Your search keyword '"Wezel, T. (Tom) van"' showing total 19 results

1. Multicenter Comparison of Molecular Tumor Boards in The Netherlands: Definition, Composition, Methods, and Targeted Therapy Recommendations

Author

Koopman, B. (Bart), Groen, H.J.M. (Henk), Ligtenberg, M.J. (Marjolijn), Grünberg, K. (Katrien), Monkhorst, K. (Kim), de Langen, A.J. (Adrianus J.), Boelens, M.C. (Mirjam C.), Paats, M.S. (Marthe), Thusen, J.H. (Jan) von der, Dinjens, W.N.M. (Winand), Solleveld, N. (Nienke), Wezel, T. (Tom) van, Gelderblom, H. (Hans), Hendriks, L.E. (Lizza E.), Speel, E.J. (Ernst-Jan), Theunissen, T.E. (Tom E.), Kroeze, L.I. (Leonie I.), Mehra, N. (Niven), Piet, B. (Berber), van der Wekken, A.J. (Anthonie J.), ter Elst, A. (Arja), Timens, W. (Wim), Willems, S.M. (Stefan Martin), Meijers, R.W.J. (Ruud), Leng, W.W.J. (Wendy) de, van Lindert, A.S.R. (Anne S.R.), Radonic, T. (Teodora), Hashemi, S.M.S. (Sayed M.S.), Heideman, D.A.M. (Danielle), Schuuring, E. (Ed), Kempen, L.C. (Leon), Koopman, B. (Bart), Groen, H.J.M. (Henk), Ligtenberg, M.J. (Marjolijn), Grünberg, K. (Katrien), Monkhorst, K. (Kim), de Langen, A.J. (Adrianus J.), Boelens, M.C. (Mirjam C.), Paats, M.S. (Marthe), Thusen, J.H. (Jan) von der, Dinjens, W.N.M. (Winand), Solleveld, N. (Nienke), Wezel, T. (Tom) van, Gelderblom, H. (Hans), Hendriks, L.E. (Lizza E.), Speel, E.J. (Ernst-Jan), Theunissen, T.E. (Tom E.), Kroeze, L.I. (Leonie I.), Mehra, N. (Niven), Piet, B. (Berber), van der Wekken, A.J. (Anthonie J.), ter Elst, A. (Arja), Timens, W. (Wim), Willems, S.M. (Stefan Martin), Meijers, R.W.J. (Ruud), Leng, W.W.J. (Wendy) de, van Lindert, A.S.R. (Anne S.R.), Radonic, T. (Teodora), Hashemi, S.M.S. (Sayed M.S.), Heideman, D.A.M. (Danielle), Schuuring, E. (Ed), and Kempen, L.C. (Leon)

Abstract

Background: Molecular tumor boards (MTBs) provide rational, genomics-driven, patient-tailored treatment recommendations. Worldwide, MTBs differ in terms of scope, composition, methods, and recommendations. This study aimed to assess differences in methods and agreement in treatment recommendations among MTBs from tertiary cancer referral centers in The Netherlands. Materials and Methods: MTBs from all tertiary cancer referral centers in The Netherlands were invited to participate. A survey assessing scope, value, logistics, composition, decision-making method, reporting, and registration of the MTBs was completed through on-site interviews with members from each MTB. Targeted therapy recommendations were compared using 10 anonymized cases. Participating MTBs were asked to provide a treatment recommendation in accordance with their own methods. Agreement was based on which molecular alteration(s) was considered actionable with the next line of targeted therapy. Results: Interviews with 24 members of eight MTBs revealed that all participating MTBs focused on rare or complex mutational cancer profiles, operated independently of cancer type–specific multidisciplinary teams, and consisted of at least (thoracic and/or medical) oncologists, pathologists, and clinical scientists in molecular pathology. Differences were the types of cancer discussed and the methods used to achieve a recommendation. Nevertheless, agreement among MTB recommendations, based on identified actionable molecular alteration(s), was high for the 10 evaluated cases (86%). Conclusion: MTBs associated with tertiary cancer referral centers in The Netherlands are similar in setup and reach a high agreement in recommendations for rare or complex mutational cancer profiles. We propose a “Dutch MTB model” for an optimal, collaborative, and nationally aligned MTB workflow. Implications for Practice: Interpretation of genomic analyses for optimal choice of target therapy for patients with cancer is becoming in

Published

2020

2. The RECAP Test Rapidly and Reliably Identifies Homologous Recombination-Deficient Ovarian Carcinomas

Author

Wijk, L.M. (Leen) van, Vermeulen, S., Meijers, M. (Matty), van Diest, M.F., ter Haar, N.T., de Jonge, M.M., Solleveld-Westerink, N., Wezel, T. (Tom) van, Gent, D.C. (Dik) van, Kroep, J. R., Bosse, T., Gaarenstroom, K.N. (Katja), Vrieling, H. (Harry), Vreeswijk, M.P. (Maaike), Wijk, L.M. (Leen) van, Vermeulen, S., Meijers, M. (Matty), van Diest, M.F., ter Haar, N.T., de Jonge, M.M., Solleveld-Westerink, N., Wezel, T. (Tom) van, Gent, D.C. (Dik) van, Kroep, J. R., Bosse, T., Gaarenstroom, K.N. (Katja), Vrieling, H. (Harry), and Vreeswijk, M.P. (Maaike)

Abstract

Recent studies have shown that the efficacy of PARP inhibitors in epithelial ovarian carcinoma (EOC) is related to tumor-specific defects in homologous recombination (HR) and extends beyond BRCA1/2 deficient EOC. A robust method with which to identify HR-deficient (HRD) carcinomas is therefore of utmost clinical importance. In this study, we investigated the proficiency of a functional HR assay based on the detection of RAD51 foci, the REcombination CAPacity (RECAP) test, in identifying HRD tumors in a cohort of prospectively collected epithelial ovarian carcinomas (EOCs). Of the 39 high-grade serous ovarian carcinomas (HGSOC), the RECAP test detected 26% (10/39) to be HRD, whereas ovarian carcinomas of other histologic subtypes (n = 10) were all HR-proficient (HRP). Of the HRD tumors that could be sequenced, 8/9 showed pathogenic BRCA1/2 variants or BRCA1 promoter hypermethylation, indicating that the RECAP test reliably identifies HRD, including but not limited to tumors related to BRCA1/2 deficiency. Furthermore, we found a trend towards better overall survival (OS) of HGSOC patients with RECAP-identified HRD tumors compared to patients with HRP tumors. This study shows that the RECAP test is an attractive alternative to DNA-based HRD tests, and further development of a clinical grade RECAP test is clearly warranted.

Published

2020

3. Cribriform architecture in radical prostatectomies predicts oncological outcome in Gleason score 8 prostate cancer patients

Author

Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Rietbergen, J.B. (John), Osanto, S. (Susanne), Pelger, R.C.M. (R. C M), Wezel, T. (Tom) van, Poel, H.G. (Henk) van der, Bekers, E.M. (Elise), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), Leenders, G.J.H.L. (Geert), Hollemans, E. (Eva), Verhoef, E.I. (Esther), Bangma, C.H. (Chris), Rietbergen, J.B. (John), Osanto, S. (Susanne), Pelger, R.C.M. (R. C M), Wezel, T. (Tom) van, Poel, H.G. (Henk) van der, Bekers, E.M. (Elise), Helleman, J. (Jozien), Roobol-Bouts, M.J. (Monique), and Leenders, G.J.H.L. (Geert)

Abstract

The Gleason score is an important parameter for clinical outcome in prostate cancer patients. Gleason score 8 is a heterogeneous disease including Gleason score 3 + 5, 4 + 4, and 5 + 3 tumors, and encompasses a broad range of tumor growth patterns. Our objective was to characterize individual growth patterns and identify prognostic parameters in Gleason score 8 prostate cancer patients. We reviewed 1064 radical prostatectomy specimens, recorded individual Gleason 4 and 5 growth patterns as well as presence of intraductal carcinoma, and evaluated biochemical recurrence- and metastasis-free survival. Gleason score 8 disease was identified in 140 (13%) patients, of whom 76 (54%) had Gleason score 3 + 5, 46 (33%) 4 + 4, and 18 (13%) 5 + 3 disease. Invasive cribriform and/or intraductal carcinoma (n = 87, 62%) was observed more frequently in Gleason score 4 + 4 (93%) than 3 + 5 (47%; P < 0.001) and 5 + 3 (44%; P < 0.001) patients. Gleason pattern 5 was present in 110 (79%) men: as single cells and/or cords in 99 (90%) and solid fields in 32 (29%) cases. Solid field pattern 5 coexisted with cribriform architecture (23/32, 72%) more frequently than nonsolid pattern 5 cases (36/78, 46%, P = 0.02). In multivariable analysis including age, prostate-specific antigen, pT-stage, surgical margin status, and lymph node metastases, presence of cribriform architecture was an independent parameter for biochemical recurrence-free (hazard ratio (HR) 2.0, 95% confidence interval (CI) 1.0–3.7; P = 0.04) and metastasis-free (HR 3.5, 95% CI 1.0–12.3; P = 0.05) survival. In conclusion, invasive cribriform and/or intraductal carcinoma occurs more frequently in Gleason score 4 + 4 prostate cancer patients than in Gleason score 3 + 5 and 5 + 3, and is an independent parameter for biochemical recurrence and metastasis. Therefore, cribriform architecture has added value in risk stratification of Gleason score 8 prostate cancer patients.

Published

2020

4. Comprehensive diagnostics of acute myeloid leukemia by whole transcriptome RNA sequencing

Author

Arindrarto, W. (Wibowo), Borràs, D.M. (Daniel M.), de Groen, R.A.L. (Ruben A. L.), van den Berg, R.R. (Redmar R.), Locher, I.J. (Irene J.), van Diessen, S.A.M.E. (Saskia A. M. E.), van der Holst, R. (Rosalie), van der Meijden, E.D. (Edith D.), Honders, M.W. (M. Willy), de Leeuw, R.H. (Rick H.), Verlaat, W. (Wina), Jedema, I. (I.), Kroes, W.G.M. (Wilma G. M.), Knijnenburg, J. (Jeroen), Wezel, T. (Tom) van, Vermaat, J.S. (Joost), Valk, P.J.M. (Peter), Janssen, B. (Bart), Knijff, P. (Peter) de, van Bergen, C.A.M. (Cornelis A. M.), Akker, E.B. (Erik) van den, Hoen, P.A.C.T. (Peter A. C. t), Kielbasa, S.M. (Szymon M.), Laros, J.F.J. (Jeroen F.), Griffioen, M., Veelken, H., Arindrarto, W. (Wibowo), Borràs, D.M. (Daniel M.), de Groen, R.A.L. (Ruben A. L.), van den Berg, R.R. (Redmar R.), Locher, I.J. (Irene J.), van Diessen, S.A.M.E. (Saskia A. M. E.), van der Holst, R. (Rosalie), van der Meijden, E.D. (Edith D.), Honders, M.W. (M. Willy), de Leeuw, R.H. (Rick H.), Verlaat, W. (Wina), Jedema, I. (I.), Kroes, W.G.M. (Wilma G. M.), Knijnenburg, J. (Jeroen), Wezel, T. (Tom) van, Vermaat, J.S. (Joost), Valk, P.J.M. (Peter), Janssen, B. (Bart), Knijff, P. (Peter) de, van Bergen, C.A.M. (Cornelis A. M.), Akker, E.B. (Erik) van den, Hoen, P.A.C.T. (Peter A. C. t), Kielbasa, S.M. (Szymon M.), Laros, J.F.J. (Jeroen F.), Griffioen, M., and Veelken, H.

Abstract

Acute myeloid leukemia (AML) is caused by genetic aberrations that also govern the prognosis of patients and guide risk-adapted and targeted therapy. Genetic aberrations in AML are structurally diverse and currently detected by different diagnostic assays. This study sought to establish whole transcriptome RNA sequencing as single, comprehensive, and flexible platform for AML diagnostics. We developed HAMLET (Human AML Expedited Transcriptomics) as bioinformatics pipeline for simultaneous detection of fusion genes, small variants, tandem duplications, and gene expression with all information assembled in an annotated, user-friendly output file. Whole transcriptome RNA sequencing was performed on 100 AML cases and HAMLET results were validated by reference assays and targeted resequencing. The data showed that HAMLET accurately detected all fusion genes and overexpression of EVI1 irrespective of 3q26 aberrations. In addition, small variants in 13 genes that are often mutated in AML were called with 99.2% sensitivity and 100% specificity, and tandem duplications in FLT3 and KMT2A were detected by a novel algorithm based on soft-clipped reads with 100% sensitivity and 97.1% specificity. In conclusion, HAMLET has the potential to provide accurate comprehensive diagnostic information relevant for AML classification, risk assessment and targeted therapy on a single technology platform.

Published

2020

5. Apparent Lack of BRAFV600E Derived HLA Class I Presented Neoantigens Hampers Neoplastic Cell Targeting by CD8+ T Cells in Langerhans Cell Histiocytosis

Author

Kemps, P.G. (Paul G.), Zondag, T.C.E. (Timo C. E.), Steenwijk, E.C. (Eline C.), Andriessen, Q. (Quirine), Borst, J. (Jelske), Vloemans, S. (Sandra), Roelen, D.L. (Dave), Voortman, L.M. (Lenard M.), Verdijk, R.M. (Robert), Noesel, C.J.M. (Carel), Cleven, A.H.G. (Arjen H G), Hawkins, C. (Cynthia), Lang, V. (Veronica), Ru, A. (Arnoud) de, Janssen, G.M.C. (George), Haasnoot, G.W. (Geert), Franken, K. (Kees), Eijk, R. (Ronald) van, Solleveld-Westerink, N. (Nienke), Wezel, T. (Tom) van, Egeler, R.M. (Maarten), Beishuizen, A. (Auke), Laar, J.A.M. (Jan) van, Abla, O. (Oussama), Bos, C. (Cor) van den, Veelen, P. (Peter) van, Halteren, A.G.S. (Astrid) van, Kemps, P.G. (Paul G.), Zondag, T.C.E. (Timo C. E.), Steenwijk, E.C. (Eline C.), Andriessen, Q. (Quirine), Borst, J. (Jelske), Vloemans, S. (Sandra), Roelen, D.L. (Dave), Voortman, L.M. (Lenard M.), Verdijk, R.M. (Robert), Noesel, C.J.M. (Carel), Cleven, A.H.G. (Arjen H G), Hawkins, C. (Cynthia), Lang, V. (Veronica), Ru, A. (Arnoud) de, Janssen, G.M.C. (George), Haasnoot, G.W. (Geert), Franken, K. (Kees), Eijk, R. (Ronald) van, Solleveld-Westerink, N. (Nienke), Wezel, T. (Tom) van, Egeler, R.M. (Maarten), Beishuizen, A. (Auke), Laar, J.A.M. (Jan) van, Abla, O. (Oussama), Bos, C. (Cor) van den, Veelen, P. (Peter) van, and Halteren, A.G.S. (Astrid) van

Abstract

Langerhans Cell Histiocytosis (LCH) is a neoplastic disorder of hematopoietic origin characterized by inflammatory lesions containing clonal histiocytes (LCH-cells) intermixed with various immune cells, including T cells. In 50-60% of LCH-patients, the somatic BRAFV600E driver mutation, which is common in many cancers, is detected in these LCH-cells in an otherwise quiet genomic landscape. Non-synonymous mutations like BRAFV600E can be a source of neoantigens capable of eliciting effective antitumor CD8+ T cell responses. This requires neopeptides to be stably presented by Human Leukocyte Antigen (HLA) class I molecules and sufficient numbers of CD8+ T cells at tumor sites. Here, we demonstrate substantial heterogeneity in CD8+ T cell density in n = 101 LCH-lesions, with BRAFV600E mutated lesions displaying significantly lower CD8+ T cell:CD1a+ LCH-cell ratios (p = 0.01) than BRAF wildtype lesions. Because LCH-lesional CD8+ T cell density had no significant impact on event-free survival, we investigated whether the intracellularly expressed BRAFV600E protein is degraded into neopeptides that are naturally processed and presented by cell surface HLA class I molecules. Epitope prediction tools revealed a single HLA class I binding BRAFV600E derived neopeptide (KIGDFGLATEK), which indeed displayed strong to intermediate binding capacity to HLA-A*03:01 and HLA-A*11:01 in an in vitro peptide-HLA binding assay. Mass spectrometry-based targeted peptidomics was used to investigate the presence of this neopeptide in HLA class I presented peptides isolated from several BRAFV600E expressing cell lines with various HLA genotypes. While the HLA-A*02:01 binding BRAF wildtype peptide KIGDFGLATV was traced in peptides isolated from al

Published

2019

6. Recommendations for the clinical interpretation and reporting of copy number gains using gene panel NGS analysis in routine diagnostics

Author

Eijkelenboom, A. (Anneke), Tops, BBJ, Berg, A. (Andrea) von, Brule, A.J.C. van den, Dinjens, W.N.M. (Winand), Dubbink, H.J. (Erik Jan), van der Elst, A, Geurts-Giele, W.R.R., Groenen, P., Groenendijk, F.H. (Floris), Heideman, D.A.M. (Danielle), Huibers, M.M.H., Huijsmans, C. J. J., Jeuken, J.W.M., Kempen, L.C. (Leon), Korpershoek, E. (Esther), Kroeze, L.I., Leng, W.W.J. (Wendy) de, van Noesel, C.J.M., Speel, E.J. (Ernst-Jan), Vogel, M.J. (Maartje), Wezel, T. (Tom) van, Nederlof, P.M. (Petra), Schuuring, E. (Ed), Ligtenberg, M.J. (Marjolijn), Eijkelenboom, A. (Anneke), Tops, BBJ, Berg, A. (Andrea) von, Brule, A.J.C. van den, Dinjens, W.N.M. (Winand), Dubbink, H.J. (Erik Jan), van der Elst, A, Geurts-Giele, W.R.R., Groenen, P., Groenendijk, F.H. (Floris), Heideman, D.A.M. (Danielle), Huibers, M.M.H., Huijsmans, C. J. J., Jeuken, J.W.M., Kempen, L.C. (Leon), Korpershoek, E. (Esther), Kroeze, L.I., Leng, W.W.J. (Wendy) de, van Noesel, C.J.M., Speel, E.J. (Ernst-Jan), Vogel, M.J. (Maartje), Wezel, T. (Tom) van, Nederlof, P.M. (Petra), Schuuring, E. (Ed), and Ligtenberg, M.J. (Marjolijn)

Abstract

Next-generation sequencing (NGS) panel analysis on DNA from formalin-fixed paraffin-embedded (FFPE) tissue is increasingly used to also identify actionable copy number gains (gene amplifications) in addition to sequence variants. While guidelines for the reporting of sequence variants are available, guidance with respect to reporting copy number gains from gene-panel NGS data is limited. Here, we report on Dutch consensus recommendations obtained in the context of the national Predictive Analysis for THerapy (PATH) project, which aims to optimize and harmonize routine diagnostics in molecular pathology. We briefly di

Published

2019

7. Validation and Implementation of BRCA1/2 Variant Screening in Ovarian Tumor Tissue

Author

de Jonge, M.M. (Marthe M.), Ruano, D. (Dina), Eijk, R. (Ronald) van, van der Stoep, N. (Nienke), Nielsen, M. (Maartje), Wijnen, J.T. (Juul), ter Haar, N.T. (Natalja T.), Baalbergen, A. (Astrid), Bos, M.E.M.M. (Monique E.M.M.), Kagie, M.J. (Marjolein ), Vreeswijk, M.P. (Maaike), Gaarenstroom, K.N. (Katja), Kroep, J.R. (Judith), Smit, V.T.H.B.M. (Vincent), Bosse, T. (Tjalling), Wezel, T. (Tom) van, van Asperen, C.J. (Christi J.), de Jonge, M.M. (Marthe M.), Ruano, D. (Dina), Eijk, R. (Ronald) van, van der Stoep, N. (Nienke), Nielsen, M. (Maartje), Wijnen, J.T. (Juul), ter Haar, N.T. (Natalja T.), Baalbergen, A. (Astrid), Bos, M.E.M.M. (Monique E.M.M.), Kagie, M.J. (Marjolein ), Vreeswijk, M.P. (Maaike), Gaarenstroom, K.N. (Katja), Kroep, J.R. (Judith), Smit, V.T.H.B.M. (Vincent), Bosse, T. (Tjalling), Wezel, T. (Tom) van, and van Asperen, C.J. (Christi J.)

Abstract

BRCA1/2 variant analysis in tumor tissue could streamline the referral of patients with epithelial ovarian, fallopian tube, or primary peritoneal cancer to genetic counselors and select patients who benefit most from targeted treatment. We investigated the sensitivity of BRCA1/2 variant analysis in formalin-fixed, paraffin-embedded tumor tissue using a combination of next-generation sequencing and copy number variant multiplex ligation-dependent probe amplification. After optimization using a training cohort of known BRCA1/2 mutation carriers, validation was performed in a prospective cohort in which screening of BRCA1/2 tumor DNA and leukocyte germline DNA was performed in parallel. BRCA1 promoter hypermethylation and pedigree analysis were also performed. In the training cohort, 45 of 46 germline BRCA1/2 variants were detected (sensitivity, 98%). In the prospective cohort (n = 62), all six germline variants were identified (sensitivity, 100%), together with five somatic BRCA1/2 variants and eight cases with BRCA1 promoter hypermethylation. In four BRCA1/2 variant–negative patients, surveillance or prophylactic management options were offered on the basis of positive family histories. We conclude that BRCA1/2 formalin-fixed, paraffin-embedded tumor tissue analysis reliably detects BRCA1/2 variants. When taking family history of BRCA1/2 variant–negative patients into account, tumor BRCA1/2 variant screening allows more efficient selection of epithelial ovarian cancer patients for genetic counseling and simultaneously selects patients who benefit most from targeted treatment.

Published

2018

8. SNP association study in PMS2-associated Lynch syndrome

Author

Ten Broeke, S.W. (Sanne W.), Elsayed, F.A. (Fadwa A.), Pagan, L. (Lisa), Olderode-Berends, M. (Maran), Garcia, E.B.G., Gille, H.J.P. (Hans), Hest, L.P. (Liselotte) van, Letteboer, T.G.W. (Tom), Kolk, L.E. (Lizet) van der, Mensenkamp, A.R. (Arjen R.), Os, T.A.M. (Theo) van, Spruijt, L. (Liesbeth), Redeker, B. (Bert), Suerink, M. (Manon), Vos, Y.J. (Yvonne), Wagner, A. (Anja), Wijnen, J.T. (Juul), Steyerberg, E.W. (Ewout), Tops, C. (Carli), Wezel, T. (Tom) van, Nielsen, M. (Maartje), Ten Broeke, S.W. (Sanne W.), Elsayed, F.A. (Fadwa A.), Pagan, L. (Lisa), Olderode-Berends, M. (Maran), Garcia, E.B.G., Gille, H.J.P. (Hans), Hest, L.P. (Liselotte) van, Letteboer, T.G.W. (Tom), Kolk, L.E. (Lizet) van der, Mensenkamp, A.R. (Arjen R.), Os, T.A.M. (Theo) van, Spruijt, L. (Liesbeth), Redeker, B. (Bert), Suerink, M. (Manon), Vos, Y.J. (Yvonne), Wagner, A. (Anja), Wijnen, J.T. (Juul), Steyerberg, E.W. (Ewout), Tops, C. (Carli), Wezel, T. (Tom) van, and Nielsen, M. (Maartje)

Abstract

Lynch syndrome (LS) patients are at high risk of developing colorectal cancer (CRC). Phenotypic variability might in part be explained by common susceptibility loci identified in Genome Wide Association Studies (GWAS). Previous studies focused mostly on MLH1, MSH2 and MSH6 carriers, with conflicting results. We aimed to determine the role of GWAS SNPs in PMS2 mutation carriers. A cohort study was performed in 507 PMS2 carriers (124 CRC cases), genotyped for 24 GWAS SNPs, including SNPs at 11q23.1 and 8q23.3. Hazard ratios (HRs) were calculated using a weighted Cox regression analysis to correct for ascertainment bias. Discrimination was assessed with a concordance statistic in a bootstrap cross-validation procedure. Individual SNPs only had non-significant associations with CRC occurrence with HRs lower than 2, although male carriers of allele A at rs1321311 (6p21.31) may have increased risk of CRC (HR = 2.1, 95% CI 1.2–3.0). A polygenic risk score (PRS) based on 24 HRs had an HR of 2.6 (95% CI 1.5–4.6) for the highest compared to the lowest quartile, but had no discriminative ability (c statistic 0.52). Previously suggested SNPs do not modify CRC risk in PMS2 carriers. Future large studies are needed for improved risk stratification among Lynch syndrome patients.

Published

2017

9. Colorectal cancer risk variants at 8q23.3 and 11q23.1 are associated with disease phenotype in APC mutation carriers

Author

Ghorbanoghli, Z., Nieuwenhuis, M.H. (Mary), Houwing-Duistermaat, J.J. (Jeanine), Jagmohan-Changur, S.C. (Shantie), Hes, F.J. (Frederik), Tops, C. (Carli), Wagner, A. (Anja), Aalfs, C.M. (Cora), Verhoef, S., Gómez García, E.B. (Encarna), Sijmons, R.H. (Rolf), Menko, F. (Fred), Letteboer, T.G.W. (Tom), Hoogerbrugge, N. (Nicoline), Wezel, T. (Tom) van, Vasen, H. (Hans), Wijnen, J.T. (Juul), Ghorbanoghli, Z., Nieuwenhuis, M.H. (Mary), Houwing-Duistermaat, J.J. (Jeanine), Jagmohan-Changur, S.C. (Shantie), Hes, F.J. (Frederik), Tops, C. (Carli), Wagner, A. (Anja), Aalfs, C.M. (Cora), Verhoef, S., Gómez García, E.B. (Encarna), Sijmons, R.H. (Rolf), Menko, F. (Fred), Letteboer, T.G.W. (Tom), Hoogerbrugge, N. (Nicoline), Wezel, T. (Tom) van, Vasen, H. (Hans), and Wijnen, J.T. (Juul)

Published

2016

10. Combined mismatch repair and POLE/POLD1 defects explain unresolved suspected Lynch syndrome cancers

Author

Jansen, A.M. (Anne Ml), Wezel, T. (Tom) van, Van Den Akker, B.E. (Brendy Ewm), Ventayol Garcia, M. (Marina), Ruano, D. (Dina), Tops, C. (Carli), Wagner, A. (Anja), Letteboer, T.G.W. (Tom), Gómez García, E.B. (Encarna), Devilee, P. (Peter), Wijnen, J.T. (Juul), Hes, F.J. (Frederik), Morreau, H. (Hans), Jansen, A.M. (Anne Ml), Wezel, T. (Tom) van, Van Den Akker, B.E. (Brendy Ewm), Ventayol Garcia, M. (Marina), Ruano, D. (Dina), Tops, C. (Carli), Wagner, A. (Anja), Letteboer, T.G.W. (Tom), Gómez García, E.B. (Encarna), Devilee, P. (Peter), Wijnen, J.T. (Juul), Hes, F.J. (Frederik), and Morreau, H. (Hans)

Abstract

Many suspected Lynch Syndrome (sLS) patients who lack mismatch repair (MMR) germline gene variants and MLH1 or MSH2 hypermethylation are currently explained by somatic MMR gene variants or, occasionally, by germline POLE variants. To further investigate unexplained sLS patients, we analyzed leukocyte and tumor DNA of 62 sLS patients using gene panel sequencing including the POLE, POLD1 and MMR genes. Forty tumors showed either one, two or more somatic MMR variants predicted to affect function. Nine sLS tumors showed a likely ultramutated phenotype and were found to carry germline (n=2) or somatic variants (n=7) in the POLE/POLD1 exonuclease domain (EDM). Six of these POLE/POLD1-EDM mutated tumors also carried somatic MMR variants. Our findings suggest that faulty proofreading may result in loss of MMR and thereby in microsatellite instability.

Published

2016

11. Whole Gene Capture Analysis of 15 CRC Susceptibility Genes in Suspected Lynch Syndrome Patients

Author

Jansen, A.M.L. (Anne M. L.), Geilenkirchen, M.A. (Marije A.), Wezel, T. (Tom) van, Jagmohan-Changur, S.C. (Shantie), Ruano, D. (Dina), Klift, H.M. (Heleen) van der, Van Den Akker, B.E.W.M. (Brendy E. W. M.), Laros, J.F.J. (Jeroen F.), Van Galen, M. (Michiel), Wagner, A. (Anja), Letteboer, T.G.W. (Tom), Gómez García, E.B. (Encarna), Tops, C. (Carli), Vasen, H. (Hans), Devilee, P. (Peter), Hes, F.J. (Frederik), Morreau, H. (Hans), Wijnen, J.T. (Juul), Jansen, A.M.L. (Anne M. L.), Geilenkirchen, M.A. (Marije A.), Wezel, T. (Tom) van, Jagmohan-Changur, S.C. (Shantie), Ruano, D. (Dina), Klift, H.M. (Heleen) van der, Van Den Akker, B.E.W.M. (Brendy E. W. M.), Laros, J.F.J. (Jeroen F.), Van Galen, M. (Michiel), Wagner, A. (Anja), Letteboer, T.G.W. (Tom), Gómez García, E.B. (Encarna), Tops, C. (Carli), Vasen, H. (Hans), Devilee, P. (Peter), Hes, F.J. (Frederik), Morreau, H. (Hans), and Wijnen, J.T. (Juul)

Abstract

Background and Aims Lynch Syndrome (LS) is caused by pathogenic germline variants in one of the mismatch repair (MMR) genes. However, up to 60% of MMR-deficient colorectal cancer cases are categorized as suspected Lynch Syndrome (sLS) because no pathogenic MMR germline variant can be identified, which leads to difficulties in clinical management. We therefore analyzed the genomic regions of 15 CRC susceptibility genes in leukocyte DNA of 34 unrelated sLS patients and 11 patients with MLH1 hypermethylated tumors with a clear family history. Methods Using targeted next-generation sequencing, we analyzed the entire non-repetitive genomic sequence, including intronic and regulatory sequences, of 15 CRC susceptibility genes. In addition, tumor DNA from 28 sLS patients was analyzed for somatic MMR variants. Results Of 1979 germline variants found in the leukocyte DNA of 34 sLS patients, one was a pathogenic variant (MLH1 c.1667+1delG). Leukocyte DNA of 11 patients with MLH1 hypermethylated tumors was negative for pathogenic germline variants in the tested CRC susceptibility genes and for germline MLH1 hypermethylation. Somatic DNA analysis of 28 sLS tumors identified eight (29%) cases with two pathogenic somatic variants, one with a VUS predicted to pathogenic and LOH, and nine cases (32%) with one pathogenic somatic variant (n = 8) or one VUS predicted to be pathogenic (n = 1). Conclusions This is the first study in sLS patients to include the entire genomic sequence of CRC susceptibility genes. An underlying somatic or germline MMR gene defect was identified in ten of 34 sLS patients (29%). In the remaining sLS patients, the underlying genetic defect explaining the MMRdeficiency in their tumors might be found outside the genomic regions harboring the MMR and other known CRC susceptibility genes.

Published

2016

12. Correspondence: SEMA4A variation and risk of colorectal cancer

Author

Kinnersley, B. (Ben), Chubb, D. (Daniel), Dobbins, S.E. (Sara E.), Frampton, M. (Matthew), Buch, T. (Thorsten), Timofeeva, M.N. (Maria N.), Castellví-Bel, S., Farrington, S.M. (Susan), Försti, A. (Asta), Hampe, J. (Jochen), Hemminki, K. (Kari), Hofstra, R.M.W. (Robert), Northwood, J.B. (John Blackman), Palles, C. (Claire), Pinheiro, M. (Manuela), Ruiz-Ponte, C. (Clara), Schafmayer, C. (Clemens), Teixeira, M.R. (Manuel R.), Westers, H. (Helga), Wezel, T. (Tom) van, Bishop, D.T. (David Timothy), Tomlinson, I. (Ian), Dunlop, M. (Malcolm), Houlston, R. (Richard), Kinnersley, B. (Ben), Chubb, D. (Daniel), Dobbins, S.E. (Sara E.), Frampton, M. (Matthew), Buch, T. (Thorsten), Timofeeva, M.N. (Maria N.), Castellví-Bel, S., Farrington, S.M. (Susan), Försti, A. (Asta), Hampe, J. (Jochen), Hemminki, K. (Kari), Hofstra, R.M.W. (Robert), Northwood, J.B. (John Blackman), Palles, C. (Claire), Pinheiro, M. (Manuela), Ruiz-Ponte, C. (Clara), Schafmayer, C. (Clemens), Teixeira, M.R. (Manuel R.), Westers, H. (Helga), Wezel, T. (Tom) van, Bishop, D.T. (David Timothy), Tomlinson, I. (Ian), Dunlop, M. (Malcolm), and Houlston, R. (Richard)

Published

2016

13. Recurrent Coding Sequence Variation Explains only A Small Fraction of the Genetic Architecture of Colorectal Cancer

Author

Timofeeva, M.N. (Maria N.), Kinnersley, B. (Ben), Farrington, S.M. (Susan M.), Whiffin, N. (Nicola), Palles, C. (Claire), Svinti, V. (Victoria), Lloyd, A. (Amy), Gorman, M. (Maggie), Ooi, L.-Y. (Li-Yin), Hosking, F. (Fay), Barclay, E. (Ella), Zgaga, L. (Lina), Dobbins, S.E. (Sara E.), Martin, L. (Lynn), Theodoratou, E. (Evropi), Broderick, P. (Peter), Tenesa, A. (Albert), Smillie, C. (Claire), Grimes, G. (Graeme), Hayward, C. (Caroline), Campbell, A. (Archie), Porteous, D. (David), Deary, I.J. (Ian), Harris, S.E. (Sarah), Northwood, J.B. (John Blackman), Barrett, J.H. (Jennifer H.), Smith, G. (Gillian), Wolf, R. (Roland), Forman, D. (David), Morreau, H. (Hans), Ruano, D. (Dina), Tops, C. (Carli), Wijnen, J.T. (Juul), Schrumpf, M. (Melanie), Boot, A. (Arnoud), Vasen, H. (Hans), Hes, F.J. (Frederik), Wezel, T. (Tom) van, Franke, A. (Andre), Lieb, W. (Wolgang), Schafmayer, C. (Clemens), Hampe, J. (Jochen), Buch, T. (Thorsten), Propping, P. (Peter), Hemminki, K. (Kari), Försti, A. (Asta), Westers, H. (Helga), Hofstra, R.M.W. (Robert), Pinheiro, M. (Manuela), Pinto, C. (Carla), Teixeira, P.J., Ruiz-Ponte, C. (Clara), Fernández-Rozadilla, C. (Ceres), Carracedo, A. (Angel), Castells, A., Castellví-Bel, S., Campbell, H. (Harry), Bishop, D.T. (David Timothy), Tomlinson, I. (Ian), Dunlop, M.G. (Malcolm), Houlston, R. (Richard), Timofeeva, M.N. (Maria N.), Kinnersley, B. (Ben), Farrington, S.M. (Susan M.), Whiffin, N. (Nicola), Palles, C. (Claire), Svinti, V. (Victoria), Lloyd, A. (Amy), Gorman, M. (Maggie), Ooi, L.-Y. (Li-Yin), Hosking, F. (Fay), Barclay, E. (Ella), Zgaga, L. (Lina), Dobbins, S.E. (Sara E.), Martin, L. (Lynn), Theodoratou, E. (Evropi), Broderick, P. (Peter), Tenesa, A. (Albert), Smillie, C. (Claire), Grimes, G. (Graeme), Hayward, C. (Caroline), Campbell, A. (Archie), Porteous, D. (David), Deary, I.J. (Ian), Harris, S.E. (Sarah), Northwood, J.B. (John Blackman), Barrett, J.H. (Jennifer H.), Smith, G. (Gillian), Wolf, R. (Roland), Forman, D. (David), Morreau, H. (Hans), Ruano, D. (Dina), Tops, C. (Carli), Wijnen, J.T. (Juul), Schrumpf, M. (Melanie), Boot, A. (Arnoud), Vasen, H. (Hans), Hes, F.J. (Frederik), Wezel, T. (Tom) van, Franke, A. (Andre), Lieb, W. (Wolgang), Schafmayer, C. (Clemens), Hampe, J. (Jochen), Buch, T. (Thorsten), Propping, P. (Peter), Hemminki, K. (Kari), Försti, A. (Asta), Westers, H. (Helga), Hofstra, R.M.W. (Robert), Pinheiro, M. (Manuela), Pinto, C. (Carla), Teixeira, P.J., Ruiz-Ponte, C. (Clara), Fernández-Rozadilla, C. (Ceres), Carracedo, A. (Angel), Castells, A., Castellví-Bel, S., Campbell, H. (Harry), Bishop, D.T. (David Timothy), Tomlinson, I. (Ian), Dunlop, M.G. (Malcolm), and Houlston, R. (Richard)

Abstract

Whilst common genetic variation in many non-coding genomic regulatory regions are known to impart risk of colorectal cancer (CRC), much of the heritability of CRC remains unexplained. To examine the role of recurrent coding sequence variation in CRC aetiology, we genotyped 12,638 CRCs cases and 29,045 controls from six European populations. Single-variant analysis identified a coding variant (rs3184504) in SH2B3 (12q24) associated with CRC risk (OR = 1.08, P = 3.9 × 10-7), and novel damaging coding variants in 3 genes previously tagged by GWAS efforts; rs16888728 (8q24) in UTP23 (OR = 1.15, P = 1.4 × 10-7); rs6580742 and rs12303082 (12q13) in FAM186A (OR = 1.11, P = 1.2 × 10-7

Published

2015

14. Colorectal cancer risk variants on 11q23 and 15q13 are associated with unexplained adenomatous polyposis

Author

Hes, F.J. (Frederik), Ruano, D. (Dina), Nieuwenhuis, M.H. (Mary), Tops, C. (Carli), Schrumpf, M. (Melanie), Nielsen, M. (Maartje), Huijts, P. (Petra), Wijnen, J.T. (Juul), Wagner, A. (Anja), Gómez García, E.B. (Encarna), Sijmons, R.H. (Rolf), Menko, F. (Fred), Letteboer, T.G.W. (Tom), Hoogerbrugge, N. (Nicoline), Harryvan, J. (Jan), Kampman, E. (Ellen), Morreau, H. (Hans), Vasen, H. (Hans), Wezel, T. (Tom) van, Hes, F.J. (Frederik), Ruano, D. (Dina), Nieuwenhuis, M.H. (Mary), Tops, C. (Carli), Schrumpf, M. (Melanie), Nielsen, M. (Maartje), Huijts, P. (Petra), Wijnen, J.T. (Juul), Wagner, A. (Anja), Gómez García, E.B. (Encarna), Sijmons, R.H. (Rolf), Menko, F. (Fred), Letteboer, T.G.W. (Tom), Hoogerbrugge, N. (Nicoline), Harryvan, J. (Jan), Kampman, E. (Ellen), Morreau, H. (Hans), Vasen, H. (Hans), and Wezel, T. (Tom) van

Abstract

Background: Colorectal adenomatous polyposis is associated with a high risk of colorectal cancer (CRC) and is frequently caused by germline mutations in APC or MUTYH. However, in about 20-30% of patients no underlying gene defect can be identified. In this study, we tested if recently identified CRC risk variants play a role in patients with >10 adenomas. Methods We analysed a total of 16 SNPs with a reported association with CR

Published

2014

15. Re: Role of the oxidative DNA damage repair gene OGG1 in colorectal tumorigenesis

Author

Kinnersley, B. (Ben), Buch, T. (Thorsten), Castellví-Bel, S., Farrington, S.M. (Susan), Försti, A. (Asta), Hampe, J. (Jochen), Hemminki, K. (Kari), Hofstra, R.M.W. (Robert), Northwood, J.B. (John Blackman), Palles, C. (Claire), Pinheiro, M.A. (Magda Avelar), Ruiz-Ponte, C. (Clara), Schafmayer, C. (Clemens), Teixeira, P.J., Westers, H. (Helga), Wezel, T. (Tom) van, Bishop, D.T. (David Timothy), Tomlinson, I.P. (Ian), Dunlop, M.G. (Malcolm), Houlston, R. (Richard), Kinnersley, B. (Ben), Buch, T. (Thorsten), Castellví-Bel, S., Farrington, S.M. (Susan), Försti, A. (Asta), Hampe, J. (Jochen), Hemminki, K. (Kari), Hofstra, R.M.W. (Robert), Northwood, J.B. (John Blackman), Palles, C. (Claire), Pinheiro, M.A. (Magda Avelar), Ruiz-Ponte, C. (Clara), Schafmayer, C. (Clemens), Teixeira, P.J., Westers, H. (Helga), Wezel, T. (Tom) van, Bishop, D.T. (David Timothy), Tomlinson, I.P. (Ian), Dunlop, M.G. (Malcolm), and Houlston, R. (Richard)

Published

2014

16. BRAF mutation-specific promoter methylation of FOX genes in colorectal cancer

Author

Roon, E.H.J. (Eddy) van, Boot, A. (Arnoud), Dihal, A.A. (Ashwin), Ernst, R.F. (Robert), Wezel, T. (Tom) van, Morreau, H. (Hans), Boer, J.M. (Judith), Roon, E.H.J. (Eddy) van, Boot, A. (Arnoud), Dihal, A.A. (Ashwin), Ernst, R.F. (Robert), Wezel, T. (Tom) van, Morreau, H. (Hans), and Boer, J.M. (Judith)

Abstract

Background: Cancer-specific hypermethylation of (promoter) CpG islands is common during the tumorigenesis of colon cancer. Although associations between certain genetic aberrations, such as BRAF mutation and microsatellite instability, and the CpG island methylator phenotype (CIMP), have been found, the mechanisms by which these associations are established are still unclear. We studied genome-wide DNA methylation differences between c

Published

2013

17. The homeobox gene MEIS1 is methylated in BRAFp.V600E mutated colon tumors

Author

Dihal, A.A. (Ashwin), Boot, A. (Arnoud), Roon, E.H.J. (Eddy) van, Schrumpf, M. (Melanie), Fariña-Sarasqueta, A. (Arantza), Fiocco, M. (Marta), Zeestraten, E.C.M. (Eliane), Kuppen, P.J.K. (Peter), Morreau, H. (Hans), Wezel, T. (Tom) van, Boer, J.M. (Judith), Dihal, A.A. (Ashwin), Boot, A. (Arnoud), Roon, E.H.J. (Eddy) van, Schrumpf, M. (Melanie), Fariña-Sarasqueta, A. (Arantza), Fiocco, M. (Marta), Zeestraten, E.C.M. (Eliane), Kuppen, P.J.K. (Peter), Morreau, H. (Hans), Wezel, T. (Tom) van, and Boer, J.M. (Judith)

Abstract

Development of colorectal cancer (CRC) can occur both via gene mutations in tumor suppressor genes and oncogenes, as well as via epigenetic changes, including DNA methylation. Site-specific methylation in CRC regulates expression of tumor-associated genes. Right-sided colon tumors more frequently have BRAFp.V600E mutations and have higher methylation grades when compared to left-sided malignancies. The aim of this study was to identify DNA methylation changes associated with BRAFp.V600E mutation status. We performed methylation profiling of colon tumor DNA, isolated from frozen sections enriched for epithelial cells by macro-dissection, and from paired healthy tissue. Single gene analyses comparing BRAFp.V600E with BRAF wild type revealed MEIS1 as the most significant differentially methylated gene (log2 fold change: 0.89, false discovery rate-adjusted P-value 2.8*10-9). This finding was validated by methylation-specific PCR that was concordant with the microarray data. Additionally, validation in an independent cohort (n=228) showed a significant association between BRAF p.V600E and MEIS1 methylation (OR: 13.0, 95% CI: 5.2 - 33.0, P<0.0001). MEIS1 methylation was associated with decreased MEIS1 gene expression in both patient samples and CRC cell lines. The same was true for gene expression of a truncated form of MEIS1, MEIS1D27, which misses exon 8 and has a proposed tumor suppression function. To trace the origin of MEIS1 promoter methylation, 14 colorectal tumors were flow-sorted. Four out of eight BRAFp.V600E tumor epithelial fractions (50%) showed MEIS1 promoter methylation, as well as three out of eight BRAFp.V600E stromal fractions (38%). Only one out of six BRAF wild type showed MEIS1 promoter methylation in both the epithelial tumor and stromal fractions (17%). In conclusion, BRAFp.V600E colon tumors showed significant MEIS1 promoter methylation, which was associated with decreased MEIS1 gene expression. Copyright

Published

2013

18. MLPAinter for MLPA interpretation: An integrated approach for the analysis, visualisation and data management of Multiplex Ligation-dependent Probe Amplification

Author

Eijk, R. (Ronald) van, Eilers, P.H.C. (Paul), Natté, R. (Remco), Cleton-Jansen, A. (Anne-Marie), Morreau, H. (Hans), Wezel, T. (Tom) van, Oosting, J. (Jan), Eijk, R. (Ronald) van, Eilers, P.H.C. (Paul), Natté, R. (Remco), Cleton-Jansen, A. (Anne-Marie), Morreau, H. (Hans), Wezel, T. (Tom) van, and Oosting, J. (Jan)

Abstract

Background: Multiplex Ligation-Dependent Probe Amplification (MLPA) is an application that can be used for the detection of multiple chromosomal aberrations in a single experiment. In one reaction, up to 50 different genomic sequences can be analysed. For a reliable work-flow, tools are needed for administrative support, data management, normalisation, visualisation, reporting and interpretation.Results: Here, we developed a data management system, MLPAInter for MLPA interpretation, that is windows executable and has a stand-alone database for monitoring and interpreting the MLPA data stream that is generated from the experimental setup to analysis, quality control and visualisation. A statistical approach is applied for the normalisation and analysis of large series of MLPA traces, making use of multiple control samples and internal controls.Conclusions: MLPAinter visualises MLPA data in plots with information about sample replicates, normalisation settings, and sample characteristics. This integrated approach helps in the automated handling of large series of MLPA data and guarantees a quick and streamlined dataflow from the beginning of an experiment to an authorised report.

Published

2010

19. Progression and tumor heterogeneity analysis in early rectal cancer

Author

Lips, E.H. (Esther), Eijk, R. (Ronald) van, Graaf, E.J.R. (Eelco) de, Doornebosch, P. (Pascal), Miranda, N.F.C.C. (Noel) de, Oosting, J. (Jan), Karsten, T.M. (Thomas), Eilers, P.H.C. (Paul), Tollenaar, R.A.E.M. (Rob), Wezel, T. (Tom) van, Morreau, H. (Hans), Lips, E.H. (Esther), Eijk, R. (Ronald) van, Graaf, E.J.R. (Eelco) de, Doornebosch, P. (Pascal), Miranda, N.F.C.C. (Noel) de, Oosting, J. (Jan), Karsten, T.M. (Thomas), Eilers, P.H.C. (Paul), Tollenaar, R.A.E.M. (Rob), Wezel, T. (Tom) van, and Morreau, H. (Hans)

Abstract

Purpose: Adequate preoperative staging of large sessile rectal tumors requires identifying adenomas that already contain an invasive focus, specifically those that are growing in or beyond the submucosa. We systematically compared chromosomal instability patterns in adenoma and carcinoma fractions of the same lesion to assess specific steps in rectal tumor progression. Experimental Design: We analyzed 36 formalin-fixed, paraffin-embedded tumors. Both the adenoma and carcinoma fractions were typed with single nucleotide polymorphism arrays and compared with 21 previously described pure adenomas. Eighteen cases were included in an intratumor heterogeneity analysis. Results: Five specific "malignant" events (gain of 8q, 13q, and 20q and loss of 17p and 18q) and aberrant staining for p53 and SMAD4 were all increased in the adenoma fractions of carcinoma cases compared with pure adenomas. Paired analysis revealed that 31% of the samples had an equal amount of malignant aberrations in their adenoma and carcinoma fractions, whereas 25% had one and 33% had two or more extra malignant events in the carcinoma fraction. Analysis of three core biopsies per patient showed a large degree of intratumor heterogeneity. However, the number of malignant aberrations in the biopsy with the most aberrations per tumor correlated with the corresponding adenoma or carcinoma fraction (r = 0.807; P < 0.001). Conclusion: Five specific chromosomal aberrations, combined with immunohistochemistry for p53 and SMAD4, can predict possible progression of sessile rectal adenomas to early rectal cancer and can, after validation studies, be added to preoperative staging. Preferably, three biopsies should be taken from each tumor to address intratumor heterogeneity.

Published

2008