Your search keyword '"Morten Grønbech Rasch"' showing total 24 results

1. Presence of Insulin-Like Growth Factor Binding Proteins Correlates With Tumor-Promoting Effects of Matrix Metalloproteinase 9 in Breast Cancer

Author

Jae-Hyun Park, Morten Grønbech Rasch, Jing Qiu, Ida Katrine Lund, and Mikala Egeblad

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The stroma of breast cancer can promote the disease’s progression, but whether its composition and functions are shared among different subtypes is poorly explored. We compared stromal components of a luminal [mouse mammary tumor virus (MMTV)–Neu] and a triple-negative/basal-like [C3(1)–Simian virus 40 large T antigen (Tag)] genetically engineered breast cancer mouse model. The types of cytokines and their expression levels were very different in the two models, as was the extent of innate immune cell infiltration; however, both models showed infiltration of innate immune cells that expressed matrix metalloproteinase 9 (MMP9), an extracellular protease linked to the progression of many types of cancer. By intercrossing with Mmp9 null mice, we found that the absence of MMP9 delayed tumor onset in the C3(1)-Tag model but had no effect on tumor onset in the MMTV-Neu model. We discovered that protein levels of insulin-like growth factor binding protein-1 (IGFBP-1), an MMP9 substrate, were increased in C3(1)-Tag;Mmp9−/− compared to C3(1)-Tag;Mmp9+/+ tumors. In contrast, IGFBP-1 protein expression was low in MMTV-Neu tumors regardless of Mmp9 status. IGFBP-1 binds and antagonizes IGFs, preventing them from activating their receptors to promote cell proliferation and survival. Tumors from C3(1)-Tag;Mmp9−/− mice had reduced IGF-1 receptor phosphorylation, consistent with slower tumor onset. Finally, gene expression analysis of human breast tumors showed that high expression of IGFBP mRNA was strongly correlated with good prognosis but not when MMP9 mRNA was also highly expressed. In conclusion, MMP9 has different effects on breast cancer progression depending on whether IGFBPs are expressed.

Published

2015

2. Inhibitory monoclonal antibodies against mouse proteases raised in gene-deficient mice block proteolytic functions in vivo

Author

Ida Katrine Lund, Morten Grønbech Rasch, Signe eIngvarsen, Jesper ePass, Daniel H Madsen, Lars H Engelholm, Niels eBehrendt, and Gunilla eHøyer-Hansen

Subjects

extracellular proteolysis, collagen internalization, in vivo models, Mouse monoclonal antibodies, plasminogen activation, Therapeutics. Pharmacology, RM1-950

Abstract

Identification of targets for cancer therapy requires the understanding of the in vivo roles of proteins, which can be derived from studies using gene-targeted mice. An alternative strategy is the administration of inhibitory monoclonal antibodies (mAbs), causing acute disruption of the target protein function(s). This approach has the advantage of being a model for therapeutic targeting. mAbs for use in mouse models can be obtained through immunization of gene-deficient mice with the autologous protein. Such mAbs react with both species-specific epitopes and epitopes conserved between species. mAbs against proteins involved in extracellular proteolysis, including plasminogen activators (uPA, tPA), their inhibitor PAI-1, the uPA receptor (uPAR), two matrix metalloproteinases (MMP9 and MMP14), as well as the collagen internalization receptor uPARAP, have been developed. The inhibitory mAbs against uPA and uPAR block plasminogen activation and thereby hepatic fibrinolysis in vivo. Wound healing, another plasmin-dependent process, is delayed by an inhibitory mAb against uPA in the adult mouse. Thromboembolism can be inhibited by anti-PAI-1 mAbs in vivo. In conclusion, function-blocking mAbs are well-suited for targeted therapy in mouse models of different diseases, including cancer.

Published

2012

3. A factor VIIIa-mimetic bispecific antibody, Mim8, ameliorates bleeding upon severe vascular challenge in hemophilia A mice

Author

Peter Thygesen, A. Henriksen, Haisun Zhu, Mette B. Hermit, Laust Bruun Johnsen, Per Jr Greisen, Søren Lund, Henrik Rahbek-Nielsen, Stine Kjellev, Kasper Lamberth, Henrik Østergaard, Eva Johansson, Thomas Lindebo Holm, Jais Rose Bjelke, Prafull S. Gandhi, Carsten Dan Ley, Daniel Elenius Madsen, Nikolai Lorenzen, Lisbeth Moreau Andersen, Zhiru Yang, Gustav Røder, Jacob Lund, Mette Loftager, Bjarne Gram Hansen, Amalie Carnbring Bonde, Rong Zhou, Ida Hilden, Thomas Egebjerg, Karina Thorn, Morten Grønbech Rasch, Xun Li, and Fabian Stavenuiter

Subjects

Male, Immunology, Hemorrhage, Pharmacology, Hemophilia A, Biochemistry, Factor IXa, Thrombosis and Hemostasis, chemistry.chemical_compound, Thrombin, hemic and lymphatic diseases, Antibodies, Bispecific, medicine, Potency, Animals, Humans, Factor VIIIa, Whole blood, Emicizumab, biology, Chemistry, Factor X, Cell Biology, Hematology, Orders of magnitude (mass), Dissociation constant, Mice, Inbred C57BL, biology.protein, Female, Antibody, medicine.drug

Abstract

Østergaard and colleagues report the development of a potent bispecific antibody, Mim8, which binds both activated factor IX and factor X, mimicking the propagation of coagulation by activated factor VIII. They detail biophysical, in vitro, and in vivo preclinical data supporting its potential as a treatment for bleeding in hemophilia A., Key Points Mim8, an anti-FIXa/anti-FX bispecific antibody, has enhanced activity over emicizumab in mouse models and in vitro hemophilia A assays.The activity of Mim8 is partly achieved through FIXa stimulatory activity residing in the anti-FIXa arm., Visual Abstract, Hemophilia A is a bleeding disorder resulting from deficient factor VIII (FVIII), which normally functions as a cofactor to activated factor IX (FIXa) that facilitates activation of factor X (FX). To mimic this property in a bispecific antibody format, a screening was conducted to identify functional pairs of anti-FIXa and anti-FX antibodies, followed by optimization of functional and biophysical properties. The resulting bispecific antibody (Mim8) assembled efficiently with FIXa and FX on membranes, and supported activation with an apparent equilibrium dissociation constant of 16 nM. Binding affinity with FIXa and FX in solution was much lower, with equilibrium dissociation constant values for FIXa and FX of 2.3 and 1.5 µM, respectively. In addition, the activity of Mim8 was dependent on stimulatory activity contributed by the anti-FIXa arm, which enhanced the proteolytic activity of FIXa by 4 orders of magnitude. In hemophilia A plasma and whole blood, Mim8 normalized thrombin generation and clot formation, with potencies 13 and 18 times higher than a sequence-identical analogue of emicizumab. A similar potency difference was observed in a tail vein transection model in hemophilia A mice, whereas reduction of bleeding in a severe tail-clip model was observed only for Mim8. Furthermore, the pharmacokinetic parameters of Mim8 were investigated and a half-life of 14 days shown in cynomolgus monkeys. In conclusion, Mim8 is an activated FVIII mimetic with a potent and efficacious hemostatic effect based on preclinical data.

Published

2020

4. A Membrane-Bound Diacylglycerol Species Induces PKCϵ-Mediated Hepatic Insulin Resistance

Author

Sandro M. Hirabara, Gary W. Cline, Rafael C. Gaspar, Panu K. Luukkonen, Mario Kahn, Jesse Rinehart, Marcos Ricardo da Silva Rodrigues, Gerald I. Shulman, Mireille J. Serlie, Dongyan Zhang, Ye Zhang, Kun Lyu, Kasper W. ter Horst, Varman T. Samuel, Morten Grønbech Rasch, Seohyuk Lee, Jonathan S. Bogan, Sanjay Bhanot, Niels Blume, Endocrinology, and AGEM - Amsterdam Gastroenterology Endocrinology Metabolism

Subjects

Male, 0301 basic medicine, nonalcoholic fatty liver disease, Physiology, hepatic insulin resistance, Mitochondrion, Article, Diglycerides, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Lipid droplet, Animals, Humans, Phosphorylation, liquid chromatography-tandem mass spectrometry, Molecular Biology, Diacylglycerol kinase, insulin receptor phosphorylation, ceramides, biology, Chemistry, Kinase, Endoplasmic reticulum, Cell Membrane, hepatic glucose production, Cell Biology, Receptor, Insulin, Rats, Cell biology, Insulin receptor, Cytosol, 030104 developmental biology, Liver, dicylglycerols, biology.protein, protein kinase C-epsilon, lipids (amino acids, peptides, and proteins), type 2 diabetes, Insulin Resistance, 030217 neurology & neurosurgery, hepatic glycogen synthesis

Abstract

Nonalcoholic fatty liver disease is strongly associated with hepatic insulin resistance (HIR); however, the key lipid species and molecular mechanisms linking these conditions are widely debated. We developed a subcellular fractionation method to quantify diacylglycerol (DAG) stereoisomers and ceramides in the endoplasmic reticulum (ER), mitochondria, plasma membrane (PM), lipid droplets, and cytosol. Acute knockdown (KD) of diacylglycerol acyltransferase-2 in liver induced HIR in rats. This was due to PM sn-1,2-DAG accumulation, which promoted PKCϵ activation and insulin receptor kinase (IRK)-T1160 phosphorylation, resulting in decreased IRK-Y1162 phosphorylation. Liver PM sn-1,2-DAG content and IRK-T1160 phosphorylation were also higher in humans with HIR. In rats, liver-specific PKCϵ KD ameliorated high-fat diet-induced HIR by lowering IRK-T1160 phosphorylation, while liver-specific overexpression of constitutively active PKCϵ-induced HIR by promoting IRK-T1160 phosphorylation. These data identify PM sn-1,2-DAGs as the key pool of lipids that activate PKCϵ and that hepatic PKCϵ is both necessary and sufficient in mediating HIR.

Published

2020

5. 205-OR: Hepatic Protein Kinase C-e Is Necessary and Sufficient in Mediating Lipid-Induced Hepatic Insulin Resistance

Author

Gary W. Cline, Gerald I. Shulman, Marcos Ricardo da Silva Rodrigues, Panu K. Luukkonen, Jesse Rinehart, Kun Lyu, Seohyuk Lee, Jonathan S. Bogan, Varman T. Samuel, Mario Kahn, Sanjay Bhanot, Morten Grønbech Rasch, Sandro M. Hirabara, Niels Blume, Mireille J. Serlie, and Dongyan Zhang

Subjects

medicine.medical_specialty, Ceramide, biology, Kinase, business.industry, Endocrinology, Diabetes and Metabolism, medicine.disease, chemistry.chemical_compound, Endocrinology, Insulin resistance, chemistry, Internal medicine, Nonalcoholic fatty liver disease, Internal Medicine, medicine, biology.protein, Phosphorylation, Glycogen synthase, business, Protein kinase B, Diacylglycerol kinase

Abstract

Nonalcoholic fatty liver disease (NAFLD) is strongly associated with hepatic insulin resistance (HIR), however the key lipid species and molecular mechanisms linking these conditions are widely debated. In order to address these questions, we examined the metabolic impact of a liver-specific antisense oligonucleotide against PKCε and found that liver-specific PKCε knockdown ameliorated high-fat diet-induced HIR in rats, reflected by ∼2x increase in insulin-stimulated hepatic glycogen synthesis rate and improved insulin-mediated suppression of endogenous glucose production during a hyperinsulinemic-hyperglycemic (HH) clamp. This was associated with increased IRK Y1162 and Akt S473 phosphorylation and could be attributed to decreased PKCε-mediated IRK T1160 phosphorylation. Overexpressing a constitutively active PKCε (A159E) in the liver induced HIR in regular chow-fed rats, reflected by reduced insulin-stimulated glycogen synthesis rate during an HH clamp. This was associated with impaired IRK Y1162 and Akt S473 phosphorylation and could be attributed to increased PKCε-mediated IRK T1160 phosphorylation. We also developed a subcellular fractionation method to quantify diacylglycerol (DAG) stereoisomers and ceramides in the endoplasmic reticulum, mitochondria, plasma membrane (PM), lipid droplet and cytosol and applied this method to a cohort of obese human subjects with and without NAFLD and HIR. Liver PM sn-1,2 DAG content was ∼5x higher in HIR individuals with NAFLD compared to insulin-sensitive individuals without NAFLD, associated with ∼3x higher IRK T1160 phosphorylation, supporting the importance of PM sn-1,2 DAG-PKCε-IRK pT1160 pathway to mediate HIR in humans with NAFLD. In contrast there were no significant differences in ceramide content in any of the subcellular compartments. Conclusion: These data identify PM sn-1,2 DAGs as the key lipids that activate PKCε, and that hepatic PKCε is both necessary and sufficient in mediating HIR. Disclosure K. Lyu: None. D. Zhang: None. M. Kahn: None. M.R.S. Rodrigues: None. S. Hirabara: None. P. Luukkonen: None. S. Lee: None. S. Bhanot: None. J. Rinehart: None. N. Blume: Employee; Self; Novo Nordisk A/S. Stock/Shareholder; Self; Novo Nordisk A/S. M. Rasch: Employee; Self; Novo Nordisk A/S. Stock/Shareholder; Self; Novo Nordisk A/S. M.J. Serlie: None. J. Bogan: None. G. Cline: None. V. Samuel: None. G.I. Shulman: Advisory Panel; Self; AstraZeneca, Janssen Research & Development, LLC, Merck & Co., Inc. Advisory Panel; Spouse/Partner; Merck & Co., Inc. Consultant; Self; Novo Nordisk A/S. Consultant; Spouse/Partner; Novo Nordisk A/S. Other Relationship; Self; Gilead Sciences, Inc., iMetabolic Biopharma Corporation. Other Relationship; Spouse/Partner; iMetabolic Biopharma Corporation. Other Relationship; Self; Maze Therapeutics. Funding U.S. Public Health Service (R01DK116774, R01DK119968, R01DK113984, P30DK045735, R01 DK092661); U.S. Department of Veternas Affairs (I01BX000901)

Published

2020

6. Cross-species reactive monoclonal antibodies against the extracellular domains of the insulin receptor and IGF1 receptor

Author

Morten Grønbech Rasch, Niels Blume, Laura Kofoed Hvidsten Ørstrup, Gerd Schluckebier, Henning Hvid, Bo Falck Hansen, Rita Slaaby, Søren Lund, Anne Lützen, Nicolaj Rasmussen, Thomas Åskov Pedersen, Zhe Wang, and Jakob Brandt

Subjects

0301 basic medicine, medicine.drug_class, Swine, Immunology, Cross Reactions, Monoclonal antibody, Epitope, Cross-species translation, Hybrid receptor, Receptor, IGF Type 1, 03 medical and health sciences, Mice, 0302 clinical medicine, Antigen, Species Specificity, medicine, Immunology and Allergy, Animals, Humans, Receptor, IGF1 receptor, biology, medicine.diagnostic_test, Chemistry, Diabetes, Antibodies, Monoclonal, HCT116 Cells, Receptor, Insulin, Rats, Insulin receptor, 030104 developmental biology, Biochemistry, Immunoassay, Monoclonal, biology.protein, Monoclonal antibodies, Rabbits, Antibody, 030215 immunology

Abstract

Translation across species of immunoassay results is often challenging due to the lack of cross-species reactivity of antibodies. In order to investigate the biology of insulin and IGF1 receptors, we generated new versatile monoclonal assay antibodies using the extracellular domain of the insulin/IGF1 hybrid receptor as the bait protein in the Adimab yeast antibody discovery platform and as the antigen in a rabbit monoclonal antibody platform. The resulting antibody clones were screened for receptor specificity as well as cross-species reactivity to both tissue and cell line derived samples. Using these strategies, we were able to identify highly specific insulin receptor monoclonal antibodies that lack cross-reactivity to the IGF1 receptor using the Adimab platform and a highly specific IGF1 receptor monoclonal antibody that lacks cross-reactivity to the insulin receptor using the rabbit antibody platform. Unlike earlier monoclonal antibodies reported in the literature, these antibodies show cross-species reactivity to the extracellular domains of mouse, rat, pig, and human receptors, indicating that they bind conserved epitopes. Furthermore, the antibodies work well in several different assay formats, including ELISA, flow cytometry, and immunoprecipitation, and therefore provide new tools to study insulin and IGF1 receptor biology with translation across several species and experimental model systems.

Published

2018

7. Monoclonal antibodies targeting the disintegrin-like domain of ADAMDEC1 modulates the proteolytic activity and enables quantification of ADAMDEC1 protein in human plasma

Author

Linda Troeberg, Helle Heibroch Petersen, Mette Loftager, Hideaki Nagase, Mari Enoksson, Jacob Lund, Morten Grønbech Rasch, Michael Toft Overgaard, and Anne Mette Elimar Bitsch

Subjects

0301 basic medicine, Carboxylic Acids, Epitope, Substrate Specificity, Epitopes, Mice, 0302 clinical medicine, Antibody Specificity, Immunology and Allergy, Cells, Cultured, chemistry.chemical_classification, Metalloproteinase, medicine.diagnostic_test, biology, Transferrin, Antibodies, Monoclonal, Cell biology, disintegrin, 030220 oncology & carcinogenesis, ELISA, Protein Binding, Immunoprecipitation, medicine.drug_class, Immunology, Enzyme-Linked Immunosorbent Assay, Monoclonal antibody, Methylation, 03 medical and health sciences, Metalloprotease, Western blot, Report, medicine, Disintegrin, Journal Article, Animals, Humans, Secretion, Protease Inhibitors, Protein Interaction Domains and Motifs, plasma, Macrophages, ADAMDEC1, Molecular biology, quantification, ADAM Proteins, Kinetics, 030104 developmental biology, chemistry, Proteolysis, biology.protein, Binding Sites, Antibody

Abstract

Decysin-1 (ADAMDEC1) is an orphan ADAM-like metalloprotease with unknown biological function and a short domain structure. ADAMDEC1 mRNA has previously been demonstrated primarily in macrophages and mature dendritic cells. Here, we generated monoclonal antibodies (mAbs) against the mature ADAMDEC1 protein, as well as mAbs specific for the ADAMDEC1 pro-form, enabling further investigations of the metalloprotease. The generated mAbs bind ADAMDEC1 with varying affinity and represent at least six different epitope bins. Binding of mAbs to one epitope bin in the C-terminal disintegrin-like domain efficiently reduces the proteolytic activity of ADAMDEC1. A unique mAb, also recognizing the disintegrin-like domain, stimulates the caseinolytic activity of ADAMDEC1 while having no significant effect on the proteolysis of carboxymethylated transferrin. Using two different mAbs binding the disintegrin-like domain, we developed a robust, quantitative sandwich ELISA and demonstrate secretion of mature ADAMDEC1 protein by primary human macrophages. Surprisingly, we also found ADAMDEC1 present in human plasma with an approximate concentration of 0.5 nM. The presence of ADAMDEC1 both in human plasma and in macrophage cell culture supernatant were biochemically validated using immunoprecipitation and Western blot analysis demonstrating that ADAMDEC1 is secreted in a mature form.

Published

2017

8. Characterization of the glucagon-like peptide-1 receptor in male mouse brain using a novel antibody and in situ hybridization

Author

Anna Secher, Casper Bo Jensen, Charles Pyke, Lotte Bjerre Knudsen, Morten Grønbech Rasch, and Anders Bjorholm Dahl

Subjects

0301 basic medicine, Male, endocrine system, In situ hybridization, Antibodies, Glucagon-Like Peptide-1 Receptor, 03 medical and health sciences, Mice, Endocrinology, Glucagon-Like Peptide 1, medicine, Animals, Receptor, In Situ Hybridization, Neurons, Messenger RNA, biology, digestive, oral, and skin physiology, Brain, Molecular biology, 030104 developmental biology, medicine.anatomical_structure, Hypothalamus, Monoclonal, biology.protein, Immunohistochemistry, Antibody, Nucleus, hormones, hormone substitutes, and hormone antagonists

Abstract

Glucagon-like peptide-1 (GLP-1) is a physiological regulator of appetite and long-acting GLP-1 receptor agonists (GLP-1RA) lower food intake and bodyweight in both human and animal studies. The effects are mediated through brain GLP-1Rs, and several brain nuclei expressing the GLP-1R may be involved. To date, mapping the complete location of GLP-1R protein in the brain has been challenged by lack of good antibodies and the discrepancy between mRNA and protein especially relevant in neuronal axonal processes. Here, we present a novel and specific monoclonal GLP-1R antibody for immunohistochemistry with murine tissue and show detailed distribution of GLP-1R expression as well as mapping of GLP-1R mRNA by non-radioactive in situ hybridization. Semi-automated image analysis was performed to map the GLP-1R distribution to atlas plates from the Allen Institute of Brain Science (AIBS). The GLP-1R was abundantly expressed in numerous regions including the septal nucleus, the hypothalamus and the brain stem. GLP-1R protein expression was also observed on neuronal projections in brain regions devoid of any mRNA which has not been observed in earlier reports. Taken together, these findings provide new knowledge on GLP-1R expression in neuronal cell bodies and neuronal projections.

Published

2017

9. Mim8 - a Next-Generation FVIII Mimetic Bi-Specific Antibody - Potently Restores the Hemostatic Capacity in Hemophilia a Settings in Vitro and In Vivo

Author

Zhiru Yang, Thomas Egebjerg, Karina Thorn, A. Henriksen, Stine Kjellev, Henrik Rahbek-Nielsen, Ida Hilden, Jais Rose Bjelke, Prafull S. Gandhi, Daniel Elenius, Søren Lund, Morten Grønbech Rasch, Jacob Lund, Carsten Dan Ley, Thomas L Holm, Mette Loftager, Mette B. Hermit, Per Jr Greisen, Rong Zhou, Marianne Kjalke, Bjarne Gram Hansen, Peter Thygesen, Nikolai Lorenzen, Henrik Østergaard, and Kasper Lamberth

Subjects

Emicizumab, Business administration, Immunology, Treatment burden, Tail vein, Cell Biology, Hematology, PK Parameters, Clot formation, Biochemistry, Thrombin generation, Specific antibody, Business, Target binding

Abstract

The treatment of hemophilia A (HA) is primarily based on replacement of factor VIII (FVIII), and in people with HA with inhibitors (HAwI) on the use of by-passing agents. Recently, a FVIII mimetic bispecific antibody emicizumab (Hemlibra®) was approved for treatment of HA and HAwI, offering a subcutaneous, prophylactic treatment opportunity with potential for significantly reducing the treatment burden. We describe the development and pre-clinical characterization of Mim8, a novel, next-generation FVIII mimetic human bispecific antibody. Mim8 is a highly potent molecule bridging factor IXa (FIXa) and factor X (FX) in development for subcutaneous treatment of people with HA and HAwI. Development of Mim8 utilized the Duobody® platform to initially screen for compatible anti-FIXa and anti-FX antibodies followed by several iterations of systematic mutational optimization. In total, more than 30,000 bispecific antibodies were analyzed. The optimization process aimed for efficient Mim8-mediated activation of FX by FIXa in the presence of procoagulant membrane, low target binding in solution, low immunogenicity risk, and for desirable biophysical parameters such as low viscosity. In vitro characterization demonstrated that Mim8 efficiently localizes FIXa and FX to the phospholipid surface and enhances FXa activation. The monovalent anti-FIXa arm alone stimulates the proteolytic activity of FIXa in the range of 15,000-fold and is an important contributor to the activity of the bispecific antibody. The dissociation constants (Kd) of Mim8 for FIXa and FX is in the micromolar range, minimizing target binding in the blood. Using thrombin generation assay in congenital HA plasma and thrombelastography (TEG) in whole blood from healthy volunteers spiked with anti-FVIII antibodies, Mim8 was capable of normalizing thrombin generation and blood clot formation, respectively, with approximately 15 times greater potency than emicizumab (Figure 1). A similar potency improvement was demonstrated in a tail vein transection bleeding model in FVIII-deficient mice co-dosed with human FIX and FX to circumvent lack of Mim8 cross reactivity to murine FIX and FX. The terminal half-life of Mim8 was estimated to 14 days (range 10-17 days) in cynomolgus monkeys and the subcutaneous bioavailability to 97%. In conclusion, Mim8 is a novel, next-generation FVIII mimetic bispecific antibody with anti-FIXa and anti-FX arms that potently stimulates FX activation resulting in efficacious haemostasis in vitro and in vivo. Mim8 has a high potency allowing for administration of small volumes in a pen device, good PK parameters, minimal target binding in the blood, and good biophysical properties. Collectively, these properties support clinical development of Mim8 as a potentially improved next-generation FVIII-mimetic prophylactic treatment option for persons with hemophilia A regardless of inhibitor status. Figure 1: Left: FXI-triggered thrombin generation assay in congenital HA plasma (mean and SD of n = 5). Right: thromboelastography in whole blood from healthy donors spiked with polyclonal anti-FVIII antibody (mean and SD of n = 3). Coagulation was triggered with low concentration (∼30 fM) of tissue factor (Innovin® 1:200,000). Shaded areas: standard deviation of controls. Blue circles: Mim8. Grey squares: a sequence identical analogue (SIA) to emicizumab (comparable data were obtained with a commercially available batch of Hemlibra®). Disclosures Kjellev: Novo Nordisk A/S: Employment, Equity Ownership. Østergaard:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Greisen:Novo Nordisk A/S: Equity Ownership, Patents & Royalties: Patents. Hermit:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Thorn:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Hansen:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Zhou:Novo Nordisk A/S: Equity Ownership, Other: Previous employment, Patents & Royalties: Patents. Bjelke:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Kjalke:Novo Nordisk A/S: Employment, Honoraria. Lund:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Holm:Novo Nordisk A/S: Equity Ownership, Other: Previous employment. Ley:Novo Nordisk A/S: Employment, Equity Ownership. Elenius:Novo Nordisk A/S: Equity Ownership, Other: Previous employment; Leo Pharma A/S: Employment, Equity Ownership. Thygesen:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Loftager:Novo Nordisk A/S: Employment, Equity Ownership. Rasch:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Lorenzen:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Gandhi:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Lamberth:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Egebjerg:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Lund:Novo Nordisk A/S: Employment, Equity Ownership. Henriksen:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Rahbek-Nielsen:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Yang:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties: Patents. Hilden:Novo Nordisk A/S: Employment, Equity Ownership, Patents & Royalties.

Published

2019

10. Imaging Tumor-Stroma Interactions during Chemotherapy Reveals Contributions of the Microenvironment to Resistance

Author

Mina J. Bissell, Mikala Egeblad, Miriam R. Fein, Eirik Frengen, Jae-Hyun Park, Jing Qiu, Zena Werb, Hanne A. Askautrud, Vicki Plaks, Pranay Sinha, Elizabeth S. Nakasone, Juwon Park, Morten Grønbech Rasch, Ying Xim Tan, Tim Kees, and Andrew J. Ewald

Subjects

Cancer Research, Receptors, CCR2, Cell, Antineoplastic Agents, Vascular permeability, Biology, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Live cell imaging, Tumor Cells, Cultured, Tumor Microenvironment, medicine, Animals, Neoplasm, Myeloid Cells, Doxorubicin, 030304 developmental biology, 0303 health sciences, Tumor microenvironment, Antibiotics, Antineoplastic, Cell Death, Macrophages, Mammary Neoplasms, Experimental, Cell Biology, medicine.disease, 3. Good health, Mice, Inbred C57BL, medicine.anatomical_structure, Matrix Metalloproteinase 9, Oncology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Cancer cell, Immunology, Cancer research, Female, Cisplatin, Intravital microscopy, medicine.drug

Abstract

SummaryLittle is known about the dynamics of cancer cell death in response to therapy in the tumor microenvironment. Intravital microscopy of chemotherapy-treated mouse mammary carcinomas allowed us to follow drug distribution, cell death, and tumor-stroma interactions. We observed associations between vascular leakage and response to doxorubicin, including improved response in matrix metalloproteinase-9 null mice that had increased vascular leakage. Furthermore, we observed CCR2-dependent infiltration of myeloid cells after treatment and that Ccr2 null host mice responded better to treatment with doxorubicin or cisplatin. These data show that the microenvironment contributes critically to drug response via regulation of vascular permeability and innate immune cell infiltration. Thus, live imaging can be used to gain insights into drug responses in situ.

Published

2012

11. Purification and characterization of recombinant full-length and protease domain of murine MMP-9 expressed in Drosophila S2 cells

Author

Gunilla Høyer-Hansen, Henrik Gårdsvoll, Morten Grønbech Rasch, Ida K. Lund, and Martin Illemann

Subjects

Gene Expression, Antibodies, Chromatography, Affinity, law.invention, Cell Line, 03 medical and health sciences, Mice, law, Animals, 030304 developmental biology, Skin, 0303 health sciences, biology, Schneider 2 cells, 030302 biochemistry & molecular biology, Hemopexin, Transfection, Molecular biology, Recombinant Proteins, 3. Good health, Protein Structure, Tertiary, Blot, Matrix Metalloproteinase 9, Polyclonal antibodies, Cell culture, biology.protein, Recombinant DNA, Drosophila, Murinae, Rabbits, Antibody, Biotechnology

Abstract

Matrix metalloproteinase-9 (MMP-9) is a 92-kDa soluble pro-enzyme implicated in pathological events including cancer invasion. It is therefore an attractive target for therapeutic intervention studies in mouse models. Development of inhibitors requires sufficient amounts of correctly folded murine MMP-9. Constructs encoding zymogens of full-length murine MMP-9 and a version lacking the O-glycosylated linker region and hemopexin domains were therefore generated and expressed in stably transfected Drosophila S2 insect cells. After 7 days of induction the expression levels of the full-length and truncated versions were 5 mg/l and 2 mg/l, respectively. The products were >95% pure after gelatin Sepharose chromatography and possessed proteolytic activity when analyzed by gelatin zymography. Using the purified full-length murine MMP-9 we raised polyclonal antibodies by immunizations of rabbits. These antibodies specifically identified pro-MMP-9 in incisional skin wound extracts from mice when used for Western blotting. Immunohistochemical analysis of paraffin embedded skin wounds from mice showed that MMP-9 protein was localized at the leading-edge keratinocytes in front of the migrating epidermal layer. No immunoreactivity was observed when the antibody was probed against skin wound material from MMP-9 deficient mice. In conclusion, we have generated and purified two proteolytically active recombinant murine MMP-9 protein constructs, which are critical reagents for future cancer drug discovery studies.

Published

2010

12. Discrimination of different forms of the murine urokinase plasminogen activator receptor on the cell surface using monoclonal antibodies

Author

Ida K. Lund, Martin Illemann, Gunilla Høyer-Hansen, Jesper Pass, and Morten Grønbech Rasch

Subjects

medicine.drug_class, Immunology, Cell, Antibody Affinity, Monoclonal antibody, Epitope, Cell Line, Receptors, Urokinase Plasminogen Activator, Mice, medicine, Animals, Humans, Immunology and Allergy, Binding site, Receptor, neoplasms, biology, Chemistry, Monocyte, Cell Membrane, Antibodies, Monoclonal, Surface Plasmon Resonance, Urokinase-Type Plasminogen Activator, Molecular biology, biological factors, Protein Structure, Tertiary, Urokinase receptor, medicine.anatomical_structure, biology.protein, Vitronectin, Binding Sites, Antibody

Abstract

The urokinase plasminogen activator receptor (uPAR) is a versatile three-domain GPI-anchored protein, which binds urokinase plasminogen activator (uPA) and thereby focalises plasminogen activation on the cell surface. Generation of a proteolytic potential is essential in both normal physiological and pathological extracellular tissue remodelling processes. uPA can also cleave uPAR, resulting in liberation of the amino-terminal domain I, which encompasses binding sites for both uPA and the adhesion molecule, vitronectin. In order to localise the different uPAR forms on the plasma membrane of murine monocyte macrophage-like P388D.1 cells, we have now generated and characterised two high-affinity murine mAbs, mR3 and mR4, raised against murine uPAR. mR3 was found to recognise an epitope located in domain I of uPAR. Surface plasmon resonance analyses and cell binding studies revealed that this mAb was able to bind preformed complexes of murine pro-uPA and murine uPAR. In contrast, mR4 recognises domains II–III in uPAR and does not bind preformed pro-uPA–uPAR complexes in similar analyses. Immunofluorescence microscopy of P388D.1 cells revealed that mR3 stained the cells equally well in the presence or absence of saturation with the amino-terminal fragment of uPA, ATF. However, the signal intensity obtained using another uPAR domain I specific mAb, mR1, was significantly reduced upon ATF saturation. Furthermore, when adding ATF, mR4 selectively stained the cleaved receptor. Applying these newly generated mAbs, we additionally demonstrated that cleaved and intact uPAR was evenly distributed on the surface of these cells.

Published

2008

13. Aberrantly glycosylated MUC1 is expressed on the surface of breast cancer cells and a target for antibody-dependent cell-mediated cytotoxicity

Author

Niels Ødum, Kirstine Lavrsen, Hans H. Wandall, Caroline B. Madsen, Henrik Clausen, Morten Grønbech Rasch, Anders Elm Pedersen, Ulla Mandel, and Anders Woetmann

Subjects

Acetylgalactosamine, Glycosylation, medicine.drug_class, medicine.medical_treatment, Antibody Affinity, Breast Neoplasms, Adenocarcinoma, Monoclonal antibody, digestive system, Biochemistry, Epitope, Cancer immunotherapy, medicine, Humans, skin and connective tissue diseases, neoplasms, Molecular Biology, MUC1, Antibody-dependent cell-mediated cytotoxicity, biology, Mucin-1, Antibody-Dependent Cell Cytotoxicity, Cancer, Antibodies, Monoclonal, Cell Biology, Immunotherapy, medicine.disease, Molecular biology, biological factors, digestive system diseases, biology.protein, MCF-7 Cells, Female, Antibody

Abstract

Protein glycosylation often changes during cancer development, resulting in the expression of cancer-associated carbohydrate antigens. In particular mucins such as MUC1 are subject to these changes. We previously identified an immunodominant Tn-MUC1 (GalNAc-α-MUC1) cancer-specific epitope not covered by immunological tolerance in MUC1 humanized mice and man. The objective of this study was to determine if mouse antibodies to this Tn-MUC1 epitope induce antibody-dependent cellular cytotoxicity (ADCC) pivotal for their potential use in cancer immunotherapy. Binding affinity of mAb 5E5 directed to Tn-MUC1 was investigated using BiaCore. The availability of Tn-MUC1 on the surface of breast cancer cells was evaluated by immunohistochemistry, confocal microscopy, and flow cytometry, followed by in vitro assessment of antibody-dependent cellular cytotoxicity by mAb 5E5. Biacore analysis demonstrated high affinity binding (KD = 1.7 nM) of mAb 5E5 to its target, Tn-MUC1. Immunolabelling with mAb 5E5 revealed surface expression of the Tn-MUC1 epitope in breast cancer tissue and cell lines, and mAb 5E5 induced ADCC in two human breast cancer cell lines, MCF7 and T47D. Aberrantly glycosylated MUC1 is expressed on the surface of breast cancer cells and a target for antibody-dependent cell-mediated cytotoxicity suggesting that antibodies targeting glycopeptide epitopes on mucins are strong candidates for cancer-specific immunotherapies.

Published

2012

14. Inhibitory Monoclonal Antibodies against Mouse Proteases Raised in Gene-Deficient Mice Block Proteolytic Functions in vivo

Author

Niels Behrendt, Lars H. Engelholm, Morten Grønbech Rasch, Gunilla Høyer-Hansen, Daniel H. Madsen, Ida K. Lund, Jesper Pass, and Signe Ingvarsen

Subjects

Proteases, medicine.drug_class, Mini Review, media_common.quotation_subject, Mouse monoclonal antibodies, Monoclonal antibody, extracellular proteolysis, Epitope, 03 medical and health sciences, In vivo, medicine, Pharmacology (medical), collagen internalization, Receptor, Internalization, 030304 developmental biology, media_common, Pharmacology, 0303 health sciences, plasminogen activation, business.industry, lcsh:RM1-950, 030302 biochemistry & molecular biology, Molecular biology, 3. Good health, Cell biology, Urokinase receptor, lcsh:Therapeutics. Pharmacology, in vivo models, Target protein, business

Abstract

Identification of targets for cancer therapy requires the understanding of the in vivo roles of proteins, which can be derived from studies using gene-targeted mice. An alternative strategy is the administration of inhibitory monoclonal antibodies (mAbs), causing acute disruption of the target protein function(s). This approach has the advantage of being a model for therapeutic targeting. mAbs for use in mouse models can be obtained through immunization of gene-deficient mice with the autologous protein. Such mAbs react with both species-specific epitopes and epitopes conserved between species. mAbs against proteins involved in extracellular proteolysis, including plasminogen activators urokinase plasminogen activator (uPA), tissue-type plasminogen activator (tPA), their inhibitor PAI-1, the uPA receptor (uPAR), two matrix metalloproteinases (MMP9 and MMP14), as well as the collagen internalization receptor uPARAP, have been developed. The inhibitory mAbs against uPA and uPAR block plasminogen activation and thereby hepatic fibrinolysis in vivo. Wound healing, another plasmin-dependent process, is delayed by an inhibitory mAb against uPA in the adult mouse. Thromboembolism can be inhibited by anti-PAI-1 mAbs in vivo. In conclusion, function-blocking mAbs are well-suited for targeted therapy in mouse models of different diseases, including cancer.

Published

2012

15. A new assay for measurement of the liberated domain I of the urokinase receptor in plasma improves the prediction of survival in colorectal cancer

Author

Ida K. Lund, Tine Thurison, Hans Jørgen Nielsen, Morten Grønbech Rasch, Gunilla Høyer-Hansen, Ib Jarle Christensen, and Anne Fog Lomholt

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Colorectal cancer, medicine.drug_class, Clinical Biochemistry, Kaplan-Meier Estimate, Monoclonal antibody, Sensitivity and Specificity, Receptors, Urokinase Plasminogen Activator, Blood plasma, medicine, Biomarkers, Tumor, Humans, Lung cancer, neoplasms, Aged, Aged, 80 and over, Immunoassay, medicine.diagnostic_test, business.industry, Biochemistry (medical), Cancer, Middle Aged, medicine.disease, Prognosis, Protein Structure, Tertiary, Urokinase receptor, Cancer research, Female, Ovarian cancer, business, Colorectal Neoplasms

Abstract

BACKGROUNDThe liberated domain I of the urokinase plasminogen activator receptor [uPAR(I)] is a significant prognostic marker in lung and ovarian cancer, although the uPAR(I) concentration is below the limit of quantification (LOQ) in a substantial proportion of patient samples (Lung Cancer 2005;48:349–55; Clin Cancer Res 2008;14:5785–93; APMIS 2009;117:755–61). This study was undertaken to design an immunoassay with improved functional sensitivity for measuring uPAR(I) and to evaluate the prognostic value of uPAR(I) for colorectal cancer (CRC) patients.METHODSSurface plasmon resonance analysis identified 2 monoclonal antibodies, R3 and R20, that simultaneously bind to the liberated uPAR(I) but not to intact uPAR. We used R3 for capture and Eu-labeled R20 for detection in designing a 2-site sandwich time-resolved fluorescence immunoassay (TR-FIA 4) for measuring liberated uPAR(I). TR-FIA 4 was validated for use with citrated plasma. The prognostic value of the uPAR(I) concentration was evaluated in 298 CRC patients. The Cox proportional hazards model was used for the uni- and multivariate survival analyses.RESULTSThe LOQ was 0.65 pmol/L. Liberated uPAR(I) was measurable in all patient samples with TR-FIA 4. In the multivariate analysis that included sex, age, tumor stage, tumor localization, and adjuvant treatment, the uPAR(I) concentration measured with TR-FIA 4 (hazard ratio, 1.72; 95% CI, 1.15–2.57; P = 0.009), as well as the concentration of intact soluble uPAR plus the cleaved uPAR fragment containing domains II and III, tumor stage, and age were independent predictors of prognosis.CONCLUSIONSTR-FIA 4 has a functional sensitivity improved 4-fold over that of the previous uPAR(I) assay. The uPAR(I) concentration measured with TR-FIA 4 is an independent predictor of prognosis in CRC patients.

Published

2010

16. Dynamic interplay between the collagen scaffold and tumor evolution

Author

Valerie M. Weaver, Mikala Egeblad, and Morten Grønbech Rasch

Subjects

Basement membrane, Scaffold, medicine.diagnostic_test, Tissue Scaffolds, Proteolysis, Cell, Regulator, Cell Biology, Biology, Article, Cell biology, Extracellular matrix, medicine.anatomical_structure, Interstitial matrix, Cell Movement, Neoplasms, medicine, Humans, Collagen, Function (biology)

Abstract

The extracellular matrix (ECM) is a key regulator of cell and tissue function. Traditionally, the ECM has been thought of primarily as a physical scaffold that binds cells and tissues together. However, the ECM also elicits biochemical and biophysical signaling. Controlled proteolysis and remodeling of the ECM network regulate tissue tension, generate pathways for migration, and release ECM protein fragments to direct normal developmental processes such as branching morphogenesis. Collagens are major components of the ECM of which basement membrane type IV and interstitial matrix type I are the most prevalent. Here we discuss how abnormal expression, proteolysis and structure of these collagens influence cellular functions to elicit multiple effects on tumors, including proliferation, initiation, invasion, metastasis, and therapy response.

Published

2010

17. Antibody-mediated targeting of the urokinase-type plasminogen activator proteolytic function neutralizes fibrinolysis in vivo

Author

Kasper Almholt, Niels Behrendt, Ida K. Lund, Leif R. Lund, Henrik Gårdsvoll, Birgitte Rønø, Morten Grønbech Rasch, Gunilla Høyer-Hansen, Annika Jögi, and John Rømer

Subjects

medicine.drug_class, medicine.medical_treatment, Enzyme-Linked Immunosorbent Assay, Biology, Monoclonal antibody, Biochemistry, Models, Biological, Epitope, Antibodies, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Fibrinolysis, medicine, Animals, Molecular Biology, 030304 developmental biology, Urokinase, 0303 health sciences, Antibodies, Monoclonal, Cell Biology, Surface Plasmon Resonance, Molecular biology, Urokinase-Type Plasminogen Activator, In vitro, Recombinant Proteins, Blot, Mice, Inbred C57BL, Kinetics, Liver, 030220 oncology & carcinogenesis, Female, Plasminogen activator, medicine.drug, Protein Binding

Abstract

Urokinase-type plasminogen activator (uPA) plays a central role in tissue remodeling processes. Most of our understanding of the role of uPA in vivo is derived from studies using gene-targeted uPA-deficient mice. To enable in vivo studies on the specific interference with uPA functionality in mouse models, we have now developed murine monoclonal antibodies (mAbs) directed against murine uPA by immunization of uPA-deficient mice with the recombinant protein. Guided by enzyme-linked immunosorbent assay, Western blotting, surface plasmon resonance, and enzyme kinetic analyses, we have selected two highly potent and inhibitory anti-uPA mAbs (mU1 and mU3). Both mAbs recognize epitopes located on the B-chain of uPA that encompasses the catalytic site. In enzyme activity assays in vitro, mU1 blocked uPA-catalyzed plasminogen activation as well as plasmin-mediated pro-uPA activation, whereas mU3 only was directed against the first of these reactions. We additionally provide evidence that mU1, but not mU3, successfully targets uPA-dependent processes in vivo. Hence, systemic administration of mU1 (i) rescued mice treated with a uPA-activable anthrax protoxin and (ii) impaired uPA-mediated hepatic fibrinolysis in tissue-type plasminogen activator (tPA)-deficient mice, resulting in a phenotype mimicking that of uPA;tPA double deficient mice. Importantly, this is the first report demonstrating specific antagonist-directed targeting of mouse uPA at the enzyme activity level in a normal physiological process in vivo.

Published

2008

18. Murine monoclonal antibodies against murine uPA receptor produced in gene-deficient mice: inhibitory effects on receptor-mediated uPA activity in vitro and in vivo

Author

Jesper Pass, Morten Grønbech Rasch, Ida K. Lund, Gunilla Høyer-Hansen, Michael Ploug, Henrik Gårdsvoll, Keld Danø, Leif R. Lund, Birgitte Rønø, John Rømer, and Annika Jögi

Subjects

Time Factors, medicine.drug_class, Cell Survival, Bacterial Toxins, Receptors, Cell Surface, Biology, Monoclonal antibody, Binding, Competitive, Epitope, Cell Line, Receptors, Urokinase Plasminogen Activator, Antigen-Antibody Reactions, Iodine Radioisotopes, Mice, In vivo, medicine, Animals, Humans, Receptor, Mice, Knockout, Antigens, Bacterial, Hybridomas, Dose-Response Relationship, Drug, Macrophages, Cell Membrane, Antibodies, Monoclonal, Plasminogen, Hematology, Molecular biology, Urokinase-Type Plasminogen Activator, In vitro, Peptide Fragments, Protein Structure, Tertiary, Urokinase receptor, Epitope mapping, Cell culture, Female, Immunization, Binding Sites, Antibody, Epitope Mapping

Abstract

SummaryBinding of urokinase plasminogen activator (uPA) to its cellular receptor, uPAR, potentiates plasminogen activation and localizes it to the cell surface. Focal plasminogen activation is involved in both normal and pathological tissue remodeling processes including cancer invasion. The interaction between uPA and uPAR therefore represents a potential target for anti-invasive cancer therapy. Inhibitors of the human uPA-uPAR interaction have no effect in the murine system. To enable in-vivo studies in murine cancer models we have now generated murine monoclonal antibodies (mAbs) against murine uPAR (muPAR) by immunizing uPAR-deficient mice with recombinant muPAR and screened for antibodies, which inhibit the muPA-muPAR interaction. Two of the twelve mAbs obtained, mR1 and mR2, interfered with the interaction between muPAR and the amino-terminal fragment of muPA (mATF) when analyzed by surface plasmon resonance. The epitope for mR1 is located on domain I of muPAR, while that of mR2 is on domains (II-III). In cell binding experiments using radiolabelled mATF, the maximal inhibition obtained with mR1 was 85% while that obtained with mR2 was 50%. The IC50 value for mR1 was 0.67 nM compared to 0.14 nM for mATF. In an assay based on modified anthrax toxins, requiring cell-bound muPA activity for its cytotoxity, a ~50% rescue of the cells could be obtained by addition of mR1. Importantly, in-vivo efficacy of mR1 was demonstrated by the ability of mR1 to rescue mice treated with a lethal dose of uPA-activatable anthrax toxins.

Published

2007

19. Beta cell specific probing with fluorescent exendin-4 is progressively reduced in type 2 diabetic mouse models

Author

Jonas Ahnfelt-Rønne, Morten Grønbech Rasch, Jacob Hecksher-Sørensen, Lauge Schäffer, and Janne Lehtonen

Subjects

0301 basic medicine, Agonist, endocrine system, medicine.medical_specialty, Cell type, medicine.drug_class, Endocrinology, Diabetes and Metabolism, Cell, Mice, Obese, 030209 endocrinology & metabolism, Biology, Diabetes Mellitus, Experimental, Islets of Langerhans, Mice, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Glucagon-Like Peptide 1, In vivo, Insulin-Secreting Cells, Internal medicine, Receptors, Glucagon, medicine, Animals, Hypoglycemic Agents, Venoms, Pancreatic islets, digestive, oral, and skin physiology, Glucagon-like peptide-1, Molecular biology, 030104 developmental biology, medicine.anatomical_structure, Diabetes Mellitus, Type 2, Disease Progression, Exenatide, Beta cell, Peptides, hormones, hormone substitutes, and hormone antagonists, Ex vivo, Research Paper

Abstract

Probes based on GLP-1R agonist exendin-4 have shown promise as in vivo β cell tracers. However, questions remain regarding the β cell specificity of exendin-4 probes, and it is unclear if the expression levels of the GLP-1R are affected in a type 2 diabetic state. Using in vivo probing followed by ex vivo imaging we found fluorescent exendin-4 probes to distinctly label the pancreatic islets in mice in a Glp-1r dependent manner. Furthermore, a co-localization study revealed a near 100 percent β cell specificity with less than one percent probing in other analyzed cell types. We then tested if probing was affected in models of type 2 diabetes using the Lepr(db/db) (db/db) and the Diet-Induced Obese (DIO) mouse. Although nearly all β cells continued to be probed, we observed a progressive decline in probing intensity in both models with the most dramatic reduction seen in db/db mice. This was paralleled by a progressive decrease in Glp-1r protein expression levels. These data confirm β cell specificity for exendin-4 based probes in mice. Furthermore, they also suggest that GLP-1R targeting probes may provide a tool to monitor β cell function rather than mass in type 2 diabetic mouse models.

Published

2015

20. Abstract 2465: Matrix metalloproteinase 9 promotes breast cancer through regulation of insulin-like growth factor-binding proteins

Author

Jing Qiu, Ida K. Lund, Mikala Egeblad, Zena Werb, Morten Grønbech Rasch, and Jae-Hyun Park

Subjects

Cancer Research, medicine.medical_specialty, biology, Mouse mammary tumor virus, Wild type, Cancer, MMP9, Matrix metalloproteinase, medicine.disease, biology.organism_classification, Insulin-like growth factor-binding protein, body regions, Breast cancer, Endocrinology, Oncology, Tumor progression, Internal medicine, medicine, biology.protein

Abstract

The matrix metalloproteinase (MMP) family is a large family of extracellularly acting proteases. MMP9 is expressed by tumor infiltrating myeloid cells and promotes tumor progression in animal models of cancer. Yet, the identities of the in vivo MMP9 substrates are not well established. Furthermore, clinical trials with broad-spectrum MMP inhibitors have shown no therapeutic benefit. We compared the effects of deleting Mmp9 between the luminal mouse mammary tumor virus (MMTV)-Neu model of breast cancer, driven by expression of rodent HER2/ErbB2, and the basal-like C3(1) SV40 large T antigen (Tag) model, driven through inactivation of p53 and Rb by Tag. Interestingly, absence of MMP9 delayed tumor-onset in C3(1)-Tag mice, but had no effect in the MMTV-Neu mice. In line with these data, we found that low MMP9 expression indeed predicts good prognosis for breast cancer patients with mutant p53, but does not influence prognosis for patients with wild type p53. The insulin-like growth factor-binding protein-1 (IGFBP-1) is an established in vitro MMP9 substrate. IGFBP-1 sequesters IGF in the extracellular matrix, leading to reduced IGF receptor activity and thereby cancer cell proliferation. Proteolysis of IGFBP by MMP9 releases IGF from the matrix. Interestingly, the protein levels of IGFBP-1 were significantly increased in the C3(1)-Tag;Mmp9−/− compared to C3(1)-Tag;Mmp9+/+ tumors. In contrast, IGFBP-1 protein levels were low in the MMTV-Neu model regardless of MMP9 status. Human breast tumors did not express IGFBP-1 but instead the other family members, IGFBP-2, -3, and -4, which all are substrates for MMP9 in vitro. We found that low levels of MMP9 were a good prognostic factor only for patients with high mRNA expression levels of the IGFBPs, and not for patients with low levels of the IGFBPs. Our findings from mouse models and human patients suggest that MMP9 promotes tumor progression in breast cancer via proteolysis of IGFBPs. Furthermore, a lack of stratification of patients based on both MMP9 and IGFBPs levels might explain why MMP inhibitors showed no clinical benefit against breast cancer. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr 2465. doi:1538-7445.AM2012-2465

Published

2012

21. Abstract 4401: Antibody-mediated targeting of the uPA proteolytic activity neutralizes uPA functions in vivo

Author

Ida K. Lund, Leif R. Lund, Gunilla Høyer-Hansen, Birgitte Rønø, Henrik Gårdsvoll, Niels Behrendt, Morten Grønbech Rasch, Annika Jögi, John Rømer, and Kasper Almholt

Subjects

Cancer Research, biology, business.industry, medicine.drug_class, Lewis lung carcinoma, Monoclonal antibody, In vitro, Epitope, Blot, Oncology, In vivo, Immunology, biology.protein, Cancer research, Medicine, Antibody, business, Plasminogen activator

Abstract

Urokinase-type plasminogen activator (uPA) plays a central role in tissue remodeling processes, during both normal physiological conditions and cancer progression. Most of our understanding of the role of uPA in vivo is derived from studies using gene-targeted uPA-deficient mice. To enable in vivo studies on the acute and specific interference with uPA functionality in adult mice, we have now developed murine monoclonal antibodies (mAbs) directed against murine uPA by immunization of uPA-deficient mice with the recombinant protein. Guided by ELISA, Western blotting, SPR and enzyme kinetic analyses, we have selected two highly potent and inhibitory anti-uPA mAbs (mU1 and mU3). Both mAbs recognize epitopes located on the B-chain of uPA that encompasses the catalytic site. In activity assays in vitro, mU1 blocked uPA-catalyzed plasminogen activation as well as plasmin-mediated pro-uPA activation, whereas mU3 only was directed against the first of these reactions. We provide evidence that acute disruption of uPA activity in the adult mouse was effective with mU1, but not mU3, because only mU1 rescued mice treated with a uPA-activable anthrax pro-toxin. Moreover, systemic administration of mU1 (i) delayed wound healing in tissue-type plasminogen activator (tPA)-deficient mice, and (ii) impaired uPA-mediated hepatic fibrinolysis in tPA-deficient mice, resulting in a phenotype mimicking that of uPA;tPA double-deficient mice. Importantly, these results demonstrate the specific antagonist-directed targeting of mouse uPA at the enzyme activity level in normal physiological processes in vivo. Preliminary results indicate that wild-type mice, which have been transplanted with murine Lewis lung carcinoma cells, display significant reduction in primary tumour growth, when treated with mU1 as compared to placebo-treated (i.e. PBS-treated) littermates. We thus suggest that mU1 is an excellent mAb candidate for therapeutic intervention studies in mouse cancer models. Note: This abstract was not presented at the AACR 101st Annual Meeting 2010 because the presenter was unable to attend. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 101st Annual Meeting of the American Association for Cancer Research; 2010 Apr 17-21; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2010;70(8 Suppl):Abstract nr 4401.

Published

2010

22. 24 Specific targeting of uPA activity with a monoclonal antibody neutralizeS uPA-dependent effects in vivo

Author

Henrik Gårdsvoll, Kasper Almholt, Niels Behrendt, Leif R. Lund, Gunilla Høyer-Hansen, Morten Grønbech Rasch, Annika Jögi, Ida K. Lund, Birgitte Rønø, and John Rømer

Subjects

Microbiology (medical), In vivo, medicine.drug_class, Chemistry, medicine, Cancer research, Immunology and Allergy, General Medicine, Monoclonal antibody, Pathology and Forensic Medicine

Published

2008

23. 31 In vivo inhibition of the murine uPA-uPAR interaction and selective identification of muPAR variants on cells using monoclonal antibodies raised in uPAR deficient mice

Author

Morten Grønbech Rasch, Annika Jögi, Ida K. Lund, Leif R. Lund, Gunilla Høyer-Hansen, Henrik Gårdsvoll, Jesper Pass, and Birgitte Rønø

Subjects

Microbiology (medical), Chemistry, medicine.drug_class, General Medicine, Monoclonal antibody, Molecular biology, Pathology and Forensic Medicine, Urokinase receptor, On cells, In vivo, medicine, Deficient mouse, Immunology and Allergy, Identification (biology)

Published

2008

24. Distribution and ultrastructural localization of the glucagon-like peptide-1 receptor (GLP-1R) in the rat brain

Author

Yvette Ruska, Balázs Gereben, Anett Szilvásy-Szabó, Morten Grønbech Rasch, Lotte Bjerre Knudsen, Charles Pyke, Richárd Sinkó, Thomas Egebjerg, Erzsébet Farkas, and Csaba Fekete

Subjects

0301 basic medicine, Male, endocrine system, Histology, Immunocytochemistry, Axonal localization, 030209 endocrinology & metabolism, GLP-1 receptor, Distribution, Glucagon-Like Peptide-1 Receptor, Rats, Sprague-Dawley, 03 medical and health sciences, 0302 clinical medicine, Arcuate nucleus, medicine, Electron microscopy, Glucose homeostasis, Animals, Axon, Circumventricular organs, Neurons, Arc (protein), Chemistry, General Neuroscience, digestive, oral, and skin physiology, Brain, Immunohistochemistry, Cell biology, Rats, 030104 developmental biology, medicine.anatomical_structure, Original Article, Brainstem, Anatomy, Nucleus, hormones, hormone substitutes, and hormone antagonists

Abstract

Glucagon-like peptide-1 (GLP-1) inhibits food intake and regulates glucose homeostasis. These actions are at least partly mediated by central GLP-1 receptor (GLP-1R). Little information is available, however, about the subcellular localization and the distribution of the GLP-1R protein in the rat brain. To determine the localization of GLP-1R protein in the rat brain, immunocytochemistry was performed at light and electron microscopic levels. The highest density of GLP-1R-immunoreactivity was observed in the circumventricular organs and regions in the vicinity of these areas like in the arcuate nucleus (ARC) and in the nucleus tractus solitarii (NTS). In addition, GLP-1R-immunreactive (IR) neuronal profiles were also observed in a number of telencephalic, diencephalic and brainstem areas and also in the cerebellum. Ultrastructural examination of GLP-1R-immunoreactivity in energy homeostasis related regions showed that GLP-1R immunoreactivity is associated with the membrane of perikarya and dendrites but GLP-1R can also be observed inside and on the surface of axon varicosities and axon terminals. In conclusion, in this study we provide a detailed map of the GLP-1R-IR structures in the CNS. Furthermore, we demonstrate that in addition to the perikaryonal and dendritic distribution, GLP-1R is also present in axonal profiles suggesting a presynaptic action of GLP-1. The very high concentration of GLP-1R-profiles in the circumventricular organs and in the ARC and NTS suggests that peripheral GLP-1 may influence brain functions via these brain areas. Supplementary Information The online version contains supplementary material available at 10.1007/s00429-020-02189-1.