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2. Potent transmission-blocking monoclonal antibodies from naturally exposed individuals target a conserved epitope on Plasmodium falciparum Pfs230

Author

Danton Ivanochko, Amanda Fabra-García, Karina Teelen, Marga van de Vegte-Bolmer, Geert-Jan van Gemert, Jocelyn Newton, Anthony Semesi, Marloes de Bruijni, Judith Bolscher, Jordache Ramjith, Marta Szabat, Stefanie Vogt, Lucas Kraft, Sherie Duncan, Shwu-Maan Lee, Moses R. Kamya, Margaret E. Feeney, Prasanna Jagannathan, Bryan Greenhouse, Robert W. Sauerwein, C. Richter King, Randall S. MacGill, Teun Bousema, Matthijs M. Jore, and Jean-Philippe Julien

Subjects
All institutes and research themes of the Radboud University Medical Center, lnfectious Diseases and Global Health Radboud Institute for Health Sciences [Radboudumc 4], Infectious Diseases, Immunology, lnfectious Diseases and Global Health Radboud Institute for Molecular Life Sciences [Radboudumc 4], Immunology and Allergy, Women's cancers Radboud Institute for Health Sciences [Radboudumc 17]
Abstract

Contains fulltext : 291404.pdf (Publisher’s version ) (Open Access) Pfs230 is essential for Plasmodium falciparum transmission to mosquitoes and is the protein targeted by the most advanced malaria-transmission-blocking vaccine candidate. Prior understanding of functional epitopes on Pfs230 is based on two monoclonal antibodies (mAbs) with moderate transmission-reducing activity (TRA), elicited from subunit immunization. Here, we screened the B cell repertoire of two naturally exposed individuals possessing serum TRA and identified five potent mAbs from sixteen Pfs230 domain-1-specific mAbs. Structures of three potent and three low-activity antibodies bound to Pfs230 domain 1 revealed four distinct epitopes. Highly potent mAbs from natural infection recognized a common conformational epitope that is highly conserved across P. falciparum field isolates, while antibodies with negligible TRA derived from natural infection or immunization recognized three distinct sites. Our study provides molecular blueprints describing P. falciparum TRA, informed by contrasting potent and non-functional epitopes elicited by natural exposure and vaccination.

Published
2023
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3. Identification of Highly Potent Transmission-Blocking Human Monoclonal Antibodies to Plasmodium falciparum Pfs230 in Naturally Exposed Individuals

Author

Danton Ivanochko, Amanda Fabra-García, Karina Teelen, Marga van de Vegte-Bolmer, Geert-Jan van Gemert, Jocelyn Newton, Anthony Semesi, Marloes de Bruijni, Judith Bolscher, Jordache Ramjith, Marta Szabat, Stefanie Vogt, Lucas Kraft, Sherie Duncan, Shwu-Maan Lee, Moses Kamya, Margo Feeney, Prasanna Jagannathan, Bryan Greenhouse, Robert W. Sauerwein, C. Richter King, Randall MacGill, Teun Bousema, Matthijs M. Jore, and Jean-Philippe Julien

Subjects
History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering
Published
2022
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4. Highly Potent Naturally Acquired Human Monoclonal Antibodies Against Pfs48/45 Block Plasmodium falciparum Transmission to Mosquitoes

Author

Amanda Fabra-Garcia, Sophia Hailemariam, Roos de Jong, Kirsten Janssen, Karina Teelen, Marga van de Vegte-Bolmer, Geert-Jan van Gemert, Danton Ivanochko, Anthony Semesi, Brandon McLeod, Martijn Vos, Marloes de Bruijni, Judith Bolscher, Marta Szabat, Stefanie Vogt, Lucas Kraft, Sherie Duncan, Moses Kamya, Margo Feeney, Prasanna Jagannathan, Bryan Greenhouse, Koen Dechering, Robert W. Sauerwein, C. Richter King, Randall MacGill, Teun Bousema, Jean-Philippe Julien, and Matthijs M. Jore

Subjects
History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering
Published
2022
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5. Non-formale Bildung in nationalen Freiwilligendiensten – Zwischen beruflicher Orientierung und kritisch-emanzipatorischem Anspruch

Author

Stefan Schäfer, Stefanie Vogt, and Stefanie Bonus

Abstract

Dass Freiwilligendienste eine Vielfalt an Bildungsmöglichkeiten bieten, scheint unbestritten und stellt gleichzeitig keine Selbstverständlichkeit dar. Bildung in Freiwilligendiens ten bewegt sich in einem Spannungsfeld zwischen kritisch-emanzipatorischem Anspruch und einer Funktionalisierung von Bildung im Kontext ökonomischer und gesellschaftlicher Anforderungen der Arbeits- und Wissensgesellschaft. Der Beitrag stellt ausgewählte Ergebnisse eines Praxisentwicklungs- und Praxisforschungsprojekts vor, das in Kooperation zwischen Forschung und Praxis durchgeführt wurde. Non-formale Bildung wird hierbei im Sinne einer Eigenaktivität der Freiwilligen verstanden. Subjektorientierung und Partizipation werden als zentrale Arbeitsprinzipien ins Zentrum der Bildungsarbeit in den Freiwilligendiensten gerückt. Der Beitrag zeigt über die ideelle Idee einer kritisch-emanzipatorischen Bildung hinaus konzeptionelle Ansatzpunkte für die pädagogische Praxis auf.

Published
2019
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6. Wissenschaftliches Arbeiten in der Sozialen Arbeit

Author

Melanie Werner, Stefanie Vogt, Lydia Scheithauer, Melanie Werner, Stefanie Vogt, and Lydia Scheithauer

Subjects
Social service, Social work education
Abstract

Wie finde ich Fachliteratur? Wie schreibe ich eine Hausarbeit? Wie halte ich eine Präsentation? Dieses Buch begleitet Sie Schritt für Schritt beim Erstellen einer wissenschaftlichen Arbeit: Sie erfahren, wie Sie wissenschaftliche Quellen finden und mit diesen arbeiten. Sie lernen, wie Sie eine Leitfrage entwickeln, einen roten Faden herausarbeiten und wie Sie die Antworten auf Ihre Fragestellung in eine schriftliche Form bringen oder mündlich präsentieren. Mit vielen Beispielen und Tipps ist das Buch eine ausführliche Arbeitshilfe für Studienanfänger•innen und ein kompaktes Nachschlagewerk für alle Studierenden der Sozialen Arbeit. Zur Reihe Das gestufte Studienmodell der Bachelor- und Masterstudiengänge verlangt von Studierenden und Lehrenden ein präzises zeitliches und inhaltliches Studienmanagement. Im sozialen Beruf ist man immer wieder mit neuen Inhalten, Anforderungen und Bedingungen konfrontiert. Die kompakten Bände der Reihe führen in die Grundlagen eines Themenbereiches ein, stellen Zusammenhänge her, beschreiben Probleme und Herausforderungen.

Published
2017

20. Frequency and phenotypic spectrum of germline mutations inPOLEand seven other polymerase genes in 266 patients with colorectal adenomas and carcinomas

Author

Holger Thiele, Guido Plotz, Susanne Raeder, Isabel Spier, Verena Steinke, Richard P. Lifton, Sukanya Horpaopan, Monika Morak, Peter Nürnberg, Dietlinde Stienen, Stefanie Vogt, Elke Holinski-Feder, Janine Altmüller, Sophia Y. Chen, Stefan Aretz, Stefanie Holzapfel, Bixiao Zhao, Per Hoffmann, Katrin Kayser, and Ronja Adam

Subjects
Genetics, Cancer Research, Amsterdam criteria, POLD1, Colorectal cancer, Biology, medicine.disease, Lynch syndrome, Germline mutation, Oncology, MUTYH, medicine, Missense mutation, DNA mismatch repair
Abstract

In a number of families with colorectal adenomatous polyposis or suspected Lynch syndrome/HNPCC, no germline alteration in the APC, MUTYH, or mismatch repair (MMR) genes are found. Missense mutations in the polymerase genes POLE and POLD1 have recently been identified as rare cause of multiple colorectal adenomas and carcinomas, a condition termed polymerase proofreading-associated polyposis (PPAP). The aim of the present study was to evaluate the clinical relevance and phenotypic spectrum of polymerase germline mutations. Therefore, targeted sequencing of the polymerase genes POLD1, POLD2, POLD3, POLD4, POLE, POLE2, POLE3 and POLE4 was performed in 266 unrelated patients with polyposis or fulfilled Amsterdam criteria. The POLE mutation c.1270C>G;p.Leu424Val was detected in four unrelated patients. The mutation was present in 1.5% (4/266) of all patients, 4% (3/77) of all familial cases and 7% (2/30) of familial polyposis cases. The colorectal phenotype in 14 affected individuals ranged from typical adenomatous polyposis to a HNPCC phenotype, with high intrafamilial variability. Multiple colorectal carcinomas and duodenal adenomas were common, and one case of duodenal carcinoma was reported. Additionally, various extraintestinal lesions were evident. Nine further putative pathogenic variants were identified. The most promising was c.1306C>T;p.Pro436Ser in POLE. In conclusion, a PPAP was identified in a substantial number of polyposis and familial colorectal cancer patients. Screening for polymerase proofreading mutations should therefore be considered, particularly in unexplained familial cases. The present study broadens the phenotypic spectrum of PPAP to duodenal adenomas and carcinomas, and identified novel, potentially pathogenic variants in four polymerase genes.

Published
2015
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21. Genome-wide CNV analysis in 221 unrelated patients and targeted high-throughput sequencing reveal novel causative candidate genes for colorectal adenomatous polyposis

Author

Isabel Spier, Verena Steinke, Sandra M. Pasternack, Stefan Aretz, Elke Holinski-Feder, Per Hoffmann, Holger Fröhlich, Janine Altmüller, Stefan Herms, Stefanie Heilmann, Andrea Hofmann, Alberto Perez-Bouza, Stefanie Vogt, Markus M. Nöthen, Dietlinde Stienen, Hartmut Engels, Stefanie Holzapfel, Holger Thiele, Franziska Degenhardt, Andreas Laner, Kathleen Keppler, Sukanya Horpaopan, Ronja Adam, Susanne Moebus, Markus Draaken, Siegfried Uhlhaas, Katrin Kayser, and Alexander M. Zink

Subjects
Genetics, Cancer Research, education.field_of_study, Candidate gene, Population, Colorectal adenoma, Biology, medicine.disease, medicine.disease_cause, Genome, Oncology, MUTYH, medicine, Copy-number variation, education, Carcinogenesis, Gene
Abstract

To uncover novel causative genes in patients with unexplained adenomatous polyposis, a model disease for colorectal cancer, we performed a genome-wide analysis of germline copy number variants (CNV) in a large, well characterized APC and MUTYH mutation negative patient cohort followed by a targeted next generation sequencing (NGS) approach. Genomic DNA from 221 unrelated German patients was genotyped on high-resolution SNP arrays. Putative CNVs were filtered according to stringent criteria, compared with those of 531 population-based German controls, and validated by qPCR. Candidate genes were prioritized using in silico, expression, and segregation analyses, data mining and enrichment analyses of genes and pathways. In 27% of the 221 unrelated patients, a total of 77 protein coding genes displayed rare, nonrecurrent, germline CNVs. The set included 26 candidates with molecular and cellular functions related to tumorigenesis. Targeted high-throughput sequencing found truncating point mutations in 12% (10/77) of the prioritized genes. No clear evidence was found for autosomal recessive subtypes. Six patients had potentially causative mutations in more than one of the 26 genes. Combined with data from recent studies of early-onset colorectal and breast cancer, recurrent potential loss-of-function alterations were detected in CNTN6, FOCAD (KIAA1797), HSPH1, KIF26B, MCM3AP, YBEY and in three genes from the ARHGAP family. In the canonical Wnt pathway oncogene CTNNB1 (β-catenin), two potential gain-of-function mutations were found. In conclusion, the present study identified a group of rarely affected genes which are likely to predispose to colorectal adenoma formation and confirmed previously published candidates for tumor predisposition as etiologically relevant.

Published
2014
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22. Wissenschaftliches Arbeiten in der Sozialen Arbeit

Author

Melanie Werner, Stefanie Vogt, and Lydia Scheithauer

Abstract

Wie finde ich Fachliteratur? Wie schreibe ich eine Hausarbeit? Wie halte ich eine Präsentation? Dieses Buch begleitet Sie Schritt für Schritt beim Erstellen einer wissenschaftlichen Arbeit: Sie erfahren, wie Sie wissenschaftliche Quellen finden und mit diesen arbeiten. Sie lernen, wie Sie eine Leitfrage entwickeln, einen roten Faden herausarbeiten und wie Sie die Antworten auf Ihre Fragestellung in eine schriftliche Form bringen oder mündlich präsentieren. Mit vielen Beispielen und Tipps ist das Buch eine ausführliche Arbeitshilfe für Studienanfänger*innen und ein kompaktes Nachschlagewerk für alle Studierenden der Sozialen Arbeit. Zur Reihe Das gestufte Studienmodell der Bachelor- und Masterstudiengänge verlangt von Studierenden und Lehrenden ein präzises zeitliches und inhaltliches Studienmanagement. Im sozialen Beruf ist man immer wieder mit neuen Inhalten, Anforderungen und Bedingungen konfrontiert. Die kompakten Bände der Reihe führen in die Grundlagen eines Themenbereiches ein, stellen Zusammenhänge her, beschreiben Probleme und Herausforderungen.

Published
2016
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23. Mutations in Subunits of the Activating Signal Cointegrator 1 Complex Are Associated with Prenatal Spinal Muscular Atrophy and Congenital Bone Fractures

Author

Susanne Morales-Gonzalez, Janbernd Kirschner, Klaus Zerres, Mickael Orgeur, Gudrun Schottmann, Esther Gill, Werner Stenzel, Ellen Knierim, Nicole I. Wolf, Hiromi Hirata, Angelika Zwirner, Yu Tanaka, Anne van Riesen, Stefanie Vogt, Markus Schuelke, Franziska Seifert, David Meierhofer, Sigmar Stricker, Sabine Rudnik-Schöneborn, Christoph Hübner, Hans H. Goebel, Pediatric surgery, and Amsterdam Neuroscience - Cellular & Molecular Mechanisms

Subjects
0301 basic medicine, Activating signal cointegrator 1 complex, Fractures, Bone, Mice, 0302 clinical medicine, arthrogryposis multiplex congenita, Genetics(clinical), Zebrafish, Genetics (clinical), ASCC1, Cells, Cultured, spinal muscular atrophy, Genetics, Arthrogryposis, Gene knockdown, biology, Homozygote, bone fractures, Gene Expression Regulation, Developmental, Nuclear Proteins, LIM Domain Proteins, Cell biology, Pedigree, Phenotype, Molecular Sequence Data, Article, Frameshift mutation, Muscular Atrophy, Spinal, 03 medical and health sciences, respiratory distress, medicine, Animals, Humans, Amino Acid Sequence, Transcription factor, Spinal Cord Regeneration, Gene Expression Profiling, neuromuscular unit, SEMA3A, Spinal muscular atrophy, Fibroblasts, Zebrafish Proteins, medicine.disease, biology.organism_classification, 030104 developmental biology, TRIP4, Mutation, Carrier Proteins, exome sequencing, 030217 neurology & neurosurgery, zebrafish model, Transcription Factors
Abstract

Transcriptional signal cointegrators associate with transcription factors or nuclear receptors and coregulate tissue-specific gene transcription. We report on recessive loss-of-function mutations in two genes ( TRIP4 and ASCC1 ) that encode subunits of the nuclear activating signal cointegrator 1 (ASC-1) complex. We used autozygosity mapping and whole-exome sequencing to search for pathogenic mutations in four families. Affected individuals presented with prenatal-onset spinal muscular atrophy (SMA), multiple congenital contractures (arthrogryposis multiplex congenita), respiratory distress, and congenital bone fractures. We identified homozygous and compound-heterozygous nonsense and frameshift TRIP4 and ASCC1 mutations that led to a truncation or the entire absence of the respective proteins and cosegregated with the disease phenotype. Trip4 and Ascc1 have identical expression patterns in 17.5-day-old mouse embryos with high expression levels in the spinal cord, brain, paraspinal ganglia, thyroid, and submandibular glands. Antisense morpholino-mediated knockdown of either trip4 or ascc1 in zebrafish disrupted the highly patterned and coordinated process of α-motoneuron outgrowth and formation of myotomes and neuromuscular junctions and led to a swimming defect in the larvae. Immunoprecipitation of the ASC-1 complex consistently copurified cysteine and glycine rich protein 1 (CSRP1), a transcriptional cofactor, which is known to be involved in spinal cord regeneration upon injury in adult zebrafish. ASCC1 mutant fibroblasts downregulated genes associated with neurogenesis, neuronal migration, and pathfinding ( SERPINF1, DAB1, SEMA3D, SEMA3A ), as well as with bone development ( TNFRSF11B, RASSF2, STC1 ). Our findings indicate that the dysfunction of a transcriptional coactivator complex can result in a clinical syndrome affecting the neuromuscular system.

Published
2016
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24. Analysis of Rare APC Variants at the mRNA Level

Author

Dietlinde Stienen, Stefanie Vogt, Stefan Aretz, Horst Hameister, Peter Propping, Elisabeth Mangold, Ingo Kurth, Judith Kötting, Elke Kaminsky, Astrid Kaufmann, Waltraut Friedl, and Siegfried Uhlhaas

Subjects
Genetics, biology, Adenomatous polyposis coli, Intron, RNA, medicine.disease, Molecular biology, Pathology and Forensic Medicine, Familial adenomatous polyposis, Exon, Gene duplication, DNA Mutational Analysis, medicine, biology.protein, Molecular Medicine, Gene
Abstract

In monogenic disorders, the functional evaluation of rare, unclassified variants helps to assess their pathogenic relevance and can improve differential diagnosis and predictive testing. We characterized six rare APC variants in patients with familial adenomatous polyposis at the mRNA level. APC variants c.531 + 5G>C and c.532-8G>A in intron 4, c.1409-2_1409delAGG in intron 10, c.1548G>A in exon 11, and a large duplication of exons 10 and 11 result in a premature stop codon attributable to aberrant transcripts whereas the variant c.1742A>G leads to the in-frame deletion of exon 13 and results in the removal of a functional motif. Mutation c.1548G>A was detected in the index patient but not in his affected father, suggesting mutational mosaicism. A literature review shows that most of the rare APC variants detected by routine diagnostics and further analyzed at the transcript level were evaluated as pathogenic. The majority of rare APC variants, particularly those located close to exon-intron boundaries, could be classified as pathogenic because of aberrant splicing. Our study shows that the characterization of rare variants at the mRNA level is crucial for the evaluation of pathogenicity and underlying mutational mechanisms, and could lead to better treatment modalities.

Published
2009
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25. 'Ich hätte gedacht, dass mehr Praxisnähe da ist'

Author

Stefanie Vogt and Melanie Werner

Abstract

Studierende aus nicht-akademischem Elternhaus studieren seltener an einer Hochschule und sehen sich aufgrund sozialer Ungleichheit auch im Studium in vielfaltigen Formen mit Benachteiligungen, Beeintrachtigungen und Hemmnissen konfrontiert. Der Beitrag beleuchtet anhand von Ergebnissen aus einem Lehrforschungsprojekt im Studiengang Soziale Arbeit an der Fachhochschule Koln insbesondere die erste Phase des Studiums und fragt danach, wie Studierende aus nicht-akademischem Elternhaus ihr Studium erleben.

Published
2016
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26. Germline hypermethylation of the APC promoter is not a frequent cause of familial adenomatous polyposis in APC/MUTYH mutation negative families

Author

Sara González, Jordi Romero-Gimenez, Ignacio Blanco, Stefan Aretz, Higinio Dopeso, Diego Arango, Angel Guerra-Moreno, Gabriel Capellá, Stefanie Vogt, and Simó Schwartz

Subjects
Genetics, congenital, hereditary, and neonatal diseases and abnormalities, Cancer Research, Mutation, Tumor suppressor gene, biology, Adenomatous polyposis coli, medicine.disease, medicine.disease_cause, Germline, Familial adenomatous polyposis, Germline mutation, Oncology, MUTYH, DNA methylation, biology.protein, medicine
Abstract

Familial adenomatous polyposis (FAP) is an autosomal dominant syndrome predisposing to colorectal cancer and affects 1 in 5-10,000 births. Inheritance of a mutant allele of the adenomatous polyposis coli (APC) gene is the cause of approximately 80% of FAP and 20-30% of an attenuated form of FAP (AFAP), whereas mutations in MUTYH account for a small proportion of the remaining cases. However, the genetic cause of FAP/AFAP in a significant number of families is not known, and cancer risk for individual members of these families cannot be assessed. There is, therefore, an acute need to identify the underlying genetic cause responsible for FAP/AFAP in APC/MUTYH mutation negative families. Hypermethylation of CpG islands in the promoter of tumor suppressor genes can result in gene silencing, has been shown to be functionally equivalent to genetic mutations and can be inherited. Moreover, APC promoter hypermethylation is observed in approximately 20% of sporadic colorectal tumors and correlates with the loss of gene expression. In our study, we used bisulfite treatment and direct sequencing of 2 regulatory regions of APC containing a total of 25 CpG dinucleotides, to investigate the possible role of germline hypermethylation of the APC promoter in FAP and AFAP families that were negative for APC and MUTYH mutations. Analysis of 21 FAP and 39 AFAP families did not identify signs of abnormal promoter methylation, indicating that this form of epigenetic silencing is not a common cause of FAP/AFAP. These results substantially contribute to clarify the potential role of germline epimutations as a cause of inherited predisposition to cancer.

Published
2007
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27. Genome-wide CNV analysis in 221 unrelated patients and targeted high-throughput sequencing reveal novel causative candidate genes for colorectal adenomatous polyposis

Author

Sukanya, Horpaopan, Isabel, Spier, Alexander M, Zink, Janine, Altmüller, Stefanie, Holzapfel, Andreas, Laner, Stefanie, Vogt, Siegfried, Uhlhaas, Stefanie, Heilmann, Dietlinde, Stienen, Sandra M, Pasternack, Kathleen, Keppler, Ronja, Adam, Katrin, Kayser, Susanne, Moebus, Markus, Draaken, Franziska, Degenhardt, Hartmut, Engels, Andrea, Hofmann, Markus M, Nöthen, Verena, Steinke, Alberto, Perez-Bouza, Stefan, Herms, Elke, Holinski-Feder, Holger, Fröhlich, Holger, Thiele, Per, Hoffmann, and Stefan, Aretz

Subjects
Adult, Adolescent, DNA Copy Number Variations, Intracellular Signaling Peptides and Proteins, Medizin, High-Throughput Nucleotide Sequencing, Kinesins, Middle Aged, Protein Serine-Threonine Kinases, DNA Glycosylases, Adenomatous Polyposis Coli, Humans, HSP110 Heat-Shock Proteins, Child, beta Catenin, Aged, Genome-Wide Association Study
Abstract

To uncover novel causative genes in patients with unexplained adenomatous polyposis, a model disease for colorectal cancer, we performed a genome-wide analysis of germline copy number variants (CNV) in a large, well characterized APC and MUTYH mutation negative patient cohort followed by a targeted next generation sequencing (NGS) approach. Genomic DNA from 221 unrelated German patients was genotyped on high-resolution SNP arrays. Putative CNVs were filtered according to stringent criteria, compared with those of 531 population-based German controls, and validated by qPCR. Candidate genes were prioritized using in silico, expression, and segregation analyses, data mining and enrichment analyses of genes and pathways. In 27% of the 221 unrelated patients, a total of 77 protein coding genes displayed rare, nonrecurrent, germline CNVs. The set included 26 candidates with molecular and cellular functions related to tumorigenesis. Targeted high-throughput sequencing found truncating point mutations in 12% (10/77) of the prioritized genes. No clear evidence was found for autosomal recessive subtypes. Six patients had potentially causative mutations in more than one of the 26 genes. Combined with data from recent studies of early-onset colorectal and breast cancer, recurrent potential loss-of-function alterations were detected in CNTN6, FOCAD (KIAA1797), HSPH1, KIF26B, MCM3AP, YBEY and in three genes from the ARHGAP family. In the canonical Wnt pathway oncogene CTNNB1 (β-catenin), two potential gain-of-function mutations were found. In conclusion, the present study identified a group of rarely affected genes which are likely to predispose to colorectal adenoma formation and confirmed previously published candidates for tumor predisposition as etiologically relevant.

Published
2015

28. Frequency and phenotypic spectrum of germline mutations in POLE and seven other polymerase genes in 266 patients with colorectal adenomas and carcinomas

Author

Isabel, Spier, Stefanie, Holzapfel, Janine, Altmüller, Bixiao, Zhao, Sukanya, Horpaopan, Stefanie, Vogt, Sophia, Chen, Monika, Morak, Susanne, Raeder, Katrin, Kayser, Dietlinde, Stienen, Ronja, Adam, Peter, Nürnberg, Guido, Plotz, Elke, Holinski-Feder, Richard P, Lifton, Holger, Thiele, Per, Hoffmann, Verena, Steinke, and Stefan, Aretz

Subjects
Adenoma, Adult, Male, Adolescent, Mutation, Missense, DNA-Directed DNA Polymerase, Polymorphism, Single Nucleotide, Young Adult, Gene Frequency, Phospholipase D, Humans, Genetic Predisposition to Disease, Child, Poly-ADP-Ribose Binding Proteins, Germ-Line Mutation, Aged, Aged, 80 and over, Family Health, DNA Polymerase II, Sequence Analysis, DNA, Middle Aged, Pedigree, Isoenzymes, Phenotype, Female, Colorectal Neoplasms
Abstract

In a number of families with colorectal adenomatous polyposis or suspected Lynch syndrome/HNPCC, no germline alteration in the APC, MUTYH, or mismatch repair (MMR) genes are found. Missense mutations in the polymerase genes POLE and POLD1 have recently been identified as rare cause of multiple colorectal adenomas and carcinomas, a condition termed polymerase proofreading-associated polyposis (PPAP). The aim of the present study was to evaluate the clinical relevance and phenotypic spectrum of polymerase germline mutations. Therefore, targeted sequencing of the polymerase genes POLD1, POLD2, POLD3, POLD4, POLE, POLE2, POLE3 and POLE4 was performed in 266 unrelated patients with polyposis or fulfilled Amsterdam criteria. The POLE mutation c.1270CG;p.Leu424Val was detected in four unrelated patients. The mutation was present in 1.5% (4/266) of all patients, 4% (3/77) of all familial cases and 7% (2/30) of familial polyposis cases. The colorectal phenotype in 14 affected individuals ranged from typical adenomatous polyposis to a HNPCC phenotype, with high intrafamilial variability. Multiple colorectal carcinomas and duodenal adenomas were common, and one case of duodenal carcinoma was reported. Additionally, various extraintestinal lesions were evident. Nine further putative pathogenic variants were identified. The most promising was c.1306CT;p.Pro436Ser in POLE. In conclusion, a PPAP was identified in a substantial number of polyposis and familial colorectal cancer patients. Screening for polymerase proofreading mutations should therefore be considered, particularly in unexplained familial cases. The present study broadens the phenotypic spectrum of PPAP to duodenal adenomas and carcinomas, and identified novel, potentially pathogenic variants in four polymerase genes.

Published
2014

29. Spectrum of novel mutations found in Waardenburg syndrome types 1 and 2: implications for molecular genetic diagnostics

Author

Gabriele Wildhardt, Oliver Bartsch, Axel Bohring, Gertrud Strobl-Wildemann, Markus Suckfüll, Juliane Wechtenbruch, Annegret Buske, Marie T. Greally, Christian Kubisch, Stefanie Vogt, Birgit Zirn, Daniela Steinberger, and Luitgard Graul-Neumann

Subjects
business.industry, Waardenburg syndrome, Point mutation, Research, Copy number analysis, Tietz syndrome, Genetics and Genomics, General Medicine, Gene mutation, Microphthalmia-associated transcription factor, Bioinformatics, medicine.disease, Congenital hearing loss, Medicine, Missense mutation, business
Abstract

Objectives Till date, mutations in the genes PAX3 and MITF have been described in Waardenburg syndrome (WS), which is clinically characterised by congenital hearing loss and pigmentation anomalies. Our study intended to determine the frequency of mutations and deletions in these genes, to assess the clinical phenotype in detail and to identify rational priorities for molecular genetic diagnostics procedures. Design Prospective analysis. Patients 19 Caucasian patients with typical features of WS underwent stepwise investigation of PAX3 and MITF . When point mutations and small insertions/deletions were excluded by direct sequencing, copy number analysis by multiplex ligation-dependent probe amplification was performed to detect larger deletions and duplications. Clinical data and photographs were collected to facilitate genotype–phenotype analyses. Setting All analyses were performed in a large German laboratory specialised in genetic diagnostics. Results 15 novel and 4 previously published heterozygous mutations in PAX3 and MITF were identified. Of these, six were large deletions or duplications that were only detectable by copy number analysis. All patients with PAX3 mutations had typical phenotype of WS with dystopia canthorum (WS1), whereas patients with MITF gene mutations presented without dystopia canthorum (WS2). In addition, one patient with bilateral hearing loss and blue eyes with iris stroma dysplasia had a de novo missense mutation (p.Arg217Ile) in MITF . MITF 3-bp deletions at amino acid position 217 have previously been described in patients with Tietz syndrome (TS), a clinical entity with hearing loss and generalised hypopigmentation. Conclusions On the basis of these findings, we conclude that sequencing and copy number analysis of both PAX3 and MITF have to be recommended in the routine molecular diagnostic setting for patients, WS1 and WS2. Furthermore, our genotype–phenotype analyses indicate that WS2 and TS correspond to a clinical spectrum that is influenced by MITF mutation type and position.

Published
2013

30. Deep intronic APC mutations explain a substantial proportion of patients with familial or early-onset adenomatous polyposis

Author

Markus Draaken, Markus M. Nöthen, Sukanya Horpaopan, Dietlinde Stienen, Elke Holinski-Feder, Stefan Aretz, Stefanie Vogt, Isabel Spier, Siegfried Uhlhaas, Michael Ludwig, Per Hoffmann, and Monika Morak

Subjects
Genetics, Mutation, biology, Adenomatous polyposis coli, Haplotype, Adenomatous Polyposis Coli Protein, Intron, medicine.disease_cause, medicine.disease, Exon skipping, Introns, Familial adenomatous polyposis, Germline mutation, Adenomatous Polyposis Coli, MUTYH, medicine, biology.protein, Humans, Genetic Predisposition to Disease, Genetics (clinical)
Abstract

To uncover pathogenic deep intronic variants in patients with colorectal adenomatous polyposis, in whom no germline mutation in the APC or MUTYH genes can be identified by routine diagnostics, we performed a systematic APC messenger RNA analysis in 125 unrelated mutation-negative cases. Overall, we identified aberrant transcripts in 8% of the patients (familial cases 30%; early-onset manifestation 21%). In eight of them, two different out-of-frame pseudoexons were found consisting of a 167-bp insertion from intron 4 in five families with a shared founder haplotype and a 83-bp insertion from intron 10 in three patients. The pseudoexon formation was caused by three different heterozygous germline mutations, which are supposed to activate cryptic splice sites. In conclusion, a few deep intronic mutations contribute substantially to the APC mutation spectrum. Complementary DNA analysis and/or target sequencing of intronic regions should be considered as an additional mutation discovery approach in polyposis patients.

Published
2011

31. Survival of MUTYH-Associated Polyposis Patients With Colorectal Cancer and Matched Control Colorectal Cancer Patients

Author

Liza N. van Steenbergen, Hans F. A. Vasen, Julian R. Sampson, Maartje Nielsen, Natalie Jones, Olaf M. Dekkers, Frederik J. Hes, Stefan Aretz, Maryska L.G. Janssen-Heijnen, Stefanie Vogt, Hans Morreau, Public Health, Clinical sciences, and Medical Genetics

Subjects
Adult, Male, Cancer Research, medicine.medical_specialty, Colorectal cancer, Population, Colonic Polyps, Kaplan-Meier Estimate, Gastroenterology, DNA Glycosylases, Bias, SDG 3 - Good Health and Well-being, MUTYH, Internal medicine, medicine, Humans, education, Selection Bias, Aged, Proportional Hazards Models, Retrospective Studies, Cancer staging, education.field_of_study, business.industry, MUTYH-Associated Polyposis, Cancer, Retrospective cohort study, Articles, Middle Aged, medicine.disease, Europe, Oncology, Case-Control Studies, tumor-infiltrating lymphocytes microsatellite instability prolonged survival prognostic-factor colon-cancer mutations carcinoma risk myh identification, Female, Colorectal Neoplasms, business, Cohort study
Abstract

Background MUTYH-associated polyposis is a recessively inherited disorder characterized by a lifetime risk of colorectal cancer that is up to 100%. Because specific histological and molecular genetic features of MUTYH-associated polyposis colorectal cancers might influence tumor behavior and patient survival, we compared survival between patients with MUTYH-associated polyposis colorectal cancer and matched control patients with colorectal cancer from the general population. Methods In this retrospective multicenter cohort study from Europe, 147 patients with MUTYH-associated polyposis colorectal cancer were compared with 272 population-based control patients with colorectal cancer who were matched for country, age at diagnosis, year of diagnosis, stage, and subsite of colorectal cancer. Kaplan-Meier survival and Cox regression analyses were used to compare survival between patients with MUTYH-associated polyposis colorectal cancer and control patients with colorectal cancer. All statistical tests were two-sided. Results Five-year survival for patients with MUTYH-associated polyposis colorectal cancer was 78% (95% confidence interval [CI] = 70% to 84%) and for control patients was 63% (95% CI = 56% to 69%) (log-rank test, P = .002). After adjustment for differences in age, stage, sex, subsite, country, and year of diagnosis, survival remained better for MUTYH-associated polyposis colorectal cancer patients than for control patients (hazard ratio of death = 0.48, 95% CI = 0.32 to 0.72). Conclusions In a European study cohort, we found statistically significantly better survival for patients with MUTYH-associated polyposis colorectal cancer than for matched control patients with colorectal cancer.

Published
2010

32. Gastrointestinal Polyposis Syndromes

Author

Waltraut Friedl and Stefanie Vogt

Subjects
medicine.medical_specialty, business.industry, Colorectal cancer, MUTYH-Associated Polyposis, Internal medicine, medicine, Peutz–Jeghers syndrome, medicine.disease, business, Gastroenterology, Familial adenomatous polyposis
Published
2009
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33. Expanded extracolonic tumor spectrum in MUTYH-associated polyposis

Author

Frederik J. Hes, Astrid Kaufmann, Christoph Engel, Stefanie Vogt, Stefan Aretz, Hans F. A. Vasen, Peter Propping, Natalie Jones, Daria Christian, Maartje Nielsen, Verena Steinke, Julian R. Sampson, Clinical sciences, and Medical Genetics

Subjects
Adult, Male, medicine.medical_specialty, Skin Neoplasms, Adolescent, Population, Breast Neoplasms, Kaplan-Meier Estimate, Gastroenterology, Risk Assessment, Familial adenomatous polyposis, DNA Glycosylases, Young Adult, Breast cancer, Risk Factors, Internal medicine, Medicine, Humans, Genetic Predisposition to Disease, Sebaceous Gland Neoplasms, Age of Onset, education, Child, Aged, Gastrointestinal Neoplasms, Retrospective Studies, Ovarian Neoplasms, education.field_of_study, Hepatology, business.industry, Incidence (epidemiology), MUTYH-Associated Polyposis, Incidence, Endoscopy, Middle Aged, medicine.disease, Lynch syndrome, Surgery, Europe, Phenotype, Adenomatous Polyposis Coli, Urinary Bladder Neoplasms, Relative risk, Female, Duodenal cancer, business
Abstract

Background & Aims MUTYH-associated polyposis (MAP) is characterized by a lifetime risk of colorectal cancer of up to 100%. However, no systematic evaluation of extracolonic manifestations has been reported. Methods A large cohort of MAP patients was recruited from a European multicenter study. Data were collected on 276 cases from 181 unrelated families. Information on extracolonic tumor spectrum and incidence were evaluated to determine cumulative lifetime risk, which was compared with that of the general population to obtain standardized incidence ratios (SIRs). Results Duodenal polyposis occurred in 17% of cases; the relative risk (SIR) of duodenal cancer was 129 (95% confidence interval [CI]: 16–466), whereas the lifetime risk was 4%. The incidence of extraintestinal malignancies among cases was almost twice that of the general population (SIR: 1.9; 95% CI: 1.4–2.5), with a lifetime risk of 38%. We observed a significant increase in the incidence of ovarian, bladder, and skin cancers (SIR: 5.7, 7.2, and 2.8, respectively) and a trend of increased risk of breast cancer among cases. The median ages of onset of these 4 malignancies ranged from 51 to 61 years. In contrast to familial adenomatous polyposis, no desmoid tumors were observed, but sebaceous gland tumors, characteristic of the Muir-Torre variant of Lynch syndrome, occurred in 5 patients. Conclusions The relative risks for several extraintestinal malignancies increased in patients with MAP, but based on the spectrum of cancers (which overlaps with that of Lynch syndrome) and the relatively advanced age at onset, intensive surveillance measures other than frequent endoscopy are unlikely to be helpful to patients with MAP.

Published
2009

34. Analysis of rare APC variants at the mRNA level: six pathogenic mutations and literature review

Author

Astrid, Kaufmann, Stefanie, Vogt, Siegfried, Uhlhaas, Dietlinde, Stienen, Ingo, Kurth, Horst, Hameister, Elisabeth, Mangold, Judith, Kötting, Elke, Kaminsky, Peter, Propping, Waltraut, Friedl, and Stefan, Aretz

Subjects
Genes, APC, Adenomatous Polyposis Coli, DNA Mutational Analysis, Mutation, Humans, RNA, Messenger, Regular Articles
Abstract

In monogenic disorders, the functional evaluation of rare, unclassified variants helps to assess their pathogenic relevance and can improve differential diagnosis and predictive testing. We characterized six rare APC variants in patients with familial adenomatous polyposis at the mRNA level. APC variants c.531 + 5G>C and c.532-8G>A in intron 4, c.1409-2_1409delAGG in intron 10, c.1548G>A in exon 11, and a large duplication of exons 10 and 11 result in a premature stop codon attributable to aberrant transcripts whereas the variant c.1742A>G leads to the in-frame deletion of exon 13 and results in the removal of a functional motif. Mutation c.1548G>A was detected in the index patient but not in his affected father, suggesting mutational mosaicism. A literature review shows that most of the rare APC variants detected by routine diagnostics and further analyzed at the transcript level were evaluated as pathogenic. The majority of rare APC variants, particularly those located close to exon-intron boundaries, could be classified as pathogenic because of aberrant splicing. Our study shows that the characterization of rare variants at the mRNA level is crucial for the evaluation of pathogenicity and underlying mutational mechanisms, and could lead to better treatment modalities.

Published
2009

35. Germline hypermethylation of the APC promoter is not a frequent cause of familial adenomatous polyposis in APC/MUTYH mutation negative families

Author

Jordi, Romero-Giménez, Higinio, Dopeso, Ignacio, Blanco, Angel, Guerra-Moreno, Sara, Gonzalez, Stefanie, Vogt, Stefan, Aretz, Simo, Schwartz, Gabriel, Capella, and Diego, Arango

Subjects
Genes, APC, Adenomatous Polyposis Coli, Base Sequence, Humans, CpG Islands, DNA Methylation, Promoter Regions, Genetic, Germ-Line Mutation, DNA Glycosylases, DNA Primers
Abstract

Familial adenomatous polyposis (FAP) is an autosomal dominant syndrome predisposing to colorectal cancer and affects 1 in 5-10,000 births. Inheritance of a mutant allele of the adenomatous polyposis coli (APC) gene is the cause of approximately 80% of FAP and 20-30% of an attenuated form of FAP (AFAP), whereas mutations in MUTYH account for a small proportion of the remaining cases. However, the genetic cause of FAP/AFAP in a significant number of families is not known, and cancer risk for individual members of these families cannot be assessed. There is, therefore, an acute need to identify the underlying genetic cause responsible for FAP/AFAP in APC/MUTYH mutation negative families. Hypermethylation of CpG islands in the promoter of tumor suppressor genes can result in gene silencing, has been shown to be functionally equivalent to genetic mutations and can be inherited. Moreover, APC promoter hypermethylation is observed in approximately 20% of sporadic colorectal tumors and correlates with the loss of gene expression. In our study, we used bisulfite treatment and direct sequencing of 2 regulatory regions of APC containing a total of 25 CpG dinucleotides, to investigate the possible role of germline hypermethylation of the APC promoter in FAP and AFAP families that were negative for APC and MUTYH mutations. Analysis of 21 FAP and 39 AFAP families did not identify signs of abnormal promoter methylation, indicating that this form of epigenetic silencing is not a common cause of FAP/AFAP. These results substantially contribute to clarify the potential role of germline epimutations as a cause of inherited predisposition to cancer.

Published
2007

36. High proportion of large genomic deletions and a genotype phenotype update in 80 unrelated families with juvenile polyposis syndrome

Author

Klaus-Michael Keller, Siegfreid Uhlhaas, Waltraut Friedl, Manfred Stolte, Lone Sunde, Astrid Kaufmann, Elke Holinski-Feder, Stefan Aretz, Reiner Siebert, Stefanie Vogt, Stefan H Blaas, Dietlinde Stienen, Steffan Loff, Peter Propping, Mark M Entius, Stefanie Spranger, and Walter Back

Subjects
Adult, Male, medicine.medical_specialty, Adolescent, Genotype, DNA Mutational Analysis, Biology, Gastroenterology, Genetic Heterogeneity, Germline mutation, Antigens, CD, Neoplastic Syndromes, Hereditary, Internal medicine, Germany, Genetics, medicine, Humans, Point Mutation, Juvenile polyposis syndrome, Age of Onset, Child, Genetics (clinical), Bone Morphogenetic Protein Receptors, Type I, Gastrointestinal Neoplasms, Smad4 Protein, Genetic heterogeneity, Intestinal Polyposis, Point mutation, PTEN Phosphohydrolase, Infant, Nucleic acid amplification technique, medicine.disease, Cadherins, digestive system diseases, Phenotype, Gastric Polyp, Child, Preschool, Mutation (genetic algorithm), Immunology, Female, Telangiectasia, Hereditary Hemorrhagic, Original Article, Chromosome Deletion, Nucleic Acid Amplification Techniques
Abstract

BACKGROUND: In patients with juvenile polyposis syndrome (JPS) the frequency of large genomic deletions in the SMAD4 and BMPR1A genes was unknown. METHODS: Mutation and phenotype analysis was used in 80 unrelated patients of whom 65 met the clinical criteria for JPS (typical JPS) and 15 were suspected to have JPS. RESULTS: By direct sequencing of the two genes, point mutations were identified in 30 patients (46% of typical JPS). Using MLPA, large genomic deletions were found in 14% of all patients with typical JPS (six deletions in SMAD4 and three deletions in BMPR1A). Mutation analysis of the PTEN gene in the remaining 41 mutation negative cases uncovered a point mutation in two patients (5%). SMAD4 mutation carriers had a significantly higher frequency of gastric polyposis (73%) than did patients with BMPR1A mutations (8%) (p Udgivelsesdato: 2007-Nov

Published
2007
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37. Detection of hepatitis C virus RNA in formalin-fixed, paraffin-embedded thin-needle liver biopsy specimens

Author

Sabine Klauck, Stefanie Vogt, Albert Roessner, Regine Schneider-Stock, and Christoph Röcken

Subjects
Adult, Male, medicine.medical_specialty, Pathology, Cirrhosis, Tissue Fixation, Hepatitis C virus, Hepacivirus, medicine.disease_cause, Formaldehyde, Biopsy, Medicine, Humans, Aged, DNA Primers, Histocytological Preparation Techniques, Paraffin Embedding, medicine.diagnostic_test, business.industry, Reverse Transcriptase Polymerase Chain Reaction, Biopsy, Needle, RNA, General Medicine, Hepatitis C, Chronic, Middle Aged, medicine.disease, Reverse transcription polymerase chain reaction, Real-time polymerase chain reaction, Liver biopsy, Feasibility Studies, RNA, Viral, Histopathology, Female, business
Abstract

We examined the feasibility of detecting hepatitis C virus (HCV) RNA in formalin-fixed, paraffin-embedded (FFPE) specimens obtained by thin-needle biopsy (TNB). Specimens obtained by large-needle biopsy (LNB) and unfixed frozen tissue served as controls. A total of 23 biopsy specimens, 13 obtained by TNB and 10 by LNB, from 20 patients with chronic hepatitis C were included in the study. HCV RNA was detected by nested reverse transcription-polymerase chain reaction (RT-PCR). HCV RNA was found in FFPE archival specimens obtained by TNB (11 [85%]) or LNB (7 [70%]). The sensitivity was similar in unfixed tissue in which HCV RNA was found in 7 (88%) of 8 TNB specimens and 6 (86%) of 7 LNB specimens. The detection of HCV RNA did not seem to be affected by storage of the paraffin blocks, the presence of advanced fibrosis and cirrhosis, or fragmentation of the core cylinder. TNB yields enough qualitative suitable material to detect HCV RNA by RT-PCR.

Published
2003

38. Increased Colorectal Cancer Incidence in Obligate Carriers of Heterozygous Mutations in MUTYH

Author

Frederik J. Hes, Stefan Aretz, Stefanie Vogt, Diana Eccles, Petra A. Wark, Daria Christian, Emma Edwards, Natalie Jones, D. Gareth Evans, Julian R. Sampson, Maartje Nielsen, Eamonn R. Maher, Hans F. A. Vasen, Clinical sciences, and Medical Genetics

Subjects
Male, Oncology, Heterozygote, medicine.medical_specialty, Colorectal cancer, DNA Mutational Analysis, Population, Risk Assessment, DNA Glycosylases, Age Distribution, MUTYH, Internal medicine, Confidence Intervals, Odds Ratio, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Registries, Sex Distribution, education, Survival rate, Aged, Probability, Aged, 80 and over, education.field_of_study, Hepatology, business.industry, Incidence, Incidence (epidemiology), MUTYH-Associated Polyposis, Gastroenterology, Colonoscopy, Odds ratio, Middle Aged, Prognosis, medicine.disease, Pedigree, Surgery, Survival Rate, Standardized mortality ratio, Mutation, Education, Medical, Continuing, Female, Colorectal Neoplasms, business
Abstract

Background & Aims MUTYH-associated polyposis (MAP) is an autosomal recessive disorder caused by mutations in the MUTYH gene. Patients with MAP are at extremely high risk of colorectal cancer, but the risks of colorectal and other cancers in heterozygous carriers of a single MUTYH mutation are uncertain. We performed a retrospective study of cancer incidence and causes of death among obligate MUTYH heterozygote individuals. Methods MAP index cases were identified from polyposis registers in Germany, The Netherlands, and the United Kingdom. Cancer incidence, cancer mortality, and all-cause mortality data were collected from 347 parents of unrelated MAP index cases and the spouses of 3 index cases who were also found to be heterozygous for single MUTYH mutations. These data were compared with appropriate national sex-, age-, and period-specific population data to obtain standardized mortality ratios (SMR) and standardized incidence ratios (SIR). Results There was a 2-fold increase in the incidence of colorectal cancer among parents of MAP cases, compared with the general population (SIR, 2.12; 95% confidence interval [CI]: 1.30–3.28). Their colorectal cancer mortality was not increased significantly (SMR, 1.02; 95% CI: 0.41–2.10) nor was overall cancer risk (SIR, 0.92; 95% CI: 0.70–1.18), cancer mortality (SMR, 1.12; 95% CI: 0.83–1.48), or overall mortality (SMR, 0.94; 95% CI: 0.80–1.08). Conclusions The risk of colorectal cancer in heterozygous carriers of single MUTYH mutations who are relatives of patients with MAP is comparable with that of first-degree relatives of patients with sporadic colorectal cancer. Screening measures should be based on this modest increase in risk.

Published
2009
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