Your search keyword '"Berit Genz"' showing total 25 results

1. Therapeutic potential of macrophage colony-stimulating factor in chronic liver disease

Author

Sahar Keshvari, Berit Genz, Ngari Teakle, Melanie Caruso, Michelle F. Cestari, Omkar L. Patkar, Brian W. C. Tse, Kamil A. Sokolowski, Hilmar Ebersbach, Julia Jascur, Kelli P. A. MacDonald, Gregory Miller, Grant A. Ramm, Allison R. Pettit, Andrew D. Clouston, Elizabeth E. Powell, David A. Hume, and Katharine M. Irvine

Subjects

chronic liver disease, liver regeneration, fibrosis resolution, inflammation, macrophages, thioacetamide, mouse, Medicine, Pathology, RB1-214

Abstract

Resident and recruited macrophages control the development and proliferation of the liver. We have previously shown in multiple species that treatment with a macrophage colony stimulating factor (CSF1)-Fc fusion protein initiated hepatocyte proliferation and promoted repair in models of acute hepatic injury in mice. Here, we investigated the impact of CSF1-Fc on resolution of advanced fibrosis and liver regeneration, using a non-resolving toxin-induced model of chronic liver injury and fibrosis in C57BL/6J mice. Co-administration of CSF1-Fc with exposure to thioacetamide (TAA) exacerbated inflammation consistent with monocyte contributions to initiation of pathology. After removal of TAA, either acute or chronic CSF1-Fc treatment promoted liver growth, prevented progression and promoted resolution of fibrosis. Acute CSF1-Fc treatment was also anti-fibrotic and pro-regenerative in a model of partial hepatectomy in mice with established fibrosis. The beneficial impacts of CSF1-Fc treatment were associated with monocyte-macrophage recruitment and increased expression of remodelling enzymes and growth factors. These studies indicate that CSF1-dependent macrophages contribute to both initiation and resolution of fibrotic injury and that CSF1-Fc has therapeutic potential in human liver disease.

Published

2022

2. Protein z exerts pro-angiogenic effects and upregulates CXCR4.

Author

Antje Butschkau, Nana-Maria Wagner, Berit Genz, and Brigitte Vollmar

Subjects

Medicine, Science

Abstract

Protein Z (PZ) is a vitamin K-dependent coagulation factor without catalytic activity. Evidence points towards PZ as an independent risk factor for the occurrence of human peripheral arterial disease. However, the role of PZ in ischemia-driven angiogenesis and vascular healing processes has not been elucidated so far.Angiogenic potency of PZ was assessed in established in vitro assays using endothelial cells. PZ-deficient (PZ(-/-)) mice and their wild-type littermates (PZ(+/+)) were subjected to hindlimb ischemia. Furthermore, PZ(-/-) mice were exposed to PZ expressing adenovirus (AdV-PZ) or control adenovirus (AdV-GFP). In an additional set of animals, PZ(-/-) mice were exposed to AdV-PZ and AdV-GFP, each in combination with the CXCR4 antagonist AMD3100.In vitro, PZ stimulated migratory activity and capillary-like tube formation of endothelial cells comparable to SDF-1. PZ(-/-) mice exhibited diminished hypoxia-driven neovascularization and reperfusion in post-ischemic hindlimbs, which was restored by adenoviral gene transfer up to levels seen in PZ(+/+) mice. The stimulatory impact of PZ on endothelial cells in vitro was abolished by siRNA targeting against PZ and PZ was not able to restore reduced migration after knock-down of CXCR4. The increased surface expression of CXCR4 on PZ-stimulated endothelial cells and the abrogated restoration of PZ(-/-) mice via AdV-PZ after concomitant treatment with the CXCR4 antagonist AMD3100 supports the idea that PZ mediates angiogenesis via a G-protein coupled pathway and involves the SDF-1/CXCR4 axis. This is underlined by the fact that addition of the G-protein inhibitor PTX to PZ-stimulated endothelial cells abolished the effect of PZ on capillary-like tube formation.The results of the current study reveal a role of PZ in ischemia-induced angiogenesis, which involves a G-protein coupled pathway and a raised surface expression of CXCR4. Our findings thereby extend the involvement of PZ from the coagulation cascade to a beneficial modulation of vascular homeostasis.

Published

2014

3. Development of Adenoviral Delivery Systems to Target Hepatic Stellate Cells In Vivo.

Author

Julia Reetz, Berit Genz, Claudia Meier, Bhavani S Kowtharapu, Franziska Timm, Brigitte Vollmar, Ottmar Herchenröder, Kerstin Abshagen, and Brigitte M Pützer

Subjects

Medicine, Science

Abstract

Hepatic stellate cells (HSCs) are known as initiator cells that induce liver fibrosis upon intoxication or other noxes. Deactivation of this ongoing remodeling process of liver parenchyma into fibrotic tissue induced by HSCs is an interesting goal to be achieved by targeted genetic modification of HSCs. The most widely applied approach in gene therapy is the utilization of specifically targeted vectors based on Adenovirus (Ad) serotype 5. To narrow down the otherwise ubiquitous tropism of parental Ad, two modifications are required: a) ablating the native tropism and b) redirecting the vector particles towards a specific entity solely present on the cells of interest. Therefore, we designed a peptide of the nerve growth factor (NGFp) with specific affinity for the p75 neurotrophin receptor (p75NTR) present on HSCs. Coupling of this NGFp to vector particles was done either via chemical conjugation using bifunctional polyethylene glycol (PEG) or, alternatively, by molecular bridging with a fusion protein specific for viral fiber knob and p75NTR. Both Ad vectors transmit the gene for the green fluorescent protein (GFP). GFP expression was monitored in vitro on primary murine HSCs as well as after systemic administration in mice with healthy and fibrotic livers using intravital fluorescence microscopy. Coupling of NGFp to Ad via S11 and/or PEGylation resulted in markedly reduced liver tropism and an enhanced adenoviral-mediated gene transfer to HSCs. Transduction efficiency of both specific Ads was uniformly higher in fibrotic livers, whereas Ad.GFP-S11-NGFp transduce activated HSCs better than Ad.GFP-PEG-NGFp. These experiments contribute to the development of a targeted gene transfer system to specifically deliver antifibrotic compounds into activated HSCs by systemically applied adenoviral vector modified with NGFp.

Published

2013

4. Correction: Development of Adenoviral Delivery Systems to Target Hepatic Stellate Cells In Vivo.

Author

Julia Reetz, Berit Genz, Claudia Meier, Bhavani S. Kowtharapu, Franziska Timm, Brigitte Vollmar, Ottmar Herchenröder, Kerstin Abshagen, and Brigitte M. Pützer

Subjects

Medicine, Science

Published

2013

5. Comparative Evaluation of Custom TNA Extraction Buffers to Obtain High-quality TNA from Shrimp and Polychaetes

Author

Joanna Gerszon, Berit Genz, Louise Franz, Melony Jay Sellars, and Ralf Joachim Moser

Subjects

Genetics, Aquatic Science

Abstract

Selecting the appropriate lysis buffers is crucial in obtaining high-quality nucleic acids for molecular pathogen detection. In this study, we compared three in-house and one commercial lysis buffer for their effectiveness in extracting high-quality TNA from Tiger shrimp and sandworm samples. Buffer L1 outperformed the commercial counterpart, producing higher TNA concentrations and concordant PCR results for all DNA and RNA targets in the Shrimp MultiPathTM. The findings underscore the significance of selecting the right extraction buffers to achieve high-quality nucleic acids for downstream molecular applications and suggest that in-house buffers can be a viable alternative to commercial ones for difficult-to-extract tissues.

Published

2023

6. Therapeutic potential of macrophage colony-stimulating factor (CSF1) in chronic liver disease

Author

Ngari Teakle, Julia Jascur, Kamil A. Sokolowski, Allison R. Pettit, Katharine M. Irvine, Brian W.C. Tse, Hilmar Ebersbach, Omkar L. Patkar, Melanie Caruso, Gregory M. Miller, Kelli P. A. MacDonald, Sahar Keshvari, David A. Hume, Grant A. Ramm, Elizabeth E. Powell, Andrew D. Clouston, Berit Genz, and Michelle Ferrari Cestari

Subjects

Macrophage colony-stimulating factor, business.industry, Monocyte, Inflammation, medicine.disease, Chronic liver disease, Fusion protein, Liver regeneration, medicine.anatomical_structure, Fibrosis, Hepatocyte, Cancer research, Medicine, medicine.symptom, business

Abstract

Resident and recruited macrophages control the development and proliferation of the liver. We showed previously in multiple species that treatment with a macrophage colony stimulating factor (CSF1)-Fc fusion protein initiated hepatocyte proliferation and promoted repair in models of acute hepatic injury in mice. Here we investigated the impact of CSF1-Fc on resolution of advanced fibrosis and liver regeneration, utilizing a non-resolving toxin-induced model of chronic liver injury and fibrosis in C57BL/6J mice. Co-administration of CSF1-Fc with exposure to thioacetamide (TAA) exacerbated inflammation consistent with monocyte contributions to initiation of pathology. After removal of TAA, either acute or chronic CSF1-Fc treatment promoted liver growth, prevented progression and promoted resolution of fibrosis. Acute CSF1-Fc treatment was also anti-fibrotic and pro-regenerative in a model of partial hepatectomy in mice with established fibrosis. The beneficial impacts of CSF1-Fc treatment were associated with monocyte-macrophage recruitment and increased expression of remodeling enzymes and growth factors. These studies indicate that CSF1-dependent macrophages contribute to both initiation and resolution of fibrotic injury and that CSF1-Fc has therapeutic potential in human liver disease.Summary statementMacrophages contribute to both progression and resolution of chronic tissue injury and fibrogenesis. Administration of a macrophage growth factor promoted liver regeneration and resolution of advanced liver fibrosis in mice.

Published

2021

7. Liver-specific Repin1 deficiency impairs transient hepatic steatosis in liver regeneration

Author

Michael Stumvoll, Bastian Degenhardt, Marcus Frank, Kerstin Abshagen, Ute Hofmann, Anna Wendt, Berit Genz, Marie Liebig, Brigitte Vollmar, Nora Klöting, and Ute Schaeper

Subjects

0301 basic medicine, Male, medicine.medical_specialty, CD36, lcsh:Medicine, Article, 03 medical and health sciences, 0302 clinical medicine, Liver Function Tests, Internal medicine, Lipid droplet, medicine, Animals, Humans, RNA, Messenger, lcsh:Science, Cell Proliferation, Multidisciplinary, medicine.diagnostic_test, biology, Chemistry, Cell growth, Liver cell, Fatty Acids, lcsh:R, RNA-Binding Proteins, Lipid metabolism, Hep G2 Cells, medicine.disease, Lipid Metabolism, Liver regeneration, Liver Regeneration, DNA-Binding Proteins, Fatty Liver, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, Liver, Organ Specificity, biology.protein, Hepatocytes, 030211 gastroenterology & hepatology, lipids (amino acids, peptides, and proteins), lcsh:Q, Steatosis, Liver function tests, Glycogen

Abstract

Transient hepatic steatosis upon liver resection supposes functional relationships between lipid metabolism and liver regeneration. Repin1 has been suggested as candidate gene for obesity and dyslipidemia by regulating key genes of lipid metabolism and lipid storage. Herein, we characterized the regenerative potential of mice with a hepatic deletion of Repin1 (LRep1−/−) after partial hepatectomy (PH) in order to determine the functional significance of Repin1 in liver regeneration. Lipid dynamics and the regenerative response were analyzed at various time points after PH. Hepatic Repin1 deficiency causes a significantly decreased transient hepatic lipid accumulation. Defects in lipid uptake, as analyzed by decreased expression of the fatty acid transporter Cd36 and Fatp5, may contribute to attenuated and shifted lipid accumulation, accompanied by altered extent and chronological sequence of liver cell proliferation in LRep1−/− mice. In vitro steatosis experiments with primary hepatocytes also revealed attenuated lipid accumulation and occurrence of smaller lipid droplets in Repin1-deficient cells, while no direct effect on proliferation in HepG2 cells was observed. Based on these results, we propose that hepatocellular Repin1 might be of functional significance for early accumulation of lipids in hepatocytes after PH, facilitating efficient progression of liver regeneration.

Published

2018

8. Microcirculatory disturbances and cellular changes during progression of hepatic steatosis to liver tumors

Author

Kerstin Abshagen, Alireza Hassanzada, Marie Liebig, Brigitte Vollmar, Malte Kämmerling, and Berit Genz

Subjects

Male, Pathology, medicine.medical_specialty, Carcinoma, Hepatocellular, Intravital Microscopy, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Liver disease, 0302 clinical medicine, Animals, Medicine, Pathological, Original Research, Histocytochemistry, business.industry, Microcirculation, Liver Neoplasms, Fatty liver, medicine.disease, Fatty Liver, Mice, Inbred C57BL, Disease Models, Animal, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Blood Vessels, 030211 gastroenterology & hepatology, Steatosis, Metabolic syndrome, Steatohepatitis, business, Intravital microscopy

Abstract

Non-alcoholic fatty liver disease is closely associated with metabolic syndrome and comprises a pathological spectrum of liver disease ranging from steatosis to steatohepatitis and can progress to fibrosis/cirrhosis and hepatocellular carcinoma. In 2013, a mouse model was described that mimics non-alcoholic fatty liver disease progression from steatohepatitis to tumors in a short time span and with high incidence. As microcirculatory disturbances play a crucial role in liver disease, the suitability of the steatosis-inflammation-tumor model for microcirculatory studies was assessed. Herein, we present a comprehensive view on morphological, microvascular, cellular, and functional aspects of non-alcoholic fatty liver disease progression in the steatosis-inflammation-tumor model using intravital microscopy, biochemical, and histological techniques. Mice develop steatohepatitis, mild fibrosis, and liver tumors at ages of 6, 12, and 20 weeks, respectively. Non-alcoholic fatty liver disease progression was accompanied by several general aspects of disease severity like increasing liver/body weight index, non-alcoholic fatty liver disease activity score, and hepatocellular apoptosis. Intravital microscopic analysis revealed significant changes in hepatic microcirculation with increasing structural alterations, elevated leukocyte adherence, and impaired nutritive perfusion. Non-alcoholic fatty liver disease was further characterized by a lower sinusoidal density with a striking rise at 20 weeks. The characteristic microcirculatory changes make the model a convenient tool for analysis of microcirculation during progression from steatosis to liver tumor. Impact statement Significant alterations of microcirculation contribute to progression of NAFLD, a chronic liver disease with increasing medical and socio-economic impact. Characterization of microcirculation in a NAFLD model reflecting all relevant stages of disease progression was still missing. Thus, we evaluated microcirculatory and cellular changes in a steatosis-inflammation-tumor model using in vivo microscopy. Analyses revealed increasing structural alterations, elevated leukocyte-endothelial interaction, and impaired nutritive perfusion. Thus, this model is suitable for further studies investigating therapeutic approaches targeting these progressive microcirculatory disturbances.

Published

2017

9. No significant impact of Foxf1 siRNA treatment in acute and chronic CCl4 liver injury

Author

Tobias Rotberg, Brigitte Vollmar, Kerstin Abshagen, and Berit Genz

Subjects

0301 basic medicine, Liver injury, business.industry, Liver cell, Activating transcription factor, medicine.disease, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Liver disease, 030104 developmental biology, Forkhead Transcription Factors, Fibrosis, Hepatic stellate cell, Cancer research, Medicine, Gene silencing, business

Abstract

Chronic liver injury of any etiology is the main trigger of fibrogenic responses and thought to be mediated by hepatic stellate cells. Herein, activating transcription factors like forkhead box f1 are described to stimulate pro-fibrogenic genes in hepatic stellate cells. By using a liver-specific siRNA delivery system (DBTC), we evaluated whether forkhead box f1 siRNA treatment exhibit beneficial effects in murine models of acute and chronic CCl4-induced liver injury. Systemic administration of DBTC-forkhead box f1 siRNA in mice was only sufficient to silence forkhead box f1 in acute CCl4 model, but was not able to attenuate liver injury as measured by liver enzymes and necrotic liver cell area. Therapeutic treatment of mice with DBTC-forkhead box f1 siRNA upon chronic CCl4 exposition failed to inhibit forkhead box f1 expression and hence lacked to diminish hepatic stellate cells activation or fibrosis development. As a conclusion, DBTC-forkhead box f1 siRNA reduced forkhead box f1 expression in a model of acute but not chronic toxic liver injury and showed no positive effects in either of these mice models. Impact statement As liver fibrosis is a worldwide health problem, antifibrotic therapeutic strategies are urgently needed. Therefore, further developments of new technologies including validation in different experimental models of liver disease are essential. Since activation of hepatic stellate cells is a key event upon liver injury, the activating transcription factor forkhead box f1 (Foxf1) represents a potential target gene. Previously, we evaluated Foxf1 silencing by a liver-specific siRNA delivery system (DBTC), exerting beneficial effects in cholestasis. The present study was designed to confirm the therapeutic potential of Foxf1 siRNA in models of acute and chronic CCl4-induced liver injury. DBTC-Foxf1 siRNA was only sufficient to silence Foxf1 in acute CCl4 model and did not ameliorate liver injury or fibrogenesis. This underlines the significance of the experimental model used. Each model displays specific characteristics in the pathogenic nature, time course and severity of fibrosis and the optimal time point for starting a therapy.

Published

2017

10. Tolerizing CTL by sustained hepatic PD-L1 expression provides a new therapy spproach in mouse sepsis

Author

Bernhard Brüne, Andreas von Knethen, Andreas Weigert, Michael J. Parnham, Kerstin Abshagen, Florian R. Greten, Mateusz Putyrski, Brigitte M. Pützer, Laura Kuchler, Edith Hintermann, Beate Fißlthaler, Berit Genz, Lisa K. Sha, Tilo Knape, Shahzad N. Syed, Urs Christen, Anne Schäfer, Volkhard A. J. Kempf, Ajay M. Shah, Martin Schulz, Katrin Schröder, Andreas Ernst, Fabian Finkelmeier, Sandra Gunne, Michael Hogardt, Ralf P. Brandes, Marina Pesic, and Publica

Subjects

0301 basic medicine, PD-L1, T cell, Medicine (miscellaneous), Down-Regulation, liver, Lymphocyte Activation, B7-H1 Antigen, Sepsis, sepsis, 03 medical and health sciences, Mice, 0302 clinical medicine, Downregulation and upregulation, In vivo, medicine, Cytotoxic T cell, Animals, ddc:610, Pharmacology, Toxicology and Pharmaceutics (miscellaneous), Gene knockout, reactive oxygen species, Mice, Knockout, business.industry, cytotoxic T cells, Liver Diseases, 030208 emergency & critical care medicine, medicine.disease, Up-Regulation, Mice, Inbred C57BL, CTL, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Knockout mouse, Cancer research, business, Research Paper, T-Lymphocytes, Cytotoxic

Abstract

Cytotoxic T lymphocyte (CTL) activation contributes to liver damage during sepsis, but the mechanisms involved are largely unknown. Understanding the underlying principle will permit interference with CTL activation and thus, provide a new therapeutic option. Methods: To elucidate the mechanism leading to CTL activation we used the Hepa1-6 cell line in vitro and the mouse model of in vivo polymicrobial sepsis, following cecal-ligation and -puncture (CLP) in wildtype, myeloid specific NOX-2, global NOX2 and NOX4 knockout mice, and their survival as a final readout. In this in vivo setting, we also determined hepatic mRNA and protein expression as well as clinical parameters of liver damage - aspartate- and alanine amino-transaminases. Hepatocyte specific overexpression of PD-L1 was achieved in vivo by adenoviral infection and transposon-based gene transfer using hydrodynamic injection. Results: We observed downregulation of PD-L1 on hepatocytes in the murine sepsis model. Adenoviral and transposon-based gene transfer to restore PD-L1 expression, significantly improved survival and reduced the release of liver damage, as PD-L1 is a co-receptor that negatively regulates T cell function. Similar protection was observed during pharmacological intervention using recombinant PD-L1-Fc. N-acetylcysteine blocked the downregulation of PD-L1 suggesting the involvement of reactive oxygen species. This was confirmed in vivo, as we observed significant upregulation of PD-L1 expression in NOX4 knockout mice, following sham operation, whereas its expression in global as well as myeloid lineage NOX2 knockout mice was comparable to that in the wild type animals. PD-L1 expression remained high following CLP only in total NOX2 knockouts, resulting in significantly reduced release of liver damage markers. Conclusion: These results suggest that, contrary to common assumption, maintaining PD-L1 expression on hepatocytes improves liver damage and survival of mice during sepsis. We conclude that administering recombinant PD-L1 or inhibiting NOX2 activity might offer a new therapeutic option in sepsis.

Published

2019

11. Serum MicroRNAs as Biomarkers in Hepatitis C: Preliminary Evidence of a MicroRNA Panel for the Diagnosis of Hepatocellular Carcinoma

Author

Diego A. Calvopina, Anna Weis, Louise Marquart, Richard Skoien, Berit Genz, and Grant A. Ramm

Subjects

0301 basic medicine, Liver Cirrhosis, Male, Cirrhosis, Microarray, Hepacivirus, Gastroenterology, lcsh:Chemistry, 0302 clinical medicine, Fibrosis, Medicine, lcsh:QH301-705.5, Spectroscopy, Early Detection of Cancer, Liver Neoplasms, Area under the curve, General Medicine, Hepatitis C, hepatocellular carcinoma, Middle Aged, 3. Good health, Computer Science Applications, Gene Expression Regulation, Neoplastic, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Biomarker (medicine), Female, medicine.medical_specialty, Carcinoma, Hepatocellular, Catalysis, Article, Inorganic Chemistry, 03 medical and health sciences, Internal medicine, microRNA, Biomarkers, Tumor, Humans, Physical and Theoretical Chemistry, Molecular Biology, business.industry, cirrhosis, Organic Chemistry, non-invasive biomarker, medicine.disease, digestive system diseases, MicroRNAs, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, serum miRNA, business

Abstract

Early diagnosis of cirrhosis and hepatocellular carcinoma (HCC) due to chronic Hepatitis C (CHC) remain clinical priorities. In this pilot study, we assessed serum microRNA (miRNA) expression to distinguish cirrhosis and HCC, alone and in combination with the aminotransferase-to-platelet ratio (APRI), Fibrosis 4 (FIB-4), and alpha-fetoprotein (AFP). Sixty CHC patients were subdivided into 3 cohorts: Mild disease (fibrosis stage F0-2, n = 20), cirrhosis (n = 20), and cirrhosis with HCC (n = 20). Circulating miRNA signatures were determined using a liver-specific real-time quantitative reverse transcription PCR (qRT-PCR) microarray assessing 372 miRNAs simultaneously. Differentially-expressed miRNA candidates were independently validated using qRT-PCR. Serum miRNA-409-3p was increased in cirrhosis versus mild disease. In HCC versus cirrhosis, miRNA-486-5p was increased, whereas miRNA-122-5p and miRNA-151a-5p were decreased. A logistic regression model-generated panel, consisting of miRNA-122-5p + miRNA-409-3p, distinguished cirrhosis from mild disease (area under the curve, AUC = 0.80, sensitivity = 85%, specificity = 70%, p &lt, 0.001). When combined with FIB-4 or APRI, performance was improved with AUC = 0.89 (p &lt, 0.001) and 0.87 (p &lt, 0.001), respectively. A panel consisting of miRNA-122-5p + miRNA-486-5p + miRNA-142-3p distinguished HCC from cirrhosis (AUC = 0.94, sensitivity = 80%, specificity = 95%, 0.001), outperforming AFP (AUC = 0.64, p = 0.065). Serum miRNAs are differentially expressed across the spectrum of disease severity in CHC. MicroRNAs have great potential as diagnostic biomarkers in CHC, particularly in HCC where they outperform the only currently-used biomarker, AFP.

Published

2019

12. Overexpression of miRNA-25-3p inhibits Notch1 signaling and TGF-β-induced collagen expression in hepatic stellate cells

Author

Michelle M. Hill, Fares Al-Ejeh, Grant A. Ramm, Anna Weis, Jamie R. Kutasovic, John K. Olynyk, Harley Robinson, Janina E.E. Tirnitz-Parker, Miranda A. Coleman, Diego A. Calvopina, Mariska Miranda, Nicole Cloonan, Berit Genz, Katharine M. Irvine, and Francis D. Gratte

Subjects

0301 basic medicine, Liver fibrosis, Notch signaling pathway, lcsh:Medicine, Article, Cell Line, Extracellular matrix, 03 medical and health sciences, Mice, 0302 clinical medicine, Downregulation and upregulation, Transforming Growth Factor beta, microRNA, Hepatic Stellate Cells, Animals, Humans, Receptor, Notch1, Receptor, lcsh:Science, Wnt Signaling Pathway, Multidisciplinary, Chemistry, lcsh:R, Wnt signaling pathway, Cell biology, MicroRNAs, 030104 developmental biology, Mechanisms of disease, Gene Expression Regulation, Cell culture, Hepatic stellate cell, lcsh:Q, Collagen, 030217 neurology & neurosurgery

Abstract

During chronic liver injury hepatic stellate cells (HSCs), the principal source of extracellular matrix in the fibrotic liver, transdifferentiate into pro-fibrotic myofibroblast-like cells - a process potentially regulated by microRNAs (miRNAs). Recently, we found serum miRNA-25-3p (miR-25) levels were upregulated in children with Cystic Fibrosis (CF) without liver disease, compared to children with CF-associated liver disease and healthy individuals. Here we examine the role of miR-25 in HSC biology. MiR-25 was detected in the human HSC cell line LX-2 and in primary murine HSCs, and increased with culture-induced activation. Transient overexpression of miR-25 inhibited TGF-β and its type 1 receptor (TGFBR1) mRNA expression, TGF-β-induced Smad2 phosphorylation and subsequent collagen1α1 induction in LX-2 cells. Pull-down experiments with biotinylated miR-25 revealed Notch signaling (co-)activators ADAM-17 and FKBP14 as miR-25 targets in HSCs. NanoString analysis confirmed miR-25 regulation of Notch- and Wnt-signaling pathways. Expression of Notch signaling pathway components and endogenous Notch1 signaling was downregulated in miR-25 overexpressing LX-2 cells, as were components of Wnt signaling such as Wnt5a. We propose that miR-25 acts as a negative feedback anti-fibrotic control during HSC activation by reducing the reactivity of HSCs to TGF-β-induced collagen expression and modulating the cross-talk between Notch, Wnt and TGF-β signaling.

Published

2018

13. Repair of cartilage defects with devitalized osteochondral tissue: A pilot animal study

Author

Andreas Wree, Bettina Hiemer, Berit Genz, Tobias Lindner, Steffen Dommerich, Rainer Bader, Thomas Tischer, J. Ostwald, and Anika Jonitz-Heincke

Subjects

Cartilage, Articular, Materials science, Knee Joint, Tissue Scaffolds, Cartilage, Hydrostatic pressure, Biomedical Engineering, Tissue integration, Pilot Projects, Knee Injuries, X-Ray Microtomography, Matrix (biology), Biomaterials, Histological staining, medicine.anatomical_structure, Rabbit model, medicine, Animals, Animal study, Rabbits, Biomedical engineering

Abstract

Devitalization using high hydrostatic pressure (HHP) treatment inactivates cells while matrix structure and biomechanical properties are maintained. Because of strong chondroinductive potential of HHP-devitalized cartilage matrix, it may be used as scaffold for reconstruction of (osteo-)chondral lesions. In this pilot study, we evaluated the feasibility of HHP-devitalized osteochondral tissue to repair osteochondral defects in a rabbit model. Removal and reimplantation of osteochondral plugs were performed in 12 female New Zealand White rabbits. From the knee joint of each animal, osteochondral plugs (diameter = 4 mm; depth = 2.5 mm) were harvested and devitalized by HHP (452 MPa for 10 min). Afterward, the plugs were reimplanted into the respective cavity, from where they were taken. Animals were sacrificed 12 weeks postoperatively and the integration of osteochondral plugs was examined using μ-CT, MRI, and histological staining. Furthermore, revitalization of HHP-treated osteochondral plugs was characterized by gene expression analyses. Macroscopic evaluation of tissue repair at implantation sites of HHP-treated osteochondral plugs showed an adequate defect filling 12 weeks after implantation. Plug margins were hardly detectable indicating successful tissue integration. Additionally, gene expression analyses demonstrated initial revitalization of the HHP-treated tissue 12 weeks postoperatively. Our preliminary data revealed that HHP-treated osteochondral plugs could be used to refill osteochondral defects in the knee joint and promote cell migration into defect site. Data indicated that HHP-treated tissue has the potential to act as functional scaffolds for reconstruction of cartilage defects. © 2019 Wiley Periodicals, Inc. J Biomed Mater Res Part B: Appl Biomater 107B: 2354-2364, 2019.

Published

2018

14. Foxf1 siRNA Delivery to Hepatic Stellate Cells by DBTC Lipoplex Formulations Ameliorates Fibrosis in Livers of Bile Duct Ligated Mice

Author

Maria Thomas, Malte Brensel, Kira Roth, Berit Genz, Ute Schaeper, Brigitte Vollmar, Kerstin Abshagen, and Volker Fehring

Subjects

Liver Cirrhosis, Pathology, medicine.medical_specialty, Biology, Mice, Cholestasis, Fibrosis, Drug Discovery, Hepatic Stellate Cells, Genetics, medicine, Animals, Gene silencing, RNA, Small Interfering, Molecular Biology, Genetics (clinical), Liver injury, Drug Carriers, Bile duct, Liver cell, Forkhead Transcription Factors, medicine.disease, medicine.anatomical_structure, Systemic administration, Hepatic stellate cell, Cancer research, Molecular Medicine, Bile Ducts

Abstract

Activation of hepatic stellate cells (HSCs) is a key event in pathogenesis of liver fibrosis and represents an orchestral interplay of inhibiting and activating transcription factors like forkhead box f1 (Foxf1), being described to stimulate pro-fibrogenic genes in HSCs. Here, we evaluated a lipidbased liver-specific delivery system (DBTC) suitable to transfer Foxf1 siRNA specifically to HSCs and examined its antifibrotic potential on primary HSCs and LX-2 cells as well as in a murine model of bile duct ligation (BDL)-induced secondary cholestasis. Foxf1 silencing reduced proliferation capacity and attenuated contractility of HSCs. Systemic administration of DBTC-lipoplexes in mice was sufficient to specifically silence genes expressed in different liver cell types. Using intravital and immunofluorescence microscopy we confirmed the specific delivery of Cy3-labeled DBTC to the liver, and particularly to HSCs. Repeated treatment with DBTC-lipoplexes resulted in siRNA-mediated silencing of Foxf1 early after BDL and finally attenuated progression of the fibrotic process. Decreased HSC activation in-effect ameliorated liver injury as shown by substantial reduction of necrotic area and deposition of extracellular matrix. Our findings suggest that Foxf1 may serve as a target gene to disrupt progression of liver fibrosis and DBTC might provide a potentially feasible and effective tool for HSC-specific delivery of therapeutic RNA.

Published

2015

15. Contents Vol. 54/55, 2015

Author

Shoji Kubo, Andreas Pascher, Fritz Klein, Volker Fendrich, Frank J. M. F. Dor, Olivier C. Manintveld, Maria Thomas, Markus Winny, Jan N. M. IJzermans, Hiroji Shinkawa, Safak Guel, Brigitte Vollmar, Daniel Seehofer, Shigekazu Takemura, Druckerei Stückle, Eline K. van den Akker, Christian Hagl, Takayoshi Nishioka, Igor M. Sauer, Satz Mengensatzproduktion, Dominik Geiger, Johann Pratschke, Kerstin Abshagen, Ronald Wilhelm Frederik de Bruijn, Marcus Bahra, Sebastian Michel, Christoph A. Reichel, Julia Benzel, D.A. Hesselink, Bruno Reichart, Andreas Andreou, Berit Genz, René Schramm, Genya Hamano, Daniel Poehnert, J.-M. Abicht, Shogo Tanaka, Mahmoud Abbas, Juergen Klempnauer, Tokuji Ito, Masahiko Kinoshita, Benjamin Struecker, Paolo Brenner, Moritz Senne, Hans-Heinrich Kreipe, and Stefan Buchholz

Subjects

Surgery

Published

2015

16. No significant impact of Foxf1 siRNA treatment in acute and chronic CCl

Author

Kerstin, Abshagen, Tobias, Rotberg, Berit, Genz, and Brigitte, Vollmar

Subjects

Biological Therapy, Biological Products, Disease Models, Animal, Mice, Treatment Outcome, Liver, Animals, Forkhead Transcription Factors, Chloroform, Chemical and Drug Induced Liver Injury, RNA, Small Interfering, Original Research

Abstract

Chronic liver injury of any etiology is the main trigger of fibrogenic responses and thought to be mediated by hepatic stellate cells. Herein, activating transcription factors like forkhead box f1 are described to stimulate pro-fibrogenic genes in hepatic stellate cells. By using a liver-specific siRNA delivery system (DBTC), we evaluated whether forkhead box f1 siRNA treatment exhibit beneficial effects in murine models of acute and chronic CCl4-induced liver injury. Systemic administration of DBTC-forkhead box f1 siRNA in mice was only sufficient to silence forkhead box f1 in acute CCl4 model, but was not able to attenuate liver injury as measured by liver enzymes and necrotic liver cell area. Therapeutic treatment of mice with DBTC-forkhead box f1 siRNA upon chronic CCl4 exposition failed to inhibit forkhead box f1 expression and hence lacked to diminish hepatic stellate cells activation or fibrosis development. As a conclusion, DBTC-forkhead box f1 siRNA reduced forkhead box f1 expression in a model of acute but not chronic toxic liver injury and showed no positive effects in either of these mice models.

Published

2017

17. Adenoviral overexpression of Lhx2 attenuates cell viability but does not preserve the stem cell like phenotype of hepatic stellate cells

Author

Kerstin Abshagen, Brigitte Vollmar, Brigitte M. Pützer, Maria Thomas, Georg Fuellen, Marcin Siatkowski, and Berit Genz

Subjects

Liver Cirrhosis, Cell Survival, LIM-Homeodomain Proteins, Collagen Type I, Adenoviridae, Extracellular matrix, Mice, Hepatic Stellate Cells, Animals, Humans, RNA, Messenger, Viability assay, Cells, Cultured, Mice, Inbred BALB C, biology, Cell growth, Cell Biology, Actins, Liver regeneration, Liver Regeneration, HEK293 Cells, Phenotype, Cell Transdifferentiation, embryonic structures, Cancer research, biology.protein, Hepatic stellate cell, Female, Stem cell, Myofibroblast, Platelet-derived growth factor receptor, Transcription Factors

Abstract

Hepatic stellate cells (HSC) are well known initiators of hepatic fibrosis. After liver cell damage, HSC transdifferentiate into proliferative myofibroblasts, representing the major source of extracellular matrix in the fibrotic organ. Recent studies also demonstrate a role of HSC as progenitor or stem cell like cells in liver regeneration. Lhx2 is described as stem cell maintaining factor in different organs and as an inhibitory transcription factor in HSC activation. Here we examined whether a continuous expression of Lhx2 in HSC could attenuate their activation and whether Lhx2 could serve as a potential target for antifibrotic gene therapy. Therefore, we evaluated an adenoviral mediated overexpression of Lhx2 in primary HSC and investigated mRNA expression patterns by qRT-PCR as well as the activation status by different in vitro assays. HSC revealed a marked increase in activation markers like smooth muscle actin alpha (αSMA) and collagen 1α independent from adenoviral transduction. Lhx2 overexpression resulted in attenuated cell viability as shown by a slightly hampered migratory and contractile phenotype of HSC. Expression of stem cell factors or signaling components was also unaffected by Lhx2. Summarizing these results, we found no antifibrotic or stem cell maintaining effect of Lhx2 overexpression in primary HSC.

Published

2014

18. Devitalisation of human cartilage by high hydrostatic pressure treatment

Author

Juliane Pasold, Steffen Dommerich, Bettina Hiemer, Rainer Bader, Andreas Wree, Anika Jonitz-Heincke, and Berit Genz

Subjects

0301 basic medicine, Multidisciplinary, Molecular medicine, Chemistry, Cartilage, Cellular differentiation, Regeneration (biology), Hydrostatic pressure, Mesenchymal stem cell, Stem-cell differentiation, Anatomy, Chondrogenesis, 600 Technik, Medizin, angewandte Wissenschaften::610 Medizin und Gesundheit, Article, Cell biology, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, medicine, Regeneration, Aggrecan, Stem cell transplantation for articular cartilage repair

Abstract

The regeneration of cartilage lesions still represents a major challenge. Cartilage has a tissue-specific architecture, complicating recreation by synthetic biomaterials. A novel approach for reconstruction is the use of devitalised cartilage. Treatment with high hydrostatic pressure (HHP) achieves devitalisation while biomechanical properties are remained. Therefore, in the present study, cartilage was devitalised using HHP treatment and the potential for revitalisation with chondrocytes and mesenchymal stem cells (MSCs) was investigated. The devitalisation of cartilage was performed by application of 480 MPa over 10 minutes. Effective cellular inactivation was demonstrated by the trypan blue exclusion test and DNA quantification. Histology and electron microscopy examinations showed undamaged cartilage structure after HHP treatment. For revitalisation chondrocytes and MSCs were cultured on devitalised cartilage without supplementation of chondrogenic growth factors. Both chondrocytes and MSCs significantly increased expression of cartilage-specific genes. ECM stainings showed neocartilage-like structure with positive AZAN staining as well as collagen type II and aggrecan deposition after three weeks of cultivation. Our results showed that HHP treatment caused devitalisation of cartilage tissue. ECM proteins were not influenced, thus, providing a scaffold for chondrogenic differentiation of MSCs and chondrocytes. Therefore, using HHP-treated tissue might be a promising approach for cartilage repair.

Published

2016

19. Differential Effects of Axin2 Deficiency on the Fibrogenic and Regenerative Response in Livers of Bile Duct-Ligated Mice

Author

Brigitte Vollmar, Berit Genz, Kerstin Abshagen, Moritz Senne, and Maria Thomas

Subjects

medicine.medical_specialty, Chemistry, Bile duct, Liver fibrosis, Wnt signaling pathway, LRP5, medicine.disease, Pathogenesis, medicine.anatomical_structure, Endocrinology, Cholestasis, Internal medicine, medicine, Cancer research, AXIN2, Hepatic stellate cell, Surgery

Abstract

Background: Wnt signaling is involved in the pathogenesis of liver fibrosis. Axin2 is a negative regulator of the canonical Wnt pathway by promoting β-catenin degradation. β-Catenin-activating and loss-of-function mutations of Axin2 are thought to be functionally relevant for liver diseases and cancer. Thus, we hypothesized that Axin2 deficiency promotes fibrogenesis. Methods: As the functions and mechanisms of how Axin2/β-catenin signaling participates in the progression of liver fibrosis are unclear, we investigated the progression of liver fibrosis in Axin2-deficient mice using Axin2-LacZ reporter mice (Axin2+/-, Axin2-/-, and Axin2+/+) which underwent bile duct ligation (BDL). Results: Here, we show that the expression of Axin2 is downregulated during fibrogenesis in wild-type mice, which is consistent with a decreased expression of the reporter gene LacZ in Axin2+/- and Axin2-/- mice. Surprisingly, no alteration in active β-catenin/Wnt signaling occurs in Axin2-deficient mice upon BDL. Despite a less pronounced liver injury, Axin2 deficiency had only minor and no significant effects on the fibrogenic response upon BDL, i.e. slightly reduced hepatic stellate cell activity and collagen mRNA expression. However, livers of Axin2-/- mice shared a stronger cell proliferation both already at baseline as well as immediately after BDL. Conclusion: Our results strongly suggest, contrary to expectation, that a deficiency in Axin2 is not equivalent to an increase in active β-catenin and target genes, indicating no functional relevance of Axin2-dependent regulation of the canonical Wnt/β-catenin pathway in the progression of cholestatic liver injury. This also suggests that the negligible effects of Axin2 deficiency during fibrogenesis may be related to an alternative pathway.

Published

2015

20. Anatomy and Physiology of the Hepatic Circulation

Author

Brigitte Vollmar, Berit Genz, Angela Kuhla, and Kerstin Abshagen

Subjects

Chemistry, Anatomy, Hepatic Circulation

Published

2015

21. Diabetes increases pancreatic fibrosis during chronic inflammation

Author

Tobias Radecke, Dietmar Zechner, Alexej Bobrowski, Niklas Knapp, Brigitte Vollmar, and Berit Genz

Subjects

Pathology, medicine.medical_specialty, Inflammation, Cystic fibrosis, General Biochemistry, Genetics and Molecular Biology, Collagen Type I, Streptozocin, Diabetes Mellitus, Experimental, Mice, Fibrosis, Diabetes mellitus, medicine, Animals, S100 Calcium-Binding Protein A4, Pancreas, business.industry, S100 Proteins, medicine.disease, Actins, Pancreatitis, Chronic Disease, medicine.symptom, business, Pancreatic fibrosis, Ceruletide

Abstract

Diabetes and fibrosis can be concurrent processes in several diseases such as cystic fibrosis or chronic pancreatitis. To evaluate whether diabetes can influence fibrosis and thus aggravate the pathological process, the progression of chronic pancreatitis was assessed in diabetic and non diabetic mice. For this purpose, insulin producing beta-cells in C57Bl/6 J mice were selectively impaired by administration of streptozotocin. Chronic pancreatitis was then induced by repetitive administration of cerulein in normoglycaemic and hyperglycaemic mice. Diabetes caused enhanced collagen I deposition within three weeks of the onset of chronic pancreatitis and increased the proliferation of interstitial cells. This was accompanied by an increased number of interlobular fibroblasts, which expressed S100A4 (fibroblast-specific protein-1) and stimulation of α-smooth muscle actin expression of pancreatic stellate cells. In addition, the observed aggravation of chronic pancreatitis by diabetes also led to a significantly enhanced atrophy of the pancreas, increased infiltration of inflammatory chloracetate esterase positive cells and enhanced acinar cell death. We conclude that diabetes has a detrimental influence on the progression of chronic pancreatitis by aggravating fibrosis, inflammation and pancreatic atrophy.

Published

2014

22. Genetic dissection of plexin signaling in vivo

Author

Jakub M. Swiercz, Stefan Offermanns, Jingjing Xia, Jonathan A. Epstein, Thomas Worzfeld, Berit Genz, Brigitte Vollmar, Amparo Acker-Palmer, Aycan Sentürk, Rohini Kuner, Mikio Hoshino, Suhua Deng, Andrew K Chan, and Alexander Korostylev

Subjects

Multidisciplinary, RHOA, animal structures, biology, Transgene, Plexin, Mutant, Mice, Transgenic, Nerve Tissue Proteins, Biological Sciences, Phenotype, Cell biology, Mice, Semaphorin, embryonic structures, biology.protein, Animals, Guanine nucleotide exchange factor, Signal transduction, Signal Transduction

Abstract

Mammalian plexins constitute a family of transmembrane receptors for semaphorins and represent critical regulators of various processes during development of the nervous, cardiovascular, skeletal, and renal system. In vitro studies have shown that plexins exert their effects via an intracellular R-Ras/M-Ras GTPase-activating protein (GAP) domain or by activation of RhoA through interaction with Rho guanine nucleotide exchange factor proteins. However, which of these signaling pathways are relevant for plexin functions in vivo is largely unknown. Using an allelic series of transgenic mice, we show that the GAP domain of plexins constitutes their key signaling module during development. Mice in which endogenous Plexin-B2 or Plexin-D1 is replaced by transgenic versions harboring mutations in the GAP domain recapitulate the phenotypes of the respective null mutants in the developing nervous, vascular, and skeletal system. We further provide genetic evidence that, unexpectedly, the GAP domain-mediated developmental functions of plexins are not brought about via R-Ras and M-Ras inactivation. In contrast to the GAP domain mutants, Plexin-B2 transgenic mice defective in Rho guanine nucleotide exchange factor binding are viable and fertile but exhibit abnormal development of the liver vasculature. Our genetic analyses uncover the in vivo context-dependence and functional specificity of individual plexin-mediated signaling pathways during development.

Published

2014

23. Impact of hyperglycemia and acute pancreatitis on the receptor for advanced glycation endproducts

Author

Dietmar, Zechner, Kai, Sempert, Berit, Genz, Franziska, Timm, Florian, Bürtin, Tim, Kroemer, Antje, Butschkau, Angela, Kuhla, and Brigitte, Vollmar

Subjects

endocrine system diseases, MAP Kinase Signaling System, Receptor for Advanced Glycation End Products, nutritional and metabolic diseases, Lipase, Diabetes Mellitus, Experimental, Mice, Inbred C57BL, Mice, Pancreatitis, Hyperglycemia, cardiovascular system, Disease Progression, Animals, Original Article, cardiovascular diseases, Phosphorylation, Receptors, Immunologic, human activities, Pancreas

Abstract

Since hyperglycemia aggravates acute pancreatitis and also activates the receptor for advanced glycation endproducts (RAGE) in other organs, we explored if RAGE is expressed in the pancreas and if its expression is regulated during acute pancreatitis and hyperglycemia. Acute pancreatitis was induced by cerulein in untreated and streptozotocin treated diabetic mice. Expression of RAGE was analyzed by Western blot and immunohistochemistry. To evaluate signal transduction the phosphorylation of ERK1/ERK2 was assessed by Western blot and the progression of acute pancreatitis was monitored by evaluation of lipase activity and the pancreas wet to dry weight ratio. RAGE is mainly expressed by acinar as well as interstitial cells in the pancreas. During acute pancreatitis infiltrating inflammatory cells also express RAGE. Using two distinct anti-RAGE antibodies six RAGE proteins with diverse molecular weight are detected in the pancreas, whereas just three distinct RAGE proteins are detected in the lung. Hyperglycemia, which aggravates acute pancreatitis, significantly reduces the production of two RAGE proteins in the inflamed pancreas.

Published

2013

24. Development of Adenoviral Delivery Systems to Target Hepatic Stellate Cells In Vivo

Author

Brigitte Vollmar, Brigitte M. Pützer, Julia Reetz, Ottmar Herchenröder, Claudia Meier, Berit Genz, Bhavani S. Kowtharapu, Franziska Timm, and Kerstin Abshagen

Subjects

Multidisciplinary, business.industry, Science, lcsh:R, lcsh:Medicine, Correction, Bioinformatics, Text mining, In vivo, Cancer research, Hepatic stellate cell, Medicine, lcsh:Q, business, lcsh:Science

Abstract

There are panels missing from Figures 2, 5, and 6. Please see the correct versions of these figures at the following links: Figure 2- Figure 5- Figure 6

Published

2013

25. Chimeric rabies viruses for trans-species comparison of lyssavirus glycoprotein ectodomain functions in virus replication and pathogenesis

Author

Berit, Genz, Tobias, Nolden, Alexandra, Negatsch, Jens-Peter, Teifke, Karl-Klaus, Conzelmann, and Stefan, Finke

Subjects

Cerebral Cortex, Neurons, Recombinant Fusion Proteins, Virus Replication, Hippocampus, Immunohistochemistry, Cell Line, Rats, Rats, Sprague-Dawley, Mice, Viral Proteins, Nucleoproteins, Gene Expression Regulation, Rabies virus, Rhabdoviridae Infections, Animals, Lyssavirus, Antigens, Viral, Cells, Cultured, Glycoproteins

Abstract

The glycoprotein G of lyssaviruses is the major determinant of virus pathogenicity and serves as a target for immunological responses to virus infections. However, assessment of the exact contribution of lyssavirus G proteins to observed differences in the pathogenicity of lyssavirus species is challenging, since the direct comparison of natural lyssaviruses does not allow specific ascription to individual virus proteins or domains. Here we describe the generation and characterization of recombinant rabies viruses (RABV) that express chimeric G proteins comprising of a RABV cytoplasma domain fused to transmembrane and ectodomain G sequences of a virulent RABV (challenge virus standard; CVS-11) or two European bat lyssaviruses (EBLV- and EBLV-2). These "envelope-switched" recombinant viruses were recovered from cDNAs. Similar growth kinetics and protein expression in neuroblastoma cell cultures and successful targeting of primary neurons showed that the chimeric G proteins were able to replace the authentic G protein in a RABV based virus vector. Inoculation of six week old CD-1 mice by the intracranial (i. c.) route of infection further demonstrated that all recombinant viruses were able to spread in the brain and to induce disease. The "envelope-switched" RABV therefore represent an important tool to further investigate the influence of lyssavirus ectodomains on virus tropism, and pathogenicity.

Published

2012