Your search keyword '"Sonia Bartunkova"' showing total 17 results

1. The ROSA26-iPSC Mouse: A Conditional, Inducible, and Exchangeable Resource for Studying Cellular (De)Differentiation

Author

Lieven Haenebalcke, Steven Goossens, Pieterjan Dierickx, Sonia Bartunkova, Jinke D’Hont, Katharina Haigh, Tino Hochepied, Dagmar Wirth, Andras Nagy, and Jody J. Haigh

Subjects

Biology (General), QH301-705.5

Abstract

Control of cellular (de)differentiation in a temporal, cell-specific, and exchangeable manner is of paramount importance in the field of reprogramming. Here, we have generated and characterized a mouse strain that allows iPSC generation through the Cre/loxP conditional and doxycycline/rtTA-controlled inducible expression of the OSKM reprogramming factors entirely from within the ROSA26 locus. After reprogramming, these factors can be replaced by genes of interest—for example, to enhance lineage-directed differentiation—with the use of a trap-coupled RMCE reaction. We show that, similar to ESCs, Dox-controlled expression of the cardiac transcriptional regulator Mesp1 together with Wnt inhibition enhances the generation of functional cardiomyocytes upon in vitro differentiation of such RMCE-retargeted iPSCs. This ROSA26-iPSC mouse model is therefore an excellent tool for studying both cellular reprogramming and lineage-directed differentiation factors from the same locus and will greatly facilitate the identification and ease of functional characterization of the genetic/epigenetic determinants involved in these complex processes.

Published

2013

2. Beta-Actin Is Involved in Modulating Erythropoiesis during Development by Fine-Tuning Gata2 Expression Levels.

Author

Davina Tondeleir, Benjamin Drogat, Karolina Slowicka, Karima Bakkali, Sonia Bartunkova, Steven Goossens, Jody J Haigh, and Christophe Ampe

Subjects

Medicine, Science

Abstract

The functions of actin family members during development are poorly understood. To investigate the role of beta-actin in mammalian development, a beta-actin knockout mouse model was used. Homozygous beta-actin knockout mice are lethal at embryonic day (E)10.5. At E10.25 beta-actin knockout embryos are growth retarded and display a pale yolk sac and embryo proper that is suggestive of altered erythropoiesis. Here we report that lack of beta-actin resulted in a block of primitive and definitive hematopoietic development. Reduced levels of Gata2, were associated to this phenotype. Consistently, ChIP analysis revealed multiple binding sites for beta-actin in the Gata2 promoter. Gata2 mRNA levels were almost completely rescued by expression of an erythroid lineage restricted ROSA26-promotor based GATA2 transgene. As a result, erythroid differentiation was restored and the knockout embryos showed significant improvement in yolk sac and embryo vascularization. These results provide new molecular insights for a novel function of beta-actin in erythropoiesis by modulating the expression levels of Gata2 in vivo.

Published

2013

3. Keratinocyte-Specific Ablation of RIPK4 Allows Epidermal Cornification but Impairs Skin Barrier Formation

Author

Michiel De Bruyne, Barbara Gilbert, Corinne Urwyler-Rösselet, Sonia Bartunkova, Saskia Lippens, Kirsten Leurs, Peter Vandenabeele, Riet De Rycke, Giel Tanghe, Philippe De Groote, Carien M. Niessen, Wim Declercq, and Marek Haftek

Subjects

Keratinocytes, 0301 basic medicine, Keratin 14, Dermatology, Protein Serine-Threonine Kinases, Biochemistry, Cell Line, Tight Junctions, Cornified envelope, Mice, 03 medical and health sciences, Microscopy, Electron, Transmission, Keratin, Stratum corneum, medicine, Animals, Humans, RNA, Small Interfering, Protein kinase A, Molecular Biology, Mice, Knockout, chemistry.chemical_classification, integumentary system, Tight junction, Epidermis (botany), Cell Membrane, Cell Differentiation, Cell Biology, Cadherins, Embryo, Mammalian, Water Loss, Insensible, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, chemistry, Epidermis, Keratinocyte

Abstract

In humans, receptor-interacting protein kinase 4 (RIPK4) mutations can lead to the autosomal recessive Bartsocas-Papas and popliteal pterygium syndromes, which are characterized by severe skin defects, pterygia, as well as clefting. We show here that the epithelial fusions observed in RIPK4 full knockout (KO) mice are E-cadherin dependent, as keratinocyte-specific deletion of E-cadherin in RIPK4 full KO mice rescued the tail-to-body fusion and fusion of oral epithelia. To elucidate RIPK4 function in epidermal differentiation and development, we generated epidermis-specific RIPK4 KO mice (RIPK4EKO). In contrast to RIPK4 full KO epidermis, RIPK4EKO epidermis was normally stratified and the outside-in skin barrier in RIPK4EKO mice was largely intact at the trunk, in contrast to the skin covering the head and the outer end of the extremities. However, RIPK4EKO mice die shortly after birth due to excessive water loss because of loss of tight junction protein claudin-1 localization at the cell membrane, which results in tight junction leakiness. In contrast, mice with keratinocyte-specific RIPK4 deletion during adult life remain viable. Furthermore, our data indicate that epidermis-specific deletion of RIPK4 results in delayed keratinization and stratum corneum maturation and altered lipid organization and is thus indispensable during embryonic development for the formation of a functional inside-out epidermal barrier.

Published

2018

4. Developing 3D SEM in a broad biological context

Author

Sophie Janssens, C Theunis, Brigitte Schepens, J-C Larsimont, Matyáš Fendrych, Christopher J. Guérin, Alain Goossens, Saskia Lippens, Xavier Saelens, Cédric Blanpain, C Mc Guire, R Van Brempt, Véronique Timmerman, Sonia Bartunkova, Bob Asselbergh, A Schertel, Y Visser, Moritz K. Nowack, Michiel Krols, Matthew Holt, Anneke Kremer, and Michal Slezak

Subjects

Serial block-face scanning electron microscopy, 0303 health sciences, Histocytological Preparation Techniques, Histology, business.industry, Context (language use), Nanotechnology, Serial section, Biology, Focused ion beam, Pathology and Forensic Medicine, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, Microscopy, Microtome, Computer vision, Artificial intelligence, business, 030217 neurology & neurosurgery, Electron Microscope Tomography, 030304 developmental biology

Abstract

When electron microscopy (EM) was introduced in the 1930s it gave scientists their first look into the nanoworld of cells. Over the last 80 years EM has vastly increased our understanding of the complex cellular structures that underlie the diverse functions that cells need to maintain life. One drawback that has been difficult to overcome was the inherent lack of volume information, mainly due to the limit on the thickness of sections that could be viewed in a transmission electron microscope (TEM). For many years scientists struggled to achieve three-dimensional (3D) EM using serial section reconstructions, TEM tomography, and scanning EM (SEM) techniques such as freeze-fracture. Although each technique yielded some special information, they required a significant amount of time and specialist expertise to obtain even a very small 3D EM dataset. Almost 20 years ago scientists began to exploit SEMs to image blocks of embedded tissues and perform serial sectioning of these tissues inside the SEM chamber. Using first focused ion beams (FIB) and subsequently robotic ultramicrotomes (serial block-face, SBF-SEM) microscopists were able to collect large volumes of 3D EM information at resolutions that could address many important biological questions, and do so in an efficient manner. We present here some examples of 3D EM taken from the many diverse specimens that have been imaged in our core facility. We propose that the next major step forward will be to efficiently correlate functional information obtained using light microscopy (LM) with 3D EM datasets to more completely investigate the important links between cell structures and their functions.

Published

2015

5. Loss of autocrine endothelial-derived VEGF significantly reduces hemangiosarcoma development in conditional p53-deficient mice

Author

Steven Goossens, Morvarid Farhang Ghahremani, Lieven Haenebalcke, Katharina Haigh, Enrico Radaelli, Sonia Bartunkova, Jody J. Haigh, and Jean-Christophe Marine

Subjects

Vascular Endothelial Growth Factor A, Endothelium, Angiogenesis, medicine.medical_treatment, Hemangiosarcoma, Mice, Transgenic, Biology, medicine.disease_cause, Malignant transformation, Report, medicine, Animals, Autocrine signalling, Molecular Biology, Growth factor, Cell Biology, medicine.disease, Endothelial stem cell, medicine.anatomical_structure, Immunology, Cancer research, Endothelium, Vascular, Tumor Suppressor Protein p53, Carcinogenesis, Developmental Biology

Abstract

Malignant transformation of the endothelium is rare, and hemangiosarcomas comprise only 1% of all sarcomas. For this reason and due to the lack of appropriate mouse models, the genetic mechanisms of malignant endothelial transformation are poorly understood. Here, we describe a hemangiosarcoma mouse model generated by deleting p53 specifically in the endothelial and hematopoietic lineages. This strategy led to a high incidence of hemangiosarcoma, with an average latency of 25 weeks. To study the in vivo roles of autocrine or endothelial cell autonomous VEGF signaling in the initiation and/or progression of hemangiosarcomas, we genetically deleted autocrine endothelial sources of VEGF in this mouse model. We found that loss of even a single conditional VEGF allele results in substantial rescue from endothelial cell transformation. These findings highlight the important role of threshold levels of autocrine VEGF signaling in endothelial malignancies and suggest a new approach for hemangiosarcoma treatment using targeted autocrine VEGF inhibition.

Published

2014

6. The EMT regulator Zeb2/Sip1 is essential for murine embryonic hematopoietic stem/progenitor cell differentiation and mobilization

Author

Lieven Haenebalcke, Katharina Haigh, Mihaela Crisan, Danny Huylebroeck, Tomomasa Yokomizo, Steven Goossens, Geert Berx, Viktor Janzen, Elaine Dzierzak, Sonia Bartunkova, Jody J. Haigh, Lieve Umans, Pieter Bogaert, Eve Seuntjens, Benjamin Drogat, Tamara Riedt, and Cell biology

Subjects

Male, Epithelial-Mesenchymal Transition, Immunology, Biology, Biochemistry, CXCR4, Mice, Cell Movement, medicine, Animals, Progenitor cell, Zinc Finger E-box Binding Homeobox 2, Homeodomain Proteins, Mice, Knockout, Integrases, Embryogenesis, Embryo, Cell Differentiation, Zinc Fingers, Cell Biology, Hematology, Cadherins, Embryo, Mammalian, Flow Cytometry, Hematopoietic Stem Cells, Embryonic stem cell, Cell biology, Hematopoiesis, Repressor Proteins, Haematopoiesis, medicine.anatomical_structure, Tumor progression, embryonic structures, Female, Genes, Lethal, Bone marrow

Abstract

Zeb2 (Sip1/Zfhx1b) is a member of the zinc-finger E-box-binding (ZEB) family of transcriptional repressors previously demonstrated to regulate epithelial-to-mesenchymal transition (EMT) processes during embryogenesis and tumor progression. We found high Zeb2 mRNA expression levels in HSCs and hematopoietic progenitor cells (HPCs), and examined Zeb2 function in hematopoiesis through a conditional deletion approach using the Tie2-Cre and Vav-iCre recombination mouse lines. Detailed cellular analysis demonstrated that Zeb2 is dispensable for hematopoietic cluster and HSC formation in the aorta-gonadomesonephros region of the embryo, but is essential for normal HSC/HPC differentiation. In addition, Zeb2-deficient HSCs/HPCs fail to properly colonize the fetal liver and/or bone marrow and show enhanced adhesive properties associated with increased β1 integrin and Cxcr4 expression. Moreover, deletion of Zeb2 resulted in embryonic (Tie2-Cre) and perinatal (Vav-icre) lethality due to severe cephalic hemorrhaging and decreased levels of angiopoietin-1 and, subsequently, improper pericyte coverage of the cephalic vasculature. These results reveal essential roles for Zeb2 in embryonic hematopoiesis and are suggestive of a role for Zeb2 in hematopoietic-related pathologies in the adult. ispartof: Blood vol:117 issue:21 pages:5620-5630 ispartof: location:United States status: published

Published

2011

7. Increased skeletal VEGF enhances β-catenin activity and results in excessively ossified bones

Author

Vice Mandic, Peter Carmeliet, Axel Behrens, Jan Tuckermann, Omar Nyabi, Andras Nagy, Steven Goossens, Karen Moermans, Lieve Coenegrachts, Michael Naessens, Jean-Pierre David, Katharina Haigh, Ingrid Stockmans, Christa Maes, Benjamin Drogat, Sonia Bartunkova, Jody J. Haigh, Geert Carmeliet, Marc Tjwa, and Lieven Haenebalcke

Subjects

Vascular Endothelial Growth Factor A, medicine.medical_specialty, Stromal cell, Cellular differentiation, Mice, Transgenic, Biology, Bone and Bones, Article, General Biochemistry, Genetics and Molecular Biology, Mesoderm, Mice, Phosphatidylinositol 3-Kinases, chemistry.chemical_compound, GSK-3, Internal medicine, Morphogenesis, medicine, Animals, Humans, Molecular Biology, Cells, Cultured, beta Catenin, Cell Proliferation, Osteoblasts, General Immunology and Microbiology, Stem Cells, General Neuroscience, Endothelial Cells, Gene Expression Regulation, Developmental, Hematopoietic stem cell, Cell Differentiation, Osteoblast, Vascular endothelial growth factor, Vascular endothelial growth factor A, Endocrinology, medicine.anatomical_structure, chemistry, Stromal Cells, Stem cell

Abstract

Vascular endothelial growth factor (VEGF) and beta-catenin both act broadly in embryogenesis and adulthood, including in the skeletal and vascular systems. Increased or deregulated activity of these molecules has been linked to cancer and bone-related pathologies. By using novel mouse models to locally increase VEGF levels in the skeleton, we found that embryonic VEGF over-expression in osteo-chondroprogenitors and their progeny largely pheno-copied constitutive beta-catenin activation. Adult induction of VEGF in these cell populations dramatically increased bone mass, associated with aberrant vascularization, bone marrow fibrosis and haematological anomalies. Genetic and pharmacological interventions showed that VEGF increased bone mass through a VEGF receptor 2- and phosphatidyl inositol 3-kinase-mediated pathway inducing beta-catenin transcriptional activity in endothelial and osteoblastic cells, likely through modulation of glycogen synthase kinase 3-beta phosphorylation. These insights into the actions of VEGF in the bone and marrow environment underscore its power as pleiotropic bone anabolic agent but also warn for caution in its therapeutic use. Moreover, the finding that VEGF can modulate beta-catenin activity may have widespread physiological and clinical ramifications.

Published

2009

8. The cardiac homeobox gene Csx/Nkx2.5 lies genetically upstream of multiple genes essential for heart development

Author

Sonia Bartunkova, Naohito Yamasaki, Zhi Chen, Makoto Tanaka, and Seigo Izumo

Subjects

Cardiovascular Abnormalities, Neovascularization, Physiologic, Xenopus Proteins, Biology, Homeobox protein Nkx-2.5, Mice, Morphogenesis, Null cell, Animals, Myocyte, Heart looping, MEF2C, Molecular Biology, Yolk Sac, Homeodomain Proteins, Genetics, Regulation of gene expression, Genes, Essential, Heart development, Chimera, Genes, Homeobox, Chromosome Mapping, Gene Expression Regulation, Developmental, Heart, Null allele, Mice, Mutant Strains, Hematopoiesis, Cell biology, Multigene Family, embryonic structures, Homeobox Protein Nkx-2.5, cardiovascular system, Transcription Factors, Developmental Biology

Abstract

Csx/Nkx2.5 is a vertebrate homeobox gene with a sequence homology to the Drosophila tinman, which is required for the dorsal mesoderm specification. Recently, heterozygous mutations of this gene were found to cause human congenital heart disease (Schott, J.-J., Benson, D. W., Basson, C. T., Pease, W., Silberbach, G. M., Moak, J. P., Maron, B. J., Seidman, C. E. and Seidman, J. G. (1998) Science 281, 108-111). To investigate the functions of Csx/Nkx2.5 in cardiac and extracardiac development in the vertebrate, we have generated and analyzed mutant mice completely null for Csx/Nkx2.5. Homozygous null embryos showed arrest of cardiac development after looping and poor development of blood vessels. Moreover, there were severe defects in vascular formation and hematopoiesis in the mutant yolk sac. Interestingly, TUNEL staining and PCNA staining showed neither enhanced apoptosis nor reduced cell proliferation in the mutant myocardium. In situ hybridization studies demonstrated that, among 20 candidate genes examined, expression of ANF, BNP, MLC2V, N-myc, MEF2C, HAND1 and Msx2 was disturbed in the mutant heart. Moreover, in the heart of adult chimeric mice generated from Csx/Nkx2.5 null ES cells, there were almost no ES cell-derived cardiac myocytes, while there were substantial contributions of Csx /Nkx2.5-deficient cells in other organs. Whole-mount β-gal staining of chimeric embryos showed that more than 20% contribution of Csx/Nkx2.5-deficient cells in the heart arrested cardiac development. These results indicate that (1) the complete null mutation of Csx/Nkx2.5 did not abolish initial heart looping, (2) there was no enhanced apoptosis or defective cell cycle entry in Csx/Nkx2.5 null cardiac myocytes, (3) Csx/Nkx2.5 regulates expression of several essential transcription factors in the developing heart, (4) Csx/Nkx2.5 is required for later differentiation of cardiac myocytes, (5) Csx/Nkx2.5 null cells exert dominant interfering effects on cardiac development, and (6) there were severe defects in yolk sac angiogenesis and hematopoiesis in the Csx/Nkx2.5 null embryos.

Published

1999

9. Vertebrate homologs oftinman andbagpipe: Roles of the homeobox genes in cardiovascular development

Author

Makoto Tanaka, Youngsook Lee, Gary E. Lyons, Sonia Bartunkova, Issei Komuro, Hidetoshi Inagaki, Hideko Kasahara, Martina Schinke, and Seigo Izumo

Subjects

Genetics, biology, Homeobox A1, Gene targeting, Cell Biology, HNF1B, biology.organism_classification, Homeobox protein Nkx-2.5, medicine.anatomical_structure, Tinman gene, embryonic structures, medicine, Homeobox, Endoderm, Zebrafish, Developmental Biology

Abstract

In Drosophila, dorsal mesodermal specification is regulated by the homeobox genes tinman and bagpipe. Vertebrate homologs of tinman and bagpipe have been isolated in various species. Moreover, there are at least four different genes related to tinman in the vertebrate, which indicates that this gene has been duplicated during evolution. One of the murine homologs of tinman is the cardiac homeobox gene Csx or Nkx2.5. Gene targeting of Csx/Nkx2.5 showed that this gene is required for completion of the looping morphogenesis of the heart. However, it is not essential for the specification of the heart cell lineage. Early cardiac development might therefore be regulated by other genes, which may act either independently or in concert with Csx/Nkx2.5. Possible candidates might be other members of the NK2 class of homeobox proteins like Tix/Nkx2.6, Nkx2.3, nkx2.7, or cNkx2.8. Murine Tix/Nkx2.6 mRNA has been detected in the heart and pharyngeal endoderm (this study). Xenopus XNkx2.3 and chicken cNkx2.3 are expressed in the heart as well as in pharyngeal and gut endoderm. In contrast, murine Nkx2.3 is expressed in the gut and pharyngeal arches but not the heart. In zebrafish and chicken, two new NK-2 class homeoproteins, nkx2.7 and cNkx2.8, have been identified. Zebrafish nkx2.7 is expressed in both, the heart and pharyngeal endoderm. In the chicken, cNkx2.8 is expressed in the heart primordia and the primitive heart tube and becomes undetectable after looping. No murine homologs of nkx2.7 or cNkx2.8 have been found so far. The overlapping expression pattern of NK2 class homeobox genes in the heart and the pharynx may suggest a common origin of these two organs. In the Drosophila genome, the tinman gene is linked to another NK family gene named bagpipe. A murine homolog of bagpipe, Bax/Nkx3.1, is expressed in somites, blood vessels, and the male reproductive system during embryogenesis (this study), suggesting that this gene's function may be relevant for the development of these organs. A bagpipe homolog in Xenopus, Xbap, is expressed in the gut masculature and a region of the facial cartilage during development. In this paper, we discuss molecular mechanisms of cardiovascular development with particular emphasis on roles of transcription factors.

Published

1998

10. p53 promotes VEGF expression and angiogenesis in the absence of an intact p21-Rb pathway

Author

Sonia Bartunkova, Jody J. Haigh, Xavier Bisteau, Jean-Christophe Marine, Lieven Haenebalcke, Pierre P. Roger, Katharina Haigh, Paco Hulpiau, Steven Goossens, Benjamin Drogat, Aart G. Jochemsen, M. Farhang Ghahremani, David Nittner, and Aleksandra Zwolinska

Subjects

Cyclin-Dependent Kinase Inhibitor p21, Vascular Endothelial Growth Factor A, p53, Angiogenesis, Molecular Sequence Data, Transplantation, Heterologous, Down-Regulation, Mice, Nude, Biology, In Vitro Techniques, Retinoblastoma Protein, chemistry.chemical_compound, Mice, angiogenesis, Cell Line, Tumor, medicine, Animals, Humans, Hypoxia, Molecular Biology, Cells, Cultured, Base Sequence, Neovascularization, Pathologic, p21, Retinoblastoma, Retinoblastoma protein, Cell Biology, Cell cycle, Fibroblasts, medicine.disease, Hypoxia-Inducible Factor 1, alpha Subunit, VEGF, Vascular endothelial growth factor, Vascular endothelial growth factor A, Disease Models, Animal, Editorial, Hypoxia-inducible factors, chemistry, Cancer research, biology.protein, Signal transduction, Tumor Suppressor Protein p53, Colorectal Neoplasms, Signal Transduction

Abstract

There is growing evidence that the p53 tumour suppressor downregulates vascular endothelial growth factor (VEGF) expression, although the underlying mechanisms remain unclear and controversial. Here we provide insights from in vitro experiments and in vivo xenotransplantation assays that highlight a dual role for p53 in regulating VEGF during hypoxia. Unexpectedly, and for the first time, we demonstrate that p53 rapidly induces VEGF transcription upon hypoxia exposure by binding, in an HIF-1α-dependent manner, to a highly conserved and functional p53-binding site within the VEGF promoter. However, during sustained hypoxia, p53 indirectly downregulates VEGF expression via the retinoblastoma (Rb) pathway in a p21-dependent manner, which is distinct from its role in cell-cycle regulation. Our findings have important implications for cancer therapy, especially for tumours that harbour wild-type TP53 and a dysfunctional Rb pathway.

Published

2013

11. Efficient ROSA26-based conditional and/or inducible transgenesis using RMCE-compatible F1 hybrid mouse embryonic stem cells

Author

Dagmar Wirth, Sonia Bartunkova, Jody J. Haigh, Katharina Haigh, Michael Naessens, Morvarid Farhang Ghahremani, Steven Goossens, Omar Nyabi, Benjamin Drogat, Pieterjan Dierickx, Lieven Haenebalcke, Natascha Kruse, and Tim Pieters

Subjects

Male, Cancer Research, RNA, Untranslated, Transgene, Gene Expression, Locus (genetics), Computational biology, Biology, Recombinases, Mice, RNA interference, Gene expression, Animals, Crosses, Genetic, Embryonic Stem Cells, Genetics, Recombinase-mediated cassette exchange, Gene Transfer Techniques, Cell Biology, Embryonic stem cell, Transgenesis, Genetic Loci, embryonic structures, Hybridization, Genetic, Female, Stem cell

Abstract

The conditional Cre/loxP system and/or the doxycycline (Dox) inducible Tet-on/off system are widely used in mouse transgenesis but often require time consuming, inefficient cloning/screening steps and extensive mouse breeding strategies. We have therefore developed a highly efficient Gateway- and recombinase-mediated cassette exchange (RMCE)-compatible system to target conditional and/or inducible constructs to the ROSA26 locus of F1 hybrid Bl6/129 ESCs, called G4 ROSALUC ESCs. By combining the Cre/loxP system with or without the inducible Tet-on system using Gateway cloning, we can rapidly generate spatial and/or temporal controllable gain-of-function constructs that can be targeted to the RMCE-compatible ROSA26 locus of the G4 ROSALUC ESCs with efficiencies close to 100 %. These novel ESC-based technologies allow for the creation of multiple gain-of-function conditional and/or inducible transgenic ESC clones and mouse lines in a highly efficient and locus specific manner. Importantly, incorporating insulator sequences into the Dox-inducible vector system resulted in robust, stable transgene expression in undifferentiated ESCs but could not fully overcome transgene mosaicism in the differentiated state.

Published

2013

12. Beta-Actin Is Involved in Modulating Erythropoiesis during Development by Fine-Tuning Gata2 Expression Levels

Author

Sonia Bartunkova, Jody J. Haigh, Christophe Ampe, Davina Tondeleir, Karima Bakkali, Benjamin Drogat, Steven Goossens, and Karolina Slowicka

Subjects

Male, Embryology, Mouse, Psychologie appliquée, Gene Expression, lcsh:Medicine, Biochemistry, Mice, Molecular Cell Biology, Signaling in Cellular Processes, Erythropoiesis, lcsh:Science, ERYTHROID DEVELOPMENT, Cells, Cultured, Genetics, Erythroid Precursor Cells, Mice, Knockout, Multidisciplinary, GATA2, Embryo, Cell Differentiation, Animal Models, Sciences bio-médicales et agricoles, Cell biology, GATA2 Transcription Factor, DIFFERENTIATION, medicine.anatomical_structure, Knockout mouse, Blood Circulation, embryonic structures, Female, Cellular Types, MESSENGER-RNA, Biologie, Research Article, Signal Transduction, animal structures, Transgene, Embryonic Development, Biology, MICE LACKING, Model Organisms, SKELETAL, medicine, Beta-actin, Animals, Yolk sac, ZINC-FINGER GENE, Blood Cells, GAMMA-ACTIN, lcsh:R, Biology and Life Sciences, Proteins, IN-VITRO, Molecular Development, Hematopoietic Stem Cells, Embryonic stem cell, Signaling, Actins, CELL-GROWTH, lcsh:Q, TRANSCRIPTION FACTOR GATA-2, Developmental Biology

Abstract

The functions of actin family members during development are poorly understood. To investigate the role of beta-actin in mammalian development, a beta-actin knockout mouse model was used. Homozygous beta-actin knockout mice are lethal at embryonic day (E)10.5. At E10.25 beta-actin knockout embryos are growth retarded and display a pale yolk sac and embryo proper that is suggestive of altered erythropoiesis. Here we report that lack of beta-actin resulted in a block of primitive and definitive hematopoietic development. Reduced levels of Gata2, were associated to this phenotype. Consistently, ChIP analysis revealed multiple binding sites for beta-actin in the Gata2 promoter. Gata2 mRNA levels were almost completely rescued by expression of an erythroid lineage restricted ROSA26-promotor based GATA2 transgene. As a result, erythroid differentiation was restored and the knockout embryos showed significant improvement in yolk sac and embryo vascularization. These results provide new molecular insights for a novel function of beta-actin in erythropoiesis by modulating the expression levels of Gata2 in vivo. © 2013 Tondeleir et al., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2013

13. Vegf regulates embryonic erythroid development through Gata1 modulation

Author

Sonia Bartunkova, Jody J. Haigh, Napoleone Ferrara, Katharina Haigh, Kim Deswarte, Omar Nyabi, Joanna Kalucka, Hamida Hammad, Steven Goossens, Sjaak Philipsen, Ursula Klingmüller, Benjamin Drogat, Laura Gutierrez, Bart N. Lambrecht, Andras Nagy, Morvarid Farhang Ghahremani, Michael Naessens, Cell biology, and Pulmonary Medicine

Subjects

Vascular Endothelial Growth Factor A, Transgene, Cellular differentiation, Immunology, Down-Regulation, Vascular Endothelial Growth Factor A/physiology, Biology, Erythroid Cells/cytology, Biochemistry, Cell Line, chemistry.chemical_compound, Erythroid Cells, hemic and lymphatic diseases, Gene expression, GATA1 Transcription Factor, Cell Lineage, Erythropoiesis, RNA, Messenger, Transgenes, RNA, Messenger/analysis, GATA2, GATA1, Cell Differentiation, Cell Biology, Hematology, GATA2 Transcription Factor/genetics, Cell biology, GATA2 Transcription Factor, Vascular endothelial growth factor, Vascular endothelial growth factor A, GATA1 Transcription Factor/genetics, chemistry

Abstract

To determine the role of vascular endothelial growth factor (Vegf) in embryonic erythroid development we have deleted or overexpressed Vegf specifically in the erythroid lineage using the EpoR-iCre transgenic line in combination with Cre/loxP conditional gain and loss of function Vegf alleles. ROSA26 promoter-based expression of the Vegf164 isoform in the early erythroid lineage resulted in a differentiation block of primitive erythroid progenitor (EryP) development and a partial block in definitive erythropoiesis between the erythroid burst-forming unit and erythroid colony-forming unit stages. Decreased mRNA expression levels of the key erythroid transcription factor Gata1 were causally linked to this phenotype. Conditional deletion of Vegf within the erythroid lineage was associated with increased Gata1 levels and increased erythroid differentiation. Expression of a ROSA26-based GATA2 transgene rescued Gata1 mRNA levels and target genes and restored erythroid differentiation in our Vegf gain of function model. These results demonstrate that Vegf modulates Gata1 expression levels in vivo and provides new molecular insight into Vegf's ability to modulate erythropoiesis.

Published

2010

14. Efficient mouse transgenesis using Gateway-compatible ROSA26 locus targeting vectors and F1 hybrid ES cells

Author

Mansour Karimi, Ilse De Vos, Pierre Hilson, Lieven Haenebalcke, Agnieszka Gembarska, Steven Goossens, Bram De Craene, Sarah De Clercq, András D Nagy, Jean-Christophe Marine, Benjamin Drogat, Sonia Bartunkova, Jody J. Haigh, Omar Nyabi, Geert Berx, Michael Naessens, Marion M. Maetens, and Katharina Haigh

Subjects

Genetically modified mouse, Génétique du développement, Génétique moléculaire, RNA, Untranslated, Transgene, Biochimie, Acides nucléiques, synthèse des protéines, Gene Targeting -- methods, Genetic Vectors, Biotechnologie, Biologie générale, Sciences de la matière vivante, Cloning, Molecular -- methods, Mice, Transgenic, Computational biology, Biology, Hybrid Cells, Cell Line, Proteins -- genetics, Mice, Complementary DNA, Genetics, Animals, Transgenes, Cloning, Molecular, Gene, Embryonic Stem Cells, Alleles, Cloning, Recombination, Genetic, Histologie, Gene targeting, Proteins, Biologie moléculaire, Embryonic stem cell, Diploidy, Transgenesis, Cancérologie, Génétique, cytogénétique, Gene Targeting, Methods Online, Biologie cellulaire, Génétique cellulaire, Biologie, Embryonic Stem Cells -- metabolism, Embryologie [animale]

Abstract

The ability to rapidly and efficiently generate reliable Cre/loxP conditional transgenic mice would greatly complement global high-throughput gene targeting initiatives aimed at identifying gene function in the mouse. We report here the generation of Cre/loxP conditional ROSA26-targeted ES cells within 3-4 weeks by using Gateway cloning to build the target vectors. The cDNA of the gene of interest can be expressed either directly by the ROSA26 promoter providing a moderate level of expression or by a CAGG promoter placed in the ROSA26 locus providing higher transgene expression. Utilization of F1 hybrid ES cells with exceptional developmental potential allows the production of germ line transmitting, fully or highly ES cell-derived mice by aggregation of cells with diploid embryos. The presented streamlined procedures accelerate the examination of phenotypical consequences of transgene expression. It also provides a unique tool for comparing the biological activity of polymorphic or splice variants of a gene, or products of different genes functioning in the same or parallel pathways in an overlapping manner., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2009

15. Cardiac and extracardiac expression of Csx/Nkx2.5 homeodomain protein

Author

Seigo Izumo, Martina Schinke, Makoto Tanaka, Hideko Kasahara, and Sonia Bartunkova

Subjects

medicine.medical_specialty, Physiology, Gestational Age, Biology, Cross Reactions, Homeobox protein Nkx-2.5, Mice, Tongue, Tinman gene, Internal medicine, Gene expression, medicine, Myocyte, Animals, Tissue Distribution, Fluorescent Antibody Technique, Indirect, In Situ Hybridization, Homeodomain Proteins, Heart development, Myocardium, Stomach, Days post coitum, Antibodies, Monoclonal, Heart, Cell biology, Endocrinology, Animals, Newborn, Liver, embryonic structures, Mesoderm formation, COS Cells, Homeobox Protein Nkx-2.5, Homeobox, Pharynx, Larynx, Cardiology and Cardiovascular Medicine, Spleen, Transcription Factors

Abstract

Abstract — Csx/Nkx2.5 is an evolutionary conserved homeobox gene related to the Drosophila tinman gene, which is essential for the dorsal mesoderm formation. Expression of Csx/Nkx2.5 mRNA is the earliest marker for heart precursor cells in all vertebrates so far examined. Previous studies have demonstrated that Csx/Nkx2.5 mRNA is highly expressed in the heart and at lower levels in the spleen, tongue, stomach, and thyroid in the murine embryo. Since some developmental genes are regulated by posttranscriptional mechanisms, we analyzed the developmental pattern of Csx protein expression at the single-cell level using Csx-specific antibodies. Immunohistochemical analysis of murine embryos at 7.8 days post coitum revealed that Csx protein is strongly expressed in the nucleus of endodermal and mesodermal cells in the cardiogenic plate. Subsequently, in the heart, Csx protein was detected only in the nucleus of myocytes of the atrium and the ventricle through the adult stage. During the fetal period, Csx protein expression in the nucleus was also noted in the spleen, stomach, liver, tongue, and anterior larynx. Unexpectedly, confocal microscopy revealed that Csx immunoreactivity was detected only in the cytoplasm of a subset of cranial skeletal muscles. Csx protein was not detected in the thyroid glands. The expression of Csx protein in all organs was markedly downregulated after birth except in the heart. These results raise the possibility that Csx/Nkx2.5 may play a role in the early developmental process of multiple tissues in addition to its role in early heart development.

Published

1998

16. Over-expression of Specific VEGF Isoforms Differentially Enhances and Patterns Bone Formation by Modulating Angiogenesis and Osteoblast Precursors

Author

Geert Carmeliet, Katharina Haigh, Sophie Torrekens, Andras Nagy, Anna Chan, Sonia Bartunkova, Jody J. Haigh, Christa Maes, and Riet Van Looveren

Subjects

Histology, medicine.anatomical_structure, Vegf isoforms, Physiology, Chemistry, Angiogenesis, Endocrinology, Diabetes and Metabolism, medicine, Over expression, Osteoblast, Bone formation, Cell biology

Published

2010

17. The ROSA26-iPSC Mouse: A Conditional, Inducible, and Exchangeable Resource for Studying Cellular (De)Differentiation

Author

Tino Hochepied, Steven Goossens, Lieven Haenebalcke, Sonia Bartunkova, Jody J. Haigh, Andras Nagy, Katharina Haigh, Pieterjan Dierickx, Jinke D’Hont, Dagmar Wirth, and Vascular Cell Biology Unit, VIB Department for Molecular Biomedical Research, Ghent University, Technologiepark 927, 9052 Zwijnaarde Ghent, Belgium.

Subjects

RNA, Untranslated, Transgene, Induced Pluripotent Stem Cells, RECOMBINATION, Mice, Transgenic, Biology, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, LOCUS, Basic Helix-Loop-Helix Transcription Factors, Transcriptional regulation, Animals, Cell Lineage, Myocytes, Cardiac, Epigenetics, Promoter Regions, Genetic, Induced pluripotent stem cell, lcsh:QH301-705.5, Gene, Alleles, Cells, Cultured, 030304 developmental biology, Genetics, 0303 health sciences, INDUCTION, Recombinase-mediated cassette exchange, Wnt signaling pathway, Biology and Life Sciences, Proteins, Cell Differentiation, Cellular Reprogramming, TIME, Cell biology, MODEL, Wnt Proteins, lcsh:Biology (General), Gene Expression Regulation, Genetic Loci, Doxycycline, Models, Animal, MESP1, Reprogramming, 030217 neurology & neurosurgery

Abstract

SUMMARY Control of cellular (de)differentiation in a temporal, cell-specific, and exchangeable manner is of paramount importance in the field of reprogramming. Here, we have generated and characterized a mouse strain that allows iPSC generation through the Cre/ loxP conditional and doxycycline/rtTA-controlled inducible expression of the OSKM reprogramming factors entirely from within the ROSA26 locus. After reprogramming, these factors can be replaced by genes of interest—for example, to enhance lineagedirected differentiation—with the use of a trapcoupled RMCE reaction. We show that, similar to ESCs, Dox-controlled expression of the cardiac transcriptional regulator Mesp1 together with Wnt inhibition enhances the generation of functional cardiomyocytes upon in vitro differentiation of such RMCE-retargeted iPSCs. This ROSA26-iPSC mouse model is therefore an excellent tool for studying both cellular reprogramming and lineage-directed differentiation factors from the same locus and will greatly facilitate the identification and ease of functional characterization of the genetic/epigenetic determinants involved in these complex processes.