Your search keyword '"Thomas Floss"' showing total 29 results

1. Sphingomyelin Synthase 1 Is Essential for Male Fertility in Mice.

Author

Anke Wittmann, Marcus O W Grimm, Harry Scherthan, Marion Horsch, Johannes Beckers, Helmut Fuchs, Valerie Gailus-Durner, Martin Hrabě de Angelis, Steven J Ford, Neal C Burton, Daniel Razansky, Dietrich Trümbach, Michaela Aichler, Axel Karl Walch, Julia Calzada-Wack, Frauke Neff, Wolfgang Wurst, Tobias Hartmann, and Thomas Floss

Subjects

Medicine, Science

Abstract

Sphingolipids and the derived gangliosides have critical functions in spermatogenesis, thus mutations in genes involved in sphingolipid biogenesis are often associated with male infertility. We have generated a transgenic mouse line carrying an insertion in the sphingomyelin synthase gene Sms1, the enzyme which generates sphingomyelin species in the Golgi apparatus. We describe the spermatogenesis defect of Sms1-/- mice, which is characterized by sloughing of spermatocytes and spermatids, causing progressive infertility of male homozygotes. Lipid profiling revealed a reduction in several long chain unsaturated phosphatidylcholins, lysophosphatidylcholins and sphingolipids in the testes of mutants. Multi-Spectral Optoacoustic Tomography indicated blood-testis barrier dysfunction. A supplementary diet of the essential omega-3 docosahexaenoic acid and eicosapentaenoic acid diminished germ cell sloughing from the seminiferous epithelium and restored spermatogenesis and fertility in 50% of previously infertile mutants. Our findings indicate that SMS1 has a wider than anticipated role in testis polyunsaturated fatty acid homeostasis and for male fertility.

Published

2016

2. The REST remodeling complex protects genomic integrity during embryonic neurogenesis

Author

Tamilla Nechiporuk, James McGann, Karin Mullendorff, Jenny Hsieh, Wolfgang Wurst, Thomas Floss, and Gail Mandel

Subjects

transcription factor, repression, genomic instability, neurogenesis, REST complex, knockout animal, Medicine, Science, Biology (General), QH301-705.5

Abstract

The timely transition from neural progenitor to post-mitotic neuron requires down-regulation and loss of the neuronal transcriptional repressor, REST. Here, we have used mice containing a gene trap in the Rest gene, eliminating transcription from all coding exons, to remove REST prematurely from neural progenitors. We find that catastrophic DNA damage occurs during S-phase of the cell cycle, with long-term consequences including abnormal chromosome separation, apoptosis, and smaller brains. Persistent effects are evident by latent appearance of proneural glioblastoma in adult mice deleted additionally for the tumor suppressor p53 protein (p53). A previous line of mice deleted for REST in progenitors by conventional gene targeting does not exhibit these phenotypes, likely due to a remaining C-terminal peptide that still binds chromatin and recruits co-repressors. Our results suggest that REST-mediated chromatin remodeling is required in neural progenitors for proper S-phase dynamics, as part of its well-established role in repressing neuronal genes until terminal differentiation.

Published

2016

3. MTO1-deficient mouse model mirrors the human phenotype showing complex I defect and cardiomyopathy.

Author

Lore Becker, Eva Kling, Evelyn Schiller, Ramona Zeh, Anja Schrewe, Sabine M Hölter, Ilona Mossbrugger, Julia Calzada-Wack, Valentina Strecker, Ilka Wittig, Iulia Dumitru, Tina Wenz, Andreas Bender, Michaela Aichler, Dirk Janik, Frauke Neff, Axel Walch, Leticia Quintanilla-Fend, Thomas Floss, Raffi Bekeredjian, Valérie Gailus-Durner, Helmut Fuchs, Wolfgang Wurst, Thomas Meitinger, Holger Prokisch, Martin Hrabě de Angelis, and Thomas Klopstock

Subjects

Medicine, Science

Abstract

Recently, mutations in the mitochondrial translation optimization factor 1 gene (MTO1) were identified as causative in children with hypertrophic cardiomyopathy, lactic acidosis and respiratory chain defect. Here, we describe an MTO1-deficient mouse model generated by gene trap mutagenesis that mirrors the human phenotype remarkably well. As in patients, the most prominent signs and symptoms were cardiovascular and included bradycardia and cardiomyopathy. In addition, the mutant mice showed a marked worsening of arrhythmias during induction and reversal of anaesthesia. The detailed morphological and biochemical workup of murine hearts indicated that the myocardial damage was due to complex I deficiency and mitochondrial dysfunction. In contrast, neurological examination was largely normal in Mto1-deficient mice. A translational consequence of this mouse model may be to caution against anaesthesia-related cardiac arrhythmias which may be fatal in patients.

Published

2014

4. HIV-1 replication in human immune cells is independent of TAR DNA binding protein 43 (TDP-43) expression.

Author

Julia Nehls, Herwig Koppensteiner, Ruth Brack-Werner, Thomas Floss, and Michael Schindler

Subjects

Medicine, Science

Abstract

The TAR DNA binding protein (TDP-43) was originally identified as a host cell factor binding to the HIV-1 LTR and thereby suppressing HIV-1 transcription and gene expression (Ou et al., J.Virol. 1995, 69(6):3584). TDP-43 is a global regulator of transcription, can influence RNA metabolism in many different ways and is ubiquitously expressed. Thus, TDP-43 could be a major factor restricting HIV-1 replication at the level of LTR transcription and gene expression. These facts prompted us to revisit the role of TDP-43 for HIV-1 replication. We utilized established HIV-1 cell culture systems as well as primary cell models and performed a comprehensive analysis of TDP-43 function and investigated its putative impact on HIV-1 gene expression. In HIV-1 infected cells TDP-43 was neither degraded nor sequestered from the nucleus. Furthermore, TDP-43 overexpression as well as siRNA mediated knockdown did not affect HIV-1 gene expression and virus production in T cells and macrophages. In summary, our experiments argue against a restricting role of TDP-43 during HIV-1 replication in immune cells.

Published

2014

5. REST/NRSF deficiency impairs autophagy and leads to cellular senescence in neurons

Author

Fabio Benfenati, Thomas Floss, Jagoda Aleksandra Kowalska, Anna Rocchi, Emanuele Carminati, and Antonio De Fusco

Subjects

Senescence, Aging, Programmed cell death, autophagy, Autophagy, Mitochondria, Neurons, Oxidative Stress, Rapamycin, Rest/nrsf, Trehalose, senescence, mitochondria, neurons, oxidative stress, rapamycin, REST/NRSF, trehalose, Animals, Cellular Senescence, Humans, Mice, Repressor Proteins, Biology, Mitochondrion, medicine.disease_cause, medicine, Transcription factor, Original Paper, Cell Biology, Original Papers, Cell biology, Proteostasis, Physiological Aging, Oxidative stress

Abstract

During aging, brain performances decline. Cellular senescence is one of the aging drivers and a key feature of a variety of human age‐related disorders. The transcriptional repressor RE1‐silencing transcription factor (REST) has been associated with aging and higher risk of neurodegenerative disorders. However, how REST contributes to the senescence program and functional impairment remains largely unknown. Here, we report that REST is essential to prevent the senescence phenotype in primary mouse neurons. REST deficiency causes failure of autophagy and loss of proteostasis, increased oxidative stress, and higher rate of cell death. Re‐establishment of autophagy reverses the main hallmarks of senescence. Our data indicate that REST has a protective role in physiological aging by regulating the autophagic flux and the senescence program in neurons, with implications for neurological disorders associated with aging., Cellular senescence is one of the aging drivers and a key feature of a variety of human age‐related disorders. The transcriptional repressor REST deficiency leads to cellular senescence in primary neurons. Rest depletion causes DNA damage, impairment of autophagic flux, mitochondrial dysfunction, and alteration of SASP genes expression. We describe a novel transcriptional regulator of the senescence program.

Published

2021

6. Neuroinflammation induces synaptic scaling through IL-1β-mediated activation of the transcriptional repressor REST/NRSF

Author

Matteo Moschetta, Fabrizia Cesca, Martina Albini, Thomas Floss, Fabio Benfenati, Anna Rocchi, Federico Carlini, Valentina Petrosino, Antonio Uccelli, Nicole Kerlero de Rosbo, Federica Buffolo, Buffolo, F., Petrosino, V., Albini, M., Moschetta, M., Carlini, F., Floss, T., Kerlero de Rosbo, N., Cesca, F., Rocchi, A., Uccelli, A., and Benfenati, F.

Subjects

0301 basic medicine, Cancer Research, T-Lymphocytes, Interleukin-1beta, Inbred C57BL, Synaptic Transmission, Synapse, Mice, 0302 clinical medicine, Conditioned, Neuroinflammation, Cerebral Cortex, Neurons, Synaptic scaling, Microglia, lcsh:Cytology, Chemistry, RE1-silencing transcription factor (REST), experimental autoimmune encephalomyelitis (EAE), Wnt signaling, IL-1β, Neurogenesis, Up-Regulation, Cell biology, medicine.anatomical_structure, Excitatory postsynaptic potential, Cytokines, Immunology, Neurotransmission, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, Downregulation and upregulation, medicine, Animals, lcsh:QH573-671, Inflammation, Cell Biology, Cellular neuroscience, Coculture Techniques, Culture Media, Conditioned, Mice, Inbred C57BL, Repressor Proteins, Culture Media, 030104 developmental biology, 030217 neurology & neurosurgery

Abstract

Neuroinflammation is associated with synapse dysfunction and cognitive decline in patients and animal models. One candidate for translating the inflammatory stress into structural and functional changes in neural networks is the transcriptional repressor RE1-silencing transcription factor (REST) that regulates the expression of a wide cluster of neuron-specific genes during neurogenesis and in mature neurons. To study the cellular and molecular pathways activated under inflammatory conditions mimicking the experimental autoimmune encephalomyelitis (EAE) environment, we analyzed REST activity in neuroblastoma cells and mouse cortical neurons treated with activated T cell or microglia supernatant and distinct pro-inflammatory cytokines. We found that REST is activated by a variety of neuroinflammatory stimuli in both neuroblastoma cells and primary neurons, indicating that a vast transcriptional change is triggered during neuroinflammation. While a dual activation of REST and its dominant-negative splicing isoform REST4 was observed in N2a neuroblastoma cells, primary neurons responded with a pure full-length REST upregulation in the absence of changes in REST4 expression. In both cases, REST upregulation was associated with activation of Wnt signaling and increased nuclear translocation of β-catenin, a well-known intracellular transduction pathway in neuroinflammation. Among single cytokines, IL-1β caused a potent and prompt increase in REST transcription and translation in neurons, which promoted a delayed and strong synaptic downscaling specific for excitatory synapses, with decreased frequency and amplitude of spontaneous synaptic currents, decreased density of excitatory synaptic connections, and decreased frequency of action potential-evoked Ca2+ transients. Most important, the IL-1β effects on excitatory transmission were strictly REST dependent, as conditional deletion of REST completely occluded the effects of IL-1β activation on synaptic transmission and network excitability. Our results demonstrate that REST upregulation represents a new pathogenic mechanism for the synaptic dysfunctions observed under neuroinflammatory conditions and identify the REST pathway as therapeutic target for EAE and, potentially, for multiple sclerosis.

Published

2021

7. Cytosolic Hsp90α and its mitochondrial isoform Trap1 are differentially required in a breast cancer model

Author

Thomas Floss, Evangelia Vartholomaiou, Didier Picard, Marta Madon-Simon, Guillaume Muhlebach, Wolfgang Wurst, and Stéphane Hagmann

Subjects

0301 basic medicine, Mitochondrion, medicine.disease_cause, Metastasis, Mice, Cytosol, chaperone, Protein Isoforms, Trap1, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), Mice, Knockout, Mammary tumor, biology, metabolism [HSP90 Heat-Shock Proteins], TRAP-1 protein, mouse, Hsp90, Immunohistochemistry, Cell Transformation, Neoplastic, Breast Cancer, Mouse Model, Oncology, Female, Hspca protein, mouse, mouse model, Immunoblotting, Breast Neoplasms, News, pathology [Breast Neoplasms], 03 medical and health sciences, Breast cancer, breast cancer, ddc:570, medicine, Animals, metastasis, ddc:610, HSP90 Heat-Shock Proteins, metabolism [Breast Neoplasms], Oncogene, Cancer, medicine.disease, Disease Models, Animal, 030104 developmental biology, Immunology, biology.protein, Cancer research, tumor metabolism, metabolism [Cytosol], Carcinogenesis, Priority Research Paper

Abstract

// Evangelia Vartholomaiou 1,* , Marta Madon-Simon 1,* , Stephane Hagmann 1 , Guillaume Muhlebach 1 , Wolfgang Wurst 2,3,4,5 , Thomas Floss 2 and Didier Picard 1 1 Departement de Biologie Cellulaire, Universite de Geneve, Sciences III, Geneve, Switzerland 2 Helmholtz Zentrum Munchen, Deutsches Forschungszentrum fur Gesundheit und Umwelt, Neuherberg, Germany 3 Deutsches Zentrum fur Neurodegenerative Erkrankungen e. V., Munchen, Germany 4 Munich Cluster for Systems Neurology, Munchen, Germany 5 Technische Universitat Munchen-Weihenstephan, Neuherberg, Germany * These authors have contributed equally to this work Correspondence: Didier Picard, email: // Keywords : Hsp90; Trap1; breast cancer; metastasis; mouse model Received : January 12, 2017 Accepted : February 15, 2017 Published : February 23, 2017 Abstract The Hsp90 family of molecular chaperones includes the cytosolic isoforms Hsp90α and Hsp90β, and the mitochondrial isoform Trap1. Hsp90α/β support a large number of client proteins in the cytoplasm and the nucleus whereas Trap1 regulates oxidative phosphorylation in mitochondria. Many of the associated proteins and cellular processes are relevant to cancer, and there is ample pharmacological and genetic evidence to support the idea that Hsp90α/β and Trap1 are required for tumorigenesis. However, a direct and comparative genetic test in a mouse cancer model has not been done. Here we report the effects of deleting the Hsp90α or Trap1 genes in a mouse model of breast cancer. Neither Hsp90α nor Trap1 are absolutely required for mammary tumor initiation, growth and metastasis induced by the polyoma middle T-antigen as oncogene. However, they do modulate growth and lung metastasis in vivo and cell proliferation, migration and invasion of isolated primary carcinoma cells in vitro . Without Hsp90α, tumor burden and metastasis are reduced, correlating with impaired proliferation, migration and invasion of cells in culture. Without Trap1, the appearance of tumors is initially delayed, and isolated cells are affected similarly to those without Hsp90α. Analysis of expression data of human breast cancers supports the conclusion that this is a valid mouse model highlighting the importance of these molecular chaperones.

Published

2017

8. Buchrezension zu: Gartenvögel rund ums Jahr

Author

Thomas Floss

Subjects

business.industry, Pharmacology toxicology, Library science, Medicine, business, Molecular Biology, Biotechnology

Published

2020

9. Sall1, Sall2, and Sall4 Are Required for Neural Tube Closure in Mice

Author

Anja Buck, Uta Matysiak-Scholze, Francisco J. Barrionuevo, Walter J. Schulz-Schaeffer, Wiktor Borozdin, Jürgen Kohlhase, Ashraf U. Mannan, Wolfgang Wurst, Thomas Floss, Ibrahim M. Adham, and Johann Böhm

Subjects

Neural Tube, Mutant, Apoptosis, Biology, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, 0302 clinical medicine, SALL4, SALL1, medicine, Animals, Neural Tube Defects, Neurulation, 030304 developmental biology, Genetics, 0303 health sciences, Skull, Neurogenesis, Intracellular Signaling Peptides and Proteins, Neural tube, Gene Expression Regulation, Developmental, Gene targeting, Embryo, Mammalian, eye diseases, 3. Good health, Cell biology, DNA-Binding Proteins, medicine.anatomical_structure, Neural Crest, Gene Targeting, Mutation, Homeotic gene, 030217 neurology & neurosurgery, Transcription Factors, Regular Articles

Abstract

Four homologs to the Drosophila homeotic gene spalt (sal) exist in both humans and mice (SALL1 to SALL4/Sall1 to Sall4, respectively). Mutations in both SALL1 and SALL4 result in the autosomal-dominant developmental disorders Townes-Brocks and Okihiro syndrome, respectively. In contrast, no human diseases have been associated with SALL2 to date, and Sall2-deficient mice have shown no apparent abnormal phenotype. We generated mice deficient in Sall2 and, contrary to previous reports, 11% of our Sall2-deficient mice showed background-specific neural tube defects, suggesting that Sall2 has a role in neurogenesis. To investigate whether Sall4 may compensate for the absence of Sall2, we generated compound Sall2 knockout/Sall4 genetrap mutant mice. In these mutants, the incidence of neural tube defects was significantly increased. Furthermore, we found a similar phenotype in compound Sall1/4 mutant mice, and in vitro studies showed that SALL1, SALL2, and SALL4 all co-localized in the nucleus. We therefore suggest a fundamental and redundant function of the Sall proteins in murine neurulation, with the heterozygous loss of a particular SALL protein also possibly compensated in humans during development.

Published

2008

10. Sall4 isoforms act during proximal-distal and anterior-posterior axis formation in the mouse embryo

Author

Martin Hrabé de Angelis, Ralf Kühn, Wolfgang Wurst, Jürgen Kohlhase, Thomas Floss, Heiko Lickert, and Nikolas Uez

Subjects

Transcription, Genetic, Ectoderm, Bone Morphogenetic Protein 4, Biology, Cell Line, Substrate Specificity, Mice, Endocrinology, Genetics, medicine, Animals, Humans, Protein Isoforms, Axis elongation, Wnt signaling pathway, Gene Expression Regulation, Developmental, Anterior Posterior Axis, Exons, Cell Biology, Embryo, Mammalian, eye diseases, Cell biology, DNA-Binding Proteins, Gastrulation, medicine.anatomical_structure, Epiblast, embryonic structures, Endoderm, NODAL, Transcription Factors

Abstract

Reciprocal signals from embryonic and extra-embryonic tissues pattern the embryo in proximal-distal (PD) and anterior-posterior (AP) fashion. Here we have analyzed three gene trap mutations of Sall4, of which one (Sall4-1a) led to a hypomorphic and recessive phenotype, demonstrating that Sall4-1a has yet undescribed extra-embryonic and embryonic functions in regulating PD and AP axis formation. In Sall4-1a mutants the self-maintaining autoregulatory interaction between Bmp4, Nodal and Wnt, which determines the PD axis was disrupted because of defects in the extra-embryonic visceral endoderm. More severely, two distinct Sall4 gene-trap mutants (Sall4-1a,b), resembling null mutants, failed to initiate Bmp4 expression in the extra-embryonic ectoderm and Nodal in the epiblast and were therefore unable to initiate PD axis formation. Tetraploid rescue underlined the extra-embryonic nature of the Sall4-1a phenotype and revealed a further embryonic function in Wnt/beta-catenin signaling to elongate the AP axis during gastrulation. This observation was supported through genetic interaction with beta-catenin mutants, since compound heterozygous mutants recapitulated the defects of Wnt3a mutants in posterior development.

Published

2008

11. The REST remodeling complex protects genomic integrity during embryonic neurogenesis

Author

Thomas Floss, Karin Mullendorff, Wolfgang Wurst, Jenny Hsieh, James C. McGann, Tamilla Nechiporuk, and Gail Mandel

Subjects

0301 basic medicine, REST complex, QH301-705.5, Science, Neurogenesis, Cellular differentiation, knockout animal, Biology, General Biochemistry, Genetics and Molecular Biology, Chromatin remodeling, Mice, 03 medical and health sciences, embryology [Brain], physiology [Stem Cells], Animals, Biology (General), Chromosome separation, Transcription factor, transcription factor, metabolism [Repressor Proteins], Rest Complex, Developmental Biology, Genomic Instability, Knockout Animals, Mouse, Repression, Stem Cells, Transcription Factors, General Immunology and Microbiology, General Neuroscience, Cell Cycle, Gene targeting, Cell Differentiation, General Medicine, Cell cycle, genomic instability, physiology [Neurons], RE1-silencing transcription factor, Molecular biology, Chromatin, Cell biology, Repressor Proteins, neurogenesis, 030104 developmental biology, Gene Knockdown Techniques, Medicine, repression, ddc:600

Abstract

The timely transition from neural progenitor to post-mitotic neuron requires down-regulation and loss of the neuronal transcriptional repressor, REST. Here, we have used mice containing a gene trap in the Rest gene, eliminating transcription from all coding exons, to remove REST prematurely from neural progenitors. We find that catastrophic DNA damage occurs during S-phase of the cell cycle, with long-term consequences including abnormal chromosome separation, apoptosis, and smaller brains. Persistent effects are evident by latent appearance of proneural glioblastoma in adult mice deleted additionally for the tumor suppressor p53 protein (p53). A previous line of mice deleted for REST in progenitors by conventional gene targeting does not exhibit these phenotypes, likely due to a remaining C-terminal peptide that still binds chromatin and recruits co-repressors. Our results suggest that REST-mediated chromatin remodeling is required in neural progenitors for proper S-phase dynamics, as part of its well-established role in repressing neuronal genes until terminal differentiation.

Published

2016

12. Sphingomyelin Synthase 1 Is Essential for Male Fertility in Mice

Author

Neal C. Burton, Martin Hrabé de Angelis, Tobias Hartmann, Julia Calzada-Wack, Axel Walch, Marion Horsch, Daniel Razansky, Wolfgang Wurst, Frauke Neff, Anke Wittmann, Johannes Beckers, Harry Scherthan, Marcus O. W. Grimm, Dietrich Trümbach, Michaela Aichler, Helmut Fuchs, Steven J. Ford, Valerie Gailus-Durner, and Thomas Floss

Subjects

0301 basic medicine, Male, Aging, Physiology, lcsh:Medicine, Transferases (Other Substituted Phosphate Groups), Apoptosis, Male infertility, Mice, 0302 clinical medicine, Animal Cells, Reproductive Physiology, Testis, biosynthesis [Fatty Acids, Omega-3], Medicine and Health Sciences, drug effects [Fertility], Testes, Cell Cycle and Cell Division, lcsh:Science, Promoter Regions, Genetic, Epididymis, Multidisciplinary, biology, Cell Death, Chromosome Biology, drug effects [Lipid Metabolism], physiology [Aging], Eicosapentaenoic acid, Spermatids, ddc, Cell biology, drug effects [Spermatogenesis], sphingomyelin synthase 1, mouse, pharmacology [Fatty Acids, Omega-3], Meiosis, medicine.anatomical_structure, Docosahexaenoic acid, Cell Processes, Anatomy, Cellular Types, drug effects [Epididymis], Sphingomyelin, Genital Anatomy, Germ cell, Research Article, medicine.medical_specialty, Urology, Research and Analysis Methods, metabolism [Epididymis], 03 medical and health sciences, Internal medicine, Sphingomyelin synthase, Fatty Acids, Omega-3, medicine, Male Infertility, Animals, ddc:610, Spermatogenesis, Immunohistochemistry Techniques, drug effects [Testis], Infertility, Male, Nutrition, lcsh:R, Reproductive System, Biology and Life Sciences, Cell Biology, medicine.disease, Lipid Metabolism, Sphingolipid, enzymology [Infertility, Male], Sperm, Diet, Histochemistry and Cytochemistry Techniques, metabolism [Transferases (Other Substituted Phosphate Groups)], Alternative Splicing, Mutagenesis, Insertional, 030104 developmental biology, Endocrinology, Fertility, Germ Cells, Infertility, genetics [Promoter Regions, Genetic], biology.protein, Immunologic Techniques, lcsh:Q, metabolism [Testis], genetics [Transferases (Other Substituted Phosphate Groups)], 030217 neurology & neurosurgery

Abstract

Sphingolipids and the derived gangliosides have critical functions in spermatogenesis, thus mutations in genes involved in sphingolipid biogenesis are often associated with male infertility. We have generated a transgenic mouse line carrying an insertion in the sphingomyelin synthase gene Sms1, the enzyme which generates sphingomyelin species in the Golgi apparatus. We describe the spermatogenesis defect of Sms1-/- mice, which is characterized by sloughing of spermatocytes and spermatids, causing progressive infertility of male homozygotes. Lipid profiling revealed a reduction in several long chain unsaturated phosphatidylcholins, lysophosphatidylcholins and sphingolipids in the testes of mutants. Multi-Spectral Optoacoustic Tomography indicated blood-testis barrier dysfunction. A supplementary diet of the essential omega-3 docosahexaenoic acid and eicosapentaenoic acid diminished germ cell sloughing from the seminiferous epithelium and restored spermatogenesis and fertility in 50% of previously infertile mutants. Our findings indicate that SMS1 has a wider than anticipated role in testis polyunsaturated fatty acid homeostasis and for male fertility.

Published

2016

13. The Hsp90 Cochaperone p23 Is Essential for Perinatal Survival

Author

Thomas Floss, Iwona Grad, Didier Picard, Sara M. Ludwig, Charles A. Miller, Wolfgang Wurst, Gary W. Hoyle, Patricia Ruiz, and Thomas Alexander Mckee

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, Morphogenesis, ddc:616.07, Phosphoproteins/genetics/physiology, Mice, Receptors, Glucocorticoid, ddc:570, medicine, Animals, HSP90 Heat-Shock Proteins, skin and connective tissue diseases, Lung, Molecular Biology, Gene, Prostaglandin-E Synthases, Skin, Cell Line, Transformed, Fibroblasts/metabolism, Mice, Knockout, biology, Articles, Cell Biology, Fibroblasts, Phosphoproteins, Cell Transformation, Viral, Molecular Chaperones/genetics/physiology, Molecular biology, Hsp90, Mice, Mutant Strains, Yeast, In vitro, Cell biology, Intramolecular Oxidoreductases, Mutagenesis, Insertional, Animals, Newborn, Cell culture, Chaperone (protein), Lung/embryology/ultrastructure, biology.protein, HSP90 Heat-Shock Proteins/metabolism/physiology, Gene Deletion, Receptors, Glucocorticoid/analysis, Skin/embryology/ultrastructure, Glucocorticoid, Molecular Chaperones, medicine.drug

Abstract

The functions of molecular chaperones have been extensively investigated biochemically in vitro and genetically in bacteria and yeast. We have embarked on a functional genomic analysis of the Hsp90 chaperone machine in the mouse by disrupting the p23 gene using a gene trap approach. p23 is an Hsp90 cochaperone that is thought to stabilize Hsp90-substrate complexes and, independently, to act as the cytosolic prostaglandin E2 synthase. Gene deletions in budding and fission yeasts and knock-down experiments with the worm have not revealed any clear in vivo requirements for p23. We find that p23 is not essential for overall prenatal development and morphogenesis of the mouse, which parallels the observation that it is dispensable for proliferation in yeast. In contrast, p23 is absolutely necessary for perinatal survival. Apart from an incompletely formed skin barrier, the lungs of p23 null embryos display underdeveloped airspaces and substantially reduced expression of surfactant genes. Correlating with the known function of glucocorticoids in promoting lung maturation and the role of p23 in the assembly of a hormone-responsive glucocorticoid receptor-Hsp90 complex, p23 null fibroblast cells have a defective glucocorticoid response. Thus, p23 contributes a nonredundant, temporally restricted, and tissue-specific function during mouse development.

Published

2006

14. Expression of neurochondrin in the developing and adult mouse brain

Author

Thomas Floss, D. M. Vogt Weisenhorn, Wolfgang Wurst, and R. Istvánffy

Subjects

Inferior colliculus, Medial geniculate nucleus, animal structures, Cerebrum, Brain, Gene Expression, Nerve Tissue Proteins, Hindbrain, Anatomy, Biology, Midbrain, Mice, medicine.anatomical_structure, nervous system, Piriform cortex, embryonic structures, Forebrain, Genetics, medicine, Animals, RNA, Messenger, Neurochondrin, reproductive and urinary physiology, Developmental Biology

Abstract

Here we describe a detailed analysis of the expression of neurochondrin ( ncdn) in the developing and adult mouse brain. Ncdn is first expressed in the hindbrain and spinal cord at embryonic day 10.5 (E10.5) followed by expression in the midbrain at E11.5. By E18 ncdn is also expressed in the diencephalon and telencephalon. However, strongest expression is still observed in the hindbrain. In adults, the expression in the forebrain is as strong as in the hindbrain. Ncdn is highly expressed in the hippocampus, piriform cortex, septum, amygdaloid complex, medial geniculate nucleus, inferior colliculus, cerebellar nuclei and the nuclei of the Vth, VIIth, and XIIth cranial nerves.

Published

2004

15. MTO1-Deficient Mouse Model Mirrors the Human Phenotype Showing Complex I Defect and Cardiomyopathy

Author

Ilona Mossbrugger, Frauke Neff, Ilka Wittig, Evelyn Schiller, Wolfgang Wurst, Valentina Strecker, Andreas Bender, Anja Schrewe, Thomas Floss, Sabine M. Hölter, Valerie Gailus-Durner, Helmut Fuchs, Julia Calzada-Wack, Thomas Meitinger, Thomas Klopstock, Raffi Bekeredjian, Martin Hrabě de Angelis, Michaela Aichler, Tina Wenz, Holger Prokisch, Ramona Zeh, Lore Becker, Dirk Janik, Iulia Dumitru, Leticia Quintanilla-Fend, Eva Kling, and Axel Walch

Subjects

Male, pathology [Myocardium], Pathology, Heredity, Mitochondrial Diseases, Mitochondrial Myopathy, Mitochondrial translation, Physiology, Respiratory chain, Cardiomyopathy, Gene Dosage, Gene Expression, pathology [Cardiomyopathies], Mitochondrion, genetics [Carrier Proteins], Mto1 protein, mouse, Biochemistry, pathology [Mitochondria], Oxidative Phosphorylation, Mice, Molecular Cell Biology, Medicine and Health Sciences, genetics [Electron Transport Complex I], Energy-Producing Organelles, genetics [Cardiomyopathies], Mice, Knockout, Multidisciplinary, Respiration, Hypertrophic cardiomyopathy, RNA-Binding Proteins, Heart, Animal Models, genetics [DNA, Mitochondrial], Mitochondria, Phenotypes, Genes, Mitochondrial, Cardiovascular Diseases, Lactic acidosis, Gene Knockdown Techniques, Medicine, Female, Cardiomyopathies, Arrhythmia, Research Article, medicine.medical_specialty, Science, Cardiology, Mutagenesis (molecular biology technique), Mouse Models, Bioenergetics, Research and Analysis Methods, Gene dosage, DNA, Mitochondrial, Mitochondrial Proteins, Oxygen Consumption, Model Organisms, medicine, Genetics, Animals, Humans, ddc:610, Clinical Genetics, physiopathology [Heart], Electron Transport Complex I, business.industry, Myocardium, Biology and Life Sciences, Human Genetics, Cell Biology, physiopathology [Cardiomyopathies], medicine.disease, metabolism [Mitochondria], Mice, Inbred C57BL, Disease Models, Animal, Protein Translation, business, Physiological Processes, Carrier Proteins

Abstract

Recently, mutations in the mitochondrial translation optimization factor 1 gene (MTO1) were identified as causative in children with hypertrophic cardiomyopathy, lactic acidosis and respiratory chain defect. Here, we describe an MTO1-deficient mouse model generated by gene trap mutagenesis that mirrors the human phenotype remarkably well. As in patients, the most prominent signs and symptoms were cardiovascular and included bradycardia and cardiomyopathy. In addition, the mutant mice showed a marked worsening of arrhythmias during induction and reversal of anaesthesia. The detailed morphological and biochemical workup of murine hearts indicated that the myocardial damage was due to complex I deficiency and mitochondrial dysfunction. In contrast, neurological examination was largely normal in Mto1-deficient mice. A translational consequence of this mouse model may be to caution against anaesthesia-related cardiac arrhythmias which may be fatal in patients.

Published

2014

16. Mitochondrial dysfunction and decrease in body weight of a transgenic knock-in mouse model for TDP-43

Author

Lisa Glasl, Elisabeth Kremmer, Dietrich Trümbach, Thomas Klopstock, Jan Rozman, Aladin Samara, Martin Klingenspor, Sebastian Koob, Wolfgang Wurst, Martin Hrabě de Angelis, Frauke Neff, Carola Stribl, Eckhard Wolf, Birgit Rathkolb, Manuela Neumann, Regina Peis, Lore Becker, Thomas Floss, Helmut Fuchs, Axel Walch, Sabine M. Hölter, Valerie Gailus-Durner, Wolfgang Hans, Andreas S. Reichert, Michaela Aichler, Johannes Beckers, and Marion Horsch

Subjects

Blood Glucose, CD36 Antigens, Male, parkin protein, Biochemistry, pathology [Mitochondria], Parkin, Inclusion bodies, Mice, cytology [Embryonic Stem Cells], Gene expression, metabolism [Fatty Acids], Gene Knock-In Techniques, Amyotrophic lateral sclerosis, metabolism [Blood Glucose], Motor Neurons, Genome, Behavior, Animal, Neurodegeneration, Fatty Acids, Molecular Bases of Disease, humanities, Mitochondria, DNA-Binding Proteins, genetics [Amyotrophic Lateral Sclerosis], Phenotype, ddc:540, Female, metabolism [DNA-Binding Proteins], Heterozygote, DNA, Complementary, Genotype, metabolism [Cholesterol, HDL], Ubiquitin-Protein Ligases, education, genetics [DNA-Binding Proteins], Mice, Transgenic, Biology, metabolism [DNA, Complementary], TARDBP, metabolism [Ubiquitin-Protein Ligases], mental disorders, medicine, Animals, Humans, Maze Learning, Letters to the Editor, Molecular Biology, Alleles, Embryonic Stem Cells, metabolism [Amyotrophic Lateral Sclerosis], Amyotrophic Lateral Sclerosis, Body Weight, Cholesterol, HDL, Wild type, nutritional and metabolic diseases, Heterozygote advantage, metabolism [Motor Neurons], Cell Biology, metabolism [CD36 Antigens], medicine.disease, Molecular biology, nervous system diseases, Gene Expression Regulation, Mutation, Mutagenesis, Site-Directed

Abstract

The majority of amyotrophic lateral sclerosis (ALS) cases as well as many patients suffering from frontotemporal lobar dementia (FTLD) with ubiquitinated inclusion bodies show TDP-43 pathology, the protein encoded by the TAR DNA-binding protein (Tardbp) gene. We used recombinase-mediated cassette exchange to introduce an ALS patient cDNA into the mouse Tdp-43 locus. Expression levels of human A315T TDP-43 protein were 300% elevated in heterozygotes, whereas the endogenous mouse Tdp-43 was decreased to 20% of wild type levels as a result of disturbed feedback regulation. Heterozygous TDP-43(A315TKi) mutants lost 10% of their body weight and developed insoluble TDP-43 protein starting as early as 3 months after birth, a pathology that was exacerbated with age. We analyzed the splicing patterns of known Tdp-43 target genes as well as genome-wide gene expression levels in different tissues that indicated mitochondrial dysfunction. In heterozygous mutant animals, we observed a relative decrease in expression of Parkin (Park2) and the fatty acid transporter CD36 along with an increase in fatty acids, HDL cholesterol, and glucose in the blood. As seen in transmission electron microscopy, neuronal cells in motor cortices of TDP-43(A315TKi) animals had abnormal neuronal mitochondrial cristae formation. Motor neurons were reduced to 90%, but only slight motoric impairment was detected. The observed phenotype was interpreted as a predisease model, which might be valuable for the identification of further environmental or genetic triggers of neurodegeneration.

Published

2014

17. A role for FGF-6 in skeletal muscle regeneration

Author

Thomas Floss, Hans-Henning Arnold, and Thomas Braun

Subjects

Male, Fibroblast Growth Factor 6, Cellular differentiation, Mice, Transgenic, Biology, MyoD, Fibroblast growth factor, Muscle hypertrophy, Mice, MyoD Protein, Proto-Oncogene Proteins, Genetics, medicine, Animals, Regeneration, Muscle, Skeletal, Myogenin, Recombination, Genetic, Stem Cells, Regeneration (biology), Glyceraldehyde-3-Phosphate Dehydrogenases, Skeletal muscle, Hypertrophy, Fibrosis, Molecular biology, Mice, Mutant Strains, Fibroblast Growth Factors, Mice, Inbred C57BL, medicine.anatomical_structure, Mutation, Female, Cell Division, Research Paper, Developmental Biology

Abstract

Fibroblast growth factor-6 (FGF-6) belongs to a family of cytokines that control cell proliferation, cell differentiation, and morphogenetic events. Individual FGFs are either expressed widely or in a restricted pattern during embryonic, fetal, and adult life. FGF-6 exhibits a restricted expression profile predominantly in the myogenic lineage. Important functions in wound healing and tissue regeneration have been proposed for various FGFs in the past, although data from knockout mice have not supported this view. We have inactivated the FGF-6 gene in mice to investigate the role of FGF-6 in skeletal muscle development and regeneration. Wild-type mice up-regulate FGF-6 after skeletal muscle injuries and completely restore experimentally damaged skeletal muscle. In contrast, FGF-6(−/−) mutant mice show a severe regeneration defect with fibrosis and myotube degeneration. The number of MyoD- and Myogenin-expressing activated satellite cells after injury were significantly reduced in mutants. This reduction was not caused by a reduced pool of quiescent satellite cells but presumably by a lack of activation or proliferation. Interbreeding of FGF-6(−/−) mutants with mdx mice leads to striking dystrophic changes in skeletal muscles of double homozygous mice characterized by myotube degeneration, the presence of large amounts of mononuclear cells, and deposition of collagen. RNA analysis revealed an up-regulation of MyoD mRNA in mdx but not in FGF-6(−/−)/mdx double mutant mice. We conclude that FGF-6 is a critical component of the muscle regeneration machinery in mammals, possibly by stimulating or activating satellite cells.

Published

1997

18. Expression of the Splicing Factor Gene SFRS10 is Reduced in Human Obesity and Contributes to Enhanced Lipogenesis

Author

Joshua Schroeder, Sarah Crunkhorn, Andrew J. Morris, Josep C. Jimenez-Chillaron, Zhaiyi Zhang, Tiina Kuulasmaa, Hongmei Ren, Mary-Elizabeth Patti, Thomas Floss, Imad Nasser, Paula Itkonen, Zhenwen Zhao, Tanner Boes, Allison B. Goldfine, Markku Laakso, Wolfgang Wurst, Carles Lerin, Stefan Stamm, Peter J. Park, Pekka Miettinen, Furkan Burak, Farrell Dearie, Jussi Pihlajamäki, and Yan Xu

Subjects

Male, Very low-density lipoprotein, metabolism [Muscle, Skeletal], Physiology, RNA-binding protein, Mice, 0302 clinical medicine, genetics [Obesity], Genome-wide association, Pre-messenger-RNA, Adipose-tissue, Insulln-resistance, Skeletal-muscle, Diabetic mice, Lipin, Metabolism, Receptor, Protein, Gene expression, blood [Lipids], genetics [RNA-Binding Proteins], genetics [Nerve Tissue Proteins], 2. Zero hunger, Regulation of gene expression, 0303 health sciences, Mice, Inbred ICR, Serine-Arginine Splicing Factors, RNA-Binding Proteins, Middle Aged, Lipids, TRA2B protein, human, Liver, 030220 oncology & carcinogenesis, Lipogenesis, RNA splicing, biosynthesis [Lipids], Female, genetics [Phosphatidate Phosphatase], Adult, medicine.medical_specialty, genetics [Lipogenesis], RNA Splicing, Phosphatidate Phosphatase, Mice, Transgenic, Nerve Tissue Proteins, Biology, Article, biosynthesis [RNA-Binding Proteins], 03 medical and health sciences, Splicing factor, Internal medicine, ddc:570, Cell Line, Tumor, metabolism [Obesity], medicine, Animals, Humans, LPIN1 protein, human, Obesity, genetics [Lipids], biosynthesis [Nerve Tissue Proteins], Muscle, Skeletal, Molecular Biology, 030304 developmental biology, Aged, Lipid metabolism, Cell Biology, Endocrinology, Gene Expression Regulation, metabolism [Liver]

Abstract

Alternative mRNA splicing provides transcript diversity and may contribute to human disease. We demonstrate that expression of several genes regulating RNA processing is decreased in both liver and skeletal muscle of obese humans. We evaluated a representative splicing factor, SFRS10, downregulated in both obese human liver and muscle and in high-fat-fed mice, and determined metabolic impact of reduced expression. SFRS10-specific siRNA induces lipogenesis and lipid accumulation in hepatocytes. Moreover, Sfrs10 heterozygous mice have increased hepatic lipogenic gene expression, VLDL secretion, and plasma triglycerides. We demonstrate that LPIN1, a key regulator of lipid metabolism, is a splicing target of SFRS10; reduced SFRS10 favors the lipogenic β isoform of LPIN1. Importantly, LPIN1β-specific siRNA abolished lipogenic effects of decreased SFRS10 expression. Together, our results indicate that reduced expression of SFRS10, as observed in tissues from obese humans, alters LPIN1 splicing, induces lipogenesis, and therefore contributes to metabolic phenotypes associated with obesity.

Published

2011

19. Musashi 2 is a regulator of the HSC compartment identified by a retroviral insertion screen and knockout mice

Author

Wolfgang Wurst, Thomas Graf, Eric M. Kallin, José F. Infante, Thomas Floss, Florencio Varas, and Luisa de Andrés-Aguayo

Subjects

Male, Myeloid, hematopoietic stem-cells, binding protein musashi, in-vivo, mammalian cns, gene-transfer, c/ebp-alpha, c-myc, rna, proliferation, expression, Immunology, Molecular Sequence Data, Regulator, Thymus Gland, Biology, Biochemistry, Leukocyte Count, Mice, Cell Movement, Gene expression, medicine, Cell Adhesion, Animals, Genetic Testing, Progenitor cell, Gene, Myeloid Progenitor Cells, Mice, Knockout, Protein Synthesis Inhibitors, RNA-Binding Proteins, Neomycin, Cell Biology, Hematology, Lymphoid Progenitor Cells, beta-Galactosidase, Molecular biology, Mice, Inbred C57BL, Haematopoiesis, Mutagenesis, Insertional, medicine.anatomical_structure, Retroviridae, Knockout mouse, Female, Stem cell, Cell Division, Spleen

Abstract

We used a retroviral integration screen to search for novel genes that regulate HSC function. One of the genes that conferred HSC dominance when overexpressed due to an adjacent retroviral insertion was Musashi 2 (Msi2), an RNA-binding protein that can act as a translational inhibitor. A gene-trap mouse model that inactivates the gene shows that Msi2 is more highly expressed in long-term (LT) and short-term (ST) HSCs, as well as in lymphoid myeloid primed progenitors (LMPPs), but much less in intermediate progenitors and mature cells. Mice lacking Msi2 are fully viable for up to a year or more, but exhibit severe defects in primitive precursors, most significantly a reduction in the number of ST-HSCs and LMPPs and a decrease in leukocyte numbers, effects that are exacerbated with age. Cell-cycle and gene-expression analyses suggest that the main hematopoietic defect in Msi2-defective mice is the decreased proliferation capacity of ST-HSCs and LMPPs. In addition, HSCs lacking Msi2 are severely impaired in competitive repopulation experiments, being overgrown by wild-type cells even when mutant cells were provided in excess. Our data indicate that Msi2 maintains the stem cell compartment mainly by regulating the proliferation of primitive progenitors downstream of LT-HSCs.

Published

2011

20. DJ-1-deficient mice show less TH-positive neurons in the ventral tegmental area and exhibit non-motoric behavioural impairments

Author

Holger Prokisch, Thomas Klopstock, Florian Giesert, Uwe Ahting, Thomas Floss, Sabine M. Hölter, Magdalena Kallnik, Philipp J. Kahle, Karin Görner, A. Röthig, M. Hrabé de Angelis, Klaus Beyer, Thu-Trang Pham, D. M. Vogt Weisenhorn, Karin Weindl, Wolfgang Wurst, and Lore Becker

Subjects

Male, Parkinson's disease, Dopamine, Protein Deglycase DJ-1, Striatum, Behavioral Neuroscience, Mice, metabolism [Dopamine], Phosphorylation, metabolism [Oncogene Proteins], Chromatography, High Pressure Liquid, Neurons, Mice, Knockout, Oncogene Proteins, Behavior, Animal, Age Factors, Immunohistochemistry, Respiratory enzyme, Mitochondria, Up-Regulation, Ventral tegmental area, physiology [Behavior, Animal], medicine.anatomical_structure, Neurology, metabolism [Neurons], Knockout mouse, genetics [Up-Regulation], Female, metabolism [Mitogen-Activated Protein Kinase 8], genetics [Mitogen-Activated Protein Kinase 8], physiology [Recognition, Psychology], Genotype, Tyrosine 3-Monooxygenase, Blotting, Western, genetics [Motor Activity], Motor Activity, Biology, Genetics, medicine, Animals, Mitogen-Activated Protein Kinase 8, ddc:610, genetics [Phosphorylation], Loss function, Analysis of Variance, PARK7 protein, mouse, Tyrosine hydroxylase, Ventral Tegmental Area, metabolism [Ventral Tegmental Area], PARK7, JNK Mitogen-Activated Protein Kinases, Recognition, Psychology, genetics [Oncogene Proteins], Peroxiredoxins, medicine.disease, metabolism [Mitochondria], metabolism [Tyrosine 3-Monooxygenase], genetics [JNK Mitogen-Activated Protein Kinases], metabolism [JNK Mitogen-Activated Protein Kinases], genetics [Mitochondria], Neuroscience

Abstract

Loss of function of DJ-1 (PARK7) is associated with autosomal recessive early-onset Parkinson's disease (PD), one of the major age-related neurological diseases. In this study, we extended former studies on DJ-1 knockout mice by identifying subtle morphological and behavioural phenotypes. The DJ-1 gene trap-induced null mutants exhibit less dopamine-producing neurons in the ventral tegmental area (VTA). They also exhibit slight changes in behaviour, i.e. diminished rearing behaviour and impairments in object recognition. Furthermore, we detected subtle phenotypes, which suggest that these animals compensate for the loss of DJ-1. First, we found a significant upregulation of mitochondrial respiratory enzyme activities, a mechanism known to protect against oxidative stress. Second, a close to significant increase in c-Jun N-terminal kinase 1 phosphorylation in old DJ-1-deficient mice hints at a differential activation of neuronal cell survival pathways. Third, as no change in the density of tyrosine hydroxylase (TH)-positive terminals in the striatum was observed, the remaining dopamine-producing neurons likely compensate by increasing axonal sprouting. In summary, the present data suggest that DJ-1 is implicated in major non-motor symptoms of PD appearing in the early phases of the disease-such as subtle impairments in motivated behaviour and cognition-and that under basal conditions the loss of DJ-1 is compensated.

Published

2010

21. Pleiotropic effects in Eya3knockout mice

Author

Magdalena Kallnik, Jochen Graw, Thomas Klopstock, Marion Horsch, Lore Becker, Valerie Gailus-Durner, Christian Stigloher, Holger Schulz, Laure Bally-Cuif, Boris Ivandic, Corinna Moerth, Claudia Dalke, Anja Schrewe, Thomas Floss, Martin Hrabé de Angelis, Jack Favor, Sabine M. Hölter, Helmut Fuchs, Wolfgang Wurst, Stefanie Topp, Oliver Puk, Torben Söker, Beatrix Naton, Wolfgang Hans, Eckhard Wolf, Eva Kling, Johannes Beckers, Ines Bolle, Department of Zebrafish Neurogenetics, Institute of Developmental Genetics, German Research Center for Environmental Health-Helmholtz-Zentrum München (HZM), Neurobiologie & Développement (N&D), Centre National de la Recherche Scientifique (CNRS), Institut de Neurobiologie Alfred Fessard (INAF), and Publica

Subjects

Male, Mutant, MESH: Base Sequence, Eye, medicine.disease_cause, MESH: Mice, Knockout, Mice, MESH: Pregnancy, 0302 clinical medicine, Pregnancy, MESH: Gene Expression Regulation, Developmental, Gene expression, MESH: Animals, lcsh:QH301-705.5, Zebrafish, MESH: Organ Specificity, In Situ Hybridization, Mice, Knockout, 0303 health sciences, Mutation, Homozygote, MESH: DNA, Gene Expression Regulation, Developmental, MESH: Lac Operon, Phenotype, DNA-Binding Proteins, Lac Operon, Organ Specificity, Knockout mouse, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Female, MESH: Homozygote, Research Article, MESH: Mutation, MESH: Mice, Transgenic, MESH: Eye, MESH: Zebrafish Proteins, Mice, Transgenic, Biology, MESH: Phenotype, MESH: Gene Expression Profiling, 03 medical and health sciences, MESH: In Situ Hybridization, MESH: Mice, Inbred C57BL, medicine, Animals, MESH: Zebrafish, RBBP7, MESH: Mice, 030304 developmental biology, Base Sequence, Gene Expression Profiling, DNA, Zebrafish Proteins, biology.organism_classification, Molecular biology, MESH: Male, Mice, Inbred C57BL, Gene expression profiling, Mutagenesis, Insertional, MESH: Mutagenesis, Insertional, lcsh:Biology (General), MESH: Female, MESH: DNA-Binding Proteins, 030217 neurology & neurosurgery, Developmental Biology

Abstract

BackgroundInDrosophila, mutations in the geneeyes absent(eya) lead to severe defects in eye development. The functions of its mammalian orthologsEya1-4are only partially understood and no mouse model exists forEya3. Therefore, we characterized the phenotype of a newEya3knockout mouse mutant.ResultsExpression analysis ofEya3byin-situhybridizations and β-Gal-staining ofEya3mutant mice revealed abundant expression of the gene throughout development, e.g. in brain, eyes, heart, somites and limbs suggesting pleiotropic effects of the mutated gene. A similar complex expression pattern was observed also in zebrafish embryos.The phenotype of young adultEya3mouse mutants was systematically analyzed within the German Mouse Clinic. There was no obvious defect in the eyes, ears and kidneys ofEya3mutant mice. Homozygous mutants displayed decreased bone mineral content and shorter body length. In the lung, the tidal volume at rest was decreased, and electrocardiography showed increased JT- and PQ intervals as well as decreased QRS amplitude. Behavioral analysis of the mutants demonstrated a mild increase in exploratory behavior, but decreased locomotor activity and reduced muscle strength. Analysis of differential gene expression revealed 110 regulated genes in heart and brain. Using real-time PCR, we confirmedNup155being down regulated in both organs.ConclusionThe loss ofEya3in the mouse has no apparent effect on eye development. The wide-spread expression ofEya3in mouse and zebrafish embryos is in contrast to the restricted expression pattern inXenopusembryos. The loss ofEya3in mice leads to a broad spectrum of minor physiological changes. Among them, the mutant mice move less than the wild-type mice and, together with the effects on respiratory, muscle and heart function, the mutation might lead to more severe effects when the mice become older. Therefore, future investigations ofEya3function should focus on aging mice.

Published

2008

22. Neurological phenotype and reduced lifespan in heterozygous Tim23 knockout mice, the first mouse model of defective mitochondrial import

Author

Andreas Bender, Martin Hrabé de Angelis, Thomas Klopstock, Helmut Fuchs, Ilka Schneider-Lohmar, Wolfgang Wurst, Arcangela Iuso, Thomas Meitinger, Lore Becker, Uwe Ahting, Eva Kling, Valerie Gailus-Durner, Holger Prokisch, Thomas Floss, and Nikolas Uez

Subjects

Genotype, Mutant, Biophysics, Biology, medicine.disease_cause, Biochemistry, Mitochondrial Membrane Transport Proteins, Tim23 knockout mouse, Mitochondrial import machinery, Mitochondrial Proteins, Mice, Life Expectancy, Forelimb, Mitochondrial Precursor Protein Import Complex Proteins, medicine, Animals, Humans, DDP1, Inner mitochondrial membrane, RBBP7, Gene, Mice, Knockout, Mutation, Hand Strength, Membrane Proteins, Membrane Transport Proteins, Cell Biology, Orofaciodigital Syndromes, Phenotype, Molecular biology, Mitochondria, Protein Transport, Blastocyst, Rotarod Performance Test, Knockout mouse, Haploinsufficiency

Abstract

The Tim23 protein is the key component of the mitochondrial import machinery. It locates to the inner mitochondrial membrane and its own import is dependent on the DDP1/TIM13 complex. Mutations in human DDP1 cause the Mohr-Tranebjaerg syndrome (MTS/DFN-1; OMIM #304700), which is one of the two known human diseases of the mitochondrial protein import machinery. We created a Tim23 knockout mouse from a gene trap embryonic stem cell clone. Homozygous Tim23 mice were not viable. Heterozygous F1 mutants showed a 50% reduction of Tim23 protein in Western blot, a neurological phenotype and a markedly reduced life span. Haploinsufficiency of the Tim23 mutation underlines the critical role of the mitochondrial import machinery for maintaining mitochondrial function.

Published

2008

23. Hdac2 regulates the cardiac hypertrophic response by modulating Gsk3 beta activity

Author

Maozhen Zhang, Yang Luo, Victor A. Ferrari, Tao Wang, Thomas Floss, Wenting Zhu, Peter J. Gruber, Patricia Ruiz Noppinger, Wolfgang Wurst, Charles S. Abrams, Chinmay M. Trivedi, Martin Goettlicher, Zhan Yin, and Jonathan A. Epstein

Subjects

medicine.medical_specialty, Molecular Sequence Data, Histone Deacetylase 2, Cardiomegaly, Mice, Transgenic, Biology, PKC alpha, General Biochemistry, Genetics and Molecular Biology, Histone Deacetylases, Muscle hypertrophy, Glycogen Synthase Kinase 3, Mice, Fetus, GSK-3, Internal medicine, medicine, Animals, GSK3B, Protein kinase B, Mice, Knockout, Glycogen Synthase Kinase 3 beta, Histone deacetylase 2, General Medicine, medicine.disease, Enzyme Activation, Isoenzymes, Repressor Proteins, Endocrinology, Heart failure, Histone deacetylase, Signal Transduction

Abstract

In the adult heart, a variety of stresses induce re-expression of a fetal gene program in association with myocyte hypertrophy and heart failure. Here we show that histone deacetylase-2 (Hdac2) regulates expression of many fetal cardiac isoforms. Hdac2 deficiency or chemical histone deacetylase (HDAC) inhibition prevented the re-expression of fetal genes and attenuated cardiac hypertrophy in hearts exposed to hypertrophic stimuli. Resistance to hypertrophy was associated with increased expression of the gene encoding inositol polyphosphate-5-phosphatase f (Inpp5f) resulting in constitutive activation of glycogen synthase kinase 3beta (Gsk3beta) via inactivation of thymoma viral proto-oncogene (Akt) and 3-phosphoinositide-dependent protein kinase-1 (Pdk1). In contrast, Hdac2 transgenic mice had augmented hypertrophy associated with inactivated Gsk3beta. Chemical inhibition of activated Gsk3beta allowed Hdac2-deficient adults to become sensitive to hypertrophic stimulation. These results suggest that Hdac2 is an important molecular target of HDAC inhibitors in the heart and that Hdac2 and Gsk3beta are components of a regulatory pathway providing an attractive therapeutic target for the treatment of cardiac hypertrophy and heart failure.

Published

2006

24. Genomewide production of multipurpose alleles for the functional analysis of the mouse genome

Author

Frank Schnütgen, Joachim Altschmied, Claudia Seisenberger, Silke De-Zolt, Melanie Hollatz, Patricia Ruiz, Norbert B. Ghyselinck, Wolfgang Wurst, Jens Hansen, Thomas Floss, Pierre Chambon, Petra P. H. Van Sloun, Harald von Melchner, Institut de génétique et biologie moléculaire et cellulaire (IGBMC), Centre National de la Recherche Scientifique (CNRS)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Louis Pasteur - Strasbourg I, and Université Louis Pasteur - Strasbourg I-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Somatic cell, medicine.disease_cause, Polymerase Chain Reaction, Genome, Mice, 0302 clinical medicine, Gene trapping, MESH: Genetic Vectors, MESH: Animals, Genetics, 0303 health sciences, Mutation, Multidisciplinary, Stem Cells, MESH: Genomics, Genomics, Biological Sciences, MESH: Genes, MESH: Mutagenesis, Site-Directed, MESH: Retroviridae, conditional mutagenesis, ES cells, gene trapping, site-specific recombination, insertional mutagenesis, MESH: Computational Biology, MESH: Mutation, Blotting, Western, Genetic Vectors, MESH: Stem Cells, Biology, Cell Line, Insertional mutagenesis, 03 medical and health sciences, medicine, Animals, MESH: Blotting, Northern, MESH: Blotting, Western, MESH: Genome, Site-specific recombination, MESH: Mice, Gene, Alleles, 030304 developmental biology, MESH: Alleles, MESH: Embryo, Computational Biology, MESH: Polymerase Chain Reaction, [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, Blotting, Northern, Embryo, Mammalian, MESH: Cell Line, Retroviridae, Genes, Mutagenesis, Site-Directed, 030217 neurology & neurosurgery

Abstract

International audience; A type of retroviral gene trap vectors has been developed that can induce conditional mutations in most genes expressed in mouse embryonic stem (ES) cells. The vectors rely on directional site-specific recombination systems that can repair and re-induce gene trap mutations when activated in succession. After the gene traps are inserted into the mouse genome, genetic mutations can be produced at a particular time and place in somatic cells. In addition to their conditional features, the vectors create multipurpose alleles amenable to a wide range of post-insertional modifications. Here we have used these directional recombination vectors to assemble the largest library of ES cell lines with conditional mutations in single genes yet assembled, presently totaling 1,000 unique genes. The trapped ES cell lines, which can be ordered from the German Gene Trap Consortium, are freely available to the scientific community.

Published

2005

25. Nephrin TRAP mice lack slit diaphragms and show fibrotic glomeruli and cystic tubular lesions

Author

Anu Pätäri, Eva Åström, Dontscho Kerjaschki, Wolfgang Wurst, Harry Holthöfer, Maija Rantanen, Thomas Floss, Franz Vauti, Sanna Lehtonen, Heikki Ahola, Tuula Palmén, and Patrizia Ruiz

Subjects

Pathology, medicine.medical_specialty, Genotype, Renal glomerulus, Kidney Glomerulus, Podocyte foot, urologic and male genital diseases, Kidney, Podocyte, Nephrin, chemistry.chemical_compound, Mice, medicine, Animals, RNA, Messenger, biology, urogenital system, Membrane Proteins, Proteins, Glomerulonephritis, General Medicine, Apical membrane, medicine.disease, Fibrosis, Immunohistochemistry, medicine.anatomical_structure, Kidney Tubules, Podocalyxin, chemistry, Nephrology, biology.protein, Glomerular Filtration Barrier

Abstract

The molecular mechanisms maintaining glomerular filtration barrier are under intensive study. This study describes a mutant Nphs1 mouse line generated by gene-trapping. Nephrin, encoded by Nphs1 , is a structural protein of interpodocyte filtration slits crucial for formation of primary urine. Nephrin trap/trap mutants show characteristic features of proteinuric disease and die soon after birth. Morphologically, fibrotic glomeruli with distorted structures and cystic tubular lesions were observed, but no prominent changes in the branching morphogenesis of the developing collecting ducts could be found. Western blotting and immunohistochemical analyses confirmed the absence of nephrin in nephrin trap/trap glomeruli. The immunohistochemical staining showed also that the interaction partner of nephrin, CD2-associated protein (CD2AP), and the slit-diaphragm-associated protein, ZO-1α − , appeared unchanged, whereas the major anionic apical membrane protein of podocytes, podocalyxin, somewhat punctate as compared with the wild-type (wt) and nephrin wt/trap stainings. Electron microscopy revealed that >90% of the podocyte foot processes were fused. The remaining interpodocyte junctions lacked slit diaphragms and, instead, showed tight adhering areas. In the heterozygote glomeruli, approximately one third of the foot processes were fused and real-time RT-PCR showed >60% decrease of nephrin-specific transcripts. These results show an effective nephrin gene elimination, resulting in a phenotype that resembles human congenital nephrotic syndrome. Although the nephrin trap/trap mice can be used to study the pathophysiology of the disease, the heterozygous mice may provide a useful model to study the gene dose effect of this crucial protein of the glomerular filtration barrier.

Published

2002

26. Reply to Jawaid et al.: Mitochondrial Dysfunction and Decrease in Body Weight of Transgenic Knock-in Mouse Model for TDP-43: the Question of Glucose?

Author

Thomas Floss

Subjects

Male, medicine.medical_specialty, Transgene, Mutant, Mitochondrion, Biology, Body weight, Biochemistry, Internal medicine, medicine, Animals, Humans, Amyotrophic lateral sclerosis, Knock in mouse, Letters to the Editor, Molecular Biology, Regulation of gene expression, Amyotrophic Lateral Sclerosis, Cell Biology, medicine.disease, Mitochondria, DNA-Binding Proteins, Endocrinology, Gene Expression Regulation, Female, Analysis of variance

Abstract

This is a response to a letter by Jawaid et al. (1). In their letter Jawaid et al. (1) refer to our recent paper on a TDP-43 transgenic knock-in (ki) mouse. The authors claim that Fig. 7 does not show differences in glucose levels of the animals and that an elevation of glucose levels would not be expected after mitochondrial dysfunction. In our measurements, glucose levels of TDP-43 ki animals were slightly elevated in ad libitum fed mice as compared with wild-type controls (ANOVA genotype-related p value was 0.04). In contrast, there was no significant difference in animals that were starved overnight. In these animals the tendency was to rather slightly lower levels. In my opinion, Fig. 7 clearly illustrates both these findings. Mitochondrial abnormalities have been found solely in the brain to date (e.g. not in spinal cords), and in a follow-up study using compound mutants of TDP-43 ki and another FTLD risk gene, we have just confirmed these findings. However, the reported observations concerning glucose and mitochondria are unrelated, as we underline in our paper (“Whether mitochondrial abnormality could explain the observed metabolic changes and altered body weight composition of hTDP-43A315T animals will be subject of future studies.”) (2).

Published

2014

27. Progressive loss of the spongiotrophoblast layer ofBirc6/Bruce mutants results in embryonic lethality

Author

Christiane Hitz, Thomas Floss, Patricia Ruiz, Daniela Vogt-Weisenhorn, and Wolfgang Wurst

Subjects

Genotype, Apoptosis Inhibitor, Molecular Sequence Data, Mutant, Embryonic Development, Mutagenesis (molecular biology technique), Apoptosis, Biology, medicine.disease_cause, Inhibitor of Apoptosis Proteins, Mice, Endocrinology, medicine, Genetics, Animals, Gene, In Situ Hybridization, Mutation, Base Sequence, Stem Cells, Wild type, Gene Expression Regulation, Developmental, Cell Biology, Embryo, Mammalian, beta-Galactosidase, Embryonic stem cell, Molecular biology, Neoplasm Proteins, Trophoblasts, Mice, Inbred C57BL, Phenotype, Mutagenesis, RNA, Genes, Lethal, human activities, circulatory and respiratory physiology

Abstract

We have generated a mouse line with a mutant allele of the mouse Bruce/Birc6 gene induced by gene trap mutagenesis. Based on its structural features, Bruce is a member of the family of apoptosis inhibitor proteins (IAPs). This mutation leads to a truncated transcript and protein and results in a complete loss of the wildtype Bruce protein. Bruce mutant mice die from a progressive loss of their placental spongiotrophoblast layer between day 11.5 and 14.5 of embryonic development. The cause of the Bruce homozygous mutant phenotype is a lack of proliferation of spongiotrophoblast cells in the developing placenta. In contrast to in vitro data, which indicate a function for Bruce in apoptosis inhibition, the in vivo results presented here suggest instead a role for Bruce in cell division. genesis 42:91–103, 2005. © 2005 Wiley-Liss, Inc.

Published

2005

28. Response to Brosch et al

Author

Stefan Stamm, Wolfgang Wurst, Farrell Dearie, Peter J. Park, Imad Nasser, Dorota Kaminska, Andrew J. Morris, Sari Venesmaa, Tanner Boes, Furkan Burak, Allison B. Goldfine, Sarah Crunkhorn, Paula Itkonen, Pekka Miettinen, Carles Lerin, Hongmei Ren, Jussi Pihlajamäki, Yan Xu, Mary-Elizabeth Patti, Joshua Schroeder, Zhaiyi Zhang, Josep C. Jimenez-Chillaron, Tiina Kuulasmaa, Markku Laakso, Zhenwen Zhao, and Thomas Floss

Subjects

business.industry, Physiology, Wish, MEDLINE, Cell Biology, Bioinformatics, Article, Experimental strategy, Splicing factor, ddc:570, Lipogenesis, Medicine, business, Gene, Molecular Biology, Human obesity

Abstract

We would like to respond to Brosch et al. regarding our manuscript "Expression of the Splicing Factor Gene SFRS10 Is Reduced in Human Obesity and Contributes to Enhanced Lipogenesis" (Pihlajamaki et al., 2011b). Brosch performed RT-PCR in liver samples from 13 lean and 34 obese individuals, finding no differences in SFRS10 or LPIN1 expression. We wish to address points raised by Brosch, including experimental strategy and analysis of human SFRS10 expression.

29. Sensitivity to oxidative stress in DJ-1-deficient dopamine neurons: an ES- derived cell model of primary Parkinsonism

Author

M. Flint Beal, Thomas Floss, Asa Abeliovich, Lichuan Yang, Cécile Martinat, Shoshana Shendelman, Thomas Leete, and Alan Jonason

Subjects

General Immunology and Microbiology, QH301-705.5, General Neuroscience, Cellular differentiation, Parkinsonism, Neurodegeneration, PARK7, Substantia nigra, Biology, medicine.disease, medicine.disease_cause, Molecular biology, General Biochemistry, Genetics and Molecular Biology, Cell biology, Dopamine, medicine, Biology (General), Stem cell, General Agricultural and Biological Sciences, Oxidative stress, medicine.drug

Abstract

The hallmark of Parkinson's disease (PD) is the selective loss of dopamine neurons in the ventral midbrain. Although the cause of neurodegeneration in PD is unknown, a Mendelian inheritance pattern is observed in rare cases, indicating a genetic factor. Furthermore, pathological analyses of PD substantia nigra have correlated cellular oxidative stress and altered proteasomal function with PD. Homozygous mutations in DJ-1 were recently described in two families with autosomal recessive Parkinsonism, one of which is a large deletion that is likely to lead to loss of function. Here we show that embryonic stem cells deficient in DJ-1 display increased sensitivity to oxidative stress and proteasomal inhibition. The accumulation of reactive oxygen species in toxin-treated DJ-1-deficient cells initially appears normal, but these cells are unable to cope with the consequent damage that ultimately leads to apoptotic death. Furthermore, we find that dopamine neurons derived from in vitro-differentiated DJ-1-deficient embryonic stem cells display decreased survival and increased sensitivity to oxidative stress. These data are consistent with a protective role for DJ-1, and demonstrate the utility of genetically modified embryonic stem cell-derived neurons as cellular models of neuronal disorders.