Your search keyword '"Winkler, Lars"' showing total 9 results

1. M01 as a novel drug enhancer for specifically targeting the blood-brain barrier.

Author

Breitkreuz-Korff O, Tscheik C, Del Vecchio G, Dithmer S, Walther W, Orthmann A, Wolburg H, Haseloff RF, Schröder L, Blasig IE, and Winkler L

Subjects

Animals, Brain metabolism, Claudin-5 metabolism, Mice, Tight Junctions metabolism, Blood-Brain Barrier metabolism, Pharmaceutical Preparations

Abstract

Drug delivery to the brain is limited for most pharmaceuticals by the blood-brain barrier (BBB) where claudin-5 dominates the paraendothelial tightening. For circumventing the BBB, we identified the compound M01 as a claudin-5 interaction inhibitor. M01 causes transient permeabilisation of the BBB depending on the concentration of small molecules in different cell culture models within 3 to 48 h. In mice, brain uptake of fluorescein peaked within the first 3 h after M01 injection and normalised within 48 h. Compared to the cytostatic paclitaxel alone, M01 improved delivery of paclitaxel to mouse brain and reduced orthotopic glioblastoma growth. Results on interactions of M01 with claudin-5 were incorporated into a binding model which suggests association of its aromatic parts with highly conserved residues of the extracellular domain of claudin-5 and adjacent transmembrane segments. Our results indicate the following mode of action: M01 preferentially binds to the extracellular claudin-5 domain, which weakens trans-interactions between adhering cells. Further decrease in membranous claudin-5 levels due to internalization and transcriptional downregulation enables the paracellular passage of small molecules. In summary, the first small molecule is introduced here as a drug enhancer, which specifically permeabilises the BBB for a sufficient interval for allowing neuropharmaceuticals to enter the brain., (Copyright © 2021 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2021

2. Tight junctions in the blood-brain barrier promote edema formation and infarct size in stroke - Ambivalent effects of sealing proteins.

Author

Winkler L, Blasig R, Breitkreuz-Korff O, Berndt P, Dithmer S, Helms HC, Puchkov D, Devraj K, Kaya M, Qin Z, Liebner S, Wolburg H, Andjelkovic AV, Rex A, Blasig IE, and Haseloff RF

Subjects

Animals, Humans, Male, Mice, Tight Junctions metabolism, Blood-Brain Barrier physiopathology, Brain Ischemia physiopathology, Edema physiopathology, Stroke physiopathology

Abstract

The outcome of stroke is greatly influenced by the state of the blood-brain barrier (BBB). The BBB endothelium is sealed paracellularly by tight junction (TJ) proteins, i.e., claudins (Cldns) and the redox regulator occludin. Functions of Cldn3 and occludin at the BBB are largely unknown, particularly after stroke. We address the effects of Cldn3 deficiency and stress factors on the BBB and its TJs. Cldn3 tightened the BBB for small molecules and ions, limited endothelial endocytosis, strengthened the TJ structure and controlled Cldn1 expression. After middle cerebral artery occlusion (MCAO) and 3-h reperfusion or hypoxia of isolated brain capillaries, Cldn1, Cldn3 and occludin were downregulated. In Cldn3 knockout mice (C3KO), the reduction in Cldn1 was even greater and TJ ultrastructure was impaired; 48 h after MCAO of wt mice, infarct volumes were enlarged and edema developed, but endothelial TJs were preserved. In contrast, junctional localization of Cldn5 and occludin, TJ density, swelling and infarction size were reduced in affected brain areas of C3KO. Taken together, Cldn3 and occludin protect TJs in stroke, and this keeps the BBB intact. However, functional Cldn3, Cldn3-regulated TJ proteins and occludin promote edema and infarction, which suggests that TJ modulation could improve the outcome of stroke.

Published

2021

3. Tight junction proteins at the blood-brain barrier: far more than claudin-5.

Author

Berndt P, Winkler L, Cording J, Breitkreuz-Korff O, Rex A, Dithmer S, Rausch V, Blasig R, Richter M, Sporbert A, Wolburg H, Blasig IE, and Haseloff RF

Subjects

Adult, Animals, Brain blood supply, Brain metabolism, Cells, Cultured, Claudin-5 metabolism, Female, Gene Expression, HEK293 Cells, Humans, Male, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Middle Aged, Protein Isoforms genetics, Protein Isoforms metabolism, Tight Junction Proteins metabolism, Tight Junctions ultrastructure, Blood-Brain Barrier, Claudin-5 genetics, Tight Junction Proteins genetics, Tight Junctions metabolism

Abstract

At the blood-brain barrier (BBB), claudin (Cldn)-5 is thought to be the dominant tight junction (TJ) protein, with minor contributions from Cldn3 and -12, and occludin. However, the BBB appears ultrastructurally normal in Cldn5 knock-out mice, suggesting that further Cldns and/or TJ-associated marvel proteins (TAMPs) are involved. Microdissected human and murine brain capillaries, quickly frozen to recapitulate the in vivo situation, showed high transcript expression of Cldn5, -11, -12, and -25, and occludin, but also abundant levels of Cldn1 and -27 in man. Protein levels were quantified by a novel epitope dilution assay and confirmed the respective mRNA data. In contrast to the in vivo situation, Cldn5 dominates BBB expression in vitro, since all other TJ proteins are at comparably low levels or are not expressed. Cldn11 was highly abundant in vivo and contributed to paracellular tightness by homophilic oligomerization, but almost disappeared in vitro. Cldn25, also found at high levels, neither tightened the paracellular barrier nor interconnected opposing cells, but contributed to proper TJ strand morphology. Pathological conditions (in vivo ischemia and in vitro hypoxia) down-regulated Cldn1, -3, and -12, and occludin in cerebral capillaries, which was paralleled by up-regulation of Cldn5 after middle cerebral artery occlusion in rats. Cldn1 expression increased after Cldn5 knock-down. In conclusion, this complete Cldn/TAMP profile demonstrates the presence of up to a dozen TJ proteins in brain capillaries. Mouse and human share a similar and complex TJ profile in vivo, but this complexity is widely lost under in vitro conditions.

Published

2019

4. Claudin peptidomimetics modulate tissue barriers for enhanced drug delivery.

Author

Dithmer S, Staat C, Müller C, Ku MC, Pohlmann A, Niendorf T, Gehne N, Fallier-Becker P, Kittel Á, Walter FR, Veszelka S, Deli MA, Blasig R, Haseloff RF, Blasig IE, and Winkler L

Subjects

Animals, Antibiotics, Antineoplastic administration & dosage, Antibiotics, Antineoplastic pharmacokinetics, Blood-Brain Barrier metabolism, Blood-Brain Barrier ultrastructure, Brain drug effects, Brain metabolism, Cell Line, Cells, Cultured, Circular Dichroism, Claudin-5 chemistry, Claudin-5 pharmacokinetics, Doxorubicin administration & dosage, Doxorubicin pharmacokinetics, Drug Delivery Systems methods, Endothelial Cells metabolism, Endothelial Cells ultrastructure, Gadolinium DTPA administration & dosage, Gadolinium DTPA pharmacokinetics, HEK293 Cells, Humans, Mice, Inbred C57BL, Microscopy, Confocal, Microscopy, Electron methods, Models, Molecular, Peptidomimetics chemistry, Peptidomimetics pharmacokinetics, Permeability drug effects, Protein Conformation, Rats, Rhodamines administration & dosage, Rhodamines pharmacokinetics, Tight Junctions drug effects, Tight Junctions metabolism, Tight Junctions ultrastructure, Time-Lapse Imaging methods, Blood-Brain Barrier drug effects, Claudin-5 pharmacology, Endothelial Cells drug effects, Peptidomimetics pharmacology

Abstract

The blood-brain barrier (BBB) formed by the microvascular endothelium limits cerebral drug delivery. The paraendothelial cleft is sealed by tight junctions (TJs) with a major contribution from claudin-5, which we selected as a target to modulate BBB permeability. For this purpose, drug-enhancer peptides were designed based on the first extracellular loop (ECL) of claudin-5 to allow transient BBB permeabilization. Peptidomimetics (C5C2 and derivatives, nanomolar affinity to claudin-5) size-selectively (≤40 kDa) and reversibly (12-48 h) increased the permeability of brain endothelial and claudin-5-transfected epithelial cell monolayers. Upon peptide uptake, the number of TJ strand particles diminished, claudin-5 was downregulated and redistributed from cell-cell contacts to the cytosol, and the cell shape was altered. Cellular permeability of doxorubicin (cytostatic drug, 580 Da) was enhanced after peptide administration. Mouse studies (3.5 μmol/kg i.v.) confirmed that, for both C5C2 and a d-amino acid derivative, brain uptake of Gd-diethylene-triamine penta-acetic acid (547 Da) was enhanced within 4 h of treatment. On the basis of our functional data, circular dichroism measurements, molecular modeling, and docking experiments, we suggest an association model between β-sheets flanked by α-helices, formed by claudin-5 ECLs, and the peptides. In conclusion, we identified claudin-5 peptidomimetics that improve drug delivery through endothelial and epithelial barriers expressing claudin-5., (© 2017 New York Academy of Sciences.)

Published

2017

5. Transmembrane proteins of the tight junctions at the blood-brain barrier: structural and functional aspects.

Author

Haseloff RF, Dithmer S, Winkler L, Wolburg H, and Blasig IE

Subjects

Animals, Biological Transport, Endothelial Cells metabolism, Humans, Tight Junctions ultrastructure, Blood-Brain Barrier cytology, Blood-Brain Barrier physiology, Membrane Proteins metabolism, Tight Junctions physiology

Abstract

The blood-brain barrier (BBB) is formed by microvascular endothelial cells sealed by tetraspanning tight junction (TJ) proteins, such as claudins and TAMPs (TJ-associated marvel proteins, occludin and tricellulin). Claudins are the major components of the TJs. At the BBB, claudin-5 dominates the TJs by preventing the paracellular permeation of small molecules. On the other hand, TAMPs regulate the structure and function of the TJs; tricellulin may tighten the barrier for large molecules. This review aims at integrating and summarizing the most relevant and recent work on how the BBB is influenced by claudin-1, -3, -5, -12 and the TAMPs occludin and tricellulin, all of which are four-transmembrane TJ proteins. The exact functions of claudin-1, -3, -12 and TAMPs at this barrier still need to be elucidated., (Copyright © 2014 Elsevier Ltd. All rights reserved.)

Published

2015

6. cCPE Fusion Proteins as Molecular Probes to Detect Claudins and Tight Junction Dysregulation in Gastrointestinal Cell Lines, Tissue Explants and Patient-Derived Organoids.

Author

Waldow, Ayk, Beier, Laura-Sophie, Arndt, Janine, Schallenberg, Simon, Vollbrecht, Claudia, Bischoff, Philip, Farrera-Sal, Martí, Loch, Florian N., Bojarski, Christian, Schumann, Michael, Winkler, Lars, Kamphues, Carsten, Ehlen, Lukas, and Piontek, Jörg

Subjects

TIGHT junctions, CHIMERIC proteins, CLAUDINS, CELL lines, ORGANOIDS, DYSPLASIA, MOLECULAR probes, BLOOD-brain barrier

Abstract

Claudins regulate paracellular permeability, contribute to epithelial polarization and are dysregulated during inflammation and carcinogenesis. Variants of the claudin-binding domain of Clostridium perfringens enterotoxin (cCPE) are highly sensitive protein ligands for generic detection of a broad spectrum of claudins. Here, we investigated the preferential binding of YFP- or GST-cCPE fusion proteins to non-junctional claudin molecules. Plate reader assays, flow cytometry and microscopy were used to assess the binding of YFP- or GST-cCPE to non-junctional claudins in multiple in vitro and ex vivo models of human and rat gastrointestinal epithelia and to monitor formation of a tight junction barrier. Furthermore, YFP-cCPE was used to probe expression, polar localization and dysregulation of claudins in patient-derived organoids generated from gastric dysplasia and gastric cancer. Live-cell imaging and immunocytochemistry revealed cell polarity and presence of tight junctions in glandular organoids (originating from intestinal-type gastric cancer and gastric dysplasia) and, in contrast, a disrupted diffusion barrier for granular organoids (originating from discohesive tumor areas). In sum, we report the use of cCPE fusion proteins as molecular probes to specifically and efficiently detect claudin expression, localization and tight junction dysregulation in cell lines, tissue explants and patient-derived organoids of the gastrointestinal tract. [ABSTRACT FROM AUTHOR]

Published

2023

7. Clinically relevant glioblastoma patient-derived xenograft models to guide drug development and identify molecular signatures.

Author

Alcaniz, Joshua, Winkler, Lars, Dahlmann, Mathias, Becker, Michael, Orthmann, Andrea, Haybaeck, Johannes, Krassnig, Stefanie, Skofler, Christina, Kratzsch, Tobias, Kuhn, Susanne A., Jödicke, Andreas, Linnebacher, Michael, Fichtner, Iduna, Walther, Wolfgang, and Hoffmann, Jens

Subjects

DRUG development, GLIOBLASTOMA multiforme, BRAIN tumors, BLOOD-brain barrier, GENE expression, THERAPEUTICS

Abstract

Glioblastoma (GBM) heterogeneity, aggressiveness and infiltrative growth drastically limit success of current standard of care drugs and efficacy of various new therapeutic approaches. There is a need for new therapies and models reflecting the complex biology of these tumors to analyze the molecular mechanisms of tumor formation and resistance, as well as to identify new therapeutic targets. We established and screened a panel of 26 patient-derived subcutaneous (s.c.) xenograft (PDX) GBM models on immunodeficient mice, of which 15 were also established as orthotopic models. Sensitivity toward a drug panel, selected for their different modes of action, was determined. Best treatment responses were observed for standard of care temozolomide, irinotecan and bevacizumab. Matching orthotopic models frequently show reduced sensitivity, as the blood-brain barrier limits crossing of the drugs to the GBM. Molecular characterization of 23 PDX identified all of them as IDH-wt (R132) with frequent mutations in EGFR, TP53, FAT1, and within the PI3K/Akt/ mTOR pathway. Their expression profiles resemble proposed molecular GBM subtypes mesenchymal, proneural and classical, with pronounced clustering for gene sets related to angiogenesis and MAPK signaling. Subsequent gene set enrichment analysis identified hallmark gene sets of hypoxia and mTORC1 signaling as enriched in temozolomide resistant PDX. In models sensitive for mTOR inhibitor everolimus, hypoxia-related gene sets reactive oxygen species pathway and angiogenesis were enriched. Our results highlight how our platform of s.c. GBM PDX can reflect the complex, heterogeneous biology of GBM. Combined with transcriptome analyses, it is a valuable tool in identification of molecular signatures correlating with monitored responses. Available matching orthotopic PDX models can be used to assess the impact of the tumor microenvironment and blood-brain barrier on efficacy. Our GBM PDX panel therefore represents a valuable platform for screening regarding molecular markers and pharmacologically active drugs, as well as optimizing delivery of active drugs to the tumor. [ABSTRACT FROM AUTHOR]

Published

2023

8. Functionalized Lipopeptide Micelles as Highly Efficient NMR Depolarization Seed Points for Targeted Cell Labelling in Xenon MRI.

Author

Schnurr, Matthias, Volk, Ines, Nikolenko, Heike, Winkler, Lars, Dathe, Margitta, and Schröder, Leif

Subjects

MICELLES, MAGNETIC resonance imaging, MAGNETIZATION transfer, ENDOTHELIAL cells, AMINO acid sequence, BRAIN-computer interfaces, LABELS, NUCLEAR magnetic resonance spectroscopy

Abstract

Improving diagnostic imaging and therapy by targeted compound delivery to pathological areas and across biological barriers is of urgent need. A lipopeptide, P‐CrA‐A2, composed of a highly cationic peptide sequence (A2), an N‐terminally attached palmitoyl chain (P) and cryptophane molecule (CrA) for preferred uptake into blood–brain barrier (BBB) capillary endothelial cells, was generated. CrA allows reversible binding of Xe for NMR detection with hyperpolarized nuclei. The lipopeptide forms size‐optimized micelles with a diameter of about 11 nm at low micromolar concentration. Their high local CrA payload has a strong and switchable impact on the bulk magnetization through Hyper‐CEST detection. Covalent fixation of CrA does not impede micelle formation and does not hamper its host functionality but simplifies Xe access to hosts for inducing saturation transfer. Xe Hyper‐CEST magnetic resonance imaging (MRI) allows for distinguishing BBB endothelial cells from control aortic endothelial cells, and the small micelle volume with a sevenfold improved CrA‐loading density compared to liposomal carriers allows preferred cell labelling with a minimally invasive volume (≈16 000‐fold more efficient than 19F cell labelling). Thus, these nanoscopic particles combine selectivity for human brain capillary endothelial cells with great sensitivity of Xe Hyper‐CEST MRI and might be a potential MRI tool in brain diagnostics. [ABSTRACT FROM AUTHOR]

Published

2020

9. Continuity of the blood-brain barrier during subarachnoid hemorrhage in mice

Author

Blecharz, Kinga G., Wagner, Josephin, Schneider, Ulf, Winkler, Lars, and Vajkoczy, Peter

Subjects

subarachniod hemorrhage, endothelium, ddc: 610, cardiovascular diseases, 610 Medical sciences, Medicine, blood-brain barrier, nervous system diseases

Abstract

Objective: Despite decades of research, processes leading to the intravascular inflammatory response accompanying subarachnoid hemorrhage (SAH) remain elusive. The herein presented study focusses on investigating the extent and the progression of blood-brain barrier (BBB) disruption through the loss[for full text, please go to the a.m. URL], 65. Jahrestagung der Deutschen Gesellschaft für Neurochirurgie (DGNC)

Published

2014