Your search keyword '"Heleen M. van der Klift"' showing total 36 results

1. Case report: a novel deep intronic splice-altering variant in DMD as a cause of Becker muscular dystrophy

Author

Shala Ghaderi Berntsson, Hans Matsson, Anna Kristoffersson, Valter Niemelä, Hermine A. van Duyvenvoorde, Cindy Richel-van Assenbergh, Heleen M. van der Klift, Olivera Casar-Borota, Carina Frykholm, and Anne-Marie Landtblom

Subjects

Becker muscular dystrophy, genetics, MLPA, mRNA, RNA sequencing, intronic variant, Genetics, QH426-470

Abstract

We present the case of a male patient who was ultimately diagnosed with Becker muscular dystrophy (BMD; MIM# 300376) after the onset of muscle weakness in his teens progressively led to significant walking difficulties in his twenties. A genetic diagnosis was pursued but initial investigation revealed no aberrations in the dystrophin gene (DMD), although immunohistochemistry and Western blot analysis suggested the diagnosis of dystrophinopathy. Eventually, after more than 10 years, an RNA analysis captured abnormal splicing where 154 nucleotides from intron 43 were inserted between exon 43 and 44 resulting in a frameshift and a premature stop codon. Normal splicing of the DMD gene was also observed. Additionally, a novel variant c.6291–13537A>G in DMD was confirmed in the genomic DNA of the patient. The predicted function of the variant aligns with the mRNA results. To conclude, we here demonstrate that mRNA analysis can guide the diagnosis of non-coding genetic variants in DMD.

Published

2023

2. Biallelic loss of LDB3 leads to a lethal pediatric dilated cardiomyopathy

Author

Tamara T. Koopmann, Yalda Jamshidi, Mohammad Naghibi-Sistani, Heleen M. van der Klift, Hassan Birjandi, Zuhair Al-Hassnan, Abdullah Alwadai, Giovanni Zifarelli, Ehsan G. Karimiani, Sahar Sedighzadeh, Amir Bahreini, Nayereh Nouri, Merlene Peter, Kyoko Watanabe, Hermine A. van Duyvenvoorde, Claudia A. L. Ruivenkamp, Aalbertine K. K. Teunissen, Arend D. J. Ten Harkel, Sjoerd G. van Duinen, Monique C. Haak, Carlos E. Prada, Gijs W. E. Santen, and Reza Maroofian

Subjects

Genetics, Genetics (clinical)

Abstract

Autosomal dominant variants in LDB3 (also known as ZASP), encoding the PDZ-LIM domain-binding factor, have been linked to a late onset phenotype of cardiomyopathy and myofibrillar myopathy in humans. However, despite knockout mice displaying a much more severe phenotype with premature death, bi-allelic variants in LDB3 have not yet been reported. Here we identify biallelic loss-of-function variants in five unrelated cardiomyopathy families by next generation sequencing. In the first family we identified compound heterozygous LOF variants in LDB3 in a fetus with bilateral talipes and mild left cardiac ventricular enlargement. Ultra-structural examination revealed highly irregular Z-disc formation, and RNA analysis demonstrated little/no expression of LDB3 protein with a functional C-terminal LIM domain in muscle tissue from the affected fetus. In a second family a homozygous LDB3 nonsense variant was identified in a young girl with severe early onset dilated cardiomyopathy with left ventricular non compaction; the same homozygous nonsense variant was identified in a third unrelated female infant with dilated cardiomyopathy. We further identified homozygous LDB3 frameshift variants in two unrelated probands diagnosed with cardiomegaly and severely reduced left ventricular ejection fraction. Our findings demonstrate that recessive LDB3 variants can lead to an early-onset severe human phenotype of cardiomyopathy and myopathy, reminiscent of the knockout mouse phenotype, and supporting a loss of function mechanism.

Published

2022

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

Author

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

Subjects

Medicine, Science

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

4. Insertion of an SVA element in MSH2 as a novel cause of Lynch syndrome

Author

Erin E. Salo-Mullen, Liying Zhang, David J. Gallagher, Vikas Rai, Magan Trottier, Yirong Li, Michael P. Farrell, Zsofia K. Stadler, Heleen M. van der Klift, and Ciyu Yang

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Retrotransposon, Minisatellite Repeats, Biology, Germline, 03 medical and health sciences, Exon, 0302 clinical medicine, Germline mutation, Alu Elements, Genetics, medicine, Humans, Gene, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Lynch syndrome, MutS Homolog 2 Protein, MSH2, 030220 oncology & carcinogenesis, DNA mismatch repair

Abstract

Germline mutations in the DNA mismatch repair (MMR) genes cause Lynch syndrome (LS). In this study, we identified and characterized a novel SINE-VNTR-Alu (SVA) insertion in exon 12 of MSH2 in an individual with early-onset colorectal cancer and a very strong LS family history. RT-PCR analysis indicated a larger aberrant MSH2 transcript in one of the family members. MSK-IMPACT next-generation sequencing and long-range PCR analyses revealed an insertion in MSH2 exon 12 at the c.1972 position in an antisense orientation. The insertion was further characterized as an SVA element approximately 3 kb in length, belonging to the SVA_F1 family of retrotransposons. This variant also segregated with LS related cancers in four affected family members in this family. Based on this evidence, this MSH2 SVA insertion is considered pathogenic.

Published

2021

5. Insertion of an SVA Element in MSH2 as a Novel Cause of Lynch Syndrome

Author

David J. Gallagher, Vikas Rai, Michael P. Farrell, Yirong Li, Magan Trottier, Erin E. Salo-Mullen, Liying Zhang, Heleen M. van der Klift, Zsofia K. Stadler, and Ciyu Yang

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Retrotransposon, Biology, medicine.disease, digestive system diseases, Lynch syndrome, Antisense Orientation, Exon, Germline mutation, MSH2, medicine, DNA mismatch repair, Gene

Abstract

Germline mutations in the DNA mismatch repair (MMR) genes cause Lynch syndrome (LS). Insertions of retrotransposons in MMR genes have been reported as a rare cause of LS. Here, we present a novel SINE-VNTR-Alu (SVA) insertion in exon 12 of MSH2 in an individual with early-onset colorectal cancer and strong LS family history. RT-PCR analysis indicated a larger aberrant MSH2 transcript in one of the family members. MSK-IMPACT next-generation sequencing testing and long-range PCR revealed an insertion in MSH2 exon 12 at the c.1972 position in an antisense orientation. The insertion was further characterized as an SVA element approximately 3 kb in length, belonging to the SVA_F1 family of retrotransposons.

Published

2020

6. An alternative approach to establishing unbiased colorectal cancer risk estimation in Lynch syndrome

Author

Inbal Kedar, Christi J. van Asperen, Jeanine J. Houwing-Duistermaat, Laurence Brugières, Sergey Nikolaev, Michael Farrell, Anja Wagner, D. Gareth Evans, Lone Sunde, Yael Goldberg, Mar Rodríguez-Girondo, Jessica I. Hoell, Katharina Wimmer, Karl Heinimann, Stefan Aretz, Maartje Nielsen, Heleen M. van der Klift, Maria Grazia Tibiletti, Tim Ripperger, Leigha Senter, Sanne W. ten Broeke, Wenche Sjursen, Encarna B. Gomez-Garcia, Stefanie Y. Zimmermann, Daniel Rueda, Marjolijn C.J. Jongmans, Noémie Lavoine, Ingrid Winship, Christina Therkildsen, Gabriel Capellá Munar, Chrystelle Colas, Alison H. Trainer, Kory Jasperson, Maurizio Genuardi, Theo A. M. van Os, Yvonne J. Vos, Mitul Modi, Hans F. A. Vasen, Manon Suerink, Suerink M., Rodriguez-Girondo M., van der Klift H.M., Colas C., Brugieres L., Lavoine N., Jongmans M., Munar G.C., Evans D.G., Farrell M.P., Genuardi M., Goldberg Y., Gomez-Garcia E., Heinimann K., Hoell J.I., Aretz S., Jasperson K.W., Kedar I., Modi M.B., Nikolaev S., van Os T.A.M., Ripperger T., Rueda D., Senter L., Sjursen W., Sunde L., Therkildsen C., Tibiletti M.G., Trainer A.H., Vos Y.J., Wagner A., Winship I., Wimmer K., Zimmermann S.Y., Vasen H.F., van Asperen C.J., Houwing-Duistermaat J.J., ten Broeke S.W., Nielsen M., Human Genetics, Clinical Genetics, Klinische Genetica, MUMC+: DA KG Polikliniek (9), and RS: GROW - R4 - Reproductive and Perinatal Medicine

Subjects

Male, Oncology, MICROSATELLITE INSTABILITY, Settore MED/03 - GENETICA MEDICA, PHENOTYPE, FAMILIES, Cohort Studies, Risk Factors, PMS2, CRITERIA, Genetics(clinical), Genetics (clinical), Mismatch Repair Endonuclease PMS2, Incidence, Incidence (epidemiology), DNA MISMATCH REPAIR, GERMLINE MUTATIONS, Middle Aged, Lynch syndrome, DNA-Binding Proteins, Cohort, colon cancer risk, Female, Colorectal Neoplasms, bMMRD, Cohort study, Adult, medicine.medical_specialty, HNPCC, colorectal cancer, FREQUENCY, Risk Assessment, BREAST, AGE, SDG 3 - Good Health and Well-being, Internal medicine, SURVEILLANCE, medicine, Humans, Genetic Predisposition to Disease, Germ-Line Mutation, Aged, business.industry, Microsatellite instability, MSH6, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Confidence interval, Mutation, business

Abstract

Purpose: Biallelic pathogenic variants in the mismatch repair (MMR) genes cause a recessive childhood cancer predisposition syndrome known as constitutional mismatch repair deficiency (CMMRD). Family members with a heterozygous MMR variant have Lynch syndrome. We aimed at estimating cancer risk in these heterozygous carriers as a novel approach to avoid complicated statistical methods to correct for ascertainment bias.Methods: Cumulative colorectal cancer incidence was estimated in a cohort of PMS2- and MSH6-associated families, ascertained by the CMMRD phenotype of the index, by using mutation probabilities based on kinship coefficients as analytical weights in a proportional hazard regression on the cause-specific hazards. Confidence intervals (CIs) were obtained by bootstrapping at the family level.Results: The estimated cumulative colorectal cancer risk at age 70 years for heterozygous PMS2 variant carriers was 8.7% (95% CI 4.3-12.7%) for both sexes combined, and 9.9% (95% CI 4.9-15.3%) for men and 5.9% (95% CI 1.6-11.1%) for women separately. For heterozygous MSH6 variant carriers these estimates are 11.8% (95% CI 4.5-22.7%) for both sexes combined, 10.0% (95% CI 1.83-24.5%) for men and 11.7% (95% CI 2.10-26.5%) for women.Conclusion: Our findings are consistent with previous reports that used more complex statistical methods to correct for ascertainment bias. These results underline the need for MMR gene-specific surveillance protocols for Lynch syndrome.

Published

2019

7. Comprehensive Mutation Analysis of PMS2 in a Large Cohort of Probands Suspected of Lynch Syndrome or Constitutional Mismatch Repair Deficiency Syndrome

Author

Maartje Nielsen, Marjolijn J. L. Ligtenberg, Yvonne Tiersma, Juul T. Wijnen, Maran J. W. Olderode-Berends, Encarna Gomez Garcia, B. Redeker, José B. M. Zonneveld, Sanne W. ten Broeke, Frederik J. Hes, Carli M. J. Tops, Peter Devilee, Theo A. M. van Os, Christi J. van Asperen, Hans J. J. P. Gille, Niels de Wind, Heleen M. van der Klift, Arjen R. Mensenkamp, Tom G.W. Letteboer, Yvonne J. Vos, Elsa C. Bik, Mark Drost, S. Verhoef, Liselotte P. van Hest, Anja Wagner, Human Genetics, Human genetics, CCA - Cancer biology, RS: GROW - R4 - Reproductive and Perinatal Medicine, MUMC+: DA KG Polikliniek (9), Klinische Genetica, Medical Genetics, and Clinical Genetics

Subjects

0301 basic medicine, DNA Mutational Analysis, pseudogenes, COLORECTAL-CANCER, Cohort Studies, 0302 clinical medicine, Mutation Carrier, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], PMS2, Missense mutation, Genetics (clinical), Mismatch Repair Endonuclease PMS2, Netherlands, Medicine(all), Genetics, Brain Neoplasms, MLH1, Neoplastic Syndromes, Hereditary/genetics, Lynch syndrome, CMMRD, missense variants, immunohistochemistry, mismatch repair, 030220 oncology & carcinogenesis, Mutation (genetic algorithm), DNA mismatch repair, Microsatellite Instability, Colorectal Neoplasms, EUROPEAN CONSORTIUM CARE, PSEUDOGENE INTERFERENCE, congenital, hereditary, and neonatal diseases and abnormalities, DNA Mutational Analysis/methods, Biology, 03 medical and health sciences, Germline mutation, Neoplastic Syndromes, Hereditary, Colorectal Neoplasms, Hereditary Nonpolyposis/genetics, SYNDROME FAMILIES, CFR PARTICIPANTS, medicine, Journal Article, Humans, Genetic Predisposition to Disease, Germ-Line Mutation, Brain Neoplasms/genetics, Microsatellite instability, Genetic Variation, Mismatch Repair Endonuclease PMS2/genetics, medicine.disease, Colorectal Neoplasms/genetics, Colorectal Neoplasms, Hereditary Nonpolyposis, GENE, digestive system diseases, 030104 developmental biology, PROMOTER HYPERMETHYLATION, 3' DELETIONS, Cancer research, NONPOLYPOSIS COLON-CANCER

Abstract

Monoallelic PMS2 germline mutations cause 5-15% of Lynch syndrome, a midlife cancer predisposition, whereas biallelic PMS2 mutations cause approximately 60% of constitutional MMR deficiency (CMMRD), a rare childhood cancer syndrome. Recently improved DNA and RNA-based strategies are applied to overcome problematic PMS2 mutation analysis due to the presence of pseudogenes and frequent gene conversion events. Here, we determined PMS2 mutation detection yield and mutation spectrum in a nationwide cohort of 396 probands. Furthermore, we studied concordance between tumor IHC/ MSI (immunohistochemistry/ microsatellite-instability) profile and mutation carrier state. Overall, we found 52 different pathogenic PMS2 variants explaining 121 Lynch syndrome and nine CMMRD patients. In vitro MMR assays suggested pathogenicity for three missense variants. Ninety-one PMS2 mutation carriers (70%) showed isolated loss of PMS2 in their tumors, for 31 (24%) no or inconclusive IHC was available, and eight carriers (6%) showed discordant IHC (presence of PMS2 or loss of both MLH1 and PMS2). Ten cases with isolated PMS2 loss (10%; 10/97) harbored MLH1 mutations. We confirmed that recently improved mutation analysis provides a high yield of PMS2 mutations in patients with isolated loss of PMS2 expression. Application of universal tumor pre-screening methods will however miss some PMS2 germline mutation carriers. This article is protected by copyright. All rights reserved.

Published

2016

8. Involvement of MBD4 inactivation in mismatch repair-deficient tumorigenesis

Author

Andrea Ventura, Riccardo Fodde, Antonio Percesepe, Alfonso Bellacosa, David P. Turner, Valentina Rovella, Maurizio Ponz de Leon, Karthik Devarajan, Juul T. Wijnen, Maurizio Genuardi, Pietro Mancuso, Salvatore Cortellino, Andres J. Klein-Szanto, Emanuela Lucci-Cordisco, Antonio Riccio, Rossella Tricarico, Heleen M. van der Klift, Pål Møller, Alessandra Viel, Kathy Q. Cai, Monica Pedroni, Paolo Radice, Lucio Bertario, Shantie Jagmohan-Changur, Giovanni Neri, Pathology, and Neurology

Subjects

Male, Carcinogenesis, Knockout, DNA Mutational Analysis, HNPCC, MBD4/MED1, colorectal cancer, mismatch repair, mutations, Settore MED/09, Settore MED/03 - GENETICA MEDICA, medicine.disease_cause, DNA Mismatch Repair, Polymerase Chain Reaction, Settore MED/06, MBD4, 03 medical and health sciences, Mice, 0302 clinical medicine, Genotype, Medicine, Missense mutation, Animals, Humans, 030304 developmental biology, Oligonucleotide Array Sequence Analysis, Genetics, Mice, Knockout, 0303 health sciences, Mutation, Endodeoxyribonucleases, business.industry, Phenotype, digestive system diseases, 3. Good health, Settore MED/03, Oncology, CpG site, 030220 oncology & carcinogenesis, DNA mismatch repair, Female, business, Colorectal Neoplasms, Research Paper

Abstract

The DNA glycosylase gene MBD4 safeguards genomic stability at CpG sites and is frequently mutated at coding poly-A tracks in mismatch repair (MMR)-defective colorectal tumors (CRC). Mbd4 biallelic inactivation in mice provided conflicting results as to its role in tumorigenesis. Thus, it is unclear whether MBD4 alterations are only secondary to MMR defects without functional consequences or can contribute to the mutator phenotype. We investigated MBD4 variants in a large series of hereditary/familial and sporadic CRC cases. Whereas MBD4 frameshifts were only detected in tumors, missense variants were found in both normal and tumor DNA. In CRC with double-MBD4/MMR and single-MBD4 variants, transition mutation frequency was increased, indicating that MBD4 defects may affect the mutational landscape independently of MMR defect. Mbd4-deficient mice showed reduced survival when combined with Mlh1-/- genotype. Taken together, these data suggest that MBD4 inactivation may contribute to tumorigenesis, acting as a modifier of MMR-deficient cancer phenotype.

Published

2015

9. The effect of genotypes and parent of origin on cancer risk and age of cancer development in PMS2 mutation carriers

Author

Olaf M. Dekkers, B. Redeker, Liesbeth Spruijt, Fred H. Menko, Gabriel Capellá Munar, Annika Lindblom, Sanne W. ten Broeke, Pål Møller, Frederik J. Hes, Arjen Mensenkamp, Carli M. J. Tops, Manon Suerink, Juul T. Wijnen, Yvonne J. Vos, Nils Rahner, Anja Wagner, Inge Bernstein, Hans F. A. Vasen, Maran Olderode, Tom G.W. Letteboer, Theo A. M. van Os, Hans Morreau, Encarna B. Gomez Garcia, Heleen M. van der Klift, Nicoline Hoogerbrugge, Maartje Nielsen, Human Genetics, RS: GROW - R4 - Reproductive and Perinatal Medicine, MUMC+: DA KG Polikliniek (9), Klinische Genetica, Human genetics, CCA - Cancer biology, Clinical sciences, and Clinical Genetics

Subjects

0301 basic medicine, Oncology, Male, genotype-phenotype correlations, Colorectal cancer, Gene Expression, VARIANTS, Bioinformatics, PHENOTYPE, FAMILIES, MISMATCH REPAIR, 0302 clinical medicine, Neoplasms, Gene expression, Genotype, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], PMS2, Age of Onset, Non-U.S. Gov't, Genetics (clinical), Mismatch Repair Endonuclease PMS2, risk, Medicine(all), Research Support, Non-U.S. Gov't, NONPOLYPOSIS COLORECTAL-CANCER, Middle Aged, Lynch syndrome, 030220 oncology & carcinogenesis, Cohort studies, Female, parent-of-origin effect, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Adult, medicine.medical_specialty, Heterozygote, Research Support, LYNCH-SYNDROME, 03 medical and health sciences, Germline mutation, SDG 3 - Good Health and Well-being, Internal medicine, medicine, Journal Article, hereditary colon cancer, Humans, Genetic Predisposition to Disease, Genetic Association Studies, Germ-Line Mutation, Aged, business.industry, Endometrial cancer, Mismatch Repair Endonuclease PMS2/genetics, medicine.disease, GENE, digestive system diseases, 030104 developmental biology, Age of onset, mutation, business, aged, 80 and over, Neoplasms/epidemiology

Abstract

PURPOSE: Lynch syndrome (LS), a heritable disorder with an increased risk of primarily colorectal cancer (CRC) and endometrial cancer (EC), can be caused by mutations in the PMS2 gene. We wished to establish whether genotype and/or parent-of-origin effects (POE) explain (part of) the reported variability in severity of the phenotype.METHODS: European PMS2 mutation carriers (n = 381) were grouped and compared based on RNA expression and whether the mutation was inherited paternally or maternally.RESULTS: Mutation carriers with loss of RNA expression (group 1) had a significantly lower age at CRC diagnosis (51.1 years vs. 60.0 years, P = 0.035) and a lower age at EC diagnosis (55.8 years vs. 61.0 years, P = 0.2, nonsignificant) compared with group 2 (retention of RNA expression). Furthermore, group 1 showed slightly higher, but nonsignificant, hazard ratios (HRs) for both CRC (HR: 1.31, P = 0.38) and EC (HR: 1.22, P = 0.72). No evidence for a significant parent-of-origin effect was found for either CRC or EC.CONCLUSIONS: PMS2 mutation carriers with retention of RNA expression developed CRC 9 years later than those with loss of RNA expression. If confirmed, this finding would justify a delay in surveillance for these cases. Cancer risk was not influenced by a parent-of-origin effect.Genet Med advance online publication 25 June 2015Genetics in Medicine (2015); doi:10.1038/gim.2015.83.

Published

2016

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

Author

Anja Wagner, Heleen M. van der Klift, Brendy E.W.M. van den Akker, Carli M. J. Tops, Encarna B. Gomez-Garcia, Juul T. Wijnen, Dina Ruano, Peter Devilee, Jeroen F. J. Laros, Tom van Wezel, Hans Morreau, Michiel van Galen, Shantie Jagmohan-Changur, Hans F. A. Vasen, Tom G.W. Letteboer, Marije A Geilenkirchen, Anne M.L. Jansen, Frederik J. Hes, Clinical Genetics, RS: GROW - R4 - Reproductive and Perinatal Medicine, MUMC+: DA KG Polikliniek (9), Klinische Genetica, and Medical Genetics

Subjects

0301 basic medicine, lcsh:Medicine, DNA Mismatch Repair, Biochemistry, Germline, White Blood Cells, Database and Informatics Methods, 0302 clinical medicine, Animal Cells, Medicine and Health Sciences, Leukocytes, DNA sequencing, Genome Sequencing, lcsh:Science, Medicine(all), Genetics, DNA methylation, Multidisciplinary, Agricultural and Biological Sciences(all), integumentary system, Genomics, Middle Aged, Genomic Databases, Chromatin, Colon/metabolism, Lynch syndrome, Nucleic acids, Gene Expression Regulation, Neoplastic, Oncology, 030220 oncology & carcinogenesis, Leukocytes/metabolism, Cohort studies, Epigenetics, DNA mismatch repair, Cellular Types, DNA modification, Colorectal Neoplasms, MutL Protein Homolog 1, Sequence Analysis, Transcriptome Analysis, Chromatin modification, Research Article, Chromosome biology, Next-Generation Sequencing, Cell biology, Colon, Sequence analysis, Immune Cells, Immunology, Rectum/metabolism, Sequence Databases, Biology, Research and Analysis Methods, MLH1, 03 medical and health sciences, Germline mutation, Colorectal Neoplasms, Hereditary Nonpolyposis/genetics, Journal Article, medicine, Humans, Molecular Biology Techniques, Sequencing Techniques, Molecular Biology, Gene, DNA sequence analysis, Germ-Line Mutation, Colorectal Cancer, Blood Cells, Biology and life sciences, MutL Protein Homolog 1/genetics, Biochemistry, Genetics and Molecular Biology(all), lcsh:R, Rectum, Cancers and Neoplasms, Computational Biology, DNA, Genome Analysis, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Colorectal Neoplasms/genetics, digestive system diseases, Biological Databases, 030104 developmental biology, lcsh:Q, Gene expression, Genetics and Molecular Biology(all)

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

11. Abstract 649: Development of a novel RNA sequencing approach that identifies aberrant splicing in cancer predisposing genes

Author

Hans Morreau, Ajay Goel, Juul T. Wijnen, Anne M.L. Jansen, Carli M. J. Tops, Frederik J. Hes, Jaap D. H. van Eendenburg, Tom van Wezel, and Heleen M. van der Klift

Subjects

Cancer Research, Oncology, Cancer-Predisposing Gene, RNA splicing, Alternative splicing, Nucleic acid, RNA, splice, Computational biology, Biology, Gene, Housekeeping gene

Abstract

Background: High-throughput sequencing efforts in molecular tumor diagnostics detect increased numbers of novel genetic variants, including the ones that are predicted to affect splicing. Current approach for predicting whether a specific variant may result in aberrant RNA transcripts often consists of in-silico prediction using bioinformatics prediction tools, which is sometimes followed by RT-PCR analysis of the RNA extracted from blood, or functional splicing reporter assays. Although high-quality patient RNA analysis is usually preferred, such RNA is not always available, or the analysis is hampered due to degradation of aberrant transcripts through nonsense-mediated decay. To overcome this issue, we investigated the possibility of analyzing RNA isolated from formalin-fixed paraffin-embedded (FFPE) tissues, with the underlying hypothesis that formalin fixation may inhibit RNA degradation, enabling the detection of aberrant RNA products. Methods: RNA analysis was performed for 13 canonical splice site variants predicted or known to affect splicing in the cancer predisposition genes MLH1, MSH2, MSH6, APC and BRCA1. Of 11 variants, total nucleic acid was obtained from FFPE tumor tissues. For two variants, no FFPE material was available, but EBV-transformed B-cells carrying a splice variant were cultured. Primers were designed to amplify the exon-exon boundary predicted to be affected. Housekeeping gene expression was assessed to determine presence of RNA. Results: Total nucleic acid was successfully isolated for 10 variants from eight FFPE tumor tissues and two EBV-transformed B-cell lines. Aberrant splicing was confirmed in all six variants known to result in splicing. Of one known splice variant, present in the B-cell line, the known aberrant splice product could only be detected after formalin fixation of the cells, suggesting that formalin fixation possibly inhibited RNA degradation. Conclusion: Aberrant splicing was successfully identified in all known splice variants and three of four variants predicted to affect splicing, of which the splice effect was previously unknown. Using a RNA sequencing approach, somatic splice variants could be easily and rapidly analyzed, enabling retrospective analysis of variants predicted to result in splicing when only FFPE material is available in clinical settings. Citation Format: Anne M. Jansen, Heleen M. van der Klift, Jaap D. van Eendenburg, Carli M. Tops, Juul T. Wijnen, Frederik J. Hes, Ajay Goel, Hans Morreau, Tom van Wezel. Development of a novel RNA sequencing approach that identifies aberrant splicing in cancer predisposing genes [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 649.

Published

2018

12. Intronic variants inBRCA1andBRCA2that affect RNA splicing can be reliably selected by splice-site prediction programs

Author

Egbert Bakker, Heleen M. van der Klift, Geraldine R. Vink, Juul T. Wijnen, Cees J. Cornelisse, Jaennelle Kraan, Maaike P.G. Vreeswijk, Peter Devilee, and Christi J. van Asperen

Subjects

Adult, endocrine system diseases, Sequence analysis, RNA Splicing, Molecular Sequence Data, Exonic splicing enhancer, Breast Neoplasms, Biology, chemistry.chemical_compound, Genetic variation, Genetics, Humans, skin and connective tissue diseases, Genetics (clinical), BRCA2 Protein, Base Sequence, BRCA1 Protein, Sequence Analysis, RNA, Intron, Genetic Variation, RNA, Introns, chemistry, RNA splicing, Female, RNA Splice Sites, Software, DNA

Abstract

A large number of sequence variants identified in BRCA1 and BRCA2 cannot be distinguished as either disease-causing mutations or neutral variants. These so-called unclassified variants (UVs) include variants that are located in the intronic sequences of BRCA1 and BRCA2. The purpose of this study was to assess the use of splice-site prediction programs (SSPPs) to select intronic variants in BRCA1 and BRCA2 that are likely to affect RNA splicing. We performed in vitro molecular characterization of RNA of six intronic variants in BRCA1 and BRCA2. In four cases (BRCA1, c.81-6T>A and c.4986+5G>T; BRCA2, c.7617+2T>G and c.8754+5G>A) a deleterious effect on RNA splicing was seen, whereas the c.135-15_-12del variant in BRCA1 showed no effect on RNA splicing. In the case of the BRCA2 c.68-7T>A variant, RNA analysis was not sufficient to establish the clinical significance. Six SSPPs were used to predict whether an effect on RNA splicing was expected for these six variants as well as for 23 intronic variants in BRCA1 for which the effect on RNA splicing has been published. Out of a total of 174 predictions, 161 (93%) were informative (i.e., the wild-type splice-site was recognized). No false-negative predictions were observed; an effect on RNA splicing was always predicted by these programs. In four cases (2.5%) a false-positive prediction was observed. For DNA diagnostic laboratories, these programs are therefore very useful to select intronic variants that are likely to affect RNA splicing for further analysis.

Published

2009

13. Genome-wide copy neutral LOH is infrequent in familial and sporadic microsatellite unstable carcinomas

Author

Anneke Middeldorp, Tom van Wezel, Frederik J. Hes, Ronald van Eijk, Hans Morreau, Jan Oosting, Carli M. J. Tops, Heleen M. van der Klift, Marjo van Puijenbroek, Juul T. Wijnen, Hans F. A. Vasen, Clinical sciences, and Medical Genetics

Subjects

Adult, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Gene Dosage, Loss of Heterozygosity, HNPCC, Biology, MLH1, DNA Mismatch Repair, Polymorphism, Single Nucleotide, Loss of heterozygosity, Chromosomal Instability, Genetics, medicine, PMS2, Humans, Mismatch repair (MMR) genes, Genetics(clinical), Unclassified variants, neoplasms, Genetics (clinical), Adaptor Proteins, Signal Transducing, Aged, Aged, 80 and over, Copy neutral loss of heterozygosity, Carcinoma, MSI-H, Nuclear Proteins, nutritional and metabolic diseases, DNA Methylation, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, MLH1 hypermethylation, digestive system diseases, Lynch syndrome, MSH6, Oncology, MSH2, Colonic Neoplasms, Microsatellite Instability, DNA mismatch repair, MutL Protein Homolog 1, SNP array

Abstract

Mismatch repair deficiency in tumors can result from germ line mutations in one of the mismatch repair (MMR) genes (MLH1, MSH2, MSH6 and PMS2), or from sporadic promoter hypermethylation of MLH1. The role of unclassified variants (UVs) in MMR genes is subject to debate. To establish the extend of chromosomal instability and copy neutral loss of heterozygosity (cnLOH), we analyzed 41 archival microsatellite unstable carcinomas, mainly colon cancer, from 23 patients with pathogenic MMR mutations, from eight patients with UVs in one of the MMR genes and 10 cases with MLH1 promoter hypermethylation. We assessed genome wide copy number abnormalities and cnLOH using SNP arrays. SNP arrays overcome the problems of detecting LOH due to instability of polymorphic microsatellite markers. All carcinomas showed relatively few chromosomal aberrations. Also cnLOH was infrequent and in Lynch syndrome carcinomas usually confined to the locus harbouring pathogenic mutations in MLH1, MSH2 or PMS2 In the carcinomas from the MMR-UV carriers such cnLOH was less common and in the carcinomas with MLH1 promoter hypermethylation no cnLOH at MLH1 occurred. MSI-H carcinomas of most MMR-UV carriers present on average with more aberrations compared to the carcinomas from pathogenic MMR mutation carriers, suggesting that another possible pathogenic MMR mutation had not been missed. The approach we describe here shows to be an excellent way to study genome-wide cnLOH in archival mismatch repair deficient tumors.

Published

2008

14. Lynch Syndrome Caused by Germline PMS2 Mutations:Delineating the Cancer Risk

Author

Rolf H. Sijmons, Manon Suerink, Richard M. Brohet, Frederik J. Hes, Mary E. Velthuizen, Carli M. J. Tops, Theo A. M. van Os, B. Redeker, Nils Rahner, Anja Wagner, Yvonne J. Vos, Encarna B. Gomez Garcia, Fred H. Menko, Heleen M. van der Klift, Hans F. A. Vasen, Arjen R. Mensenkamp, Inge Bernstein, Tom G.W. Letteboer, Annika Lindblom, Sanne W. ten Broeke, Gabriel Capellá Munar, Pål Møller, Juul T. Wijnen, Liesbeth Spruijt, Maartje Nielsen, Nicoline Hoogerbrugge, Klinische Genetica, Populatie Genetica, RS: GROW - Oncology, RS: GROW - R4 - Reproductive and Perinatal Medicine, Human Genetics, Ethical, Legal, Social Issues in Genetics (ELSI), Guided Treatment in Optimal Selected Cancer Patients (GUTS), Erasmus MC other, Clinical Genetics, Human genetics, CCA - Oncogenesis, and Clinical sciences

Subjects

Oncology, Male, Cancer Research, Colorectal cancer, DNA Mutational Analysis, VARIANTS, GUIDELINES, FAMILIES, Cohort Studies, Gene Frequency, Risk Factors, PMS2, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], CRITERIA, Mismatch Repair Endonuclease PMS2, Genetics, Medicine(all), Adenosine Triphosphatases, Aged, 80 and over, Adenosine Triphosphatases/genetics, Genetic Predisposition to Disease/genetics, COLON-CANCER, MLH1, NONPOLYPOSIS COLORECTAL-CANCER, Middle Aged, DNA Repair Enzymes/genetics, CARRIERS, Lynch syndrome, DNA-Binding Proteins, Female, Colorectal Neoplasms, Cohort study, Rare cancers Radboud Institute for Health Sciences [Radboudumc 9], Adult, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Genotype, Germline mutation, SDG 3 - Good Health and Well-being, Internal medicine, Colorectal Neoplasms, Hereditary Nonpolyposis/genetics, SURVEILLANCE, medicine, Humans, Genetic Predisposition to Disease, Germ-Line Mutation, Aged, Family Health, business.industry, Endometrial cancer, Cancer, medicine.disease, Colorectal Neoplasms/genetics, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Endometrial Neoplasms, DNA Repair Enzymes, CLINICAL MANAGEMENT, business, Endometrial Neoplasms/genetics, DNA-Binding Proteins/genetics

Abstract

Purpose The clinical consequences of PMS2 germline mutations are poorly understood compared with other Lynch-associated mismatch repair gene (MMR) mutations. The aim of this European cohort study was to define the cancer risk faced by PMS2 mutation carriers. Methods Data were collected from 98 PMS2 families ascertained from family cancer clinics that included a total of 2,548 family members and 377 proven mutation carriers. To adjust for potential ascertainment bias, a modified segregation analysis model was used to calculate colorectal cancer (CRC) and endometrial cancer (EC) risks. Standardized incidence ratios (SIRs) were calculated to estimate risks for other Lynch syndrome–associated cancers. Results The cumulative risk (CR) of CRC for male mutation carriers by age 70 years was 19%. The CR among female carriers was 11% for CRC and 12% for EC. The mean age of CRC development was 52 years, and there was a significant difference in mean age of CRC between the probands (mean, 47 years; range, 26 to 68 years) and other family members with a PMS2 mutation (mean, 58 years; range, 31 to 86 years; P < .001). Significant SIRs were observed for cancers of the small bowel, ovaries, breast, and renal pelvis. Conclusion CRC and EC risks were found to be markedly lower than those previously reported for the other MMR. However, these risks embody the isolated risk of carrying a PMS2 mutation, and it should be noted that we observed a substantial variation in cancer phenotype within and between families, suggesting the influence of genetic modifiers and lifestyle factors on cancer risks.

Published

2015

15. Heterozygous Mutations in PMS2 Cause Hereditary Nonpolyposis Colorectal Carcinoma (Lynch Syndrome)

Author

Margreet G.F.M. Ausems, Yvonne M.C. Hendriks, Hans Morreau, Heleen M. van der Klift, Annette H. J. T. Vriends, Anja Wagner, Carli M. J. Tops, Theo A. M. van Os, Encarna Gomez, Juul T. Wijnen, Hans F. A. Vasen, Martijn H. Breuning, Marjo van Puijenbroek, Shantie Jagmohan–Changur, and Clinical Genetics

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Base Pair Mismatch, DNA Mutational Analysis, Biology, MLH1, Polymerase Chain Reaction, PMS2, medicine, Humans, Point Mutation, neoplasms, Adaptor Proteins, Signal Transducing, Mismatch Repair Endonuclease PMS2, Sequence Deletion, Adenosine Triphosphatases, Genetics, Base Sequence, Hepatology, Genetic Carrier Screening, Point mutation, Gastroenterology, Genetic Variation, Nuclear Proteins, nutritional and metabolic diseases, Microsatellite instability, Exons, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Lynch syndrome, Pedigree, DNA-Binding Proteins, MSH6, DNA Repair Enzymes, Phenotype, MSH2, Cancer research, Female, DNA mismatch repair, Carrier Proteins, MutL Protein Homolog 1

Abstract

Background #x0026; Aims: The role of the mismatch repair gene PMS2 in hereditary nonpolyposis colorectal carcinoma (HNPCC) is not fully clarified. To date, only 7 different heterozygous truncating PMS2 mutations have been reported in HNPCC-suspected families. Our aim was to further assess the role of PMS2 in HNPCC. Methods: We performed Southern blot analysis in 112 patients from MLH1-, MSH2-, and MSH6-negative HNPCC-like families. A subgroup (n = 38) of these patients was analyzed by denaturing gradient gel electrophoresis (DGGE). In a second study group consisting of 775 index patients with familial colorectal cancer, we performed immunohistochemistry using antibodies against MLH1, MSH2, MSH6, and PMS2 proteins. In 8 of 775 tumors, only loss of PMS2 expression was found. In these cases, we performed Southern blot analysis and DGGE. Segregation analysis was performed in the families with a (possibly) deleterious mutation. Results: Seven novel mutations were identified: 4 genomic rearrangements and 3 truncating point mutations. Three of these 7 families fulfill the Amsterdam II criteria. The pattern of inheritance is autosomal dominant with a milder phenotype compared with families with pathogenic MLH1 or MSH2 mutations. Microsatellite instability and immunohistochemical analysis performed in HNPCC-related tumors from proven carriers showed a microsatellite instability high phenotype and loss of PMS2 protein expression in all tumors. Conclusions: We show that heterozygous truncating mutations in PMS2 do play a role in a small subset of HNPCC-like families. PMS2 mutation analysis is indicated in patients diagnosed with a colorectal tumor with absent staining for the PMS2 protein.

Published

2006

16. Splicing analysis for exonic and intronic mismatch repair gene variants associated with Lynch syndrome confirms high concordance between minigene assays and patient RNA analyses

Author

Carli M. J. Tops, Niki van der Steenstraten, Juul T. Wijnen, Anne M.L. Jansen, Peter Devilee, Heleen M. van der Klift, and Elsa C. Bik

Subjects

Genetics, mismatch repair genes, minigene assay, RNA, Original Articles, Biology, Aberrant splicing, Exon, Lynch syndrome, MSH2, RNA splicing, patient RNA analysis, DNA mismatch repair, splice, variant classification, Molecular Biology, Gene, Genetics (clinical), Minigene

Abstract

A subset of DNA variants causes genetic disease through aberrant splicing. Experimental splicing assays, either RT-PCR analyses of patient RNA or functional splicing reporter minigene assays, are required to evaluate the molecular nature of the splice defect. Here, we present minigene assays performed for 17 variants in the consensus splice site regions, 14 exonic variants outside these regions, and two deep intronic variants, all in the DNA mismatch-repair (MMR) genes MLH1, MSH2, MSH6, and PMS2, associated with Lynch syndrome. We also included two deep intronic variants in APC and PKD2. For one variant (MLH1 c.122A>G), our minigene assay and patient RNA analysis could not confirm the previously reported aberrant splicing. The aim of our study was to further investigate the concordance between minigene splicing assays and patient RNA analyses. For 30 variants results from patient RNA analyses were available, either performed by our laboratory or presented in literature. Some variants were deliberately included in this study because they resulted in multiple aberrant transcripts in patient RNA analysis, or caused a splice effect other than the prevalent exon skip. While both methods were completely concordant in the assessment of splice effects, four variants exhibited major differences in aberrant splice patterns. Based on the present and earlier studies, together showing an almost 100% concordance of minigene assays with patient RNA analyses, we discuss the weight given to minigene splicing assays in the current criteria proposed by InSiGHT for clinical classification of MMR variants.

Published

2014

17. Marfan-like habitus and familial adenomatous polyposis in two unrelated males: a significant association?

Author

Juul T. Wijnen, George A. Calin, Ana Ionita, Kerstin Hansson, Hans G. Dauwerse, Alexandru Oproiu, Steliana Calin, Cor Breukel, Heleen M. van der Klift, Adri Mulder, Ron Smits, Dragos Stefanescu, Riccardo Fodde, Neurology, Gastroenterology & Hepatology, and Pathology

Subjects

Adult, Male, Marfan syndrome, congenital, hereditary, and neonatal diseases and abnormalities, Genes, APC, Fibrillin-2, Molecular Sequence Data, Chromosomal rearrangement, Biology, Fibrillins, medicine.disease_cause, Germline, Marfan Syndrome, Frameshift mutation, Familial adenomatous polyposis, Exon, Genetics, medicine, Humans, Amino Acid Sequence, In Situ Hybridization, Fluorescence, Genetics (clinical), Mutation, Microfilament Proteins, Chromosome, medicine.disease, Pedigree, Adenomatous Polyposis Coli, Female

Abstract

Familial adenomatous polyposis (FAP) can be considered as a condition of the whole body as extracolonic features derived from all the three embryonic lineages are recorded with varying frequency in addition to the presence of multiple adenomas in the large intestine. Here, we describe two unrelated cases of FAP with unusual extracolonic phenotypes, namely several abnormalities of mesodermal origin strongly resembling Marfan syndrome (MFS) or a Marfan-like habitus. Conventional cytogenetic and FISH analysis did not reveal any gross chromosomal rearrangement on the long arm of chromosome 5 where the APC and FBN2 genes were located. However, in case 2 the FAP-causing mutation in the APC gene was found in the donor splice site of exon 4 and was shown to result in a frameshift and a premature termination codon. We propose that such connective tissue abnormalities may result from germline APC mutations in combination with specific genetic and/or environmental modifying factors.

Published

1999

18. Molecular analysis of the APC gene in 105 Dutch kindreds with familial adenomatous polyposis: 67 germline mutations identified by DGGE, PTT, and southern analysis

Author

Rob. B. van der Luijt, P. Meera Khan, Hans F.A. Vasen, Carli M.J. Tops, Inge S.J. van Leeuwen‐Cornelisse, Juul Th. Wijnen, Heleen M. van der Klift, Rob J. Plug, Gerrit Griffioen, and Riccardo Fodde

Subjects

Genetics, Genetics (clinical)

Published

1997

19. Molecular, cytogenetic, and phenotypic studies of a constitutional reciprocal translocation t(5; I0)(q22; q25) responsible for familial adenomatous polyposis in a Dutch pedigree

Author

Cor Breukel, Heleen M. van der Klift, Rob B. van der Luijt, P. Meera Khan, Hans F. A. Vasen, Riccardo Fodde, Pleun Snel, Carli M. J. Tops, Inge van Leeuwen-Cornelisse, Frederik J. M. Slors, Ellen Van Noort, Geoffrey C. Beverstock, and Hans G. Dauwerse

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, biology, Adenomatous polyposis coli, Translocation Breakpoint, Chromosomal translocation, Gene rearrangement, medicine.disease, Null allele, Molecular biology, Germline, Familial adenomatous polyposis, Germline mutation, Genetics, biology.protein, medicine

Abstract

Familial adenomatous polyposis (FAP) is an inherited predisposition to colorectal cancer caused by germline mutations in the adenomatous polyposis coli (APC) gene located on chromosome segment 5q21-q22. We detected a germline rearrangement of the APC gene in a Dutch FAP family by screening genomic DNA samples with APC cDNA probes. Subsequent molecular and cytogenetic studies revealed a constitutional reciprocal translocation t(5; 10) (q22; q25) that resulted in the disruption of the APC gene. Southern blot and polymorphic marker analysis indicated that part of the APC gene had been deleted. Analysis of the APC protein product indicated that the translocation breakpoint did not lead t o the formation of a detectable truncated APC protein but apparently resulted in a null allele. Evaluation of the clinical phenotypes in the patients suggested that they exhibited features of an unusual form of FAP characterized by a slightly delayed age of onset of colorectal cancer and a reduced number of colorectal polyps. The latter were mainly sessile and were located predominantly in the proximal colon. To our knowledge, this is the first description of FAP caused by a reciprocal translocation disrupting the APC gene. © 1995 Wiley-Liss, Inc.

Published

1995

20. Insertion of an SVA element, a nonautonomous retrotransposon, in PMS2 intron 7 as a novel cause of Lynch syndrome

Author

Frederik J. Hes, Peter Devilee, Carli M. J. Tops, Juul T. Wijnen, Heleen M. van der Klift, Clinical sciences, and Medical Genetics

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Retroelements, Biology, LINE-1-mediated retrotransposition, Introns/genetics, symbols.namesake, Germline mutation, Genetics, PMS2, medicine, Humans, Colorectal Neoplasms, Hereditary Nonpolyposis/etiology, Genetics (clinical), Mismatch Repair Endonuclease PMS2, Southern blot, Adenosine Triphosphatases, Sanger sequencing, Mutation Spectra, Adenosine Triphosphatases/genetics, Intron, DNA Repair Enzymes/genetics, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Molecular biology, Introns, Lynch syndrome, DNA-Binding Proteins, genomic DNA, SVA, DNA Repair Enzymes, symbols, Retroelements/genetics, DNA-Binding Proteins/genetics

Abstract

Heterozygous germline mutations in the mismatch repair gene PMS2 predispose carriers for Lynch syndrome, an autosomal dominant predisposition to cancer. Here, we present a LINE-1-mediated retrotranspositional insertion in PMS2 as a novel mutation type for Lynch syndrome. This insertion, detected with Southern blot analysis in the genomic DNA of the patient, is characterized as a 2.2 kb long 5' truncated SVA_F element. The insertion is not detectable by current diagnostic testing limited to MLPA and direct Sanger sequencing on genomic DNA. The molecular nature of this insertion could only be resolved in RNA from cultured lymphocytes in which nonsense-mediated RNA decay was inhibited. Our report illustrates the technical problems encountered in the detection of this mutation type. Especially large heterozygous insertions will remain unnoticed because of preferential amplification of the smaller wild-type allele in genomic DNA, and are probably underreported in the mutation spectra of autosomal dominant disorders.

Published

2012

21. Analysis and interpretation of RNA splicing alterations in genes involved in genetic disorders

Author

Maaike P G, Vreeswijk and Heleen M, van der Klift

Subjects

Electrophoresis, Agar Gel, DNA, Complementary, RNA Splicing, DNA Mutational Analysis, DNA, Fibroblasts, Polymerase Chain Reaction, Neoplasms, Mutation, Animals, Humans, RNA, Genetic Predisposition to Disease, Genetic Testing, Lymphocytes, Cells, Cultured, Germ-Line Mutation

Abstract

Germ line mutations in genes involved in hereditary cancer syndromes, such as BRCA1 and BRCA2 in breast cancer and MSH2, MSH6, MLH1, and PSM2 in hereditary nonpolyposis colorectal cancer (HNPCC, more recently indicated as Lynch syndrome), confer a high risk to develop cancer. Mutation analysis in these genes has resulted in the identification of a large number of sequence variants, of which mutations causing frame shifts and nonsense codons are considered undoubtedly to be pathogenic. Many variants, however, cannot be classified as either disease-causing mutations or neutral variants and are therefore called unclassified variants (UVs). A subset of these variants may have an effect on RNA splicing. Appropriate RNA analysis will enable the characterization of the exact molecular nature of this effect and hence, is essential to determine the clinical relevance of the genomic variant. This chapter describes the design and implementation of RNA analysis as an indispensible tool in today's clinical diagnostic setting.

Published

2012

22. Analysis and Interpretation of RNA Splicing Alterations in Genes Involved in Genetic Disorders

Author

Maaike P.G. Vreeswijk and Heleen M. van der Klift

Subjects

Genetics, MSH6, MSH2, RNA splicing, medicine, Cancer, Biology, medicine.disease, Bioinformatics, MLH1, Gene, Germline, Lynch syndrome

Abstract

Germ line mutations in genes involved in hereditary cancer syndromes, such as BRCA1 and BRCA2 in breast cancer and MSH2, MSH6, MLH1, and PSM2 in hereditary nonpolyposis colorectal cancer (HNPCC, more recently indicated as Lynch syndrome), confer a high risk to develop cancer. Mutation analysis in these genes has resulted in the identification of a large number of sequence variants, of which mutations causing frame shifts and nonsense codons are considered undoubtedly to be pathogenic. Many variants, however, cannot be classified as either disease-causing mutations or neutral variants and are therefore called unclassified variants (UVs). A subset of these variants may have an effect on RNA splicing. Appropriate RNA analysis will enable the characterization of the exact molecular nature of this effect and hence, is essential to determine the clinical relevance of the genomic variant. This chapter describes the design and implementation of RNA analysis as an indispensible tool in today's clinical diagnostic setting.

Published

2012

23. Paediatric intestinal cancer and polyposis due to bi-allelic PMS2 mutations: Case series, review and follow-up guidelines

Author

Robert M.W. Hofstra, Carli M. J. Tops, Jan H. Kleibeuker, Yvonne J. Vos, Heleen M. van der Klift, Maria J W Olderode-Berends, Rolf H. Sijmons, Rene Scheenstra, Frans Peters, Johanna C. Herkert, Hermine E. Veenstra-Knol, Renee C. Niessen, and Arend Karrenbeld

Subjects

Proband, Male, Cancer Research, Pathology, DNA Repair, Base Pair Mismatch, Gastroenterology, PMS2, Child, Mismatch Repair Endonuclease PMS2, Adenosine Triphosphatases, Intestinal Polyposis, Follow-up recommendations, WIRELESS CAPSULE ENDOSCOPY, NONPOLYPOSIS COLORECTAL-CANCER, GERMLINE MUTATIONS, Syndrome, Immunohistochemistry, Constitutional MMR-deficiency syndrome, Lynch syndrome, DNA-Binding Proteins, Oncology, Child, Preschool, HEMATOLOGICAL MALIGNANCY, Female, Microsatellite Instability, Adult, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Adenoma, EARLY-ONSET, LYNCH-SYNDROME, MISMATCH-REPAIR-DEFICIENCY, Familial adenomatous polyposis, Frameshift mutation, Paediatric gastrointestinal cancer, AU-LAIT SPOTS, Germline mutation, Internal medicine, Intestinal Neoplasms, medicine, Humans, Gastrointestinal cancer, Germ-Line Mutation, Family Health, business.industry, medicine.disease, digestive system diseases, DNA Repair Enzymes, TURCOT-SYNDROME, Mutation, Bi-allelic PMS2 mutation, business, Gene Deletion, Follow-Up Studies, Microsatellite Repeats

Abstract

Background Bi-allelic germline mutations of one of the DNA mismatch repair genes, so far predominantly found in PMS2 , cause constitutional MMR-deficiency syndrome. This rare disorder is characterised by paediatric intestinal cancer and other malignancies. We report the clinical, immunohistochemical and genetic characterisation of four families with bi-allelic germline PMS2 mutations. We present an overview of the published gastrointestinal manifestations of CMMR-D syndrome and propose recommendations for gastro-intestinal screening. Methods and Results The first proband developed a cerebral angiosarcoma at age 2 and two colorectal adenomas at age 7. Genetic testing identified a complete PMS2 gene deletion and a frameshift c.736_741delinsTGTGTGTGAAG (p.Pro246CysfsX3) mutation. In the second family, both the proband and her brother had multiple intestinal adenomas, initially wrongly diagnosed as familial adenomatous polyposis. A splice site c.2174+1G>A, and a missense c.137G>T (p.Ser46Ile) mutation in PMS2 were identified. The third patient was diagnosed with multiple colorectal adenomas at age 11; he developed a high-grade dysplastic colorectal adenocarcinoma at age 21. Two intragenic PMS2 deletions were found. The fourth proband developed a cerebral anaplastic ganglioma at age 9 and a high-grade colerectal dysplastic adenoma at age 10 and carries a homozygous c.2174+1G>A mutation. Tumours of all patients showed microsatellite instability and/or loss of PMS2 expression. Conclusions Our findings show the association between bi-allelic germline PMS2 mutations and severe childhood-onset gastrointestinal manifestations, and support the notion that patients with early-onset gastrointestinal adenomas and cancer should be investigated for CMMR-D syndrome. We recommend yearly follow-up with colonoscopy from age 6 and simultaneous video-capsule small bowel enteroscopy from age 8.

Published

2011

24. Novel MLH1 duplication identified in Colombian families with Lynch syndrome

Author

Heleen M. van der Klift, Luis G. Carvajal-Carmona, María Dolores Giráldez, Magdalena Echeverry, Teresa Ocaña, Antoni Castells, Francesc Balaguer, Montserrat Milà, Angela M. Jones, Juul T. Wijnen, Sergi Castellví-Bel, Irene Madrigal, Virginia Alonso-Espinaco, Carlos Gustavo Trujillo, Jenifer Muñoz, Alejandro Vélez, and Ian Tomlinson

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Colombia, Biology, DNA Mismatch Repair, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Antigens, Neoplasm, Gene Duplication, Gene duplication, medicine, Humans, Multiplex ligation-dependent probe amplification, neoplasms, Germ-Line Mutation, Genetics (clinical), Adaptor Proteins, Signal Transducing, Mismatch Repair Endonuclease PMS2, 030304 developmental biology, Amsterdam Criteria II, Adenosine Triphosphatases, Genetics, 0303 health sciences, Nuclear Proteins, Microsatellite instability, nutritional and metabolic diseases, Epithelial Cell Adhesion Molecule, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Immunohistochemistry, Lynch syndrome, digestive system diseases, Pedigree, 3. Good health, DNA-Binding Proteins, MSH6, DNA Repair Enzymes, MutS Homolog 2 Protein, MSH2, 030220 oncology & carcinogenesis, Female, Microsatellite Instability, Colorectal Neoplasms, MutL Protein Homolog 1, Cell Adhesion Molecules

Abstract

Purpose: Lynch syndrome accounts for 2-4% of all colorectal cancer, and is mainly caused by germline mutations in the DNA mismatch repair genes. Our aim was to characterize the genetic mutation responsible for Lynch syndrome in an extensive Colombian family and to study its prevalence in Antioquia. Methods: A Lynch syndrome family fulfilling Amsterdam criteria II was studied by immunohistochemistry and by multiplex ligation-dependent probe amplification (MLPA). Results were confirmed by additional independent MLPA, Southern blotting, and sequencing. Results: Index case tumor immunohistochemistry results were MLH1-, MSH2+, MSH6+, and PMS2-. MLPA analysis detected a duplication of exons 12 and 13 of MLH1. This mutation was confirmed and characterized precisely to span 4219 base pairs. Duplication screening in this family led to the identification of six additional carriers and 13 noncarriers. We also screened 123 early-onset independent colorectal cancer cases from the same area and identified an additional unrelated carrier. CONCLUSION:: A novel duplication of exons 12 and 13 of the MLH1 gene was detected in two independent Lynch syndrome families from Colombia. A putative founder effect and prescreening Lynch syndrome Antioquia families for this specific mutation before thorough mismatch repair mutational screening could be suggested. © 2011 Lippincott Williams and Wilkins.

Published

2011

25. Comprehensive Genetic Analysis of Seven Large Families with Mismatch Repair Proficient Colorectal Cancer

Author

Tom van Wezel, Shantie Jagmohan-Changur, Hans Morreau, Richard S. Houlston, Hans F. A. Vasen, Juul T. Wijnen, Anneke Middeldorp, Emily L. Webb, Jeanine J. Houwing-Duistermaat, Carli M. J. Tops, Marjo van Puijenbroek, Heleen M. van der Klift, and Peter Devilee

Subjects

Adenoma, Adult, Cancer Research, Linkage disequilibrium, DNA Copy Number Variations, Colorectal cancer, Disease, Gene mutation, Biology, DNA Mismatch Repair, Polymorphism, Single Nucleotide, Linkage Disequilibrium, Genetic linkage, Genetics, medicine, Humans, SNP, Aged, Aged, 80 and over, Family Health, Histocytochemistry, Family aggregation, genome-wide association copy number changes chromosomal instability susceptibility locus adenomatous polyposis linkage analysis lynch syndrome neutral loh risk scan, Middle Aged, medicine.disease, digestive system diseases, DNA mismatch repair, Chromosomes, Human, Pair 3, Colorectal Neoplasms

Abstract

Approximately 40% of colorectal cancer (CRC) families with a diagnosis of hereditary nonpolyposis CRC on the basis of clinical criteria are not a consequence of mismatch repair (MMR) deficiency. Such families provide supporting evidence for the existence of a hitherto unidentified highly penetrant gene mutation. To gain further understanding of MMR-competent familial colorectal cancer (FCC), we studied seven large families with an unexplained predisposition for CRC to identify genetic regions that could harbor CRC risk factors. First, we conducted a genome-wide linkage scan using 10K single-nucleotide polymorphism (SNP) arrays to search for disease loci. Second, we studied the genomic profiles of the tumors of affected family members to identify commonly altered genomic regions likely to harbor tumor suppressor genes. Finally, we studied the possible role of recently identified low-risk variants in the familial aggregation of CRC in these families. Linkage analysis did not reveal clear regions of linkage to CRC. However, our results provide support linkage to 3q, a region that has previously been linked to CRC susceptibility. Tumor profiling did not reveal any genomic regions commonly targeted in the tumors studied here. Overall, the genomic profiles of the tumors show some resemblance to sporadic CRC, but additional aberrations were also present. Furthermore, the FCC families did not appear to have an enrichment of low-risk CRC susceptibility loci. These data suggest that factors other than a highly penetrant risk factor, such as low or moderate-penetrance risk factors, may explain the increased cancer risk in a subset of familial CRCs. (C) 2010 Wiley-Liss, Inc.

Published

2010

26. Quantification of Sequence Exchange Events between PMS2 and PMS2CL Provides a Basis for Improved Mutation Scanning of Lynch Syndrome Patients

Author

Anja Wagner, Annette H. J. T. Vriends, Merel W. Boogaard, Angel Alonso, Carli M. J. Tops, Frederik J. Hes, Juul T. Wijnen, Hans F. A. Vasen, Encarna B. Gomez Garcia, Liselotte P. van Hest, Heleen M. van der Klift, Margreet G. E. M. Ausems, Peter Devilee, Hans Morreau, Elsa C. Bik, Louise Izatt, Kerstin Hansson, Anne-Marijke Borgstein, Andrew Green, Wendy A. G. van Zelst-Stams, Clinical sciences, Medical Genetics, Human genetics, CCA - Oncogenesis, Klinische Genetica, Genetica & Celbiologie, and RS: GROW - School for Oncology and Reproduction

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Pseudogene, PMS2 PMS2CL pseudogene Lynch syndrome HNPCC hereditary colorectal-cancer gene conversion hnpcc msh6 pseudogenes defects, HNPCC, Biology, Polymerase Chain Reaction, PMS2CL, Exon, PMS2, Humans, genetics, Genetics(clinical), Multiplex ligation-dependent probe amplification, Gene, Genetics (clinical), Sequence (medicine), Mismatch Repair Endonuclease PMS2, Genetics, Adenosine Triphosphatases, Hereditary cancer and cancer-related syndromes [ONCOL 1], Intron, Molecular biology, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, DNA-Binding Proteins, DNA Repair Enzymes, Lynch syndrome, Case-Control Studies, Mutation (genetic algorithm), Mutation, Pseudogenes

Abstract

Contains fulltext : 89529.pdf (Publisher’s version ) (Closed access) Heterozygous mutations in PMS2 are involved in Lynch syndrome, whereas biallelic mutations are found in Constitutional mismatch repair-deficiency syndrome patients. Mutation detection is complicated by the occurrence of sequence exchange events between the duplicated regions of PMS2 and PMS2CL. We investigated the frequency of such events with a nonspecific polymerase chain reaction (PCR) strategy, co-amplifying both PMS2 and PMS2CL sequences. This allowed us to score ratios between gene and pseudogene-specific nucleotides at 29 PSV sites from exon 11 to the end of the gene. We found sequence transfer at all investigated PSVs from intron 12 to the 3' end of the gene in 4 to 52% of DNA samples. Overall, sequence exchange between PMS2 and PMS2CL was observed in 69% (83/120) of individuals. We demonstrate that mutation scanning with PMS2-specific PCR primers and MLPA probes, designed on PSVs, in the 3' duplicated region is unreliable, and present an RNA-based mutation detection strategy to improve reliability. Using this strategy, we found 19 different putative pathogenic PMS2 mutations. Four of these (21%) are lying in the region with frequent sequence transfer and are missed or called incorrectly as homozygous with several PSV-based mutation detection methods. 01 mei 2010

Published

2010

27. Facioscapulohumeral muscular dystrophy gene in Dutch families is not linked to markers for familial adenomatous polyposis on the long arm of chromosome 5

Author

P. Meera Khan, Rune R. Frants, Oebele F. Brouwer, Cisca Wijmenga, George W. Padberg, and Heleen M. van der Klift

Subjects

Male, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Cosegregation, Genetic Linkage, Facial Muscles, Locus (genetics), Biology, Muscular Dystrophies, Familial adenomatous polyposis, Genetic linkage, medicine, Humans, Facioscapulohumeral muscular dystrophy, Muscular dystrophy, neoplasms, Gene, Netherlands, Genetics, medicine.disease, digestive system diseases, Adenomatous Polyposis Coli, Neurology, Genetic marker, Chromosomes, Human, Pair 5, Female, Neurology (clinical)

Abstract

Cosegregation of facioscapulohumeral muscular dystrophy (FSHD) and familial adenomatous polyposis (FAP) has been described in two small families. The gene for FAP is located on the long arm of chromosome 5. We studied two large Dutch families with FSHD and found no evidence for linkage with gene markers closely linked to FAP. These results strongly suggest that the FSHD gene segregating in the Dutch families is not localized close to the FAP locus on chromosome 5.

Published

1990

28. Molecular characterization of the spectrum of genomic deletions in the mismatch repair genes MSH2, MLH1, MSH6, and PMS2 responsible for hereditary nonpolyposis colorectal cancer (HNPCC)

Author

Pål Møller, Anja Wagner, Carli M. J. Tops, Pierre Hutter, Juul T. Wijnen, Riccardo Fodde, Gabriela Möslein, Daniela Barana, Cristina Oliani, Paul Verkuilen, Hans F. A. Vasen, John Burn, Maija R.J. Kohonen-Corish, Robyn Otway, C. D. DeLozier-Blanchet, Heleen M. van der Klift, William D. Foulkes, Henry T. Lynch, Neurology, Clinical Genetics, and Pathology

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, DNA Repair, Base Pair Mismatch, Alu element, Biology, MLH1, SDG 3 - Good Health and Well-being, Proto-Oncogene Proteins, Genetics, PMS2, Humans, neoplasms, Adaptor Proteins, Signal Transducing, Mismatch Repair Endonuclease PMS2, Adenosine Triphosphatases, Gene Rearrangement, nutritional and metabolic diseases, Nuclear Proteins, Gene rearrangement, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Neoplasm Proteins, Long interspersed nuclear element, MSH6, DNA-Binding Proteins, Blotting, Southern, DNA Repair Enzymes, MutS Homolog 2 Protein, MSH2, Chromosome breakage, Carrier Proteins, MutL Protein Homolog 1, Gene Deletion

Abstract

A systematic search by Southern blot analysis in a cohort of 439 hereditary nonpolyposis colorectal cancer (HNPCC) families for genomic rearrangements in the main mismatch repair (MMR) genes, namely, MSH2, MLH1, MSH6, and PMS2, identified 48 genomic rearrangements causative of this inherited predisposition to colorectal cancer in 68 unrelated kindreds. Twenty-nine of the 48 rearrangements were found in MSH2, 13 in MLH1, 2 in MSH6, and 4 in PMS2. The vast majority were deletions, although one previously described large inversion, an intronic insertion, and a more complex rearrangement also were found. Twenty-four deletion breakpoints have been identified and sequenced in order to determine the underlying recombination mechanisms. Most fall within repetitive sequences, mainly Alu repeats, in agreement with the differential distribution of deletions between the MSH2 and MLH1 genes: the higher number and density of Alu repeats in MSH2 corresponded with a higher incidence of genomic rearrangement at this disease locus when compared with other MMR genes. Long interspersed nuclear element (LINE) repeats, relatively abundant in, for example, MLH1, did not seem to contribute to the genesis of the deletions, presumably because of their older evolutionary age and divergence among individual repeat units when compared with short interspersed nuclear element (SINE) repeats, including Alu repeats. Moreover, Southern blot analysis of the introns and the genomic regions flanking the MMR genes allowed us to detect 6 novel genomic rearrangements that left the coding region of the disease-causing gene intact. These rearrangements comprised 4 deletions upstream of the coding region of MSH2 (3 cases) and MSH6 (1 case), a 2-kb insertion in intron 7 of PMS2, and a small (459-bp) deletion in intron 13 of MLH1. The characterization of these genomic rearrangements underlines the importance of genomic deletions in the etiology of HNPCC and will facilitate the development of PCR-based tests for their detection in diagnostic laboratories.

Published

2005

29. Serrated adenomas and mixed polyposis caused by a splice acceptor deletion in the mouse Smad4 gene

Author

Hans Morreau, Heleen M. van der Klift, Riccardo Fodde, Ron Smits, Lia Molenaar, Peter Devilee, Peter Hohenstein, Ada C Struijk, Gert-Jan B. van Ommen, Shantie Jagmohan-Changur, Henk van Kranen, Cees J. Cornelisse, Joyce Elsinga, Pathology, and Gastroenterology & Hepatology

Subjects

Male, Cancer Research, Candidate gene, Colonic Polyps, Loss of Heterozygosity, Mice, Inbred Strains, Biology, medicine.disease_cause, Frameshift mutation, Cell Line, Loss of heterozygosity, Adenomatous Polyps, Mice, SDG 3 - Good Health and Well-being, Transforming Growth Factor beta, Genetics, medicine, Animals, Fetal Death, Sequence Deletion, Smad4 Protein, Mutation, Splice site mutation, Hyperplasia, Gene Expression Profiling, Homozygote, Null allele, Molecular biology, digestive system diseases, DNA-Binding Proteins, Mice, Inbred C57BL, Disease Models, Animal, Hyperplastic Polyp, Chromosomal region, Trans-Activators, Female, Genes, Lethal, RNA Splice Sites, Colorectal Neoplasms, Signal Transduction

Abstract

Serrated adenomas, hyperplastic polyps, and admixed hyperplastic/adenomatous polyps form a distinct group of colorectal tumors, the molecular genetic basis of which is still poorly understood. We describe a novel mouse model for serrated adenomas and mixed polyposis, here referred to as Sad (serrated adenomas), caused by a spontaneously risen splice site mutation in the murine Smad4 gene. The Sad chromosomal region was identified by genetic linkage and loss of heterozygosity (LOH) analysis. Subsequently, several candidate genes were investigated by expression and mutation analysis. By use of genetic linkage and LOH analysis, we mapped the Sad candidate to mouse chromosome 18, 44 – 48 cM, syntenic to human chromosome band 18q21. Within this chromosomal interval, the Smad2, Smad4, and Smad7 genes were analyzed for the presence of a disease-causing mutation in affected animals. A single nucleotide (nt) deletion was identified in the intron 5/exon 6 splice acceptor site of the Smad4 gene. The single base deletion results in a frameshift and an early termination codon through activation of a cryptic splice site 4 nt downstream in exon 6. The resulting mRNA is unstable, and the Sad mutation is thus likely to represent a null allele. Identification of a Smad4 mutation in the Sad mouse model provides further support for the involvement of the Smad genes, and thus the TGFB pathway, in the serrated/hyperplastic route to colorectal cancer. © 2003 Wiley-Liss, Inc.

Published

2003

30. A 10-Mb paracentric inversion of chromosome arm 2p inactivates MSH2 and is responsible for hereditary nonpolyposis colorectal cancer in a North-American kindred

Author

Vladimir Bezrookove, Patrick Franken, Ron Smits, Henry T. Lynch, Riccardo Fodde, Barbara Franklin, Juul T. Wijnen, Cor Breukel, Anja Wagner, Yulia Kinarsky, Heleen M. van der Klift, Jane F. Lynch, Alicia Barrows, Clinical Genetics, and Neurology

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Locus (genetics), Biology, Hybrid Cells, Polymerase Chain Reaction, Mice, SDG 3 - Good Health and Well-being, Proto-Oncogene Proteins, Genetics, Missense mutation, Animals, Humans, Gene Silencing, Allele, neoplasms, In Situ Hybridization, Fluorescence, Southern blot, Chromosomal inversion, Aged, Adenosine Triphosphatases, Contig, Point mutation, Gene Expression Profiling, nutritional and metabolic diseases, Middle Aged, Molecular biology, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Pedigree, DNA-Binding Proteins, Blotting, Southern, MutS Homolog 2 Protein, MSH2, Chromosomes, Human, Pair 2, Chromosome Inversion, Cytogenetic Analysis, Female

Abstract

Genomic deletions of the MSH2 gene are a frequent cause of hereditary nonpolyposis colorectal cancer (HNPCC), a common hereditary predisposition to the development of tumors in several organs including the gastrointestinal and urinary tracts and endometrium. The mutation spectrum at the MSH2 gene is extremely heterogeneous because it includes nonsense and missense point mutations, small insertions and deletions leading to frameshifts, and larger genomic deletions, the latter representing approximately 25% of the total mutation burden. Here, we report the identification and molecular characterization of the first paracentric inversion of the MSH2 locus known to cause HNPCC. Southern blot analysis and inverse PCR showed that the centromeric and telomeric breakpoints of the paracentric inversion map within intron 7 and to a contig 10 Mb 3' of MSH2, respectively. Pathogenicity of the paracentric inversion was demonstrated by conversion analysis. The patient's lymphocytes were employed to generate somatic cell hybrids to analyze the expression of the inverted MSH2 allele in an Msh2-deficient rodent cellular background. The inversion was shown to abolish MSH2 expression by both northern and western analysis. This study confirms that Southern blot analysis still represents a useful and informative tool to screen for and identify complex genomic rearrangements in HNPCC. Moreover, monoallelic expression analysis represents an attractive approach to demonstrate pathogenicity of unusual mutations in autosomal dominant hereditary conditions.

Published

2002

31. Hereditary nonpolyposis colorectal cancer families not complying with the Amsterdam criteria show extremely low frequency of mismatch-repair-gene mutations

Author

Heleen M. van der Klift, Bert Bakker, Monique Losekoot, Riccardo Fodde, Juul T. Wijnen, Pål Møller, Hans F. A. Vasen, Inge van Leeuwen-Cornelisse, Adri Mulder, and P. Meera Khan

Subjects

Amsterdam criteria, congenital, hereditary, and neonatal diseases and abnormalities, Protein Denaturation, DNA Repair, Colorectal cancer, Denmark, Biology, Gene mutation, medicine.disease_cause, Germline mutation, Proto-Oncogene Proteins, Genetics, medicine, Humans, Genetics(clinical), Genetics (clinical), Germ-Line Mutation, Genetic testing, Adaptor Proteins, Signal Transducing, Czech Republic, Netherlands, Mutation, medicine.diagnostic_test, Nucleic Acid Heteroduplexes, Microsatellite instability, nutritional and metabolic diseases, Nuclear Proteins, Reference Standards, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, digestive system diseases, Neoplasm Proteins, DNA-Binding Proteins, MutS Homolog 2 Protein, Italy, Case-Control Studies, DNA mismatch repair, Electrophoresis, Polyacrylamide Gel, Carrier Proteins, MutL Protein Homolog 1, Research Article, Microsatellite Repeats

Abstract

SummaryHereditary nonpolyposis colorectal cancer (HNPCC) is a common autosomal dominant cancer-susceptibility condition characterized by early onset colorectal cancer. Germ-line mutations in one of four DNA mismatch repair (MMR) genes, hMSH2, hMLH1, hPMS1, or hPMS2, are known to cause HNPCC. Although many mutations in these genes have been found in HNPCC kindreds complying with the so-called Amsterdam criteria, little is known about the involvement of these genes in families not satisfying these criteria but showing clear-cut familial clustering of colorectal cancer and other cancers. Here, we applied denaturing gradient-gel electrophoresis to screen for hMSH2 and hMLH1 mutations in two sets of HNPCC families, one set comprising families strictly complying with the Amsterdam criteria and another set in which at least one of the criteria was not satisfied. Interestingly, hMSH2 and hMLH1 mutations were found in 49% of the kindreds fully complying with the Amsterdam criteria, whereas a disease-causing mutation could be identified in only 8% of the families in which the criteria were not satisfied fully. In correspondence with these findings, 4 of 6 colorectal tumors from patients belonging to kindreds meeting the criteria showed microsat-ellite instability, whereas only 3 of 11 tumors from the other set of families demonstrated this instability. Although the number of tumors included in the study admittedly is small, the frequencies of mutations in the MMR genes show obvious differences between the two clinical sets of families. These results also emphasize the practical importance of the Amsterdam criteria, which provide a valid clinical subdivision between families, on the basis of their chance of carrying an hMSH2 or an hMLH1 mutation, and which bear important consequences for genetic testing and counseling and for the management of colorectal cancer families.

Published

1997

32. Spectrum of genetic alterations in Muir-Torre syndrome is the same as in HNPCC

Author

Juul T. Wijnen, Riccardo Fodde, Daniela Barana, Paolo Radice, Cristina Oliani, Heleen M. van der Klift, Elena Dalla Longa, and Gian Luigi Cetto

Subjects

Adult, Male, Muir–Torre syndrome, Neoplastic Syndromes, Hereditary, Proto-Oncogene Proteins, Humans, Medicine, Nuclear protein, Genetics (clinical), Adaptor Proteins, Signal Transducing, Genetics, MutS Homolog 2 Protein, business.industry, Nuclear Proteins, Signal transducing adaptor protein, Middle Aged, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Neoplasm Proteins, Pedigree, DNA-Binding Proteins, Carrier protein, Mutation, Female, Carrier Proteins, MutL Protein Homolog 1, business

Published

2004

33. Eight novel inactivating germ line mutations at the APC gene identified by denaturing gradient gel electrophoresis

Author

Carli M. J. Tops, Hans F. A. Vasen, Riccardo Fodde, Gerrit Griffioen, Juul T. Wijnen, Heleen M. van der Klift, Rob B. van der Luijt, P. Meera Khan, and Inge van Leeuwen-Cornelisse

Subjects

Male, Adenomatous polyposis coli, Genetic Linkage, Molecular Sequence Data, Familial adenomatous polyposis, Exon, Genetics, medicine, Humans, Gene, Polymorphism, Genetic, biology, Base Sequence, Point mutation, Nucleic Acid Heteroduplexes, DNA, Exons, medicine.disease, Molecular biology, Stop codon, Pedigree, Adenomatous Polyposis Coli, Mutation, biology.protein, Electrophoresis, Polyacrylamide Gel, Female, Restriction fragment length polymorphism, Temperature gradient gel electrophoresis

Abstract

Familial adenomatous polyposis (FAP) is a dominantly inherited condition predisposing to colorectal cancer. The recent isolation of the responsible gene (adenomatous polyposis coli or APC) has facilitated the search for germ line mutations in affected individuals. Previous authors have used the RNase protection assay and the single-strand conformation polymorphisms procedure to screen for mutations. In this study we used denaturing gradient gel electrophoresis (DGGE). DGGE analysis of 10 APC exons (4, 5, 7, 8, 9, 10, 12, 13, 14, and part of 15) in 33 unrelated Dutch FAP patients has led to the identification of eight novel germ line mutations resulting in stop codons or frameshifts. The results reported here indicate that (1) familial adenomatous polyposis is caused by an extremely heterogeneous spectrum of point mutations; (2) all the mutations found in this study are chain terminating; and (3) DGGE represents a rapid and sensitive technique for the detection of mutations in the unusually large APC gene. An extension of the DGGE analysis to the entire coding region in a sufficient number of clinically well-characterized, unrelated patients will facilitate the establishment of genotype-phenotype correlations. On the other hand, the occurrence of an extremely heterogeneous spectrum of mutations spread throughout the entire length of the large APC gene among the FAP patients indicates that this approach may not be useful as a rapid presymptomatic diagnostic procedure in a routine laboratory. Nevertheless, the above DGGE approach has incidentally led to the identification of a common polymorphism in exon 13. Such intragenic polymorphisms offer a practical approach to a more rapid procedure for presymptomatic diagnosis of FAP by linkage analysis in informative families.

Published

1992

34. A procedure for the detection of linkage with high density SNP arrays in a large pedigree with colorectal cancer

Author

Quinta Helmer, Tom van Wezel, Peter Devilee, Hans Morreau, Shantie Jagmohan-Changur, Hans F. A. Vasen, Juul T. Wijnen, Jeanine J. Houwing-Duistermaat, Carli M. J. Tops, Anneke Middeldorp, and Heleen M. van der Klift

Subjects

Quality Control, Cancer Research, Genotype, Single-nucleotide polymorphism, Pedigree chart, Biology, lcsh:RC254-282, Polymorphism, Single Nucleotide, Linkage Disequilibrium, Genetic linkage, Genetics, SNP, Humans, Genetic Predisposition to Disease, Genotyping, Germ-Line Mutation, Adaptor Proteins, Signal Transducing, Oligonucleotide Array Sequence Analysis, Linkage (software), Nuclear Proteins, Tag SNP, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, SNP genotyping, Pedigree, Oncology, Carrier Proteins, Colorectal Neoplasms, MutL Protein Homolog 1, Research Article

Abstract

Background The apparent dominant model of colorectal cancer (CRC) inheritance in several large families, without mutations in known CRC susceptibility genes, suggests the presence of so far unidentified genes with strong or moderate effect on the development of CRC. Linkage analysis could lead to identification of susceptibility genes in such families. In comparison to classical linkage analysis with multi-allelic markers, single nucleotide polymorphism (SNP) arrays have increased information content and can be processed with higher throughput. Therefore, SNP arrays can be excellent tools for linkage analysis. However, the vast number of SNPs on the SNP arrays, combined with large informative pedigrees (e.g. >35–40 bits), presents us with a computational complexity that is challenging for existing statistical packages or even exceeds their capacity. We therefore setup a procedure for linkage analysis in large pedigrees and validated the method by genotyping using SNP arrays of a colorectal cancer family with a known MLH1 germ line mutation. Methods Quality control of the genotype data was performed in Alohomora, Mega2 and SimWalk2, with removal of uninformative SNPs, Mendelian inconsistencies and Mendelian consistent errors, respectively. Linkage disequilibrium was measured by SNPLINK and Merlin. Parametric linkage analysis using two flanking markers was performed using MENDEL. For multipoint parametric linkage analysis and haplotype analysis, SimWalk2 was used. Results On chromosome 3, in the MLH1-region, a LOD score of 1.9 was found by parametric linkage analysis using two flanking markers. On chromosome 11 a small region with LOD 1.1 was also detected. Upon linkage disequilibrium removal, multipoint linkage analysis yielded a LOD score of 2.1 in the MLH1 region, whereas the LOD score dropped to negative values in the region on chromosome 11. Subsequent haplotype analysis in the MLH1 region perfectly matched the mutation status of the family members. Conclusion We developed a workflow for linkage analysis in large families using high-density SNP arrays and validated this workflow in a family with colorectal cancer. Linkage disequilibrium has to be removed when using SNP arrays, because it can falsely inflate the LOD score. Haplotype analysis is adequate and can predict the carrier status of the family members.

35. Cancer Risks for PMS2-Associated Lynch Syndrome.

Author

Ten Broeke SW, van der Klift HM, Tops CMJ, Aretz S, Bernstein I, Buchanan DD, de la Chapelle A, Capella G, Clendenning M, Engel C, Gallinger S, Gomez Garcia E, Figueiredo JC, Haile R, Hampel HL, Hopper JL, Hoogerbrugge N, von Knebel Doeberitz M, Le Marchand L, Letteboer TGW, Jenkins MA, Lindblom A, Lindor NM, Mensenkamp AR, Møller P, Newcomb PA, van Os TAM, Pearlman R, Pineda M, Rahner N, Redeker EJW, Olderode-Berends MJW, Rosty C, Schackert HK, Scott R, Senter L, Spruijt L, Steinke-Lange V, Suerink M, Thibodeau S, Vos YJ, Wagner A, Winship I, Hes FJ, Vasen HFA, Wijnen JT, Nielsen M, and Win AK

Subjects

Adult, Aged, Female, Heterozygote, Humans, Male, Middle Aged, Mutation, Colorectal Neoplasms, Hereditary Nonpolyposis genetics, Mismatch Repair Endonuclease PMS2 genetics, Neoplasms epidemiology, Neoplasms genetics, Penetrance

Abstract

Purpose: Lynch syndrome due to pathogenic variants in the DNA mismatch repair genes MLH1, MSH2, and MSH6 is predominantly associated with colorectal and endometrial cancer, although extracolonic cancers have been described within the Lynch tumor spectrum. However, the age-specific cumulative risk (penetrance) of these cancers is still poorly defined for PMS2-associated Lynch syndrome. Using a large data set from a worldwide collaboration, our aim was to determine accurate penetrance measures of cancers for carriers of heterozygous pathogenic PMS2 variants., Methods: A modified segregation analysis was conducted that incorporated both genotyped and nongenotyped relatives, with conditioning for ascertainment to estimates corrected for bias. Hazard ratios (HRs) and corresponding 95% CIs were estimated for each cancer site for mutation carriers compared with the general population, followed by estimation of penetrance., Results: In total, 284 families consisting of 4,878 first- and second-degree family members were included in the analysis. PMS2 mutation carriers were at increased risk for colorectal cancer (cumulative risk to age 80 years of 13% [95% CI, 7.9% to 22%] for males and 12% [95% CI, 6.7% to 21%] for females) and endometrial cancer (13% [95% CI, 7.0%-24%]), compared with the general population (6.6%, 4.7%, and 2.4%, respectively). There was no clear evidence of an increased risk of ovarian, gastric, hepatobiliary, bladder, renal, brain, breast, prostate, or small bowel cancer., Conclusion: Heterozygous PMS2 mutation carriers were at small increased risk for colorectal and endometrial cancer but not for any other Lynch syndrome-associated cancer. This finding justifies that PMS2-specific screening protocols could be restricted to colonoscopies. The role of risk-reducing hysterectomy and bilateral salpingo-oophorectomy for PMS2 mutation carriers needs further discussion.

Published

2018

36. Lynch syndrome caused by germline PMS2 mutations: delineating the cancer risk.

Author

ten Broeke SW, Brohet RM, Tops CM, van der Klift HM, Velthuizen ME, Bernstein I, Capellá Munar G, Gomez Garcia E, Hoogerbrugge N, Letteboer TG, Menko FH, Lindblom A, Mensenkamp AR, Moller P, van Os TA, Rahner N, Redeker BJ, Sijmons RH, Spruijt L, Suerink M, Vos YJ, Wagner A, Hes FJ, Vasen HF, Nielsen M, and Wijnen JT

Subjects

Adult, Aged, Aged, 80 and over, Cohort Studies, Colorectal Neoplasms genetics, DNA Mutational Analysis, Endometrial Neoplasms genetics, Family Health, Female, Gene Frequency, Genotype, Humans, Male, Middle Aged, Mismatch Repair Endonuclease PMS2, Risk Factors, Adenosine Triphosphatases genetics, Colorectal Neoplasms, Hereditary Nonpolyposis genetics, DNA Repair Enzymes genetics, DNA-Binding Proteins genetics, Genetic Predisposition to Disease genetics, Germ-Line Mutation

Abstract

Purpose: The clinical consequences of PMS2 germline mutations are poorly understood compared with other Lynch-associated mismatch repair gene (MMR) mutations. The aim of this European cohort study was to define the cancer risk faced by PMS2 mutation carriers., Methods: Data were collected from 98 PMS2 families ascertained from family cancer clinics that included a total of 2,548 family members and 377 proven mutation carriers. To adjust for potential ascertainment bias, a modified segregation analysis model was used to calculate colorectal cancer (CRC) and endometrial cancer (EC) risks. Standardized incidence ratios (SIRs) were calculated to estimate risks for other Lynch syndrome-associated cancers., Results: The cumulative risk (CR) of CRC for male mutation carriers by age 70 years was 19%. The CR among female carriers was 11% for CRC and 12% for EC. The mean age of CRC development was 52 years, and there was a significant difference in mean age of CRC between the probands (mean, 47 years; range, 26 to 68 years) and other family members with a PMS2 mutation (mean, 58 years; range, 31 to 86 years; P < .001). Significant SIRs were observed for cancers of the small bowel, ovaries, breast, and renal pelvis., Conclusion: CRC and EC risks were found to be markedly lower than those previously reported for the other MMR. However, these risks embody the isolated risk of carrying a PMS2 mutation, and it should be noted that we observed a substantial variation in cancer phenotype within and between families, suggesting the influence of genetic modifiers and lifestyle factors on cancer risks., (© 2014 by American Society of Clinical Oncology.)

Published

2015