Your search keyword '"Frauke Stanke"' showing total 4 results

1. Very mild disease phenotype of congenic Cftr TgH(neoim)Hgu cystic fibrosis mice

Author

Balázs Tóth, Marion Burmester, Frauke Stanke, Gerhard Breves, S. Jansen, Martina Dorsch, Hugo R. de Jonge, Martina Wilke, Nikoletta Charizopoulou, Burkhard Tümmler, Hans-Jürgen Hedrich, Sabine Leonhard-Marek, Dirk Wedekind, Alice G. M. Bot, Public Health, Biochemistry, and Erasmus MC other

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, lcsh:QH426-470, Cystic Fibrosis, Genotype, Genetic Linkage, Mutant, Congenic, Cystic Fibrosis Transmembrane Conductance Regulator, medicine.disease_cause, Cystic fibrosis, Mice, Mice, Congenic, SDG 3 - Good Health and Well-being, Chlorides, Inbred strain, Genetics, medicine, Animals, Mice, Inbred CFTR, Genetics(clinical), Genetics (clinical), Analysis of Variance, Mutation, biology, Body Weight, Colforsin, Wild type, medicine.disease, Cystic fibrosis transmembrane conductance regulator, lcsh:Genetics, Disease Models, Animal, Fertility, Phenotype, biology.protein, Carbachol, Female, Research Article, Microsatellite Repeats

Abstract

Background A major boost to cystic fibrosis disease research was given by the generation of various mouse models using gene targeting in embryonal stem cells. Moreover, the introduction of the same mutation on different inbred strains generating congenic strains facilitated the search for modifier genes. From the original Cftr TgH(neoim)Hgu mouse model with a divergent genetic background (129/Sv, C57BL/6, HsdOla:MF1) two inbred mutant mouse strains CF/1-Cftr TgH(neoim)Hgu and CF/3-Cftr TgH(neoim)Hgu had been generated using strict brother × sister mating. CF/1-Cftr TgH(neoim)Hgu and CF/3-Cftr TgH(neoim)Hgu mice were fertile and showed normal growth and lifespan. In this work the Cftr TgH(neoim)Hgu insertional mutation was backcrossed from CF/3-Cftr TgH(neoim)Hgu onto the inbred backgrounds C57BL/6J and DBA/2J generating congenic animals in order to clarify the differential impact of the Cftr mutation and the genetic background on the disease phenotype of the cystic fibrosis mutant mice. Clinical and electrophysiological features of the two congenic strains were compared with those of CF/1-Cftr TgH(neoim)Hgu and CF/3-Cftr TgH(neoim)Hgu and wild type controls. Results Under the standardized housing conditions of the animal facility, the four mouse strains CF/1-Cftr TgH(neoim)Hgu , CF/3-Cftr TgH(neoim)Hgu , D2.129P2(CF/3)-Cftr TgH(neoim)Hgu and B6.129P2(CF/3)-Cftr TgH(neoim)Hgu exhibited normal life expectancy. Growth of congenic cystic fibrosis mice was comparable with that of wild type controls. All mice but D2.129P2(CF/3)-Cftr TgH(neoim)Hgu females were fertile. Short circuit current measurements revealed characteristic response profiles of the HsdOla:MF1, DBA/2J and C57BL/6J backgrounds in nose, ileum and colon. All cystic fibrosis mouse lines showed the disease-typical hyperresponsiveness to amiloride in the respiratory epithelium. The mean chloride secretory responses to carbachol or forskolin were 15–100% of those of the cognate wild type control animals. Conclusion The amelioration of the clinical features and of the basic defect that had emerged during the generation of CF/3-Cftr TgH(neoim)Hgu mice was retained in the congenic mice indicating that the Cftr linkage group or other loci shared between the inbred strains contain(s) the major modifier(s) of attenuation of cystic fibrosis symptoms.

Published

2008

2. Genetic variants of chemokine receptor CCR7 in patients with systemic lupus erythematosus, Sjogren's syndrome and systemic sclerosis

Author

Daniel Kahlmann, Torsten Witte, Frauke Stanke, Ana Clara Marques Davalos-Misslitz, Reinhold Förster, and Lars Ohl

Subjects

Male, Untranslated region, Silent mutation, Receptors, CCR7, lcsh:QH426-470, Molecular Sequence Data, C-C chemokine receptor type 7, Single-nucleotide polymorphism, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Autoimmunity, Exon, Immune system, Gene Frequency, Genes, Reporter, Germany, Genetics, medicine, Humans, Lupus Erythematosus, Systemic, Genetic Predisposition to Disease, Genetics(clinical), Genetic Testing, Luciferases, Genetics (clinical), DNA Primers, Autoimmune disease, Scleroderma, Systemic, Base Sequence, Sequence Analysis, DNA, medicine.disease, Molecular biology, lcsh:Genetics, Sjogren's Syndrome, Immunology, Female, Research Article

Abstract

Background The chemokine receptor CCR7 is a key organizer of the immune system. Gene targeting in mice revealed that Ccr7-deficient animals are severely impaired in the induction of central and peripheral tolerance. Due to these defects, Ccr7-deficient mice spontaneously develop multi-organ autoimmunity showing symptoms similar to those observed in humans suffering from connective tissue autoimmune diseases. However, it is unknown whether mutations of CCR7 are linked to autoimmunity in humans. Results DNA samples were collected from 160 patients suffering from connective tissue autoimmune disease (Sjogren's syndrome, n = 40; systemic lupus erythematosus, SLE, n = 20 and systemic sclerosis, n = 100) and 40 health subjects (n = 40). All participants in this study were of German descent. Samples were screened for single nucleotide polymorphisms (SNP) by sequencing the coding region of the CCR7 gene as well asthe exon flaking intron sites and parts of the regions encoding for the 5'- and 3'-UTR. CCR7 variants were rare. We identified six different sequence variants, which occurred in heterozygosis. The identified SNP were observed at position -60 C/T (observed 1x), +6,476 A/G (7x), +6,555 C/T (15x), +6,560 C/T (6x), +10,440 A/G (3x) and +11,475 C/A (1x). Four of these variants (+6,476 A/G, +6,555 C/T, +6,560 C/T and +10,440 A/G) display allelic frequencies between 1% and 5 % and were present in both patients and control groups. The variants +6,476 A/G, +6,555 C/T, +6,560 C/T are located in the intron 2, while the +10,440 A/G variant corresponds to a silent mutation in exon 3. The variants -60 C/T and +11,475 C/A which are located at the 5'-UTR and 3-UTR respectively, display allelic frequencies below 1%. No correlation between these variants and the autoimmune diseases investigated could be observed. However, reporter gene expression assay demonstrated that the mutation at the -60 C/T position in homozygosis leads to reduced luciferase activity. Conclusion These results suggest that variants of CCR7 gene occur at an extremely low frequency in the German population and that neither Sjogren's syndrome, systemic lupus erythematosus, nor systemic sclerosis are associated with these variants. Nevertheless, the decreased luciferase activity observed in cells transfected with the promoter region bearing the -60 C/T mutation suggests that this CCR7 variant could potentially lead to increased susceptibility to autoimmunity.

Published

2007

3. Spontaneous rescue from cystic fibrosis in a mouse model

Author

Martina Wilke, Hans J. Hedrich, S. Jansen, Hugo R. de Jonge, Burkhard Tümmler, Huub Jorna, Frauke Stanke, Nikoletta Charizopoulou, Martina Dorsch, Alice G. M. Bot, Biochemistry, Developmental Biology, and Erasmus MC other

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Cystic Fibrosis, Genotype, lcsh:QH426-470, RNA Splicing, Cystic Fibrosis Transmembrane Conductance Regulator, Respiratory Mucosa, Cystic fibrosis, Mice, Chlorides, Intestinal mucosa, Inbred strain, Genetics, medicine, Animals, Mice, Inbred CFTR, RNA, Messenger, Intestinal Mucosa, Respiratory system, Genetics (clinical), biology, Electric Conductivity, Wild type, Genomics, respiratory system, medicine.disease, Immunohistochemistry, Phenotype, Molecular biology, Mice, Mutant Strains, Cystic fibrosis transmembrane conductance regulator, Disease Models, Animal, lcsh:Genetics, biology.protein, Female, Microsatellite Repeats, Research Article

Abstract

Background From the original Cftr TgH(neoim)Hgu mutant mouse model with a divergent genetic background (129P2, C57BL/6, MF1) we have generated two inbred Cftr TgH(neoim)Hgu mutant strains named CF/1-Cftr TgH(neoim)Hgu and CF/3-Cftr TgH(neoim)Hgu , which are fertile and show normal growth and lifespan. Initial genome wide scan analysis with microsatellite markers indicated that the two inbred strains differed on the genetic level. In order to further investigate whether these genetic differences have an impact on the disease phenotype of cystic fibrosis we characterised the phenotype of the two inbred strains. Results Reduced amounts, compared to wild type control animals, of correctly spliced Cftr mRNA were detected in the nasal epithelia, lungs and the intestine of both inbred Cftr TgH(neoim)Hgu strains, with higher residual amount observed for CF/1-Cftr TgH(neoim)Hgu than CF/3-Cftr TgH(neoim)Hgu for every investigated tissue. Accordingly the amounts of wild type Cftr protein in the intestine were 9% for CF/1-Cftr TgH(neoim)Hgu and 4% for CF/3-Cftr TgH(neoim)Hgu . Unlike the apparent strain and/or tissue specific regulation of Cftr mRNA splicing, short circuit current measurements in the respiratory and intestinal epithelium revealed that both strains have ameliorated the basic defect of cystic fibrosis with a presentation of a normal electrophysiology in both tissues. Conclusion Unlike the outbred Cftr TgH(neoim)Hgu insertional mouse model, which displayed the electrophysiological defect in the gastrointestinal and respiratory tracts characteristic of cystic fibrosis, both inbred Cftr TgH(neoim)Hgu strains have ameliorated the electrophysiological defect. On the basis of these findings both CF/1-Cftr TgH(neoim)Hgu and CF/3-Cftr TgH(neoim)Hgu offer an excellent model whereby determination of the minimal levels of protein required for the restoration of the basic defect of cystic fibrosis can be studied, along with the modulating factors which may affect this outcome.

Published

2006

4. [Untitled]

Author

Martina Dorsch, Nikoletta Charizopoulou, Hans-Jürgen Hedrich, Frauke Stanke, S. Jansen, Burkhard Tümmler, and Julia R. Dorin

Subjects

Genetics, Germline mutation, Inbred strain, Haplotype, Mutant, Congenic, Microsatellite, Locus (genetics), Biology, Molecular biology, Genetics (clinical), Germline

Abstract

A major boost to the cystic fibrosis disease research was given by the generation of various mouse models using gene targeting in embryonal stem cells. Moreover, the introduction of the same mutation on different inbred strains generating congenic strains facilitated the search for modifier genes. From the original CftrTgH(neoim)HguCF mouse model we have generated using strict brother × sister mating two inbred CftrTgH(neoim)Hgumouse lines (CF/1 and CF/3). Thereafter, the insertional mutation was introgressed from CF/3 into three inbred backgrounds (C57BL/6, BALB/c, DBA/2J) generating congenic animals. In every backcross cycle germline transmission of the insertional mutation was monitored by direct probing the insertion via Southern RFLP. In order to bypass this time consuming procedure we devised an alternative PCR based protocol whereby mouse strains are differentiated at the Cftr locus by Cftr intragenic microsatellite genotypes that are tightly linked to the disrupted locus. Using this method we were able to identify animals carrying the insertional mutation based upon the differential haplotypic backgrounds of the three inbred strains and the mutant CftrTgH(neoim)Hguat the Cftr locus. Moreover, this method facilitated the identification of the precise vector excision from the disrupted Cftr locus in two out of 57 typed animals. This reversion to wild type status took place without any loss of sequence revealing the instability of insertional mutations during the production of congenic animals. We present intragenic microsatellite markers as a tool for fast and efficient identification of the introgressed locus of interest in the recipient strain during congenic animal breeding. Moreover, the same genotyping method allowed the identification of a vector excision event, posing questions on the stability of insertional mutations in mice.

Published

2004