Your search keyword '"Koczera P"' showing total 24 results

1. Advanced ultrasound methods to improve chronic kidney disease diagnosis

Author

Fleig, Susanne, Magnuska, Zuzanna Anna, Koczera, Patrick, Salewski, Jannine, Djudjaj, Sonja, Schmitz, Georg, and Kiessling, Fabian

Published

2024

2. Advanced ultrasound methods to improve chronic kidney disease diagnosis

Author

Susanne Fleig, Zuzanna Anna Magnuska, Patrick Koczera, Jannine Salewski, Sonja Djudjaj, Georg Schmitz, and Fabian Kiessling

Subjects

Medical technology, R855-855.5, Medical physics. Medical radiology. Nuclear medicine, R895-920

Abstract

Abstract Chronic kidney disease (CKD) affects 850 million people worldwide and is associated with significant cardiovascular morbidity and mortality. Routine laboratory tests do not reflect early stages of microcirculatory changes and vascular rarefaction that characterise kidney fibrosis, the common endpoint of CKD. Imaging techniques that detect CKD in early stages could promote timely treatment with new drugs like SGLT2 inhibitors, thus, decreasing CKD progression and the cardiovascular disease burden. Ultrasound is the most used imaging modality in CKD, as it is non-invasive and radiation free. Initially, ultrasound imaging was applied to assess kidney macro-morphology and to rule out ureteral obstruction. The development of higher frequency probes allowed for more detailed imaging of kidney parenchyma, and advances in Doppler ultrasound provided insights into segmental arterial flow patterns including resistive indices as an indirect measure of microcirculatory impedance, elevated values of which correlated with progressive organ failure and fibrosis. Today, low-flow detection methods and matrix probes better resolve organ parenchyma and smaller vascular beds, and contrast-enhanced ultrasound allows perfusion measurement. Particularly, super-resolution ultrasound imaging, a technology currently being in clinical translation, can characterise the microcirculation morphologically and functionally in unrivalled detail. This is accompanied by rapid developments in radiomics and machine learning supporting ultrasound image acquisition and processing, as well as lesion detection and characterisation. This perspective article introduces emerging ultrasound methods for the diagnosis of CKD and discusses how the promising technical and analytical advancements can improve disease management after successful translation to clinical application.

Published

2024

3. Neutrophil Hitchhiking Enhances Liposomal Dexamethasone Therapy of Sepsis

Author

Mathur, Ritvik, Elsafy, Sara, Press, Adrian T., Brück, Julian, Hornef, Mathias, Martin, Lukas, Schürholz, Tobias, Marx, Gernot, Bartneck, Matthias, Kiessling, Fabian, Metselaar, Josbert Maarten, Storm, Gert, Lammers, Twan, Sofias, Alexandros Marios, and Koczera, Patrick

Abstract

Sepsis is characterized by a dysregulated immune response and is very difficult to treat. In the cecal ligation and puncture (CLP) mouse model, we show that nanomedicines can effectively alleviate systemic and local septic events by targeting neutrophils. Specifically, by decorating the surface of clinical-stage dexamethasone liposomes with cyclic arginine-glycine-aspartic acid (cRGD) peptides, we promote their engagement with neutrophils in the systemic circulation, leading to their prominent accumulation at primary and secondary sepsis sites. cRGD-targeted dexamethasone liposomes potently reduce immature circulating neutrophils and neutrophil extracellular traps in intestinal sepsis induction sites and the liver. Additionally, they mitigate inflammatory cytokines systemically and locally while preserving systemic IL-10 levels, contributing to lower IFN-γ/IL-10 ratios as compared to control liposomes and free dexamethasone. Our strategy addresses sepsis at the cellular level, illustrating the use of neutrophils both as a therapeutic target and as a chariot for drug delivery.

Published

2024

4. The Synthetic Antimicrobial Peptide 19-2.5 Interacts with Heparanase and Heparan Sulfate in Murine and Human Sepsis.

Author

Lukas Martin, Rebecca De Santis, Patrick Koczera, Nadine Simons, Hajo Haase, Lena Heinbockel, Klaus Brandenburg, Gernot Marx, and Tobias Schuerholz

Subjects

Medicine, Science

Abstract

Heparanase is an endo-β-glucuronidase that cleaves heparan sulfate side chains from their proteoglycans. Thereby, heparanase liberates highly potent circulating heparan sulfate-fragments (HS-fragments) and triggers the fatal and excessive inflammatory response in sepsis. As a potential anti-inflammatory agent for sepsis therapy, peptide 19-2.5 belongs to the class of synthetic anti-lipopolysaccharide peptides; however, its activity is not restricted to Gram-negative bacterial infection. We hypothesized that peptide 19-2.5 interacts with heparanase and/or HS, thereby reducing the levels of circulating HS-fragments in murine and human sepsis. Our data indicate that the treatment of septic mice with peptide 19-2.5 compared to untreated control animals lowers levels of plasma heparanase and circulating HS-fragments and reduces heparanase activity. Additionally, mRNA levels of heparanase in heart, liver, lung, kidney and spleen are downregulated in septic mice treated with peptide 19-2.5 compared to untreated control animals. In humans, plasma heparanase level and activity are elevated in septic shock. The ex vivo addition of peptide 19-2.5 to plasma of septic shock patients decreases heparanase activity but not heparanase level. Isothermal titration calorimetry revealed a strong exothermic reaction between peptide 19-2.5 and heparanase and HS-fragments. However, a saturation character has been identified only in the peptide 19-2.5 and HS interaction. In conclusion, the findings of our current study indicate that peptide 19-2.5 interacts with heparanase, which is elevated in murine and human sepsis and consecutively attenuates the generation of circulating HS-fragments in systemic inflammation. Thus, peptide 19-2.5 seems to be a potential anti-inflammatory agent in sepsis.

Published

2015

5. Fluorescently labeled microbubbles for facilitating translational molecular ultrasound studies

Author

Koczera, Patrick, Wu, Zhuojun, Fokong, Stanley, Theek, Benjamin, Appold, Lia, Jorge, Samuel, Möckel, Diana, Liu, Zhe, Curaj, Adelina, Storm, Gert, van Zandvoort, Marc, Kiessling, Fabian, and Lammers, Twan

Published

2012

6. Drug Loading in Poly(butyl cyanoacrylate)-Based Polymeric Microbubbles.

Author

Mengjiao Liu, Dasgupta, Anshuman, Koczera, Patrick, Schipper, Sandra, Rommel, Dirk, Shi, Yang, Kiessling, Fabian, and Lammers, Twan

Published

2020

7. Drug Loading in Poly(butyl cyanoacrylate)-Based Polymeric Microbubbles

Author

Liu, Mengjiao, Dasgupta, Anshuman, Koczera, Patrick, Schipper, Sandra, Rommel, Dirk, Shi, Yang, Kiessling, Fabian, and Lammers, Twan

Abstract

Microbubbles (MB) are routinely used ultrasound (US) contrast agents that have recently attracted increasing attention as stimuli-responsive drug delivery systems. To better understand MB-based drug delivery, we studied the role of drug hydrophobicity and molecular weight on MB loading, shelf-life stability, US properties, and drug release. Eight model drugs, varying in hydrophobicity and molecular weight, were loaded into the shell of poly(butyl cyanoacrylate) (PBCA) MB. In the case of drugs with progesterone as a common structural backbone (i.e., for corticosteroids), loading capacity and drug release correlated well with hydrophobicity and molecular weight. Conversely, when employing drugs with no structural similarity (i.e., four different fluorescent dyes), loading capacity and release did not correlate with hydrophobicity and molecular weight. All model drug-loaded MB formulations could be equally efficiently destroyed upon exposure to US. Together, these findings provide valuable insights on how the physicochemical properties of (model) drug molecules affect their loading and retention in and US-induced release from polymeric MB, thereby facilitating the development of drug-loaded MB formulations for US-triggered drug delivery.

Published

2020

8. Noninvasive Optical Imaging of Nanomedicine Biodistribution

Author

Kunjachan, Sijumon, Gremse, Felix, Theek, Benjamin, Koczera, Patrick, Pola, Robert, Pechar, Michal, Etrych, Tomas, Ulbrich, Karel, Storm, Gert, Kiessling, Fabian, and Lammers, Twan

Abstract

Nanomedicines are sub-micrometer-sized carrier materials designed to improve the biodistribution of i.v. administered (chemo-) therapeutic agents. In recent years, ever more efforts in the nanomedicine field have employed optical imaging (OI) techniques to monitor biodistribution and target site accumulation. Thus far, however, the longitudinal assessment of nanomedicine biodistribution using OI has been impossible, due to limited light penetration (in the case of 2D fluorescence reflectance imaging; FRI) and to the inability to accurately allocate fluorescent signals to nonsuperficial organs (in the case of 3D fluorescence molecular tomography; FMT). Using a combination of high-resolution microcomputed tomography (μCT) and FMT, we have here set out to establish a hybrid imaging protocol for noninvasively visualizing and quantifying the accumulation of near-infrared fluorophore-labeled nanomedicines in tissues other than superficial tumors. To this end, HPMA-based polymeric drug carriers were labeled with Dy750, their biodistribution and tumor accumulation were analyzed using FMT, and the resulting data sets were fused with anatomical μCT data sets in which several different physiologically relevant organs were presegmented. The robustness of 3D organ segmentation was validated, and the results obtained using 3D CT-FMT were compared to those obtained upon standard 3D FMT and 2D FRI. Our findings convincingly demonstrate that combining anatomical μCT with molecular FMT facilitates the noninvasive assessment of nanomedicine biodistribution.

Published

2013

9. Urologic Examination with the New Radiopaque Mediums, Diatrizoate, Acetrizoate and Diprotrizoate - A Clinical Comparison

Author

Hoffman, Howard A., Koczera, Stanley J., Portnoy, Nelson L., Simas, Wilson, and Hastreiter, Alois R.

Published

1956

10. Sodium Diatrizoate for Intravenous Pyelography - A Report of 100 Cases

Author

Hoffman, Howard A., Koczera, Stanley J., Portnoy, Nelson L., Lewis, Emery O., Vogt, Edward C., and Simas, Wilson

Published

1955

11. Five months is too long to wait.

Author

Robert Koczera

Published

2009

12. Microbubble-encapsulated Cobalt Nitrato Complexes for Ultrasound-triggerable Nitric Oxide Delivery.

Author

Koczera P, Thomas F, Rama E, Thoröe-Boveleth S, Kiessling F, Lammers T, and Herres-Pawlis S

Subjects

Mice, Animals, Humans, Molecular Structure, Cell Line, Tumor, Cell Survival drug effects, Macrophages drug effects, Macrophages metabolism, Ultrasonic Waves, Structure-Activity Relationship, Nitric Oxide chemistry, Nitric Oxide metabolism, Cobalt chemistry, Coordination Complexes chemistry, Coordination Complexes pharmacology, Coordination Complexes chemical synthesis, Microbubbles

Abstract

Cobalt complexes exhibit versatile reactivity with nitric oxide (NO), enabling their utilization in applications ranging from homogeneous catalysis to NO-based modulation of biological processes. However, the coordination geometry around the cobalt center is complex, the therapeutic window of NO is narrow, and controlled NO delivery is difficult. To better understand the complexation of cobalt with NO, we prepared four cobalt nitrato complexes and present a structure-property relationship for ultrasound-triggerable NO release. We hypothesized that modulation of the coordination geometry by ligand-modification would improve responsiveness to mechanical stimuli, like ultrasound. To enable eventual therapeutic testing, we here first demonstrate the in vitro tolerability of [Co(ethylenediamine) 2 (NO)(NO 3 )](NO 3 ) in A431 epidermoid carcinoma cells and J774A.1 murine macrophages, and we subsequently show successful encapsulation of the complex in poly(butyl cyanoacrylate) microbubbles. These hybrid Co-NO-containing microbubbles may in the future aid in ultrasound imaging-guided treatment of NO-responsive vascular pathologies., (© 2024 The Author(s). ChemMedChem published by Wiley-VCH GmbH.)

Published

2024

13. Ultrasound Localization Microscopy for Breast Cancer Imaging in Patients: Protocol Optimization and Comparison with Shear Wave Elastography.

Author

Porte C, Lisson T, Kohlen M, von Maltzahn F, Dencks S, von Stillfried S, Piepenbrock M, Rix A, Dasgupta A, Koczera P, Boor P, Stickeler E, Schmitz G, and Kiessling F

Subjects

Humans, Female, Microscopy methods, Breast, Ultrasonography methods, Microbubbles, Elasticity Imaging Techniques methods, Breast Neoplasms diagnostic imaging

Abstract

Objective: Ultrasound localization microscopy (ULM) has gained increasing attention in recent years because of its ability to visualize blood vessels at super-resolution. The field of oncology, in particular, could benefit from detailed vascular characterization, for example, for diagnosis and therapy monitoring. This study was aimed at refining ULM for breast cancer patients by optimizing the measurement protocol, identifying translational challenges and combining ULM and shear wave elastography., Methods: We computed ULM images of 11 patients with breast cancer by recording contrast-enhanced ultrasound (CEUS) sequences and post-processing them in an offline pipeline. For CEUS, two different doses and injection speeds of SonoVue were applied. The best injection protocol was determined based on quantitative parameters derived from so-called occurrence maps. In addition, a suitable measurement time window was determined, also considering the occurrence of motion. ULM results were compared with shear wave elastography and histological vessel density., Results: At the higher dose and injection speed, the highest number of microbubbles, number of tracks and vessel coverage were achieved, leading to the most detailed representation of tumor vasculature. Even at the highest concentration, no significant overlay of microbubble signals occurred. Motion significantly reduced the number of usable frames, thus limiting the measurement window to 3.5 min. ULM vessel coverage was comparable to the histological vessel fraction and correlated significantly with mean tumor elasticity., Conclusion: The settings for microbubble injection strongly influence ULM images, thus requiring optimized protocols for different indications. Patient and examiner motion was identified as the main translational challenge for ULM., Competing Interests: Conflict of interest The authors declare no competing interests., (Copyright © 2023 World Federation for Ultrasound in Medicine & Biology. Published by Elsevier Inc. All rights reserved.)

Published

2024

14. Theranostic Trigger-Responsive Carbon Monoxide-Generating Microbubbles.

Author

Pathak V, Roemhild K, Schipper S, Groß-Weege N, Nolte T, Ruetten S, Buhl EM, El Shafei A, Weiler M, Martin L, Marx G, Schulz V, Kiessling F, Lammers T, and Koczera P

Subjects

Carbon Monoxide, Endothelial Cells, Humans, Hypoxia, Precision Medicine, Reactive Oxygen Species, Microbubbles, Organometallic Compounds

Abstract

Carbon monoxide (CO) is a gaseous signaling molecule that modulates inflammation, cell survival, and recovery after myocardial infarction. However, handling and dosing of CO as a compressed gas are difficult. Here, light-triggerable and magnetic resonance imaging (MRI)-detectable CO release from dimanganese decacarbonyl (CORM-1) are demonstrated, and the development of CORM-1-loaded polymeric microbubbles (COMB) is described as an ultrasound (US)- and MRI-imageable drug delivery platform for triggerable and targeted CO therapy. COMB are synthesized via a straightforward one-step loading protocol, present a narrow size distribution peaking at 2 µm, and show excellent performance as a CORM-1 carrier and US contrast agent. Light irradiation of COMB induces local production and release of CO, as well as enhanced longitudinal and transversal relaxation rates, enabling MRI monitoring of CO delivery. Proof-of-concept studies for COMB-enabled light-triggered CO release show saturation of hemoglobin with CO in human blood, anti-inflammatory differentiation of macrophages, reduction of hypoxia-induced reactive oxygen species (ROS) production, and inhibition of ischemia-induced apoptosis in endothelial cells and cardiomyocytes. These findings indicate that CO-generating MB are interesting theranostic tools for attenuating hypoxia-associated and ROS-mediated cell and tissue damage in cardiovascular disease., (© 2022 The Authors. Small published by Wiley-VCH GmbH.)

Published

2022

15. Effects of contrast-enhanced ultrasound treatment on neoadjuvant chemotherapy in breast cancer.

Author

Rix A, Piepenbrock M, Flege B, von Stillfried S, Koczera P, Opacic T, Simons N, Boor P, Thoröe-Boveleth S, Deckers R, May JN, Lammers T, Schmitz G, Stickeler E, and Kiessling F

Subjects

Adult, Animals, Carboplatin administration & dosage, Carboplatin therapeutic use, Contrast Media pharmacology, Female, Humans, Mice, Mice, Inbred BALB C, Microbubbles, Middle Aged, Perfusion, Prospective Studies, Triple Negative Breast Neoplasms drug therapy, Ultrasonography, Ultrasonography, Doppler methods, Breast Neoplasms therapy, Neoadjuvant Therapy methods, Ultrasonic Therapy methods

Abstract

Purpose: Preclinical and clinical data indicate that contrast-enhanced ultrasound can enhance tumor perfusion and vessel permeability, thus, improving chemotherapy accumulation and therapeutic outcome. Therefore, we investigated the effects of high mechanical index (MI) contrast-enhanced Doppler ultrasound (CDUS) on tumor perfusion in breast cancer. Methods: In this prospective study, breast cancer patients were randomly assigned to receive either 18 minutes of high MI CDUS during chemotherapy infusion (n = 6) or chemotherapy alone (n = 5). Tumor perfusion was measured before and after at least six chemotherapy cycles using motion-model ultrasound localization microscopy. Additionally, acute effects of CDUS on vessel perfusion and chemotherapy distribution were evaluated in mice bearing triple-negative breast cancer (TNBC). Results: Morphological and functional vascular characteristics of breast cancer in patients were not significantly influenced by high MI CDUS. However, complete clinical tumor response after neoadjuvant chemotherapy was lower in high MI CDUS-treated (1/6) compared to untreated patients (4/5) and size reduction of high MI CDUS treated tumors tended to be delayed at early chemotherapy cycles. In mice with TNBC high MI CDUS decreased the perfused tumor vessel fraction (p < 0.01) without affecting carboplatin accumulation or distribution. Higher vascular immaturity and lower stromal stabilization may explain the stronger vascular response in murine than human tumors. Conclusion: High MI CDUS had no detectable effect on breast cancer vascularization in patients. In mice, the same high MI CDUS setting did not affect chemotherapy accumulation although strong effects on the tumor vasculature were detected histologically. Thus, sonopermeabilization in human breast cancers might not be effective using high MI CDUS protocols and future applications may rather focus on low MI approaches triggering microbubble oscillations instead of destruction. Furthermore, our results show that there are profound differences in the response of mouse and human tumor vasculature to high MI CDUS, which need to be further explored and considered in clinical translation., Competing Interests: Competing Interests: The authors have declared that no competing interest exists., (© The author(s).)

Published

2021

16. PBCA-based polymeric microbubbles for molecular imaging and drug delivery.

Author

Koczera P, Appold L, Shi Y, Liu M, Dasgupta A, Pathak V, Ojha T, Fokong S, Wu Z, van Zandvoort M, Iranzo O, Kuehne AJC, Pich A, Kiessling F, and Lammers T

Subjects

Animals, Antibodies administration & dosage, Antibodies chemistry, Biotin administration & dosage, Biotin chemistry, Brain metabolism, Carotid Arteries diagnostic imaging, Carotid Arteries metabolism, Cell Line, Tumor, Dextrans administration & dosage, Dextrans chemistry, E-Selectin immunology, Enbucrilate chemistry, Fluorescein-5-isothiocyanate administration & dosage, Fluorescein-5-isothiocyanate analogs & derivatives, Fluorescein-5-isothiocyanate chemistry, Fluorescent Dyes administration & dosage, Fluorescent Dyes chemistry, Humans, Male, Mice, Nude, Molecular Imaging, Neoplasms diagnostic imaging, Neoplasms metabolism, Neoplasms pathology, Neovascularization, Pathologic, Rhodamines administration & dosage, Rhodamines chemistry, Streptavidin administration & dosage, Streptavidin chemistry, Ultrasonic Waves, Ultrasonography, Vascular Cell Adhesion Molecule-1 immunology, Vascular Endothelial Growth Factor Receptor-2 immunology, Drug Delivery Systems, Enbucrilate administration & dosage, Microbubbles

Abstract

Microbubbles (MB) are routinely used as contrast agents for ultrasound (US) imaging. We describe different types of targeted and drug-loaded poly(n-butyl cyanoacrylate) (PBCA) MB, and demonstrate their suitability for multiple biomedical applications, including molecular US imaging and US-mediated drug delivery. Molecular imaging of angiogenic tumor blood vessels and inflamed atherosclerotic endothelium is performed by modifying the surface of PBCA MB with peptides and antibodies recognizing E-selectin and VCAM-1. Stable and inertial cavitation of PBCA MB enables sonoporation and permeabilization of blood vessels in tumors and in the brain, which can be employed for direct and indirect drug delivery. Direct drug delivery is based on US-induced release of (model) drug molecules from the MB shell. Indirect drug delivery refers to US- and MB-mediated enhancement of extravasation and penetration of co-administered drugs and drug delivery systems. These findings are in line with recently reported pioneering proof-of-principle studies showing the usefulness of (phospholipid) MB for molecular US imaging and sonoporation-enhanced drug delivery in patients. They aim to exemplify the potential and the broad applicability of combining MB with US to improve disease diagnosis and therapy., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

17. The Ribonuclease A Superfamily in Humans: Canonical RNases as the Buttress of Innate Immunity.

Author

Koczera P, Martin L, Marx G, and Schuerholz T

Subjects

Humans, Models, Biological, Immunity, Innate, Multigene Family, Ribonuclease, Pancreatic metabolism

Abstract

In humans, the ribonuclease A (RNase A) superfamily contains eight different members that have RNase activities, and all of these members are encoded on chromosome 14. The proteins are secreted by a large variety of different tissues and cells; however, a comprehensive understanding of these proteins' physiological roles is lacking. Different biological effects can be attributed to each protein, including antiviral, antibacterial and antifungal activities as well as cytotoxic effects against host cells and parasites. Different immunomodulatory effects have also been demonstrated. This review summarizes the available data on the human RNase A superfamily and illustrates the significant role of the eight canonical RNases in inflammation and the host defence system against infections.

Published

2016

18. The Human Host Defense Ribonucleases 1, 3 and 7 Are Elevated in Patients with Sepsis after Major Surgery--A Pilot Study.

Author

Martin L, Koczera P, Simons N, Zechendorf E, Hoeger J, Marx G, and Schuerholz T

Subjects

Aged, Biomarkers blood, Case-Control Studies, Female, Humans, Male, Middle Aged, Sepsis etiology, Surgical Wound Infection complications, Autoantigens blood, Eosinophil Cationic Protein blood, Ribonuclease P blood, Ribonucleases blood, Sepsis blood, Surgical Wound Infection blood

Abstract

Sepsis is the most common cause of death in intensive care units and associated with widespread activation of host innate immunity responses. Ribonucleases (RNases) are important components of the innate immune system, however the role of RNases in sepsis has not been investigated. We evaluated serum levels of RNase 1, 3 and 7 in 20 surgical sepsis patients (Sepsis), nine surgical patients (Surgery) and 10 healthy controls (Healthy). RNase 1 and 3 were elevated in Sepsis compared to Surgery (2.2- and 3.1-fold, respectively; both p < 0.0001) or compared to Healthy (3.0- and 15.5-fold, respectively; both p < 0.0001). RNase 1 showed a high predictive value for the development of more than two organ failures (AUC 0.82, p = 0.01). Patients with renal dysfunction revealed higher RNase 1 levels than without renal dysfunction (p = 0.03). RNase 1 and 3 were higher in respiratory failure than without respiratory failure (p < 0.0001 and p = 0.02, respectively). RNase 7 was not detected in Healthy patients and only in two patients of Surgery, however RNase 7 was detected in 10 of 20 Sepsis patients. RNase 7 was higher in renal or metabolic failure than without failure (p = 0.04 and p = 0.02, respectively). In conclusion, RNase 1, 3 and 7 are secreted into serum under conditions with tissue injury, such as major surgery or sepsis. Thus, RNases might serve as laboratory parameters to diagnose and monitor organ failure in sepsis.

Published

2016

19. The Endothelial Glycocalyx: New Diagnostic and Therapeutic Approaches in Sepsis.

Author

Martin L, Koczera P, Zechendorf E, and Schuerholz T

Subjects

Animals, Glucuronidase, Humans, Mice, Endothelium physiology, Endothelium physiopathology, Glycocalyx physiology, Models, Immunological, Sepsis physiopathology

Abstract

Sepsis is defined as a life-threatening organ dysfunction caused by a dysregulated host response to infection. The endothelial glycocalyx is one of the earliest sites involved during sepsis. This fragile layer is a complex network of cell-bound proteoglycans, glycosaminoglycan side chains, and sialoproteins lining the luminal side of endothelial cells with a thickness of about 1 to 3  μ m. Sepsis-associated alterations of its structure affect endothelial permeability and result in the liberation of endogenous damage-associated molecular patterns (DAMPs). Once liberated in the circulatory system, DAMPs trigger the devastating consequences of the proinflammatory cascades in sepsis and septic shock. In this way, the injury to the glycocalyx with the consecutive release of DAMPs contributes to a number of specific clinical effects of sepsis, including acute kidney injury, respiratory failure, and septic cardiomyopathy. Moreover, the extent of glycocalyx degradation serves as a marker of endothelial dysfunction and sepsis severity. In this review, we highlight the crucial role of the glycocalyx in sepsis as a diagnostic tool and discuss the potential of members of the endothelial glycocalyx serving as hopeful therapeutic targets in sepsis-associated multiple organ failures.

Published

2016

20. The Synthetic Antimicrobial Peptide 19-2.5 Interacts with Heparanase and Heparan Sulfate in Murine and Human Sepsis.

Author

Martin L, De Santis R, Koczera P, Simons N, Haase H, Heinbockel L, Brandenburg K, Marx G, and Schuerholz T

Subjects

Adult, Animals, Anti-Infective Agents chemical synthesis, Enzyme-Linked Immunosorbent Assay, Humans, Mice, Peptides chemical synthesis, Sepsis enzymology, Anti-Infective Agents therapeutic use, Glucuronidase metabolism, Heparitin Sulfate metabolism, Peptides therapeutic use, Sepsis drug therapy, Sepsis metabolism

Abstract

Heparanase is an endo-β-glucuronidase that cleaves heparan sulfate side chains from their proteoglycans. Thereby, heparanase liberates highly potent circulating heparan sulfate-fragments (HS-fragments) and triggers the fatal and excessive inflammatory response in sepsis. As a potential anti-inflammatory agent for sepsis therapy, peptide 19-2.5 belongs to the class of synthetic anti-lipopolysaccharide peptides; however, its activity is not restricted to Gram-negative bacterial infection. We hypothesized that peptide 19-2.5 interacts with heparanase and/or HS, thereby reducing the levels of circulating HS-fragments in murine and human sepsis. Our data indicate that the treatment of septic mice with peptide 19-2.5 compared to untreated control animals lowers levels of plasma heparanase and circulating HS-fragments and reduces heparanase activity. Additionally, mRNA levels of heparanase in heart, liver, lung, kidney and spleen are downregulated in septic mice treated with peptide 19-2.5 compared to untreated control animals. In humans, plasma heparanase level and activity are elevated in septic shock. The ex vivo addition of peptide 19-2.5 to plasma of septic shock patients decreases heparanase activity but not heparanase level. Isothermal titration calorimetry revealed a strong exothermic reaction between peptide 19-2.5 and heparanase and HS-fragments. However, a saturation character has been identified only in the peptide 19-2.5 and HS interaction. In conclusion, the findings of our current study indicate that peptide 19-2.5 interacts with heparanase, which is elevated in murine and human sepsis and consecutively attenuates the generation of circulating HS-fragments in systemic inflammation. Thus, peptide 19-2.5 seems to be a potential anti-inflammatory agent in sepsis.

Published

2015

21. Theranostic USPIO-Loaded Microbubbles for Mediating and Monitoring Blood-Brain Barrier Permeation.

Author

Lammers T, Koczera P, Fokong S, Gremse F, Ehling J, Vogt M, Pich A, Storm G, van Zandvoort M, and Kiessling F

Abstract

Efficient and safe drug delivery across the blood-brain barrier (BBB) remains to be one of the major challenges of biomedical and (nano-) pharmaceutical research. Here, we show that poly(butyl cyanoacrylate)-based microbubbles (MB), carrying ultrasmall superparamagnetic iron oxide (USPIO) nanoparticles within their shell, can be used to mediate and monitor BBB permeation. Upon exposure to transcranial ultrasound pulses, USPIO-MB are destroyed, resulting in acoustic forces inducing vessel permeability. At the same time, USPIO are released from the MB shell, they extravasate across the permeabilized BBB and they accumulate in extravascular brain tissue, thereby providing non-invasive R 2 *-based magnetic resonance imaging information on the extent of BBB opening. Quantitative changes in R 2 * relaxometry were in good agreement with 2D and 3D microscopy results on the extravascular deposition of the macromolecular model drug FITC-dextran into the brain. Such theranostic materials and methods are considered to be useful for mediating and monitoring drug delivery across the BBB, and for enabling safe and efficient treatment of CNS disorders.

Published

2015

22. Image-guided, targeted and triggered drug delivery to tumors using polymer-based microbubbles.

Author

Fokong S, Theek B, Wu Z, Koczera P, Appold L, Jorge S, Resch-Genger U, van Zandvoort M, Storm G, Kiessling F, and Lammers T

Subjects

Acoustics, Animals, Cell Line, Tumor, Coumarins administration & dosage, Coumarins chemistry, Enbucrilate, Fluorescent Dyes administration & dosage, Fluorescent Dyes chemistry, Mice, Microscopy, Fluorescence, Rhodamines administration & dosage, Rhodamines chemistry, Thiazoles administration & dosage, Thiazoles chemistry, Vascular Endothelial Growth Factor Receptor-2 metabolism, Cyanoacrylates chemistry, Drug Delivery Systems, Microbubbles, Neoplasms metabolism

Abstract

Microbubbles (MB) are routinely used contrast agents for functional and molecular ultrasound (US) imaging. In addition, they have been attracting more and more attention for drug delivery purposes, enabling e.g. US-mediated drug delivery across biological barriers and US-induced triggered drug release from the MB shell. The vast majority of efforts in this regard have thus far focused on phospholipid-based soft-shell MB, which are suboptimal for stably incorporating large amounts of drug molecules because of their relatively thin shell. Using poly(butyl cyanoacrylate) (PBCA)-based hard-shell MB, we show here that both hydrophilic (Rhodamine-B) and hydrophobic (Coumarin-6) model drugs can be efficiently and stably entrapped within the ~50 nm shell of PBCA MB. In addition, we demonstrate that model drug loading does not negatively affect the acoustic properties of the MB, and that functionalizing the surface of fluorophore-loaded MB with anti-VEGFR2 antibodies enables image-guided and targeted model drug delivery to tumor blood vessels. Finally, we show both in vitro and in vivo that disintegrating VEGFR2-targeted MB with high-mechanical index US pulses leads to high levels of model drug release. Consequently, these findings indicate that polymer-based MB are highly suitable systems for image-guided, targeted and triggered drug delivery to tumors and tumor blood vessels., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

23. Versatile synthetic strategies for PBCA-based hybrid fluorescent microbubbles and their potential theranostic applications to cell labelling and imaging.

Author

Liu Z, Koczera P, Doleschel D, Kiessling F, and Gätjens J

Subjects

Animals, Cell Line, Tumor, Contrast Media chemistry, Drug Carriers chemistry, Enbucrilate, Humans, Magnetic Resonance Imaging, Magnetite Nanoparticles chemistry, Mice, Mice, Nude, Microscopy, Confocal, Neoplasms pathology, Vascular Endothelial Growth Factor Receptor-2 metabolism, Cyanoacrylates chemistry, Fluorescent Dyes chemistry, Microbubbles

Abstract

This research reports the versatile synthetic strategies for hybrid PBCA microbubbles as contrast agents and drug carriers loaded with fluorescent dyes and magnetic nanoparticles serving in vitro cell labelling and in vivo target imaging. These multifunctional probes therefore prove their potential biomedical applications in cancer diagnostics and treatment., (This journal is © The Royal Society of Chemistry 2012)

Published

2012

24. Ultrasound microbubbles for molecular diagnosis, therapy, and theranostics.

Author

Kiessling F, Fokong S, Koczera P, Lederle W, and Lammers T

Subjects

Animals, Clinical Trials as Topic, Drug Delivery Systems, Genetic Therapy methods, Humans, Vascular Endothelial Growth Factor Receptor-2 metabolism, Contrast Media, Microbubbles, Molecular Diagnostic Techniques, Thrombolytic Therapy methods, Ultrasonics

Abstract

Ultrasound imaging is clinically established for routine screening examinations of breast, abdomen, neck, and other soft tissues, as well as for therapy monitoring. Microbubbles as vascular contrast agents improve the detection and characterization of cancerous lesions, inflammatory processes, and cardiovascular pathologies. Taking advantage of the excellent sensitivity and specificity of ultrasound for microbubble detection, molecular imaging can be realized by binding antibodies, peptides, and other targeting moieties to microbubble surfaces. Molecular microbubbles directed against various targets such as vascular endothelial growth factor receptor-2, vascular cell adhesion molecule 1, intercellular adhesion molecule 1, selectins, and integrins were developed and were shown in preclinical studies to be able to selectively bind to tumor blood vessels and atherosclerotic plaques. Currently, the first microbubble formulations targeted to angiogenic vessels in prostate cancers are being evaluated clinically. However, microbubbles can be used for more than diagnosis: disintegrating microbubbles emit acoustic forces that are strong enough to induce thrombolysis, and they can also be used for facilitating drug and gene delivery across biologic barriers. This review on the use of microbubbles for ultrasound-based molecular imaging, therapy, and theranostics addresses innovative concepts and identifies areas in which clinical translation is foreseeable in the near future.

Published

2012