Your search keyword '"Katharina Wimmer"' showing total 122 results

1. Constitutional mismatch repair deficiency mimicking Lynch syndrome is associated with hypomorphic mismatch repair gene variants

Author

Richard Gallon, Carlijn Brekelmans, Marie Martin, Vincent Bours, Esther Schamschula, Albert Amberger, Martine Muleris, Chrystelle Colas, Jeroen Dekervel, Gert De Hertogh, Jérôme Coupier, Orphal Colleye, Edith Sepulchre, John Burn, Hilde Brems, Eric Legius, and Katharina Wimmer

Subjects

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

Abstract

Abstract Lynch syndrome (LS) and constitutional mismatch repair deficiency (CMMRD) are distinct cancer syndromes caused, respectively, by mono- and bi-allelic germline mismatch repair (MMR) variants. LS predisposes to mainly gastrointestinal and genitourinary cancers in adulthood. CMMRD predisposes to brain, haematological, and LS-spectrum cancers from childhood. Two suspected LS patients with first cancer diagnosis aged 27 or 38 years were found to be homozygous for an MMR (likely) pathogenic variant, MSH6 c.3226C>T (p.(Arg1076Cys)), or variant of uncertain significance (VUS), MLH1 c.306G>A (p.(Glu102=)). MLH1 c.306G>A was shown to cause leaky exon 3 skipping. The apparent genotype-phenotype conflict was resolved by detection of constitutional microsatellite instability in both patients, a hallmark feature of CMMRD. A hypomorphic effect of these and other variants found in additional late onset CMMRD cases, identified by literature review, likely explains a LS-like phenotype. CMMRD testing in carriers of compound heterozygous or homozygous MMR VUS may find similar cases and novel hypomorphic variants. Individualised management of mono- and bi-allelic carriers of hypomorphic MMR variants is needed until we better characterise the associated phenotypes.

Published

2024

2. LinkedSV for detection of mosaic structural variants from linked-read exome and genome sequencing data

Author

Li Fang, Charlly Kao, Michael V. Gonzalez, Fernanda A. Mafra, Renata Pellegrino da Silva, Mingyao Li, Sören-Sebastian Wenzel, Katharina Wimmer, Hakon Hakonarson, and Kai Wang

Subjects

Science

Abstract

Compared to single nucleotide variants and short indels, structural variants (SVs) are often more challenging to detect using high-throughput sequencing based methods. Here, the authors develop LinkedSV, a computational tool for SV detection using linked-read exome and genome sequencing data.

Published

2019

3. Teenage-Onset Colorectal Cancers in a Digenic Cancer Predisposition Syndrome Provide Clues for the Interaction between Mismatch Repair and Polymerase δ Proofreading Deficiency in Tumorigenesis

Author

Esther Schamschula, Miriam Kinzel, Annekatrin Wernstedt, Klaus Oberhuber, Hendrik Gottschling, Simon Schnaiter, Nicolaus Friedrichs, Sabine Merkelbach-Bruse, Johannes Zschocke, Richard Gallon, and Katharina Wimmer

Subjects

digenic, colorectal cancer (CRC) in adolescents and young adults (AYA), POL-LYNCH, Lynch syndrome (LS), polymerase proofreading (PP), Pol δ, Microbiology, QR1-502

Abstract

Colorectal cancer (CRC) in adolescents and young adults (AYA) is very rare. Known predisposition syndromes include Lynch syndrome (LS) due to highly penetrant MLH1 and MSH2 alleles, familial adenomatous polyposis (FAP), constitutional mismatch-repair deficiency (CMMRD), and polymerase proofreading-associated polyposis (PPAP). Yet, 60% of AYA-CRC cases remain unexplained. In two teenage siblings with multiple adenomas and CRC, we identified a maternally inherited heterozygous PMS2 exon 12 deletion, NM_000535.7:c.2007-786_2174+493del1447, and a paternally inherited POLD1 variant, NP_002682.2:p.Asp316Asn. Comprehensive molecular tumor analysis revealed ultra-mutation (>100 Mut/Mb) and a large contribution of COSMIC signature SBS20 in both siblings’ CRCs, confirming their predisposition to AYA-CRC results from a high propensity for somatic MMR deficiency (MMRd) compounded by a constitutional Pol δ proofreading defect. COSMIC signature SBS20 as well as SBS26 in the index patient’s CRC were associated with an early mutation burst, suggesting MMRd was an early event in tumorigenesis. The somatic second hits in PMS2 were through loss of heterozygosity (LOH) in both tumors, suggesting PPd-independent acquisition of MMRd. Taken together, these patients represent the first cases of cancer predisposition due to heterozygous variants in PMS2 and POLD1. Analysis of their CRCs supports that POLD1-mutated tumors acquire hypermutation only with concurrent MMRd.

Published

2022

4. No Overt Clinical Immunodeficiency Despite Immune Biological Abnormalities in Patients With Constitutional Mismatch Repair Deficiency

Author

Victoria K. Tesch, Hanna IJspeert, Andrea Raicht, Daniel Rueda, Nerea Dominguez-Pinilla, Luis M. Allende, Chrystelle Colas, Thorsten Rosenbaum, Denisa Ilencikova, Hagit N. Baris, Michaela H. M. Nathrath, Manon Suerink, Danuta Januszkiewicz-Lewandowska, Iman Ragab, Amedeo A. Azizi, Soeren S. Wenzel, Johannes Zschocke, Wolfgang Schwinger, Matthias Kloor, Claudia Blattmann, Laurence Brugieres, Mirjam van der Burg, Katharina Wimmer, and Markus G. Seidel

Subjects

primary immunodeficiency, hyper-IgM syndrome, DNA repair defect, mismatch repair, somatic hypermutation, class-switch recombination, Immunologic diseases. Allergy, RC581-607

Abstract

Immunoglobulin class-switch recombination (CSR) and somatic hypermutations (SHMs) are prerequisites for antibody and immunoglobulin receptor maturation and adaptive immune diversity. The mismatch repair (MMR) machinery, consisting of homologs of MutSα, MutLα, and MutSβ (MSH2/MSH6, MLH1/PMS2, and MSH2/MSH3, respectively) and other proteins, is involved in CSR, primarily acting as a backup for nonhomologous end-joining repair of activation-induced cytidine deaminase-induced DNA mismatches and, furthermore, in addition to error-prone polymerases, in the repair of SHM-induced DNA breaks. A varying degree of antibody formation defect, from IgA or selective IgG subclass deficiency to common variable immunodeficiency and hyper-IgM syndrome, has been detected in a small number of patients with constitutional mismatch repair deficiency (CMMRD) due to biallelic loss-of-function mutations in one of the MMR genes (PMS2, MSH6, MLH1, or MSH2). To elucidate the clinical relevance of a presumed primary immunodeficiency (PID) in CMMRD, we systematically collected clinical history and laboratory data of a cohort of 15 consecutive, unrelated patients (10 not previously reported) with homozygous/compound heterozygous mutations in PMS2 (n = 8), MSH6 (n = 5), and MLH1 (n = 2), most of whom manifested with typical malignancies during childhood. Detailed descriptions of their genotypes, phenotypes, and family histories are provided. Importantly, none of the patients showed any clinical warning signs of PID (infections, immune dysregulation, inflammation, failure to thrive, etc.). Furthermore, we could not detect uniform or specific patterns of laboratory abnormalities. The concentration of IgM was increased in 3 out of 12, reduced in 3 out of 12, and normal in 6 out of 12 patients, while concentrations of IgG and IgG subclasses, except IgG4, and of IgA, and specific antibody formation were normal in most. Class-switched B memory cells were reduced in 5 out of 12 patients, and in 9 out of 12 also the CD38hiIgM− plasmablasts were reduced. Furthermore, results of next generation sequencing-based analyses of antigen-selected B-cell receptor rearrangements showed a significantly reduced frequency of SHM and an increased number of rearranged immunoglobulin heavy chain (IGH) transcripts that use IGHG3, IGHG1, and IGHA1 subclasses. T cell subsets and receptor repertoires were unaffected. Together, neither clinical nor routine immunological laboratory parameters were consistently suggestive of PID in these CMMRD patients, but previously shown abnormalities in SHM and rearranged heavy chain transcripts were confirmed.

Published

2018

5. N-myc Modulates Expression of p73 in Neuroblastoma

Author

Xiaoxiang Zhu, Katharina Wimmer, Rork Kuick, Barbara J. Lamb, Stephanie Motyka, Rama Jasty, Valerie P. Castle, and Samir M. Hanash

Subjects

demoblastoma, N-myq p73, amplification, chromosome 1p36, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The human p73 gene is a homolog of p53, which has been localized to chromosome 1p36 in a region that is frequently deleted in neuroblastoma. Transfection of the p73 gene into neuroblastoma cells that lack detectable p73 protein has been shown to result in growth suppression and to induce neuronal differentiation. In this study, we have identified by means of restriction landmark genome scanning. (RLGS) a genomic fragment that was frequently reduced in intensity in neuroblastomas. The cloned fragment contained exon 1 of p73 as well as intronic and promoter sequences. We investigated the genomic and expression status of p73 and N-myc in 34 neuroblastoma tumors and 12 neuroblastoma cell lines. Approximately a third of neuroblastomas in our series exhibited deletion of p73. Most tumors analyzed exhibited reduced expression of p73, as determined by quantitative RT-PCR, in the absence of detectable p73 gene deletion. The reduced expression of p73 correlated with overexpression of N-myc in a statistically significant manner. The N-myc gene was transfected into two neuroblastoma cell lines that lacked N-myc amplification to determine its effect on p73 RNA levels. p73 was detectable at low level by RTPCR in untransfected SK-N-AS cells and became undetectable following N-myc transfection, whereas in SH-EP1 cells, p73 levels were substantially reduced following transfection but remained detectable. Our data suggest that the N-myc gene modulates expression of p73, allowing neuroblastoma cells to escape the growth suppressing properties of p73.

Published

2002

6. The NF1 gene contains hotspots for L1 endonuclease-dependent de novo insertion.

Author

Katharina Wimmer, Tom Callens, Annekatrin Wernstedt, and Ludwine Messiaen

Subjects

Genetics, QH426-470

Abstract

Long interspersed (L1) and Alu elements are actively amplified in the human genome through retrotransposition of their RNA intermediates by the -100 still retrotranspositionally fully competent L1 elements. Retrotransposition can cause inherited disease if such an element is inserted near or within a functional gene. Using direct cDNA sequencing as the primary assay for comprehensive NF1 mutation analysis, we uncovered in 18 unrelated index patients splicing alterations not readily explained at the genomic level by an underlying point-mutation or deletion. Improved PCR protocols avoiding allelic drop-out of the mutant alleles uncovered insertions of fourteen Alu elements, three L1 elements, and one poly(T) stretch to cause these splicing defects. Taken together, the 18 pathogenic L1 endonuclease-mediated de novo insertions represent the largest number of this type of mutations characterized in a single human gene. Our findings show that retrotransposon insertions account for as many as -0.4% of all NF1 mutations. Since altered splicing was the main effect of the inserted elements, the current finding was facilitated by the use of RNA-based mutation analysis protocols, resulting in improved detection compared to gDNA-based approaches. Six different insertions clustered in a relatively small 1.5-kb region (NF1 exons 21(16)-23(18)) within the 280-kb NF1 gene. Furthermore, three different specific integration sites, one of them located in this cluster region, were each used twice, i.e. NM_000267.3(NF1):c.1642-1_1642 in intron 14(10c), NM_000267.3(NF1):c.2835_2836 in exon 21(16), and NM_000267.3(NF1):c.4319_4320 in exon 33(25). Identification of three loci that each served twice as integration site for independent retrotransposition events as well as 1.5-kb cluster region harboring six independent insertions supports the notion of non-random insertion of retrotransposons in the human genome. Currently, little is known about which features make sites particularly vulnerable to L1 EN-mediated insertions. The here identified integration sites may serve to elucidate these features in future studies.

Published

2011

7. Constitutional mismatch repair-deficiency syndrome

Author

Katharina Wimmer and Christian P. Kratz

Subjects

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

Published

2010

8. Detection of constitutional mismatch repair deficiency in children and adolescents with acute lymphoblastic leukemia

Author

Richard, Gallon, Rachel, Phelps, Leigh, Betts, Christine, Hayes, Dino, Masic, Julie A E, Irving, Ciaron, McAnulty, Vaskar, Saha, Ajay, Vora, Katharina, Wimmer, Jayashree, Motwani, Christine, Macartney, John, Burn, Michael S, Jackson, Anthony V, Moorman, and Mauro, Santibanez-Koref

Subjects

Cancer Research, Oncology, Hematology

Published

2022

9. Updated diagnostic criteria and nomenclature for neurofibromatosis type 2 and schwannomatosis

Author

Scott R. Plotkin, Ludwine Messiaen, Eric Legius, Patrice Pancza, Robert A. Avery, Jaishri O. Blakeley, Dusica Babovic-Vuksanovic, Rosalie Ferner, Michael J. Fisher, Jan M. Friedman, Marco Giovannini, David H. Gutmann, Clemens Oliver Hanemann, Michel Kalamarides, Hildegard Kehrer-Sawatzki, Bruce R. Korf, Victor-Felix Mautner, Mia MacCollin, Laura Papi, Katherine A. Rauen, Vincent Riccardi, Elizabeth Schorry, Miriam J. Smith, Anat Stemmer-Rachamimov, David A. Stevenson, Nicole J. Ullrich, David Viskochil, Katharina Wimmer, Kaleb Yohay, Susan M. Huson, Pierre Wolkenstein, D. Gareth Evans, Monique Anten, Arthur Aylsworth, Diana Baralle, Sebastien Barbarot, Fred Barker, Shay Ben-Shachar, Amanda Bergner, Didier Bessis, Ignacio Blanco, Catherine Cassiman, Patricia Ciavarelli, Maurizio Clementi, Thierry Frébourg, Alicia Gomes, Dorothy Halliday, Chris Hammond Helen Hanson Arvid Heiberg, Pascal Joly, Justin T. Jordan, Matthias Karajannis, Daniela Kroshinsky, Margarita Larralde, Conxi Lázaro, Lu Le, Michael Link, Robert Listernick, Conor Mallucci, Vanessa L. Merker, Christopher Moertel, Amy Mueller, Joanne Ngeow, Rianne Oostenbrink, Roger Packer, Allyson Parry, Juha Peltonen, Dominique Pichard, Bruce Poppe, Nilton Rezende, Luiz Oswaldo Rodrigues, Tena Rosser, Martino Ruggieri, Eduard Serra, Verena Steinke-Lange, Stavros Michael Stivaros, Amy Taylor, Jaan Toelen, James Tonsgard, Eva Trevisson, Meena Upadhyaya, Ali Varan, Meredith Wilson, Hao Wu, Gelareh Zadeh, and Pediatrics

Subjects

Neurofibromatosis 2, Consensus, Neurofibromatosis 1, Skin Neoplasms, Neurofibromatoses, NF2, Neurofibromatosis, SMARCB1, Schwannomatosis, lztr1, Humans, Genetics (clinical), Neurilemmoma

Abstract

PURPOSE: Neurofibromatosis type 2 (NF2) and schwannomatosis (SWN) are genetically distinct tumor predisposition syndromes with overlapping phenotypes. We sought to update the diagnostic criteria for NF2 and SWN by incorporating recent advances in genetics, ophthalmology, neuropathology, and neuroimaging. METHODS: We used a multistep process, beginning with a Delphi method involving global disease experts and subsequently involving non-neurofibromatosis clinical experts, patients, and foundations/patient advocacy groups. RESULTS: We reached consensus on the minimal clinical and genetic criteria for diagnosing NF2 and SWN. These criteria incorporate mosaic forms of these conditions. In addition, we recommend updated nomenclature for these disorders to emphasize their phenotypic overlap and to minimize misdiagnosis with neurofibromatosis type 1. CONCLUSION: The updated criteria for NF2 and SWN incorporate clinical features and genetic testing, with a focus on using molecular data to differentiate the 2 conditions. It is likely that continued refinement of these new criteria will be necessary as investigators study the diagnostic properties of the revised criteria and identify new genes associated with SWN. In the revised nomenclature, the term "neurofibromatosis 2" has been retired to improve diagnostic specificity. ispartof: GENETICS IN MEDICINE vol:24 issue:9 pages:1967-1977 ispartof: location:United States status: published

Published

2022

10. Analysis of 200 unrelated individuals with a constitutional NF1 deep intronic pathogenic variant reveals that variants flanking the alternatively spliced NF1 exon 31 [23a] cause a classical neurofibromatosis type 1 phenotype while altering predominantly NF1 isoform type II

Author

Magdalena Koczkowska, Yunjia Chen, Jing Xie, Tom Callens, Alicia Gomes, Katharina Wimmer, and Ludwine M. Messiaen

Subjects

Genetics, Genetics (clinical)

Abstract

Neurofibromatosis type 1 results from loss-of-function NF1 pathogenic variants (PVs). Up to 30% of all NF1 PVs disrupt mRNA splicing, including deep intronic variants. Here, we retrospectively investigated the spectrum of NF1 deep intronic PVs in a cohort of 8,090 unrelated individuals from the University of Alabama at Birmingham (UAB) dataset with a molecularly confirmed neurofibromatosis type 1. All variants were identified through their effect on the NF1 transcript, followed by variant characterization at the DNA-level. A total of 68 distinct variants, which were ≥ 20 nucleotides away from the closest exon–intron junction, were identified in 2.5% unrelated individuals with NF1 (200/8,090). Nine different pathogenic splice variants, identified in 20 probands, led to exonization of different parts of intron 30 [23.2] or 31 [23a]. The two major NF1 transcript isoforms, distinguished by the absence (type I) or presence (type II) of the alternatively spliced cassette exon 31 [23a], are equally expressed in blood in control individuals without NF1 or NF1-affected individuals carrying their PV not in the introns flanking exon 31 [23a]. By fragment and cloning analysis we demonstrated that the exonization of intron 31 [23a] sequences due to deep intronic PV predominantly affects the NF1 isoform II. Seven additional (likely) pathogenic NF1 deep intronic variants not observed in the UAB dataset were found by classification of 36 variants identified by a literature search. Hence, the unique list of these 75 deep intronic (likely) PVs should be included in any comprehensive NF1 testing strategy.

Published

2023

11. Constitutional Microsatellite Instability, Genotype, and Phenotype Correlations in Constitutional Mismatch Repair Deficiency

Author

Richard Gallon, Rachel Phelps, Christine Hayes, Laurence Brugieres, Léa Guerrini-Rousseau, Chrystelle Colas, Martine Muleris, Neil A.J. Ryan, D. Gareth Evans, Hannah Grice, Emily Jessop, Annabel Kunzemann-Martinez, Lilla Marshall, Esther Schamschula, Klaus Oberhuber, Amedeo A. Azizi, Hagit Baris Feldman, Andreas Beilken, Nina Brauer, Triantafyllia Brozou, Karin Dahan, Ugur Demirsoy, Benoît Florkin, William Foulkes, Danuta Januszkiewicz-Lewandowska, Kristi J. Jones, Christian P. Kratz, Stephan Lobitz, Julia Meade, Michaela Nathrath, Hans-Jürgen Pander, Claudia Perne, Iman Ragab, Tim Ripperger, Thorsten Rosenbaum, Daniel Rueda, Tomasz Sarosiek, Astrid Sehested, Isabel Spier, Manon Suerink, Stefanie-Yvonne Zimmermann, Johannes Zschocke, Gillian M. Borthwick, Katharina Wimmer, John Burn, Michael S. Jackson, and Mauro Santibanez-Koref

Subjects

Constitutional Mutation Burden, Hepatology, Pediatric Cancer, Gastroenterology, Functional Test, Replication Error Repair

Abstract

BACKGROUND & AIMS: Constitutional mismatch repair deficiency (CMMRD) is a rare recessive childhood cancer predisposition syndrome caused by germline mismatch repair variants. Constitutional microsatellite instability (cMSI) is a CMMRD diagnostic hallmark and may associate with cancer risk. We quantified cMSI in a large CMMRD patient cohort to explore genotype-phenotype correlations using novel MSI markers selected for instability in blood.METHODS: Three CMMRD, 1 Lynch syndrome, and 2 control blood samples were genome sequenced to >120× depth. A pilot cohort of 8 CMMRD and 38 control blood samples and a blinded cohort of 56 CMMRD, 8 suspected CMMRD, 40 Lynch syndrome, and 43 control blood samples were amplicon sequenced to 5000× depth. Sample cMSI score was calculated using a published method comparing microsatellite reference allele frequencies with 80 controls.RESULTS: Thirty-two mononucleotide repeats were selected from blood genome and pilot amplicon sequencing data. cMSI scoring using these MSI markers achieved 100% sensitivity (95% CI, 93.6%-100.0%) and specificity (95% CI 97.9%-100.0%), was reproducible, and was superior to an established tumor MSI marker panel. Lower cMSI scores were found in patients with CMMRD with MSH6 deficiency and patients with at least 1 mismatch repair missense variant, and patients with biallelic truncating/copy number variants had higher scores. cMSI score did not correlate with age at first tumor.CONCLUSIONS: We present an inexpensive and scalable cMSI assay that enhances CMMRD detection relative to existing methods. cMSI score is associated with mismatch repair genotype but not phenotype, suggesting it is not a useful predictor of cancer risk.

Published

2023

12. Constitutional POLE variants causing a phenotype reminiscent of constitutional mismatch repair deficiency

Author

Julia Meade, Katharina Wimmer, Maria Anna Misiakou, Birgitte Bertelsen, Hendrik Gottschling, Johannes Zschocke, Astrid Sehested, David Scheie, Helga Fibiger Munch-Petersen, Richard Gallon, Matthias Schmuth, Olga Østrup, Linea Melchior, Elena Kessler, Reetesh K. Pai, and Tomasz Sarosiek

Subjects

Adult, POLD1, Brain Neoplasms, Somatic cell, Cancer, Biology, medicine.disease, DNA Mismatch Repair, Phenotype, Germline, Neoplastic Syndromes, Hereditary, Mutation, cardiovascular system, Genetics, medicine, Cancer research, Humans, Proofreading, DNA mismatch repair, Colorectal Neoplasms, Gene, Genetics (clinical)

Abstract

Heterozygous POLE or POLD1 germline pathogenic variants (PVs) cause polymerase proofreading associated polyposis (PPAP), a constitutional polymerase proofreading deficiency that typically presents with colorectal adenomas and carcinomas in adulthood. Constitutional mismatch-repair deficiency (CMMRD), caused by germline bi-allelic PVs affecting one of four MMR genes, results in a high propensity for hematological, brain, intestinal tract, and other malignancies in childhood. Non-malignant clinical features, such as skin pigmentation alterations, are found in nearly all CMMRD patients and are important diagnostic markers. Here, we excluded CMMRD in three cancer patients with highly suspect clinical phenotypes, but identified in each a constitutional heterozygous POLE PV. These, and two additional POLE PVs identified in published CMMRD-like patients, have not previously been reported as germline PVs despite all being well-known somatic mutations in hyper-mutated tumors. Together, these five cases show that specific POLE PVs may have a stronger "mutator" effect than known PPAP-associated POLE PVs and may cause a CMMRD-like phenotype distinct from PPAP. The common underlying mechanism, i.e. a constitutional replication error repair defect, and a similar tumor spectrum provide a good rationale for monitoring these patients with a severe constitutional polymerase proofreading deficiency according to protocols proposed for CMMRD. This article is protected by copyright. All rights reserved.

Published

2021

13. Predisposition to cancer in children and adolescents

Author

Marjolijn C.J. Jongmans, Rosalyn Jewell, Léa Guerrini-Rousseau, Lisa Golmard, Till Milde, Katharina Wimmer, Eamonn R. Maher, Franck Bourdeaut, Kathy Pritchard-Jones, Hélène Cavé, Laurence Brugières, Christian P. Kratz, Catriona Duncan, Sam Behjati, Marion Gauthier-Villars, and Kristian W. Pajtler

Subjects

Male, medicine.medical_specialty, Adolescent, Genetic counseling, MEDLINE, Cancer therapy, Medical Oncology, Risk Assessment, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, 030225 pediatrics, Developmental and Educational Psychology, Humans, Medicine, Genetic Predisposition to Disease, Genetic Testing, 030212 general & internal medicine, Child, Intensive care medicine, Genetic testing, Cancer prevention, medicine.diagnostic_test, business.industry, Paediatric oncology, Cancer, medicine.disease, Pediatrics, Perinatology and Child Health, Female, business, Risk assessment

Abstract

Childhood malignancies are rarely related to known environmental exposures, and it has become increasingly evident that inherited genetic factors play a substantial causal role. Large-scale sequencing studies have shown that approximately 10% of children with cancer have an underlying cancer predisposition syndrome. The number of recognised cancer predisposition syndromes and cancer predisposition genes are constantly growing. Imaging and laboratory technologies are improving, and knowledge of the range of tumours and risk of malignancy associated with cancer predisposition syndromes is increasing over time. Consequently, surveillance measures need to be constantly adjusted to address these new findings. Management recommendations for individuals with pathogenic germline variants in cancer predisposition genes need to be established through international collaborative studies, addressing issues such as genetic counselling, cancer prevention, cancer surveillance, cancer therapy, psychological support, and social-ethical issues. This Review represents the work by a group of experts from the European Society for Paediatric Oncology (SIOPE) and aims to summarise the current knowledge and define future research needs in this evolving field.

Published

2021

14. Constitutional mismatch repair deficiency is the diagnosis in 0.41% of pathogenic NF1/SPRED1 variant negative children suspected of sporadic neurofibromatosis type 1

Author

Ludwine Messiaen, Klaus Oberhuber, Michael S. Jackson, Yunjia Chen, Katharina Wimmer, Markus A. Keller, Juan A. Perez-Valencia, Johannes Zschocke, Richard Gallon, Jakob Koch, John Burn, Alicia Gomes, and Mauro Santibanez-Koref

Subjects

Canada, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Neurofibromatosis 1, Genetic counseling, DNA Mismatch Repair, neurofibromatosis type 1, Article, Germline, Neoplastic Syndromes, Hereditary, constitutional mismatch repair deficiency, PMS2, Humans, childhood cancer, Medicine, Neurofibromatosis, Child, Genetics (clinical), Adaptor Proteins, Signal Transducing, Mismatch Repair Endonuclease PMS2, Retrospective Studies, founder variant, Brain Neoplasms, business.industry, Microsatellite instability, medicine.disease, Europe, MSH6, North America, microsatellite instability, DNA mismatch repair, Colorectal Neoplasms, business, Founder effect

Abstract

Purpose Biallelic germline mismatch repair (MMR) gene pathogenic variants (PVs) cause constitutional MMR deficiency (CMMRD), a highly penetrant childhood cancer syndrome phenotypically overlapping with neurofibromatosis type 1 (NF1). CMMRD testing in suspected NF1 children without NF1/SPRED1 PVs enables inclusion of CMMRD positives into monitoring programs prior to tumor onset. However, testing is associated with potential harms and the prevalence of CMMRD among these children is unknown. Methods Using a simple and scalable microsatellite instability (MSI) assay of non-neoplastic leukocyte DNA to detect CMMRD, we retrospectively screened >700 children suspected of sporadic NF1 but lacking NF1/SPRED1 PVs. Results For three of seven MSI-positive patients germline MMR gene PVs confirmed the diagnosis of CMMRD. Founder variants NM_000535.5(PMS2):c.736_741delinsTGTGTGTGAAG, prevalent in Europe and North America, and NM_000179.2(MSH6):c.10C>G, affecting 1:400 French Canadians, represented two of five PVs. The prevalence of CMMRD was 3/735 (0.41%, 95% confidence interval [CI]: 0.08–1.19%). Conclusion Our empirical data provide reliable numbers for genetic counseling and confirm previous prevalence estimations, on which Care for CMMRD consortium guidelines are based. These advocate CMMRD testing of preselected patients rather than offering reflex testing to all suspected sporadic NF1 children lacking NF1/SPRED1 PVs. The possibility of founder effects should be considered alongside these testing guidelines.

Published

2020

15. Erfassung von erblichem Dickdarm- und Gebärmutterkrebs

Author

R. Kain, Katharina Wimmer, Johannes Zschocke, G. Webersinke, G. Uyanik, Sigurd Lax, W. Hulla, Michael R. Speicher, Gerald Hoefler, and B. Zelger

Subjects

Gynecology, medicine.medical_specialty, Oncology, business.industry, Medicine, Hematology, business

Abstract

ZusammenfassungDie Möglichkeit einer Tumorerkrankung auf Basis eines familiären Tumorprädispositionssyndroms muss bei jeder Krebsdiagnose in Betracht gezogen werden. Die Erfassung erkrankter „Index“-PatientInnen ist entscheidend für die Ermittlung des Risikos für Neu- oder Wiedererkrankungen bei den Betroffenen wie auch für das Auftreten von Tumoren bei bisher gesunden Verwandten. Die Erfassung von PatientInnen mit familiärer Tumorprädisposition erlaubt es, Betroffene in Vorsorgeprogramme zur Senkung von Morbidität und Letalität aufzunehmen. Für das erbliche Brust- und Eierstockkrebssyndrom besteht in Österreich ein breites Bewusstsein. Dadurch wird eine zufriedenstellende Erfassung der PatientInnen erreicht. Das ist für das Lynch-Syndrom, welches bei 2–3 % aller Kolorektal- und Endometriumkarzinome vorliegt, leider nicht der Fall. Um die Identifizierung von Lynch-Syndrom-PatientInnen zu verbessern, empfiehlt die Österreichische Arbeitsgemeinschaft Pathologie-Humangenetik (die Österreichische Arbeitsgemeinschaft Pathologie-Humangenetik setzt sich aus jeweils fünf Delegierten der Österreichischen Gesellschaft für Klinische Pathologie und Molekularpathologie und der Österreichischen Gesellschaft für Humangenetik zusammen) in diesem Konsensus-Statement eine diagnostische Strategie, die möglichst alle Lynch-Syndrom-assoziierten Kolorektal- und Endometriumkarzinome im Rahmen der pathologischen Tumorbeurteilung erfasst. Durch eine darauf basierende systematische Zuweisung von PatientInnen mit Verdacht auf Lynch-Syndrom an ein Zentrum für medizinische Genetik zur genetischen Beratung und weiterführenden genetischen Diagnostik wird sichergestellt, dass auch Familienangehörige mit Lynch-Syndrom erfasst werden.

Published

2020

16. LinkedSV for detection of mosaic structural variants from linked-read exome and genome sequencing data

Author

Sören-Sebastian Wenzel, Kai Wang, Katharina Wimmer, Li Fang, Renata Pellegrino da Silva, Charlly Kao, Hakon Hakonarson, Fernanda Abani Mafra, Mingyao Li, and Michael Gonzalez

Subjects

0301 basic medicine, Computer science, Science, DNA Mutational Analysis, Sequencing data, General Physics and Astronomy, Computational biology, Biology, Genome informatics, Barcode, Genome, Article, General Biochemistry, Genetics and Molecular Biology, DNA sequencing, law.invention, Genomic analysis, Chromosome Breakpoints, 03 medical and health sciences, 0302 clinical medicine, law, Sequencing, Humans, Exome, Repeated sequence, Indel, lcsh:Science, Exome sequencing, Sequence Deletion, Neurofibromin 1, Multidisciplinary, Base Sequence, Models, Genetic, Genome, Human, Breakpoint, Variant allele, Sequence Analysis, DNA, General Chemistry, 030104 developmental biology, 030220 oncology & carcinogenesis, Genomic Structural Variation, lcsh:Q, Software

Abstract

Linked-read sequencing provides long-range information on short-read sequencing data by barcoding reads originating from the same DNA molecule, and can improve detection and breakpoint identification for structural variants (SVs). Here we present LinkedSV for SV detection on linked-read sequencing data. LinkedSV considers barcode overlapping and enriched fragment endpoints as signals to detect large SVs, while it leverages read depth, paired-end signals and local assembly to detect small SVs. Benchmarking studies demonstrate that LinkedSV outperforms existing tools, especially on exome data and on somatic SVs with low variant allele frequencies. We demonstrate clinical cases where LinkedSV identifies disease-causal SVs from linked-read exome sequencing data missed by conventional exome sequencing, and show examples where LinkedSV identifies SVs missed by high-coverage long-read sequencing. In summary, LinkedSV can detect SVs missed by conventional short-read and long-read sequencing approaches, and may resolve negative cases from clinical genome/exome sequencing studies., Compared to single nucleotide variants and short indels, structural variants (SVs) are often more challenging to detect using high-throughput sequencing based methods. Here, the authors develop LinkedSV, a computational tool for SV detection using linked-read exome and genome sequencing data.

Published

2019

17. High yield of surveillance in patients diagnosed with constitutional mismatch repair deficiency

Author

Zeinab Ghorbanoghli, Mariëtte van Kouwen, Birgitta Versluys, Delphine Bonnet, Christine Devalck, Julie Tinat, Danuta Januszkiewicz-Lewandowska, Consuelo Calvino Costas, Edouard Cottereau, James C H Hardwick, Katharina Wimmer, Laurence Brugieres, Chrystelle Colas, and Hans F A Vasen

Subjects

genetic predisposition to disease, Genetics, germ-line mutation, Genetics (clinical)

Abstract

BackgroundConstitutional mismatch repair deficiency (CMMRD) is a rare autosomal recessively inherited syndrome that is caused by biallelic pathogenic variants of the mismatch repair genes. It is characterised by the development of multiple tumours in the first and second decade of life including brain, gastrointestinal and haematological tumours often resulting in early death. In order to improve the prognosis of these patients, the European collaborative group ‘care for CMMRD’ developed a surveillance programme in 2014 and established a registry of patients with CMMRD in Paris. The aim of the study was to evaluate the outcome of this programme.MethodsTwenty-two patients with a definitive diagnosis of CMMRD and with at least one follow-up study were selected from the registry. Medical data on the outcome of surveillance were collected from these patients.ResultsDuring a mean follow-up of 4 years, the programme detected eight malignant tumours including three brain tumours, three upper gastrointestinal cancers and two colorectal cancers. Most tumours could successfully be treated. In addition, many adenomas were detected in the duodenum, and colorectum and subsequently removed. Seven patients developed a symptomatic malignancy, including two brain tumours, one small bowel cancer and four haematological malignancies. At the end of the follow-up, 16 out of 22 patients (73%) who participated in the surveillance programme were still alive.ConclusionThe study suggests a beneficial effect of surveillance of the digestive tract and brains.

Published

2022

18. Revised diagnostic criteria for neurofibromatosis type 1 and Legius syndrome: an international consensus recommendation

Author

Matthias A. Karajannis, A Taylor, Diana Baralle, Rosalie E. Ferner, A Gomes, Dave Viskochil, J Toelen, Rianne Oostenbrink, Christopher L. Moertel, Laura Papi, Conxi Lázaro, H Wu, Michael D. Wilson, Shay Ben-Shachar, Pierre Wolkenstein, Sirkku Peltonen, Plotkin, P Joly, Dominique C. Pichard, Michael Fisher, Steinke-Lange, T Frébourg, P Ciavarelli, H Hanson, Mia MacCollin, I Blanco, D Bessis, Meena Upadhyaya, C Cassiman, Dusica Babovic-Vuksanovic, Riccardi, Juha Peltonen, James H. Tonsgard, B Poppe, Katharina Wimmer, M Larralde, P Pancza, A Heiberg, Bruce R. Korf, Mautner, D. G. R. Evans, Robert Listernick, Tena Rosser, S Barbarot, Eva Trevisson, D Stevenson, M Anten, Eduard Serra, Miriam J. Smith, Christopher J Hammond, Susan M Huson, Yemima Berman, Marco Giovannini, C Mallucci, Anat Stemmer-Rachamimov, G Tadini, Robert A. Avery, N Rezende, Nicole J. Ullrich, CO Hanemann, SM Stivaros, Hildegard Kehrer-Sawatzki, A Parry, D Kroshinsky, Maurizio Clementi, JT Jordan, A Varan, Joanne Ngeow, A Mueller, G Zadeh, Michel Kalamarides, D Halliday, M Link, Elizabeth K. Schorry, Roger J. Packer, Vanessa L. Merker, David H. Gutmann, Arthur S. Aylsworth, Karin Soares Gonçalves Cunha, V-F Mautner, Amanda L. Bergner, David A. Stevenson, Eric Legius, L Le, M Ruggieri, Fred G. Barker, Ludwine Messiaen, Jan M. Friedman, J. Blakeley, Kaleb Yohay, Katherine A. Rauen, LO Rodrigues, and Pediatrics

Subjects

0301 basic medicine, medicine.medical_specialty, Consensus, Neurofibromatosis 1, Delphi method, MEDLINE, MUTATION ANALYSIS, MOSAICISM, Patient advocacy, Article, 03 medical and health sciences, 0302 clinical medicine, REVEALS, SEQUENCE VARIANTS, medicine, Humans, Cafe-au-Lait Spots, Genetic Testing, Medical physics, Neurofibromatosis, Genetics (clinical), Genetic testing, Genetics & Heredity, Legius syndrome, Science & Technology, IDENTIFICATION, medicine.diagnostic_test, business.industry, medicine.disease, GENE, 030104 developmental biology, CHOROIDAL ABNORMALITIES, 030220 oncology & carcinogenesis, business, Life Sciences & Biomedicine

Abstract

PURPOSE: By incorporating major developments in genetics, ophthalmology, dermatology, and neuroimaging, to revise the diagnostic criteria for neurofibromatosis type 1 (NF1) and to establish diagnostic criteria for Legius syndrome (LGSS). METHODS: We used a multistep process, beginning with a Delphi method involving global experts and subsequently involving non-NF experts, patients, and foundations/patient advocacy groups. RESULTS: We reached consensus on the minimal clinical and genetic criteria for diagnosing and differentiating NF1 and LGSS, which have phenotypic overlap in young patients with pigmentary findings. Criteria for the mosaic forms of these conditions are also recommended. CONCLUSION: The revised criteria for NF1 incorporate new clinical features and genetic testing, whereas the criteria for LGSS were created to differentiate the two conditions. It is likely that continued refinement of these new criteria will be necessary as investigators (1) study the diagnostic properties of the revised criteria, (2) reconsider criteria not included in this process, and (3) identify new clinical and other features of these conditions. For this reason, we propose an initiative to update periodically the diagnostic criteria for NF1 and LGSS. ispartof: GENETICS IN MEDICINE vol:23 issue:8 pages:1506-1513 ispartof: location:United States status: published

Published

2021

19. Clinical spectrum of individuals with pathogenic N F1 missense variants affecting p.Met1149, p.Arg1276, and p.Lys1423: genotype–phenotype study in neurofibromatosis type 1

Author

Giulio Piluso, Katharina Wimmer, Veronica Saletti, Eniko K. Pivnick, Geraldine Kelly-Mancuso, Karen W. Gripp, Cristin Griffis, Louanne Hudgins, Alessandro De Luca, Michael F. Wangler, M. Daniela D'Agostino, Marica Eoli, Cynthia M. Powell, Laura A. Baker, Mayra Martinez Ojeda, Silvia Esposito, Elizabeth A. Sellars, Kory Keller, David D. Weaver, James T. Bennett, Nicole J. Ullrich, Allison L. Goetsch, Donald Basel, Bruce R. Korf, Stephanie Fox, Katelyn Hodge, Laura Dosa, Robert S. Greenwood, Mario Bengala, Andrea M. Lewis, Ruth Sheffer, Valentina Pinna, Fanny Cortés, Dusica Babovic-Vuksanovic, Aaina Kochhar, Rosemarie Smith, Concepción Hernández-Chico, Elizabeth Siqveland, Robert Listernick, Lola K. Clarkson, Punita Gupta, E. Haan, Martin B. Delatycki, Amy Theos, Noa Ruhrman Shahar, Teresa Giugliano, Carey McDougall, Mitch Cunningham, David W. Stockton, Tom Callens, Maria Cristina Digilio, Yunjia Chen, Ludwine Messiaen, Eva Trevisson, Samantha A. Schrier Vergano, Caleb Rogers, Magdalena Koczkowska, Kathleen Claes, Christine Fauth, Jan Liebelt, Pamela Trapane, Eric Johns, John M. Slopis, Chelsea Chambers, Tamara L. Haygarth, Lesley K. McGregor, Alberto Spalice, Małgorzata J.M. Nowaczyk, Mary Ella M Pierpont, Kaleb Yohay, Alicia Gomes, Vickie Zurcher, Gail E. Tomlinson, Angie W. Lichty, Stephanie E Wallace, Rachel K. Hachen, Isabelle Maystadt, S. Lane Rutledge, Yael Goldberg, Grace Tran, Ulrich A. Schatz, Allison Schreiber, Jenneke van den Ende, Michael J. Lyons, Mary Louise Freckmann, Kim Armfield Uhas, Alesha D. Hicks, Maurizio Clementi, Haley Streff, June Ortenberg, John Pappas, Nancy J. Mendelsohn, Sandra Janssens, Karin Panzer, Yolanda Martin, Elaine H. Zackai, Sandra Giustini, Linlea Armstrong, Katherine A. Bosanko, Angela Sharp, Daryl A. Scott, Jonathan Zonana, Robert J. Hopkin, Eric Legius, Dinel A. Pond, Daniela Melis, Claudia Santoro, and Sarah A. Sandaradura

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, 0303 health sciences, medicine.medical_specialty, education.field_of_study, Pulmonic stenosis, 030305 genetics & heredity, Population, Spinal neurofibromas, Biology, medicine.disease, Phenotype, Gastroenterology, nervous system diseases, 03 medical and health sciences, Internal medicine, Cohort, Genetics, medicine, Missense mutation, Noonan syndrome, Neurofibromatosis, education, Genetics (clinical), 030304 developmental biology

Abstract

We report 281 individuals carrying a pathogenic recurrent NF1 missense variant at p.Met1149, p.Arg1276, or p.Lys1423, representing three nontruncating NF1 hotspots in the University of Alabama at Birmingham (UAB) cohort, together identified in 1.8% of unrelated NF1 individuals. About 25% (95% confidence interval: 20.5-31.2%) of individuals heterozygous for a pathogenic NF1 p.Met1149, p.Arg1276, or p.Lys1423 missense variant had a Noonan-like phenotype, which is significantly more compared with the "classic" NF1-affected cohorts (all p < .0001). Furthermore, p.Arg1276 and p.Lys1423 pathogenic missense variants were associated with a high prevalence of cardiovascular abnormalities, including pulmonic stenosis (all p < .0001), while p.Arg1276 variants had a high prevalence of symptomatic spinal neurofibromas (p < .0001) compared with "classic" NF1-affected cohorts. However, p.Met1149-positive individuals had a mild phenotype, characterized mainly by pigmentary manifestations without externally visible plexiform neurofibromas, symptomatic spinal neurofibromas or symptomatic optic pathway gliomas. As up to 0.4% of unrelated individuals in the UAB cohort carries a p.Met1149 missense variant, this finding will contribute to more accurate stratification of a significant number of NF1 individuals. Although clinically relevant genotype-phenotype correlations are rare in NF1, each affecting only a small percentage of individuals, together they impact counseling and management of a significant number of the NF1 population.

Published

2019

20. Paediatric systemic lupus erythematosus as a manifestation of constitutional mismatch repair deficiency

Author

Melyssa Aronson, Helen Toledano, Lili Bazak, Efrat Sofrin, Gil Amarilyo, Alan R. Shuldiner, Claudia Gonzaga-Jauregui, Noa Ruhrman-Shahar, Katharina Wimmer, Lina Basel-Salmon, Naama Orenstein, Hibs Al-tarrah, Pola Smirin-Yosef, Yael Goldberg, and Uri Tabori

Subjects

0301 basic medicine, medicine.medical_specialty, Neurofibromatosis 1, Childhood cancer, MLH1, DNA Mismatch Repair, Pediatrics, 03 medical and health sciences, 0302 clinical medicine, Neoplastic Syndromes, Hereditary, Genetics, PMS2, Humans, Lupus Erythematosus, Systemic, Medicine, Neurofibromatosis, Child, Genetics (clinical), Brain Neoplasms, business.industry, medicine.disease, Dermatology, DNA-Binding Proteins, MSH6, Phenotype, 030104 developmental biology, MSH2, Child, Preschool, 030220 oncology & carcinogenesis, Mutation, MISMATCH REPAIR DEFICIENCY, Female, DNA mismatch repair, Colorectal Neoplasms, business

Abstract

Biallelic mutations in any of the four mismatch repair genes MSH2, MSH6, MLH1 and PMS2 result in one of the most aggressive childhood cancer predisposition syndromes, termed constitutional mismatch repair deficiency (CMMRD) syndrome. In addition to a very high tumour risk, the CMMRD phenotype is often characterised by the presence of signs reminiscent of neurofibromatosis type 1. Although paediatric systemic lupus erythematosus (pSLE) has been reported so far in three patients with CMMRD, it has not been considered a diagnostic feature of the syndrome. We report here two additional female patients with pSLE and CMMRD due to biallelic pathogenic variants in MSH6. Hence, there are a total of five out of approximately 200 (2.5%) currently reported patients with CMMRD that also have pSLE, suggesting pSLE should raise the suspicion of a diagnosis of CMMRD, especially if supported by additional indicative features

Published

2019

21. Overview of hereditary breast and ovarian cancer (HBOC) guidelines across Europe

Author

David Humberto Marmolejo, Mark Yu Zheng Wong, Svetlana Bajalica-Lagercrantz, Marc Tischkowitz, Judith Balmaña, Attila Balázs Patócs, Pierre Chappuis, Chrystelle Colas, Maurizio Genuardi, Maria Haanpää, Hildegunn Hoberg Vetti, Nicoline Hoogerbrugge, Arvids Irmejs, Tiina Kahre, Barbara Klink, Mateja Krajc, Tamara Hussong Milagre, Robin de Putter, Verena Steinke-Lange, Karin Wadt, and Katharina Wimmer

Subjects

Oncology, medicine.medical_specialty, PALB2, medicine.medical_treatment, Breast Neoplasms, Germline, Breast cancer, Internal medicine, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Genetics, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, skin and connective tissue diseases, CHEK2, Mastectomy, Genetics (clinical), Genetic testing, Ovarian Neoplasms, medicine.diagnostic_test, business.industry, General Medicine, medicine.disease, Europe, Female, Age of onset, Ovarian cancer, business

Abstract

Item does not contain fulltext Hereditary breast and ovarian cancer (HBOC) is a syndrome defined by an increased risk of developing breast and/or ovarian cancer most commonly due to germline disease-causing variants in the BRCA1 and BRCA2 genes, but also other causative genes such as PALB2, ATM and CHEK2. As genetic testing becomes more prevalent and new clinical data emerge, updates of national guidelines are required to incorporate these advances in our knowledge. The aim of this work is to review the guidelines for HBOC genetic testing and clinical surveillance across European countries, mostly affiliated to the European Reference Network (ERN) for Genetic Tumor Risk Syndroms (GENTURIS). Young onset breast cancer (BC), triple negative phenotype, or bilateral BC are considered as criteria for genetic testing in all, with differences in age limits. Testing of invasive epithelial non-mucinous ovarian cancer is also universally accepted. While breast magnetic resonance imaging (MRI) is consistently recommended in high-risk individuals, age of onset for mammograms differ between 30 and 40 years. Risk-reducing mastectomy is commonly offered as an option, while risk-reducing salpingo-oophorectomy is universally recommended. The largest differences are observed with respect to ovarian surveillance prior to risk-reducing salpingo-oophorectomy and in breast surveillance for carriers of non-BRCA1/2 genes. These differences in national guidelines reflect the variations in clinical consensus that may be reached in the absence of consistent evidence for some recommendations.

Published

2021

22. Revised diagnostic criteria for neurofibromatosis type 1 and Legius syndrome

Author

International Consensus Group on Neurofibromatosis Diagnostic Criteria (I-NF-DC), Eric Legius, Ludwine Messiaen, Pierre Wolkenstein, Patrice Pancza, Robert A. Avery, Yemima Berman, Jaishri Blakeley, Dusica Babovic-Vuksanovic, Karin Soares Cunha, Rosalie E. Ferner, Michael J. Fisher, Jan M. Friedman, David H. Gutmann, Hildegard Kehrer-Sawatzki, Bruce R. Korf, Victor Felix Mautner, Sirkku Peltonen, Katherine A. Rauen, Vincent Riccardi, Elizabeth Schorry, Anat Stemmer-Rachamimov, David A. Stevenson, Gianluca Tadini, Nicole J. Ullrich, David Viskochil, Katharina Wimmer, Kaleb Yohay, Alicia Gomes, Justin T. Jordan, Victor Mautner, Vanessa L. Merker, Miriam J. Smith, David Stevenson, Monique Anten, Arthur Aylsworth, Diana Baralle, Sebastien Barbarot, Fred Barker, Shay Ben-Shachar, Amanda Bergner, Didier Bessis, Ignacio Blanco, Catherine Cassiman, Patricia Ciavarelli, Maurizio Clementi, Thierry Frébourg, Marco Giovannini, Dorothy Halliday, R. (Rianne) Oostenbrink, B (Bruce) Poppe, International Consensus Group on Neurofibromatosis Diagnostic Criteria (I-NF-DC), Eric Legius, Ludwine Messiaen, Pierre Wolkenstein, Patrice Pancza, Robert A. Avery, Yemima Berman, Jaishri Blakeley, Dusica Babovic-Vuksanovic, Karin Soares Cunha, Rosalie E. Ferner, Michael J. Fisher, Jan M. Friedman, David H. Gutmann, Hildegard Kehrer-Sawatzki, Bruce R. Korf, Victor Felix Mautner, Sirkku Peltonen, Katherine A. Rauen, Vincent Riccardi, Elizabeth Schorry, Anat Stemmer-Rachamimov, David A. Stevenson, Gianluca Tadini, Nicole J. Ullrich, David Viskochil, Katharina Wimmer, Kaleb Yohay, Alicia Gomes, Justin T. Jordan, Victor Mautner, Vanessa L. Merker, Miriam J. Smith, David Stevenson, Monique Anten, Arthur Aylsworth, Diana Baralle, Sebastien Barbarot, Fred Barker, Shay Ben-Shachar, Amanda Bergner, Didier Bessis, Ignacio Blanco, Catherine Cassiman, Patricia Ciavarelli, Maurizio Clementi, Thierry Frébourg, Marco Giovannini, Dorothy Halliday, R. (Rianne) Oostenbrink, and B (Bruce) Poppe

Abstract

Purpose: By incorporating major developments in genetics, ophthalmology, dermatology, and neuroimaging, to revise the diagnostic criteria for neurofibromatosis type 1 (NF1) and to establish diagnostic criteria for Legius syndrome (LGSS). Methods: We used a multistep process, beginning with a Delphi method involving global experts and subsequently involving non-NF experts, patients, and foundations/patient advocacy

Published

2021

23. Report of the fifth meeting of the European Consortium 'Care for CMMRD' (C4CMMRD), Leiden, The Netherlands, July 6th 2019

Author

M le Mentec, Chrystelle Colas, Marta Pineda, Richard Gallon, Hans F. A. Vasen, Zeinab Ghorbanoghli, Laurence Brugières, Manon Suerink, Katharina Wimmer, Clara Ruiz-Ponte, Yael Goldberg, James C. H. Hardwick, E M A Bleiker, Martine Muleris, Tim Ripperger, Patrick R. Benusiglio, Matthias Kloor, CHU Saint-Antoine [AP-HP], and Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)

Subjects

0303 health sciences, Cancer Research, medicine.medical_specialty, business.industry, [SDV]Life Sciences [q-bio], MEDLINE, Review, Human genetics, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Family medicine, Epidemiology, Genetics, medicine, business, Genetics (clinical), ComputingMilieux_MISCELLANEOUS, 030304 developmental biology

Abstract

International audience

Published

2020

24. High-sensitivity microsatellite instability assessment for the detection of mismatch repair defects in normal tissue of biallelic germline mismatch repair mutation carriers

Author

Christian P. Kratz, Ugur Demirsoy, Anna Fernández, Elia Grau Garces, Angela Velasco, Núria Bonifaci, Victor Moreno, Michaela Nathrath, Hector Salvador, Conxi Lázaro, Marta Pineda, Manon Suerink, Joan Brunet, Benjamin Puliafito, Gabriel Capellá, Amedeo A. Azizi, Maribel González-Acosta, Daniel Rueda, Iman A. Ragab, Karin Dahan, Thomas Imschweiler, Danuta Januszkiewicz-Lewandowska, Benoit Florkin, Thorsten Rosenbaum, Hans-Jürgen Pander, Luis Ignacio Gonzalez-Granado, Rosa Ayala, Silvia Iglesias, Katharina Wimmer, Fátima Marín, Matilde Navarro, Francesc Balaguer, Pilar Guerra-García, Stephan Lobitz, and Tim Ripperger

Subjects

Male, 0301 basic medicine, Oncology, ADN, medicine.disease_cause, DNA Mismatch Repair, Germline, 0302 clinical medicine, highly sensitive methodologies, lynch syndrome, Child, Diagnostics, Genetics (clinical), next generation sequencing, Mutation, Brain Neoplasms, High-Throughput Nucleotide Sequencing, Lynch syndrome, ddc, DNA-Binding Proteins, MutS Homolog 2 Protein, Child, Preschool, 030220 oncology & carcinogenesis, Microsatellite, Female, Microsatellite Instability, DNA mismatch repair, Colorectal Neoplasms, Adult, Heterozygote, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Reparació de l'ADN, DNA repair, constitutional mismatch repair deficiency, DNA sequencing, Young Adult, 03 medical and health sciences, Germline mutation, Neoplastic Syndromes, Hereditary, Càncer colorectal, Internal medicine, Genetics, medicine, Humans, microsatellite instability, neoplasms, Germ-Line Mutation, business.industry, Infant, Microsatellite instability, nutritional and metabolic diseases, DNA, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Colorectal cancer, digestive system diseases, 030104 developmental biology, business

Abstract

IntroductionLynch syndrome (LS) and constitutional mismatch repair deficiency (CMMRD) are hereditary cancer syndromes associated with mismatch repair (MMR) deficiency. Tumours show microsatellite instability (MSI), also reported at low levels in non-neoplastic tissues. Our aim was to evaluate the performance of high-sensitivity MSI (hs-MSI) assessment for the identification of LS and CMMRD in non-neoplastic tissues.Materials and methodsBlood DNA samples from 131 individuals were grouped into three cohorts: baseline (22 controls), training (11 CMMRD, 48 LS and 15 controls) and validation (18 CMMRD and 18 controls). Custom next generation sequencing panel and bioinformatics pipeline were used to detect insertions and deletions in microsatellite markers. An hs-MSI score was calculated representing the percentage of unstable markers.ResultsThe hs-MSI score was significantly higher in CMMRD blood samples when compared with controls in the training cohort (pMSH2 carriers (n=5) compared with MSH6 carriers (n=15). The hs-MSI analysis did not detect a difference between LS and control blood samples (p=0.564).ConclusionsThe hs-MSI approach is a valuable tool for CMMRD diagnosis, especially in suspected patients harbouring MMR variants of unknown significance or non-detected biallelic germline mutations.

Published

2020

25. 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

26. Diagnostic challenges in a child with early onset desmoplastic medulloblastoma and homozygous variants in MSH2 and MSH6

Author

Triantafyllia Brozou, Olivier Lascols, Michaela Kuhlen, Chrystelle Colas, Julia Taeubner, Christine Fauth, Jessica I. Hoell, Katharina Wimmer, Joerg Felsberg, Jasmin C. Riemer, Sebastian Ginzel, Arndt Borkhardt, Martine Muleris, Michael Gombert, Department of Medical Genetics, Medical University of Vienna, Vienna, Centre de Recherche Saint-Antoine (UMRS893), Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre Régional de Lutte contre le cancer Georges-François Leclerc [Dijon] (UNICANCER/CRLCC-CGFL), UNICANCER, Division of Clinical Genetics, Department of Medical Genetics, Molecular and and Clinical Pharmacology, Innsbruck Medical University [Austria] (IMU), Clinic of Pediatric Oncology, Hematology and Clinical Immunology, and Center for Child and Adolescent Health, Heinrich-Heine-University

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Pathology, medicine.medical_specialty, [SDV]Life Sciences [q-bio], education, Brief Communication, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Cell Line, Tumor, Genetics, Humans, Medicine, Genetic Testing, Cerebellar Neoplasms, Cells, Cultured, Genetics (clinical), business.industry, Desmoplastic medulloblastoma, Homozygote, Infant, Microsatellite instability, medicine.disease, Phenotype, 3. Good health, DNA-Binding Proteins, MSH6, MutS Homolog 2 Protein, 030104 developmental biology, MSH2, 030220 oncology & carcinogenesis, Immunohistochemistry, Female, DNA mismatch repair, business, Medulloblastoma

Abstract

Constitutional mismatch repair deficiency (CMMRD) is an autosomal recessively inherited childhood cancer susceptibility syndrome caused by biallelic germline mutations in one of the mismatch repair (MMR) genes. The spectrum of CMMRD-associated tumours is very broad and many CMMRD patients additionally display signposting non-neoplastic features, most frequently café-au-lait macules and other pigmentation alterations. We report on a 13-month-old girl suspected of having CMMRD due to a desmoplastic medulloblastoma and a striking skin pigmentation that included multiple café-au-lait macules, hypopigmented areas and Mongolian spots. Whole-exome sequencing revealed homozygosity for MSH2 variant p.(Leu92Val) and MSH6 variant p.(Val809del), both variants of uncertain significance (VUS). Immunohistochemical analysis of the tumour tissue showed expression of all four MMR proteins and gMSI testing was negative. However, functional assays demonstrated that the cells of the patient displayed methylation tolerance and ex vivo microsatellite instability, which unequivocally confirmed the diagnosis of CMMRD. Taken together, the results render the MSH2 variant unlikely to be responsible for the phenotype, while they are compatible with MSH6-associated CMMRD. This case illustrates the diagnostic strategy of confirming CMMRD syndrome in patients with VUS.

Published

2018

27. HGG-44. DEFECTS OF MISMATCH REPAIR PROTEINS IN PEDIATRIC HIGH GRADE GLIOMAS

Author

Irene Slavc, Andreas Peyrl, Philippe Muller, Leonhard Müllauer, Katharina Wimmer, Christine Haberler, and Thomas Czech

Subjects

Cancer Research, congenital, hereditary, and neonatal diseases and abnormalities, business.industry, Cancer, nutritional and metabolic diseases, Tumor cells, medicine.disease, digestive system diseases, Oncology, Glioma, Cancer research, Medicine, AcademicSubjects/MED00300, DNA mismatch repair, AcademicSubjects/MED00310, Neurology (clinical), Msh2 gene, business, High Grade Glioma, neoplasms

Abstract

Hetero- and homozygous germline mutations of the mismatch repair genes MLH1, PMS2, MSH2 and MSH6 cause Lynch and constitutional mismatch repair (CMMRD) cancer predisposition syndrome, respectively. Affected CMMRD individuals are at risk to develop a variety of neoplasms including CNS tumors, particularly high grade gliomas (HGG), during childhood. Currently, few data exist on the prevalence of CMMRD in children with pediatric HGG. We screened a consecutive series of 79 supratentorial HGGs. Tumor tissue was available in 42 patients, 5 were reclassified as non-HGGs. Immunohistochemistry with antibodies against MLH1, PMS2, MSH2 and MSH6 was performed in 37 tumors. Four patients (3 families) with known CMMRD were included. The evaluation of the slides was performed blinded to the CMMRD status. All four patients with known CMMRD (3 patients with PMS2, one with MSH6 mutation) were identified, showing loss of PMS2 and MSH2/MSH6, respectively. Additionally, we identified 6 patients with loss of MSH2/MSH6 staining in tumor cells, but retained staining in preexisting cells, indicating a pattern like in Lynch syndrome. NGS sequencing of these tumor tissues revealed in 2 patients MSH2 mutations and in one patient a hypermutator phenotype with MSH2 and MSH6 mutations. In 3/6 patients no mutations in the MMR genes were detectable. In summary, we found a low prevalence of CMMRD among HGGs, but identified also 2 patients with probable Lynch syndrome. Immunhistochemistry is an effective tool to screen for patients with MMR defects and should be performed in HGGs to optimize treatment and offer affected families genetic counseling.

Published

2020

28. Seltene Tumordispositionssyndrome mit Manifestation im Kindesalter

Author

Tim Ripperger, Katharina Wimmer, and Christian Kratz

Subjects

0301 basic medicine, Gynecology, 03 medical and health sciences, medicine.medical_specialty, 030104 developmental biology, 0302 clinical medicine, business.industry, 030220 oncology & carcinogenesis, Genetics, Medicine, business, Genetics (clinical)

Abstract

Zusammenfassung Bei etwa 7–10 % der pädiatrischen Krebspatienten werden zugrunde liegende Tumordispositionssyndrome (TDS) vermutet. Das Erkennen von TDS hat klinische Implikationen für die Krebsprävention und -früherkennung, die Krebstherapie und -nachsorge, die psychosoziale Unterstützung sowie die Beratung von Angehörigen und Identifizierung weiterer Anlageträger in den betroffenen Familien. Hinweise auf das Vorliegen eines TDS anhand von Eigen- und Familienanamnese, Untersuchungsbefund sowie gegebenenfalls Tumorhistologie und -genetik müssen daher möglichst früh erkannt werden, um bei Verdacht auf Vorliegen eines TDS eine humangenetische Beratung und gegebenenfalls genetische Diagnostik zu veranlassen. Wissenschaftliche Untersuchungen zu TDS liefern Einblicke in die Biologie der Gewebe- und Tumorentwicklung und weisen auf mögliche Ansatzpunkte zielgerichteter Therapien hin. Die vorliegende Arbeit gibt eine Übersicht über TDS mit erhöhtem Risiko für Wilms-Tumoren (Nephroblastome), Neuroblastome oder Medulloblastome. Zusätzlich werden zwei vergleichsweise neu beschriebene Syndrome mit breitem Neoplasiespektrum erläutert: die konstitutionelle Mismatch-Reparatur-Defizienz (CMMRD) und das DICER1-Syndrom. Neben der Erläuterung der klinischen Charakteristika und der genetischen Grundlagen werden für die tägliche Praxis Hinweise zur Indikation von genetischen Untersuchungen und Früherkennung bei TDS aufgeführt. Die Betreuung der Betroffenen und ihrer Angehörigen sollte möglichst interdisziplinär erfolgen. Forschung zu TDS, zum Beispiel im Rahmen von Registern für TDS, ist essenziell, um langfristig die medizinische Versorgung von Menschen zu verbessern, die bedingt durch konstitutionelle genetische Veränderungen ein erhöhtes Krebsrisiko haben.

Published

2017

29. Connections between constitutional mismatch repair deficiency syndrome and neurofibromatosis type 1

Author

Ludwine Messiaen, Thorsten Rosenbaum, and Katharina Wimmer

Subjects

0301 basic medicine, Oncology, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Childhood cancer, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Café au lait spot, Internal medicine, Genetics, medicine, Neurofibromatosis, Rhabdomyosarcoma, neoplasms, Genetics (clinical), business.industry, medicine.disease, nervous system diseases, 030104 developmental biology, 030220 oncology & carcinogenesis, MISMATCH REPAIR DEFICIENCY, DNA mismatch repair, medicine.symptom, business

Abstract

Constitutional mismatch repair (MMR) deficiency (CMMRD) is a rare childhood cancer susceptibility syndrome resulting from biallelic germline loss-of-function mutations in one of the MMR genes. Individuals with CMMRD have high risk to develop a broad spectrum of malignancies and frequently display features reminiscent of neurofibromatosis type 1 (NF1). Evaluation of the clinical findings of genetically proven CMMRD patients shows that not only multiple cafe-au-lait macules but also any of the diagnostic features of NF1 may be present in a CMMRD patient. This phenotypic overlap may lead to misdiagnosis of CMMRD patients as having NF1, which impedes adequate management of the patients and their families. The spectrum of CMMRD-associated childhood malignancies includes high-grade glioma, acute myeloid leukaemia or rhabdomyosarcoma, also reported as associated with NF1. Reported associations between NF1 and these malignancies are to a large extent based on studies that neither proved the presence of an NF1 germline mutation nor ruled-out CMMRD in the affected. Hence, these associations are challenged by our current knowledge of the phenotypic overlap between NF1 and CMMRD and should be re-evaluated in future studies. Recent advances in the diagnostics of CMMRD should render it possible to definitely state or refute this diagnosis in these individuals.

Published

2017

30. Osteoclast and osteoblast response to strontium-doped struvite coatings on titanium for improved bone integration

Author

Julia Zerweck, Claus Moseke, M. Meininger, Andrea Ewald, Uwe Gbureck, Katharina Wimmer, and Cornelia Wolf-Brandstetter

Subjects

Struvite, Biomedical Engineering, chemistry.chemical_element, 030209 endocrinology & metabolism, 02 engineering and technology, Electrolyte, engineering.material, Bone and Bones, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Coating, Osteoclast, Strontium nitrate, medicine, Animals, Titanium, Strontium, Nitrates, Osteoblasts, Osteoblast, Prostheses and Implants, 021001 nanoscience & nanotechnology, medicine.anatomical_structure, chemistry, Chemical engineering, engineering, 0210 nano-technology

Abstract

To develop implants with improved bone ingrowth, titanium substrates were coated with homogeneous and dense struvite (MgNH4PO4·6H2O) layers by means of electrochemically assisted deposition. Strontium nitrate was added to the coating electrolyte in various concentrations, in order to fabricate Sr-doped struvite coatings with Sr loading ranging from 10.6 to 115 μg/cm2. It was expected and observed that osteoclast activity surrounding the implant was inhibited. The cytocompatibility of the coatings and the effect of Sr-ions in different concentrations on osteoclast formation were analyzed in vitro. Osteoclast differentiation was elucidated on morphological, biochemical as well as on gene expression level. It could be shown that moderate concentrations of Sr2+ had an inhibitory effect on osteoclast formation, while the growth of osteoblastic cells was not negatively influenced compared to pure struvite surfaces. In summary, the electrochemically deposited Sr-doped struvite coatings are a promising approach to improve bone implant ingrowth.

Published

2019

31. Constitutional mismatch repair deficiency–associated brain tumors: report from the European C4CMMRD consortium

Author

Irene Slavc, Felipe Andreiuolo, Michaela Kuhlen, Chrystelle Colas, Laurence Brugières, Vanessa Perez-Alonso, Léa Guerrini-Rousseau, Jacques Grill, Sheila Unger, Cécile Faure-Conter, Salma Moalla, Yael Goldberg, Maurizio Genuardi, Astrid Sehested, Franck Bourdeaut, Katharina Wimmer, Christine Devalck, Enrico Opocher, Pascale Varlet, and Karin Dahan

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Clinical Investigations, Brain tumor, Consanguinity, Settore MED/03 - GENETICA MEDICA, 03 medical and health sciences, café-au-lait spot, 0302 clinical medicine, Germline mutation, Internal medicine, Glioma, Café au lait spot, constitutional mismatch repair deficiency, medicine, childhood cancer, business.industry, Standard treatment, MMR biallelic germline mutation, Cancer, medicine.disease, predisposition, 030104 developmental biology, repair, 030220 oncology & carcinogenesis, DNA mismatch repair, medicine.symptom, business, brain tumor, high-grade glioma

Abstract

Background Malignant brain tumors (BT) are among the cancers most frequently associated with constitutional mismatch repair deficiency (CMMRD), a rare childhood cancer predisposition syndrome resulting from biallelic germline mutations in mismatch repair genes. This study analyzed data from the European “Care for CMMRD” (C4CMMRD) database to describe their clinical characteristics, treatments, and outcome with the aim of improving its diagnosis/treatment. Methods Retrospective analysis of data on patients with CMMRD and malignant BT from the C4CMMRD database up to July 2017. Results Among the 87 registered patients, 49 developed 56 malignant BTs: 50 high-grade gliomas (HGG) (with giant multinucleated cells in 16/21 histologically reviewed tumors) and 6 embryonal tumors. The median age at first BT was 9.2 years [1.1–40.6], with nine patients older than 18. Twenty-seven patients developed multiple malignancies (including16 before the BT). Most patients received standard treatment, and eight patients immunotherapy for relapsed HGG. The 3- and 5-year overall survival (OS) rates were 30% (95% CI: 19–45) and 22% (95% CI: 12–37) after the first BT, with worse prognosis for HGG (3-year OS = 20.5%). Six patients were alive (median follow-up 2.5 years) and 43 dead (38 deaths, 88%, were BT-related). Other CMMRD-specific features were café-au-lait macules (40/41), multiple BTs (5/15), developmental brain anomalies (11/15), and consanguinity (20/38 families). Conclusions Several characteristics could help suspecting CMMRD in pediatric malignant BTs: giant cells on histology, previous malignancies, parental consanguinity, café-au-lait macules, multiple BTs, and developmental brain anomalies. The prognosis of CMMRD-associated BT treated with standard therapies is poor requiring new therapeutic up-front approaches.

Published

2019

32. Expanding the clinical phenotype of individuals with a 3-bp in-frame deletion of the NF1 gene (c.2970_2972del): an update of genotype-phenotype correlation

Author

Lynne M. Bird, Justin T. Jordan, Laura Dosa, Sébastien Perreault, Punita Gupta, Surya P. Rednam, Nicole J. Ullrich, Donald Basel, Linda M. Randolph, Leah W. Burke, Andrea Shugar, Angela Sharp, Ludwine Messiaen, Carey McDougall, Alicia Gomes, Andrea M. Lewis, Maurice J. Mahoney, Rachel K. Hachen, Marie T. McDonald, Katherine A. Rauen, Colette DeFilippo, Carmelo Piscopo, Maria Cristina Digilio, Sandra Janssens, Mary Ella M Pierpont, Lois J. Starr, Eric Legius, Michael F. Wangler, G. Bradley Schaefer, Arthur S. Aylsworth, Pamela Trapane, Ashraf Syed, Laurence E. Walsh, Alesha D. Hicks, Emily Wakefield, Robert Listernick, Nancy J. Mendelsohn, Elaine H. Zackai, Fortunato Lonardo, Dinel A. Pond, Robert S. Greenwood, Alessandro De Luca, Elizabeth K. Schorry, Rianne Oostenbrink, Katharina Wimmer, Ellen Denayer, Felicity Collins, Peter Kannu, Daryl A. Scott, S. Lane Rutledge, Yolanda Martin, Shelley K. Dills, Amedeo A. Azizi, Kristi J. Jones, David T. Miller, Gary Bellus, Yunjia Chen, Tom Callens, Magdalena Koczkowska, Kathleen Claes, Rick van Minkelen, Mayra Martinez Ojeda, Ashley Cannon, Bruce R. Korf, Cristin Griffis, Maria Blazo, Mari Mori, Veronica Saletti, Elizabeth Siqveland, Concepción Hernández-Chico, Pediatrics, and Clinical Genetics

Subjects

0301 basic medicine, Male, CHILDREN, 030105 genetics & heredity, GUIDELINES, neurofibroma, Correlation, Medicine and Health Sciences, Type 1 Neurofibromatosis, Neurofibroma, Child, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), learning difficulties, Genetics (clinical), Sequence Deletion, Genetics, Pediatric, Genetics & Heredity, Neurofibromin 1, Learning Disabilities, ASSOCIATION, genotype–phenotype correlation, Plexiform, Child, Preschool, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, NERVE SHEATH TUMORS, Female, p.Met992del, Adult, congenital, hereditary, and neonatal diseases and abnormalities, Heterozygote, VONRECKLINGHAUSEN NEUROFIBROMATOSIS, Neurofibromatosis 1, Adolescent, Clinical Sciences, Mutation, Missense, Biology, genotype-phenotype correlation, Article, Genotype phenotype, Neurofibromatosis, 03 medical and health sciences, Young Adult, Rare Diseases, Clinical Research, medicine, Humans, Genetic Predisposition to Disease, Clinical phenotype, Preschool, Gene, neoplasms, Genetic Association Studies, Neurofibroma, Plexiform, MUTATIONS, OPTIC PATHWAY TUMORS, Neurosciences, Correction, Biology and Life Sciences, Infant, SOUTH EAST WALES, medicine.disease, NOONAN SYNDROME, nervous system diseases, Brain Disorders, 030104 developmental biology, NF1, Mutation, Noonan syndrome, TYPE-1 NEUROFIBROMATOSIS, Missense

Abstract

PURPOSE: Neurofibromatosis type 1 (NF1) is characterized by a highly variable clinical presentation, but almost all NF1-affected adults present with cutaneous and/or subcutaneous neurofibromas. Exceptions are individuals heterozygous for the NF1 in-frame deletion, c.2970_2972del (p.Met992del), associated with a mild phenotype without any externally visible tumors. METHODS: A total of 135 individuals from 103 unrelated families, all carrying the constitutional NF1 p.Met992del pathogenic variant and clinically assessed using the same standardized phenotypic checklist form, were included in this study. RESULTS: None of the individuals had externally visible plexiform or histopathologically confirmed cutaneous or subcutaneous neurofibromas. We did not identify any complications, such as symptomatic optic pathway gliomas (OPGs) or symptomatic spinal neurofibromas; however, 4.8% of individuals had nonoptic brain tumors, mostly low-grade and asymptomatic, and 38.8% had cognitive impairment/learning disabilities. In an individual with the NF1 constitutional c.2970_2972del and three astrocytomas, we provided proof that all were NF1-associated tumors given loss of heterozygosity at three intragenic NF1 microsatellite markers and c.2970_2972del. CONCLUSION: We demonstrate that individuals with the NF1 p.Met992del pathogenic variant have a mild NF1 phenotype lacking clinically suspected plexiform, cutaneous, or subcutaneous neurofibromas. However, learning difficulties are clearly part of the phenotypic presentation in these individuals and will require specialized care. ispartof: GENETICS IN MEDICINE vol:21 issue:4 pages:867-876 ispartof: location:United States status: published

Published

2019

33. Constitutional mismatch repair deficiency as a differential diagnosis of neurofibromatosis type 1: consensus guidelines for testing a child without malignancy

Author

Christian P. Kratz, Manon Suerink, Irene Slavc, Ludwine Messiaen, Marjolijn C.J. Jongmans, Katharina Wimmer, Yael Goldberg, Franck Bourdeaut, Martine Muleris, Eric Legius, Mariëtte C.A. van Kouwen, Hans F. A. Vasen, Chrystelle Colas, Maartje Nielsen, Laurence Brugiѐres, Fred H. Menko, Tim Ripperger, VU University Medical Center [Amsterdam], Unité de génétique et biologie des cancers (U830), Université Paris Descartes - Paris 5 (UPD5)-Institut Curie [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre de Recherche Saint-Antoine (UMRS893), Université Pierre et Marie Curie - Paris 6 (UPMC)-Institut National de la Santé et de la Recherche Médicale (INSERM), Department of Clinical Genetics, Leiden University Medical Center (LUMC), Human Genetics, Catholic University of Leuven, Department of Medical Genetics, Medical University of Vienna, Vienna, Université Paris Descartes - Paris 5 (UPD5)-Institut Curie-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre de Recherche Saint-Antoine (CR Saint-Antoine), and Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Pierre et Marie Curie - Paris 6 (UPMC)

Subjects

0301 basic medicine, Parents, Pediatrics, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Neurofibromatosis 1, [SDV]Life Sciences [q-bio], Genetic Counseling, 030105 genetics & heredity, Malignancy, Diagnosis, Differential, 03 medical and health sciences, Germline mutation, Neoplastic Syndromes, Hereditary, Tumours of the digestive tract Radboud Institute for Molecular Life Sciences [Radboudumc 14], Genetics, medicine, Humans, Genetic Testing, Neurofibromatosis, Genetics (clinical), ComputingMilieux_MISCELLANEOUS, Adaptor Proteins, Signal Transducing, Mismatch Repair Endonuclease PMS2, Legius syndrome, business.industry, Brain Neoplasms, Incidence, Patient Selection, Guideline, medicine.disease, 3. Good health, 030104 developmental biology, Mutation, Practice Guidelines as Topic, MISMATCH REPAIR DEFICIENCY, Medical genetics, Differential diagnosis, business, Colorectal Neoplasms, MutL Protein Homolog 1

Abstract

Constitutional mismatch repair deficiency (CMMRD) is a rare childhood cancer predisposition syndrome caused by biallelic germline mutations in one of four mismatch-repair genes. Besides very high tumour risks, CMMRD phenotypes are often characterised by the presence of signs reminiscent of neurofibromatosis type 1 (NF1). Because NF1 signs may be present prior to tumour onset, CMMRD is a legitimate differential diagnosis in an otherwise healthy child suspected to have NF1/Legius syndrome without a detectable underlying NF1/SPRED1 germline mutation. However, no guidelines indicate when to counsel and test for CMMRD in this setting. Assuming that CMMRD is rare in these patients and that expected benefits of identifying CMMRD prior to tumour onset should outweigh potential harms associated with CMMRD counselling and testing in this setting, we aimed at elaborating a strategy to preselect, among children suspected to have NF1/Legius syndrome without a causative NF1/SPRED1 mutation and no overt malignancy, those children who have a higher probability of having CMMRD. At an interdisciplinary workshop, we discussed estimations of the frequency of CMMRD as a differential diagnosis of NF1 and potential benefits and harms of CMMRD counselling and testing in a healthy child with no malignancy. Preselection criteria and strategies for counselling and testing were developed and reviewed in two rounds of critical revisions. Existing diagnostic CMMRD criteria were adapted to serve as a guideline as to when to consider CMMRD as differential diagnosis of NF1/Legius syndrome. In addition, counselling and testing strategies are suggested to minimise potential harms.

Published

2019

34. Mystique, langage, musique : dire l’indicible au Moyen Âge

Author

Katharina Wimmer

Published

2019

35. Early colorectal cancers provide new evidence for a Lynch Syndrome-to-CMMRD Phenotypic Continuum

Author

Consuelo Calviño-Costas, Sahra Bodo, Ceres Fernandez-Rozadilla, Martine Muleris, Esther Schamschula, Anael López-Novo, A. Lancho, Clara Ruiz-Ponte, Katharina Wimmer, Xabier Bello, José Manuel Cameselle-Teijeiro, Angel Carracedo, Miriam Alvarez-Barona, Jorge Amigo, Chrystelle Colas, A Dacal, Universidade de Santiago de Compostela. Departamento de Ciencias Forenses, Anatomía Patolóxica, Xinecoloxía e Obstetricia, e Pediatría, Fundación Pública Galega Medicina Xenómica - SERGAS [Santiago de Compostela, Spain] (Grupo de Medicina Xenómica), CIBER de Enfermedades Raras (CIBERER)-Universidade de Santiago de Compostela [Spain] (USC ), Innsbruck Medical University [Austria] (IMU), Department of Biosciences [Salzburg, Austria ), Paris-Lodron-Universität Salzburg (PLUS), Centre de Recherche Saint-Antoine (CR Saint-Antoine), Sorbonne Université (SU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-CHU Saint-Antoine [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Servicio de Gastroenterología [Lugo, Spain], Hospital Universitario Lucus Augusti [Lugo, Spain], Servicio de Pediatría [Lugo, Spain], Servicio de Anatomía Patológica [Santiago de Compostela, Spain], Complejo Hospitalario Universitario de Santiago de Compostela [Saint-Jacques-de-Compostelle, Espagne] (CHUS), Centro de Investigación Biomédica en Red de Enfermedades Raras - CIBERER [Santiago de Compostela, Spain] (Grupo de Medicina Xenómica), Universidade de Santiago de Compostela [Spain] (USC ), Institut Curie [Paris], Innsbruck Medical University = Medizinische Universität Innsbruck (IMU), Centre de Recherche Saint-Antoine (CRSA), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), and Gestionnaire, Hal Sorbonne Université

Subjects

0301 basic medicine, Genetic modifiers, Cancer Research, Colorectal cancer, phenotypic continuum, [SDV.CAN]Life Sciences [q-bio]/Cancer, MLH1, lcsh:RC254-282, 03 medical and health sciences, [SDV.MHEP.PED] Life Sciences [q-bio]/Human health and pathology/Pediatrics, 0302 clinical medicine, [SDV.CAN] Life Sciences [q-bio]/Cancer, [SDV.BBM.GTP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Genomics [q-bio.GN], Medicine, whole-exome sequencing, Allele, Exome sequencing, Genetics, [SDV.MHEP.PED]Life Sciences [q-bio]/Human health and pathology/Pediatrics, Cancer prevention, Phenotypic continuum, business.industry, Communication, Cancer, [SDV.MHEP.HEG]Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology, genetic modifiers, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, [SDV.MHEP.HEG] Life Sciences [q-bio]/Human health and pathology/Hépatology and Gastroenterology, Lynch syndrome, CMMRD, 3. Good health, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Whole-exome sequencing, [SDV.BBM.GTP] Life Sciences [q-bio]/Biochemistry, Molecular Biology/Genomics [q-bio.GN], DNA mismatch repair, business

Abstract

Lynch syndrome (LS) is the most common hereditary colorectal cancer (CRC) syndrome, caused by heterozygous mutations in the mismatch repair (MMR) genes. Biallelic mutations in these genes lead however, to constitutive mismatch repair deficiency (CMMRD). In this study, we follow the diagnostic journey of a 12-year old patient with CRC, with a clinical phenotype overlapping CMMRD. We perform molecular and functional assays to discard a CMMRD diagnosis then identify by exome sequencing and validation in a cohort of 134 LS patients, a candidate variant in the MLH1 UTR region in homozygosis. We propose that this variant, together with other candidates, could be responsible for age-of-onset modulation. Our data support the idea that low-risk modifier alleles may influence early development of cancer in LS leading to a LS-to-CMMRD phenotypic continuum. Therefore, it is essential that larger efforts are directed to the identification and study of these genetic modifiers, in order to provide optimal cancer prevention strategies to these patients. This research was funded by Spanish National Centre for Genomic Analysis (CNAG, Barcelona). This work was supported by the 2013 CNAG call: 300-exomes to elucidate Rare-Diseases to C.R.-P SI

Published

2019

36. Constitutional mismatch repair deficiency-associated brain tumors: report from the European C4CMMRD consortium

Author

Léa Guerrini-Rousseau, 1 2, Pascale Varlet, 3, Chrystelle Colas, 4, Felipe Andreiuolo, 3, Franck Bourdeaut, 5, Karin Dahan, 6, Christine Devalck, 7, Cécile Faure-Conter, 8, Genuardi, M., Yael Goldberg, 11, Michaela Kuhlen, 12, Salma Moalla, 13, Enrico Opocher, 14, Vanessa Perez-Alonso, 15, Astrid Sehested, 16, Irene Slavc, 17, Sheila Unger, 18, Katharina Wimmer, 19, Jacques Grill, 1 2, Laurence Brugières, 1, Genuardi M. (ORCID:0000-0002-7410-8351), Léa Guerrini-Rousseau, 1 2, Pascale Varlet, 3, Chrystelle Colas, 4, Felipe Andreiuolo, 3, Franck Bourdeaut, 5, Karin Dahan, 6, Christine Devalck, 7, Cécile Faure-Conter, 8, Genuardi, M., Yael Goldberg, 11, Michaela Kuhlen, 12, Salma Moalla, 13, Enrico Opocher, 14, Vanessa Perez-Alonso, 15, Astrid Sehested, 16, Irene Slavc, 17, Sheila Unger, 18, Katharina Wimmer, 19, Jacques Grill, 1 2, Laurence Brugières, 1, and Genuardi M. (ORCID:0000-0002-7410-8351)

Abstract

Background: Malignant brain tumors (BT) are among the cancers most frequently associated with constitutional mismatch repair deficiency (CMMRD), a rare childhood cancer predisposition syndrome resulting from biallelic germline mutations in mismatch repair genes. This study analyzed data from the European "Care for CMMRD" (C4CMMRD) database to describe their clinical characteristics, treatments, and outcome with the aim of improving its diagnosis/treatment. Methods: Retrospective analysis of data on patients with CMMRD and malignant BT from the C4CMMRD database up to July 2017. Results: Among the 87 registered patients, 49 developed 56 malignant BTs: 50 high-grade gliomas (HGG) (with giant multinucleated cells in 16/21 histologically reviewed tumors) and 6 embryonal tumors. The median age at first BT was 9.2 years [1.1-40.6], with nine patients older than 18. Twenty-seven patients developed multiple malignancies (including16 before the BT). Most patients received standard treatment, and eight patients immunotherapy for relapsed HGG. The 3- and 5-year overall survival (OS) rates were 30% (95% CI: 19-45) and 22% (95% CI: 12-37) after the first BT, with worse prognosis for HGG (3-year OS = 20.5%). Six patients were alive (median follow-up 2.5 years) and 43 dead (38 deaths, 88%, were BT-related). Other CMMRD-specific features were café-au-lait macules (40/41), multiple BTs (5/15), developmental brain anomalies (11/15), and consanguinity (20/38 families). Conclusions: Several characteristics could help suspecting CMMRD in pediatric malignant BTs: giant cells on histology, previous malignancies, parental consanguinity, café-au-lait macules, multiple BTs, and developmental brain anomalies. The prognosis of CMMRD-associated BT treated with standard therapies is poor requiring new therapeutic up-front approaches. Keywords: MMR biallelic germline mutation; brain tumor; café-au-lait spot; childhood cancer; constitutional mismatch repair deficiency; high-grade glioma; predisp

Published

2019

37. A novel germline POLE mutation causes an early onset cancer prone syndrome mimicking constitutional mismatch repair deficiency

Author

Rainer Nustede, Katharina Wimmer, Ulrich Lehmann, Johannes Zschocke, Andreas Beilken, Tim Ripperger, Laura Valle, Diana Steinmann, Christian P. Kratz, Tanja Reineke-Plaass, Christine Fauth, Benno M. Ure, and Britta Lamottke

Subjects

Male, 0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Polymerase proofreading-associated polyposis, Skin Neoplasms, Adolescent, DNA repair, Biology, medicine.disease_cause, Germline, 03 medical and health sciences, 0302 clinical medicine, Germline mutation, Café-au-lait macule, Neoplastic Syndromes, Hereditary, Genetics, medicine, Humans, Genetics(clinical), Age of Onset, Poly-ADP-Ribose Binding Proteins, Germ-Line Mutation, Genetics (clinical), Mutation, POLD1, Brain Neoplasms, Cafe-au-Lait Spots, Cancer, Microsatellite instability, Pilomatricoma, DNA Polymerase II, Pilomatrixoma, medicine.disease, Colon cancer, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Original Article, Microsatellite Instability, Colorectal Neoplasms, Hair Diseases, Constitutional mismatch repair deficiency

Abstract

In a 14-year-old boy with polyposis and rectosigmoid carcinoma, we identified a novel POLE germline mutation, p.(Val411Leu), previously found as recurrent somatic mutation in 'ultramutated' sporadic cancers. This is the youngest reported cancer patient with polymerase proofreading-associated polyposis indicating that POLE mutation p.(Val411Leu) may confer a more severe phenotype than previously reported POLE and POLD1 germline mutations. The patient had multiple café-au-lait macules and a pilomatricoma mimicking the clinical phenotype of constitutional mismatch repair deficiency. We hypothesize that these skin features may be common to different types of constitutional DNA repair defects associated with polyposis and early-onset cancer.

Published

2016

38. PMS2 inactivation by a complex rearrangement involving an HERV retroelement and the inverted 100-kb duplicon on 7p22.1

Author

Johannes Zschocke, Christian P. Kratz, Annekatrin Wernstedt, Tim Ripperger, Julia Vogt, Katharina Wimmer, and Brigitte Pabst

Subjects

Male, 0301 basic medicine, Locus (genetics), Chromosomal rearrangement, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Neoplastic Syndromes, Hereditary, Genetics, PMS2, Humans, Child, Gene, Genetics (clinical), Mismatch Repair Endonuclease PMS2, Sequence Inversion, Gene Rearrangement, Brain Neoplasms, Chromosome Fragile Sites, Chromosomal fragile site, Endogenous Retroviruses, Homozygote, Gene rearrangement, 030104 developmental biology, Chromosome Fragile Site, 030220 oncology & carcinogenesis, Colorectal Neoplasms, Chromosomes, Human, Pair 7

Abstract

Biallelic PMS2 mutations are responsible for more than half of all cases of constitutional mismatch repair deficiency (CMMRD), a recessively inherited childhood cancer predisposition syndrome. The mismatch repair gene PMS2 is partly embedded within one copy of an inverted 100-kb low-copy repeat (LCR) on 7p22.1. In an individual with CMMRD syndrome, PMS2 was found to be homozygously inactivated by a complex chromosomal rearrangement, which separates the 5'-part from the 3'-part of the gene. The rearrangement involves sequences of the inverted 100-kb LCR and a human endogenous retrovirus element and may be associated with an inversion that is indistinguishable from the known inversion polymorphism affecting the ~0.7-Mb sequence intervening the LCR. Its formation is best explained by a replication-based mechanism (RBM) such as fork stalling and template switching/microhomology-mediated break-induced replication (FoSTeS/MMBIR). This finding supports the hypothesis that the inverted LCR can not only facilitate the formation of the non-allelic homologous recombination-mediated inversion polymorphism but it also promotes the occurrence of more complex rearrangements that can be associated with a large inversion, as well, but are mediated by a RBM. This further suggests that among the inversion polymorphism on 7p22.1, more complex rearrangements might be hidden. Furthermore, as the locus is embedded in a common fragile site (CFS) region, this rearrangement also supports the recently raised hypothesis that CFS sequence motifs may facilitate replication-based rearrangement mechanisms.

Published

2016

39. Cleft lip/palate and hereditary diffuse gastric cancer: report of a family harboring a CDH1 c.687 + 1G A germline mutation and review of the literature

Author

Florian Obermair, Wolfgang Kranewitter, Katharina Wimmer, Jonathan Burghofer, Anna Schossig, Melanie Rammer, Hans-Christoph Duba, Gerald Webersinke, Beate Mayrbaeurl, and Theodora Malli

Subjects

0301 basic medicine, Adult, Male, Cancer Research, Heterozygote, Cleft Lip, 030105 genetics & heredity, medicine.disease_cause, CDH1, 03 medical and health sciences, Exon, 0302 clinical medicine, Germline mutation, Antigens, CD, Neoplastic Syndromes, Hereditary, Stomach Neoplasms, Genetics, medicine, Humans, Protein Interaction Domains and Motifs, Genetics (clinical), Germ-Line Mutation, Aged, Mutation, Splice site mutation, biology, Cancer, Exons, bacterial infections and mycoses, medicine.disease, Cadherins, Human genetics, Pedigree, Cleft Palate, stomatognathic diseases, Oncology, 030220 oncology & carcinogenesis, biology.protein, Female, Hereditary diffuse gastric cancer

Abstract

Hereditary diffuse gastric cancer (HDGC) is an autosomal-dominantly inherited cancer syndrome associated with a high risk for diffuse gastric and lobular breast cancer, caused by heterozygous CDH1 germline mutations. Of note, also cleft lip/palate (CLP) has been described in few HDGC families. Here we report on an extensive pedigree presenting with HDGC, CLP and a CDH1 splice site mutation (c.687 + 1G > A) and review the literature for families with CDH1 mutations, HDGC and CLP. Transcript analysis showed that the c.687 + 1G > A mutation leads to loss of the last 42 bp of exon 5 and is consequently predicted to cause loss of 14 amino acids in the first extracellular cadherin repeat (EC) domain. Five mutation carriers developed diffuse gastric cancer and four individuals presented with CLP. Wild type CDH1 expression levels did not differ between CDH1 mutation carriers with CLP compared to those without CLP. Beside this extensive pedigree, we outline another previously unreported HDGC/CLP family with a CDH1 (c.1711 + 1G > C) germline mutation in this study. Review of the literature revealed a significant enrichment of CDH1 mutations within the EC domains in CLP/HDGC families (Fisher’s exact test, p = 0.007) in comparison to CDH1 mutations associated with HDGC only. Report of further CLP/HDGC associated mutations is necessary to confirm this observation. This study highlights that CLP represents an important phenotypic feature of CDH1 germline mutation carriers and emphasizes the inclusion of CLP in the HDGC testing criteria. The underlying causes for the appearance of variable phenotypes in CDH1 mutation carriers could include genetic variation, epigenetic changes and environmental factors and should be investigated in future studies.

Published

2018

40. Constitutional Mismatch Repair Deficiency

Author

Laurence Brugières, Katharina Wimmer, and Chrystelle Colas

Subjects

Biallelic Mutation, congenital, hereditary, and neonatal diseases and abnormalities, business.industry, Colorectal cancer, nutritional and metabolic diseases, medicine.disease, MLH1, digestive system diseases, Lynch syndrome, MSH6, MSH2, Cancer research, PMS2, Medicine, Neurofibromatosis, business

Abstract

Inherited heterozygous mutations in the MMR genes result in Lynch syndrome (LS). Individuals with biallelic mutation of one of the MMR genes developed malignancies in childhood. This recessively inherited condition is named CMMRD for constitutional mismatch repair deficiency. The spectrum of tumours is distinct from LS. Malignant brain tumours are at least as frequent as gastrointestinal tumours, and in more than a third of cases, haematological malignancies were also reported. Patients also displayed clinical features of neurofibromatosis type 1. The most commonly involved genes in CMMRD are PMS2 and MSH6, while biallelic MLH1 and MSH2 mutations are rare.

Published

2018

41. Correction: Expanding the clinical phenotype of individuals with a 3-bp in-frame deletion of the NF1 gene (c.2970_2972del): an update of genotype–phenotype correlation

Author

Ludwine Messiaen, Ashley Cannon, Concepción Hernández-Chico, Yolanda Martin, Andrea Shugar, Mary Ella M Pierpont, Robert S. Greenwood, Yunjia Chen, Fortunato Lonardo, Ellen Denayer, Arthur S. Aylsworth, Shelley K. Dills, Mayra Martinez Ojeda, Elizabeth K. Schorry, Amedeo A. Azizi, Lois J. Starr, Andrea M. Lewis, Rianne Oostenbrink, Bruce R. Korf, Pamela Trapane, Peter Kannu, Daryl A. Scott, Elizabeth Siqveland, Rick van Minkelen, Justin T. Jordan, Laura Dosa, Nancy J. Mendelsohn, David T. Miller, Dinel A. Pond, Alessandro De Luca, Elaine H. Zackai, Rachel K. Hachen, Donald Basel, Linda M. Randolph, Eric Legius, Maurice J. Mahoney, Tom Callens, Maria Cristina Digilio, Alesha D. Hicks, Carmelo Piscopo, Sandra Janssens, Katherine A. Rauen, Michael F. Wangler, Ashraf Syed, Emily Wakefield, Punita Gupta, Lynne M. Bird, Alicia Gomes, Marie T. McDonald, Katharina Wimmer, S. Lane Rutledge, Colette DeFilippo, Robert Listernick, Kathleen Claes, Surya P. Rednam, Nicole J. Ullrich, Leah W. Burke, Carey McDougall, Sébastien Perreault, Gary Bellus, Magdalena Koczkowska, Cristin Griffis, Laurence E. Walsh, Angela Sharp, Felicity Collins, Maria Blazo, Kristi J. Jones, Mari Mori, Veronica Saletti, and G. Bradley Schaefer

Subjects

Genetics, Correlation, Frame (networking), ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, Biology, Clinical phenotype, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), Gene, Genetics (clinical), Genotype phenotype

Abstract

A correction has been published to this Article. The PDF and HTML have been updated accordingly.

Published

2019

42. Constitutional Mismatch Repair Deficiency in Israel: High Proportion of Founder Mutations in MMR Genes and Consanguinity

Author

Israela Lerer, Marisa Halpern, Nurit Magal, Hagit N. Baris, Valerie Drasinover, Zohar Levi, Katharina Wimmer, Shlomi Cohen, Inbal Barnes-Kedar, Dov Hershkovitz, Helen Toledano, Tamar Peretz, Dani Bercovich, Elizabeth E. Half, Revital Kariv, Alexander Lossos, and Yael Goldberg

Subjects

0301 basic medicine, Genetics, congenital, hereditary, and neonatal diseases and abnormalities, business.industry, Hematology, Consanguinity, Gene mutation, medicine.disease, digestive system diseases, Lynch syndrome, MSH6, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Germline mutation, Oncology, MSH2, 030220 oncology & carcinogenesis, Pediatrics, Perinatology and Child Health, medicine, PMS2, business, Founder effect

Abstract

Background Heterozygous germline mutations in any of the mismatch repair (MMR) genes, MLH1, MSH2, MSH6, and PMS2, cause Lynch syndrome (LS), an autosomal dominant cancer predisposition syndrome conferring a high risk of colorectal, endometrial, and other cancers in adulthood. Offspring of couples where both spouses have LS have a 1:4 risk of inheriting biallelic MMR gene mutations. These cause constitutional MMR deficiency (CMMRD) syndrome, a severe recessively inherited cancer syndrome with a broad tumor spectrum including mainly hematological malignancies, brain tumors, and colon cancer in childhood and adolescence. Many CMMRD children also present with cafe au lait spots and axillary freckling mimicking neurofibromatosis type 1. Procedure We describe our experience in seven CMMRD families demonstrating the role and importance of founder mutations and consanguinity on its prevalence. Clinical presentations included brain tumors, colon cancer, lymphoma, and small bowel cancer. Results In children from two nonconsanguineous Ashkenazi Jewish (AJ) families, the common Ashkenazi founder mutations were detected; these were homozygous in one family and compound heterozygous in the other. In four consanguineous families of various ancestries, different homozygous mutations were identified. In a nonconsanguineous Caucasus/AJ family, lack of PMS2 was demonstrated in tumor and normal tissues; however, mutations were not identified. Conclusions CMMRD is rare, but, especially in areas where founder mutations for LS and consanguinity are common, pediatricians should be aware of it since they are the first to encounter these children. Early diagnosis will enable tailored cancer surveillance in the entire family and a discussion regarding prenatal genetic diagnosis.

Published

2015

43. Decoding NF1 Intragenic Copy-Number Variations

Author

Katharina Wimmer, Arkadiusz Piotrowski, Chuanhua Fu, Kathleen Claes, Meng-Chang Hsiao, Ludwine Messiaen, and Tom Callens

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Neurofibromatosis 1, DNA Copy Number Variations, DNA Mutational Analysis, Alu element, Biology, Polymerase Chain Reaction, Article, Structural variation, Chromosome Breakpoints, symbols.namesake, Genetics, Humans, Genetics(clinical), Copy-number variation, In Situ Hybridization, Fluorescence, Genetics (clinical), Comparative Genomic Hybridization, Neurofibromin 1, Breakpoint, Intron, Mendelian inheritance, symbols, Homologous recombination, Comparative genomic hybridization

Abstract

Genomic rearrangements can cause both Mendelian and complex disorders. Currently, several major mechanisms causing genomic rearrangements, such as non-allelic homologous recombination (NAHR), non-homologous end joining (NHEJ), fork stalling and template switching (FoSTeS), and microhomology-mediated break-induced replication (MMBIR), have been proposed. However, to what extent these mechanisms contribute to gene-specific pathogenic copy-number variations (CNVs) remains understudied. Furthermore, few studies have resolved these pathogenic alterations at the nucleotide-level. Accordingly, our aim was to explore which mechanisms contribute to a large, unique set of locus-specific non-recurrent genomic rearrangements causing the genetic neurocutaneous disorder neurofibromatosis type 1 (NF1). Through breakpoint-spanning PCR as well as array comparative genomic hybridization, we have identified the breakpoints in 85 unrelated individuals carrying an NF1 intragenic CNV. Furthermore, we characterized the likely rearrangement mechanisms of these 85 CNVs, along with those of two additional previously published NF1 intragenic CNVs. Unlike the most typical recurrent rearrangements mediated by flanking low-copy repeats (LCRs), NF1 intragenic rearrangements vary in size, location, and rearrangement mechanisms. We propose the DNA-replication-based mechanisms comprising both FoSTeS and/or MMBIR and serial replication stalling to be the predominant mechanisms leading to NF1 intragenic CNVs. In addition to the loop within a 197-bp palindrome located in intron 40, four Alu elements located in introns 1, 2, 3, and 50 were also identified as intragenic-rearrangement hotspots within NF1.

Published

2015

44. panelcn.MOPS: Copy-number detection in targeted NGS panel data for clinical diagnostics

Author

Günter Klambauer, Johannes Zschocke, Ludwine Messiaen, Sepp Hochreiter, Antigoni Tzika, Verena Haunschmid, Julia Vogt, Katharina Wimmer, and Gundula Povysil

Subjects

0301 basic medicine, Quality Control, DNA Copy Number Variations, Computational biology, Biology, Sensitivity and Specificity, Rendering (computer graphics), 03 medical and health sciences, symbols.namesake, User-Computer Interface, Software, Targeted ngs, Region of interest, copy‐number variation, Databases, Genetic, Genetics, Methods, Computer Graphics, Humans, Copy-number variation, deletion, Genetics (clinical), clinical diagnostics, Gene Library, Sanger sequencing, panel sequencing, business.industry, Computational Biology, High-Throughput Nucleotide Sequencing, Reproducibility of Results, Sequence Analysis, DNA, R package, 030104 developmental biology, duplication, symbols, business, targeted next‐generation sequencing, Algorithms, Panel data

Abstract

Targeted next‐generation‐sequencing (NGS) panels have largely replaced Sanger sequencing in clinical diagnostics. They allow for the detection of copy‐number variations (CNVs) in addition to single‐nucleotide variants and small insertions/deletions. However, existing computational CNV detection methods have shortcomings regarding accuracy, quality control (QC), incidental findings, and user‐friendliness. We developed panelcn.MOPS, a novel pipeline for detecting CNVs in targeted NGS panel data. Using data from 180 samples, we compared panelcn.MOPS with five state‐of‐the‐art methods. With panelcn.MOPS leading the field, most methods achieved comparably high accuracy. panelcn.MOPS reliably detected CNVs ranging in size from part of a region of interest (ROI), to whole genes, which may comprise all ROIs investigated in a given sample. The latter is enabled by analyzing reads from all ROIs of the panel, but presenting results exclusively for user‐selected genes, thus avoiding incidental findings. Additionally, panelcn.MOPS offers QC criteria not only for samples, but also for individual ROIs within a sample, which increases the confidence in called CNVs. panelcn.MOPS is freely available both as R package and standalone software with graphical user interface that is easy to use for clinical geneticists without any programming experience. panelcn.MOPS combines high sensitivity and specificity with user‐friendliness rendering it highly suitable for routine clinical diagnostics.

Published

2017

45. Diagnostic criteria for constitutional mismatch repair deficiency syndrome: suggestions of the European consortium ‘Care for CMMRD’ (C4CMMRD)

Author

Hans F. A. Vasen, Yael Goldberg, Irene Slavc, Denisa Ilencikova, Anne-Marie Gerdes, Noémie Lavoine, Clara Ruiz-Ponte, Chrystelle Colas, Laurence Brugières, Christian P. Kratz, Alex Duval, Brigit Burkhardt, Martine Muleris, Olivier Caron, Natacha Entz-Werle, and Katharina Wimmer

Subjects

Pediatrics, medicine.medical_specialty, Population, Malignancy, CMMRD syndrome, Germline mutation, Neoplastic Syndromes, Hereditary, Genetics, medicine, PMS2, Humans, education, Genetics (clinical), education.field_of_study, Brain Neoplasms, business.industry, Cancer, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Lynch syndrome, Europe, MSH6, MSH2, Colorectal Neoplasms, business, Pigmentation Disorders

Abstract

Constitutional mismatch repair deficiency (CMMRD) syndrome is a distinct childhood cancer predisposition syndrome that results from biallelic germline mutations in one of the four MMR genes, MLH1, MSH2, MSH6 or PMS2. The tumour spectrum is very broad, including mainly haematological, brain and intestinal tract tumours. Patients show a variety of non-malignant features that are indicative of CMMRD. However, currently no criteria that should entail diagnostic evaluation of CMMRD exist. We present a three-point scoring system for the suspected diagnosis CMMRD in a paediatric/young adult cancer patient. Tumours highly specific for CMMRD syndrome are assigned three points, malignancies overrepresented in CMMRD two points and all other malignancies one point. According to their specificity for CMMRD and their frequency in the general population, additional features are weighted with 1-2 points. They include multiple hyperpigmented and hypopigmented skin areas, brain malformations, pilomatricomas, a second childhood malignancy, a Lynch syndrome (LS)-associated tumour in a relative and parental consanguinity. According to the scoring system, CMMRD should be suspected in any cancer patient who reaches a minimum of three points by adding the points of the malignancy and the additional features. The diagnostic steps to confirm or refute the suspected diagnosis are outlined. We expect that application of the suggested strategy for CMMRD diagnosis will increase the number of patients being identified at the time when they develop their first tumour. This will allow adjustment of the treatment modalities, offering surveillance strategies for second malignancies and appropriate counselling of the entire family.

Published

2014

46. EPCAMgermline and somatic rearrangements in lynch syndrome: identification of a novel 3′EPCAMdeletion

Author

Gert De Hertogh, Eric Legius, Marijke Spaepen, Eline Beert, Xavier Sagaert, Hilde Brems, Esther Neven, Gert Matthijs, and Katharina Wimmer

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Mutation, Somatic cell, nutritional and metabolic diseases, Epithelial cell adhesion molecule, Biology, medicine.disease, medicine.disease_cause, Molecular biology, digestive system diseases, Germline, Lynch syndrome, Loss of heterozygosity, MSH6, chemistry.chemical_compound, chemistry, MSH2, Genetics, medicine, neoplasms

Abstract

3′EPCAM (Epithelial Cell Adhesion Molecule) genomic rearrangements can be a cause of mismatch repair deficiency in rare Lynch syndrome families. 3′EPCAM deletions include the polyadenylation signal and might result in promoter hypermethylation of the centromeric MSH2 gene in cis. A somatic rearrangement in trans affecting MSH2 is responsible for the final mismatch repair deficiency in the corresponding tumors but the mechanisms are not well documented. In this report two germline 3′EPCAM deletions are described together with the corresponding somatic mutations in the patient's colorectal tumors. Mutation and breakpoint analysis resulted in the identification of one novel (c.556-531_*872del) and one known EPCAM deletion (c.859-689_*14697del). Both deletions resulted from Alu mediated homologous recombination causing aberrant EPCAM-MSH2 fusion transcripts. The colorectal tumors of the deletion carriers were MSI-high. Strong hypermethylation of the MSH2 promoter was measured. Analysis of somatic genomic rearrangements showed a 4 Mb deletion including the EPCAM, MSH2 and MSH6 genes in one tumor and copy neutral loss of heterozygosity in the EPCAM-MSH2 region in the other tumor. This indicates that hemi- and homozygous hypermethylation of the MSH2 promoter and hence complete silencing of MSH2 expression was responsible for the mismatch repair deficiency in both colorectal tumors. © 2013 Wiley Periodicals, Inc.

Published

2013

47. KohlschutterTonz Syndrome

Author

John Hardy, Heather C Mefford, Eleanna Kara, Corina Hennig, Arianna Tucci, Silvia Palmeri, Thomas Bast, Katharina Wimmer, Katherine A. Fawcett, Coro Paisán-Ruiz, Evan E. Eichler, Anna Schossig, Sebastiano Musumeci, Henry Houlden, Johannes Zschocke, Roel Hordijk, Andrew B. Singleton, Matthew Moore, Dian Donnai, Simon Shorvon, Alessandro Malandrini, Vincent Plagnol, Michael B. Tennison, Nicole I. Wolf, Salmo Raskin, Andreas Tzschach, Dena G. Hernandez, Roger K. Hall, Raoul C.M. Hennekam, Ian P Hayes, Chien Ning Lo, ANS - Amsterdam Neuroscience, APH - Amsterdam Public Health, Human Genetics, Paediatrics, Pediatric surgery, and NCA - Brain mechanisms in health and disease

Subjects

Male, Genetic Linkage, KohlschutterTonz, ROGDI, amelogenesis imperfecta, epilepsy, Biology, Kohlschütter-Tönz syndrome, Compound heterozygosity, Bioinformatics, medicine.disease_cause, Article, Genetic Heterogeneity, symbols.namesake, Genetic linkage, Genetics, medicine, Humans, Exome, Genetics (clinical), Exome sequencing, Sanger sequencing, AMELOGENESIS-IMPERFECTA, Mutation, Genetic heterogeneity, DEMENTIA, Infant, Membrane Proteins, Nuclear Proteins, YELLOW TEETH, Sequence Analysis, DNA, medicine.disease, Pedigree, TONZ-SYNDROME, FAMILY, Phenotype, Child, Preschool, ENAMEL HYPOPLASIA, symbols, Female, Gene Deletion

Abstract

Kohlschutter-Tonz syndrome (KTS) is a rare autosomal recessive disorder characterized by amelogenesis imperfecta, psychomotor delay or regression and seizures starting early in childhood. KTS was established as a distinct clinical entity after the first report by Kohlschutter in 1974, and to date, only a total of 20 pedigrees have been reported. The genetic etiology of KTS remained elusive until recently when mutations in ROGDI were independently identified in three unrelated families and in five likely related Druze families. Herein, we report a clinical and genetic study of 10 KTS families. By using a combination of whole exome sequencing, linkage analysis, and Sanger sequencing, we identify novel homozygous or compound heterozygous ROGDI mutations in five families, all presenting with a typical KTS phenotype. The other families, mostly presenting with additional atypical features, were negative for ROGDI mutations, suggesting genetic heterogeneity of atypical forms of the disease. © 2012 Wiley Periodicals, Inc.

Published

2013

48. Agenesis of the corpus callosum and gray matter heterotopia in three patients with constitutional mismatch repair deficiency syndrome

Author

Mieke M. van Haelst, Rutger A.J. Nievelstein, Stephen P. Robertson, Milan Rimac, Danielle Bodmer, Michael T. Gabbett, Minna Nyström, Annekatrin Wernstedt, Johan Offerhaus, Birgit Krabichler, Johannes Zschocke, Martine Raphael, Katharina Wimmer, Minttu Kansikas, Wayne Nicholls, Ulrich Strasser, Annette F. Baas, Pediatric surgery, Human genetics, Amsterdam Neuroscience - Complex Trait Genetics, Amsterdam Reproduction & Development (AR&D), Pathology, and Other departments

Subjects

Male, Gray matter heterotopia, Pediatrics, Contractile Proteins, 0302 clinical medicine, Pregnancy, PMS2, Child, Agenesis of the corpus callosum, Genetics (clinical), Mismatch Repair Endonuclease PMS2, Adenosine Triphosphatases, 0303 health sciences, education.field_of_study, Microfilament Proteins, Nuclear Proteins, Syndrome, Parotid Neoplasms, 3. Good health, DNA-Binding Proteins, Heterotopia (medicine), Child, Preschool, 030220 oncology & carcinogenesis, Female, Microsatellite Instability, MutL Protein Homolog 1, medicine.medical_specialty, Filamins, Population, Biology, Article, 03 medical and health sciences, Internal medicine, Genetics, medicine, Humans, education, Adaptor Proteins, Signal Transducing, 030304 developmental biology, constitutional mismatch repair deficiency syndrome, agenesis of corpus callosum, gray matter heterotopia, biallelic germline mutation, childhood cancer, medicine.disease, DNA Repair-Deficiency Disorders, Pediatric cancer, MSH6, DNA Repair Enzymes, Endocrinology, MSH2, Mutation, Agenesis of Corpus Callosum, Glioblastoma, Malformations of Cortical Development, Group II

Abstract

Constitutional mismatch repair deficiency (CMMR-D) syndrome is a rare inherited childhood cancer predisposition caused by biallelic germline mutations in one of the four mismatch repair (MMR)-genes, MLH1, MSH2, MSH6 or PMS2. Owing to a wide tumor spectrum, the lack of specific clinical features and the overlap with other cancer predisposing syndromes, diagnosis of CMMR-D is often delayed in pediatric cancer patients. Here, we report of three new CMMR-D patients all of whom developed more than one malignancy. The common finding in these three patients is agenesis of the corpus callosum (ACC). Gray matter heterotopia is present in two patients. One of the 57 previously reported CMMR-D patients with brain tumors (therefore all likely had cerebral imaging) also had ACC. With the present report the prevalence of cerebral malformations is at least 4/60 (6.6%). This number is well above the population birth prevalence of 0.09-0.36 live births with these cerebral malformations, suggesting that ACC and heterotopia are features of CMMR-D. Therefore, the presence of cerebral malformations in pediatric cancer patients should alert to the possible diagnosis of CMMR-D. ACC and gray matter heterotopia are the first congenital malformations described to occur at higher frequency in CMMR-D patients than in the general population. Further systematic evaluations of CMMR-D patients are needed to identify possible other malformations associated with this syndrome. European Journal of Human Genetics (2013) 21, 55-61; doi: 10.1038/ejhg.2012.117; published online 13 June 2012

Published

2013

49. High prevalence of BRCA1 stop mutation c.4183C>T in the Tyrolean population

Author

Heidi Fiegl, Ingrid Weber, Laura Pölsler, Katharina Wimmer, Albert Amberger, Annekatrin Wernstedt, Raphael Johannes Morscher, Christian Marth, Johannes Zschocke, Anne Oberguggenberger, Willi Oberaigner, Christine Fauth, Pia Traunfellner, B Sperner-Unterweger, Michael Hubalek, Medical Genetics, University of Zurich, and Zschocke, Johannes

Subjects

0301 basic medicine, Oncology, endocrine system diseases, 0302 clinical medicine, skin and connective tissue diseases, Genetics (clinical), Ovarian Neoplasms, Genetics, education.field_of_study, medicine.diagnostic_test, BRCA1 Protein, Incidence (epidemiology), Middle Aged, BRCA2 Protein/genetics, Founder Effect, 030220 oncology & carcinogenesis, Codon, Terminator, Female, Adult, medicine.medical_specialty, 2716 Genetics (clinical), Population, Breast Neoplasms, 610 Medicine & health, Breast Neoplasms/genetics, Article, 03 medical and health sciences, Ovarian Neoplasms/genetics, Breast cancer, 1311 Genetics, Internal medicine, medicine, Humans, Genetic Testing, education, Genetic testing, Aged, BRCA2 Protein, business.industry, Cancer, Codon, Terminator/genetics, medicine.disease, Cancer registry, 030104 developmental biology, 10036 Medical Clinic, BRCA1 Protein/genetics, mutation, business, Ovarian cancer, aged, 80 and over, Founder effect

Abstract

Screening for founder mutations in BRCA1 and BRCA2 has been discussed as a cost-effective testing strategy in certain populations. In this study, comprehensive BRCA1 and BRCA2 testing was performed in a routine diagnostic setting. The prevalence of the BRCA1 stop mutation c.4183C>T, p.(Gln1395Ter), was determined in unselected breast and ovarian cancer patients from different regions in the Tyrol. Cancer registry data were used to evaluate the impact of this mutation on regional cancer incidence. The mutation c.4183C>T was detected in 30.4% of hereditary BRCA1-associated breast and ovarian cancer patients in our cohort. It was also identified in 4.1% of unselected (26% of unselected triple negative) Tyrolean breast cancer patients and 6.8% of unselected ovarian cancer patients from the Lower Inn Valley (LIV) region. Cancer incidences showed a region-specific increase in age-stratified breast and ovarian cancer risk with standardized incidence ratios of 1.23 and 2.13, respectively. We, thus, report a Tyrolean BRCA1 founder mutation that correlates to a local increase in the breast and ovarian cancer risks. On the basis of its high prevalence, we suggest that targeted genetic analysis should be offered to all women with breast or ovarian cancer and ancestry from the LIV region.

Published

2016

50. Improved multiplex ligation‐dependent probe amplification analysis identifies a deleterious PMS2 allele generated by recombination with crossover between PMS2 and PMS2CL

Author

Katharina Wimmer, Johannes Zschocke, Noemie Staehli, Salvatore Girlando, Ludwine Messiaen, Emanuele Valtorta, Franco Armelao, Giancarlo Marra, Annekatrin Wernstedt, Karl Heinimann, Roberto Togni, and Michael Baudis

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Pseudogene, Biology, Polymerase Chain Reaction, 03 medical and health sciences, Exon, 0302 clinical medicine, Germline mutation, Genetics, Humans, Multiplex, Multiplex ligation-dependent probe amplification, Allele, Alleles, Research Articles, Aged, Mismatch Repair Endonuclease PMS2, Neoplasm Staging, 030304 developmental biology, Adenosine Triphosphatases, Aged, 80 and over, Recombination, Genetic, 0303 health sciences, Breakpoint, Intron, DNA, Neoplasm, Middle Aged, digestive system diseases, DNA-Binding Proteins, DNA Repair Enzymes, 030220 oncology & carcinogenesis, Mutation, Female, Colorectal Neoplasms, Nucleic Acid Amplification Techniques, Gene Deletion, Pseudogenes

Abstract

Heterozygous PMS2 germline mutations are associated with Lynch syndrome. Up to one third of these mutations are genomic deletions. Their detection is complicated by a pseudogene (PMS2CL), which – owing to extensive interparalog sequence exchange – closely resembles PMS2 downstream of exon 12. A recently redesigned multiplex ligation-dependent probe amplification (MLPA) assay identifies PMS2 copy number alterations with improved reliability when used with reference DNAs containing equal numbers of PMS2- and PMS2CL-specific sequences. We selected eight such reference samples – all publicly available – and used them with this assay to study 13 patients with PMS2-defective colorectal tumors. Three presented deleterious alterations: an Alu-mediated exon deletion; a 125-kb deletion encompassing PMS2 and four additional genes (two with tumor-suppressing functions); and a novel deleterious hybrid PMS2 allele produced by recombination with crossover between PMS2 and PMS2CL, with the breakpoint in intron 10 (the most 5′ breakpoint of its kind reported thus far). We discuss mechanisms that might generate this allele in different chromosomal configurations (and their diagnostic implications) and describe an allele-specific PCR assay that facilitates its detection. Our data indicate that the redesigned PMS2 MLPA assay is a valid first-line option. In our series, it identified roughly a quarter of all PMS2 mutations. © 2012 Wiley Periodicals, Inc.

Published

2012