Your search keyword '"Tommy Martinsson"' showing total 552 results

1. Personalized circulating tumor DNA analysis for sensitive disease monitoring and detection of relapse in neuroblastoma

Author

Ida Rahmqvist, Enya Engström, Elisabeth Mellström, Raghda R. Ibrahim, Fani Pujol-Calderón, Agnes Dahlstrand Rudin, Anna Ordqvist Redfors, Niki Rostamzadeh, Rita Di Rienzo, Wilma Franssila, Robert Khashan, Moe Xylander, Christin Karlsson, Torben Ek, Daniel Andersson, Tobias Österlund, Jennie Gaarder, Henrik Fagman, Susanne Fransson, Tommy Martinsson, Anders Ståhlberg, and Martin Dalin

Subjects

Circulating tumor DNA, Neuroblastoma, Pediatric cancer, Liquid biopsy, Personalized medicine, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Circulating tumor DNA (ctDNA) has shown potential as a non-invasive tumor biomarker in neuroblastoma. Previous studies used generic assays for detection of selected predefined oncogenic variants as markers of ctDNA, which limits the sensitivity and excludes a subset of patients from analysis. Here we assessed patient-specific ctDNA analysis for treatment evaluation and detection of relapse in neuroblastoma. We generated personalized sequencing panels targeting 10 tumor-specific single nucleotide variants (SNVs) for each patient and performed ctDNA analysis of 136 plasma samples collected longitudinally in 13 children with neuroblastoma. ctDNA was detected using ultra-deep next generation sequencing with unique molecular identifiers to eliminate polymerase-induced errors. We found that the levels of ctDNA at diagnosis correlated with risk group and decreased gradually during effective treatment. All samples collected during follow-up in patients without disease relapse were ctDNA-negative. All four relapses were associated with elevated ctDNA levels, and a majority of the analyzed SNVs were detected at time of relapse. In one case, ctDNA became positive 78 days before the relapse was diagnosed with routine assessment and increased by over a thousandfold before the start of additional treatment. Overall, ctDNA was more uniformly elevated at diagnosis, showed less putative false positive results, and was more sensitive for detection of relapse compared to five serum or urine tumor markers used in clinical routine. In conclusion, personalized ctDNA analysis is suitable for clinical monitoring of tumor burden and may be used in all neuroblastoma patients regardless of risk group or tumor genetics.

Published

2024

2. Joint single-cell genetic and transcriptomic analysis reveal pre-malignant SCP-like subclones in human neuroblastoma

Author

Thale K. Olsen, Jörg Otte, Shenglin Mei, Bethel Tesfai Embaie, Polina Kameneva, Huaitao Cheng, Teng Gao, Vasilios Zachariadis, Ioanna Tsea, Åsa Björklund, Emil Kryukov, Ziyi Hou, Anna Johansson, Erik Sundström, Tommy Martinsson, Susanne Fransson, Jakob Stenman, Shahrzad Shirazi Fard, John Inge Johnsen, Per Kogner, Igor Adameyko, Martin Enge, Peter V. Kharchenko, and Ninib Baryawno

Subjects

Neuroblastoma, Schwann cell precursors, Childhood cancer, Tumor heterogeneity, Tumor evolution, Clonality, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Neuroblastoma (NB) is a heterogeneous embryonal malignancy and the deadliest tumor of infancy. It is a complex disease that can result in diverse clinical outcomes. In some children, tumors regress spontaneously. Others respond well to existing treatments. But for the high-risk group, which constitutes approximately 40% of all patients, the prognosis remains dire despite collaborative efforts in basic and clinical research. While its exact cellular origin is still under debate, NB is assumed to arise from the neural crest cell lineage including multipotent Schwann cell precursors (SCPs), which differentiate into sympatho-adrenal cell states eventually producing chromaffin cells and sympathoblasts. Methods To investigate clonal development of neuroblastoma cell states, we performed haplotype-specific analysis of human tumor samples using single-cell multi-omics, including joint DNA/RNA sequencing of sorted single cells (DNTR-seq). Samples were also assessed using immunofluorescence stainings and fluorescence in-situ hybridization (FISH). Results Beyond adrenergic tumor cells, we identify subpopulations of aneuploid SCP-like cells, characterized by clonal expansion, whole-chromosome 17 gains, as well as expression programs of proliferation, apoptosis, and a non-immunomodulatory phenotype. Conclusion Aneuploid pre-malignant SCP-like cells represent a novel feature of NB. Genetic evidence and tumor phylogeny suggest that these clones and malignant adrenergic populations originate from aneuploidy-prone cells of migrating neural crest or SCP origin, before lineage commitment to sympatho-adrenal cell states. Our findings expand the phenotypic spectrum of NB cell states. Considering the multipotency of SCPs in development, we suggest that the transformation of fetal SCPs may represent one possible mechanism of tumor initiation in NB with chromosome 17 aberrations as a characteristic element.

Published

2024

3. Altered methylation of imprinted genes in neuroblastoma: implications for prognostic refinement

Author

Medha Suman, Maja Löfgren, Susanne Fransson, Jewahri Idris Yousuf, Johanna Svensson, Anna Djos, Tommy Martinsson, Per Kogner, Teresia Kling, and Helena Carén

Subjects

Neuroblastoma, Genomic imprinting, DNA methylation, Copy number alterations, Medicine

Abstract

Abstract Background Neuroblastoma (NB) is a complex disease, and the current understanding of NB biology is limited. Deregulation in genomic imprinting is a common event in malignancy. Since imprinted genes play crucial roles in early fetal growth and development, their role in NB pathogenesis could be suggested. Methods We examined alterations in DNA methylation patterns of 369 NB tumours at 49 imprinted differentially methylated regions (DMRs) and assessed its association with overall survival probabilities and selected clinical and genomic features of the tumours. In addition, an integrated analysis of DNA methylation and allele-specific copy number alterations (CNAs) was performed, to understand the correlation between the two molecular events. Results Several imprinted regions with aberrant methylation patterns in NB were identified. Regions that underwent loss of methylation in > 30% of NB samples were DMRs annotated to the genes NDN, SNRPN, IGF2, MAGEL2 and HTR5A and regions with gain of methylation were NNAT, RB1 and GPR1. Methylation alterations at six of the 49 imprinted DMRs were statistically significantly associated with reduced overall survival: MIR886, RB1, NNAT/BLCAP, MAGEL2, MKRN3 and INPP5F. RB1, NNAT/BLCAP and MKRN3 were further able to stratify low-risk NB tumours i.e. tumours that lacked MYCN amplification and 11q deletion into risk groups. Methylation alterations at NNAT/BLCAP, MAGEL2 and MIR886 predicted risk independently of MYCN amplification or 11q deletion and age at diagnosis. Investigation of the allele-specific CNAs demonstrated that the imprinted regions that displayed most alterations in NB tumours harbor true epigenetic changes and are not result of the underlying CNAs. Conclusions Aberrant methylation in imprinted regions is frequently occurring in NB tumours and several of these regions have independent prognostic value. Thus, these could serve as potentially important clinical epigenetic markers to identify individuals with adverse prognosis. Incorporation of methylation status of these regions together with the established risk predictors may further refine the prognostication of NB patients.

Published

2024

4. Heterogeneous SSTR2 target expression and a novel KIAA1549::BRAF fusion clone in a progressive metastatic lesion following 177Lutetium-DOTATATE molecular radiotherapy in neuroblastoma: a case report

Author

Se Whee Sammy Park, Susanne Fransson, Fredrik Sundquist, Joachim N. Nilsson, Per Grybäck, Sandra Wessman, Jacob Strömgren, Anna Djos, Henrik Fagman, Helene Sjögren, Kleopatra Georgantzi, Nikolas Herold, Per Kogner, Dan Granberg, Mark N. Gaze, Tommy Martinsson, Kasper Karlsson, and Jakob J. E. Stenman

Subjects

LuDO-N clinical trial, 177Lutetium-DOTATATE, molecular radiotherapy, neuroblastoma, tumor heterogeneity, KIAA1649::BRAF gene fusion, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

In this case report, we present the treatment outcomes of the first patient enrolled in the LuDO-N trial. The patient is a 21-month-old girl diagnosed with high-risk neuroblastoma (NB) and widespread skeletal metastasis. The patient initially underwent first-line therapy according to SIOPEN HRNBL-1 but was switched to second-line treatments due to disease progression, and she was finally screened for enrollment in the LuDO-N trial due to refractory disease. Upon enrollment, the patient received two rounds of the radiolabeled somatostatin analogue lutetium-177 octreotate (177Lu-DOTATATE), which was well tolerated. A dosimetry analysis revealed a heterogeneous uptake across tumor lesions, resulting in a significant absorbed dose of 54 Gy in the primary tumor, but only 2 Gy at one of the metastatic sites in the distal femur. While the initial treatment response showed disease stabilization, the distal femoral metastasis continued to progress, leading to the eventual death of the patient. A tissue analysis of the biopsies collected throughout the course of the disease revealed heterogeneous drug target expression of somatostatin receptor 2 (SSTR2) across and within tumor lesions. Furthermore, genomic profiling revealed a novel KIAA1549::BRAF fusion oncogene amplification in the distal femoral metastasis at recurrence that might be related with resistance to radiation, possibly through the downregulation of SSTR2. This case report demonstrates a mixed response to molecular radiotherapy (MRT) with 177Lu-DOTATATE. The observed variation in SSTR2 expression between tumor lesions suggests that heterogeneous target expression may have been the reason for treatment failure in this patient’s case. Further investigation within the LuDO-N trial will give a more comprehensive understanding of the correlation between SSTR2 expression levels and treatment outcomes, which will be important to advance treatment strategies based on MRT for children with high-risk NB.

Published

2024

5. Amplification of CDK4 and MDM2: a detailed study of a high-risk neuroblastoma subgroup

Author

Angela Martinez-Monleon, Hanna Kryh Öberg, Jennie Gaarder, Ana P. Berbegall, Niloufar Javanmardi, Anna Djos, Marek Ussowicz, Sabine Taschner-Mandl, Inge M. Ambros, Ingrid Øra, Bengt Sandstedt, Klaus Beiske, Ruth Ladenstein, Rosa Noguera, Peter F. Ambros, Lena Gordon Murkes, Gustaf Ljungman, Per Kogner, Susanne Fransson, and Tommy Martinsson

Subjects

Medicine, Science

Abstract

Abstract In neuroblastoma, MYCN amplification and 11q-deletion are important, although incomplete, markers of high-risk disease. It is therefore relevant to characterize additional alterations that can function as prognostic and/or predictive markers. Using SNP-microarrays, a group of neuroblastoma patients showing amplification of one or multiple 12q loci was identified. Two loci containing CDK4 and MDM2 were commonly co-amplified, although amplification of either locus in the absence of the other was observed. Pharmacological inhibition of CDK4/6 with ribociclib or abemaciclib decreased proliferation in a broad set of neuroblastoma cell lines, including CDK4/MDM2-amplified, whereas MDM2 inhibition by Nutlin-3a was only effective in p53wild-type cells. Combined CDK4/MDM2 targeting had an additive effect in p53wild-type cell lines, while no or negative additive effect was observed in p53mutated cells. Most 12q-amplified primary tumors were of abdominal origin, including those of intrarenal origin initially suspected of being Wilms’ tumor. An atypical metastatic pattern was also observed with low degree of bone marrow involvement, favoring other sites such as the lungs. Here we present detailed biological data of an aggressive neuroblastoma subgroup hallmarked by 12q amplification and atypical clinical presentation for which our in vitro studies indicate that CDK4 and/or MDM2 inhibition also could be beneficial.

Published

2022

6. The loss of DLG2 isoform 7/8, but not isoform 2, is critical in advanced staged neuroblastoma

Author

Simon Keane, Tommy Martinsson, Per Kogner, and Katarina Ejeskär

Subjects

Neuroblastoma, DLG, DLG2, LIN7A, L27, Isoform, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract Background Neuroblastoma is a childhood neural crest tumor showing large clinical and genetic heterogeneity, one form displaying 11q-deletion is very aggressive. It has been shown that 11q-deletion results in decreased expression of DLG2, a gene residing in the deleted region. DLG2 has a number of different isoforms with the main difference is the presence or absence of a L27 domain. The L27 domain containing DLG proteins can form complexes with CASK/MPP and LIN7 protein family members, which will control cell polarity and signaling. Methods We evaluated the DLG gene family and the LIN7 gene family for their expression in differently INSS staged neuroblastoma from publically available data and primary tumors, we included two distinct DLG1 and DLG2 N-terminal transcript isoforms encoding L27 domains for their expression. Functionality of DLG2 isoforms and of LIN7A were evaluated in the 11q-deleted neuroblastoma cell line SKNAS. Results In neuroblastoma only two DLG2 isoforms were expressed: isoform 2 and isoform 7/8. Using the array data we could determine that higher expression of DLG members that contain L27 domains correlated to better survival and prognosis. Whilst DLG1 showed a decrease in both isoforms with increased INSS stage, only the full length L27 containing DLG2 transcripts DLG2-isoform 7/8 showed a decrease in expression in high stage neuroblastoma. We could show that the protein encoded by DLG2-isoform 7 could bind to LIN7A, and increased DLG2-isoform 7 gene expression increased the expression of LIN7A, this reduced neuroblastoma cell proliferation and viability, with increased BAX/BCL2 ratio indicating increased apoptosis. Conclusion We have provided evidence that gene expression of the L27 domain containing DLG2-isoform 7/8 but not L27 domain lacking DLG2-isoform 2 is disrupted in neuroblastoma, in particular in the aggressive subsets of tumors. The presence of the complete L27 domain allows for the binding to LIN7A, which will control cell polarity and signaling, thus affecting cancer cell viability.

Published

2021

7. Whole-genome sequencing of recurrent neuroblastoma reveals somatic mutations that affect key players in cancer progression and telomere maintenance

Author

Susanne Fransson, Angela Martinez-Monleon, Mathias Johansson, Rose-Marie Sjöberg, Caroline Björklund, Gustaf Ljungman, Torben Ek, Per Kogner, and Tommy Martinsson

Subjects

Medicine, Science

Abstract

Abstract Neuroblastoma is the most common and deadly childhood tumor. Relapsed or refractory neuroblastoma has a very poor prognosis despite recent treatment advances. To investigate genomic alterations associated with relapse and therapy resistance, whole-genome sequencing was performed on diagnostic and relapsed lesions together with constitutional DNA from seven children. Sequencing of relapsed tumors indicates somatic alterations in diverse genes, including those involved in RAS-MAPK signaling, promoting cell cycle progression or function in telomere maintenance and immortalization. Among recurrent alterations, CCND1-gain, TERT-rearrangements, and point mutations in POLR2A, CDK5RAP, and MUC16 were shown in ≥ 2 individuals. Our cohort contained examples of converging genomic alterations in primary-relapse tumor pairs, indicating dependencies related to specific genetic lesions. We also detected rare genetic germline variants in DNA repair genes (e.g., BARD1, BRCA2, CHEK2, and WRN) that might cooperate with somatically acquired variants in these patients with highly aggressive recurrent neuroblastoma. Our data indicate the importance of monitoring recurrent neuroblastoma through sequential genomic characterization and that new therapeutic approaches combining the targeting of MAPK signaling, cell cycle progression, and telomere activity are required for this challenging patient group.

Published

2020

8. Multifocal Neuroblastoma and Central Hypoventilation in An Infant with Germline ALK F1174I Mutation

Author

Anna Djos, Diana Treis, Susanne Fransson, Lena Gordon Murkes, Sandra Wessman, Jurate Ásmundsson, Agneta Markström, Per Kogner, and Tommy Martinsson

Subjects

ALK, PHOX2B, neuroblastoma, neurocristopathies, Medicine (General), R5-920

Abstract

A preterm infant with central hypoventilation was diagnosed with multifocal neuroblastoma. Congenital anomalies of the autonomic nervous system in association with neuroblastoma are commonly associated with germline mutations in PHOX2B. Further, the ALK gene is frequently mutated in both familial and sporadic neuroblastoma. Sanger sequencing of ALK and PHOX2B, SNP microarray of three tumor samples and whole genome sequencing of tumor and blood were performed. Genetic testing revealed a germline ALK F1174I mutation that was present in all tumor samples as well as in normal tissue samples from the patient. Neither of the patient’s parents presented the ALK variant. Array profiling of the three tumor samples showed that two of them had only numerical aberrations, whereas one sample displayed segmental alterations, including a gain at chromosome 2p, resulting in two copies of the ALK-mutated allele. Whole genome sequencing confirmed the presence of the ALK variant and did not detect any aberrations in the coding or promotor region of PHOX2B. This study is to our knowledge the first to report a de novoALK F1174I germline mutation. This may not only predispose to congenital multifocal neuroblastoma but may also contribute to the respiratory dysfunction seen in this patient.

Published

2022

9. 11q Deletion or ALK Activity Curbs DLG2 Expression to Maintain an Undifferentiated State in Neuroblastoma

Author

Joachim Tetteh Siaw, Niloufar Javanmardi, Jimmy Van den Eynden, Dan Emil Lind, Susanne Fransson, Angela Martinez-Monleon, Anna Djos, Rose-Marie Sjöberg, Malin Östensson, Helena Carén, Gunhild Trøen, Klaus Beiske, Ana P. Berbegall, Rosa Noguera, Wei-Yun Lai, Per Kogner, Ruth H. Palmer, Bengt Hallberg, and Tommy Martinsson

Subjects

ALK, neuroblastoma, DLG2, tumor suppressor, retinoic acid, ERK, Biology (General), QH301-705.5

Abstract

Summary: High-risk neuroblastomas typically display an undifferentiated or poorly differentiated morphology. It is therefore vital to understand molecular mechanisms that block the differentiation process. We identify an important role for oncogenic ALK-ERK1/2-SP1 signaling in the maintenance of undifferentiated neural crest-derived progenitors through the repression of DLG2, a candidate tumor suppressor gene in neuroblastoma. DLG2 is expressed in the murine “bridge signature” that represents the transcriptional transition state when neural crest cells or Schwann cell precursors differentiate to chromaffin cells of the adrenal gland. We show that the restoration of DLG2 expression spontaneously drives neuroblastoma cell differentiation, highlighting the importance of DLG2 in this process. These findings are supported by genetic analyses of high-risk 11q deletion neuroblastomas, which identified genetic lesions in the DLG2 gene. Our data also suggest that further exploration of other bridge genes may help elucidate the mechanisms underlying the differentiation of NC-derived progenitors and their contribution to neuroblastomas.

Published

2020

10. A new GTF2I-BRAF fusion mediating MAPK pathway activation in pilocytic astrocytoma.

Author

Tajana Tešan Tomić, Josefin Olausson, Annica Wilzén, Magnus Sabel, Katarina Truvé, Helene Sjögren, Sándor Dósa, Magnus Tisell, Birgitta Lannering, Fredrik Enlund, Tommy Martinsson, Pierre Åman, and Frida Abel

Subjects

Medicine, Science

Abstract

Pilocytic astrocytoma (PA) is the most common pediatric brain tumor. A recurrent feature of PA is deregulation of the mitogen activated protein kinase (MAPK) pathway most often through KIAA1549-BRAF fusion, but also by other BRAF- or RAF1-gene fusions and point mutations (e.g. BRAFV600E). These features may serve as diagnostic and prognostic markers, and also facilitate development of targeted therapy. The aims of this study were to characterize the genetic alterations underlying the development of PA in six tumor cases, and evaluate methods for fusion oncogene detection. Using a combined analysis of RNA sequencing and copy number variation data we identified a new BRAF fusion involving the 5' gene fusion partner GTF2I (7q11.23), not previously described in PA. The new GTF2I-BRAF 19-10 fusion was found in one case, while the other five cases harbored the frequent KIAA1549-BRAF 16-9 fusion gene. Similar to other BRAF fusions, the GTF2I-BRAF fusion retains an intact BRAF kinase domain while the inhibitory N-terminal domain is lost. Functional studies on GTF2I-BRAF showed elevated MAPK pathway activation compared to BRAFWT. Comparing fusion detection methods, we found Fluorescence in situ hybridization with BRAF break apart probe as the most sensitive method for detection of different BRAF rearrangements (GTF2I-BRAF and KIAA1549-BRAF). Our finding of a new BRAF fusion in PA further emphasis the important role of B-Raf in tumorigenesis of these tumor types. Moreover, the consistency and growing list of BRAF/RAF gene fusions suggests these rearrangements to be informative tumor markers in molecular diagnostics, which could guide future treatment strategies.

Published

2017

11. Correction: A new GTF2I-BRAF fusion mediating MAPK pathway activation in pilocytic astrocytoma.

Author

Tajana Tešan Tomić, Josefin Olausson, Annica Wilzén, Magnus Sabel, Katarina Truvé, Helene Sjögren, Sándor Dósa, Magnus Tisell, Birgitta Lannering, Fredrik Enlund, Tommy Martinsson, Pierre Åman, and Frida Abel

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0175638.].

Published

2017

12. Neuroblastoma after Childhood: Prognostic Relevance of Segmental Chromosome Aberrations, ATRX Protein Status, and Immune Cell Infiltration

Author

Ana P. Berbegall, Eva Villamón, Irene Tadeo, Tommy Martinsson, Adela Cañete, Victoria Castel, Samuel Navarro, and Rosa Noguera

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Neuroblastoma (NB) is a common malignancy in children but rarely occurs during adolescence or adulthood. This subgroup is characterized by an indolent disease course, almost uniformly fatal, yet little is known about the biologic characteristics. The aim of this study was to identify differential features regarding DNA copy number alterations, α-thalassemia/mental retardation syndrome X-linked (ATRX) protein expression, and the presence of tumor-associated inflammatory cells. Thirty-one NB patients older than 10 years who were included in the Spanish NB Registry were considered for the current study; seven young and middle-aged adult patients (range 18-60 years) formed part of the cohort. We performed single nucleotide polymorphism arrays, immunohistochemistry for immune markers (CD4, CD8, CD20, CD11b, CD11c, and CD68), and ATRX protein expression. Assorted genetic profiles were found with a predominant presence of a segmental chromosome aberration (SCA) profile. Preadolescent and adolescent NB tumors showed a higher number of SCA, including 17q gain and 11q deletion. There was also a marked infiltration of immune cells, mainly high and heterogeneous, in young and middle-aged adult tumors. ATRX negative expression was present in the tumors. The characteristics of preadolescent, adolescent, young adult, and middle-aged adult NB tumors are different, not only from childhood NB tumors but also from each other. Similar examinations of a larger number of such tumor tissues from cooperative groups should lead to a better older age–dependent tumor pattern and to innovative, individual risk-adapted therapeutic approaches for these patients.

Published

2014

13. Cell culture and Drosophila model systems define three classes of anaplastic lymphoma kinase mutations in neuroblastoma

Author

Damini Chand, Yasuo Yamazaki, Kristina Ruuth, Christina Schönherr, Tommy Martinsson, Per Kogner, Edward F. Attiyeh, John Maris, Olena Morozova, Marco A. Marra, Miki Ohira, Akira Nakagawara, Per-Erik Sandström, Ruth H. Palmer, and Bengt Hallberg

Subjects

Medicine, Pathology, RB1-214

Abstract

SUMMARY Neuroblastoma is a childhood extracranial solid tumour that is associated with a number of genetic changes. Included in these genetic alterations are mutations in the kinase domain of the anaplastic lymphoma kinase (ALK) receptor tyrosine kinase (RTK), which have been found in both somatic and familial neuroblastoma. In order to treat patients accordingly requires characterisation of these mutations in terms of their response to ALK tyrosine kinase inhibitors (TKIs). Here, we report the identification and characterisation of two novel neuroblastoma ALK mutations (A1099T and R1464STOP), which we have investigated together with several previously reported but uncharacterised ALK mutations (T1087I, D1091N, T1151M, M1166R, F1174I and A1234T). In order to understand the potential role of these ALK mutations in neuroblastoma progression, we have employed cell culture-based systems together with the model organism Drosophila as a readout for ligand-independent activity. Mutation of ALK at position 1174 (F1174I) generates a gain-of-function receptor capable of activating intracellular targets such as ERK (extracellular signal regulated kinase) and STAT3 (signal transducer and activator of transcription 3) in a ligand-independent manner. Analysis of these previously uncharacterised ALK mutants and comparison with ALKF1174 mutants suggests that ALK mutations observed in neuroblastoma fall into three classes. These classes are: (i) gain-of-function ligand-independent mutations such as ALKF1174l, (ii) kinase-dead ALK mutants, e.g. ALKI1250T (Schönherr et al., 2011a) and (iii) ALK mutations that are ligand-dependent in nature. Irrespective of the nature of the observed ALK mutants, in every case the activity of the mutant ALK receptors could be abrogated by the ALK inhibitor crizotinib (Xalkori/PF-02341066), albeit with differing levels of sensitivity.

Published

2013

14. Genetic instability and intratumoral heterogeneity in neuroblastoma with MYCN amplification plus 11q deletion.

Author

Eva Villamón, Ana P Berbegall, Marta Piqueras, Irene Tadeo, Victoria Castel, Anna Djos, Tommy Martinsson, Samuel Navarro, and Rosa Noguera

Subjects

Medicine, Science

Abstract

Genetic analysis in neuroblastoma has identified the profound influence of MYCN amplification and 11q deletion in patients' prognosis. These two features of high-risk neuroblastoma usually occur as mutually exclusive genetic markers, although in rare cases both are present in the same tumor. The purpose of this study was to characterize the genetic profile of these uncommon neuroblastomas harboring both these high-risk features.We selected 18 neuroblastomas with MNA plus 11q loss detected by FISH. Chromosomal aberrations were analyzed using Multiplex Ligation-dependent Probe Amplification and Single Nucleotide Polymorphism array techniques.This group of tumors has approximately the same high frequency of aberrations as found earlier for 11q deleted tumors. In some cases, DNA instability generates genetic heterogeneity, and must be taken into account in routine genetic diagnosis.

Published

2013

15. Tumor development, growth characteristics and spectrum of genetic aberrations in the TH-MYCN mouse model of neuroblastoma.

Author

Agnes Rasmuson, Lova Segerström, Maria Nethander, Jennie Finnman, Lotta H M Elfman, Niloufar Javanmardi, Staffan Nilsson, John Inge Johnsen, Tommy Martinsson, and Per Kogner

Subjects

Medicine, Science

Abstract

BackgroundThe TH-MYCN transgenic neuroblastoma model, with targeted MYCN expression to the developing neural crest, has been used to study neuroblastoma development and evaluate novel targeted tumor therapies.MethodsWe followed tumor development in 395 TH-MYCN (129X1/SvJ) mice (125 negative, 206 hemizygous and 64 homozygous mice) by abdominal palpations up to 40 weeks of age. DNA sequencing of MYCN in the original plasmid construct and mouse genomic DNA was done to verify the accuracy. Copy number analysis with Affymetrix® Mouse Diversity Genotyping Arrays was used to characterize acquired genetic aberrations.ResultsDNA sequencing confirmed presence of human MYCN cDNA in genomic TH-MYCN DNA corresponding to the original plasmid construct. Tumor incidence and growth correlated significantly to transgene status with event-free survival for hemizygous mice at 50%, and 0% for homozygous mice. Hemizygous mice developed tumors at 5.6-19 weeks (median 9.1) and homozygous mice at 4.0-6.9 weeks (5.4). The mean treatment window, time from palpable tumor to sacrifice, for hemizygous and homozygous mice was 15 and 5.2 days, respectively. Hemizygous mice developing tumors as early as homozygous mice had a longer treatment window. Age at tumor development did not influence treatment window for hemizygous mice, whereas treatment window in homozygous mice decreased significantly with increasing age. Seven out of 10 analysed tumors had a flat DNA profile with neither segmental nor numerical chromosomal aberrations. Only three tumors from hemizygous mice showed acquired genetic features with one or more numerical aberrations. Of these, one event corresponded to gain on the mouse equivalent of human chromosome 17.ConclusionHemizygous and homozygous TH-MYCN mice have significantly different neuroblastoma incidence, tumor growth characteristics and treatment windows but overlap in age at tumor development making correct early genotyping essential to evaluate therapeutic interventions. Contrasting previous studies, our data show that TH-MYCN tumors have few genetic aberrations.

Published

2012

16. Supplementary table 3-5 from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Supplementary Table S3. Related to Figure 3. Gene ontology for genes with higher expression in patient tumors vs. PDOXs. Supplementary Table S4. Related to Figure 3. List of the gene clusters defined across PDOXs #1-5 obtained from serial orthotopic passaging. Supplementary Table S5. Related to Figure 3. List of enriched Gene Ontology terms by cluster defined in PDOXs #1-5.

Published

2023

17. Supplementary table 8-14 from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Supplementary Table S8. Related to Figure 5. List of top varying peptides based on SD across all samples derived from Patient/PDOX #5. Supplementary Table S9. Related to Figure 5. List of top varying phospho-peptides based on SD across all samples derived from Patient/PDOX #5. Supplementary Table S10. Related to Figure 5. List of enriched Gene Ontology terms by cluster derived from the protein clusters defined in Suppl. Table S8. Supplementary Table S11. Related to Figure 5. List of enriched Gene Ontology terms by cluster derived from the phospho-protein clusters defined in Suppl. Table S9. Supplementary Table S12. Related to Figure 5. List of differentially expressed proteins from group 1-3 of PDOX #5. Supplementary Table S13. Related to Figure 5. List of differentially expressed phosphorylated proteins from group 1-3 of PDOX #5. Supplementary Table S14. Related to Figure 5. List of peptides measured in the targeted PRM assay.

Published

2023

18. Supplementary Table 1 from Meta-analysis of Neuroblastomas Reveals a Skewed ALK Mutation Spectrum in Tumors with MYCN Amplification

Author

Frank Speleman, Rogier Versteeg, Jan Cools, Angelika Eggert, Huib Caron, Miki Ohira, Akira Nakagawara, Tommy Martinsson, Per Kogner, Isabelle Janoueix-Lerosey, Olivier Delattre, Rosa Noguera, Marleen Renard, Klaus Beiske, Nadine Van Roy, Joëlle Vermeulen, Caroline Van Den Broecke, Alexander Schramm, Johannes H. Schulte, Geneviève Laureys, Anne De Paepe, Tom Van Maerken, Jasmien Hoebeeck, Jo Vandesompele, Arjan Lakeman, Ellen M. Westerhout, Michaël Porcu, Piotr Zabrocki, Candy Kumps, Katleen De Preter, and Sara De Brouwer

Abstract

PDF file - 1.29MB

Published

2023

19. Figure S2 from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Supplementary Figure S2. Related to Figure 4. Intratumor heterogeneity is less prominent than intertumor heterogeneity.

Published

2023

20. Data from Meta-analysis of Neuroblastomas Reveals a Skewed ALK Mutation Spectrum in Tumors with MYCN Amplification

Author

Frank Speleman, Rogier Versteeg, Jan Cools, Angelika Eggert, Huib Caron, Miki Ohira, Akira Nakagawara, Tommy Martinsson, Per Kogner, Isabelle Janoueix-Lerosey, Olivier Delattre, Rosa Noguera, Marleen Renard, Klaus Beiske, Nadine Van Roy, Joëlle Vermeulen, Caroline Van Den Broecke, Alexander Schramm, Johannes H. Schulte, Geneviève Laureys, Anne De Paepe, Tom Van Maerken, Jasmien Hoebeeck, Jo Vandesompele, Arjan Lakeman, Ellen M. Westerhout, Michaël Porcu, Piotr Zabrocki, Candy Kumps, Katleen De Preter, and Sara De Brouwer

Abstract

Purpose: Activating mutations of the anaplastic lymphoma kinase (ALK) were recently described in neuroblastoma. We carried out a meta-analysis of 709 neuroblastoma tumors to determine their frequency and mutation spectrum in relation to genomic and clinical parameters, and studied the prognostic significance of ALK copy number and expression.Experimental Design: The frequency and type of ALK mutations, copy number gain, and expression were analyzed in a new series of 254 neuroblastoma tumors. Data from 455 published cases were used for further in-depth analysis.Results: ALK mutations were present in 6.9% of 709 investigated tumors, and mutations were found in similar frequencies in favorable [International Neuroblastoma Staging System (INSS) 1, 2, and 4S; 5.7%] and unfavorable (INSS 3 and 4; 7.5%) neuroblastomas (P = 0.087). Two hotspot mutations, at positions R1275 and F1174, were observed (49% and 34.7% of the mutated cases, respectively). Interestingly, the F1174 mutations occurred in a high proportion of MYCN-amplified cases (P = 0.001), and this combined occurrence was associated with a particular poor outcome, suggesting a positive cooperative effect between both aberrations. Furthermore, the F1174L mutant was characterized by a higher degree of autophosphorylation and a more potent transforming capacity as compared with the R1275Q mutant. Chromosome 2p gains, including the ALK locus (91.8%), were associated with a significantly increased ALK expression, which was also correlated with poor survival.Conclusions: ALK mutations occur in equal frequencies across all genomic subtypes, but F1174L mutants are observed in a higher frequency of MYCN-amplified tumors and show increased transforming capacity as compared with the R1275Q mutants. Clin Cancer Res; 16(17); 4353–62. ©2010 AACR.

Published

2023

21. Supplementary Table 2 from Meta-analysis of Neuroblastomas Reveals a Skewed ALK Mutation Spectrum in Tumors with MYCN Amplification

Author

Frank Speleman, Rogier Versteeg, Jan Cools, Angelika Eggert, Huib Caron, Miki Ohira, Akira Nakagawara, Tommy Martinsson, Per Kogner, Isabelle Janoueix-Lerosey, Olivier Delattre, Rosa Noguera, Marleen Renard, Klaus Beiske, Nadine Van Roy, Joëlle Vermeulen, Caroline Van Den Broecke, Alexander Schramm, Johannes H. Schulte, Geneviève Laureys, Anne De Paepe, Tom Van Maerken, Jasmien Hoebeeck, Jo Vandesompele, Arjan Lakeman, Ellen M. Westerhout, Michaël Porcu, Piotr Zabrocki, Candy Kumps, Katleen De Preter, and Sara De Brouwer

Abstract

PDF file - 42K

Published

2023

22. Supplementary table 6-7 from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Supplementary Table S6. Related to Figure 4. Top 1000 varying genes based on SD across all samples derived from Patient/PDOX #5. Supplementary Table S7. Related to Figure 4. List of enriched Gene Ontology terms by cluster derived from the gene clusters defined in Suppl. Table S6.

Published

2023

23. Supplementary table 1-2 from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Supplementary Table S1. Related to Figure 1. List of all somatic mutations detected in patient tumors, and in PDOXs from low and high in vivo generations. Supplementary Table S2. Related to Figure 2. List of all chromosomal copy number changes in patient tumors, and in PDOXs from low and high in vivo generations.

Published

2023

24. Data from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Patient-derived xenografts (PDX) and the Avatar, a single PDX mirroring an individual patient, are emerging tools in preclinical cancer research. However, the consequences of intratumor heterogeneity for PDX modeling of biomarkers, target identification, and treatment decisions remain underexplored. In this study, we undertook serial passaging and comprehensive molecular analysis of neuroblastoma orthotopic PDXs, which revealed strong intrinsic genetic, transcriptional, and phenotypic stability for more than 2 years. The PDXs showed preserved neuroblastoma-associated gene signatures that correlated with poor clinical outcome in a large cohort of patients with neuroblastoma. Furthermore, we captured spatial intratumor heterogeneity using ten PDXs from a single high-risk patient tumor. We observed diverse growth rates, transcriptional, proteomic, and phosphoproteomic profiles. PDX-derived transcriptional profiles were associated with diverse clinical characteristics in patients with high-risk neuroblastoma. These data suggest that high-risk neuroblastoma contains elements of both temporal stability and spatial intratumor heterogeneity, the latter of which complicates clinical translation of personalized PDX–Avatar studies into preclinical cancer research.Significance: These findings underpin the complexity of PDX modeling as a means to advance translational applications against neuroblastoma. Cancer Res; 78(20); 5958–69. ©2018 AACR.

Published

2023

25. Supplementary Methods from Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Daniel Bexell, Sven Påhlman, David Gisselsson, Tommy Martinsson, Jan Koster, Jenny Karlsson, Rosa Noguera, Ana P. Berbegall, Javanshir Esfandyari, Siv Beckman, Anna Börjesson, Torbjörn Backman, Ingrid Øra, Karin Hansson, Jakob Willforss, Fredrik Levander, Håkan Axelson, David Lindgren, Angela Martinez-Monleon, Susanne Fransson, Kristoffer von Stedingk, and Noémie Braekeveldt

Abstract

Supplementary methods and legends to supplementary figures and tables

Published

2023

26. Supplementary Figure Legend from Appearance of the Novel Activating F1174S ALK Mutation in Neuroblastoma Correlates with Aggressive Tumor Progression and Unresponsiveness to Therapy

Author

Bengt Hallberg, Ruth H. Palmer, Kristina Ruuth, Joel Weinmar, Christina Schönherr, Sattu Kamaraj, Per Kogner, Magnus Hansson, Helena Caren, Jonas Abrahamsson, Therese Eriksson, and Tommy Martinsson

Abstract

Supplementary Figure Legend from Appearance of the Novel Activating F1174S ALK Mutation in Neuroblastoma Correlates with Aggressive Tumor Progression and Unresponsiveness to Therapy

Published

2023

27. m6A modification of TERRA RNA is required for telomere maintenance and is a therapeutic target for ALT positive Neuroblastoma

Author

Roshan Vaid, Ketan Thombare, Akram Mendez, Rebeca Burgos-Panadero, Anna Djos, Daniel Jachimowicz, Christoph Bartenhagen, Navinder Kumar, Carina Sihlbom, Susanne Fransson, John Inge Johnsen, Per Kogner, Tommy Martinsson, Matthias Fischer, and Tanmoy Mondal

Abstract

Telomerase-negative tumors can maintain telomere length by alternative lengthening of telomeres (ALT) but the mechanism behind ALT is poorly understood. Aggressive Neuroblastoma (NB), in particular, relapsed tumors are positive for ALT (ALT+) which suggests that better dissection of the ALT mechanism could provide novel therapeutic opportunities. TERRA long non-coding RNA (lncRNA) which is derived from the telomere ends is localized to telomeres in R-loop dependent manner and is essential for telomere maintenance. In the present study, we provide evidence that RNA modification at theN6position of internal adenosine (m6A) in TERRA RNA by methyltransferase METTL3 is essential for telomere maintenance in ALT+ cells and that loss of TERRA m6A/METTL3 leads to telomere damage. We observed that R-loop enriched TERRA is abundantly m6A modified and m6A mediated recruitment of hnRNPA2B1 to TERRA RNA is essential for R-loop formation. Our data suggest that m6A drives telomere targeting of TERRA via R-loop and this m6A mediated R-loop formation could be a widespread mechanism utilized by other chromatin-interacting lncRNAs. Furthermore, treating ALT+ NB cells with METTL3 inhibitor leads to compromised telomere targeting of TERRA and accumulation of DNA damage over telomere, suggesting METTL3 inhibition could be a therapeutic opportunity for ALT+ NB.

Published

2022

28. Whole-genome sequencing of recurrent neuroblastoma reveals somatic mutations that affect key players in cancer progression and telomere maintenance

Author

Gustaf Ljungman, Per Kogner, Tommy Martinsson, Angela Martinez-Monleon, Caroline Björklund, Torben Ek, Mathias Johansson, Rose-Marie Sjöberg, and Susanne Fransson

Subjects

Adult, Male, DNA Copy Number Variations, DNA repair, Somatic cell, Science, Biology, Germline, Article, Neuroblastoma, medicine, Biomarkers, Tumor, Genetics, Humans, Gene Regulatory Networks, CHEK2, Aged, Cancer, Medicinsk genetik, Whole genome sequencing, Aged, 80 and over, Cancer och onkologi, Multidisciplinary, Whole Genome Sequencing, Telomere Homeostasis, Middle Aged, Telomere, medicine.disease, Prognosis, Gene Expression Regulation, Neoplastic, Oncology, Cancer and Oncology, Mutation, Cancer research, Disease Progression, Medicine, Female, Neoplasm Recurrence, Local, Medical Genetics

Abstract

Neuroblastoma is the most common and deadly childhood tumor. Relapsed or refractory neuroblastoma has a very poor prognosis despite recent treatment advances. To investigate genomic alterations associated with relapse and therapy resistance, whole-genome sequencing was performed on diagnostic and relapsed lesions together with constitutional DNA from seven children. Sequencing of relapsed tumors indicates somatic alterations in diverse genes, including those involved in RAS-MAPK signaling, promoting cell cycle progression or function in telomere maintenance and immortalization. Among recurrent alterations, CCND1-gain, TERT-rearrangements, and point mutations in POLR2A, CDK5RAP, and MUC16 were shown in ≥ 2 individuals. Our cohort contained examples of converging genomic alterations in primary-relapse tumor pairs, indicating dependencies related to specific genetic lesions. We also detected rare genetic germline variants in DNA repair genes (e.g., BARD1, BRCA2, CHEK2, and WRN) that might cooperate with somatically acquired variants in these patients with highly aggressive recurrent neuroblastoma. Our data indicate the importance of monitoring recurrent neuroblastoma through sequential genomic characterization and that new therapeutic approaches combining the targeting of MAPK signaling, cell cycle progression, and telomere activity are required for this challenging patient group.

Published

2020

29. Sustained Response to Entrectinib in an Infant With a Germline ALKAL2 Variant and Refractory Metastatic Neuroblastoma With Chromosomal 2p Gain and Anaplastic Lymphoma Kinase and Tropomyosin Receptor Kinase Activation

Author

Diana, Treis, Ganesh, Umapathy, Susanne, Fransson, Jikui, Guan, Patricia, Mendoza-García, Joachim T, Siaw, Sandra, Wessman, Lena, Gordon Murkes, Jakob J E, Stenman, Anna, Djos, Lotta H M, Elfman, John Inge, Johnsen, Bengt, Hallberg, Ruth H, Palmer, Tommy, Martinsson, and Per, Kogner

Subjects

Male, Neuroblastoma, Germ Cells, Indazoles, Chromosomes, Human, Pair 2, Benzamides, Cytokines, Genetic Variation, Humans, Infant, Anaplastic Lymphoma Kinase, Receptor, trkA, Protein Kinase Inhibitors

Published

2022

30. PPM1D Is a Therapeutic Target in Childhood Neural Tumors

Author

Johnsen, Jelena Milosevic, Diana Treis, Susanne Fransson, Gabriel Gallo-Oller, Baldur Sveinbjörnsson, Nina Eissler, Keiji Tanino, Kazuyasu Sakaguchi, Tommy Martinsson, Malin Wickström, Per Kogner, and John Inge

Subjects

neuroblastoma, medulloblastoma, chromosome 17q gain, p53, WIP1, PPM1D, neoplasms

Abstract

Childhood medulloblastoma and high-risk neuroblastoma frequently present with segmental gain of chromosome 17q corresponding to aggressive tumors and poor patient prognosis. Located within the 17q-gained chromosomal segments is PPM1D at chromosome 17q23.2. PPM1D encodes a serine/threonine phosphatase, WIP1, that is a negative regulator of p53 activity as well as key proteins involved in cell cycle control, DNA repair and apoptosis. Here, we show that the level of PPM1D expression correlates with chromosome 17q gain in medulloblastoma and neuroblastoma cells, and both medulloblastoma and neuroblastoma cells are highly dependent on PPM1D expression for survival. Comparison of different inhibitors of WIP1 showed that SL-176 was the most potent compound inhibiting medulloblastoma and neuroblastoma growth and had similar or more potent effects on cell survival than the MDM2 inhibitor Nutlin-3 or the p53 activator RITA. SL-176 monotherapy significantly suppressed the growth of established medulloblastoma and neuroblastoma xenografts in nude mice. These results suggest that the development of clinically applicable compounds inhibiting the activity of WIP1 is of importance since PPM1D activating mutations, genetic gain or amplifications and/or overexpression of WIP1 are frequently detected in several different cancers.

Published

2021

31. PPM1D Is a Therapeutic Target in Childhood Neural Tumors

Author

Jelena Milosevic, Diana Treis, Susanne Fransson, Gabriel Gallo-Oller, Baldur Sveinbjörnsson, Nina Eissler, Keiji Tanino, Kazuyasu Sakaguchi, Tommy Martinsson, Malin Wickström, Per Kogner, and John Inge Johnsen

Subjects

chromosome 17q gain, p53, neuroblastoma, PPM1D, WIP1, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medulloblastoma, neoplasms, RC254-282, Article

Abstract

Simple Summary Medulloblastoma and neuroblastoma are childhood tumors of the central nervous system or the peripheral nervous system, respectively. These are the most common and deadly tumors of childhood. A common genetic feature of medulloblastoma and neuroblastoma is frequent segmental gain or amplification of chromosome 17q. Located on chromosome 17q23.2 is PPM1D which encodes WIP1, a phosphatase that acts as a regulator of p53 and DNA repair. Overexpression of WIP1 correlates with poor patient prognosis. We investigated the effects of genetic or pharmacologic inhibition of WIP1 activity and found that medulloblastoma and neuroblastoma cells were strongly dependent on WIP1 expression for survival. We also tested a number of small molecule inhibitors of WIP1 and show that SL-176 was the most effective compound suppressing the growth of medulloblastoma and neuroblastoma in vitro and in vivo. Abstract Childhood medulloblastoma and high-risk neuroblastoma frequently present with segmental gain of chromosome 17q corresponding to aggressive tumors and poor patient prognosis. Located within the 17q-gained chromosomal segments is PPM1D at chromosome 17q23.2. PPM1D encodes a serine/threonine phosphatase, WIP1, that is a negative regulator of p53 activity as well as key proteins involved in cell cycle control, DNA repair and apoptosis. Here, we show that the level of PPM1D expression correlates with chromosome 17q gain in medulloblastoma and neuroblastoma cells, and both medulloblastoma and neuroblastoma cells are highly dependent on PPM1D expression for survival. Comparison of different inhibitors of WIP1 showed that SL-176 was the most potent compound inhibiting medulloblastoma and neuroblastoma growth and had similar or more potent effects on cell survival than the MDM2 inhibitor Nutlin-3 or the p53 activator RITA. SL-176 monotherapy significantly suppressed the growth of established medulloblastoma and neuroblastoma xenografts in nude mice. These results suggest that the development of clinically applicable compounds inhibiting the activity of WIP1 is of importance since PPM1D activating mutations, genetic gain or amplifications and/or overexpression of WIP1 are frequently detected in several different cancers.

Published

2021

32. Single-nuclei transcriptomes from human adrenal gland reveal distinct cellular identities of low and high-risk neuroblastoma tumors

Author

Susanne Schlisio, Per Kogner, Marketa Kaucka, Igor Adameyko, Tommy Martinsson, Qiaolin Deng, Petra Bullova, Oscar C. Bedoya-Reina, Catharina Larsson, Wenyu Li, Peter V. Kharchenko, C. Christofer Juhlin, H. Pui, M. Arceo, M. Plescher, and Johan Holmberg

Subjects

Male, Chromaffin Cells, Cell, Adrenal Gland Neoplasms, General Physics and Astronomy, Transcriptome, Mice, Neuroblastoma, Adrenal Glands, Cancer genetics, education.field_of_study, Membrane Glycoproteins, Multidisciplinary, Adrenal gland, Cell Differentiation, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Child, Preschool, Female, Single-Cell Analysis, Childhood Neuroblastoma, Cell type, Science, Population, Biology, Malignancy, Risk Assessment, Article, General Biochemistry, Genetics and Molecular Biology, Paediatric cancer, Species Specificity, Biomarkers, Tumor, medicine, Animals, Humans, Receptor, trkB, education, Progenitor, Cell Nucleus, Infant, General Chemistry, medicine.disease, Survival Analysis, Embryonic stem cell, Early Diagnosis, Cancer research

Abstract

Childhood neuroblastoma has a remarkable variability in outcome. Age at diagnosis is one of the most important prognostic factors, with children less than 1 year old having favorable outcomes. Here we study single-cell and single-nuclei transcriptomes of neuroblastoma with different clinical risk groups and stages, including healthy adrenal gland. We compare tumor cell populations with embryonic mouse sympatho-adrenal derivatives, and post-natal human adrenal gland. We provide evidence that low and high-risk neuroblastoma have different cell identities, representing two disease entities. Low-risk neuroblastoma presents a transcriptome that resembles sympatho- and chromaffin cells, whereas malignant cells enriched in high-risk neuroblastoma resembles a subtype of TRKB+ cholinergic progenitor population identified in human post-natal gland. Analyses of these populations reveal different gene expression programs for worst and better survival in correlation with age at diagnosis. Our findings reveal two cellular identities and a composition of human neuroblastoma tumors reflecting clinical heterogeneity and outcome., Childhood neuroblastoma can be separated into high and low risk groups, with prognosis depending on age at diagnosis. Here, the authors show that low and high risk neuroblastoma tumours are composed of different cell types with different malignancy potential.

Published

2021

33. Amplification of CDK4 and MDM2: a detailed study of a high-risk neuroblastoma subgroup

Author

Angela Martinez-Monleon, Hanna Kryh Öberg, Jennie Gaarder, Ana P. Berbegall, Niloufar Javanmardi, Anna Djos, Marek Ussowicz, Sabine Taschner-Mandl, Inge M. Ambros, Ingrid Øra, Bengt Sandstedt, Klaus Beiske, Ruth Ladenstein, Rosa Noguera, Peter F. Ambros, Lena Gordon Murkes, Gustaf Ljungman, Per Kogner, Susanne Fransson, and Tommy Martinsson

Subjects

Cancer och onkologi, Neuroblastoma, Multidisciplinary, Cancer and Oncology, Cell- och molekylärbiologi, Gene Amplification, Cyclin-Dependent Kinase 4, Humans, Proto-Oncogene Proteins c-mdm2, Tumor Suppressor Protein p53, Prognosis, Cell and Molecular Biology

Abstract

In neuroblastoma, MYCN amplification and 11q-deletion are important, although incomplete, markers of high-risk disease. It is therefore relevant to characterize additional alterations that can function as prognostic and/or predictive markers. Using SNP-microarrays, a group of neuroblastoma patients showing amplification of one or multiple 12q loci was identified. Two loci containing CDK4 and MDM2 were commonly co-amplified, although amplification of either locus in the absence of the other was observed. Pharmacological inhibition of CDK4/6 with ribociclib or abemaciclib decreased proliferation in a broad set of neuroblastoma cell lines, including CDK4/MDM2-amplified, whereas MDM2 inhibition by Nutlin-3a was only effective in p53wild-type cells. Combined CDK4/MDM2 targeting had an additive effect in p53wild-type cell lines, while no or negative additive effect was observed in p53mutated cells. Most 12q-amplified primary tumors were of abdominal origin, including those of intrarenal origin initially suspected of being Wilms’ tumor. An atypical metastatic pattern was also observed with low degree of bone marrow involvement, favoring other sites such as the lungs. Here we present detailed biological data of an aggressive neuroblastoma subgroup hallmarked by 12q amplification and atypical clinical presentation for which our in vitro studies indicate that CDK4 and/or MDM2 inhibition also could be beneficial.

Published

2021

34. Frequency and Prognostic Impact of

Author

Angela, Bellini, Ulrike, Pötschger, Virginie, Bernard, Eve, Lapouble, Sylvain, Baulande, Peter F, Ambros, Nathalie, Auger, Klaus, Beiske, Marie, Bernkopf, David R, Betts, Jaydutt, Bhalshankar, Nick, Bown, Katleen, de Preter, Nathalie, Clément, Valérie, Combaret, Jaime, Font de Mora, Sally L, George, Irene, Jiménez, Marta, Jeison, Barbara, Marques, Tommy, Martinsson, Katia, Mazzocco, Martina, Morini, Annick, Mühlethaler-Mottet, Rosa, Noguera, Gaelle, Pierron, Maria, Rossing, Sabine, Taschner-Mandl, Nadine, Van Roy, Ales, Vicha, Louis, Chesler, Walentyna, Balwierz, Victoria, Castel, Martin, Elliott, Per, Kogner, Geneviève, Laureys, Roberto, Luksch, Josef, Malis, Maja, Popovic-Beck, Shifra, Ash, Olivier, Delattre, Dominique, Valteau-Couanet, Deborah A, Tweddle, Ruth, Ladenstein, and Gudrun, Schleiermacher

Subjects

Male, N-Myc Proto-Oncogene Protein, Gene Amplification, Infant, Prognosis, Europe, Survival Rate, Neuroblastoma, Clinical Trials, Phase III as Topic, Mutation Rate, Risk Factors, Child, Preschool, Humans, Anaplastic Lymphoma Kinase, Female, Follow-Up Studies, Randomized Controlled Trials as Topic

Abstract

In neuroblastoma (NB), the ALK receptor tyrosine kinase can be constitutively activated through activating point mutations or genomic amplification. We studiedDiagnostic tumor samples were available from 1,092 HR-NBL1/SIOPEN patients to determineGenomicGenetic alterations of

Published

2021

35. Frequency and prognostic impact of ALK amplifications and mutations in the European Neuroblastoma Study Group (SIOPEN) high-risk neuroblastoma trial (HR-NBL1)

Author

Ulrike Pötschger, Gudrun Schleiermacher, Sally L George, Nick Bown, Jaydutt Bhalshankar, Sylvain Baulande, Peter F. Ambros, Josef Malis, Gaëlle Pierron, Eve Lapouble, Katia Mazzocco, Virginie Bernard, Jaime Font de Mora, Katleen De Preter, Annick Mühlethaler-Mottet, Nadine Van Roy, Martina Morini, Genevieve Laureys, Bárbara Marques, Dominique Valteau-Couanet, Olivier Delattre, Marta Jeison, Victoria Castel, Shifra Ash, Valérie Combaret, Nathalie Auger, Ruth Ladenstein, Sabine Taschner-Mandl, Louis Chesler, Maria Rossing, David R. Betts, Ales Vicha, Rosa Noguera, Klaus Beiske, Angela Bellini, Walentyna Balwierz, Deborah A. Tweddle, Maja Popovic-Beck, Marie Bernkopf, Nathalie Clément, Per Kogner, Tommy Martinsson, Roberto Luksch, Martin Elliott, and Irene Jiménez

Subjects

0301 basic medicine, Cancer Research, Prognostic Impact, Anaplastic Lymphoma Kinase/genetics, Child, Preschool, Clinical Trials, Phase III as Topic, Europe, Female, Follow-Up Studies, Gene Amplification, Humans, Infant, Male, Mutation Rate, N-Myc Proto-Oncogene Protein/genetics, Neuroblastoma/genetics, Prognosis, Randomized Controlled Trials as Topic, Risk Factors, Survival Rate, European Neuroblastoma Study Group, SIOPEN, RELAPSE, 03 medical and health sciences, Neuroblastoma, 0302 clinical medicine, Text mining, hemic and lymphatic diseases, REVEALS, Medicine and Health Sciences, KINASE, Medicine, High risk neuroblastoma, HETEROGENEITY, CRIZOTINIB, SEGMENTAL CHROMOSOMAL ALTERATIONS, ACTIVATING MUTATIONS, PEDIATRIC-PATIENTS, business.industry, ALK receptor tyrosine kinase, Point mutation, REARRANGEMENTS, CHEMOTHERAPY, medicine.disease, Doenças Genéticas, 030104 developmental biology, ALK, Oncology, 030220 oncology & carcinogenesis, Cancer research, business

Abstract

Purpose: In neuroblastoma (NB), the ALK receptor tyrosine kinase can be constitutively activated through activating point mutations or genomic amplification. We studied ALK genetic alterations in high-risk (HR) patients on the HR-NBL1/SIOPEN trial to determine their frequency, correlation with clinical parameters, and prognostic impact. Materials and methods: Diagnostic tumor samples were available from 1,092 HR-NBL1/SIOPEN patients to determine ALK amplification status (n = 330), ALK mutational profile (n = 191), or both (n = 571). Results: Genomic ALK amplification (ALKa) was detected in 4.5% of cases (41 out of 901), all except one with MYCN amplification (MNA). ALKa was associated with a significantly poorer overall survival (OS) (5-year OS: ALKa [n = 41] 28% [95% CI, 15 to 42]; no-ALKa [n = 860] 51% [95% CI, 47 to 54], [P < .001]), particularly in cases with metastatic disease. ALK mutations (ALKm) were detected at a clonal level (> 20% mutated allele fraction) in 10% of cases (76 out of 762) and at a subclonal level (mutated allele fraction 0.1%-20%) in 3.9% of patients (30 out of 762), with a strong correlation between the presence of ALKm and MNA (P < .001). Among 571 cases with known ALKa and ALKm status, a statistically significant difference in OS was observed between cases with ALKa or clonal ALKm versus subclonal ALKm or no ALK alterations (5-year OS: ALKa [n = 19], 26% [95% CI, 10 to 47], clonal ALKm [n = 65] 33% [95% CI, 21 to 44], subclonal ALKm (n = 22) 48% [95% CI, 26 to 67], and no alteration [n = 465], 51% [95% CI, 46 to 55], respectively; P = .001). Importantly, in a multivariate model, involvement of more than one metastatic compartment (hazard ratio [HR], 2.87; P < .001), ALKa (HR, 2.38; P = .004), and clonal ALKm (HR, 1.77; P = .001) were independent predictors of poor outcome. Conclusion: Genetic alterations of ALK (clonal mutations and amplifications) in HR-NB are independent predictors of poorer survival. These data provide a rationale for integration of ALK inhibitors in upfront treatment of HR-NB with ALK alterations. Key Objective: High risk neuroblastoma (HR-NB) is one of the most difficult childhood cancers to cure. This study examined whether the presence of an ALK alteration (amplification or mutation) was associated with a poor prognosis in a large patient series treated on the prospective European high-risk neuroblastoma trial (HR-NBL1). Knowledge Generated: We found that ALK amplification or clonal mutation was associated with inferior prognosis in patients with HR-NB and both are independent prognostic variables on multivariate analysis. To our knowledge, this is the first study to report the highly prognostic significance of ALK amplification in HR-NB. Relevance: As ALK can be targeted therapeutically, this study convincingly argues for the introduction of ALK inhibitors for upfront management of patients with HR-NB with ALK aberrations. Importantly, the prognostic significance of ALK alterations included a subgroup of trial patients treated with the current standard of care for HR-NB including anti-GD2 immunotherapy. info:eu-repo/semantics/publishedVersion

Published

2021

36. The loss of DLG2 isoform 7/8, but not isoform 2, is critical in advanced staged neuroblastoma

Author

Per Kogner, Simon Keane, Tommy Martinsson, and Katarina Ejeskär

Subjects

Gene isoform, Cancer Research, Isoform, Protein family, Cell- och molekylärbiologi, Biology, L27, lcsh:RC254-282, LIN7A, 03 medical and health sciences, Neuroblastoma, 0302 clinical medicine, Gene expression, Genetics, medicine, Gene family, lcsh:QH573-671, CASK, Gene, 030304 developmental biology, 0303 health sciences, Cancer och onkologi, lcsh:Cytology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, DLG2, Cell biology, DLG, Oncology, 030220 oncology & carcinogenesis, Cancer and Oncology, DLG1, biology.protein, Primary Research, Cell and Molecular Biology

Abstract

Background Neuroblastoma is a childhood neural crest tumor showing large clinical and genetic heterogeneity, one form displaying 11q-deletion is very aggressive. It has been shown that 11q-deletion results in decreased expression of DLG2, a gene residing in the deleted region. DLG2 has a number of different isoforms with the main difference is the presence or absence of a L27 domain. The L27 domain containing DLG proteins can form complexes with CASK/MPP and LIN7 protein family members, which will control cell polarity and signaling. Methods We evaluated the DLG gene family and the LIN7 gene family for their expression in differently INSS staged neuroblastoma from publically available data and primary tumors, we included two distinct DLG1 and DLG2 N-terminal transcript isoforms encoding L27 domains for their expression. Functionality of DLG2 isoforms and of LIN7A were evaluated in the 11q-deleted neuroblastoma cell line SKNAS. Results In neuroblastoma only two DLG2 isoforms were expressed: isoform 2 and isoform 7/8. Using the array data we could determine that higher expression of DLG members that contain L27 domains correlated to better survival and prognosis. Whilst DLG1 showed a decrease in both isoforms with increased INSS stage, only the full length L27 containing DLG2 transcripts DLG2-isoform 7/8 showed a decrease in expression in high stage neuroblastoma. We could show that the protein encoded by DLG2-isoform 7 could bind to LIN7A, and increased DLG2-isoform 7 gene expression increased the expression of LIN7A, this reduced neuroblastoma cell proliferation and viability, with increased BAX/BCL2 ratio indicating increased apoptosis. Conclusion We have provided evidence that gene expression of the L27 domain containing DLG2-isoform 7/8 but not L27 domain lacking DLG2-isoform 2 is disrupted in neuroblastoma, in particular in the aggressive subsets of tumors. The presence of the complete L27 domain allows for the binding to LIN7A, which will control cell polarity and signaling, thus affecting cancer cell viability.

Published

2021

37. Malignant Schwann cell precursors mediate intratumoral plasticity in human neuroblastoma

Author

Asa Bjoerklund, Ninib Baryawno, Igor Adameyko, Ziyi Hou, Shenglin Mei, Peter V. Kharchenko, Thale Kristin Olsen, Susanne Fransson, Polina Kameneva, John Inge Johnsen, Anna Johansson, Erik Sundstroem, Per Kogner, Tommy Martinsson, Joerg Otte, and Emil Kryukov

Subjects

education.field_of_study, Mesenchymal stem cell, Population, Adrenergic, Neural crest, Schwann cell, Biology, Malignancy, medicine.disease, Transcriptome, medicine.anatomical_structure, Neuroblastoma, medicine, Cancer research, education

Abstract

Neuroblastoma is a heterogeneous embryonal malignancy and the most deadly tumor of childhood, although a minor subset may show spontaneous differentiation. It arises from the multipotent neural crest lineage during development. Some of this multipotency is retained in neuroblastoma, which can give rise to both adrenergic and mesenchymal tumor cells. The mechanisms enabling such dual fates are unknown, but likely help neuroblastoma to evade existing therapies. To understand neuroblastoma plasticity, we analyzed patient tumors using single-cell transcriptomics. In addition to the heterogeneous adrenergic and mesenchymal populations, we identify a subpopulation of malignant cells resembling Schwann cell precursors (SCPs). This SCP-like population connects the adrenergic and mesenchymal compartments through transitions structurally reminiscent of the SCP cell-fate decision fork that occurs during normal development. While the directionality of such transitions in neuroblastoma remains to be established, this finding expands the potential reservoirs of malignant cells, and suggests intratumoral plasticity mechanisms relevant for therapeutic resistance and relapse.

Published

2020

38. Familial intestinal degenerative neuropathy with chronic intestinal pseudo-obstruction linked to a gene locus with duplication in chromosome 9

Author

Hasse Abrahamsson, Hans Linander, Staffan Nilsson, Frida Ahlfors, Susanne Fransson, and Tommy Martinsson

Subjects

Intestinal pseudo-obstruction, Adult, Diarrhea, Male, Locus (genetics), Chromosome 9, Nerve Tissue Proteins, Biology, Severity of Illness Index, 03 medical and health sciences, 0302 clinical medicine, Gene Duplication, Gene duplication, medicine, Humans, Family, Gene, Genetics, Sweden, Intestinal Pseudo-Obstruction, Gastroenterology, medicine.disease, Pedigree, Intestines, Genetic Loci, 030220 oncology & carcinogenesis, Chronic Disease, Heredodegenerative Disorders, Nervous System, 030211 gastroenterology & hepatology, Female, Chromosomes, Human, Pair 9

Abstract

Background: Intestinal degenerative neuropathy without extra-intestinal involvement occurs as familial forms (FIDN) but the genetics behind is unknown. We studied a Swedish family with autosomal do...

Published

2019

39. Low Frequency ALK Hotspots Mutations In Neuroblastoma Tumours Detected By Ultra-deep Sequencing: Implications For ALK Inhibitor Treatment

Author

Susanne Fransson, Tommy Martinsson, Rose-Marie Sjöberg, Staffan Nilsson, Niloufar Javanmardi, Per Kogner, Katarina Truvé, and Anna Djos

Subjects

Adult, Male, 0301 basic medicine, Adolescent, medicine.drug_class, Mutant, lcsh:Medicine, Kaplan-Meier Estimate, Biology, Polymorphism, Single Nucleotide, Article, Fusion gene, Neuroblastoma, Young Adult, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Mutation Rate, hemic and lymphatic diseases, Biomarkers, Tumor, medicine, Humans, Anaplastic lymphoma kinase, Anaplastic Lymphoma Kinase, Molecular Targeted Therapy, lcsh:Science, Child, Protein Kinase Inhibitors, Aged, Aged, 80 and over, Sanger sequencing, Multidisciplinary, Point mutation, lcsh:R, High-Throughput Nucleotide Sequencing, Ultra deep sequencing, Exons, Middle Aged, Prognosis, medicine.disease, ALK inhibitor, 030104 developmental biology, Mutation, symbols, Cancer research, lcsh:Q, Female, 030217 neurology & neurosurgery

Abstract

The ALK tyrosine kinase receptor is oncogenically activated in neuroblastoma. Whereas numerous ALK fusion genes have been reported in different malignancies, in neuroblastoma ALK is mainly activated through point mutations. Three hotspot residues (F1174, F1245, and R1275) account for 85% of mutant ALK seen in neuroblastoma. In a cohort of 105 Swedish neuroblastoma cases of all stages, these hotspot regions were re-sequenced (>5000X). ALK mutations were detected in 16 of 105 patients (range of variant allele fraction: 2.7–60%). Mutations at the F1174 and F1245 hotspot were observed in eleven and three cases respectively. ALK mutations were also detected at the I1171 and L1240 codons in one tumor each. No mutations were detected at R1275. Sanger sequencing could confirm ALK status for all mutated samples with variant allele fraction above 15%. Four of the samples with subclonal ALK mutation fraction below this would have gone undetected relying on Sanger sequencing only. No distinct mutation spectrum in relation to neuroblastoma tumours genomic subtypes could be detected although there was a paucity of ALK mutations among 11q-deleted tumors. As ALK mutations status opens up an excellent opportunity for application of small molecule inhibitors targeting ALK, early and sensitive detection of ALK alterations is clinically important considering its potential role in tumour progression.

Published

2019

40. Analysis of ALK, MYCN, and the ALK ligand ALKAL2 (FAM150B/AUGα) in neuroblastoma patient samples with chromosome arm 2p rearrangements

Author

Ganesh Umapathy, Marcus Borenäs, Jelena Milosevic, Per Kogner, Bengt Hallberg, Tommy Martinsson, Ruth H. Palmer, Anna Djos, Susanne Fransson, Niloufar Javanmardi, and Malin Östensson

Subjects

Cancer Research, Mutation, Somatic cell, Point mutation, Context (language use), Biology, medicine.disease, medicine.disease_cause, Ligand (biochemistry), 03 medical and health sciences, 0302 clinical medicine, hemic and lymphatic diseases, 030220 oncology & carcinogenesis, Neuroblastoma, Genetics, medicine, Cancer research, Anaplastic lymphoma kinase, Receptor

Abstract

Gain of chromosome arm 2p is a previously described entity in neuroblastoma (NB). This genomic address is home to two important oncogenes in NB-MYCN and anaplastic lymphoma kinase (ALK). MYCN amplification is a critical prognostic factor coupled with poor prognosis in NB. Mutation of the ALK receptor tyrosine kinase has been described in both somatic and familial NB. Here, ALK activation occurs in the context of the full-length receptor, exemplified by activating point mutations in NB. ALK overexpression and activation, in the absence of genetic mutation has also been described in NB. In addition, the recently identified ALK ligand ALKAL2 (previously described as FAM150B and AUGα) is also found on the distal portion of 2p, at 2p25. Here we analyze 356 NB tumor samples and discuss observations indicating that gain of 2p has implications for the development of NB. Finally, we put forward the hypothesis that the effect of 2p gain may result from a combination of MYCN, ALK, and the ALK ligand ALKAL2.

Published

2019

41. The genetic tumor background is an important determinant for heterogeneous MYCN ‐amplified neuroblastoma

Author

Rosa Noguera, Clemens Brunner, Tommy Martinsson, Ruth Ladenstein, Inge M. Ambros, Andrea Ziegler, Dominik Bogen, Marek Ussowicz, Freimut H. Schilling, Gabriele Amann, Reza Abbasi, Martin Benesch, Diana Walder, and Peter F. Ambros

Subjects

Male, 0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Tumor Markers and Signatures, uniparental disomy, Adolescent, MYCN amplification, Aneuploidy, Biology, Polymorphism, Single Nucleotide, N-Myc Proto-Oncogene Protein, Benign tumor, Genetic Heterogeneity, Neuroblastoma, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Child, In Situ Hybridization, Fluorescence, Chromosome Aberrations, Oncogene Proteins, Genetic heterogeneity, Gene Amplification, Infant, Nuclear Proteins, medicine.disease, Uniparental disomy, 030104 developmental biology, Oncology, Child, Preschool, 030220 oncology & carcinogenesis, intratumoral heterogeneity, Cancer research, Female, Chromosome Deletion, Trisomy, SNP array

Abstract

Amplification of MYCN is the signature genetic aberration of 20–25% of neuroblastoma and a stratifying marker associated with aggressive tumor behavior. The detection of heterogeneous MYCN amplification (hetMNA) poses a diagnostic dilemma due to the uncertainty of its relevance to tumor behavior. Here, we aimed to shed light on the genomic background which permits hetMNA in neuroblastoma and tied the occurrence to other stratifying markers and disease outcome. We performed SNP analysis using Affymetrix Cytoscan HD arrays on 63 samples including constitutional DNA, tumor, bone marrow and relapse samples of 26 patients with confirmed hetMNA by MYCN‐FISH. Tumors of patients ≤18m were mostly aneuploid with numeric chromosomal aberrations (NCAs), presented a prominent MNA subclone and carried none or a few segmental chromosomal aberrations (SCAs). In older patients, tumors were mostly di‐ or tetraploid, contained a lower number of MNA cells and displayed a multitude of SCAs including concomitant 11q deletions. These patients often suffered disease progression, tumor dissemination and relapse. Restricted to aneuploid tumors, we detected chromosomes with uniparental di‐ or trisomy (UPD/UPT) in almost every sample. UPD11 was exclusive to tumors of younger patients whereas older patients featured UPD14. In this study, the MNA subclone appears to be constraint by the tumor environment and thus less relevant for tumor behavior in aggressive tumors with a high genomic instability and many segmental aberrations. A more benign tumor background and lower tumor stage may favor an outgrowth of the MNA clone but tumors generally responded better to treatment., What's new? MYCN amplification (MNA) in neuroblastoma (NB) generally associates with an aggressive tumor behavior and detection of MNA leads to an automatic upstaging of the tumor in non‐stage 1 tumors. But what if only a fraction of the tumor cells is MYCN‐amplified? To investigate the diagnostic importance of heterogeneous MNA, the authors conducted a genetic analysis of samples from 26 NB patients with a particular focus on accompanying genetic aberrations. They concluded that tumor behavior is largely dependent on patient age and other chromosomal alterations in the genetic tumor background rather than the mere presence of the MNA clone.

Published

2016

42. The 1p36 Tumor Suppressor KIF 1Bβ Is Required for Calcineurin Activation, Controlling Mitochondrial Fission and Apoptosis

Author

John Inge Johnsen, Olga Surova, Susanne Schlisio, Erik Smedler, Zhi Xiong Chen, Per Uhlén, Karin Wallis, Rajappa S. Kenchappa, Shuijie Li, Tommy Martinsson, Stuart M. Fell, Per Kogner, and Ulf Hellman

Subjects

0301 basic medicine, Phosphatase, Cell Biology, Biology, medicine.disease, General Biochemistry, Genetics and Molecular Biology, Cell biology, Dephosphorylation, Calcineurin, 03 medical and health sciences, 030104 developmental biology, Biochemistry, Apoptosis, Neuroblastoma, medicine, Phosphorylation, Mitochondrial fission, Signal transduction, Molecular Biology, Developmental Biology

Abstract

KIF1Bβ is a candidate 1p36 tumor suppressor that regulates apoptosis in the developing sympathetic nervous system. We found that KIF1Bβ activates the Ca(2+)-dependent phosphatase calcineurin (CN) by stabilizing the CN-calmodulin complex, relieving enzymatic autoinhibition and enabling CN substrate recognition. CN is the key mediator of cellular responses to Ca(2+) signals and its deregulation is implicated in cancer, cardiac, neurodegenerative, and immune disease. We show that KIF1Bβ affects mitochondrial dynamics through CN-dependent dephosphorylation of Dynamin-related protein 1 (DRP1), causing mitochondrial fission and apoptosis. Furthermore, KIF1Bβ actuates recognition of all known CN substrates, implying a general mechanism for KIF1Bβ in Ca(2+) signaling and how Ca(2+)-dependent signaling is executed by CN. Pathogenic KIF1Bβ mutations previously identified in neuroblastomas and pheochromocytomas all fail to activate CN or stimulate DRP1 dephosphorylation. Importantly, KIF1Bβ and DRP1 are silenced in 1p36 hemizygous-deleted neuroblastomas, indicating that deregulation of calcineurin and mitochondrial dynamics contributes to high-risk and poor-prognosis neuroblastoma.

Published

2016

43. Patient-Derived Xenograft Models Reveal Intratumor Heterogeneity and Temporal Stability in Neuroblastoma

Author

Ingrid Øra, Ana P. Berbegall, David Gisselsson, Javanshir Esfandyari, Jenny Karlsson, Fredrik Levander, Anna Börjesson, Kristoffer von Stedingk, Rosa Noguera, Karin Hansson, Angela Martinez-Monleon, Torbjörn Backman, Siv Beckman, David Lindgren, Jan Koster, Daniel Bexell, Håkan Axelson, Jakob Willforss, Sven Påhlman, Noémie Braekeveldt, Susanne Fransson, Tommy Martinsson, Oncogenomics, and CCA - Cancer biology and immunology

Subjects

0301 basic medicine, Male, Proteomics, Cancer Research, Genotype, Biology, Polymorphism, Single Nucleotide, Transcriptome, Translational Research, Biomedical, 03 medical and health sciences, Mice, Neuroblastoma, 0302 clinical medicine, Intratumor heterogeneity, medicine, Biomarkers, Tumor, Animals, Humans, In patient, Tumor xenograft, Neoplasm Staging, Gene Expression Profiling, Infant, medicine.disease, Phenotype, Gene expression profiling, Disease Models, Animal, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, Female, Neoplasm Transplantation

Abstract

Patient-derived xenografts (PDX) and the Avatar, a single PDX mirroring an individual patient, are emerging tools in preclinical cancer research. However, the consequences of intratumor heterogeneity for PDX modeling of biomarkers, target identification, and treatment decisions remain under-explored. In this study, we undertook serial passaging and comprehensive molecular analysis of neuroblastoma orthotopic PDXs, which revealed strong intrinsic genetic, transcriptional, and phenotypic stability for more than 2 years. The PDXs showed preserved neuroblastoma-associated gene signatures that correlated with poor clinical outcome in a large cohort of patients with neuroblastoma. Furthermore, we captured spatial intratumor heterogeneity using ten PDXs from a single high-risk patient tumor. We observed diverse growth rates, transcriptional, proteomic, and phosphoproteomic profiles. PDX-derived transcriptional profiles were associated with diverse clinical characteristics in patients with high-risk neuroblastoma. These data suggest that high-risk neuroblastoma contains elements of both temporal stability and spatial intratumor heterogeneity, the latter of which complicates clinical translation of personalized PDX-Avatar studies into preclinical cancer research. Significance: These findings underpin the complexity of PDX modeling as a means to advance translational applications against neuroblastoma. (C) 2018 AACR.

Published

2018

44. COX/mPGES-1/PGE 2 pathway depicts an inflammatory-dependent high-risk neuroblastoma subset

Author

Marina Korotkova, Per-Johan Jakobsson, Karin Larsson, Helena Idborg, Anna Kock, John Inge Johnsen, Per Kogner, Tommy Martinsson, and Marie Henriksson

Subjects

medicine.medical_treatment, Vimentin, Inflammation, Biology, Dinoprostone, Proinflammatory cytokine, Mice, Neuroblastoma, Fibroblast activation protein, alpha, Tumor Microenvironment, medicine, Animals, Humans, RNA, Messenger, Prostaglandin E2, Prostaglandin-E Synthases, Tumor microenvironment, Multidisciplinary, Chromosomes, Human, Pair 11, Biological Sciences, medicine.disease, Intramolecular Oxidoreductases, Disease Models, Animal, Prostaglandin-Endoperoxide Synthases, biology.protein, Cancer research, lipids (amino acids, peptides, and proteins), Chromosome Deletion, medicine.symptom, medicine.drug, Prostaglandin E

Abstract

The majority of solid tumors are presented with an inflammatory microenvironment. Proinflammatory lipid mediators including prostaglandin E2 (PGE2) contribute to the establishment of inflammation and have been linked to tumor growth and aggressiveness. Here we show that high-risk neuroblastoma with deletion of chromosome 11q represents an inflammatory subset of neuroblastomas. Analysis of enzymes involved in the production of proinflammatory lipid mediators showed that 11q-deleted neuroblastoma tumors express high levels of microsomal prostaglandin E synthase-1 (mPGES-1) and elevated levels of PGE2. High mPGES-1 expression also corresponded to poor survival of neuroblastoma patients. Investigation of the tumor microenvironment showed high infiltration of tumor-promoting macrophages with high expression of the M2-polarization markers CD163 and CD206. mPGES-1-expressing cells in tumors from different subtypes of neuroblastoma showed differential expression of one or several cancer-associated fibroblast markers such as vimentin, fibroblast activation protein α, α smooth muscle actin, and PDGF receptor β. Importantly, inhibition of PGE2 production with diclofenac, a nonselective COX inhibitor, resulted in reduced tumor growth in an in vivo model of 11q-deleted neuroblastoma. Collectively, these results suggest that PGE2 is involved in the tumor microenvironment of specific neuroblastoma subgroups and indicate that therapeutic strategies using existing anti-inflammatory drugs in combination with current treatment should be considered for certain neuroblastomas.

Published

2015

45. MEK inhibitor trametinib does not prevent the growth of anaplastic lymphoma kinase (ALK)-addicted neuroblastomas

Author

Ganesh, Umapathy, Jikui, Guan, Dan E, Gustafsson, Niloufar, Javanmardi, Diana, Cervantes-Madrid, Anna, Djos, Tommy, Martinsson, Ruth H, Palmer, and Bengt, Hallberg

Subjects

Mice, Inbred BALB C, Lung Neoplasms, Oncogene Proteins, Fusion, MAP Kinase Signaling System, Pyridones, Receptor Protein-Tyrosine Kinases, Antineoplastic Agents, Mechanistic Target of Rapamycin Complex 2, Pyrimidinones, Xenograft Model Antitumor Assays, Mice, Neuroblastoma, Cell Line, Tumor, Animals, Humans, Anaplastic Lymphoma Kinase, Female, Protein Kinase Inhibitors, Proto-Oncogene Proteins c-akt, Mitogen-Activated Protein Kinase 7

Abstract

Activation of the RAS-RAF-MEK-ERK signaling pathway is implicated in driving the initiation and progression of multiple cancers. Several inhibitors targeting the RAS-MAPK pathway are clinically approved as single- or polyagent therapies for patients with specific types of cancer. One example is the MEK inhibitor trametinib, which is included as a rational polytherapy strategy for treating EML4-ALK-positive, EGFR-activated, or KRAS-mutant lung cancers and neuroblastomas that also contain activating mutations in the RAS-MAPK pathway. In addition, in neuroblastoma, a heterogeneous disease, relapse cases display an increased rate of mutations in

Published

2017

46. Correction: A new GTF2I-BRAF fusion mediating MAPK pathway activation in pilocytic astrocytoma

Author

Katarina Truvé, Frida Abel, Sándor Dósa, Tajana Tešan Tomić, Annica Wilzén, Magnus Tisell, Tommy Martinsson, Josefin Olausson, Fredrik Enlund, Helene Sjögren, Birgitta Lannering, Pierre Åman, and Magnus Sabel

Subjects

0301 basic medicine, MAPK/ERK pathway, Multidisciplinary, Pilocytic astrocytoma, business.industry, lcsh:R, Astrocytoma, lcsh:Medicine, medicine.disease, Bioinformatics, Fusion gene, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Text mining, 030220 oncology & carcinogenesis, Complementary DNA, Medicine, lcsh:Q, business, lcsh:Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0175638.].

Published

2017

47. Rho-associated kinase is a therapeutic target in neuroblastoma

Author

Jessika Lannerholm-Palm, Per Kogner, Tommy Martinsson, Bertha Brodin, David Forsberg, John Inge Johnsen, Susanne Fransson, Eric Herlenius, Baldur Sveinbjørnsson, Thale Kristin Olsen, Cecilia Dyberg, Teodora Andonova, and Malin Wickström

Subjects

0301 basic medicine, RHOA, Mice, Nude, VDP::Medical disciplines: 700::Clinical medical disciplines: 750::Communicable diseases: 776, Biology, Mice, Neuroblastoma, 03 medical and health sciences, VDP::Medisinske Fag: 700::Klinisk medisinske fag: 750::Infeksjonsmedisin: 776, GSK-3, Cell Line, Tumor, medicine, Animals, Humans, ROCK1, Protein Kinase Inhibitors, neoplasms, N-Myc Proto-Oncogene Protein, rho-Associated Kinases, Glycogen Synthase Kinase 3 beta, Multidisciplinary, Kinase, Wnt signaling pathway, Neural crest, medicine.disease, Xenograft Model Antitumor Assays, 030104 developmental biology, PNAS Plus, biology.protein, Cancer research, N-Myc, Signal Transduction

Abstract

Source at: http://doi.org/10.1073/pnas.1706011114 Neuroblastoma is a peripheral neural system tumor that originates from the neural crest and is the most common and deadly tumor of infancy. Here we show that neuroblastoma harbors frequent mutations of genes controlling the Rac/Rho signaling cascade important for proper migration and differentiation of neural crest cells during neuritogenesis. RhoA is activated in tumors from neuroblastoma patients, and elevated expression of Rho-associated kinase (ROCK)2 is associated with poor patient survival. Pharmacological or genetic inhibition of ROCK1 and 2, key molecules in Rho signaling, resulted in neuroblastoma cell differentiation and inhibition of neuroblastoma cell growth, migration, and invasion. Molecularly, ROCK inhibition induced glycogen synthase kinase 3β-dependent phosphorylation and degradation of MYCN protein. Small-molecule inhibition of ROCK suppressed MYCN-driven neuroblastoma growth in TH-MYCN homozygous transgenic mice and MYCN gene-amplified neuroblastoma xenograft growth in nude mice. Interference with Rho/Rac signaling might offer therapeutic perspectives for high-risk neuroblastoma.

Published

2017

48. Influence of segmental chromosome abnormalities on survival in children over the age of 12 months with unresectable localised peripheral neuroblastic tumours without MYCN amplification

Author

Valérie Combaret, A. Valent, Bárbara Marques, Ales Vicha, Tommy Martinsson, N. Van Roy, Riccardo Haupt, Gian Paolo Tonini, Gudrun Schleiermacher, Alberto Garaventa, M. Jeison, Stefano Parodi, Peter F. Ambros, Claudio Gambini, Giovanni Erminio, J.A. Kohler, I.M. Ambros, Nicole Gross, John Lunec, Raffaella Defferrari, Rosa Noguera, Ana P. Berbegall, Jérôme Couturier, Clare Bedwell, Deborah A. Tweddle, Klaus Beiske, Jean Bénard, Eva Villamón, Katia Mazzocco, and Nick Bown

Subjects

Cancer Research, medicine.medical_specialty, Pathology, MYCN Amplification, Kaplan-Meier Estimate, unresectable, Gastroenterology, Disease-Free Survival, segmental chromosome alterations, Neuroblastoma, neuroblastoma, DDX1, FISH, aCGH, Older patients, Peripheral Nervous System Neoplasms, Internal medicine, MYCN, medicine, Humans, Multiplex ligation-dependent probe amplification, Gain, Chromosome Aberrations, Oncogene Proteins, Comparative Genomic Hybridization, N-Myc Proto-Oncogene Protein, business.industry, Significant difference, Gene Amplification, Segmental Chromosome abnormalities, Infant, Nuclear Proteins, Chromosome, Prognosis, localised, medicine.disease, Doenças Genéticas, MLPA, 3. Good health, Peripheral, Oncology, Mycn amplification, Clinical Study, Histopathology, business

Abstract

Background: The prognostic impact of segmental chromosome alterations (SCAs) in children older than 1 year, diagnosed with localised unresectable neuroblastoma (NB) without MYCN amplification enrolled in the European Unresectable Neuroblastoma (EUNB) protocol is still to be clarified, while, for other group of patients, the presence of SCAs is associated with poor prognosis. Methods: To understand the role of SCAs we performed multilocus/pangenomic analysis of 98 tumour samples from patients enrolled in the EUNB protocol. Results: Age at diagnosis was categorised into two groups using 18 months as the age cutoff. Significant difference in the presence of SCAs was seen in tumours of patients between 12 and 18 months and over 18 months of age at diagnosis, respectively (P = 0.04). A significant correlation (P = 0.03) was observed between number of SCAs per tumour and age. Event-free (EFS) and overall survival (OS) were calculated in both age groups, according to both the presence and number of SCAs. In older patients, a poorer survival was associated with the presence of SCAs (EFS = 46% vs 75%, P = 0.023; OS = 66.8% vs 100%, P = 0.003). Moreover, OS of older patients inversely correlated with number of SCAs (P = 0.002). Finally, SCAs provided additional prognostic information beyond histoprognosis, as their presence was associated with poorer OS in patients over 18 months with unfavourable International Neuroblastoma Pathology Classification (INPC) histopathology (P = 0.018). Conclusions: The presence of SCAs is a negative prognostic marker that impairs outcome of patients over the age of 18 months with localised unresectable NB without MYCN amplification, especially when more than one SCA is present. Moreover, in older patients with unfavourable INPC tumour histoprognosis, the presence of SCAs significantly affects OS.

Published

2014

49. Intragenic anaplastic lymphoma kinase (ALK) rearrangements: Translocations as a novel mechanism ofALKactivation in neuroblastoma tumors

Author

Rosa Noguera, Susanne Fransson, Niloufar Javanmardi, Ana P. Berbegall, Magnus Hansson, Kristina Ruuth, Ruth H. Palmer, Anna Djos, Bengt Hallberg, Per Kogner, Tommy Martinsson, and Jonas Abrahamsson

Subjects

Genetics, Cancer Research, Kinase, Gene rearrangement, Amplicon, Biology, medicine.disease, medicine.disease_cause, Lymphoma, Exon, hemic and lymphatic diseases, Neuroblastoma, medicine, Cancer research, Anaplastic lymphoma kinase, Carcinogenesis

Abstract

Anaplastic lymphoma kinase (ALK) has been demonstrated to be deregulated in sporadic as well as in familiar cases of neuroblastoma (NB). Whereas ALK-fusion proteins are common in lymphoma and lung cancer, there are few reports of ALK rearrangements in NB indicating that ALK mainly exerts its oncogenic capacity via activating mutations and/or overexpression in this tumor type. In this study, 332 NB tumors and 13 cell lines were screened by high resolution single nucleotide polymorphism microarray. Gain of 2p was detected in 23% (60/332) of primary tumors and 46% (6/13) of cell lines, while breakpoints at the ALK locus were detected in four primary tumors and two cell lines. These were further analyzed by next generation sequencing and a targeted enrichment approach. Samples with both ALK and MYCN amplification displayed complex genomic rearrangements with multiple breakpoints within the amplicon. None of the translocations characterized in primary NB tumors are likely to result in a chimeric protein. However, immunohistochemical analysis reveals high levels of phosphorylated ALK in these samples despite lack of initial exons, possibly due to alternative transcription initiation sites. Both ALK proteins predicted to arise from such alterations and from the abnormal ALK exon 4-11 deletion observed in the CLB-BAR cell line show strong activation of downstream targets STAT3 and extracellular signal-regulated kinase (ERK) when expressed in PC12 cells. Taken together, our data indicate a novel, although rare, mechanism of ALK activation with implications for NB tumorigenesis.

Published

2014

50. Neuroblastoma after Childhood: Prognostic Relevance of Segmental Chromosome Aberrations, ATRX Protein Status, and Immune Cell Infiltration

Author

Samuel Navarro, Rosa Noguera, Adela Cañete, Victoria Castel, Ana P. Berbegall, Irene Tadeo, Eva Villamón, and Tommy Martinsson

Subjects

Male, Cancer Research, Het, heterogeneous, Gene Expression, Neuroblastoma, Immunophenotyping, Registries, Young adult, Neoplasm Metastasis, MLPA, multiplex ligation probe amplification, Child, In Situ Hybridization, Fluorescence, Nuclear Proteins, Middle Aged, AYA, adolescent and young adults, Prognosis, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, NCA, numerical chromosome aberration, Immunohistochemistry, Female, SCA, segmental chromosome aberration, IHC, immunohistochemistry, NB, neuroblastoma, Adult, X-linked Nuclear Protein, Adolescent, aSNP, single nucleotide polymorphism array, Biology, Malignancy, Chromosome aberration, Polymorphism, Single Nucleotide, lcsh:RC254-282, Article, Young Adult, Lymphocytes, Tumor-Infiltrating, cnLOH, copy-neutral loss of heterozygosity, medicine, Humans, Hom, homogeneous, ATRX, Neoplasm Staging, Chromosome Aberrations, DNA Helicases, medicine.disease, Spain, MNNA, MYCN not amplified, Cancer research, FSCA, focal segmental chromosome aberration, CD8, MNA, MYCN amplified

Abstract

Neuroblastoma (NB) is a common malignancy in children but rarely occurs during adolescence or adulthood. This subgroup is characterized by an indolent disease course, almost uniformly fatal, yet little is known about the biologic characteristics. The aim of this study was to identify differential features regarding DNA copy number alterations, α-thalassemia/mental retardation syndrome X-linked (ATRX) protein expression, and the presence of tumor-associated inflammatory cells. Thirty-one NB patients older than 10 years who were included in the Spanish NB Registry were considered for the current study; seven young and middle-aged adult patients (range 18-60 years) formed part of the cohort. We performed single nucleotide polymorphism arrays, immunohistochemistry for immune markers (CD4, CD8, CD20, CD11b, CD11c, and CD68), and ATRX protein expression. Assorted genetic profiles were found with a predominant presence of a segmental chromosome aberration (SCA) profile. Preadolescent and adolescent NB tumors showed a higher number of SCA, including 17q gain and 11q deletion. There was also a marked infiltration of immune cells, mainly high and heterogeneous, in young and middle-aged adult tumors. ATRX negative expression was present in the tumors. The characteristics of preadolescent, adolescent, young adult, and middle-aged adult NB tumors are different, not only from childhood NB tumors but also from each other. Similar examinations of a larger number of such tumor tissues from cooperative groups should lead to a better older age–dependent tumor pattern and to innovative, individual risk-adapted therapeutic approaches for these patients.

Published

2014