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461 results on '"Hilgendorf I"'

1. Everolimus-Loaded Reconstituted High-Density Lipoprotein Prepared by a Novel Dual Centrifugation Approach for Anti-Atherosclerotic Therapy

Author

Deuringer B, Härdtner C, Krebs K, Thomann R, Holzer M, Hilgendorf I, and Süss R

Subjects
atherosclerosis, cholesterol efflux, drug delivery, everolimus, proliferation, protein-conjugate, Medicine (General), R5-920
Abstract

Benedikt Deuringer,1 Carmen Härdtner,2 Katja Krebs,2 Ralf Thomann,3 Martin Holzer,1 Ingo Hilgendorf,2,4,* Regine Süss1,* 1Department of Pharmaceutical Technology and Biopharmacy, Institute of Pharmaceutical Sciences, University of Freiburg, Freiburg, 79104, Germany; 2Department of Cardiology and Angiology, University Heart Center Freiburg-Bad Krozingen and Faculty of Medicine, University of Freiburg, Freiburg, 79106, Germany; 3FMF Materials Research Center, University of Freiburg, Freiburg, 79104, Germany; 4Institute for Experimental Cardiovascular Medicine, University Heart Center Freiburg-Bad Krozingen and Faculty of Medicine, University of Freiburg, Freiburg, 79110, Germany*These authors contributed equally to this workCorrespondence: Benedikt Deuringer, Pharmaceutical Technology and Biopharmacy, Sonnenstraße 5, Freiburg, 79104, Germany, Tel +49 761 203 6329, Fax +49 761 203 6326, Email bdeuringer@pharmazeutischetechnologie.dePurpose: The conventional techniques for the preparation of reconstituted high-density lipoprotein (rHDL) are hampered by long process times, the need for large amounts of starting material, and harsh preparation conditions. Here, we present a novel rHDL preparation method to overcome these challenges. Furthermore, we propose a dual mode of action for rHDL loaded with the immunosuppressant drug everolimus (Eve-rHDL) in the context of atherosclerosis and cardiovascular disease.Methods: We use dual centrifugation for rHDL nanoparticle preparation and characterize the physicochemical properties by NS-TEM, N-PAGE, DLS, AF4, and HPLC. In addition, we determine the biological efficacy in human and murine cell culture with regard to cellular uptake, cholesterol efflux, and proliferation.Results: We confirm the characteristic particle size of 10 nm, discoidal morphology, and chemical composition of the rHDL preparations and identify dual centrifugation as an ideal method for cost-effective aseptic rHDL manufacturing. rHDL can be prepared in approx. 1.5 h with batch sizes as little as 89 μL. Moreover, we demonstrate the cholesterol efflux capacity and anti-proliferative activity of Eve-rHDL in vitro. The anti-proliferative effects were comparable to free Eve, thus confirming the suitability of rHDL as a capable drug delivery vehicle.Conclusion: Eve-rHDL shows great efficacy in vitro and may further be employed to target atherosclerotic plaques in vivo. Highly effective anti-atherosclerotic therapy might be feasible by reducing both inflammatory- and lipid burden of the plaques. Dual centrifugation is an ideal technique for the efficient application of the rHDL platform in cardiovascular disease and beyond.Keywords: atherosclerosis, cholesterol efflux, drug delivery, everolimus, proliferation, protein-conjugate

Published
2022

3. GPR15-dependent T cell recruitment in the acute phase of viral myocarditis is associated with improved virus elimination and outcome

Author

Lindner, D, primary, Brauninger, H, additional, Stoffers, B, additional, Bacmeister, L, additional, Kupsch, S, additional, Vico, T, additional, Marchini, T, additional, Escher, F, additional, Klingel, K, additional, Kirchhof, P, additional, Blankenberg, S, additional, Zeller, T, additional, Wolf, D, additional, Hilgendorf, I, additional, and Westermann, D, additional

Published
2024
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10. Recruited macrophages incorporate into the resident cardiac macrophage pool and converge into a common phenotype in the healing infarct, but not in the failing heart exposed to pressure overload

Author

Vico, T, primary, Taglinger, M, additional, Haacke, V, additional, Zehender, C, additional, Heinz, B, additional, Von Ehr, A, additional, Dederichs, T, additional, Ehlert, C, additional, Dufner, B, additional, Westermann, D, additional, and Hilgendorf, I, additional

Published
2023
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14. DNMT3A CHIP-driver mutations IGNITE the bone marrow

Author

Dederichs, T.-S., primary, Ehlert, C., additional, Becker, H., additional, Pfeifer, D., additional, Niemoeller, C., additional, Anto-Michel, N., additional, Zirlik, A., additional, Bode, C., additional, Wolf, D., additional, Von Zur Mühlen, C., additional, Kaier, K., additional, Preissl, S., additional, Heidt, T., additional, Westermann, D., additional, and Hilgendorf, I., additional

Published
2023
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18. Spätfolgen der allogenen Blutstammzelltransplantation

Author

Hilgendorf, I., Hochhaus, A., Adamietz, Irenäus A., editor, Bechstein, Wolf O., editor, Christiansen, Hans, editor, Doehn, Christian, editor, Hochhaus, Andreas, editor, Hofheinz, Ralf-Dieter, editor, Lichtenegger, Werner, editor, Lordick, Florian, editor, Schadendorf, Dirk, editor, Untch, Michael, editor, and Wittekind, Christian, editor

Published
2016
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19. Comprehensive assessments and related interventions to enhance the long-term outcomes of child, adolescent and young adult cancer survivors – presentation of the CARE for CAYA-Program study protocol and associated literature review

Author

Salchow, J., Mann, J., Koch, B., von Grundherr, J., Jensen, W., Elmers, S., Straub, L. A., Vettorazzi, E., Escherich, G., Rutkowski, S., Dwinger, S., Bergelt, C., Sokalska-Duhme, M., Bielack, S., Calaminus, G., Baust, K., Classen, C. F., Rössig, C., Faber, J., Faller, H., Hilgendorf, I., Gebauer, J., Langer, T., Metzler, M., Schuster, S., Niemeyer, C., Puzik, A., Reinhardt, D., Dirksen, U., Sander, A., Köhler, M., Habermann, J. K., Bokemeyer, C., and Stein, A.

Published
2020
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20. Das CARE-for-CAYA-Programm: Präventionskonzept für junge Menschen nach Krebserkrankung

Author

Quidde, J., Koch, B., Salchow, J., Jensen, W., von Grundherr, J., Escherich, G., Rutkowski, S., Schulz-Kindermann, F., Bergelt, C., Bokemeyer, C., Sokalska-Duhme, M., Bielack, S., Calaminus, G., Classen, C. F., Rössig, C., Faber, J., Faller, H., Hilgendorf, I., Langer, T., Metzler, M., Schuster, S., Niemeyer, C., Pierce, A., Reinhardt, D., Sander, A., Köhler, M., and Stein, A.

Published
2017
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21. GPR55 deficiency in B-cells promotes atherosclerosis and regulates plasma cell maturation

Author

Guillamat-Prats, R, primary, Hering, D, additional, Rami, M, additional, Haerdtner, C, additional, Santovito, D, additional, Rinne, P, additional, Pagano, S, additional, Nicolas Vuilleumier, N, additional, Schmid, S, additional, Janjic, A, additional, Enard, W, additional, Weber, C, additional, Maegdefessel, L, additional, Hilgendorf, I, additional, and Steffens, S, additional

Published
2022
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22. The role of P2Y12 in cardiovascular disease beyond atherothrombosis: P2Y12 signaling promotes emergency hematopoiesis after myocardial infarction

Author

Seung, H, primary, Wrobel, J, additional, Wadle, C, additional, Buehler, T, additional, Chiang, D, additional, Rettkowski, J, additional, Cabezas-Wallscheid, N, additional, Hechler, B, additional, Wolf, D, additional, Duerschmied, D, additional, Idzko, M, additional, Bode, C, additional, Von Zur Muehlen, C, additional, Hilgendorf, I, additional, and Heidt, T, additional

Published
2022
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23. NLRP3 mediates atheromatous plaque macrophage proliferation

Author

Haerdtner, C, primary, Remmersmann, F, additional, Von Ehr, A, additional, Dederichs, T S, additional, Vico, T, additional, Krebs, K, additional, Wolf, D, additional, Sager, H, additional, Bode, C, additional, Westermann, D, additional, and Hilgendorf, I, additional

Published
2022
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25. B cell-specific GPR55 deficiency promotes atherosclerosis

Author

Guillamat-Prats, R., primary, Hering, D., additional, Rami, M., additional, Hädtner, C., additional, Santovito, D., additional, Rinne, P., additional, Bindila, L., additional, Hristov, M., additional, Pagano, S., additional, Vuilleumier, N., additional, Schmid, S., additional, Janjic, A., additional, Enard, W., additional, Weber, C., additional, Maegdefessel, L., additional, Faussner, A., additional, Hilgendorf, I., additional, and Steffens, S., additional

Published
2022
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34. P2Y12 Inhibition in Murine Myocarditis Results in Reduced Platelet Infiltration and Preserved Ejection Fraction

Author

Schmidt, SN, Reichardt, W, Kaufmann, BA, Wadle, C, von Elverfeldt, D, Stachon, P, Hilgendorf, I, Wolf, D, Heidt, T, Duerschmied, D, Peter, K, Bode, C, von zur Muehlen, C, Maier, A, Schmidt, SN, Reichardt, W, Kaufmann, BA, Wadle, C, von Elverfeldt, D, Stachon, P, Hilgendorf, I, Wolf, D, Heidt, T, Duerschmied, D, Peter, K, Bode, C, von zur Muehlen, C, and Maier, A

Abstract

Previous mouse studies have shown the increased presence of platelets in the myocardium during early stages of myocarditis and their selective detection by MRI. Here, we aimed to depict early myocarditis using molecular contrast-enhanced ultrasound of activated platelets, and to evaluate the impact of a P2Y12 receptor platelet inhibition. Experimental autoimmune myocarditis was induced in BALB/c mice by subcutaneous injection of porcine cardiac myosin and complete Freund adjuvant (CFA). Activated platelets were targeted with microbubbles (MB) coupled to a single-chain antibody that binds to the "ligand-induced binding sites" of the GPIIb/IIIa-receptor (=LIBS-MB). Alongside myocarditis induction, a group of mice received a daily dose of 100 g prasugrel for 1 month. Mice injected with myosin and CFA had a significantly deteriorated ejection fraction and histological inflammation on day 28 compared to mice only injected with myosin. Platelets infiltrated the myocardium before reduction in ejection fraction could be detected by echocardiography. No selective binding of the LIBS-MB contrast agent could be detected by either ultrasound or histology. Prasugrel therapy preserved ejection fraction and significantly reduced platelet aggregates in the myocardium compared to mice without prasugrel therapy. Therefore, P2Y12 inhibition could be a promising early therapeutic target in myocarditis, requiring further investigation.

Published
2021

39. Current practice in nutrition after allogeneic hematopoietic stem cell transplantation – Results from a survey among hematopoietic stem cell transplant centers

Author

Toenges, R., primary, Greinix, H., additional, Lawitschka, A., additional, Halter, J., additional, Baumgartner, A., additional, Simon, A., additional, Arends, J., additional, Jäger, P., additional, Middeke, M., additional, Hilgendorf, I., additional, Klein, S., additional, Wagner-Drouet, E.M., additional, Schmid, C., additional, Bug, G., additional, and Wolff, D., additional

Published
2021
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40. Transcriptomic characterization of human choroidal neovascular membranes identifies calprotectin as a novel biomarker for patients with AMD

Author

Lange, C, Schlecht, A, Boneva, S, Wolf, J, Zhang, P, Prinz, G, Horres, R, Bucher, F, Auw-Haedrich, C, Hansen, L, Stahl, A, Hilgendorf, I, Agostini, H, Wieghofer, P, and Schlunck, G

Subjects
ddc: 610, 610 Medical sciences, Medicine, eye diseases
Abstract

Purpose: Although genome-wide association studies, animal models, and cell culture systems have yielded important insights into the pathogenesis of neovascular age-related macular degeneration (nAMD), the underlying molecular pathways remain ill defined. The current study aims to explore the transcriptome[for full text, please go to the a.m. URL], 7th International Symposium on AMD: Age-related Macular Degeneration - Understanding Pathogenetic Mechanisms of Disease

Published
2020
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42. Evaluation of pregnancies after allogeneic stem cell transplantation during the last 15years in Germany

Author

Sockel, K., Frank, S., Neu, A., Ditschkowski, M., Hilgendorf, I., Goeckenjan, M., Stoelzel, F., Middeke, J. M., Kroeger, N., Ayuketang, Ayuk F., Eder, M., Bethge, W., Finke, J., Bertz, H., Kobbe, G., Kaufmann, M., Platzbecker, U., Beverungen, D., Schmid, C., von Bonin, M., Heberling, L., Teipel, R., Bug, G., Fraccaroli, A., Tischer, J., Holler, B., Wolff, D., Luft, T., Roesler, W., Schaefer-Eckart, K., Dressler, S., Scheid, C., Holtick, U., Klein, S., Blau, I. -W., Burchert, A., Wulf, G., Hasenkamp, J., Kaun, S., Wittke, C., Wortmann, F., Bornhaeuser, M., Schetelig, J., Sockel, K., Frank, S., Neu, A., Ditschkowski, M., Hilgendorf, I., Goeckenjan, M., Stoelzel, F., Middeke, J. M., Kroeger, N., Ayuketang, Ayuk F., Eder, M., Bethge, W., Finke, J., Bertz, H., Kobbe, G., Kaufmann, M., Platzbecker, U., Beverungen, D., Schmid, C., von Bonin, M., Heberling, L., Teipel, R., Bug, G., Fraccaroli, A., Tischer, J., Holler, B., Wolff, D., Luft, T., Roesler, W., Schaefer-Eckart, K., Dressler, S., Scheid, C., Holtick, U., Klein, S., Blau, I. -W., Burchert, A., Wulf, G., Hasenkamp, J., Kaun, S., Wittke, C., Wortmann, F., Bornhaeuser, M., and Schetelig, J.

Published
2020

43. Molecular magnetic resonance imaging of activated platelets allows noninvasive detection of early myocarditis in mice

Author

Maier, A, Braig, M, Jakob, K, Bienert, T, Schaeper, M, Merkle, A, Wadle, C, Menza, M, Neudorfer, I, Bojti, I, Stachon, P, Duerschmied, D, Hilgendorf, I, Heidt, T, Bode, C, Peter, K, Klingel, K, von Elverfeldt, D, Muehlen, CVZ, Maier, A, Braig, M, Jakob, K, Bienert, T, Schaeper, M, Merkle, A, Wadle, C, Menza, M, Neudorfer, I, Bojti, I, Stachon, P, Duerschmied, D, Hilgendorf, I, Heidt, T, Bode, C, Peter, K, Klingel, K, von Elverfeldt, D, and Muehlen, CVZ

Abstract

MRI sensitivity for diagnosis and localization of early myocarditis is limited, although it is of central clinical interest. The aim of this project was to test a contrast agent targeting activated platelets consisting of microparticles of iron oxide (MPIO) conjugated to a single-chain antibody directed against ligand-induced binding sites (LIBS) of activated glycoprotein IIb/IIIa (= LIBS-MPIO). Myocarditis was induced by subcutaneous injection of an emulsion of porcine cardiac myosin and complete Freund's adjuvant in mice. 3D 7 T in-vivo MRI showed focal signal effects in LIBS-MPIO injected mice 2 days after induction of myocarditis, whereas in control-MPIO injected mice no signal was detectable. Histology confirmed CD41-positive staining, indicating platelet involvement in myocarditis in mice as well as in human specimens with significantly higher LIBS-MPIO binding compared to control-MPIO in both species. Quantification of the myocardial MRI signal confirmed a signal decrease after LIBS-MPIO injection and significant less signal in comparison to control-MPIO injection. These data show, that platelets are involved in inflammation during the course of myocarditis in mice and humans. They can be imaged non-invasively with LIBS-MPIO by molecular MRI at an early time point of the inflammation in mice, which is a valuable approach for preclinical models and of interest for both diagnostic and prognostic purposes.

Published
2020

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