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Featured researches published by Michael Ausborn.


International Journal of Pharmaceutics | 2008

Stability of proteins encapsulated in injectable and biodegradable poly(lactide-co-glycolide)-glucose millicylinders.

Jichao Kang; Oliver Lambert; Michael Ausborn; Steven P. Schwendeman

PURPOSE To characterize protein stability in poly(lactide-co-glycolide) 50/50-glucose star (PLGA-Glu) injectable millicylinders and to compare results with linear PLGA 50/50. METHODS Bovine serum albumin (BSA), a model protein, was encapsulated in PLGA-Glu and linear PLGA millicylinders by solvent-extrusion and incubated under physiological conditions. Important system properties were characterized, including: polymer molecular weight distribution, soluble acidic residues, polymer morphology, polymer water uptake, microclimate pH, protein content and release, and protein aggregation. The polymer microclimate late in the release incubation was simulated and protein recovery was analyzed by UV280, size exclusion chromatography, amino acid analysis, and a modified Bradford assay. RESULTS PLGA-Glu contained higher levels of low molecular weight oligomers, more rapidly biodegraded, and exhibited a lower microclimate pH than the linear 50/50 PLGA, which is the most acidic type in the PLGA family. BSA, when encapsulated in PLGA-Glu millicylinders, underwent extensive noncovalent insoluble aggregation over 2 weeks in vitro release, which was almost completely inhibited upon co-encapsulation of Mg(OH)2. However, by 5 weeks release for base-containing formulations, although insoluble aggregation was still suppressed, the soluble fraction of protein in the polymer was unrecoverable by the modified Bradford assay. Polymer microclimate simulations with extensive protein analysis strongly suggested that the low recovery was mostly caused by base-catalyzed hydrolysis of the oligomeric fraction of BSA. CONCLUSIONS In PLGA-Glu, the acidic microclimate was similarly responsible for insoluble aggregation of encapsulated BSA. BSA aggregation was inhibited in millicylinders by co-incorporation into the polymer an insoluble base, but over a shorter release interval than linear PLGA likely because of a more acidic microclimate in the star polymer.


Journal of Controlled Release | 2003

In vivo biocompatibility and biodegradation of poly(ethylene carbonate)

Mahrokh Dadsetan; Elizabeth M. Christenson; F. Unger; Michael Ausborn; Thomas Kissel; Anne Hiltner; James M. Anderson


Archive | 2002

Ophthalmic deport formulations for periocular or subconjunctival administration

Marklus Ahlheim; Michael Ausborn; David Bodmer; Christian Schoch


Journal of Controlled Release | 2007

Poly(ethylene carbonate): a thermoelastic and biodegradable biomaterial for drug eluting stent coatings?

Florian Unger; Ullrich Westedt; Phillip Hanefeld; Ralf Wombacher; Sven Zimmermann; Andreas Greiner; Michael Ausborn; Thomas Kissel


Archive | 2003

Microparticles prepared using an ionic liquid

Michael Ausborn; Thomas Kissel; Ernst Küsters


Archive | 2008

Ophthalmic depot formulations for periocular or suconjunctival administration

Marklus Ahlheim; Michael Ausborn; David Bodmer; Christian Schoch


Archive | 2003

Pharmaceutical Composition Comprising Octreotide Microparticles

Olivier Lambert; Michael Ausborn; Holger Petersen; Rolf Loeffler; Jean Daniel Bonny


Archive | 2011

Pharmaceutical composition including octreotide microparticle

Michael Ausborn; Jean-Daniel Bonny; Olivier Lambert; Rolf Loeffler; Holger Petersen; オリヴィエ・ランベール; ジャン−ダニエル・ボニー; ホルガー・ペーターゼン; ミヒャエル・アウスボルン; ロルフ・レフラー


Archive | 2010

Depot preparation for eyes for administration on eye surrounding or subconjunctivally

Markus Ahlheim; Michael Ausborn; David Bodmer; Christian Schoch; クリスティアン・ショッホ; ダフィト・ボドマー; マルクス・アールハイム; ミヒャエル・アウスボルン


Archive | 2008

Medicine composition containing octreotide grains

Michael Ausborn; Olivier Lambert; Rolf Lofler; Holger Petersen

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