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Featured researches published by Klaus Langer.


Journal of Nanomedicine & Biotherapeutic Discovery | 2016

Flurbiprofen-loaded Nanoparticles Can Cross a Primary Porcine In vitroBlood-brain Barrier Model to Reduce Amyloid-ò42 Burden

Julia Stab; Iavor Zlatev; Bastian Raudszus; Sabrina Meister; Claus U. Pietrzik; Klaus Langer; Hagen von Briesen; Sylvia Wagner

Elevated amyloid-β42 (Aβ42) in the brain is expected to cause nAlzheimer’s Disease n(AD). Reducing Aβ42 is therefore a cornerstone in causal drug development. Nevertheless, many promising substances failed in clinical trials, because reaching the target organ in vivo is difficult. The brain is protected by the Blood-Brain Barrier (BBB) that shields off most molecules to maintain the brain homeostasis. Brain-targeted nanoparticles are one successful tool to bypass this problem: by acting as Trojan horses they carry embedded drugs across the BBB for brain disorder treatment. Here, flurbiprofen, a γ-secretase modulator, was embedded in Poly(Lactic Acid) (PLA) nanoparticles. We tested if the drug-loaded nanoparticles affected the integrity of our advanced in vitro BBB model in transendothelial electrical resistance measurements and permeability assays, and investigated the nanoparticle-cell interaction in flow cytometry and confocal laser scanning microscopy. Furthermore, we assessed the drug transport capacity by highperformance liquid nchromatography nand the biological efficacy of the embedded drug in an Aβ42-detecing ELISA. We also verified the viability of the AD model cells by a cellular viability assay. After adding flurbiprofen-loaded nanoparticles to the blood compartment of a Transwell® model, the drug was detectable in the brain compartment, where it induced an Aβ42 lowering effect. Flurbiprofen from nanoparticles crossed the BBB without impairing barrier integrity, whereas the free drug was highly cytotoxic and destroyed the barrier. Ligand coupling of napolipoprotein nE3 to the nanoparticles increased cellular uptake. Hence, we expect an even more pronounced Aβ42 reducing effect for apolipoprotein-modified, flurbiprofen-loaded nanoparticles. In conclusion, we enabled transport of a hardly permeable drug across an advanced in vitro BBB model, opening opportunities in the treatment and prevention of AD and other brain disorders. Using a primary porcine BBB model that displays excellent barrier characteristics, we show that flurbiprofen-loaded nanoparticles reduce Aβ42 burden without impairing barrier function.


Archive | 2002

Nanoparticles made of protein with coupled apolipoprotein e for penetration of the blood-brain barrier and methods for the production thereof

Joerg Kreuter; Klaus Langer; Carolin Weber; Renad N. Alyautdin


Archive | 2010

Nanoparticle carrier systems based on poly(dl-lactic-co-glycolic acid) (plga) for photodynamic therapy (pdt)

Klaus Langer; Thomas Knobloch; Beate Röder; Annegret Preuss; Volker Albrecht; Susanna Gräfe; Arno Wiehe; Briesen Hagen Von; Karin Löw; Sylvia Wagner


Archive | 2010

Nanoparticle carrier systems based on human serum albumin for photodynamic therapy

Klaus Langer; Matthias Wacker; Beate Röder; Annegret Preuss; Volker Albrecht; Susanna Gräfe; Arno Wiehe; Hagen von Briesen; Karin Löw; Sylvia Wagner


Archive | 2006

Protein-Based Carrier System for Overcoming Resistance in Tumour Cells

Sebastian Dreis; Klaus Langer; Joerg Kreuter; Martin Michaelis; Jindrich Cinatl


Archive | 2010

ANTI INTEGRIN ANTIBODIES LINKED TO NANOPARTICLES LOADED WITH CHEMOTHERAPEUTIC AGENTS

Klaus Langer; Marion Anhorn; Joerg Kreuter; Florian Rothweiler; Hagen von Briesen; Sylvia Wagner; Martin Michaelis; Jindrich Cinatl


Archive | 2007

Active Agent-Loaded Nanoparticles Based On Hydrophilic Proteins

Jörg Kreuter; Klaus Langer; Kerstin Michaelis; Telli Hekmatara; Sebastian Dreis


Archive | 2005

Carrier system in the form of protein-based nanoparticles for the cell-specific enrichment of pharmaceutically active substances

Sabine Balthasar; Hagen von Briesen; Norbert Dinauer; Jörg Kreuter; Klaus Langer; Heidrun Wartlick


Archive | 2012

Nanoparticles as mrt contrast media for the diagnosis of hepatocellular carcinoma

Jörg Kreuter; Karsten Ulbrich; Klaus Langer; Thomas Knobloch; Albrecht Piiper; Verena Köberle; Hüdayi Korkusuz; Thomas J. Vogel


Archive | 2005

Trägersystem in Form von Nanopartikeln auf Proteinbasis zur zellspezifischen Anreicherung von pharmazeutisch aktiven Wirkstoffen

Sabine Balthasar; Hagen von Briesen; Norbert Dinauer; Jörg Kreuter; Klaus Langer; Heidrun Wartlick

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Jörg Kreuter

Goethe University Frankfurt

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Sebastian Dreis

Goethe University Frankfurt

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Telli Hekmatara

Goethe University Frankfurt

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Kerstin Michaelis

Goethe University Frankfurt

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Arno Wiehe

Free University of Berlin

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Beate Röder

Humboldt University of Berlin

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Heidrun Wartlick

Goethe University Frankfurt

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