Your search keyword '"Petra Prückl"' showing total 3 results

1. Standardized, systemic phenotypic analysis of Umod(C93F) and Umod(A227T) mutant mice.

Author

Elisabeth Kemter, Petra Prückl, Birgit Rathkolb, Kateryna Micklich, Thure Adler, Lore Becker, Johannes Beckers, Dirk H Busch, Alexander A Götz, Wolfgang Hans, Marion Horsch, Boris Ivandic, Martin Klingenspor, Thomas Klopstock, Jan Rozman, Anja Schrewe, Holger Schulz, Helmut Fuchs, Valérie Gailus-Durner, Martin Hrabé de Angelis, Eckhard Wolf, and Bernhard Aigner

Subjects

Medicine, Science

Abstract

Uromodulin-associated kidney disease (UAKD) summarizes different clinical features of an autosomal dominant heritable disease syndrome in humans with a proven uromodulin (UMOD) mutation involved. It is often characterized by hyperuricemia, gout, alteration of urine concentrating ability, as well as a variable rate of disease progression inconstantly leading to renal failure and histological alterations of the kidneys. We recently established the two Umod mutant mouse lines Umod(C93F) and Umod(A227T) on the C3H inbred genetic background both showing kidney defects analogous to those found in human UAKD patients. In addition, disease symptoms were revealed that were not yet described in other published mouse models of UAKD. To examine if further organ systems and/or metabolic pathways are affected by Umod mutations as primary or secondary effects, we describe a standardized, systemic phenotypic analysis of the two mutant mouse lines Umod(A227T) and Umod(C93F) in the German Mouse Clinic. Different genotypes as well as different ages were tested. Beside the already published changes in body weight, body composition and bone metabolism, the influence of the Umod mutation on energy metabolism was confirmed. Hematological analysis revealed a moderate microcytic and erythropenic anemia in older Umod mutant mice. Data of the other analyses in 7-10 month-old mutant mice showed single small additional effects.

Published

2013

2. Distinct Morphological and Behavioural Alterations in ENU-Induced Heterozygous Trpc7K810Stop Mutant Mice

Author

Susanne K. Sauer, Stefan Krebs, Petra Prückl, Bernhard Aigner, Martin Hrabě de Angelis, Birgit Rathkolb, and Maike Howaldt

Subjects

Heterozygote, growth, seizure, Mutant, Mutagenesis (molecular biology technique), TRPC7, Biology, QH426-470, medicine.disease_cause, Mice, Mutant protein, Seizures, Exome Sequencing, medicine, Genetics, Animals, ddc:610, Amino Acid Sequence, tissue irritation, Gene, Genetics (clinical), Alleles, Genetic Association Studies, TRPC Cation Channels, Mice, Knockout, Mutation, Mice, Inbred C3H, Genome, Behavior, Animal, Communication, animal model, Phenotype, Stop codon, Mutagenesis, Animal Model, Growth, Seizure, Tissue Irritation, Trpc7, Knockout mouse, Models, Animal

Abstract

Trpc7 (transient receptor potential cation channel, subfamily C, member 7; 862 amino acids) knockout mice are described showing no clear phenotypic alterations, therefore, the functional relevance of the gene remains unclear. A complementary approach for the functional analysis of a given gene is the examination of individuals harbouring a mutant allele of the gene. In the phenotype-driven Munich ENU mouse mutagenesis project, a high number of phenotypic parameters was used for establishing novel mouse models on the genetic background of C3H inbred mice. The phenotypically dominant mutant line SMA002 was established and further examined. Analysis of the causative mutation as well as the phenotypic characterization of the mutant line were carried out. The causative mutation was detected in the gene Trpc7 which leads to the production of a truncated protein due to the novel stop codon at amino acid position 810 thereby affecting the highly conserved cytoplasmic C terminus of the protein. Trpc7 heterozygous mutant mice of both sexes were viable and fertile, but showed distinct morphological and behavioural alterations which is in contrast to the published phenotype of Trpc7 knockout mice. Thus, the Trpc7K810Stop mutation leads to a dominant negative effect of the mutant protein.

Published

2021

3. Standardized, systemic phenotypic analysis of UmodC93F and UmodA227T mutant mice

Author

Johannes Beckers, Jan Rozman, Marion Horsch, Thure Adler, Eckhard Wolf, Birgit Rathkolb, Martin Klingenspor, Wolfgang Hans, Bernhard Aigner, Dirk H. Busch, Boris Ivandic, Holger Schulz, Valerie Gailus-Durner, Elisabeth Kemter, Thomas Klopstock, Lore Becker, Martin Hrabé de Angelis, Petra Prückl, Anja Schrewe, Kateryna Micklich, Alexander Götz, and Helmut Fuchs

Subjects

Male, Tamm–Horsfall protein, Genotype, Mutant, lcsh:Medicine, Biology, medicine.disease_cause, Uromodulin, medicine, Animals, Hyperuricemia, lcsh:Science, Genetics, Mice, Inbred C3H, Kidney, Mutation, Multidisciplinary, lcsh:R, Anemia, Reference Standards, medicine.disease, Phenotype, medicine.anatomical_structure, biology.protein, lcsh:Q, Female, Kidney Diseases, Energy Metabolism, Research Article, Kidney disease

Abstract

Uromodulin-associated kidney disease (UAKD) summarizes different clinical features of an autosomal dominant heritable disease syndrome in humans with a proven uromodulin (UMOD) mutation involved. It is often characterized by hyperuricemia, gout, alteration of urine concentrating ability, as well as a variable rate of disease progression inconstantly leading to renal failure and histological alterations of the kidneys. We recently established the two Umod mutant mouse lines Umod(C93F) and Umod(A227T) on the C3H inbred genetic background both showing kidney defects analogous to those found in human UAKD patients. In addition, disease symptoms were revealed that were not yet described in other published mouse models of UAKD. To examine if further organ systems and/or metabolic pathways are affected by Umod mutations as primary or secondary effects, we describe a standardized, systemic phenotypic analysis of the two mutant mouse lines Umod(A227T) and Umod(C93F) in the German Mouse Clinic. Different genotypes as well as different ages were tested. Beside the already published changes in body weight, body composition and bone metabolism, the influence of the Umod mutation on energy metabolism was confirmed. Hematological analysis revealed a moderate microcytic and erythropenic anemia in older Umod mutant mice. Data of the other analyses in 7-10 month-old mutant mice showed single small additional effects.

Published

2013