Your search keyword '"Sylke Winkler"' showing total 6 results

1. Low Threshold for Cutaneous Allergen Sensitization but No Spontaneous Dermatitis or Atopy in FLG-Deficient Mice

Author

Rolf Jessberger, Alexander H. Dalpke, Stefan Beissert, Axel Roers, Andreas Dahl, Maria Chapsa, Buqing Yi, Rayk Behrendt, Padraic G. Fallon, Michael Hiller, Sébastien Boutin, Lina Muhandes, Sylke Winkler, Martin Pippel, and Yan Ge

Subjects

0301 basic medicine, Allergy, Dermatology, Filaggrin Proteins, Ichthyosis Vulgaris, Immunoglobulin E, Biochemistry, Dermatitis, Atopic, Atopy, Mice, 03 medical and health sciences, 0302 clinical medicine, Hypersensitivity, Animals, Medicine, Molecular Biology, Sensitization, Skin, Mice, Inbred BALB C, Whole Genome Sequencing, biology, business.industry, Ichthyosis, Microbiota, Cell Biology, Atopic dermatitis, Allergens, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, biology.protein, Female, business, Filaggrin, Ichthyosis vulgaris

Abstract

Loss of FLG causes ichthyosis vulgaris. Reduced FLG expression compromises epidermal barrier function and is associated with atopic dermatitis, allergy, and asthma. The flaky tail mouse harbors two mutations that affect the skin barrier, Flgft, resulting in hypomorphic FLG expression, and Tmem79ma, inactivating TMEM79. Mice defective only for TMEM79 featured dermatitis and systemic atopy, but also Flgft/ft BALB/c congenic mice developed eczema, high IgE, and spontaneous asthma, suggesting that FLG protects from atopy. In contrast, a targeted Flg-knockout mutation backcrossed to BALB/c did not result in dermatitis or atopy. To resolve this discrepancy, we generated FLG-deficient mice on pure BALB/c background by inactivating Flg in BALB/c embryos. These mice feature an ichthyosis phenotype, barrier defect, and facilitated percutaneous sensitization. However, they do not develop dermatitis or atopy. Whole-genome sequencing of the atopic Flgft BALB/c congenics revealed that they were homozygous for the atopy-causing Tmem79matted mutation. In summary, we show that FLG deficiency does not cause atopy in mice, in line with lack of atopic disease in a fraction of patients with ichthyosis vulgaris carrying two Flg null alleles. However, the absence of FLG likely promotes and modulates dermatitis caused by other genetic barrier defects.

Published

2021

2. Mutations affecting liver development and function in Medaka, Oryzias latipes, screened by multiple criteria

Author

Yukihiro Hirose, Akihito Yasuoka, Hiroshi Nishina, Felix Loosli, Hiroshi Suwa, Clemens Grabher, Katsutoshi Niwa, Satoshi Asaka, Hiroki Yoda, Takao Sasado, Kota Saito, Rebecca Quiring, Matthias Carl, Sanae Kunimatsu, Keiko Abe, Daiju Kitagawa, Tomonori Deguchi, Chikako Morinaga, Thorsten Henrich, Masakazu Osakada, Sylke Winkler, Tomomi Watanabe, Ryumei Kurashige, Katsuhito Takahashi, Yousuke Takahama, Hisato Kondoh, Joachim Wittbrodt, Toshiaki Katada, Norimasa Iwanami, Makoto Furutani-Seiki, and Filippo Del Bene

Subjects

Genetics, Mutation, Embryology, Liver morphogenesis, Endoderm, Mutant, Oryzias, Gallbladder, Mutagenesis (molecular biology technique), Biology, Lipid Metabolism, medicine.disease_cause, Phenotype, Complementation, Liver, Endoderm formation, medicine, Animals, Gene, In Situ Hybridization, Body Patterning, Developmental Biology

Abstract

We report here mutations affecting various aspects of liver development and function identified by multiple assays in a systematic mutagenesis screen in Medaka. The 22 identified recessive mutations assigned to 19 complementation groups fell into five phenotypic groups. Group 1, showing defective liver morphogenesis, comprises mutations in four genes, which may be involved in the regulation of growth or patterning of the gut endoderm. Group 2 comprises mutations in three genes that affect the laterality of the liver; in kendama mutants of this group, the laterality of the heart and liver is uncoupled and randomized. Group 3 includes mutations in three genes altering bile color, indicative of defects in hemoglobin-bilirubin metabolism and globin synthesis. Group 4 consists of mutations in three genes, characterized by a decrease in the accumulation of fluorescent metabolite of a phospholipase A(2) substrate, PED6, in the gall bladder. Lipid metabolism or the transport of lipid metabolites may be affected by these mutations. Mutations in Groups 3 and 4 may provide animal models for relevant human diseases. Group 5 mutations in six genes affect the formation of endoderm, endodermal rods and hepatic bud from which the liver develops. These Medaka mutations, identified by morphological and metabolite marker screens, should provide clues to understanding molecular mechanisms underlying formation of a functional liver.

Published

2004

3. Mutations affecting retina development in Medaka

Author

Felix Loosli, Rebecca Quiring, Hiroshi Suwa, Harun Elmasri, Caroline Iquel, Chikako Morinaga, Sanae Kunimatsu, Katsutoshi Niwa, Christoph Winkler, Clemens Grabher, Yukihiro Hirose, Annette Krone, Thorsten Henrich, Filippo Del Bene, Tomonori Deguchi, Beate Wittbrodt, Matthias Carl, Sylke Winkler, Akihito Yasuoka, Takao Sasado, Masakazu Osakada, Juan Ramón Martínez-Morales, Hisato Kondoh, Martina Rembold, Joachim Wittbrodt, Tomomi Watanabe, Makoto Furutani-Seiki, Hiroki Yoda, Norimasa Iwanami, Roche, Japan Science and Technology Agency, Company of Biologists, Boehringer Ingelheim Fonds, Marie Curie Memorial Foundation, German Research Foundation, and European Commission

Subjects

Embryology, genetic structures, Teleost, Mutant, Oryzias, Mutagenesis (molecular biology technique), Genes, Recessive, Biology, Optic cup (anatomical), medicine.disease_cause, Eye, Retina, Optic vesicle formation, medicine, Animals, Genetics, Mutation, Pigmentation, Cell Differentiation, Large scale, Optic vesicle, eye diseases, Medaka, medicine.anatomical_structure, Mutagenesis, sense organs, Neural plate, Developmental Biology

Abstract

12 páginas, 5 figuras, 1 tabla.-- et al., In a large scale mutagenesis screen of Medaka we identified 60 recessive zygotic mutations that affect retina development. Based on the onset and type of phenotypic abnormalities, the mutants were grouped into five categories: the first includes 11 mutants that are affected in neural plate and optic vesicle formation. The second group comprises 15 mutants that are impaired in optic vesicle growth. The third group includes 18 mutants that are affected in optic cup development. The fourth group contains 13 mutants with defects in retinal differentiation. 12 of these have smaller eyes, whereas one mutation results in enlarged eyes. The fifth group consists of three mutants with defects in retinal pigmentation. The collection of mutants will be used to address the molecular genetic mechanisms underlying vertebrate eye formation., This work was supported by the Roche Research Foundation (F.L.) the Japanese Agency for Science and Technology (JST) (R.Q., M.C., S.W.), the Company of Biologists Ltd (F.D.B.), the Boehringer Ingelheim Foundation (C.G.), the Marie Curie Foundation (J-R. M-M.) and through grants from the DFG, EC (J.W) and HFSP (H.K, J.W.).

Published

2004

4. A systematic genome-wide screen for mutations affecting organogenesis in Medaka, Oryzias latipes

Author

Katsutoshi Niwa, Harun Elmasri, Toshiaki Katada, Norimasa Iwanami, Makoto Furutani-Seiki, Yasuko Okamoto, Tomonori Deguchi, Noboru Nakajima, Akihito Yasuoka, Yukihiro Hirose, Yousuke Takahama, Clemens Grabher, Ai Shinomiya, Yasuko Kota, Sanae Kunimatsu, Hisato Kondoh, Hiroshi Mitani, Akihiro Momoi, Tomomi Watanabe, Rebecca Quiring, Katsuhito Takahashi, Hiroshi Nishina, Toshiyuki Yamanaka, Joachim Wittbrodt, Hiroki Yoda, Takeshi Todo, Hiroshi Suwa, Kota Saito, Daiju Kitagawa, Sylke Winkler, Keiko Abe, Chikako Morinaga, Matthias Carl, Satoshi Asaka, Thorsten Henrich, Minoru Tanaka, Filippo Del Bene, Takao Sasado, Masakazu Osakada, Mirana Ramialison, Christoph Winkler, and Felix Loosli

Subjects

Embryology, animal structures, DNA repair, Oryzias, Organogenesis, Mutagenesis (molecular biology technique), Thymus Gland, Eye, Radiation Tolerance, Prosencephalon, Animals, Zebrafish, Gene, Genetics, biology, fungi, biology.organism_classification, Phenotype, Germ cell migration, Germ Cells, Somites, Research Design, embryonic structures, Mutation, Nerve tract, Developmental Biology

Abstract

A large-scale mutagenesis screen was performed in Medaka to identify genes acting in diverse developmental processes. Mutations were identified in homozygous F3 progeny derived from ENU-treated founder males. In addition to the morphological inspection of live embryos, other approaches were used to detect abnormalities in organogenesis and in specific cellular processes, including germ cell migration, nerve tract formation, sensory organ differentiation and DNA repair. Among 2031 embryonic lethal mutations identified, 312 causing defects in organogenesis were selected for further analyses. From these, 126 mutations were characterized genetically and assigned to 105 genes. The similarity of the development of Medaka and zebrafish facilitated the comparison of mutant phenotypes, which indicated that many mutations in Medaka cause unique phenotypes so far unrecorded in zebrafish. Even when mutations of the two fish species cause a similar phenotype such as one-eyed-pinhead or parachute, more genes were found in Medaka than in zebrafish that produced the same phenotype when mutated. These observations suggest that many Medaka mutants represent new genes and, therefore, are important complements to the collection of zebrafish mutants that have proven so valuable for exploring genomic function in development.

Published

2004

5. Genetic dissection of the formation of the forebrain in Medaka, Oryzias latipes

Author

Satoshi Asaka, Chritoph Winkler, Hiroshi Suwa, Chikako Morinaga, Sylke Winkler, Masakazu Osakada, Takao Sasado, Kota Saito, Thorsten Henrich, Akihito Yasuoka, Sanae Kunimatsu, Felix Loosli, Hiroshi Nishina, Rebecca Quiring, Katsutoshi Niwa, Akihiro Momoi, Harun Elmasri, Hiroki Yoda, Yukihiro Hirose, Toshiaki Katada, Norimasa Iwanami, Tomonori Deguchi, Tomomi Watanabe, Matthias Carl, Makoto Furutani-Seiki, Filippo Del Bene, Daiju Kitagawa, Clemens Grabher, Joachim Wittbrodt, and Hisato Kondoh

Subjects

Genetics, Mutation, Embryology, biology, Mutant, Oryzias, medicine.disease_cause, biology.organism_classification, Phenotype, Diencephalon, Prosencephalon, Forebrain, medicine, biology.protein, Animals, Sonic hedgehog, Zebrafish, Gene, Developmental Biology

Abstract

The forebrain, consisting of the telencephalon and diencephalon, is essential for processing sensory information. To genetically dissect formation of the forebrain in vertebrates, we carried out a systematic screen for mutations affecting morphogenesis of the forebrain in Medaka. Thirty-three mutations defining 25 genes affecting the morphological development of the forebrain were grouped into two classes. Class 1 mutants commonly showing a decrease in forebrain size, were further divided into subclasses 1A to 1D. Class 1A mutation (1 gene) caused an early defect evidenced by the lack of bf1 expression, Class 1B mutations (6 genes) patterning defects revealed by the aberrant expression of regional marker genes, Class 1C mutation (1 gene) a defect in a later stage, and Class 1D (3 genes) a midline defect analogous to the zebrafish one-eyed pinhead mutation. Class 2 mutations caused morphological abnormalities in the forebrain without considerably affecting its size, Class 2A mutations (6 genes) caused abnormalities in the development of the ventricle, Class 2B mutations (2 genes) severely affected the anterior commissure, and Class 2C (6 genes) mutations resulted in a unique forebrain morphology. Many of these mutants showed the compromised sonic hedgehog expression in the zona-limitans-intrathalamica (zli), arguing for the importance of this structure as a secondary signaling center. These mutants should provide important clues to the elucidation of the molecular mechanisms underlying forebrain development, and shed new light on phylogenically conserved and divergent functions in the developmental process.

Published

2004

6. Phased full Length SMRT sequencing of HLA-DPB1

Author

Sylke Winkler, Christoph König, Carolin Zweiniger, Irina Boehme, Kathrin Lang, Nicola Gscheidel, Maarten T. Penning, Gerhard Schöfl, Erik H. Rozemuller, Alexander H. Schmidt, Yannick Duport, Sylvia Clausing, and Vinzenz Lange

Subjects

Genetics, HLA-DPB1, Sequence analysis, Immunology, Genotype, Consensus sequence, Immunology and Allergy, Locus (genetics), General Medicine, Biology, Amplicon, Genotyping, Single molecule real time sequencing

Abstract

Aim In contrast to exon-based HLA-typing approaches, whole gene genotyping crucially depends on full-length sequences submitted to the IMGT/HLA Database. Currently, full-length sequences are provided for only 7 out of 520 HLA-DPB1 alleles. Therefore, we developed a fully phased whole-gene sequencing approach for DPB1, to facilitate further exploration of the allelic structure at this locus. Methods Primers were developed flanking the UTR-regions of DPB1 resulting in a 12 kb amplicon. Using a 4-primer approach, secondary primers containing barcodes were combined with the gene-specific primers to obtain barcoded full-gene amplicons in a single amplification step. Amplicons were pooled, purified, and ligated to SMRT bells (i.e. annealing points for sequencing primers) following standard protocols from Pacific Biosciences. Taking advantage of the SMRT chemistry, pools of 48 amplicons were sequenced full length in single runs on a Pacific Biosciences RSII instrument. Demultiplexing was performed using the SMRT portal. Sequence analysis was performed using the NGSengine software (GenDx). Results We analyzed a set of 48 randomly picked samples. With 3 exceptions due to PCR failure, all genotype assignments conformed to standard genotyping results based on exons 2 and 3. Allelic proportions for heterozygous positions were evenly distributed (range 0.4–0.6) for all samples, suggesting unbiased amplifications. Despite the high per-read raw error rates typical for SMRT sequencing ( ∼ 15%) the consensus sequence proved highly reliable. All consensus sequences for exons 2 and 3 were in full accordance with their MiSeq-derived sequences. We describe novel intronic sequence variation of the 7 so far genomically defined alleles, as well as 7 whole-length DPB1 alleles with hitherto unknown intronic regions. One of these alleles (HLA-DPB1∗131:01) is classified as rare. Conclusion Here we present a whole gene amplification and sequencing workflow for DPB1 alleles utilizing single molecule real-time (SMRT) sequencing from Pacific Biosciences. Validation of consensus sequences against known exonic sequences highlights the reliability of this technology. This workflow will facilitate amending the IMGT/HLA Database for DPB1.

Published

2015