14 results on '"Martin Kragl"'
Search Results
2. Deletion of the RabGAP TBC1D1 Leads to Enhanced Insulin Secretion and Fatty Acid Oxidation in Islets From Male Mice
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Torben Stermann, Eckhard Lammert, D Altenhofen, Kay Jeruschke, Tanja Schallschmidt, Christian de Wendt, D. Margriet Ouwens, Jürgen Weiss, Anna Pujol, Alexandra Chadt, Hadi Al-Hasani, G. Hege Thoresen, Tim Benninghoff, Fatima Bosch, Martin Kragl, Sandra Lebek, Carmen Weidlich, Franziska Menzel, and Ingo Rustenbeck
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Male ,0301 basic medicine ,endocrine system ,medicine.medical_specialty ,medicine.medical_treatment ,Islets of Langerhans ,Mice ,03 medical and health sciences ,Endocrinology ,Insulin-Secreting Cells ,Internal medicine ,medicine ,Animals ,Insulin ,Secretion ,Beta oxidation ,Mice, Knockout ,geography ,geography.geographical_feature_category ,Chemistry ,Pancreatic islets ,Fatty Acids ,GTPase-Activating Proteins ,Skeletal muscle ,Lipid metabolism ,Lipid Metabolism ,Islet ,030104 developmental biology ,medicine.anatomical_structure ,Mitochondrial fission - Abstract
The Rab guanosine triphosphatase-activating protein (RabGAP) TBC1D1 has been shown to be a key regulator of glucose and lipid metabolism in skeletal muscle. Its function in pancreatic islets, however, is not yet fully understood. Here, we aimed to clarify the specific impact of TBC1D1 on insulin secretion and substrate use in pancreatic islets. We analyzed the dynamics of glucose-stimulated insulin secretion (GSIS) and lipid metabolism in isolated islets from Tbc1d1-deficient (D1KO) mice. To further investigate the underlying cellular mechanisms, we conducted pharmacological studies in these islets. In addition, we determined morphology and number of both pancreatic islets and insulin vesicles in β-cells using light and transmission electron microscopy. Isolated pancreatic islets from D1KO mice exhibited substantially increased GSIS compared with wild-type (WT) controls. This was attributed to both enhanced first and second phase of insulin secretion, and this enhanced secretion persisted during repetitive glucose stimuli. Studies with sulfonylureas or KCl in isolated islets demonstrated that TBC1D1 exerts its function via a signaling pathway at the level of membrane depolarization. In line, ultrastructural analysis of isolated pancreatic islets revealed both higher insulin-granule density and number of docked granules in β-cells from D1KO mice compared with WT controls. Like in skeletal muscle, lipid use in isolated islets was enhanced upon D1KO, presumably as a result of a higher mitochondrial fission rate and/or higher mitochondrial activity. Our results clearly demonstrate a dual role of TBC1D1 in controlling substrate metabolism of the pancreatic islet.
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- 2018
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3. Determination of Postprandial Glycemic Responses by Continuous Glucose Monitoring in a Real-World Setting
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Tobias Martin, Martin Kragl, Martin Röhling, Stephan Martin, Kerstin Kempf, Lutz Heinemann, M Wonnemann, and H. H. Klein
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Adult ,Blood Glucose ,Male ,0301 basic medicine ,medicine.medical_specialty ,Blood sugar ,lcsh:TX341-641 ,030209 endocrinology & metabolism ,Article ,03 medical and health sciences ,0302 clinical medicine ,Internal medicine ,Dietary Carbohydrates ,medicine ,Humans ,Blood Glucose Measurement ,Glycemic ,Whole Grains ,Nutrition and Dietetics ,business.industry ,Blood Glucose Self-Monitoring ,Area under the curve ,Bread ,Venous blood ,Middle Aged ,Postprandial Period ,Healthy Volunteers ,Glucose ,030104 developmental biology ,Endocrinology ,Postprandial ,Blood chemistry ,Glycemic Index ,Area Under Curve ,Female ,continuous glucose monitoring ,business ,lcsh:Nutrition. Foods and food supply ,Body mass index ,postprandial glucose response ,Food Science - Abstract
Background: Self-monitoring of blood glucose using capillary glucose testing (C) has a number of shortcomings compared to continuous glucose monitoring (CGM). We aimed to compare these two methods and used blood glucose measurements in venous blood (IV) as a reference. Postprandial blood glucose levels were measured after 50 g oral glucose load and after the consumption of a portion of different foods containing 50 g of carbohydrates. We also evaluated the associations between postprandial glucose responses and the clinical characteristics of the participants at the beginning of the study. Methods: 12 healthy volunteers (age: 36 ±, 17 years, BMI: 24.9 ±, 3.5 kg/m², ) ate white bread (WB) and whole grain (WG) bread and drank a 50 g glucose drink as reference. Postprandial glucose responses were evaluated by CGM, IV and C blood glucose measurements. Incremental area under the curve (AUCi) of postprandial blood glucose was calculated for 1 h (AUCi 0-60) and 2 h (AUCi 0-120). Results: After the consumption of white bread and whole grain bread, the AUCi 0-60 min did not differ between CGM and IV or C. AUCi 0-120 min of CGM showed no difference compared to C. Correlation analyses revealed a positive association of age with glucose AUCi 0-120 (r = 0.768, P = 0.004) and WG AUCi 0-120 (r = 0.758, P = 0.004), fasting blood glucose correlated with WG AUCi 0-120 (r = 0.838, P <, 0.001). Conclusion: Despite considerable inter-individual variability of postprandial glycemic responses, CGM evaluated postprandial glycemic excursions which had comparable results compared to standard blood glucose measurements under real-life conditions. Associations of AUCi 0-60 and AUCi 0-120 postprandial glucose response with age or fasting blood glucose could be shown.
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- 2019
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4. Muscle and connective tissue progenitor populations show distinct Twist1 and Twist3 expression profiles during axolotl limb regeneration
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Elly M. Tanaka, Kiyokazu Agata, Yuka Taniguchi, Kathleen Roensch, Martin Kragl, Ina Nüsslein, Akira Tazaki, Tetsutaro Hayashi, and Hiroshi Tarui
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Cell type ,animal structures ,Cellular differentiation ,Polymerase Chain Reaction ,Mesoderm ,Limb bud ,Axolotl ,Limb development ,Animals ,Regeneration ,Cell Lineage ,Progenitor cell ,Muscle, Skeletal ,Molecular Biology ,In Situ Hybridization ,Connective Tissue Cells ,Skin ,Genetics ,biology ,Stem Cells ,Twist-Related Protein 1 ,Extremities ,Cell Biology ,biology.organism_classification ,Cell biology ,Ambystoma mexicanum ,body regions ,Connective tissue metabolism ,Connective Tissue ,Transcriptome ,Blastema ,Developmental Biology - Abstract
Limb regeneration involves re-establishing a limb development program from cells within adult tissues. Identifying molecular handles that provide insight into the relationship between cell differentiation status and cell lineage is an important step to study limb blastema cell formation. Here, using single cell PCR, focusing on newly isolated Twist1 sequences, we molecularly profile axolotl limb blastema cells using several progenitor cell markers. We link their molecular expression profile to their embryonic lineage via cell tracking experiments. We use in situ hybridization to determine the spatial localization and extent of overlap of different markers and cell types. Finally, we show by single cell PCR that the mature axolotl limb harbors a small but significant population of Twist1(+) cells.
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- 2013
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5. Cells keep a memory of their tissue origin during axolotl limb regeneration
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Eugen Nacu, Malcolm Maden, Hans H. Epperlein, Shahryar Khattak, Martin Kragl, Elly M. Tanaka, and Dunja Knapp
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animal structures ,Transgene ,Cell ,Ambystoma ,Regenerative medicine ,Animals, Genetically Modified ,Tendons ,Cell Movement ,Axolotl ,medicine ,Animals ,Regeneration ,Cell Lineage ,Progenitor cell ,Ambystoma mexicanum ,Multidisciplinary ,biology ,Muscles ,Regeneration (biology) ,fungi ,Cell Differentiation ,Extremities ,Anatomy ,biology.organism_classification ,Cell biology ,body regions ,Cartilage ,medicine.anatomical_structure ,Epidermal Cells ,Organ Specificity ,Schwann Cells ,Blastema - Abstract
During limb regeneration adult tissue is converted into a zone of undifferentiated progenitors called the blastema that reforms the diverse tissues of the limb. Previous experiments have led to wide acceptance that limb tissues dedifferentiate to form pluripotent cells. Here we have reexamined this question using an integrated GFP transgene to track the major limb tissues during limb regeneration in the salamander Ambystoma mexicanum (the axolotl). Surprisingly, we find that each tissue produces progenitor cells with restricted potential. Therefore, the blastema is a heterogeneous collection of restricted progenitor cells. On the basis of these findings, we further demonstrate that positional identity is a cell-type-specific property of blastema cells, in which cartilage-derived blastema cells harbour positional identity but Schwann-derived cells do not. Our results show that the complex phenomenon of limb regeneration can be achieved without complete dedifferentiation to a pluripotent state, a conclusion with important implications for regenerative medicine.
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- 2009
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6. Sheep primary cells as in vitro models to investigate Mycoplasma agalactiae host cell interactions
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Shrilakshmi, Hegde, Cordula, Gabriel, Martin, Kragl, and Rohini, Chopra-Dewasthaly
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Sheep ,Short Communication ,Epithelial Cells ,ruminant mycoplasmosis ,invasion ,Models, Biological ,Mycoplasma agalactiae ,adhesion ,Host-Pathogen Interactions ,immunohistochemistry ,Animals ,Mycoplasma Infections ,Stromal Cells ,Cells, Cultured ,primary cell culture ,host cell interactions - Abstract
Appropriate infection models are imperative for the understanding of pathogens like mycoplasmas that are known for their strict host and tissue specificity, and lack of suitable cell and small animal models has hindered pathogenicity studies. This is particularly true for the economically important group of ruminant mycoplasmas whose virulence factors need to be elucidated for designing effective intervention strategies. Mycoplasma agalactiae serves as a useful role model especially because it is phylogenetically very close to M. bovis and causes similar symptoms by as yet unknown mechanisms. Here, we successfully prepared and characterized four different primary sheep cell lines, namely the epithelial and stromal cells from the mammary gland and uterus, respectively. Using immunohistochemistry, we identified vimentin and cytokeratin as specific markers to confirm the typical cell phenotypes of these primary cells. Furthermore, M. agalactiae’s consistent adhesion and invasion into these primary cells proves the reliability of these cell models. Mimicking natural infections, mammary epithelial and stromal cells showed higher invasion and adhesion rates compared to the uterine cells as also seen via double immunofluorescence staining. Altogether, we have generated promising in vitro cell models to study host–pathogen interactions of M. agalactiae and related ruminant pathogens in a more authentic manner., The study is an important step forward in developing in vitro models that will facilitate analyses of Mycoplasma agalactiae and related ruminant mycoplasmas' host–pathogen interactions at the molecular level., Graphical Abstract Figure. The study is an important step forward in developing in vitro models that will facilitate analyses of Mycoplasma agalactiae and related ruminant mycoplasmas' host–pathogen interactions at the molecular level.
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- 2015
7. Characterization of pancreatic NMDA receptors as possible drug targets for diabetes treatment
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Jan Eglinger, Maša Skelin Klemen, Olaf Kletke, Eckhard Lammert, Daniel Eberhard, Alena Welters, Silke Otter, Martin Köhler, Stephan Wnendt, Nikolaj Klöcker, Annelie Fischer, Jorge Ferrer, Tim Heise, Diran Herebian, Ertan Mayatepek, Thomas Meissner, Lorenzo Piemonti, Andraž Stožer, Freimut Schliess, Martin Kragl, Bernard Thorens, Per Olof Berggren, Marjan Slak Rupnik, Alin Stirban, Jan Marquard, Marquard, Jan, Otter, Silke, Welters, Alena, Stirban, Alin, Fischer, Annelie, Eglinger, Jan, Herebian, Diran, Kletke, Olaf, Klemen, MaÅ¡a Skelin, Stoå¾er, Andraå, Wnendt, Stephan, Piemonti, Lorenzo, Kã¶hler, Martin, Ferrer, Jorge, Thorens, Bernard, Schliess, Freimut, Rupnik, Marjan Slak, Heise, Tim, Berggren, Per Olof, Klã¶cker, Nikolaj, Meissner, Thoma, Mayatepek, Ertan, Eberhard, Daniel, Kragl, Martin, Lammert, Eckhard, and Pathology/molecular and cellular medicine
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Male ,endocrine system diseases ,medicine.medical_treatment ,Dextromethorphan ,Mice ,Dextrorphan ,Insulin-Secreting Cells ,Pancrea ,Insulin ,Mice, Knockout ,Glucose tolerance test ,geography.geographical_feature_category ,medicine.diagnostic_test ,Research Support, Non-U.S. Gov't ,Medicine (all) ,General Medicine ,Middle Aged ,Islet ,3. Good health ,medicine.anatomical_structure ,Peptide ,Female ,medicine.drug ,Human ,Adult ,endocrine system ,medicine.medical_specialty ,Cell Survival ,Nerve Tissue Proteins ,Receptors, N-Methyl-D-Aspartate ,General Biochemistry, Genetics and Molecular Biology ,Cell Line ,Islets of Langerhans ,Research Support, N.I.H., Extramural ,Internal medicine ,Diabetes mellitus ,Journal Article ,medicine ,Animals ,Humans ,Pancreas ,geography ,Biochemistry, Genetics and Molecular Biology (all) ,business.industry ,Animal ,Venoms ,Pancreatic islets ,Type 2 Diabetes Mellitus ,Islets of Langerhan ,Glucose Tolerance Test ,medicine.disease ,Venom ,Mice, Inbred C57BL ,Disease Models, Animal ,Endocrinology ,Glucose ,nervous system ,Diabetes Mellitus, Type 2 ,Insulin-Secreting Cell ,Drug Design ,Nerve Tissue Protein ,Exenatide ,Calcium ,business ,Peptides - Abstract
In the nervous system, NMDA receptors (NMDARs) participate in neurotransmission and modulate the viability of neurons. In contrast, little is known about the role of NMDARs in pancreatic islets and the insulin-secreting beta cells whose functional impairment contributes to diabetes mellitus. Here we found that inhibition of NMDARs in mouse and human islets enhanced their glucose-stimulated insulin secretion (GSIS) and survival of islet cells. Further, NMDAR inhibition prolonged the amount of time that glucose-stimulated beta cells spent in a depolarized state with high cytosolic Ca(2+) concentrations. We also noticed that, in vivo, the NMDAR antagonist dextromethorphan (DXM) enhanced glucose tolerance in mice, and that in vitro dextrorphan, the main metabolite of DXM, amplified the stimulatory effect of exendin-4 on GSIS. In a mouse model of type 2 diabetes mellitus (T2DM), long-term treatment with DXM improved islet insulin content, islet cell mass and blood glucose control. Further, in a small clinical trial we found that individuals with T2DM treated with DXM showed enhanced serum insulin concentrations and glucose tolerance. Our data highlight the possibility that antagonists of NMDARs may provide a useful adjunct treatment for diabetes.
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- 2014
8. The biomechanical properties of an epithelial tissue determine the location of its vasculature
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Eckhard Lammert, Kay Jeruschke, Silke Otter, Chunguang Chen, Stephan Speier, Oliver Kuss, Martin Kragl, Haiko Karsjens, Daniel Eberhard, Rajib Schubert, Daniel J. Müller, Jürgen Weiss, David Alsteens, Barbara Bartosinska, and UCL - SST/ISV - Institut des sciences de la vie
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Male ,Vascular Endothelial Growth Factor A ,0301 basic medicine ,Science ,Neovascularization, Physiologic ,General Physics and Astronomy ,Protein Serine-Threonine Kinases ,Biology ,Article ,Basement Membrane ,Epithelium ,General Biochemistry, Genetics and Molecular Biology ,Neovascularization ,Islets of Langerhans ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Glucose Intolerance ,Insulin Secretion ,Cell Adhesion ,medicine ,Animals ,Insulin ,Mice, Knockout ,Basement membrane ,geography ,Multidisciplinary ,geography.geographical_feature_category ,Pancreatic islets ,Endothelial Cells ,Epithelial Cells ,Actomyosin ,General Chemistry ,Islet ,Biomechanical Phenomena ,Cell biology ,Mice, Inbred C57BL ,Endothelial stem cell ,Vascular endothelial growth factor A ,030104 developmental biology ,medicine.anatomical_structure ,Immunology ,Female ,medicine.symptom ,Cell adhesion ,Angiogenesis ,030217 neurology & neurosurgery ,Blood vessel - Abstract
An important question is how growing tissues establish a blood vessel network. Here we study vascular network formation in pancreatic islets, endocrine tissues derived from pancreatic epithelium. We find that depletion of integrin-linked kinase (ILK) in the pancreatic epithelial cells of mice results in glucose intolerance due to a loss of the intra-islet vasculature. In turn, blood vessels accumulate at the islet periphery. Neither alterations in endothelial cell proliferation, apoptosis, morphology, Vegfa expression and VEGF-A secretion nor ‘empty sleeves’ of vascular basement membrane are found. Instead, biophysical experiments reveal that the biomechanical properties of pancreatic islet cells, such as their actomyosin-mediated cortex tension and adhesive forces to endothelial cells, are significantly changed. These results suggest that a sorting event is driving the segregation of endothelial and epithelial cells and indicate that the epithelial biomechanical properties determine whether the blood vasculature invades or envelops a growing epithelial tissue., Nature Communications, 7, ISSN:2041-1723
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- 2016
9. Calcineurin/NFATc signaling: role in postnatal β cell development and diabetes mellitus
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Martin Kragl and Eckhard Lammert
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medicine.medical_specialty ,Cell growth ,Pancreatic islets ,Enteroendocrine cell ,Cell Biology ,Cell cycle ,Biology ,medicine.disease ,General Biochemistry, Genetics and Molecular Biology ,Article ,Serine ,Calcineurin ,Endocrinology ,medicine.anatomical_structure ,Internal medicine ,Diabetes mellitus ,medicine ,Molecular Biology ,Gene ,Developmental Biology - Abstract
Little is known about the mechanisms governing neonatal growth and maturation of organs. Here we demonstrate that calcineurin/Nuclear Factor of Activated T cells (Cn/NFAT) signaling regulates neonatal pancreatic development in mouse and human islets. Inactivation of calcineurin b1 (Cnb1) in mouse islets impaired dense core granule biogenesis, decreased insulin secretion, and reduced cell proliferation and mass, culminating in lethal diabetes. Pancreatic β cells lacking Cnb1 failed to express genes revealed to be direct NFAT targets required for replication, insulin storage, and secretion. In contrast, glucokinase activation stimulated Cn-dependent expression of these genes. Calcineurin inhibitors, such as tacrolimus, used for human immunosuppression, induce diabetes. Tacrolimus exposure reduced Cn/NFAT-dependent expression of factors essential for insulin dense core granule formation and secretion and neonatal β cell proliferation, consistent with our genetic studies. Discovery of conserved pathways regulating β cell maturation and proliferation suggests new strategies for controlling β cell growth or replacement in human islet diseases.
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- 2012
10. Novel insights into the flexibility of cell and positional identity during urodele limb regeneration
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Eugeniu Nacu, Elly M. Tanaka, Dunja Knapp, Martin Kragl, Hans-Henning Epperlein, Shahryar Khattak, and Esther Schnapp
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Flexibility (anatomy) ,Body Patterning ,Cell ,Urodela ,Tretinoin ,Choristoma ,Biochemistry ,Epithelium ,biology.animal ,Genetics ,medicine ,Animals ,Regeneration ,Peripheral Nerves ,Molecular Biology ,Wound Healing ,biology ,Regeneration (biology) ,Vertebrate ,Extremities ,Anatomy ,Adult Stem Cells ,medicine.anatomical_structure ,Salamander ,Stem cell ,Wound healing ,Neuroscience - Abstract
The ability of diverse metazoans to regenerate whole-body structures was first described systematically by Spallanzani in 1768 and continues to fascinate biologists today. Given the current interest in stem cell biology and its therapeutic potential, examples of vertebrate regeneration garner strong interest. Among regeneration-competent vertebrates such as the fish, frog, and salamander, the salamander is particularly impressive because it can regenerate the entire limb and tail as well as various internal organs as an adult (Goss 1969). This spectacular natural phenomenon leads us to ask what cellular properties allow regeneration and what prevents this phenomenon in other vertebrates. From this perspective, it is imperative to know whether the stem cells in regenerating limbs harbor particularly special traits such as a higher plasticity in cell fate compared to tissue stem cells in other organisms. Flexibility in cell fate needs to be considered with respect not only to tissue identity, but also to patterning because limb amputation causes cells in a particular limb segment to form more distal limb elements. How positional identity is encoded in stem cells and how it is controlled to produce only the missing portion of the limb are also questions of fundamental importance.
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- 2008
11. Hedgehog signaling controls dorsoventral patterning, blastema cell proliferation and cartilage induction during axolotl tail regeneration
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Lee L. Rubin, Elly M. Tanaka, Martin Kragl, and Esther Schnapp
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Patched Receptors ,Tail ,medicine.medical_specialty ,animal structures ,Cyclopamine ,PAX6 Transcription Factor ,Receptors, Cell Surface ,Biology ,Ambystoma ,chemistry.chemical_compound ,Internal medicine ,medicine ,Animals ,Paired Box Transcription Factors ,Regeneration ,Hedgehog Proteins ,Sonic hedgehog ,Eye Proteins ,Molecular Biology ,Floor plate ,Body Patterning ,Cell Proliferation ,Homeodomain Proteins ,MSX1 Transcription Factor ,Regeneration (biology) ,Neural tube ,High Mobility Group Proteins ,PAX7 Transcription Factor ,SOX9 Transcription Factor ,Hedgehog signaling pathway ,Cell biology ,Repressor Proteins ,Somite ,medicine.anatomical_structure ,Endocrinology ,Cartilage ,chemistry ,Spinal Cord ,biology.protein ,Trans-Activators ,Blastema ,Developmental Biology ,Signal Transduction ,Transcription Factors - Abstract
Tail regeneration in urodeles requires the coordinated growth and patterning of the regenerating tissues types, including the spinal cord,cartilage and muscle. The dorsoventral (DV) orientation of the spinal cord at the amputation plane determines the DV patterning of the regenerating spinal cord as well as the patterning of surrounding tissues such as cartilage. We investigated this phenomenon on a molecular level. Both the mature and regenerating axolotl spinal cord express molecular markers of DV progenitor cell domains found during embryonic neural tube development, including Pax6, Pax7 and Msx1. Furthermore, the expression of Sonic hedgehog (Shh) is localized to the ventral floor plate domain in both mature and regenerating spinal cord. Patched1 receptor expression indicated that hedgehog signaling occurs not only within the spinal cord but is also transmitted to the surrounding blastema. Cyclopamine treatment revealed that hedgehog signaling is not only required for DV patterning of the regenerating spinal cord but also had profound effects on the regeneration of surrounding, mesodermal tissues. Proliferation of tail blastema cells was severely impaired, resulting in an overall cessation of tail regeneration, and blastema cells no longer expressed the early cartilage marker Sox9. Spinal cord removal experiments revealed that hedgehog signaling, while required for blastema growth is not sufficient for tail regeneration in the absence of the spinal cord. By contrast to the cyclopamine effect on tail regeneration, cyclopamine-treated regenerating limbs achieve a normal length and contain cartilage. This study represents the first molecular localization of DV patterning information in mature tissue that controls regeneration. Interestingly, although tail regeneration does not occur through the formation of somites, the Shh-dependent pathways that control embryonic somite patterning and proliferation may be utilized within the blastema,albeit with a different topography to mediate growth and patterning of tail tissues during regeneration.
- Published
- 2005
12. Vitamin B2 (riboflavin) and a mixture of vitamin B2 and C affects MMC efficiency in aerated media under irradiation
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Linda, Fuga, Martin, Kragl, and Nikola, Getoff
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Oxygen ,Gamma Rays ,Mitomycin ,Riboflavin ,Escherichia coli ,Drug Synergism ,Radiation-Protective Agents ,Ascorbic Acid ,Reactive Oxygen Species ,Oxidation-Reduction ,Peroxides - Abstract
Vitamin B2 (Riboflavin) acts as a strong radiation protecting agent in Escherichia coli bacteria (AB1157) in aerated media. This ability is reinforced by the addition of vitamin C. Under the influence of gamma-radiation, vitamin B2 completely suppresses the cytostatic activity of mitomycin C (MMC). In the presence of both vitamins, B2 and C, MMC is converted from an efficient cytostatic to a rather strong radiation protecting agent. This effect opens a new pathway for specific protection of normal mammalian cells (with a high O2-content) under treatment with ionizing radiation.
- Published
- 2005
13. 19-P015 Plasticity of cells during axolotl limb regeneration
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Andrea Merseburg, Elly M. Tanaka, Dunja Knapp, Martin Kragl, Shahryar Khattak, Eugen Nacu, Malcolm Maden, and Hans H. Epperlein
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Embryology ,biology ,Axolotl ,Anatomy ,Plasticity ,biology.organism_classification ,Neuroscience ,Developmental Biology - Published
- 2009
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14. NMDA receptor dependent anti-diabetic effects
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Barbara Bartosinska, Alena Welters, Eckhard Lammert, Annett Schroeter, Maša Skelin Klemen, Silke Otter, Jan Marquard, Nikolaj Klöcker, Martin Köhler, Fatih Demir, Daniel Eberhard, Diran Herebian, Andraz Stozer, Stephan Wnendt, Alin Stirban, Per Olof Berggren, Marjan Slak Rupnik, Freimut Schliess, Thomas Meissner, Tim Heise, Ertan Mayatepek, Martin Kragl, and Olaf Kletke
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medicine.medical_specialty ,Endocrinology ,business.industry ,Internal medicine ,Meeting Abstract ,medicine ,NMDA receptor ,AMPA receptor ,Hypoglycemia ,Bioinformatics ,Insulin secretion ,medicine.disease ,business - Abstract
NMDA receptor dependent anti-diabetic effects Jan Marquard, Silke Otter, Alena Welters, Diran Herebian, Fatih Demir, Annett Schroeter, Olaf Kletke, Martin Kragl, Daniel Eberhard, Barbara Bartosinska, Masa Skelin Klemen, Andraz Stozer, Martin Kohler, Alin Stirban, Freimut Schliess, Tim Heise, Stephan Wnendt, Marjan Slak Rupnik, Per-Olof Berggren, Nikolaj Klocker, Thomas Meissner, Ertan Mayatepek, Eckhard Lammert
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