect subclonal mutations upfront, a deep-sequencing approach with high specificity and sensitivity is required. Here, we performed a proof-of-principle study to detect low-level mosaic RAS pathway mutations by deep sequencing using random tagging-based single molecule Molecular Inversion Probes (smMIPs). The smMIP-based approach could sensitively detect variants with allele frequency as low as 0.4%, which could all be confirmed by other techniques. In comparison, with standard deep-sequencing techniques we reached a detection threshold of only 2.5%, which hampered detection of seven low-level mosaic mutations representing 24% of all detected mutations. We conclude that smMIP-based deep-sequencing outperforms standard deep-sequencing techniques by showing lower background noise and high specificity, and is the preferred technology for detecting mutations upfront, particularly in genes in which mutations show limited clustering in hotspots.

Published

2018

19. Clonal evolution mechanisms in NT5C2 mutant relapsed acute lymphoblastic leukemia

Author

Alberto Ambesi-Impiombato, Hossein Khiabanian, Mignon L. Loh, Gannie Tzoneva, Koichi Oshima, Chelsea L. Dieck, Giuseppe Basso, Maria Luisa Sulis, Julie M. Gastier-Foster, Maddalena Paganin, Ilaria Iacobucci, Chioma J. Madubata, Adolfo A. Ferrando, Esmé Waanders, Jiangyan Yu, Raul Rabadan, Charles G. Mullighan, Marta Sanchez-Martin, Motohiro Kato, Katsuyoshi Koh, and Renate Kirschner-Schwabe

Subjects

0301 basic medicine, Male, medicine.medical_treatment, Mutant, Drug Resistance, medicine.disease_cause, Somatic evolution in cancer, Mice, 0302 clinical medicine, IMP Dehydrogenase, Recurrence, hemic and lymphatic diseases, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Receptor, Notch1, Cytotoxicity, 5-Nucleotidase, 5'-Nucleotidase, Cancer, Pediatric, Mutation, Multidisciplinary, Guanosine, Mercaptopurine, Lymphoblast, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Phenotype, 3. Good health, 5.1 Pharmaceuticals, 030220 oncology & carcinogenesis, Gain of Function Mutation, Female, Development of treatments and therapeutic interventions, Receptor, Pediatric Cancer, Childhood Leukemia, General Science & Technology, Biology, Article, Clonal Evolution, 03 medical and health sciences, Rare Diseases, All institutes and research themes of the Radboud University Medical Center, Nucleotidase, medicine, Genetics, Animals, Humans, Cell Proliferation, Chemotherapy, Notch1, Animal, Xenograft Model Antitumor Assays, Disease Models, Animal, 030104 developmental biology, HEK293 Cells, Drug Resistance, Neoplasm, Purines, Disease Models, Cancer research, Neoplasm

Abstract

Relapsed acute lymphoblastic leukaemia (ALL) is associated with resistance to chemotherapy and poor prognosis. Gain-of-function mutations in the 5'-nucleotidase, cytosolic II (NT5C2) gene induce resistance to 6-mercaptopurine and are selectively present in relapsed ALL. Yet, the mechanisms involved in NT5C2 mutation-driven clonal evolution during the initiation of leukaemia, disease progression and relapse remain unknown. Here we use a conditional-and-inducible leukaemia model to demonstrate that expression of NT5C2(R367Q), a highly prevalent relapsed-ALL NT5C2 mutation, induces resistance to chemotherapy with 6-mercaptopurine at the cost of impaired leukaemia cell growth and leukaemia-initiating cell activity. The loss-of-fitness phenotype of NT5C2+/R367Q mutant cells is associated with excess export of purines to the extracellular space and depletion of the intracellular purine-nucleotide pool. Consequently, blocking guanosine synthesis by inhibition of inosine-5'-monophosphate dehydrogenase (IMPDH) induced increased cytotoxicity against NT5C2-mutant leukaemia lymphoblasts. These results identify the fitness cost of NT5C2 mutation and resistance to chemotherapy as key evolutionary drivers that shape clonal evolution in relapsed ALL and support a role for IMPDH inhibition in the treatment of ALL.

Published

2018

20. Relapse-Fated Latent Diagnosis Subclones in Acute B Lineage Leukemia Are Drug Tolerant and Possess Distinct Metabolic Programs

Author

Michael Rusch, John E. Dick, Stephanie M. Dobson, Debbie Payne-Turner, Scott R. Olsen, Esmé Waanders, Laura García-Prat, Xiaotu Ma, Zhaohui Gu, Geoffrey Neale, Yiping Fan, Quaid Morris, Charles G. Mullighan, Sagi Abelson, Michelle Chan-Seng-Yue, Jessica McLeod, Olga I. Gan, Michael N. Edmonson, John Easton, Jeff Wintersinger, Ildiko Grandal, Stephanie Z. Xie, Pankaj Gupta, Steven M. Chan, Robert Vanner, Ying Shao, Mark D. Minden, Gary D. Bader, Veronique Voisin, Mohsen Hosseini, Cynthia J. Guidos, Jinghui Zhang, and Jayne S. Danska

Subjects

0301 basic medicine, Drug, Male, Lineage (genetic), Increased drug tolerance, media_common.quotation_subject, Disease, Biology, Chromatin remodeling, Article, 03 medical and health sciences, 0302 clinical medicine, Recurrence, Limiting dilution, medicine, Humans, media_common, medicine.disease, Clone Cells, Leukemia, Leukemia, Myeloid, Acute, 030104 developmental biology, Proteostasis, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female

Abstract

Disease recurrence causes significant mortality in B-progenitor acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples shows relapse often arising from minor diagnosis subclones. However, why therapy eradicates some subclones while others survive and progress to relapse remains obscure. Elucidation of mechanisms underlying these differing fates requires functional analysis of isolated subclones. Here, large-scale limiting dilution xenografting of diagnosis and relapse samples, combined with targeted sequencing, identified and isolated minor diagnosis subclones that initiate an evolutionary trajectory toward relapse [termed diagnosis Relapse Initiating clones (dRI)]. Compared with other diagnosis subclones, dRIs were drug-tolerant with distinct engraftment and metabolic properties. Transcriptionally, dRIs displayed enrichment for chromatin remodeling, mitochondrial metabolism, proteostasis programs, and an increase in stemness pathways. The isolation and characterization of dRI subclones reveals new avenues for eradicating dRI cells by targeting their distinct metabolic and transcriptional pathways before further evolution renders them fully therapy-resistant. Significance: Isolation and characterization of subclones from diagnosis samples of patients with B-ALL who relapsed showed that relapse-fated subclones had increased drug tolerance and distinct metabolic and survival transcriptional programs compared with other diagnosis subclones. This study provides strategies to identify and target clinically relevant subclones before further evolution toward relapse. See related video: https://vimeo.com/442838617 See related article by E. Waanders et al .

Published

2019

21. Germline activating TYK2 mutations in pediatric patients with two primary acute lymphoblastic leukemia occurrences

Author

Blanca Scheijen, E Sonneveld, A. Geurts van Kessel, J.M. van de Vorst, Esmé Waanders, Marjolijn C.J. Jongmans, Agata Pastorczak, V H J van der Velden, Hanka Venselaar, Roland P. Kuiper, F.N. van Leeuwen, C. E. Van Der Schoot, S.V. van Reijmersdal, B. Gruhn, A.H.A. van Dijk, Robbert D.A. Weren, Peter M. Hoogerbrugge, Nicoline Hoogerbrugge, J J van Dongen, Immunology, Landsteiner Laboratory, and Clinical Haematology

Subjects

Male, Models, Molecular, 0301 basic medicine, Cancer Research, Genotype, Protein Conformation, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Biology, Polymorphism, Single Nucleotide, Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], Germline, 03 medical and health sciences, Germline mutation, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], medicine, Genetic predisposition, Humans, Exome, Genetic Predisposition to Disease, Protein Interaction Domains and Motifs, Phosphorylation, Alleles, Genetic Association Studies, Germ-Line Mutation, TYK2 Kinase, Genetics, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], High-Throughput Nucleotide Sequencing, Cancer, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, STAT Transcription Factors, Leukemia, 030104 developmental biology, Amino Acid Substitution, Oncology, Tyrosine kinase 2, Female, Janus kinase, Nanomedicine Radboud Institute for Molecular Life Sciences [Radboudumc 19], Tyrosine kinase, Protein Binding, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

The contribution of genetic predisposing factors to the development of pediatric acute lymphoblastic leukemia (ALL), the most frequently diagnosed cancer in childhood, has not been fully elucidated. Children presenting with multiple de novo leukemias are more likely to suffer from genetic predisposition. Here, we selected five of these patients and analyzed the mutational spectrum of normal and malignant tissues. In two patients, we identified germline mutations in TYK2, a member of the JAK tyrosine kinase family. These mutations were located in two adjacent codons of the pseudokinase domain (p.Pro760Leu and p.Gly761Val). In silico modeling revealed that both mutations affect the conformation of this autoregulatory domain. Consistent with this notion, both germline mutations promote TYK2 autophosphorylation and activate downstream STAT family members, which could be blocked with the JAK kinase inhibitor I. These data indicate that germline activating TYK2 mutations predispose to the development of ALL.

Published

2016

22. Recognition of genetic predisposition in pediatric cancer patients: An easy-to-use selection tool

Author

Marjolijn J. L. Ligtenberg, Marjolijn C.J. Jongmans, Roland P. Kuiper, Peter M. Hoogerbrugge, Jan Loeffen, Nicoline Hoogerbrugge, Esmé Waanders, and Pediatrics

Subjects

0301 basic medicine, Congenital anomalies, Review, Disease, Selection tool, 0302 clinical medicine, Neoplasms, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Genetics(clinical), Family history, Non-U.S. Gov't, Child, Genetics (clinical), Research Support, Non-U.S. Gov't, Age Factors, General Medicine, Syndrome, Dysmorphisms, Phenotype, 030220 oncology & carcinogenesis, Child, Preschool, Population Surveillance, Childhood cancer, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Risk, medicine.medical_specialty, Genetic counseling, Research Support, Malignancy, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Journal Article, medicine, Genetic predisposition, Genetics, Humans, Abnormalities, Multiple, Genetic Predisposition to Disease, Intensive care medicine, Selection (genetic algorithm), Genetic Association Studies, business.industry, Cancer, medicine.disease, Pediatric cancer, Cancer susceptibility, 030104 developmental biology, business, Meta-Analysis

Abstract

Contains fulltext : 171348.pdf (Publisher’s version ) (Open Access) Genetic predisposition for childhood cancer is under diagnosed. Identifying these patients may lead to therapy adjustments in case of syndrome-related increased toxicity or resistant disease and syndrome-specific screening programs may lead to early detection of a further independent malignancy. Cancer surveillance might also be warranted for affected relatives and detection of a genetic mutation can allow for reproductive counseling. Here we present an easy-to-use selection tool, based on a systematic review of pediatric cancer predisposing syndromes, to identify patients who may benefit from genetic counseling. The selection tool involves five questions concerning family history, the type of malignancy, multiple primary malignancies, specific features and excessive toxicity, which results in the selection of those patients that may benefit from referral to a clinical geneticist.

Published

2016

23. TRIM28 haploinsufficiency predisposes to Wilms tumor

Author

Bernt Popp, Abbas Agaimy, Georgia Vasileiou, Marjolijn C.J. Jongmans, Illja J. Diets, Nel Roeleveld, Nicoline Hoogerbrugge, Markus Metzler, Denisa Ilencikova, Roland P. Kuiper, Annelies M. C. Mavinkurve-Groothuis, Didem Seven, Steffen Uebe, Arif B. Ekici, Jenny Wegert, Rajith Bhaskaran, Esmé Waanders, Manfred Gessler, Christian Thiel, Juliane Hoyer, Ronald R. de Krijger, André Reis, Norbert Graf, Simon V. van Reijmersdal, Christian Vokuhl, Michel V. Hadjihannas, and İÜC

Subjects

Male, Haploinsufficiency/genetics, Cancer Research, Carcinogenesis, Whole Exome Sequencing/methods, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Loss of Heterozygosity, Haploinsufficiency, Tripartite Motif-Containing Protein 28, medicine.disease_cause, Germ-Line Mutation/genetics, Kidney Neoplasms/genetics, Germline, Loss of Function Mutation/genetics, 0302 clinical medicine, Loss of Function Mutation, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Child, Non-U.S. Gov't, Exome sequencing, Genetic Predisposition to Disease/genetics, Research Support, Non-U.S. Gov't, Wilms tumor, Wilms Tumor/physiology, DNA, Neoplasm, Kidney Neoplasms, Oncology, Child, Preschool, 030220 oncology & carcinogenesis, Female, Heterozygote, Genes, Wilms Tumor, Mitotic crossover, Genotype, Tumor suppressor gene, DNA repair, Biology, Research Support, Wilms Tumor, 03 medical and health sciences, Exome Sequencing, Journal Article, medicine, Humans, Genetic Predisposition to Disease, Preschool, DNA, Neoplasm/genetics, Germ-Line Mutation, Genes, Wilms Tumor/physiology, Neoplasm/genetics, Loss of Heterozygosity/genetics, TRIM28, Infant, Wilms' tumor, DNA, medicine.disease, haploinsufficiency, Wilms Tumor/genetics, Reconstructive and regenerative medicine Radboud Institute for Health Sciences [Radboudumc 10], Genes, Tripartite Motif-Containing Protein 28/genetics, Cancer research, Carcinogenesis/genetics, genetic predisposition

Abstract

Graf, Norbert/0000-0002-2248-323X; Reis, Andre/0000-0002-6301-6363; Diets, Illja/0000-0001-7603-8898; Popp, Bernt/0000-0002-3679-1081; Thiel, Christian T/0000-0003-3817-7277; Roeleveld, Nel/0000-0002-3390-4466; Reis, AlessanRSS/0000-0001-8486-7469; Vasileiou, Georgia/0000-0002-1993-1134; Gessler, Manfred/0000-0002-7915-6045 WOS:000472571300008 PubMed ID: 30694527 Two percent of patients with Wilms tumors have a positive family history. In many of these cases the genetic cause remains unresolved. By applying germline exome sequencing in two families with two affected individuals with Wilms tumors, we identified truncating mutations in TRIM28. Subsequent mutational screening of germline and tumor DNA of 269 children affected by Wilms tumor was performed, and revealed seven additional individuals with germline truncating mutations, and one individual with a somatic truncating mutation in TRIM28. TRIM28 encodes a complex scaffold protein involved in many different processes, including gene silencing, DNA repair and maintenance of genomic integrity. Expression studies on mRNA and protein level showed reduction of TRIM28, confirming a loss-of-function effect of the mutations identified. The tumors showed an epithelial-type histology that stained negative for TRIM28 by immunohistochemistry. The tumors were bilateral in six patients, and 10/11 tumors are accompanied by perilobar nephrogenic rests. Exome sequencing on eight tumor DNA samples from six individuals showed loss-of-heterozygosity (LOH) of the TRIM28-locus by mitotic recombination in seven tumors, suggesting that TRIM28 functions as a tumor suppressor gene in Wilms tumor development. Additionally, the tumors showed very few mutations in known Wilms tumor driver genes, suggesting that loss of TRIM28 is the main driver of tumorigenesis. In conclusion, we identified heterozygous germline truncating mutations in TRIM28 in 11 children with mainly epithelial-type Wilms tumors, which become homozygous in tumor tissue. These data establish TRIM28 as a novel Wilms tumor predisposition gene, acting as a tumor suppressor gene by LOH. Dutch Cancer SocietyKWF Kankerbestrijding [KUN2012-5366]; KiKa Foundation [127] Grant sponsor: Dutch Cancer Society; Grant number: KUN2012-5366; Grant sponsor: The KiKa Foundation (project 127)

Published

2019

24. High Yield of Pathogenic Germline Mutations Causative or Likely Causative of the Cancer Phenotype in Selected Children with Cancer

Author

Eveline J. Kamping, Wojciech Młynarski, Diede A G van Bladel, Nicoline Hoogerbrugge, Anja Wagner, Roland P. Kuiper, Marjolijn J. L. Ligtenberg, Marjolijn C.J. Jongmans, Jan Loeffen, Denisa Ilencikova, Dylan A. Mordaunt, Lesley M McGregor, Eveline S. J. M. de Bont, Antonis Kattamis, Gijs W. E. Santen, Thatjana Gardeitchik, Arjen R. Mensenkamp, Elizabeth Thompson, Agata Pastorczak, Martine J. van Belzen, Saskia M. J. Hopman, Maran J. W. Olderode-Berends, Anneke Vulto van Silfhout, Carlo Marcelis, David A. Koolen, Esmé Waanders, Illja J. Diets, Peter M. Hoogerbrugge, Erica H. Gerkes, Damage and Repair in Cancer Development and Cancer Treatment (DARE), Stem Cell Aging Leukemia and Lymphoma (SALL), Pediatrics, and Clinical Genetics

Subjects

0301 basic medicine, Male, Cancer Research, INTELLECTUAL DISABILITY, WEAVER SYNDROME, Craniofacial Abnormalities, 0302 clinical medicine, Neoplasms, Genotype, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Medicine, Exome, Child, Exome sequencing, Genetics, Rubinstein-Taybi Syndrome, GENETIC-VARIATION, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Phenotype, Oncology, 030220 oncology & carcinogenesis, Child, Preschool, Female, LI-FRAUMENI SYNDROME, Hand Deformities, Congenital, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Adolescent, Micrognathism, ACUTE MYELOID-LEUKEMIA, 03 medical and health sciences, Germline mutation, SDG 3 - Good Health and Well-being, WINTER CEREBROFRONTOFACIAL SYNDROME, Exome Sequencing, Genetic predisposition, Congenital Hypothyroidism, Humans, Abnormalities, Multiple, Genetic Predisposition to Disease, Coffin–Siris syndrome, Germ-Line Mutation, ACUTE LYMPHOBLASTIC-LEUKEMIA, PEDIATRIC CANCER, CHILDHOOD-CANCER, business.industry, COFFIN-SIRIS SYNDROME, Cancer, Infant, medicine.disease, Pediatric cancer, 030104 developmental biology, Li–Fraumeni syndrome, Face, business, Neck

Abstract

Purpose: In many children with cancer and characteristics suggestive of a genetic predisposition syndrome, the genetic cause is still unknown. We studied the yield of pathogenic mutations by applying whole-exome sequencing on a selected cohort of children with cancer. Experimental Design: To identify mutations in known and novel cancer-predisposing genes, we performed trio-based whole-exome sequencing on germline DNA of 40 selected children and their parents. These children were diagnosed with cancer and had at least one of the following features: (1) intellectual disability and/or congenital anomalies, (2) multiple malignancies, (3) family history of cancer, or (4) an adult type of cancer. We first analyzed the sequence data for germline mutations in 146 known cancer-predisposing genes. If no causative mutation was found, the analysis was extended to the whole exome. Results: Four patients carried causative mutations in a known cancer-predisposing gene: TP53 and DICER1 (n = 3). In another 4 patients, exome sequencing revealed mutations causing syndromes that might have contributed to the malignancy (EP300-based Rubinstein–Taybi syndrome, ARID1A-based Coffin–Siris syndrome, ACTB-based Baraitser–Winter syndrome, and EZH2-based Weaver syndrome). In addition, we identified two genes, KDM3B and TYK2, which are possibly involved in genetic cancer predisposition. Conclusions: In our selected cohort of patients, pathogenic germline mutations causative or likely causative of the cancer phenotype were found in 8 patients, and two possible novel cancer-predisposing genes were identified. Therewith, our study shows the added value of sequencing beyond a cancer gene panel in selected patients, to recognize childhood cancer predisposition. Clin Cancer Res; 24(7); 1594–603. ©2018 AACR.

Published

2018

25. Intragenic amplification of PAX5: a novel subgroup in B-cell precursor acute lymphoblastic leukemia?

Author

Yuka Yamashita, Grazia Fazio, Hélène Cavé, Sabine Strehl, Kentaro Ohki, Judith M. Boer, Renate Kirschner-Schwabe, Agata Pastorczak, Eva Froňková, Joelle Tchinda, Markéta Žaliová, Marleen Bakkus, Monique L. den Boer, Cristina Leschi, Christine J. Harrison, Lucy Chilton, Stefanie Groeneveld-Krentz, Renate Panzer-Grümayer, Anthony V. Moorman, Wojciech Młynarski, Martin Stanulla, Giovanni Cazzaniga, Andishe Attarbaschi, Maria S. Pombo-de-Oliveira, Thayana Conceição Barbosa, Rosemary Sutton, Jan Trka, Gisela Barbany, Karin Nebral, Claire Schwab, Toshihiko Imamura, Roland P. Kuiper, Esmé Waanders, Ingegerd Ivanov Öfverholm, University of Zurich, Clinical Biology, Hematology, Pediatrics, Schwab, C, Nebral, K, Chilton, L, Leschi, C, Waanders, E, Boer, J, Žaliová, M, Sutton, R, Öfverholm, I, Ohki, K, Yamashita, Y, Groeneveld-Krentz, S, Froňková, E, Bakkus, M, Tchinda, J, Barbosa, T, Fazio, G, Mlynarski, W, Pastorczak, A, Cazzaniga, G, Pombo-de-Oliveira, M, Trka, J, Kirschner-Schwabe, R, Imamura, T, Barbany, G, Stanulla, M, Attarbaschi, A, Panzer-Grümayer, R, Kuiper, R, den Boer, M, Cavé, H, Moorman, A, Harrison, C, and Strehl, S

Subjects

0301 basic medicine, MED/03 - GENETICA MEDICA, business.industry, Lymphoblastic Leukemia, 2720 Hematology, hemic and immune systems, 610 Medicine & health, Hematology, 3. Good health, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Text mining, medicine.anatomical_structure, immune system diseases, 10036 Medical Clinic, 030220 oncology & carcinogenesis, hemic and lymphatic diseases, Cancer research, Medicine, PAX5, business, PAX5, B-cell precursor acute lymphoblastic leukemia, poor outcome, B cell

Abstract

Key Points Intragenic PAX5 amplification defines a novel, relapse-prone subtype of B-cell precursor acute lymphoblastic leukemia with a poor outcome.

Published

2017

26. Intragenic amplification of

Author

Claire, Schwab, Karin, Nebral, Lucy, Chilton, Cristina, Leschi, Esmé, Waanders, Judith M, Boer, Markéta, Žaliová, Rosemary, Sutton, Ingegerd Ivanov, Öfverholm, Kentaro, Ohki, Yuka, Yamashita, Stefanie, Groeneveld-Krentz, Eva, Froňková, Marleen, Bakkus, Joelle, Tchinda, Thayana da Conceição, Barbosa, Grazia, Fazio, Wojciech, Mlynarski, Agata, Pastorczak, Giovanni, Cazzaniga, Maria S, Pombo-de-Oliveira, Jan, Trka, Renate, Kirschner-Schwabe, Toshihiko, Imamura, Gisela, Barbany, Martin, Stanulla, Andishe, Attarbaschi, Renate, Panzer-Grümayer, Roland P, Kuiper, Monique L, den Boer, Hélène, Cavé, Anthony V, Moorman, Christine J, Harrison, and Sabine, Strehl

Subjects

immune system diseases, hemic and lymphatic diseases, hemic and immune systems, Stimulus Report

Abstract

Intragenic PAX5 amplification defines a novel, relapse-prone subtype of B-cell precursor acute lymphoblastic leukemia with a poor outcome.

Published

2017

27. Childhood neuroendocrine tumours: a descriptive study revealing clues for genetic predisposition

Author

Illja J. Diets, Iris D. Nagtegaal, Jan Loeffen, Marjolijn C.J. Jongmans, Esmé Waanders, Nicoline Hoogerbrugge, I. de Blaauw, and Pediatrics

Subjects

Oncology, Male, medicine.medical_specialty, Bone marrow transplant, Cancer Research, von Hippel-Lindau Disease, Adolescent, 030209 endocrinology & metabolism, Brain cancer, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Genetic predisposition, neuroendocrine tumour, Journal Article, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Medicine, Humans, Genetic Predisposition to Disease, Registries, Child, Netherlands, business.industry, Paediatric oncology, Incidence, Multiple Endocrine Neoplasia, Infant, Neuroendocrine tumour, Pancreatic Neoplasms, Neuroendocrine Tumors, Reconstructive and regenerative medicine Radboud Institute for Molecular Life Sciences [Radboudumc 10], Appendiceal Neoplasms, paediatric oncology, 030220 oncology & carcinogenesis, Apoptosis pathway, Child, Preschool, Anti cancer drugs, Clinical Study, Female, Descriptive research, business, genetic predisposition, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]

Abstract

Contains fulltext : 169917pub.pdf (Publisher’s version ) (Closed access) BACKGROUND: Neuroendocrine tumours (NETs) are rare in children and limited data are available. We aimed to specify tumour and patient characteristics and to investigate the role of genetic predisposition in the aetiology of paediatric NETs. METHODS: Using the Dutch Pathology Registry PALGA, we collected patient- and tumour data of paediatric NETs in the Netherlands between 1991 and 2013 (N=483). RESULTS: The incidence of paediatric NETs in the Netherlands is 5.40 per one million per year. The majority of NETs were appendiceal tumours (N=441;91.3%). Additional surgery in appendiceal NETs was indicated in 89 patients, but performed in only 27 of these patients. Four out of five patients with pancreatic NETs were diagnosed with Von Hippel-Lindau disease (N=2) and Multiple Endocrine Neoplasia type 1 (N=2). In one patient with an appendiceal NET Familial Adenomatous Polyposis was diagnosed. On the basis of second primary tumours or other additional diagnoses, involvement of genetic predisposition was suggestive in several others. CONCLUSIONS: We identified a significant number of patients with a confirmed or suspected tumour predisposition syndrome and show that paediatric pancreatic NETs in particular are associated with genetic syndromes. In addition, we conclude that treatment guidelines for appendiceal paediatric NETs need revision and improved implementation.

Published

2017

28. Tumor suppressors BTG1 and IKZF1 cooperate during mouse leukemia development and increase relapse risk in B-cell precursor acute lymphoblastic leukemia patients

Author

Esmé Waanders, Martin A. Horstmann, Luciano Dalla-Pozza, Nicola C. Venn, Esther Tijchon, Rob Pieters, Peter M. Hoogerbrugge, Laurens T. van der Meer, Judith M. Boer, Frank N. van Leeuwen, Blanca Scheijen, Liesbeth van Emst, Rene Marke, Dorette van Ingen Schenau, Gabriele Escherich, Roland P. Kuiper, Edwin Sonneveld, Rosemary Sutton, Monique L. den Boer, and Pediatrics

Subjects

Male, 0301 basic medicine, Adolescent, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Drug resistance, Biology, Ikaros Transcription Factor, Mice, 03 medical and health sciences, 0302 clinical medicine, Recurrence, CDKN2A, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, hemic and lymphatic diseases, Biomarkers, Tumor, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], medicine, Animals, Humans, Genetic Predisposition to Disease, Cumulative incidence, Child, B cell, Mice, Knockout, Tumor Suppressor Proteins, Epistasis, Genetic, Articles, Hematology, Acute Lymphoblastic Leukemia, Prognosis, medicine.disease, Phenotype, Neoplasm Proteins, 3. Good health, Patient Outcome Assessment, Disease Models, Animal, Leukemia, Cell Transformation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Drug Resistance, Neoplasm, Child, Preschool, 030220 oncology & carcinogenesis, Cancer research, Female, PAX5, BTG1, Gene Deletion

Abstract

Contains fulltext : 169866.pdf (Publisher’s version ) (Open Access) Deletions and mutations affecting lymphoid transcription factor IKZF1 (IKAROS) are associated with an increased relapse risk and poor outcome in B-cell precursor acute lymphoblastic leukemia. However, additional genetic events may either enhance or negate the effects of IKZF1 deletions on prognosis. In a large discovery cohort of 533 childhood B-cell precursor acute lymphoblastic leukemia patients, we observed that single-copy losses of BTG1 were significantly enriched in IKZF1-deleted B-cell precursor acute lymphoblastic leukemia (P=0.007). While BTG1 deletions alone had no impact on prognosis, the combined presence of BTG1 and IKZF1 deletions was associated with a significantly lower 5-year event-free survival (P=0.0003) and a higher 5-year cumulative incidence of relapse (P=0.005), when compared with IKZF1-deleted cases without BTG1 aberrations. In contrast, other copy number losses commonly observed in B-cell precursor acute lymphoblastic leukemia, such as CDKN2A/B, PAX5, EBF1 or RB1, did not affect the outcome of IKZF1-deleted acute lymphoblastic leukemia patients. To establish whether the combined loss of IKZF1 and BTG1 function cooperate in leukemogenesis, Btg1-deficient mice were crossed onto an Ikzf1 heterozygous background. We observed that loss of Btg1 increased the tumor incidence of Ikzf1+/- mice in a dose-dependent manner. Moreover, murine B cells deficient for Btg1 and Ikzf1+/- displayed increased resistance to glucocorticoids, but not to other chemotherapeutic drugs. Together, our results identify BTG1 as a tumor suppressor in leukemia that, when deleted, strongly enhances the risk of relapse in IKZF1-deleted B-cell precursor acute lymphoblastic leukemia, and augments the glucocorticoid resistance phenotype mediated by the loss of IKZF1 function.

Published

2017

29. Independent prognostic value of BCR-ABL1-like signature and IKZF1 deletion, but not high CRLF2 expression, in children with B-cell precursor ALL

Author

Edwin Sonneveld, Gabriele Escherich, Vincent H.J. van der Velden, Roland P. Kuiper, Esmé Waanders, Marieke E. Willemse, Monique L. den Boer, Peter M. Hoogerbrugge, Lisa J. Russell, Simon V. van Reijmersdal, Martin A. Horstmann, Leila Mohammadi Khankahdani, Hester A. de Groot-Kruseman, Frank N. van Leeuwen, Rob Pieters, Arian van der Veer, Dimitris Rizopoulos, William E. Evans, Christine J. Harrison, Pediatrics, Immunology, and Epidemiology

Subjects

Male, Adolescent, Immunology, Fusion Proteins, bcr-abl, Value (computer science), Biochemistry, Ikaros Transcription Factor, Text mining, Predictive Value of Tests, Recurrence, Risk Factors, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, hemic and lymphatic diseases, medicine, Humans, Cumulative incidence, Receptors, Cytokine, Child, Genetics and epigenetic pathways of disease Translational research [NCMLS 6], B cell, business.industry, Incidence (epidemiology), Incidence, Infant, Cell Biology, Hematology, Gene signature, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Prognosis, Minimal residual disease, Age-related aspects of cancer Immune Regulation [ONCOL 2], medicine.anatomical_structure, Predictive value of tests, Child, Preschool, Cancer research, Female, business

Abstract

Item does not contain fulltext Most relapses in childhood B-cell precursor acute lymphoblastic leukemia (BCP-ALL) are not predicted using current prognostic features. Here, we determined the co-occurrence and independent prognostic relevance of 3 recently identified prognostic features: BCR-ABL1-like gene signature, deletions in IKZF1, and high CRLF2 messenger RNA expression (CRLF2-high). These features were determined in 4 trials representing 1128 children with ALL: DCOG ALL-8, ALL9, ALL10, and Cooperative ALL (COALL)-97/03. BCR-ABL1-like, IKZF1-deleted, and CRLF2-high cases constitute 33.7% of BCR-ABL1-negative, MLL wild-type BCP-ALL cases, of which BCR-ABL1-like and IKZF1 deletion (co)occurred most frequently. Higher cumulative incidence of relapse was found for BCR-ABL1-like and IKZF1-deleted, but not CRLF2-high, cases relative to remaining BCP-ALL cases, reflecting the observations in each of the cohorts analyzed separately. No relapses occurred among cases with CRLF2-high as single feature, whereas 62.9% of all relapses in BCR-ABL1-negative, MLL wild-type BCP-ALL occurred in cases with BCR-ABL1-like signature and/or IKZF1 deletion. Both the BCR-ABL1-like signature and IKZF1 deletions were prognostic features independent of conventional prognostic markers in a multivariate model, and both remained prognostic among cases with intermediate minimal residual disease. The BCR-ABL1-like signature and an IKZF1 deletion, but not CRLF2-high, are prognostic factors and are clinically of importance to identify high-risk patients who require more intensive and/or alternative therapies.

Published

2013

30. Molecular origin of childhood acute lymphoblastic leukemia

Author

Charles G. Mullighan, Marjolijn C.J. Jongmans, and Esmé Waanders

Subjects

Medicine(all), Cell type, Treatment response, Oncogenic pathways, Disease, Biology, Acute lymphoblastic leukemia, Bioinformatics, medicine.disease, Germline, Leukemogenic, Germline susceptibility, Leukemia, Pediatric Acute Lymphoblastic Leukemia, medicine, Genetic profiling, Childhood Acute Lymphoblastic Leukemia, Mutations

Abstract

Our understanding of the genetic etiology of pediatric acute lymphoblastic leukemia (ALL) has advanced greatly in the past few decades. Due to the advent of genome-wide profiling techniques for copy number alterations (CNAs) as well as sequence mutations, we have thoroughly characterized many different genetic subtypes of ALL. Each subtype harbors alterations activating leukemogenic pathways and differs in prevalence, prognosis, cell type, and treatment response. The interplay of founding leukemogenic aberrations, acquired mutations, and germline composition of the patient is important for the development and progression of the disease. Moreover, genomic profiling has identified genetic alterations that have been integrated into diagnostic testing algorithms and are being evaluated as targets for therapy. Despite these advances, the genetic basis of a minority of ALL cases remains unknown, and the frequency of these enigmatic cases rises with patient age. Much work remains in studying these last uncharacterized groups to fully understand leukemia development and improve outcomes.

Published

2016

31. Integrated use of minimal residual disease classification and IKZF1 alteration status accurately predicts 79% of relapses in pediatric acute lymphoblastic leukemia

Author

C. E. Van Der Schoot, V H J van der Velden, A. J. P. Veerman, V de Haas, Esmé Waanders, J J van Dongen, A. Geurts van Kessel, Roland P. Kuiper, F.N. van Leeuwen, Peter M. Hoogerbrugge, S.V. van Reijmersdal, Pediatric surgery, CCA - Disease profiling, Landsteiner Laboratory, Clinical Haematology, Paediatric Oncology, Immunology, and Pediatrics

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Prognostic factor, Neoplasm, Residual, Immunology, Kaplan-Meier Estimate, Biochemistry, Risk Assessment, Sensitivity and Specificity, Intermediate group, Ikaros Transcription Factor, Pediatric Acute Lymphoblastic Leukemia, Predictive Value of Tests, Recurrence, Internal medicine, hemic and lymphatic diseases, medicine, Humans, Child, Genetics and epigenetic pathways of disease Translational research [NCMLS 6], Gene Rearrangement, Hematology, business.industry, Hazard ratio, Cancer, Gene rearrangement, Cell Biology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Minimal residual disease, Surgery, Age-related aspects of cancer Immune Regulation [ONCOL 2], body regions, Leukemia, Predictive value of tests, Cohort, Mutation, Risk assessment, Large group, business, After treatment

Abstract

Abstract 272 The response to therapy as determined by minimal residual disease (MRD) is currently used for stratification in treatment protocols for pediatric acute lymphoblastic leukemia (ALL). Even though MRD classification clearly identifies patients at low or at high risk for relapse, it also results in a large intermediate group (50 to 60% of patients), which still contains approximately half of all relapse cases. To improve risk stratification, we evaluated the added value of the IKZF1 alteration status, recently identified as a prognostic factor, in precursor-B-ALL patients. In an unbiased cohort of 131 uniformly treated precursor-B-ALL patients, we determined MRD levels at 42 and 84 days after treatment initiation using RQ-PCR analysis of Ig/TCR rearrangements. Based on these levels, patients were divided into three groups: MRD-Low (MRD-L), MRD-Medium (MRD-M) and MRD-High (MRD-H). IKZF1 alterations at diagnosis were determined using multiplex ligation-dependent probe amplification and genomic sequencing. We confirmed the strong prognostic significance of MRD classification, which was independent of IKZF1 status. Importantly, in the large MRD-M group (n=81; 62% of patients) containing 46% of the relapsed patients, IKZF1 alteration status identified 8 out of 11 relapsed patients (72%). The 9 year relapse-free survival (RFS) for IKZF1 mutated patients in this MRD-M group was 27% compared to 96% for patients wild-type for IKZF1 (P Disclosures: No relevant conflicts of interest to declare.

Published

2011

32. A germ line mutation in cathepsin B points toward a role in asparaginase pharmacokinetics

Author

Peter M. Hoogerbrugge, Hanka Venselaar, Debbie M. Roeleveld, C Lanvers, Laurens T. van der Meer, Frank N. van Leeuwen, Marloes Levers, Joachim Boos, Esmé Waanders, Roger J. M. Brüggemann, Roland P. Kuiper, and D. Maroeska te Loo

Subjects

Asparaginase, medicine.diagnostic_test, business.industry, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Lymphoblastic Leukemia, Immunology, Cell Biology, Hematology, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Pharmacology, Biochemistry, Cathepsin B, chemistry.chemical_compound, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Germline mutation, Pharmacokinetics, chemistry, Therapeutic drug monitoring, hemic and lymphatic diseases, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], medicine, business, Nanomedicine Radboud Institute for Molecular Life Sciences [Radboudumc 19], Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5]

Abstract

To the editor: l-Asparaginase (ASNase) is a key component of protocols used to treat acute lymphoblastic leukemia (ALL). Poorly understood interpatient differences in ASNase pharmacokinetics demand therapeutic drug monitoring to prevent patients from receiving an inadequate dose.[1][1] Although it

Published

2014

33. Relapse-Initiating Clones Preexisting at Diagnosis in B- Cell Acute Lymphoblastic Leukemia Help Predict Molecular Pathways of Relapse

Author

Debbie Payne-Turner, Michael Rusch, Xiaotu Ma, John E. Dick, Alex Murison, Ying Shao, Mark D. Minden, Jessica McLeod, Jeffery Wintersinger, John Easton, Mathieu Lupien, Yiping Fan, Charles G. Mullighan, Laura Garcia Prat, Michelle Chan-Seng-Yue, Michael N. Edmonson, Zhaohui Gu, Pankaj Gupta, Jinghui Zhang, Stephanie M. Dobson, Esmé Waanders, Quaid Morris, Robert Vanner, and Olga I. Gan

Subjects

Immunology, Clone (cell biology), Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, Somatic evolution in cancer, Transplantation, Leukemia, Acute lymphocytic leukemia, medicine, Cancer research, Epigenetics, Gene, Exome sequencing

Abstract

Disease recurrence remains a significant cause of mortality in B-cell acute lymphoblastic leukemia (B-ALL). Genomic analysis of matched diagnosis and relapse samples have demonstrated that relapse arises from a minor subclone already present at diagnosis and not the dominant clone in the majority of patients. However, the reasons why only some clones survive therapy and generate relapse are obscure and elucidation of the mechanisms that underlie these differing fates may be revealed by functional analysis of isolated subclones. Previous work has shown that the subclonal diversity in B-ALL exists at the level of the leukemia-initiating cells capable of generating patient derived xenografts (Notta et al., Nature, 2011). In order to investigate the functional consequences of genetic clonal evolution during disease progression, we performed in-depth genomic and functional analysis of 14 paired diagnosis/relapse samples from adult and pediatric B-ALL patients with varying cytogenetic abnormalities. Diagnosis-specific, relapse-specific, and shared clonal and subclonal variants were identified by whole exome sequencing of the patient samples. Targeted sequencing of these variants in 372 xenografts generated by transplantation of CD19+ cells in a limiting cell dilution assay uncovered clonal variation. This analysis provided for the unequivocal identification of minor subclones ancestral to the relapse, termed diagnosis Relapse-Initiating (dRI) clones, in the diagnostic sample. Our xenografting approach enabled the physical isolation of dRI clones providing a unique opportunity to interrogate their epigenetic and transcriptional landscapes in order to unravel their relapse initiating capacity. To this end, representative diagnosis, dRI and relapse clones from 5 of the 14 patients were subjected to RNAseq and ATACseq (assay for transposase-accessible chromatin using sequencing) analysis. Despite the differences in transcriptional and chromatin openness between patients, principal component analysis of subclones from individual patients positioned the dRI clones as evolutionary intermediates between the diagnosis and relapse clones. Hierarchical clustering of the most significantly differentially expressed genes and open chromatin regions demonstrated that dRI clones shared gene expression and chromatin accessibility signatures with both the dominant diagnosis clone as well as the dominant relapse clone. To gain mechanistic insight into the data we used gene set enrichment analysis (GSEA) and identified common molecular pathways present in all patients that were enriched in dRI clones and persisted at the time of relapse in comparison to the dominant diagnosis clone. dRI and relapse clones converged in the activation of genes involved in cellular functions such as endocytosis, autophagy and innate immune response. In addition, cell surface proteins like ABC transporters and ephrins were also upregulated in dRI and relapse clones. Remarkably, functional interrogation of dRI clones in secondary xenografts, in comparison to more representative diagnosis clones, displayed increased tolerance to standard chemotherapeutic agents (dexamethasone, L-asparaginase and vincristine). Investigation of the molecular pathways and cellular receptors/transporters identified by gene expression analysis are being assessed in vitro and in vivo as potential targets for novel therapeutic approaches and disease monitoring. Overall, we have shown evidence that minor subclones at diagnosis, ancestral to the relapse clone, possess functional advantages and unique properties over other diagnostic subclones prior to treatment exposure. In depth analysis of pathways identified in these dRI subclones will shed light on potential new therapeutic approaches for abrogating and reducing disease recurrence in B-ALL. Disclosures Mullighan: Amgen: Honoraria, Speakers Bureau; Cancer Prevention and Research Institute of Texas: Consultancy; Abbvie: Research Funding; Pfizer: Honoraria, Research Funding, Speakers Bureau; Loxo Oncology: Research Funding.

Published

2018

34. Genetic Analysis of B-Cell Acute Lymphoblastic Leukemia Dissemination to the Central Nervous System Identifies Clonal Selection and Therapeutic Vulnerability

Author

Stephanie M. Dobson, Esmé Waanders, Jessica McLeod, Jayne S. Danska, James A. Kennedy, Ildiko Grandal, Robert Vanner, Mark D. Minden, Olga I. Gan, Veronique Voisin, Cynthia J. Guidos, John E. Dick, and Charles G. Mullighan

Subjects

biology, Immunology, Copy number analysis, Chromosomal translocation, Cell Biology, Hematology, Disease, medicine.disease, Biochemistry, Transcriptome, 03 medical and health sciences, Leukemia, chemistry.chemical_compound, 0302 clinical medicine, medicine.anatomical_structure, KMT2A, chemistry, 030220 oncology & carcinogenesis, Omacetaxine mepesuccinate, Cancer research, medicine, biology.protein, Bone marrow

Abstract

Without prophylactic therapy, B-cell Acute Lymphoblastic Leukemia (B-ALL) spreads to the leptomeninges of the central nervous system (CNS) in up to 70% of patients. CNS involvement is more common in certain high risk B-ALL subgroups, including patients with KMT2A (MLL)-translocations, and disease relapse in the CNS carries a poor prognosis. The genetic determinants and biology of B-ALL dissemination to the CNS are poorly defined and therefore therapies targeting the drivers of CNS disease are lacking. Whereas B-ALL exhibits significant subclonal diversity that contributes to functional heterogeneity and disease relapse, recent reports suggest similar clonal composition of bone marrow (BM) and CNS disease, with the potential for CNS dissemination being a universal property of B-ALL cells (Williams et al. 2016, Bartram et al. 2018). Furthermore, functional studies of leptomeningeal disease have focused on the invasion of B-ALL cells into the CNS but limited studies have addressed the selection of genetic clones with the ability to grow within the subarachnoid space. To better define the evolutionary history and biology of leptomeningeal B-ALL we performed targeted DNA, SNP copy number, RNA sequencing, and functional analysis on cells isolated from matched BM and CNS tissue of patient derived xenografts (PDX) generated from a cohort of paired diagnosis and relapse samples from 14 pediatric and adult B-ALL patients of varying cytogenetics. The majority of primary patient samples yielded CNS disease 20 weeks after intrafemoral injection into NSG mice. CNS disease burden was higher in PDXs derived from relapsed B-ALL samples. Human B-ALL cells isolated from the CNS of PDXs retained competence to repopulate disease in the BM, spleen, and CNS upon serial transplantation. Targeted DNA sequencing results analyzed using a Bayesian clustering method revealed different genetic clonal composition between matched BM and CNS cells in approximately half of the xenografts. PDXs from relapse samples were more likely to show genetic discordance between the BM and CNS. Copy number analysis also confirmed frequent genetic discordance between cells isolated from the BM and CNS from individual PDXs. Interestingly, in one patient all PDXs generated from the relapse sample displayed chromosome 6p and 17p hemi-deletions that were unique to the CNS. In total, PDXs from four patients showed recurrent enrichment of specific lesions in CNS-engrafting cells, suggesting that transit to and/or survival within the subarachnoid space can be the product of selection for genetic clones with increased CNS tropism. RNA-seq of matched BM and CNS cells derived from 45 of the primary PDXs demonstrated that CNS-isolated cells were transcriptionally distinct from their matched BM. These differences were most pronounced in samples from patients with MLL-AF4 translocations, whose CNS isolated cells grouped together in multi-dimensional scaling. Using GSEA, the most highly CNS-enriched gene sets in MLL samples were related to mRNA translation initiation and polypeptide elongation. Translation-related gene sets are similarly enriched in the blasts of MLL B-ALL patients with CNS disease in the COG 9906 study. CNS-isolated cells from PDXs of MLL patients exhibited altered rates of protein synthesis compared to matched BM-isolated cells. Treatment of PDXs with the clinically-approved translational inhibitor omacetaxine mepesuccinate (OMA) effectively decreased rates of translation in CNS-engrafting cells. Moreover, OMA reduced leukemia burden nearly 4-fold in PDXs bearing established CNS infiltration generated from two MLL patients. Our data represent an advance in the understanding of B-ALL CNS disease. We present a rich resource of genomic and transcriptomic data from xenografts spanning multiple B-ALL subgroups across diagnosis and relapse and have identified selection for genetically and biologically distinct clones in the CNS, contrary to the current model. Furthermore, we demonstrate that in MLL patients, dysregulation of protein synthesis occurs at CNS dissemination and targeting this process is a novel therapeutic paradigm that may benefit patients with CNS disease. Disclosures Mullighan: Cancer Prevention and Research Institute of Texas: Consultancy; Pfizer: Honoraria, Research Funding, Speakers Bureau; Loxo Oncology: Research Funding; Amgen: Honoraria, Speakers Bureau; Abbvie: Research Funding.

Published

2018

35. Abstract 5173: Genetic profiling of central nervous system dissemination of B-acute lymphoblastic leukemia reveals clonal selection and therapeutic vulnerability

Author

Cynthia J. Guidos, Jayne S. Danska, Ildiko Grandal, Abdellatif Daghrach, Charles G. Mullighan, Jessica McLeod, Erwin M. Schoof, John E. Dick, Stephanie M. Dobson, Olga I. Gan, Robert Vanner, Mark D. Minden, James A. Kennedy, Esmé Waanders, and Veroniqu Voisin

Subjects

0301 basic medicine, Cancer Research, Copy number analysis, Cancer, Biology, medicine.disease, Metastasis, Transplantation, 03 medical and health sciences, Leukemia, chemistry.chemical_compound, 030104 developmental biology, medicine.anatomical_structure, Oncology, chemistry, Omacetaxine mepesuccinate, medicine, Cancer research, Bone marrow, B Acute Lymphoblastic Leukemia

Abstract

B-cell acute lymphoblastic leukemia (B-ALL) readily disseminates to the leptomeninges of the central nervous system (CNS). CNS involvement is more frequent in certain poor prognosis subgroups including patients with MLL-AF4 translocations, and late CNS relapse is often lethal. The biology and clonal history of CNS leukemia are poorly defined and consequently therapies exploiting drivers of metastasis are lacking. To characterize leptomeningeal leukemia we performed targeted DNA sequencing, SNP copy number analysis, RNA sequencing, and functional analysis on cells isolated from the bone marrow (BM) and CNS of xenografts generated from a cohort of paired diagnosis and relapse samples from 14 B-ALL patients. The majority of patient samples disseminated to the CNS following intrafemoral injection into irradiated NSG mice, with greater CNS involvement in xenografts derived from relapse patient samples. Secondary transplantation of both BM- and CNS-purified cells demonstrated their capacity to re-engraft BM, CNS, and spleen. Targeted-sequencing results were analyzed using a Bayesian clustering method to determine the clonal composition of matched BM and CNS, demonstrating discordance in subclonal prevalence in nearly half the xenografts tested. Xenografts derived from two patient samples demonstrated recurrent enrichment of a particular subclone in the CNS versus BM. Similarly, copy number analysis identified frequent discordance between BM and CNS tissues within individual mice. All xenografts from one patient exhibited chromosome 6p and 17p hemi-deletions that were exclusive to CNS cells. While these data suggest that individual B-ALLs harbor subclones with CNS tropism, there were no recurrently enriched single nucleotide mutations or copy number alterations across all patients. RNA-sequencing of 45 BM and CNS pairs from primary xenografts demonstrated that CNS-isolated cells were consistently distinct from their matched BM. GSEA analysis of xenografts generated from patients with MLL-AF4 translocations (MLL) (n=2 patients, 26 mice), identified CNS cell enrichment of gene sets related to mRNA translation and nascent peptide elongation compared to BM. MLL-CNS cells exhibited altered rates of protein synthesis compared to BM cells from the same mouse. The clinically-approved translation inhibitor omacetaxine mepesuccinate effectively diminished protein translation rates of CNS isolated cells and reduced CNS engraftment by four fold in xenografts derived from two MLL-AF4 patients. These data demonstrate that the CNS microenvironment selects for the outgrowth of B-ALL cells with genetically and/or biologically distinct properties. Moreover, we demonstrate that in MLL-AF4 patients, altered protein synthesis occurs in CNS dissemination and that targeting this process may clinically benefit patients with CNS disease. Citation Format: Robert J. Vanner, Stephanie M. Dobson, Ildiko Grandal, Olga Gan, Jessica McLeod, James Kennedy, Veroniqu Voisin, Abdellatif Daghrach, Erwin M. Schoof, Cynthia Guidos, Jayne Danska, Esme Waanders, Mark Minden, Charles G. Mullighan, John E. Dick. Genetic profiling of central nervous system dissemination of B-acute lymphoblastic leukemia reveals clonal selection and therapeutic vulnerability [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 5173.

Published

2018

36. Carbohydrate antigen 19-9 is extremely elevated in polycystic liver disease

Author

Joost P. H. Drenth, Fred C.G.J. Sweep, Frederik Nevens, Loes van Keimpema, Esmé Waanders, Johannes T. Brouwer, Martijn G.H. van Oijen, Raymond Aerts, and Oncology

Subjects

Adult, Male, medicine.medical_specialty, CA-19-9 Antigen, Genetics and epigenetic pathways of disease [NCMLS 6], endocrine system diseases, Membrane transport and intracellular motility [NCMLS 5], Aetiology, screening and detection [ONCOL 5], Biology, Malignancy, Gastroenterology, Translational research [ONCOL 3], Internal medicine, medicine, Humans, Cyst, Molecular gastro-enterology and hepatology [IGMD 2], Aged, Tumor marker, Hepatology, Cysts, Cyst Fluid, Liver Diseases, Polycystic liver disease, Middle Aged, medicine.disease, Immunohistochemistry, digestive system diseases, Endocrinology, Biomarker (medicine), Female, CA19-9, Hepatic Cyst, Biomarkers, Follow-Up Studies, Kidney disease

Abstract

Contains fulltext : 80299.pdf (Publisher’s version ) (Closed access) BACKGROUND/AIMS: Carbohydrate antigen 19-9 (CA19-9) is used as a biomarker to differentiate benign from malignant gastrointestinal disorders. We examined the value of CA19-9 measurement in polycystic livers after observing high CA19-9 cyst fluid levels in a benign polycystic liver case. METHODS: We determined CA19-9 levels in serum (n=120) and hepatic cyst fluid (n=81), from patients with polycystic livers (n=109) and simple hepatic cysts (n=24). Further, we analysed CA19-9 expression in normal and polycystic liver tissue (n=17). RESULTS: Cyst fluid CA19-9 levels from both polycystic livers and simple hepatic cysts were extremely high (median 91 000 U/ml, range 14-15 870 000 U/ml; median 85 000 U/ml, range 332-1 744 000 U/ml respectively). Serum CA19-9 levels were significantly higher in polycystic liver patients (median 30 U/ml, range 0-1200 U/ml) compared with patients with simple hepatic cysts (median 10 U/ml, range 3-200 U/ml, P=0.0011). Serum CA19-9 levels correlated with those in cyst fluid (r=0.3979, P=0.0399), polycystic liver volume (r=0.3870, P=0.0025) and the size of the largest cyst (simple cysts group; r=0.5319, P=0.0280). Cyst epithelia showed strong CA19-9 expression. Evacuation of cyst fluid in four patients resulted in a dramatic decrease in the serum CA19-9 levels (60-95%). CONCLUSIONS: CA19-9 levels are high in the cyst fluid and serum of polycystic liver disease patients due to production and secretion by cyst epithelia. It does not reflect malignancy in these patients and may be of value as a biomarker for intervention efficiency assessment.

Published

2009

37. Tumor suppressor IKZF1 mediates glucocorticoid resistance in B-cell precursor acute lymphoblastic leukemia

Author

Jacqueline Cloos, Blanca Scheijen, Peter M. Hoogerbrugge, E Sonneveld, Jorn Havinga, Rene Marke, Marc Demkes, Rob Pieters, Esmé Waanders, Laurensia Yuniati, Gertjan J.L. Kaspers, Roland P. Kuiper, F.N. van Leeuwen, D van Ingen Schenau, Geert Poelmans, Hematology laboratory, CCA - Cancer biology, and Pediatric surgery

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, Genotype, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Prednisolone, Dexamethasone, law.invention, 03 medical and health sciences, Ikaros Transcription Factor, Mice, 0302 clinical medicine, law, hemic and lymphatic diseases, Internal medicine, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], medicine, Animals, Humans, Glucocorticoids, B cell, Hematology, business.industry, hemic and immune systems, medicine.disease, Mice, Mutant Strains, Leukemia, Haematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Immunology, Cancer research, Suppressor, Stem cell, business, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

Tumor suppressor IKZF1 mediates glucocorticoid resistance in B-cell precursor acute lymphoblastic leukemia

Published

2016

38. Independent development of lymphoid and histiocytic malignancies from a shared early precursor

Author

Alexander Hoischen, Peter M. Hoogerbrugge, Roland P. Kuiper, F.N. van Leeuwen, Eveline J. Kamping, Marjolijn C.J. Jongmans, Esmé Waanders, D. M W M Te Loo, Konnie M. Hebeda, Patricia J. T. A. Groenen, and Annet Simons

Subjects

Histiocytic Disorders, Malignant, Male, Cancer Research, Pathology, Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Immunoenzyme Techniques, Cancer development and immune defence Radboud Institute for Health Sciences [Radboudumc 2], 0302 clinical medicine, Immunophenotyping, Neoplasm Recurrence, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Prospective Studies, Aged, 80 and over, Hematology, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Prognosis, Combined Modality Therapy, Survival Rate, Oncology, Neoplasm Invasiveness, Lymphatic Metastasis, 030220 oncology & carcinogenesis, Immunoenzyme techniques, Female, Lymphoma, Large B-Cell, Diffuse, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Adult, Lymphatic metastasis, medicine.medical_specialty, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Biology, 03 medical and health sciences, Internal medicine, Biomarkers, Tumor, medicine, Humans, Histiocyte, Aged, Neoplasm Staging, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], medicine.disease, Lymphoma, Case-Control Studies, Neoplasm Grading, Neoplasm Recurrence, Local, Follow-Up Studies, 030215 immunology

Abstract

Independent development of lymphoid and histiocytic malignancies from a shared early precursor

Published

2016

39. Deregulation of DUX4 and ERG in acute lymphoblastic leukemia

Author

Selina M. Luger, Kerstin B. Kaufmann, Lei Wei, Robert S. Fulton, William E. Evans, Mignon L. Loh, Michelle L. Churchman, Sofia Bakogianni, Jun J. Yang, Chunxu Qu, Mary V. Relling, Ching-Hon Pui, Kelly McCastlain, Sheila A. Shurtleff, Cheryl L. Willman, Marcus L Valentine, Kerri Ochoa, Li Ding, Heather L. Mulder, Guido Marcucci, Cheng Cheng, Steven M. Kornblau, Deqing Pei, Janis Racevskis, Kristy Boggs, James R. Downing, Xiaotu Ma, Yunchao Chang, Debbie Payne-Turner, Yu Liu, Charles Lu, John Easton, John E. Dick, Bhavin Vadodaria, Wendy Stock, Shin-ichiro Takayanagi, Charles G. Mullighan, Michael N. Edmonson, Gang Wu, Scott Newman, Pankaj Gupta, Erno Wienholds, Krzysztof Mrózek, Matthew C. Foster, Elisabeth Paietta, Meenakshi Devidas, Elaine R. Mardis, Yongjin Li, Beisi Xu, Iannis Aifantis, James Dalton, Xiang Chen, Esmé Waanders, Clara D. Bloomfield, Stephen P. Hunger, Sima Jeha, I-Ming L. Chen, Lucinda Fulton, Kathryn G. Roberts, Guangchun Song, Susana C. Raimondi, Richard K. Wilson, Yanling Liu, Yashodhan Tabib, Ilaria Iacobucci, Ji Wen, Jingjing Wang, Jacob M. Rowe, Martin S. Tallman, Jessica Kohlschmidt, Michael Rusch, Hiroki Yoshihara, Jing Ma, Jinghui Zhang, Richard C. Harvey, and Panagiotis Ntziachristos

Subjects

Adult, 0301 basic medicine, Gene isoform, Adolescent, genetic structures, Biology, Article, Young Adult, 03 medical and health sciences, Transactivation, 0302 clinical medicine, Transcriptional Regulator ERG, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Genetics, Humans, Protein Isoforms, Transcription factor, Gene Rearrangement, Homeodomain Proteins, Regulation of gene expression, Gene Expression Profiling, ETS transcription factor family, Gene rearrangement, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Molecular biology, eye diseases, Gene Expression Regulation, Neoplastic, Cell Transformation, Neoplastic, 030104 developmental biology, 030220 oncology & carcinogenesis, sense organs, Transcription Factor Gene, Gene Deletion

Abstract

Chromosomal rearrangements deregulating hematopoietic transcription factors are common in acute lymphoblastic leukemia (ALL).1,2 Here, we show that deregulation of the homeobox transcription factor gene DUX4 and the ETS transcription factor gene ERG are hallmarks of a subtype of B-progenitor ALL that comprises up to 7% of B-ALL. DUX4 rearrangement and overexpression was present in all cases, and was accompanied by transcriptional deregulation of ERG, expression of a novel ERG isoform, ERGalt, and frequent ERG deletion. ERGalt utilizes a non-canonical first exon whose transcription was initiated by DUX4 binding. ERGalt retains the DNA-binding and transactivating domains of ERG, but inhibits wild-type ERG transcriptional activity and is transforming. These results illustrate a unique paradigm of transcription factor deregulation in leukemia, in which DUX4 deregulation results in loss-of-function of ERG, either by deletion or induction of expression of an isoform that is a dominant negative inhibitor of wild type ERG function.

Published

2016

40. A RAG driver on the road to pediatric ALL

Author

Esmé Waanders and Roland P. Kuiper

Subjects

Gene Rearrangement, Homeodomain Proteins, Recombination, Genetic, Genetics, Oncogene Proteins, Fusion, Mechanism (biology), Lymphoblastic Leukemia, Genetic Variation, Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], Biology, Article, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, hemic and lymphatic diseases, Core Binding Factor Alpha 2 Subunit, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], medicine, Humans, Gene, Recombination, B cell

Abstract

The ETV6-RUNX1 fusion gene, found in 25% of childhood acute lymphoblastic leukemia (ALL), is acquired in utero but requires additional somatic mutations for overt leukemia. We used exome and low-coverage whole-genome sequencing to characterize secondary events associated with leukemic transformation. RAG-mediated deletions emerge as the dominant mutational process, characterized by recombination signal sequence motifs near the breakpoints; incorporation of non-templated sequence at the junction; ~30-fold enrichment at promoters and enhancers of genes actively transcribed in B-cell development and an unexpectedly high ratio of recurrent to non-recurrent structural variants. Single cell tracking shows that this mechanism is active throughout leukemic evolution with evidence of localized clustering and re-iterated deletions. Integration of point mutation and rearrangement data identifies ATF7IP and MGA as two new tumor suppressor genes in ALL. Thus, a remarkably parsimonious mutational process transforms ETV6-RUNX1 lymphoblasts, targeting the promoters, enhancers and first exons of genes that normally regulate B-cell differentiation.

Published

2014

41. On the monophyly of chromalveolates using a six-protein phylogeny of eukaryotes

Author

Patrick J. Keeling, Esmé Waanders, and James T. Harper

Subjects

Sequence analysis, Molecular Sequence Data, Biology, medicine.disease_cause, Microbiology, Evolution, Molecular, Monophyly, Cytosol, Phylogenetics, medicine, Animals, Plastids, Ciliophora, Plastid, Gene, Phylogeny, Ecology, Evolution, Behavior and Systematics, Chromalveolata, Genetics, fungi, Eukaryota, Proteins, Protist, Sequence Analysis, DNA, General Medicine, biology.organism_classification, Eukaryotic Cells, Molecular phylogenetics, Dinoflagellida, Apicomplexa, Cryptophyta

Abstract

A global phylogeny of major eukaryotic lineages is a significant and ongoing challenge to molecular phylogenetics. Currently, there are five hypothesized major lineages or ‘supergroups' of eukaryotes. One of these, the chromalveolates, represents a large fraction of protist and algal diversity. The chromalveolate hypothesis was originally based on similarities between the photosynthetic organelles (plastids) found in many of its members and has been supported by analyses of plastid-related genes. However, since plastids can move between eukaryotic lineages, it is important to provide additional support from data generated from the nuclear-cytosolic host lineage. Genes coding for six different cytosolic proteins from a variety of chromalveolates (yielding 68 new gene sequences) have been characterized so that multiple gene analyses, including all six major lineages of chromalveolates, could be compared and concatenated with data representing all five hypothesized supergroups. Overall support for much of the phylogenies is decreased over previous analyses that concatenated fewer genes for fewer taxa. Nevertheless, four of the six chromalveolate lineages (apicomplexans, ciliates, dinoflagellates and heterokonts) consistently form a monophyletic assemblage, whereas the remaining two (cryptomonads and haptophytes) form a weakly supported group. Whereas these results are consistent with the monophyly of chromalveolates inferred from plastid data, testing this hypothesis is going to require a substantial increase in data from a wide variety of organisms.

Published

2005

42. Mammaglobin is associated with low-grade, steroid receptor-positive breast tumors from postmenopausal patients, and has independent prognostic value for relapse-free survival time

Author

Peggy Manders, Paul N. Span, Fred C.G.J. Sweep, J. J. T. M. Heuvel, John A. Foekens, Mark A. Watson, Esmé Waanders, and Louk V.A.M. Beex

Subjects

Oncology, Adult, Cancer Research, medicine.medical_specialty, Pathology, Multivariate analysis, medicine.drug_class, Mammary gland, Breast Neoplasms, Disease-Free Survival, Mammaglobin, Breast cancer, Mammaglobin-A, Internal medicine, medicine, Biomarkers, Tumor, Humans, Uteroglobin, RNA, Messenger, RNA, Neoplasm, Aged, Netherlands, Molecular diagnosis, prognosis and monitoring [UMCN 1.2], Aged, 80 and over, biology, business.industry, Endocrinology and reproduction [UMCN 5.2], Hazard ratio, Mammaglobin A, Progesterone Receptor Status, Middle Aged, medicine.disease, Neoplasm Proteins, Postmenopause, medicine.anatomical_structure, Estrogen, Multivariate Analysis, biology.protein, Regression Analysis, Female, business

Abstract

Purpose The tumor mRNA expression levels of mammaglobin, a novel breast-specific and breast cancer-associated marker, were correlated with disease outcome in 280 patients with primary breast cancer. Patients and Methods Mammaglobin expression levels were assessed by quantitative reverse transcriptase polymerase chain reaction in frozen tumor tissue from breast cancer patients with a median age of 60 years (range, 30 to 88 years) and a median follow-up of 85 months (range, 2 to 169 months). Results High expression levels were associated with low-grade tumors (P = .018), with positive estrogen and progesterone receptor status (P < .001), and postmenopausal status (P = .010). In the analysis of all patients, low tumor mammaglobin expression levels predicted an early relapse both in Cox univariate (hazard ratio [HR], 0.52; 95% CI, 0.34 to 0.79; P = .002) and multivariate regression analyses corrected for the traditional prognostic factors (HR, 0.55; 95% CI, 0.35 to 0.88; P = .012). The association of mammaglobin expression with the rate of relapse was particularly favorable in patients who received adjuvant tamoxifen treatment (HR, 0.35; 95% CI, 0.17 to 0.71; P = .004). Conclusion These results demonstrate that the assessment of the tumor mRNA expression level of the breast-specific protein mammaglobin could be useful to stratify patients for individual adjuvant treatment strategies.

Published

2004

43. Outcome of children with hypodiploid ALL treated with risk-directed therapy based on MRD levels

Author

Guangchun Song, Mary V. Relling, James R. Downing, Charles G. Mullighan, Yiping Fan, William E. Evans, Wing Leung, Hiroto Inaba, Susana C. Raimondi, John K. Choi, W. Paul Bowman, Dario Campana, Esmé Waanders, Debbie Payne-Turner, Jinghui Zhang, Wenjian Yang, Sima Jeha, Deqing Pei, Xiaotu Ma, Ching-Hon Pui, Jun J. Yang, Elaine Coustan-Smith, and Kathryn G. Roberts

Subjects

Oncology, Male, medicine.medical_specialty, Pathology, Neoplasm, Residual, Adolescent, medicine.medical_treatment, Immunology, Treatment outcome, Hematopoietic stem cell transplantation, Biochemistry, Polymerase Chain Reaction, Flow cytometry, Precursor Cell Lymphoblastic Leukemia Lymphoma, Risk Factors, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Correspondence, medicine, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Humans, Child, medicine.diagnostic_test, business.industry, Hematopoietic Stem Cell Transplantation, Infant, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Flow Cytometry, Prognosis, Treatment Outcome, Child, Preschool, Female, Neoplasm Recurrence, Local, business, Hypodiploid Acute Lymphoblastic Leukemia

Abstract

To the editor: Hypodiploid acute lymphoblastic leukemia (ALL) with

Published

2015

44. Severe Polycystic Liver Disease Is Not Caused by Large Deletions of the PRKCSH Gene

Author

Wybrich R, Cnossen, Jake S F, Maurits, Jody, Salomon, René H M, Te Morsche, Esmé, Waanders, and Joost P H, Drenth

Subjects

Adult, Male, Cysts, Liver Diseases, Calcium-Binding Proteins, Intracellular Signaling Peptides and Proteins, Membrane Proteins, RNA-Binding Proteins, Middle Aged, Humans, Female, Multiplex Polymerase Chain Reaction, Glucosidases, Research Articles, Aged, Molecular Chaperones, Retrospective Studies, Sequence Deletion

Abstract

BACKGROUND: Isolated polycystic liver disease (ADPLD) is an autosomal dominant Mendelian disorder. Heterozygous PRKCSH (where PRKCSH is protein kinase C substrate 80K‐H (80 kDa protein, heavy chain; MIM*177060) mutations are the most frequent cause. Routine molecular testing using Sanger sequencing identifies pathogenic variants in the PRKCSH (15%) and SEC63 (where SEC63 is Saccharomyces cerevisiae homolog 63 (MIM*608648); 6%) genes, but about approximately 80% of patients meeting the clinical ADPLD criteria carry no PRKCSH or SEC63 mutation. Cyst tissue often shows somatic deletions with loss of heterozygosity that was recently recognized as a general mechanism in ADPLD. We hypothesized that germline deletions in the PRKCSH gene may be responsible for hepatic cystogenesis in a significant number of mutation‐negative ADPLD patients. METHODS: In this study, we designed a multiplex ligation‐dependent probe amplification (MLPA) assay to screen for deletions of PRKCSH exons. Genomic DNA from 60 patients with an ADPLD phenotype was included. RESULTS: MLPA analysis detected no exon deletions in mutation‐negative ADPLD patients. CONCLUSION: Large copy number variations on germline level are not present in patients with a clinical diagnosis of ADPLD. MLPA analysis of the PRKCSH gene should not be considered as a diagnostic method to explain hepatic cystogenesis.

Published

2014

45. Identification of a recurrent germline PAX5 mutation and susceptibility to pre-B cell acute lymphoblastic leukemia

Author

Katherine L. Tucker, Samantha Hansford, Guangchun Song, Tom Walsh, Paul A. Meyers, Martin Fleisher, Kenan Onel, Vundavalli V. Murty, Nicholas D. Socci, Deepa Bhojwani, Sharon E. Plon, Susana C. Raimondi, Jeremy Wechsler, Ming Lee, Hamish S. Scott, Jinghui Zhang, Peter Maslak, Andrew E. Timms, Sohela Shah, Megan Harlan Fleischut, Agnes Viale, Jing Ma, Annet Simons, Rohini Rau-Murthy, Lily Offit, Xiaoni Gao, Kathryn G. Roberts, Robert J. Klein, Georgia Chenevix-Trench, Kenneth Offit, Scott W. Lowe, Esmé Waanders, Rosemary Sutton, Mary Claire King, Jun Li, David S. Ziegler, Suresh C. Jhanwar, Deborah I. Ritter, Mark J. Daly, Shann Ching Chen, Joseph Vijai, Sarah M. Lo, Marshall S. Horwitz, Jason Littman, John T. Sandlund, Cornelius Miething, Joshua D. Schiffman, James E. Hayes, Michael Rusch, David A. Wheeler, Jinjun Cheng, Gang Wu, Rajmohan Murali, David Altshuler, Kasmintan A. Schrader, Roland P. Kuiper, Katherine L. Nathanson, Steven M. Lipkin, Charles G. Mullighan, Marina Corines, Christopher N. Hahn, Panduka Nagahawatte, David G. Huntsman, Ross L. Levine, Lei Wei, Christopher Manschreck, Janine Senz, James R. Downing, Thomas Kitzing, and Jun J. Yang

Subjects

Somatic cell, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Germline, Article, Loss of heterozygosity, Germline mutation, immune system diseases, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, hemic and lymphatic diseases, Genetics, medicine, Humans, Genetic Predisposition to Disease, Allele, Genetics and epigenetic pathways of disease Translational research [NCMLS 6], B cell, Germ-Line Mutation, Mutation, Leukemia, PAX5 Transcription Factor, medicine.disease, medicine.anatomical_structure, FOS: Biological sciences, Human chromosome abnormalities--Diagnosis, Cancer research

Abstract

Contains fulltext : 126772.pdf (Publisher’s version ) (Closed access) Somatic alterations of the lymphoid transcription factor gene PAX5 (also known as BSAP) are a hallmark of B cell precursor acute lymphoblastic leukemia (B-ALL), but inherited mutations of PAX5 have not previously been described. Here we report a new heterozygous germline variant, c.547G>A (p.Gly183Ser), affecting the octapeptide domain of PAX5 that was found to segregate with disease in two unrelated kindreds with autosomal dominant B-ALL. Leukemic cells from all affected individuals in both families exhibited 9p deletion, with loss of heterozygosity and retention of the mutant PAX5 allele at 9p13. Two additional sporadic ALL cases with 9p loss harbored somatic PAX5 substitutions affecting Gly183. Functional and gene expression analysis of the PAX5 mutation demonstrated that it had significantly reduced transcriptional activity. These data extend the role of PAX5 alterations in the pathogenesis of pre-B cell ALL and implicate PAX5 in a new syndrome of susceptibility to pre-B cell neoplasia.

Published

2013

46. Abstract LB-341: Evolving functional heterogeneity in B-acute lymphoblastic leukemia

Author

Stephanie M. Dobson, Robert Vanner, Esmé Waanders, Olga I. Gan, Jessica McLeod, Ildiko Grandal, Debbie Payne-Turner, Michael Edmonson, Zhaohui Gu, Xioatu Ma, Yiping Fan, Pankaj Gupta, Sagi Abelson, Michael Rusch, Ying Shao, Scott Olsen, Geoffrey Neale, John Easton, Cynthia J. Guidos, Jayne S. Danska, Jinghui Zhang, Mark D. Minden, Charles G. Mullighan, and John E. Dick

Subjects

Cancer Research, Oncology

Abstract

Current cancer therapies are directed at molecular markers or dominant pathways present in the bulk of neoplastic cells. However, recent studies have identified many genetically distinct subclones co-existing within a single neoplasm. In over 50% of patients with relapsed acute lymphoblastic leukemia (ALL), the genetic clones present at relapse are not the dominant clone present at diagnosis, but have evolved from a minor or ancestral clone (Mullighan et al., Science, 2008). Previous work has shown that this subclonal diversity in B-ALL exists at the level of the leukemia-initiating cells (L-IC) capable of generating patient derived xenografts (Notta et al., Nature, 2011). In order to investigate the functional consequences of genetic clonal evolution during disease progression, we performed in-depth genomic and functional analysis of 14 paired diagnosis/relapse samples from adult and pediatric B-ALL patients of varying cytogenetics. Patient samples were subjected to whole exome sequencing (WES), SNP analysis and RNA sequencing. Diagnosis-specific, relapse-specific, and shared variants at both clonal and subclonal frequencies were identified. Limiting dilution analysis by transplantation of CD19+ leukemic blasts into 870 immune-deficient mice (xenografts) identified no significant trend in enrichment in L-IC frequency between paired patient samples with a median frequency of 1 in 2691. Despite similar frequencies of L-IC, functional differences within identically sourced patient xenografts were observed, including increased leukemic dissemination of relapse cells to distal sites such as the central nervous system (CNS), differences in engraftment levels and differences in immunophenotypes. Targeted-sequencing and copy number analysis of the xenografts, in comparison to the patient sample from which they were derived, has uncovered clonal variation and the unequivocal identification of minor subclones ancestral to the relapse in xenografts transplanted with the diagnostic sample from 8 patients. Some of these subclones are rare and were not captured through standard WES analysis of the patient samples, highlighting the value of xenografting to functionally identify and viably isolate subclones for further study. Interrogation of the therapeutic responses of the ‘relapse-like’ diagnosis subclones in secondary xenografts displayed differential resistance to standard chemotherapeutic agents (vincristine and L-asparaginase) pre-existing in the patient diagnosis samples prior to treatment. Furthermore, investigation of different sites of leukemic infiltration in the xenografts provided evidence of distinct clonal selection in the CNS, a known site of disease relapse, in comparison to the bone marrow. Using this data we can begin to draw the evolutionary paths to relapse. We have shown evidence that minor subclones at diagnosis, ancestral to the relapsing clone, possess functional advantages over other diagnostic clones. Overall, this work provides a substantial advance in connecting genetic diversity to functional consequences, thereby furthering our understanding of the heterogeneity identified in B-ALL and its contributions to therapy failure and disease recurrence. Citation Format: Stephanie M. Dobson, Robert Vanner, Esmé Waanders, Olga I. Gan, Jessica McLeod, Ildiko Grandal, Debbie Payne-Turner, Michael Edmonson, Zhaohui Gu, Xioatu Ma, Yiping Fan, Pankaj Gupta, Sagi Abelson, Michael Rusch, Ying Shao, Scott Olsen, Geoffrey Neale, John Easton, Cynthia J. Guidos, Jayne S. Danska, Jinghui Zhang, Mark D. Minden, Charles G. Mullighan, John E. Dick. Evolving functional heterogeneity in B-acute lymphoblastic leukemia. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr LB-341.

Published

2016

47. Abstract A25: Evolving functional heterogeneity in B-acute lymphoblastic leukemia

Author

Yiping Fan, Stephanie M. Dobson, John Easton, Charles G. Mullighan, Olga I. Gan, Mark D. Minden, John E. Dick, Jessica McLeod, Michael Rusch, Esmé Waanders, Debbie Payne-Turner, Pankaj Gupta, Zhaohui Gu, Robert Vanner, Xiaotu Ma, Cynthia J. Guidos, Jinghui Zhang, and Jayne S. Danska

Subjects

Genetics, Oncology, Cancer Research, medicine.medical_specialty, business.industry, Copy number analysis, Clone (cell biology), Cancer, medicine.disease, Somatic evolution in cancer, Transplantation, Internal medicine, Medicine, B Acute Lymphoblastic Leukemia, business, Exome sequencing, SNP array

Abstract

Current cancer therapies are directed at molecular markers or dominant pathways present in the bulk of neoplastic cells. However, recent studies have identified many genetically distinct subclones co-existing within a single neoplasm. In over 50% of patients with relapsed acute lymphoblastic leukemia (ALL), the genetic clones present at relapse are not the dominant clone present at diagnosis, but have evolved from a minor or ancestral clone (Mullighan et al., Science, 2008). Previous work has shown that this subclonal diversity in B-ALL exists at the level of the leukemia-initiating cells (L-IC) capable of generating patient derived xenografts (Notta et al., Nature, 2011). In order to investigate the functional consequences of genetic clonal evolution during disease progression, we performed in-depth genomic and functional analysis of 14 paired diagnosis/relapse samples from adult and pediatric B-ALL patients of varying cytogenetics. Patient samples were subjected to whole exome sequencing (WES), SNP analysis and RNA sequencing. Diagnosis-specific, relapse-specific, and shared variants at both clonal and subclonal frequencies were identified. Limiting dilution analysis by transplantation of CD19+ leukemic blasts into 870 immune-deficient mice (xenografts) identified no significant trend in enrichment in L-IC frequency between paired patient samples with a median frequency of 1 in 2691. Despite similar frequencies of L-IC, functional differences within identically sourced patient xenografts were observed, including increased leukemic dissemination of relapse cells to distal sites such as the central nervous system (CNS), differences in engraftment levels and differences in immunophenotypes. Targeted-sequencing and copy number analysis of the xenografts, in comparison to the patient sample from which they were derived, has uncovered clonal variation and the unequivocal identification of minor subclones ancestral to the relapse in xenografts transplanted with the diagnostic sample from 8 patients. Some of these subclones are rare and were not captured through standard WES analysis of the patient samples, highlighting the value of xenografting to functionally identify and viably isolate subclones for further study. Interrogation of the therapeutic responses of the ‘relapse-like’ diagnosis subclones in secondary xenografts displayed differential resistance to standard chemotherapeutic agents (vincristine and L-asparaginase) pre-existing in the patient diagnosis samples prior to treatment. Furthermore, investigation of different sites of leukemic infiltration in the xenografts provided evidence of distinct clonal selection in the CNS, a known site of disease relapse, in comparison to the bone marrow. Using this data we can begin to draw the evolutionary paths to relapse. We have shown evidence that minor subclones at diagnosis, ancestral to the relapsing clone, possess functional advantages over other diagnostic clones. Overall, this work provides a substantial advance in connecting genetic diversity to functional consequences, thereby furthering our understanding of the heterogeneity identified in B-ALL and its contributions to therapy failure and disease recurrence. Citation Format: Stephanie M. Dobson, Robert Vanner, Esme Waanders, Olga I. Gan, Jessica McLeod, Ildiko Grandal, Debbie Payne-Turner, Michael Edmonson, Zhaohui Gu, Xioatu Ma, Yiping Fan, Pankaj Gupta, Sagi Abelson, Michael Rusch, Ying Shao, Scott Olsen, Geoffrey Neale, John Easton, Cynthia J. Guidos, Jayne S. Danska, Jinghui Zhang, Mark D. Minden, Charles G. Mullighan, John E. Dick. Evolving functional heterogeneity in B-acute lymphoblastic leukemia. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr LB-341.

Published

2016

48. Secondary, somatic mutations might promote cyst formation in patients with autosomal dominant polycystic liver disease

Author

Esmé Waanders, Joost P.H. Drenth, Ruoyu Xing, Manoe J. Janssen, Jannes Woudenberg, Rene H. M. te Morsche, and Henry B.P.M. Dijkman

Subjects

Adult, DNA Mutational Analysis, Autosomal dominant polycystic kidney disease, Loss of Heterozygosity, Membrane transport and intracellular motility [NCMLS 5], Biology, Polymorphism, Single Nucleotide, Loss of heterozygosity, Germline mutation, SEC63, Translational research [ONCOL 3], parasitic diseases, medicine, Humans, Cyst, Allele, Molecular gastro-enterology and hepatology [IGMD 2], Genetics and epigenetic pathways of disease Translational research [NCMLS 6], Germ-Line Mutation, Hepatology, Cysts, PRKCSH, Liver Diseases, Polycystic liver disease, Calcium-Binding Proteins, Intracellular Signaling Peptides and Proteins, Gastroenterology, Middle Aged, medicine.disease, Mutation, Cancer research, Female, Molecular gastro-enterology and hepatology Translational research [IGMD 2], Glucosidases

Abstract

Item does not contain fulltext BACKGROUND & AIMS: Heterozygous germline mutations in PRKCSH cause autosomal dominant polycystic liver disease (PCLD), but it is not clear how they lead to cyst formation. We investigated whether mutations in cyst epithelial cells and corresponding loss of the PRKCSH gene product (hepatocystin) contributed to cyst development. METHODS: Liver cyst material was collected through laparoscopic cyst fenestration from 8 patients with PCLD who had a heterozygous germline mutation in PRKCSH. Tissue sections from 71 cysts (2-14 per patient) were obtained for hepatocystin staining and mutation analysis. Cyst epithelium was acquired using laser microdissection; DNA was isolated and analyzed for loss of heterozygosity (LOH) and somatic mutations using restriction analysis and sequencing. Common single nucleotide polymorphisms (SNPs) in a 70-kilobase region surrounding the germline mutation were used to determine variations in the genomic region with LOH. RESULTS: The wild-type allele of PRKCSH was lost (LOH) in 76% of cysts (54/71). Hepatocystin was not detected in cyst epithelia with LOH, whereas heterozygous cysts still expressed hepatocystin. The variation observed in the LOH region analysis indicates that cysts develop independently. We also detected somatic mutations in PRKCSH in 17% (2/12) of the cysts without LOH. Trans-heterozygous mutations in SEC63 were not observed. CONCLUSIONS: Among patients with PCLD who have a heterozygous germline mutation in PRKCSH, we found secondary, somatic mutations (second hits) in more than 76% of the liver cyst epithelia. PCLD is recessive at the cellular level, and loss of functional PRKCSH is an important step in cystogenesis.

Published

2011

49. TET2 mutations in childhood leukemia

Author

Saskia Langemeijer, E Sonneveld, Esmé Waanders, Marion Massop, Ellen Stevens-Linders, Marian Stevens-Kroef, P. van Hoogen, Christian M. Zwaan, A. Geurts van Kessel, Roland P. Kuiper, M.M. van den Heuvel-Eibrink, Jeroen D Hooijer, Peter M. Hoogerbrugge, S.V. van Reijmersdal, Joop H. Jansen, and Pediatrics

Subjects

Cancer Research, medicine.medical_specialty, Childhood leukemia, Biology, medicine.disease_cause, Dioxygenases, Translational research [ONCOL 3], Internal medicine, Proto-Oncogene Proteins, medicine, Humans, Genetics and epigenetic pathways of disease Translational research [NCMLS 6], Child, Mutation, Immune Regulation Translational research [NCMLS 2], Hematology, Cancer, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Age-related aspects of cancer Immune Regulation [ONCOL 2], DNA-Binding Proteins, Leukemia, Leukemia, Myeloid, Acute, Oncology, Immunology

Abstract

Contains fulltext : 98390.pdf (Publisher’s version ) (Closed access)

Published

2011

50. Microarray-based genomic profiling as a diagnostic tool in acute lymphoblastic leukemia

Author

Marian Stevens-Kroef, Roland P. Kuiper, Ad Geurts van Kessel, Peter M. Hoogerbrugge, Sabine van Gessel, Eva van den Berg, Daniel Olde Weghuis, Esmé Waanders, Najat El Idrissi-Zaynoun, and Arnold Simons

Subjects

Male, Cancer Research, Microarray, Chronic lymphocytic leukemia, Gene Dosage, Biology, Bioinformatics, Gene dosage, Polymorphism, Single Nucleotide, Sensitivity and Specificity, HEMATOLOGIC MALIGNANCIES, ARRAY ANALYSIS, CDKN2A, CHRONIC-LYMPHOCYTIC-LEUKEMIA, Genetics, medicine, MYELODYSPLASTIC SYNDROMES, Humans, Child, Genetics and epigenetic pathways of disease Translational research [NCMLS 6], CYTOGENETIC TOOL, In Situ Hybridization, Fluorescence, Oligonucleotide Array Sequence Analysis, Chromosome Aberrations, medicine.diagnostic_test, MUTATIONS, Myelodysplastic syndromes, DELETION, Gold standard (test), Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, IKZF1, DNA Fingerprinting, ETV6, Karyotyping, Female, MENTAL-RETARDATION, Fluorescence in situ hybridization

Abstract

Contains fulltext : 98100.pdf (Publisher’s version ) (Closed access) In acute lymphoblastic leukemia (ALL) specific genomic abnormalities provide important clinical information. In most routine clinical diagnostic laboratories conventional karyotyping, in conjunction with targeted screens using e.g., fluorescence in situ hybridization (FISH), is currently considered as the gold standard to detect such aberrations. Conventional karyotyping, however, is limited in its resolution and yield, thus hampering the genetic diagnosis of ALL. We explored whether microarray-based genomic profiling would be feasible as an alternative strategy in a routine clinical diagnostic setting. To this end, we compared conventional karyotypes with microarray-deduced copy number aberration (CNA) karyotypes in 60 ALL cases. Microarray-based genomic profiling resulted in a CNA detection rate of 90%, whereas for conventional karyotyping this was 61%. In addition, many small (< 5 Mb) genetic lesions were encountered, frequently harboring clinically relevant ALL-related genes such as CDKN2A/B, ETV6, PAX5, and IKZF1. From our data we conclude that microarray-based genomic profiling serves as a robust tool in the genetic diagnosis of ALL, outreaching conventional karyotyping in CNA detection both in terms of sensitivity and specificity. We also propose a practical workflow for a comprehensive and objective interpretation of CNAs obtained through microarray-based genomic profiling, thereby facilitating its application in a routine clinical diagnostic setting.

Published

2011