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Featured researches published by Gerhard Muhrer.


International Journal of Pharmaceutics | 2010

Solubility of Ketoprofen in colloidal PLGA.

Johannes Kluge; Marco Mazzotti; Gerhard Muhrer

The successful design and development of pharmaceutical drug-polymer composites requires detailed information about the phase behavior of the drug-polymer binary system. This study presents an extended investigation of the phase equilibrium established between the chiral anti-inflammatory drug Ketoprofen (KET) and the bio-compatible and biodegradable polymer poly(lactic-co-glycolic) acid 5050 (PLGA). Equilibration experiments were carried out in aqueous suspensions of KET crystals together with PLGA in the form of spherical amorphous nanoparticles obtained by supercritical fluid extraction of emulsions (SFEE). The influence of temperature was studied in the range between 0°C and 50°C, while the effect of KET chirality was investigated by using two different crystalline forms of KET, namely enantiopure S-KET and a racemic compound, RS-KET, in equilibration experiments. It was found that the level of KET established in PLGA at equilibrium increases with temperature, e.g. from 6.9 wt.% at 20°C to 25.8 wt.% at 40°C for the case of S-KET. At each temperature level, the solubility of KET in PLGA was lower for equilibration with RS-KET, significantly higher for equilibration with S-KET, and the highest for simultaneous equilibration with both crystalline species. Experimental solubility data of KET in PLGA were also described in a model based on the Sanchez-Lacombe equation of state. For experiments carried out at 10°C or below, an equilibrium state could not be reached even after a prolonged equilibration period, presumably because the polymer phase had undergone a transition into the glassy state. For this temperature range, where an experimental equilibration is not any more possible, the model may be used to estimate the solubility of KET in PLGA by extrapolation.


Journal of Supercritical Fluids | 2009

Production of PLGA micro- and nanocomposites by supercritical fluid extraction of emulsions: I. Encapsulation of lysozyme

Johannes Kluge; Francesco Fusaro; Nathalie Casas; Marco Mazzotti; Gerhard Muhrer


International Journal of Pharmaceutics | 2006

Use of compressed gas precipitation to enhance the dissolution behavior of a poorly water-soluble drug: Generation of drug microparticles and drug–polymer solid dispersions

Gerhard Muhrer; Ulrich Meier; Francesco Fusaro; Siria Albano; Marco Mazzotti


Journal of Supercritical Fluids | 2012

High pressure homogenization of pharmaceutical solids

Johannes Kluge; Gerhard Muhrer; Marco Mazzotti


Journal of Supercritical Fluids | 2009

Rational design of drug–polymer co-formulations by CO2 anti-solvent precipitation

Johannes Kluge; Francesco Fusaro; Gerhard Muhrer; Ranjit Thakur; Marco Mazzotti


Journal of Supercritical Fluids | 2009

Compressed CO2 antisolvent precipitation of lysozyme

Francesco Fusaro; Johannes Kluge; Marco Mazzotti; Gerhard Muhrer


Archive | 2009

Polymorph of (R)-3- (2-Hydroxy-2, 2-Diphenyl -Acetoxy) -1- (Isoxazol-s-ylcarbamoyl-methyl)-1-Azoni A-Bicyclo-[2.2.2] Octane Bromide

Stephanie Monnier; Gerhard Muhrer


Archive | 2008

Process for reducing the tendency of a glycopyyronium salt to aggegate during storage.

Gerhard Muhrer; Norbert Rasenack; Michael Juhnke


Archive | 2006

Process for removing residual volatile monomers from a polymer in powder form

Gerhard Muhrer; Gesine Winzenburg


Archive | 2010

Process for removing residual volatile monomers from a polymer in powder form or troche form

Gerhard Muhrer; Gesine Winzenburg

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