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1. Undetected Neuromuscular Disease in Patients after Heart Transplantation.

Author

Bekele, Biniam Melese, Gazzerro, Elisabetta, Schoenrath, Felix, Falk, Volkmar, Rost, Simone, Hoerning, Selina, Jelting, Yvonne, Zaum, Ann-Kathrin, Spuler, Simone, and Knierim, Jan

Subjects
HEART transplant recipients, HEART, NEUROMUSCULAR diseases, CARDIAC patients, MUSCLE weakness, NEUROLOGIC examination
Abstract

(1) Heart transplantation (HTX) improves the overall survival and functional status of end-stage heart failure patients with cardiomyopathies (CMPs). The majority of CMPs have genetic causes, and the overlap between CMPs and inherited myopathies is well documented. However, the long-term outcome in skeletal muscle function and possibility of an undiagnosed underlying genetic cause of both a cardiac and skeletal pathology remain unknown. (2) Thirty-nine patients were assessed using open and standardized interviews on muscle function, a quality-of-life (EuroQol EQ-5D-3L) questionnaire, and a physical examination (Medical Research Council Muscle scale). Whole-exome sequencing was completed in three stages for those with skeletal muscle weakness. (3) Seven patients (17.9%) reported new-onset muscle weakness and motor limitations. Objective muscle weakness in the upper and lower extremities was seen in four patients. In three of them, exome sequencing revealed pathogenic/likely pathogenic variants in the genes encoding nexilin, myosin heavy chain, titin, and SPG7. (4) Our findings support a positive long-term outcome of skeletal muscle function in HTX patients. However, 10% of patients showed clinical signs of myopathy due to a possible genetic cause. The integration of genetic testing and standardized neurological assessment of motor function during the peri-HTX period should be considered. [ABSTRACT FROM AUTHOR]

Published
2024
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5. Homozygous Inversion on Chromosome 13 Involving SGCG Detected by Short Read Whole Genome Sequencing in a Patient Suffering from Limb-Girdle Muscular Dystrophy

Author

Pluta, Natalie, primary, Hoffjan, Sabine, additional, Zimmer, Frederic, additional, Köhler, Cornelia, additional, Lücke, Thomas, additional, Mohr, Jennifer, additional, Vorgerd, Matthias, additional, Nguyen, Hoa Huu Phuc, additional, Atlan, David, additional, Wolf, Beat, additional, Zaum, Ann-Kathrin, additional, and Rost, Simone, additional

Published
2022
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8. CRISPR/Cas9-edited PKP2 knock-out (JMUi001-A-2) and DSG2 knock-out (JMUi001-A-3) iPSC lines as an isogenic human model system for arrhythmogenic cardiomyopathy (ACM)

Author

Janz, Anna, Zink, Miriam, Cirnu, Alexandra, Hartleb, Annika, Albrecht, Christina, Rost, Simone, Klopocki, Eva, Günther, Katharina, Edenhofer, Frank, Ergün, Süleyman, and Gerull, Brenda

Subjects
Desmoglein 2, QH301-705.5, Induced Pluripotent Stem Cells, Mutation, Humans, Myocytes, Cardiac, ddc:610, Biology (General), CRISPR-Cas Systems, Cardiomyopathies, Plakophilins
Abstract

Arrhythmogenic cardiomyopathy (ACM) is characterized by fibro-fatty replacement of the myocardium, heart failure and life-threatening ventricular arrhythmias. Causal mutations were identified in genes encoding for proteins of the desmosomes, predominantly plakophilin-2 (PKP2) and desmoglein-2 (DSG2). We generated gene-edited knock-out iPSC lines for PKP2 (JMUi001-A-2) and DSG2 (JMUi001-A-3) using the CRISPR/Cas9 system in a healthy control iPSC background (JMUi001-A). Stem cell-like morphology, robust expression of pluripotency markers, embryoid body formation and normal karyotypes confirmed the generation of high quality iPSCs to provide a novel isogenic human in vitro model system mimicking ACM when differentiated into cardiomyocytes.

Published
2021

10. The genetic basis of resistance to anticoagulants in rodents

Author

Pelz, Hans-Joachim, Rost, Simone, Hunerberg, Mirja, Fregin, Andreas, Heiberg, Ann-Charlotte, Baert, Kristof, MacNicoll, Alan D., Prescott, Colin V., Walker, Anne-Sophie, Oldenburg, Johannes, and Muller, Clemens R.

Subjects
Rodenticides -- Research, Genetics -- Research, Anticoagulants (Medicine) -- Research, Anticoagulants (Medicine) -- Usage, Anticoagulants (Medicine) -- Genetic aspects, Genetic research, Biological sciences
Abstract

Anticoagulant compounds, i.e., derivatives of either 4-hydroxycoumarin (e.g., warfarin, bromadiolone) or indane-l,3-dione (e.g., diphacinone, chlorophacinone), have been in worldwide use as rodenticides for >50 years. These compounds inhibit blood coagulation by repression of the vitamin K reductase reaction (VKOR). Anticoagulant-resistant rodent populations have been reported from many countries and pose a considerable problem for pest control. Resistance is transmitted as an autosomal dominant trait although, until recently, the basic genetic mutation was unknown. Here, we report on the identification of eight different mutations in the VKORC1 gene in resistant laboratory strains of brown rats and house mice and in wild-caught brown rats from various locations in Europe with five of these mutations affecting only two amino acids (Tyr139Cys, Tyr139Ser, Tyr139Phe and Leu128Gln, Leu128Ser). By recombinant expression of VKORC1 constructs in HEK293 cells we demonstrate that mutations at Tyr139 confer resistance to warfarin at variable degrees while the other mutations, in addition, dramatically reduce VKOR activity. Our data strongly argue for at least seven independent mutation events in brown rats and two in mice. They suggest that mutations in VKORC1 are the genetic basis of anticoagulant resistance in wild populations of rodents, although the mutations alone do not explain all aspects of resistance that have been reported. We hypothesize that these mutations, apart from generating structural changes in the VKORC1 protein, may induce compensatory mechanisms to maintain blood clotting. Our findings provide the basis for a DNA-based field monitoring of anticoagulant resistance in rodents.

Published
2005

11. Mutations in VKORC1 cause warfarin resistance and multiple coagulation factor deficiency type 2

Author

Rost, Simone, Fregin, Andreas, Ivaskevicius, Vytautas, Conzelmann, Ernst, Hortnagel, Konstanze, Pelz, Hans-Joachim, Lappegard, Knut, Seifried, Erhard, Scharrer, Inge, Tuddenham, Edward G. D., Muller, Clemens R., Strom, Tim M., and Oldenburg, Johannes

Subjects
Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Author(s): Simone Rost [1, 2, 10]; Andreas Fregin [1, 10]; Vytautas Ivaskevicius [3]; Ernst Conzelmann [4]; Konstanze Hörtnagel [2]; Hans-Joachim Pelz [5]; Knut Lappegard [6]; Erhard Seifried [3]; Inge Scharrer [...]

Published
2004
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13. Generation of two patient-derived iPSC lines from siblings (LIBUCi001-A and LIBUCi002-A) and a genetically modified iPSC line (JMUi001-A-1) to mimic dilated cardiomyopathy with ataxia (DCMA) caused by a homozygous DNAJC19 mutation

Author

Janz, Anna, primary, Chen, Ruping, additional, Regensburger, Martina, additional, Ueda, Yuichiro, additional, Rost, Simone, additional, Klopocki, Eva, additional, Günther, Katharina, additional, Edenhofer, Frank, additional, Duff, Henry J., additional, Ergün, Süleyman, additional, and Gerull, Brenda, additional

Published
2020
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14. Targeted Gene Expression Profile Reveals CDK4 as Therapeutic Target for Selected Patients With Adrenocortical Carcinoma

Author

Liang, Raimunde, primary, Weigand, Isabel, additional, Lippert, Juliane, additional, Kircher, Stefan, additional, Altieri, Barbara, additional, Steinhauer, Sonja, additional, Hantel, Constanze, additional, Rost, Simone, additional, Rosenwald, Andreas, additional, Kroiss, Matthias, additional, Fassnacht, Martin, additional, Sbiera, Silviu, additional, and Ronchi, Cristina L., additional

Published
2020
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15. Exon-4 Mutations in KRAS Affect MEK/ERK and PI3K/AKT Signaling in Human Multiple Myeloma Cell Lines

Author

Weißbach, Susann, primary, Heredia-Guerrero, Sofia Catalina, additional, Barnsteiner, Stefanie, additional, Großhans, Lukas, additional, Bodem, Jochen, additional, Starz, Hanna, additional, Langer, Christian, additional, Appenzeller, Silke, additional, Knop, Stefan, additional, Steinbrunn, Torsten, additional, Rost, Simone, additional, Einsele, Hermann, additional, Bargou, Ralf Christian, additional, Rosenwald, Andreas, additional, Stühmer, Thorsten, additional, and Leich, Ellen, additional

Published
2020
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16. Targeted Gene Expression Profile Reveals CDK4 as Therapeutic Target for Selected Patients With Adrenocortical Carcinoma

Author

Liang, Raimunde, Weigand, Isabel, Lippert, Juliane, Kircher, Stefan, Altieri, Barbara, Steinhauer, Sonja, Hantel, Constanze, Rost, Simone, Rosenwald, Andreas, Kroiss, Matthias, Fassnacht, Martin, Sbiera, Silviu, Ronchi, Cristina L, University of Zurich, and Ronchi, Cristina L

Subjects
2712 Endocrinology, Diabetes and Metabolism, 10265 Clinic for Endocrinology and Diabetology, 610 Medicine & health
Published
2020

18. Novel mutations in the VKORC1 gene of wild rats and mice – a response to 50 years of selection pressure by warfarin?

Author

Jäkel Thomas, Song Ki-Joon, MacNicoll Alan D, León Vanina, Menzel Sandra, Pelz Hans-Joachim, Rost Simone, Oldenburg Johannes, and Müller Clemens R

Subjects
Genetics, QH426-470
Abstract

Abstract Background Coumarin derivatives have been in world-wide use for rodent pest control for more than 50 years. Due to their retarded action as inhibitors of blood coagulation by repression of the vitamin K reductase (VKOR) activity, they are the rodenticides of choice against several species. Resistance to these compounds has been reported for rodent populations from many countries around the world and poses a considerable problem for efficacy of pest control. Results In the present study, we have sequenced the VKORC1 genes of more than 250 rats and mice trapped in anticoagulant-exposed areas from four continents, and identified 18 novel and five published missense mutations, as well as eight neutral sequence variants, in a total of 178 animals. Mutagenesis in VKORC1 cDNA constructs and their recombinant expression revealed that these mutations reduced VKOR activities as compared to the wild-type protein. However, the in vitro enzyme assay used was not suited to convincingly demonstrate the warfarin resistance of all mutant proteins Conclusion Our results corroborate the VKORC1 gene as the main target for spontaneous mutations conferring warfarin resistance. The mechanism(s) of how mutations in the VKORC1 gene mediate insensitivity to coumarins in vivo has still to be elucidated.

Published
2009
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20. De novo factor VIII gene intron 22 inversion in a female carrier presents as a somatic mosaicism

Author

El Maarri, Osman, Oldenburg, Johannes, Rost, Simone, Leuer, Marco, Olek, Klaus, Muller, Clemen R., Schwaab, Rainer, El Maarri, Osman, Oldenburg, Johannes, Rost, Simone, Leuer, Marco, Olek, Klaus, Muller, Clemen R., and Schwaab, Rainer

Abstract

The intron 22 inversion represents the most prevalentfactor VIII gene defect in severe hemophilia A, accounting for about 40% of all mutations. It is hypothesized that the inversion mutations occur almost exclusively in germ cells during meiotic cell division by intrachromosomal recombination between 1 of 2 telomeric copies of the Int22h region and its intragenic homologue. The majority of inversion mutations originate in male germ cells, where the lack of bivalent formation may facilitate flipping of the telomeric end of the single X chromosome. This is the first intron 22 inversion that presents as a somatic mosaicism in a female, affecting only about 50% of lymphocyte and fibroblast cells of the proposita. Supposing a post-zygotic de novo mutation as the usual cause of somatic mosaicism, the finding would imply that the intron 22 inversion mutation is not restricted to meiotic cell divisions but can also occur during mitotic cell divisions, either in germ cell precursors or in somatic cells.

Published
2017

23. Confirmation of warfarin resistance of naturally occurring VKORC1 variants by coexpression with coagulation factor IX and in silico protein modelling

Author

Müller, Elisabeth, Keller, Alexander, Fregin, Andreas, Müller, Clemens R, and Rost, Simone

Subjects
Genetics, Genetics(clinical), ddc:610
Abstract

Background VKORC1 has been identified some years ago as the gene encoding vitamin K epoxide reductase (VKOR) – the target protein for coumarin derivates like warfarin or phenprocoumon. Resistance against warfarin and other coumarin-type anticoagulants has been frequently reported over the last 50 years in rodents due to problems in pest control as well as in thrombophilic patients showing variable response to anticoagulant treatment. Many different mutations have already been detected in the VKORC1 gene leading to warfarin resistance in rats, mice and in humans. Since the conventional in vitro dithiothreitol (DTT)-driven VKOR enzymatic assay often did not reflect the in vivo status concerning warfarin resistance, we recently developed a cell culture-based method for coexpression of VKORC1 with coagulation factor IX and subsequent measurement of secreted FIX in order to test warfarin inhibition in wild-type and mutated VKORC1. Results In the present study, we coexpressed wild-type factor IX with 12 different VKORC1 variants which were previously detected in warfarin resistant rats and mice. The results show that amino acid substitutions in VKORC1 maintain VKOR activity and are associated with warfarin resistance. When we projected in silico the amino acid substitutions onto the published three-dimensional model of the bacterial VKOR enzyme, the predicted effects matched well the catalytic mechanism proposed for the bacterial enzyme. Conclusions The established cell-based system for coexpression of VKORC1 and factor IX uses FIX activity as an indicator of carboxylation efficiency. This system reflects the warfarin resistance status of VKORC1 mutations from anticoagulant resistant rodents more closely than the traditional DTT-driven enzyme assay. All mutations studied were also predicted to be involved in the reaction mechanism.

Published
2014

24. Molecular Causes of Vitamin K-dependent Coagulation Disorders

Author

Rost, Simone Esther

Subjects
ddc:570, Koagulopathie, Vitamin-K-Gruppe, Genanalyse
Abstract

Vitamin K ist ein essentieller Cofaktor für die posttranslationale Gamma-Carboxylierung von sog. Vitamin K-abhängigen Gerinnungsfaktoren, Knochenproteinen, Zellwachstum-regulierenden und weiteren Proteinen mit noch unbekannter Funktion. Defekte im Vitamin K-Stoffwechsel führen einerseits zu zwei verschiedenen Formen des familiären Mangels aller Vitamin K-abhängigen Gerinnungsfaktoren (VKCFD1 und 2) und andererseits zur Resistenz oder Hypersensitivität gegenüber Cumarinderivaten, wie Warfarin, die als Vitamin K-Antagonisten zur Antikoagulationstherapie bei thromboembolischen Erkrankungen, aber auch zur Bekämpfung von Ratten und Mäusen eingesetzt werden. Die Aufklärung und Charakterisierung der molekularen Ursachen dieser Erkrankungen wird in dieser Doktorarbeit anhand von Veröffentlichungen dokumentiert. Ausgehend von der Charakterisierung zweier Familien mit dem VKCFD2-Phänotyp, wird die Kartierung des VKCFD2-Locus auf dem kurzen Arm von Chromosom 16 beschrieben. Durch eine systematische Mutationssuche in der ca. 130 Gene umfassenden Kandidatenregion von Chromosom 16 konnte das für diese Erkrankung und die Warfarinresistenz ursächliche Gen ausfindig gemacht werden. Dabei handelt es sich um das Gen für die entscheidende Komponente der Vitamin K-Epoxid-Reduktase (VKORC1), die den Recycling-Prozess von Vitamin K im sog. Vitamin K-Zyklus katalysiert. Die Charakterisierung des VKORC1-Proteins umfasst dessen subzelluläre Lokalisation, den Vergleich orthologer Proteine in verschiedenen Species und die funktionelle Charakterisierung von rekombinant exprimiertem VKORC1. Durch positionsspezifische Mutagenesen und anschließende Expression in humanen Nierenzellen konnten mehrere für die Funktion der VKORC1 relevante Aminosäuren identifiziert werden. Die posttranslationale Modifikation der Vitamin K-abhängigen Proteine wird von der Gamma-Glutamyl-Carboxylase (GGCX) katalysiert. Defekte in diesem Enzym wurden von zwei verschiedenen Arbeitsgruppen als Ursache für die erste Form der VKCFD-Erkrankung nachgewiesen. In dieser Doktorarbeit werden drei weitere, von unserer Arbeitsgruppe identifizierte Mutationen im GGCX-Gen beschrieben, unter denen sich ein nachgewiesener Founder-Effekt an Position 485 des Proteins befindet. Die Arg485Pro-Variante wurde rekombinant in Insektenzellen exprimiert und konnte mittels kinetischer Studien als VKCFD1-verursachende Mutation verifiziert werden., Vitamin K is an essential cofactor for the posttranslational gamma-carboxylation of the so-called vitamin K-dependent coagulation factors, bone proteins, cell growth regulating proteins and others of unknown function. Defects in vitamin K metabolism cause two different forms of combined deficiency of vitamin K-dependent coagulation factors (VKCFD type 1 and type 2) as well as resistance or hypersensitivity to coumarin derivates, such as warfarin, which act as vitamin K antagonists. Coumarins are used for anticoagulation therapy of thromboembolic diseases and in higher dosis also for rodent pest control. The aim of this thesis is to characterize the molecular basis of these diseases. This work has led to six publications. The VKCFD type 2 phenotype as described in two unrelated families was used to perform a homozygosity mapping of the VKCFD2 locus on the short arm of chromosome 16. A systematic mutation screening in the candidate region on chromosome 16 comprising approximately 130 putative genes resulted in the identification of the gene causative for VKCFD2 and the allelic phenotype warfarin resistance. This gene encodes the first identified component of the vitamin K epoxide reductase (VKORC1) which catalyzes the reduction of vitamin K epoxide as an important part of the so-called vitamin K cycle. Characterization of the VKORC1 protein includes its subcellular localization, comparison of orthologous proteins in different species and functional studies of the recombinant VKORC1. Amino acids which are relevant for protein structure or function were identified by site-directed mutagenesis experiments and subsequent expression in human embryonic kidney cells (HEK293). Posttranslational modification of the vitamin K-dependent proteins is catalysed by the gamma-glutamyl carboxylase (GGCX), an enzyme of the endoplasmic reticulum. Mutations in the gene encoding this enzyme were demonstrated to be causative for VKCFD type 1 by two different working groups. Our working group identified three additional mutations in the GGCX gene. Recurrent mutations at position 485 of the protein were shown to result from a founder effect. The Arg485Pro variant was recombinantly expressed in insect cells using the baculovirus system and could be verified as a causative mutation for the VKCFD1 phenotype by kinetic studies.

Published
2006

25. Novel recessive myotilin mutation causes severe myofibrillar myopathy

Author

Schessl, Joachim, Bach, Elisa, Rost, Simone, Feldkirchner, Sarah, Kubny, Christiana, Mueller, Stefan, Hanisch, Franz-Georg, Kress, Wolfram, Schoser, Benedikt, Schessl, Joachim, Bach, Elisa, Rost, Simone, Feldkirchner, Sarah, Kubny, Christiana, Mueller, Stefan, Hanisch, Franz-Georg, Kress, Wolfram, and Schoser, Benedikt

Abstract

We identified the first homozygous and hence recessive mutation in the myotilin gene (MYOT) in a family affected by a severe myofibrillar myopathy (MFM). MFM is a rare, progressive and devastating disease of human skeletal muscle with distinct histopathological pattern of protein aggregates and myofibrillar degeneration. So far, only heterozygous missense mutations in MYOT have been associated with autosomal dominant myofibrillar myopathy, limb-girdle muscular dystrophy type 1A and distal myopathy. Myotilin itself is highly expressed in skeletal and cardiac muscle and is localized at the Z-disc and therefore interacts in sarcomere assembly. We performed whole-exome sequencing in a German family clinically diagnosed with MFM and identified a homozygous mutation in exon 2, c.16C > G (p.Arg6Gly). Using laser microdissection followed by quantitative mass spectrometry, we identified the myotilin protein as one component showing the highest increased abundance in the aggregates in the index patient. We suggest that the combined approach has a high potential as a new tool for the confirmation of unclassified variants which are found in whole-exome sequencing approaches.

Published
2014

28. Novel form of X-linked nonsyndromic hearing loss with cochlear malformation caused by a mutation in the type IV collagen gene COL4A6

Author

Rost, Simone, primary, Bach, Elisa, additional, Neuner, Cordula, additional, Nanda, Indrajit, additional, Dysek, Sandra, additional, Bittner, Reginald E, additional, Keller, Alexander, additional, Bartsch, Oliver, additional, Mlynski, Robert, additional, Haaf, Thomas, additional, Müller, Clemens R, additional, and Kunstmann, Erdmute, additional

Published
2013
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30. Diagnostic approach for FSHD revisited: SMCHD1 mutations cause FSHD2 and act as modifiers of disease severity in FSHD1.

Author

Larsen, Mirjam, Rost, Simone, El Hajj, Nady, Ferbert, Andreas, Deschauer, Marcus, Walter, Maggie C, Schoser, Benedikt, Tacik, Pawel, Kress, Wolfram, and Müller, Clemens R

Subjects
*FACIOSCAPULOHUMERAL muscular dystrophy, *MUSCLE abnormalities, *METHYLATION kinetics, *SHOULDER girdle, *CHROMOSOME abnormalities, *DISEASES
Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is an autosomal dominant muscular disorder with a wide clinical variability. Contractions of the D4Z4 macrosatellite repeat on chromosome 4q35 are the molecular basis of the pathophysiology. Recently, in a subset of patients without D4Z4 repeat contractions, variants in the SMCHD1 gene have been identified that lead to hypomethylation of D4Z4 and thus DUX4 transcription, which causes FSHD type 2. In this study, we have screened 55 FSHD1-negative and 40 FSHD1-positive patients from unrelated families for potentially pathogenic variants in SMCHD1 by next-generation sequencing (NGS). We identified variants in SMCHD1 in 11 index patients, including missense, splice site and non-sense mutations. We developed a pyrosequencing assay to determine the methylation status of the D4Z4 repeat array and found significantly lower methylation levels for FSHD2 patients than for healthy controls and FSHD1 patients. Two out of eleven SMCHD1 mutation carriers had moderately contracted D4Z4 alleles thus these patients are suffering from FSHD1 and 2. Comparing the phenotype of patients, all FSHD2 patients were relatively mildly affected while patients with FSHD1+2 were much more severely affected than expected from their D4Z4 copy number. Our findings confirm the role of SMCHD1 mutations in FSHD2 and as a modifier of disease severity. With SMCHD1 variants found in 16.4% of phenotypic FSHD patients without D4Z4 repeat contractions, the incidence of FSHD2 is rather high and hence we suggest including sequencing of SMCHD1, haplotyping and methylation analysis in the workflow of molecular FSHD diagnostics. [ABSTRACT FROM AUTHOR]

Published
2015
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31. Mutations in the VKORC1 Gene Cause Warfarin Resistance, Warfarin Sensitivity and Combined Deficiency of Vitamin K Dependent Coagulation Factors.

Author

Oldenburg, Johannes, primary, Rost, Simone, primary, Fregin, Andreas, primary, Geisen, Christof, primary, Ivaskevicius, Vytautas, primary, Seifried, Erhard, primary, Scharrer, Inge, primary, Heistinger, Maximilian, primary, Tuddenham, Edward, primary, Muller-Reible, Clemens, primary, and Zieger, Barbara, primary

Published
2004
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32. Novel form of X-linked nonsyndromic hearing loss with cochlear malformation caused by a mutation in the type IV collagen gene COL4A6.

Author

Rost, Simone, Bach, Elisa, Neuner, Cordula, Nanda, Indrajit, Dysek, Sandra, Bittner, Reginald E, Keller, Alexander, Bartsch, Oliver, Mlynski, Robert, Haaf, Thomas, Müller, Clemens R, and Kunstmann, Erdmute

Subjects
*X-linked genetic disorders, *HEARING disorders, *KIDNEY diseases, *CATARACT
Abstract

Hereditary hearing loss is the most common human sensorineural disorder. Genetic causes are highly heterogeneous, with mutations detected in >40 genes associated with nonsyndromic hearing loss, to date. Whereas autosomal recessive and autosomal dominant inheritance is prevalent, X-linked forms of nonsyndromic hearing impairment are extremely rare. Here, we present a Hungarian three-generation family with X-linked nonsyndromic congenital hearing loss and the underlying genetic defect. Next-generation sequencing and subsequent segregation analysis detected a missense mutation (c.1771G>A, p.Gly591Ser) in the type IV collagen gene COL4A6 in all affected family members. Bioinformatic analysis and expression studies support this substitution as being causative. COL4A6 encodes the alpha-6 chain of type IV collagen of basal membranes, which forms a heterotrimer with two alpha-5 chains encoded by COL4A5. Whereas mutations in COL4A5 and contiguous X-chromosomal deletions involving COL4A5 and COL4A6 are associated with X-linked Alport syndrome, a nephropathy associated with deafness and cataract, mutations in COL4A6 alone have not been related to any hereditary disease so far. Moreover, our index patient and other affected family members show normal renal and ocular function, which is not consistent with Alport syndrome, but with a nonsyndromic type of hearing loss. In situ hybridization and immunostaining demonstrated expression of the COL4A6 homologs in the otic vesicle of the zebrafish and in the murine inner ear, supporting its role in normal ear development and function. In conclusion, our results suggest COL4A6 as being the fourth gene associated with X-linked nonsyndromic hearing loss. [ABSTRACT FROM AUTHOR]

Published
2014
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33. Novel mutations in the VKORC1 gene of wild rats and mice -- a response to 50 years of selection pressure by warfarin?

Author

Rost, Simone, Pelz, Hans-Joachim, Menzel, Sandra, MacNicoll, Alan D., León, Vanina, Ki-Joon Song, Jäkel, Thomas, Oldenburg, Johannes, and Müller, Clemens R.

Subjects
*COUMARINS, *RODENT control, *BLOOD coagulation, *GENES, *GENETIC mutation
Abstract

Background: Coumarin derivatives have been in world-wide use for rodent pest control for more than 50 years. Due to their retarded action as inhibitors of blood coagulation by repression of the vitamin K reductase (VKOR) activity, they are the rodenticides of choice against several species. Resistance to these compounds has been reported for rodent populations from many countries around the world and poses a considerable problem for efficacy of pest control. Results: In the present study, we have sequenced the VKORC1 genes of more than 250 rats and mice trapped in anticoagulant-exposed areas from four continents, and identified 18 novel and five published missense mutations, as well as eight neutral sequence variants, in a total of 178 animals. Mutagenesis in VKORC1 cDNA constructs and their recombinant expression revealed that these mutations reduced VKOR activities as compared to the wild-type protein. However, the in vitro enzyme assay used was not suited to convincingly demonstrate the warfarin resistance of all mutant proteins Conclusion: Our results corroborate the VKORC1 gene as the main target for spontaneous mutations conferring warfarin resistance. The mechanism(s) of how mutations in the VKORC1 gene mediate insensitivity to coumarins in vivo has still to be elucidated. [ABSTRACT FROM AUTHOR]

Published
2009
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34. De novo factor VIIIgene intron 22 inversion in a female carrier presents as a somatic mosaicism

Author

Oldenburg, Johannes, Rost, Simone, El-Maarri, Osman, Leuer, Marco, Olek, Klaus, Müller, Clemens R., and Schwaab, Rainer

Abstract

The intron 22 inversion represents the most prevalentfactor VIIIgene defect in severe hemophilia A, accounting for about 40% of all mutations. It is hypothesized that the inversion mutations occur almost exclusively in germ cells during meiotic cell division by intrachromosomal recombination between 1 of 2 telomeric copies of the Int22h region and its intragenic homologue. The majority of inversion mutations originate in male germ cells, where the lack of bivalent formation may facilitate flipping of the telomeric end of the single X chromosome. This is the first intron 22 inversion that presents as a somatic mosaicism in a female, affecting only about 50% of lymphocyte and fibroblast cells of the proposita. Supposing a post-zygotic de novo mutation as the usual cause of somatic mosaicism, the finding would imply that the intron 22 inversion mutation is not restricted to meiotic cell divisions but can also occur during mitotic cell divisions, either in germ cell precursors or in somatic cells.

Published
2000
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35. Updated Structure of CNBP Repeat Expansions in Patients With Myotonic Dystrophy Type 2 and Its Implication for Standard Diagnostics.

Author

Wendlandt M, Erdmann H, Rost S, Lucas MC, Becker K, Kleinle S, Timmer M, Bier A, Wunderlich G, Wenninger S, Walter MC, Neuhann T, Schoser B, Holinski-Feder E, and Abicht A

Abstract

Background and Objectives: Myotonic dystrophy type 2 (DM2) is a multisystemic repeat disorder caused by the expansion of an unstable CCTG tetranucleotide repeat in the noncoding region of the CNBP gene. Standard diagnostic is based on Southern blot analysis or a unidirectional RP-PCR that amplifies the repeat from the downstream end., Methods: Our study reevaluated 80 patients (cohort 1) with clinical suspicion of DM2 but homozygous negative results using the standard diagnostic repeat-primed PCR (RP-PCR). Reanalysis was performed using a second RP-PCR that amplifies the repeat from the opposite direction. Individual samples were further analyzed by Oxford Nanopore Technology long-read sequencing, Sanger sequencing, and another RP-PCR. In addition, repeat expansions were further characterized in 168 patients with confirmed DM2 (cohort 2)., Results: We identified 5 of the 80 patients (cohort 1) with expanded repeats in CNBP and, as such, reclassified them as positive for DM2. The initial false-negative results were attributed to variants within the primer binding site of the standard RP-PCR in one patient and an additional novel (TCTG) n repeat downstream to the known (CCTG) n repeat in 4 other patients. By analyzing a cohort of 168 patients with confirmed DM2 (cohort 2), we found that the additional (TCTG) n repeat is present in at least 84% of patients., Discussion: Our study revealed the presence of an additional repeat (TCTG) n in most of the patients living with DM2. Large expansions of this repeat likely hinder sufficient amplification of the disease causing (CCTG) n repeat. Because the (TCTG) n repeat is likely mosaic in length, (CCTG) n repeat expansions are correctly detected in most patients. However, a few patients are at risk of a false-negative result using the standard RP-PCR, which had a false-negative rate of 0.7% (5/674) and a sensitivity of 97.3% in the cohort studied. Based on our findings, we propose (TG) v (TCTG) w (CCTG) n (TCTG') m as the updated model for the structure of CNBP repeat expansions and recommend adapting the diagnostic guidelines accordingly. The effect of the (TCTG) n repeat on the phenotype remains to be determined but could be key for establishing a phenotype-genotype correlation for DM2 that remained elusive so far., Competing Interests: The authors report no relevant disclosures. Go to Neurology.org/NG for full disclosures., (Copyright © 2024 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Academy of Neurology.)

Published
2024
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36. Confirmation of warfarin resistance of naturally occurring VKORC1 variants by coexpression with coagulation factor IX and in silico protein modelling.

Author

Müller E, Keller A, Fregin A, Müller CR, and Rost S

Subjects
Amino Acid Substitution, Animals, Bacterial Proteins genetics, HEK293 Cells, Humans, Isoenzymes genetics, Mice, Models, Molecular, Mutagenesis, Site-Directed, Mutation, Rats, Synechococcus enzymology, Factor IX genetics, Metabolism, Inborn Errors genetics, Vitamin K Epoxide Reductases genetics
Abstract

Background: VKORC1 has been identified some years ago as the gene encoding vitamin K epoxide reductase (VKOR) - the target protein for coumarin derivates like warfarin or phenprocoumon. Resistance against warfarin and other coumarin-type anticoagulants has been frequently reported over the last 50 years in rodents due to problems in pest control as well as in thrombophilic patients showing variable response to anticoagulant treatment. Many different mutations have already been detected in the VKORC1 gene leading to warfarin resistance in rats, mice and in humans. Since the conventional in vitro dithiothreitol (DTT)-driven VKOR enzymatic assay often did not reflect the in vivo status concerning warfarin resistance, we recently developed a cell culture-based method for coexpression of VKORC1 with coagulation factor IX and subsequent measurement of secreted FIX in order to test warfarin inhibition in wild-type and mutated VKORC1., Results: In the present study, we coexpressed wild-type factor IX with 12 different VKORC1 variants which were previously detected in warfarin resistant rats and mice. The results show that amino acid substitutions in VKORC1 maintain VKOR activity and are associated with warfarin resistance. When we projected in silico the amino acid substitutions onto the published three-dimensional model of the bacterial VKOR enzyme, the predicted effects matched well the catalytic mechanism proposed for the bacterial enzyme., Conclusions: The established cell-based system for coexpression of VKORC1 and factor IX uses FIX activity as an indicator of carboxylation efficiency. This system reflects the warfarin resistance status of VKORC1 mutations from anticoagulant resistant rodents more closely than the traditional DTT-driven enzyme assay. All mutations studied were also predicted to be involved in the reaction mechanism.

Published
2014
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