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14 results on '"Jonkers, Y. M. H."'

2. Targeted therapy for Ewing's sarcoma: significance of heterogeneity

Author

Addy van de Luijtgaarden, Graaf, W. T. A., Otte-Höller, I., Schreuder, H. W. B., Versleijen-Jonkers, Y. M. H., and Slootweg, P. J.

Subjects
Translational research [ONCOL 3], Quality of Care [ONCOL 4]
Abstract

Item does not contain fulltext BACKGROUND: Survival in Ewing's sarcoma (ES) is limited. Experience with insulin-like growth factor targeting drugs, which require specific molecular tumour alterations, herald a major breakthrough. We screened for tumour heterogeneity within patients by DNA quantification. MATERIALS AND METHODS: DNA image cytometry (IC) was performed on 41 samples from 21 patients, evaluating if ploidy state remained constant over time and between different lesions within patients and the prognostic value of ploidy was assessed. RESULTS: DNA content varied over time and different ploidy states were found to coexist at a single timepoint. Non-diploid DNA content was associated with shorter overall survival (median, 19 vs. 84 months, p=0.047). CONCLUSION: We encountered a change and heterogeneity of ploidy state. This implies that screening for targets on a single tumour sample is insufficient and may lead to under- or overtreatment. The fact that non-diploid DNA content was associated with an adverse outcome confirms that this technique discriminates biologically different tumour clones. 01 september 2010

Published
2010

3. DNA copy number status is a powerful predictor of poor survival in endocrine pancreatic tumor patients

Author

Jonkers, Y. M. H., Claessen, S. M. H., Perren, A., Schmitt, A. M., Hofland, L. J., de Herder, W., de Krijger, R. R., Verhofstad, A. A. J., Hermus, A .R., Kummer, J .A., Skogseid, Britt M., Volante, M., Voogd, A. C., Ramaekers, F. C. S., Speel, E. J. M., Jonkers, Y. M. H., Claessen, S. M. H., Perren, A., Schmitt, A. M., Hofland, L. J., de Herder, W., de Krijger, R. R., Verhofstad, A. A. J., Hermus, A .R., Kummer, J .A., Skogseid, Britt M., Volante, M., Voogd, A. C., Ramaekers, F. C. S., and Speel, E. J. M.

Abstract

The clinical behavior of endocrine pancreatic tumors (EPTs) is difficult to predict in the absence of metastases or invasion to adjacent organs. Several markers have been indicated as potential predictors of metastatic disease, such as tumor size 2 cm, Ki67 proliferative index 2%, cytokeratin (CK) 19 status, and recently in insulinomas, chromosomal instability (CIN). The goal of this study was to evaluate the value of these markers, and in particular of the CIN, to predict tumor recurrence or progression and tumor-specific death, using a series of 47 insulinomas and 24 non-insulinoma EPTs. From these EPT cases, a genomic profile has been generated and follow-up data have been obtained. The proliferative index has been determined in 68 tumors and a CK19 expression pattern in 50 tumors. Results are statistically analyzed using Kaplan–Meier plots and the log-rank statistic. General CIN, as well as specific chromosomal alterations such as 3p and 6q loss and 12q gain, turned out to be the most powerful indicators for poor tumor-free survival (P0.0004) and tumor-specific death (P0.0113) in insulinomas. The CIN, chromosome 7q gain, and a proliferative index 2% were reliable in predicting a poor tumor-free survival in non-insulinoma EPTs (P0.0181, whereas CK19 expression was the most optimal predictor of tumor-specific death in these tumors. In conclusion, DNA copy number status is the most sensitive and efficient marker of adverse clinical outcome in insulinomas and of potential interest in non-insulinoma EPTs. As a consequence, this marker should be considered as a prognosticator to improve clinical d

Published
2007
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4. Molecular parameters associated with insulinoma progression : chromosomal instability versus p53 and CK19 status

Author

Jonkers, Y. M. H., Claessen, S. M. H., Veltman, J. A., Geurts van Kessel, A., Dinjens, W. N. M., Skogseid, Britt, Ramaekers, F. C. S., Speel, E-J. M., Jonkers, Y. M. H., Claessen, S. M. H., Veltman, J. A., Geurts van Kessel, A., Dinjens, W. N. M., Skogseid, Britt, Ramaekers, F. C. S., and Speel, E-J. M.

Abstract

Insulinomas represent the predominant syndromic subtype of endocrine pancreatic tumors (EPTs). Their metastatic potential cannot be predicted reliably using histopathological criteria. In the past few years, several attempts have been made to identify prognostic markers, among them TP53 mutations and immunostaining of p53 and recently cytokeratin 19 (CK19). In a previous study using conventional comparative genomic hybridization (CGH) we have shown that chromosomal instability (CIN) is associated with metastatic disease in insulinomas. It was our aim to evaluate these potential parameters in a single study. For the determination of CIN, we applied CGH to microarrays because it allows a high-resolution detection of DNA copy number changes in comparison with conventional CGH as well as the analysis of chromosomal regions close to the centromeres and telomeres, and at 1pter -> p32, 16p, 19 and 22. These regions are usually excluded from conventional CGH analysis, because they may show DNA gains in negative control hybridizations. Array CGH analysis of 30 insulinomas (15 tumors of benign, eight tumors of uncertain and seven tumors of malignant behavior) revealed that >= 20 chromosomal alterations and >= 6 telomeric losses were the best predictors of malignant progression. A subset of 22 insulinomas was further investigated for TP53 exon 5-8 gene mutations, and p53 and CK19 expression. Only one malignant tumor was shown to harbor an arginine 273 serine mutation and immunopositivity for p53. CK19 immunopositivity was detected in three malignant tumors and one tumor with uncertain behavior. In conclusion, our results indicate that CIN as well as telomeric loss are very powerful indicators for malignant progression in sporadic insulinomas. Our data do not support a critical role for p53 and CK19 as molecular parameters for this purpose.

Published
2006
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6. DNA copy number status is a powerful predictor of poor survival in endocrine pancreatic tumor patients

Author

Jonkers, Y M H, primary, Claessen, S M H, additional, Perren, A, additional, Schmitt, A M, additional, Hofland, L J, additional, de Herder, W, additional, de Krijger, R R, additional, Verhofstad, A A J, additional, Hermus, A R, additional, Kummer, J A, additional, Skogseid, B, additional, Volante, M, additional, Voogd, A C, additional, Ramaekers, F C S, additional, and Speel, E J M, additional

Published
2007
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9. Targeting angiosarcomas of the soft tissues: A challenging effort in a heterogeneous and rare disease.

Author

Weidema ME, Versleijen-Jonkers YMH, Flucke UE, Desar IME, and van der Graaf WTA

Subjects
Female, Humans, Male, Rare Diseases, Hemangiosarcoma pathology, Hemangiosarcoma therapy, Soft Tissue Neoplasms pathology, Soft Tissue Neoplasms therapy
Abstract

Angiosarcomas are rare malignant tumors with a heterogeneous clinical presentation and generally poor prognosis. It has been difficult to establish consistent molecular characteristics and driver events in angiosarcoma development. Oncogenic and angiogenesis-related pathways have been investigated pre-clinically and clinically with varying results. A few promising responses to checkpoint inhibitors have been described, but immunological features require further elucidation. With this review we present an overview of the critical biological pathways and processes affected in angiosarcoma, and their potential role in novel, non-cytotoxic, systemic treatments., (Copyright © 2019 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2019
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10. High prevalence of late adverse events in malignant bone tumour survivors diagnosed at adult age.

Author

van de Luijtgaarden AC, Kapusta L, Bellersen L, Bokkerink JP, Kaal SE, Versleijen-Jonkers YM, Schreuder HW, and van der Graaf WT

Subjects
Academic Medical Centers, Adolescent, Adult, Bone Neoplasms therapy, Cardiomyopathies epidemiology, Disease-Free Survival, Doxorubicin adverse effects, Female, Humans, Male, Middle Aged, Musculoskeletal Diseases epidemiology, Netherlands epidemiology, Osteosarcoma therapy, Prevalence, Sarcoma, Ewing therapy, Survivors, Young Adult, Antineoplastic Agents adverse effects, Bone Neoplasms complications, Cardiomyopathies etiology, Musculoskeletal Diseases etiology, Osteosarcoma complications, Sarcoma, Ewing complications
Abstract

Background: Late treatment-related adverse events are particularly prevalent in survivors of childhood bone cancer because of the combination of cytotoxic drugs, major surgery and radiotherapy. Existing studies for late toxicity in survivors of Ewing's sarcoma (ES) and osteosarcoma (OS) diagnosed at adult age have focused on specific sequelae. We investigated a broad spectrum of potential late effects in these patients., Methods: Relapse-free OS and ES patients aged ≥ 16 at diagnosis and treated at the Radboud University Medical Centre (1982-2007) were invited for systematic late toxicity screening. This included history taking, physical examination, echocardiogram, bone densitometry, audiogram, and serum and urine screening for renal toxicity and infertility. Adverse events were graded according to the Common Terminology Criteria for Adverse Events version 3.0., Results: In 24 survivors (63% male, mean age at screening 45.7 years, mean follow-up 10.9 years, 70% OS) we found a median of eight adverse events. Frequent findings included abnormal gait, osteoporosis, pain, left ventricular systolic dysfunction, obesity and nephropathy. The maximum grade of any adverse event was mild in four (17%), moderate in 11 (46%), severe in six (25%), and disabling in three cases (13%). There was a trend towards more events in patients diagnosed at an older age., Conclusion: The incidence of late adverse events in this study of survivors of bone tumours diagnosed at adult age is higher than in any previously published childhood cancer survivorship study. Older patients seem to be particularly at risk. Our findings underscore the need for systematic screening of late effects in bone cancer survivors of adult age at diagnosis.

Published
2014

11. Targeted therapy for Ewing's sarcoma: significance of heterogeneity.

Author

Van De Luijtgaarden AC, Van Der Graaf WT, Otte-Höller I, Schreuder HW, Versleijen-Jonkers YM, and Slootweg PJ

Subjects
Bone Neoplasms mortality, Drug Delivery Systems, Humans, Image Cytometry, Kaplan-Meier Estimate, Prognosis, Sarcoma, Ewing mortality, Bone Neoplasms genetics, DNA, Neoplasm genetics, Ploidies, Sarcoma, Ewing genetics
Abstract

Background: Survival in Ewing's sarcoma (ES) is limited. Experience with insulin-like growth factor targeting drugs, which require specific molecular tumour alterations, herald a major breakthrough. We screened for tumour heterogeneity within patients by DNA quantification., Materials and Methods: DNA image cytometry (IC) was performed on 41 samples from 21 patients, evaluating if ploidy state remained constant over time and between different lesions within patients and the prognostic value of ploidy was assessed., Results: DNA content varied over time and different ploidy states were found to coexist at a single timepoint. Non-diploid DNA content was associated with shorter overall survival (median, 19 vs. 84 months, p=0.047)., Conclusion: We encountered a change and heterogeneity of ploidy state. This implies that screening for targets on a single tumour sample is insufficient and may lead to under- or overtreatment. The fact that non-diploid DNA content was associated with an adverse outcome confirms that this technique discriminates biologically different tumour clones.

Published
2010

12. Molecular alterations during insulinoma tumorigenesis.

Author

Jonkers YM, Ramaekers FC, and Speel EJ

Subjects
Genetic Markers, Humans, Insulinoma pathology, Insulinoma surgery, Neoplasm Invasiveness, Neoplasm Metastasis genetics, Neoplasm Metastasis pathology, Pancreatic Neoplasms pathology, Pancreatic Neoplasms surgery, Signal Transduction physiology, Insulinoma genetics, Pancreatic Neoplasms genetics
Abstract

Insulinomas are the most common functioning endocrine pancreatic tumors (EPTs). They present with clinical symptoms as a consequence of hypoglycemia induced by inappropriate insulin secretion. The etiology of these tumors is poorly understood. Some tumors may harbor MEN1 gene mutations, the susceptibility gene of the multiple endocrine neoplasia type I syndrome, but most cases show wildtype MEN1. Currently, no reliable clinical tests are available to differentiate benign from malignant tumors. Approximately 30% of the tumors are unresectable, and they often show different growth rates, which hampers treatment. Therefore, a better understanding of the molecular processes underlying the development and progression of insulinomas is required to improve diagnosis, prognosis and therapy. Here we summarize the progress that has been made in insulinoma research in the past decade. We describe the clinical detection, classification and treatment of these tumors, and review the multiplicity of molecular and genetic studies that investigated tumor development and progression using either primary tumors, transgenic mouse models or tumor-derived cell lines. The identification of many interactors of the MEN1 gene product menin, as well as recurrent chromosomal abnormalities that pinpoint candidate genes of interest will likely result in a better understanding of the molecular pathways involved in insulinoma tumorigenesis. In addition, these studies will pave the way for the identification of novel targets for therapeutical intervention and more reliable markers for clinical diagnosis and prognosis.

Published
2007
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13. Novel candidate tumour suppressor gene loci on chromosomes 11q23-24 and 22q13 involved in human insulinoma tumourigenesis.

Author

Jonkers YM, Claessen SM, Feuth T, van Kessel AG, Ramaekers FC, Veltman JA, and Speel EJ

Subjects
Chromosomal Instability genetics, Chromosome Deletion, Chromosomes, Human, Pair 4 genetics, Chromosomes, Human, Pair 9 genetics, DNA, Neoplasm genetics, Female, Humans, In Situ Hybridization, Fluorescence methods, Male, Middle Aged, Ploidies, Chromosome Aberrations, Chromosomes, Human, Pair 11 genetics, Chromosomes, Human, Pair 22 genetics, Genes, Tumor Suppressor, Insulinoma genetics, Pancreatic Neoplasms genetics
Abstract

Insulinomas represent the predominant syndromic subtype of endocrine pancreatic tumours. Previous molecular studies have shown that gain of chromosome 9q rather than MEN1 gene mutation is an important early event in tumour development and that chromosomal instability is associated with metastatic disease. In order to identify new gene loci and to define further the critical genetic events in insulinoma tumourigenesis, 27 insulinomas were investigated by array-based comparative genomic hybridization (array CGH) on 3.7 k genomic BAC arrays (resolution < or =1 Mb). Fluorescence in situ hybridization was used to validate alterations in a subset of tumours. Array CGH most frequently detected loss of chromosomes 11q and 22q and gains of chromosome 9q. The chromosomal regions of interest (CRI) included 11q24.1 (56%), 22q13.1 (67%), 22q13.31 (56%), and 9q32 (63%). Evaluation of the simultaneous occurrence of these aberrations in the individual tumours revealed that gain of 9q32 and loss of 22q13.1 are early genetic events in insulinomas, occurring independently of the other alterations. In tumours with increased genomic complexity, these alterations were often detected simultaneously, occurring in the same tumour cells. Losses of 11q24.1 and 22q13.31 were also associated with these more advanced tumour cases. The CRIs identified most likely harbour crucial candidate genes important in insulinoma tumourigenesis.

Published
2006
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14. Chromosomal instability predicts metastatic disease in patients with insulinomas.

Author

Jonkers YM, Claessen SM, Perren A, Schmid S, Komminoth P, Verhofstad AA, Hofland LJ, de Krijger RR, Slootweg PJ, Ramaekers FC, and Speel EJ

Subjects
Adult, Diagnosis, Differential, Female, Humans, Insulinoma genetics, Insulinoma pathology, Male, Middle Aged, Mutation, Neoplasm Metastasis, Nucleic Acid Hybridization, Pancreatic Neoplasms genetics, Pancreatic Neoplasms pathology, Prognosis, Chromosomal Instability genetics, Insulinoma diagnosis, Pancreatic Neoplasms diagnosis, Proto-Oncogene Proteins genetics
Abstract

Endocrine pancreatic tumors (EPTs) comprise a highly heterogeneous group of tumors with different clinical behavior and genetic makeup. Insulinomas represent the predominant syndromic subtype of EPTs. The metastatic potential of insulinomas can frequently not be predicted using histopathological criteria, and also molecular markers indicating malignant progression are unreliable because of the small number of cases per subtype studied so far. For the identification of reliable indicators of metastatic disease, we investigated 62 sporadic insulinomas (44 benign and 18 tumors with metastases) by means of comparative genomic hybridization (CGH). In addition, the role of MEN1 (multiple endocrine neoplasia type 1) gene mutations was determined to assess specific chromosomal alterations associated with dysfunction of this endocrine tumor-related tumor suppressor gene. Only one case with a somatic MEN1 mutation was identified (1527del7bp), indicating that the MEN1 gene plays a minor pathogenic role in sporadic insulinomas. CGH analysis revealed that the total number of aberrations per tumor differs strongly between the benign and the malignant group (4.2 vs 14.1; P<0.0001). Furthermore, chromosome 9q gain was found to be the most frequent aberration in both benign and malignant insulinomas, whereas chromosome 6q losses and 12q, 14q and 17pq gains are strongly associated with metastatic disease. Our study shows that chromosomal instability, as defined by > or =5 gains together with > or =5 losses, or total number of gains and losses > or =8, rather than parameters such as tumor size and proliferation index, is the most powerful indicator for the development of metastatic disease in patients with sporadic insulinoma.

Published
2005
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