Your search keyword '"Bettina Prager"' showing total 6 results

1. Integration of Hi-C with short and long-read genome sequencing reveals the structure of germline rearranged genomes

Author

Robert Schöpflin, Uirá Souto Melo, Hossein Moeinzadeh, David Heller, Verena Laupert, Jakob Hertzberg, Manuel Holtgrewe, Nico Alavi, Marius-Konstantin Klever, Julius Jungnitsch, Emel Comak, Seval Türkmen, Denise Horn, Yannis Duffourd, Laurence Faivre, Patrick Callier, Damien Sanlaville, Orsetta Zuffardi, Romano Tenconi, Nehir Edibe Kurtas, Sabrina Giglio, Bettina Prager, Anna Latos-Bielenska, Ida Vogel, Merete Bugge, Niels Tommerup, Malte Spielmann, Antonio Vitobello, Vera M. Kalscheuer, Martin Vingron, and Stefan Mundlos

Subjects

Science

Abstract

Here the authors characterize structural variations (SVs) in a cohort of individuals with complex genomic rearrangements, identifying breakpoints by employing short- and long-read genome sequencing and investigate their impact on gene expression and the three-dimensional chromatin architecture. They find breakpoints are enriched in inactive regions and can result in chromatin domain fusions.

Published

2022

2. PORCNmutations in focal dermal hypoplasia: coping with lethality

Author

Kaatje Heinelt, Juliane Strien, Annalisa Patrizi, María del Carmen Boente, Karl-Heinz Grzeschik, Yasemin Alanay, Nicolas Chassaing, Ben C.J. Hamel, Ingo Lohrisch, Marie Eleanore O. Nicolas, G. Eda Utine, Ian O. Ellis, Carlo Marcelis, Jeffrey A. Ascherman, Katrina Prescott, Bart Loeys, Arne König, Mauro Paradisi, Christina Raissa I. Francisco, Wolfgang Kastrup, Frank Oeffner, Patricia Silvia Della Giovanna, Paul J. Benke, Dorothea Bornholdt, Maria Piccione, Yasmin Mehraein, Cristina Has, Andreas R. Janecke, Ineke van der Burgt, Bettina Prager, Dana Pagliarini, Hildegunde Piza-Katzer, Marc S. Zeller, and Rudolf Happle

Subjects

Genetics, Mutation, Genetic counseling, Nonsense mutation, Biology, medicine.disease_cause, medicine.disease, Focal dermal hypoplasia, PORCN, medicine, Missense mutation, Skewed X-inactivation, Genetics (clinical), Loss function

Abstract

The X-linked dominant trait focal dermal hypoplasia (FDH, Goltz syndrome) is a developmental defect with focal distribution of affected tissues due to a block of Wnt signal transmission from cells carrying a detrimental PORCN mutation on an active X-chromosome. Molecular characterization of 24 unrelated patients from different ethnic backgrounds revealed 23 different mutations of the PORCN gene in Xp11.23. Three were microdeletions eliminating PORCN and encompassing neighboring genes such as EBP, the gene associated with Conradi-Hunermann-Happle syndrome (CDPX2). 12/24 patients carried nonsense mutations resulting in loss of function. In one case a canonical splice acceptor site was mutated, and 8 missense mutations exchanged highly conserved amino acids. FDH patients overcome the consequences of potentially lethal X-chromosomal mutations by extreme skewing of X-chromosome inactivation in females, enabling transmission of the trait in families, or by postzygotic mosaicism both in male and female individuals. Molecular characterization of the PORCN mutations in cases diagnosed as Goltz syndrome is particularly relevant for genetic counseling of patients and their families since no functional diagnostic test is available and carriers of the mutation might otherwise be overlooked due to considerable phenotypic variability associated with the mosaic status.

Published

2009

3. Universal pooled plasma (Uniplas(®)) does not induce complement-mediated hemolysis of human red blood cells in vitro

Author

Jürgen Römisch, Hubert Brandstätter, Janja Brainovic, Andrea Heger, Bettina Prager, and Rhoda Cortes

Subjects

Male, Lysis, Erythrocytes, Hematology, Antigen-Antibody Complex, Biology, medicine.disease, Molecular biology, Hemolysis, In vitro, ABO Blood-Group System, Titer, Plasma, Immune system, Isoantibodies, ABO blood group system, Monoclonal, medicine, biology.protein, Humans, Female, Antibody

Abstract

Background Pooling of plasma of different blood groups before large scale manufacturing of Uniplas ® results in the formation of low levels of soluble immune complexes (CIC). The aim of this study was to investigate the level and removal of CIC during Uniplas ® manufacturing. In addition, an in vitro hemolysis assay should be developed and investigate if Uniplas ® does induce complement-mediated hemolysis of human red blood cells (RBC). Materials and methods In-process samples from Uniplas ® (universal plasma) and Octaplas(LG) ® (blood group specific plasma) routine manufacturing batches were tested on CIC using commercially available ELISA test kits. In addition, CIC was produced by admixing heat-aggregated immunoglobulins or monoclonal anti-A/anti-B antibodies to plasma and removal of CIC was followed in studies of the Uniplas ® manufacturing process under down-scale conditions. The extent of RBC lysis was investigated in plasma samples using the in-house hemolysis assay. Results Levels of CIC in Uniplas ® are within the normal ranges for plasma and comparable to that found in Octaplas(LG) ® . Down-scale experiments showed that both IgG/IgM-CIC levels are significantly removed on average by 40–50% during Uniplas ® manufacturing. Uniplas ® does not induce hemolysis of RBCs in vitro . Hemolysis occurs only after spiking with high titers of anti-A/anti-B antibodies and depends on the antibody specificity (i.e. titer) in the plasma sample. Conclusion The results of this study confirm the safety of Uniplas ® regarding transfusion to patients of all ABO blood groups.

Published

2012

4. Partial trisomy 22q12→qter in prenatal diagnosis

Author

Gunter Mehner, Erika Tolkendorf, and Bettina Prager

Subjects

Adult, medicine.medical_specialty, Amniotic fluid, Chromosomes, Human, Pair 22, Aneuploidy, Chromosome Disorders, Trisomy, Chromosomal translocation, Prenatal diagnosis, Translocation, Genetic, Pregnancy, Gene duplication, medicine, Humans, Genetics (clinical), Chromosome Aberrations, Gynecology, Fetus, Fetal Growth Retardation, business.industry, Obstetrics and Gynecology, medicine.disease, In utero, Karyotyping, Pregnancy Trimester, Second, Amniocentesis, Female, business

Abstract

Ultrasound examination of a 27-year-old primigravida at 26 weeks' gestation revealed fetal growth retardation, malformation of the ventricular septum, and a neck fold. Chromosome analysis of the amniotic fluid showed an abnormal 46,XY karyotype with an obvious metacentric chromosome 17. Chromosome analysis of the mother revealed a balanced t (17;22) (p13;q12) translocation. The fetus thus has a rare familial duplication 22q12----qter. Eight live-born and severely malformed infants with this duplication have been reported in the literature.

Published

1991

5. Shprintzen-Goldberg syndrome: fourteen new patients and a clinical analysis

Author

Stephanie Demuth, Peter N. Robinson, Beate Mitulla, Lutz Pfeiffer, Ursula Jung, Mirja Somer, Sigrid Tinschert, Rainer König, Bettina Prager, Petra Muschke, Dietmar Müller, Luitgard M. Neumann, and Herbert Enders

Subjects

Joint hypermobility, Adult, Heart Defects, Congenital, Male, Pediatrics, medicine.medical_specialty, Adolescent, Craniosynostosis, Marfan Syndrome, Craniofacial Abnormalities, Arachnodactyly, Camptodactyly, Craniosynostoses, stomatognathic system, Genetics, medicine, Humans, Abnormalities, Multiple, Hypertelorism, Child, Genetics (clinical), business.industry, Palate, Shprintzen–Goldberg syndrome, Ear, Anatomy, Syndrome, medicine.disease, Hypotonia, Palpebral fissure, Child, Preschool, Karyotyping, medicine.symptom, business

Abstract

The Shprintzen-Goldberg syndrome (SGS) is a disorder of unknown cause comprising craniosynostosis, a marfanoid habitus and skeletal, neurological, cardiovascular, and connective-tissue anomalies. There are no pathognomonic signs of SGS and diagnosis depends on recognition of a characteristic combination of anomalies. Here, we describe 14 persons with SGS and compare their clinical findings with those of 23 previously reported individuals, including two families with more than one affected individual. Our analysis suggests that there is a characteristic facial appearance, with more than two thirds of all individuals having hypertelorism, down-slanting palpebral fissures, a high-arched palate, micrognathia, and apparently low-set and posteriorly rotated ears. Other commonly reported manifestations include hypotonia in at least the neonatal period, developmental delay, and inguinal or umbilical hernia. The degree of reported intellectual impairment ranges from mild to severe. The most common skeletal manifestations in SGS were arachnodactyly, pectus deformity, camptodactyly, scoliosis, and joint hypermobility. None of the skeletal signs alone is specific for SGS. Our study includes 14 mainly German individuals with SGS evaluated over a period of 10 years. Given that only 23 other persons with SGS have been reported to date worldwide, we suggest that SGS may be more common than previously assumed.

Published

2005

6. Mild phenotype in two unrelated patients with a partial deletion of 21q22.2-q22.3 defined by FISH and molecular studies

Author

Rita Exeler, Annelore Junge, Juergen Horst, Ingo Kennerknecht, Thomas Schmitt-John, Oliver Bartsch, Bettina Prager, Daniela Ehling, Beate Behre, and J. Wirth

Subjects

Male, Monosomy, Chromosomes, Human, Pair 21, Biology, Exon, Holoprosencephaly, medicine, Humans, Genetics (clinical), In Situ Hybridization, Fluorescence, DNA Primers, medicine.diagnostic_test, Base Sequence, Breakpoint, Marfanoid, Infant, Newborn, medicine.disease, Subtelomere, Molecular biology, Palpebral fissure, Phenotype, Karyotyping, Female, Chromosome Deletion, Fluorescence in situ hybridization

Abstract

We describe two unrelated patients with cytogenetically visible deletions of 21q22.2-q22.3 and mild phenotypes. Both patients presented minor dysmorphic features including thin marfanoid build, facial asymmetry, downward-slanting palpebral fissures, depressed nasal bridge, small nose with bulbous tip, and mild mental retardation (MR). FISH and molecular studies indicated common deleted areas but different breakpoints. In patient 1, the breakpoint was fine mapped to a 5.2 kb interval between exon 5 and exon 8 of the ETS2 gene. The subtelomeric FISH probe was absent on one homologue 21 indicating a terminal deletion spanning approximately 7.9 Mb in size. In patient 2, the proximal breakpoint was determined to be 300-700 kb distal to ETS2, and the distal breakpoint 2.5-0.3 Mb from the 21q telomere, indicating an interstitial deletion sized approximately 4.7-7.3 Mb. The 21q- syndrome is rare and typically associated with a severe phenotype, but different outcomes depending on the size and location of the deleted area have been reported. Our data show that monosomy 21q of the area distal to the ETS2 gene, representing the terminal 7.9 Mb of 21q, may result in mild phenotypes comprising facial anomalies, thin marfanoid build, and mild MR, with or without signs of holoprosencephaly.

Published

2004