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1. Histological and SEM assessment of blood stasis in kidney blood vessels after pepeated intra-arterial application of radiographic contrast media

Author

Lamby, Philipp, Minkow, Alexander, Handt, Stefan, Falter, Johannes, Schellenberg, Eva-Lotte, Graf, Stefanie, Hiebl, Bernhard, Haerteis, Silke, Gemeinhardt, Ole, Krüger-Genge, Anne, Klosterhalfen, Bernd, Jung, Ernst-Michael, Franke, Ralf-Peter, Momeni, Arash, Prantl, Lukas, and Jung, Friedrich

Subjects
610 Medizin, IODIXANOL, IOPROMIDE, Nephrotoxizität, Article, Kidney, Pathology, DDC 570 / Life sciences, renal pathology, ddc:570, 570 Biowissenschaften, Biologie, Iopromid, ddc:610, lcsh:Science, acute kidney injury, nephrotoxicity, nephropathy, iodinated contrast media, electron microscopy, histopathology, Contrast media, Microcirculation, Injuries, Histopathologie, Microscopy, Electron, Nierenverletzung, lcsh:Q, INDUCED NEPHROPATHY, DDC 610 / Medicine & health, ERYTHROCYTE MORPHOLOGY, Mikrozirkulation
Abstract

Background: After application of iodinated contrast media (CM), a pronounced deterioration of the microcirculation in skin and myocardium was reported. Clinically, the repeated application of CM, especially, led to an increase of the renal resistance index (RRI). With respect to the transiency of the RRI increase, it is reasonable to assume that the deterioration of blood flow could be due to transient blood stasis caused by reversible morphologic cell alterations due to osmotic discrepancies between CM and human blood. Therefore, the hypothesis was investigated whether CM are able to induce in vivo such blood stasis and cell deformations in the renal vasculature of well-hydrated pigs. Methods: The in vivo study was performed as a prospective randomized examination to compare the effects of two different CM in 16 pigs (German Landrace). Pigs were randomized to receive either Iodixanol (n = 8), or Iopromide (n = 8). Each animal received 10 injections separated by 5-min intervals via the suprarenal aorta at a rate of 10 mL/s according to the usual procedure during a cardiac catheter examination. Finally, the kidneys were explanted and processed for histology (H & E staining and fibrin staining according to Weigert) as well as for scanning electron microscopy (SEM) with regards to morphologic correlates explaining the changes in the microcirculation. Results: In each of the predefined four categories of vascular diameters, blood stasis were found, but clearly more often after application of Iopromide than after application of Iodixanol (p < 0.001). In addition, Iopromide induced more blood stasis in all of the examined kidney regions compared to Iodixanol (p = 0.0001). There were no obstructive events in the middle cortex following the application of Iodixanol. Except for the region around a puncture channel of a placed-in catheter probe, no fibrin was detected in Weigert’s fibrin-stained samples, neither around the histologically assessed thrombi nor in vessels with blood stasis. Complementary SEM analyses revealed in a few cases only a slight generation of fibrin and thrombi and deformations, such as echinocyte and “box-like” deformations. Conclusions: According to previous in vitro studies, pathological erythrocyte deformations, such as echinocyte and box-like formation of erythrocytes, were observed also in vivo. In addition, blood stasis and/or thrombi could be detected in histological samples from explanted kidneys from young pigs after repeated in vivo administration of CM. In only a few cases, mural platelet aggregates within minimal fibrin meshes occurred only after the application of Iopromide.

Published
2020
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2. In Vitro Thrombogenicity Testing of Biomaterials

Author

Braune, Steffen (Dr.), Latour, Robert A., Reinthaler, Markus, Landmesser, Ulf, Lendlein, Andreas, and Jung, Friedrich

Subjects
ddc:570, Institut für Chemie
Abstract

The short- and long-term thrombogenicity of implant materials is still unpredictable, which is a significant challenge for the treatment of cardiovascular diseases. A knowledge-based approach for implementing biofunctions in materials requires a detailed understanding of the medical device in the biological system. In particular, the interplay between material and blood components/cells as well as standardized and commonly acknowledged in vitro test methods allowing a reproducible categorization of the material thrombogenicity requires further attention. Here, the status of in vitro thrombogenicity testing methods for biomaterials is reviewed, particularly taking in view the preparation of test materials and references, the selection and characterization of donors and blood samples, the prerequisites for reproducible approaches and applied test systems. Recent joint approaches in finding common standards for a reproducible testing are summarized and perspectives for a more disease oriented in vitro thrombogenicity testing are discussed.

Published
2019

3. Vascular Endothelial Cell Biology: An Update

Author

Krüger-Genge, Anne, Blocki, Anna, Franke, Ralf-Peter, Jung, Friedrich, and Publica

Subjects
Blood Platelets, endothelium, Review, Blood-vessels Growth, Angiogenese, shear stress, lcsh:Chemistry, angiogenesis, DDC 570 / Life sciences, Glycocalyces, ddc:570, Leukocytes, Animals, Humans, Endothelium, Glykokalyx, Shear-Stress, lcsh:QH301-705.5, thrombosis, Endothelial Cells, Thrombosis, Thrombose, lcsh:Biology (General), lcsh:QD1-999, Regional Blood Flow, Endothelium, Vascular, glycocalyx
Abstract

The vascular endothelium, a monolayer of endothelial cells (EC), constitutes the inner cellular lining of arteries, veins and capillaries and therefore is in direct contact with the components and cells of blood. The endothelium is not only a mere barrier between blood and tissues but also an endocrine organ. It actively controls the degree of vascular relaxation and constriction, and the extravasation of solutes, fluid, macromolecules and hormones, as well as that of platelets and blood cells. Through control of vascular tone, EC regulate the regional blood flow. They also direct inflammatory cells to foreign materials, areas in need of repair or defense against infections. In addition, EC are important in controlling blood fluidity, platelet adhesion and aggregation, leukocyte activation, adhesion, and transmigration. They also tightly keep the balance between coagulation and fibrinolysis and play a major role in the regulation of immune responses, inflammation and angiogenesis. To fulfill these different tasks, EC are heterogeneous and perform distinctly in the various organs and along the vascular tree. Important morphological, physiological and phenotypic differences between EC in the different parts of the arterial tree as well as between arteries and veins optimally support their specified functions in these vascular areas. This review updates the current knowledge about the morphology and function of endothelial cells, particularly their differences in different localizations around the body paying attention specifically to their different responses to physical, biochemical and environmental stimuli considering the different origins of the EC.

Published
2019

4. Effect of iodinated contrast media on renal perfusion: A randomized comparison study in pigs using quantitative contrast-enhanced ultrasound (CEUS)

Author

Lamby, Philipp, Jung, Friedrich, Graf, Stefanie, Schellenberg, Lotte, Falter, Johannes, Platz Batista da Silva, Natascha, Schreml, Stephan, Prantl, Lukas, Franke, Ralf P., and Jung, Ernst M.

Subjects
ddc:610, Swine, Iohexol, Microcirculation, lcsh:R, 610 Medizin, Hemodynamics, lcsh:Medicine, Contrast Media, Kidney, Article, ACUTE KIDNEY INJURY, HUMAN ERYTHROCYTES, MICROCIRCULATION, MORPHOLOGY, DISEASE, OSMOLAR, ULTRASONOGRAPHY, DIFFERENTIATION, INTRAARTERIAL, MORTALITY, Triiodobenzoic Acids, Animals, lcsh:Q, lcsh:Science
Abstract

The administration of iodinated contrast media (CM) can cause microcirculatory disorder leading to acute renal dysfunction. In a prospective, randomized investigation two CM (Iodixanol vs Iopromide) were compared in 16 pigs. Each animal received 10 intra-aortal injections (5 ml Iodixanol or 4.32 ml Iopromide). Microcirculation was assessed using contrast-enhanced ultrasound (CEUS) directly on the kidney surface using time-to-peak (TTP) and blood-volume-analysis. Macroscopic observations were documented. Post mortem residual CM distribution in the kidneys was detected using X-ray. TTP was significantly prolonged over the descending vasa recta of the Iopromide group. This coincided with a visible marble-like pattern on the kidney surface occurring in 30 out of 80 Iopromide-injections but in 4 out of 80 Iodixanol-injections (p = 0.007). The blood volume over the entire kidney did not change after Iodixanol-application, but decreased by about 6.1% after Iopromide-application. The regional blood volume in the renal cortex showed a tendency to decrease by about 13.5% (p = 0.094) after Iodixanol-application, and clearly decreased by about 31.7% (p = 0.022) after Iopromide-application. The study revealed a consistent influence of repeated injections of two different CM on the kidney perfusion using three different imaging methods (CEUS analysis, macroscopic observation and X-ray analysis).

Published
2017
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5. Adhesion and activation of platelets from subjects with coronary artery disease and apparently healthy individuals on biomaterials

Author

Braune, Steffen, Gross, M., Walter, M., Zhou, Shengqiang, Dietze, Siegfried, Rutschow, S., Lendlein, Andreas, Tschoepe, C., and Jung, Friedrich

Subjects
Institut für Chemie
Abstract

On the basis of the clinical studies in patients with coronary artery disease (CAD) presenting an increased percentage of activated platelets, we hypothesized that hemocompatibility testing utilizing platelets from healthy individuals may result in an underestimation of the materials' thrombogenicity. Therefore, we investigated the interaction of polymer-based biomaterials with platelets from CAD patients in comparison to platelets from apparently healthy individuals. In vitro static thrombogenicity tests revealed that adherent platelet densities and total platelet covered areas were significantly increased for the low (polydimethylsiloxane, PDMS) and medium (Collagen) thrombogenic surfaces in the CAD group compared to the healthy subjects group. The area per single platelet—indicating the spreading and activation of the platelets—was markedly increased on PDMS treated with PRP from CAD subjects. This could not be observed for collagen or polytetrafluoroethylene (PTFE). For the latter material, platelet adhesion and surface coverage did not differ between the two groups. Irrespective of the substrate, the variability of these parameters was increased for CAD patients compared to healthy subjects. This indicates a higher reactivity of platelets from CAD patients compared to the healthy individuals. Our results revealed, for the first time, that utilizing platelets from apparently healthy donors bears the risk of underestimating the thrombogenicity of polymer-based biomaterials.

Published
2016

6. Poly(ethylene glycol) grafting to Poly(ether imide) membranes - influence on protein adsorption and Thrombocyte adhesion

Author

Neffe, Axel Thomas, von Rüsten-Lange, Maik, Braune, Steffen, Lützow, Karola, Roch, Toralf, Richau, Klaus, Jung, Friedrich, and Lendlein, Andreas

Subjects
technology, industry, and agriculture, Institut für Chemie
Abstract

The chain length and end groups of linear PEG grafted on smooth surfaces is known to influence protein adsorption and thrombocyte adhesion. Here, it is explored whether established structure function relationships can be transferred to application relevant, rough surfaces. Functionalization of poly(ether imide) (PEI) membranes by grafting with monoamino PEG of different chain lengths (M-n=1kDa or 10kDa) and end groups (methoxy or hydroxyl) is proven by spectroscopy, changes of surface hydrophilicity, and surface shielding effects. The surface functionalization does lead to reduction of adsorption of BSA, but not of fibrinogen. The thrombocyte adhesion is increased compared to untreated PEI surfaces. Conclusively, rough instead of smooth polymer or gold surfaces should be investigated as relevant models.

Published
2013

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