Hans Wim Pieter Vermeersch
Tibotec
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Publication
Featured researches published by Hans Wim Pieter Vermeersch.
American Journal of Health-system Pharmacy | 2008
Pak Chan; Amanda Bishop; Thomas C. Kupiec; Lawrence A Trissel; Dilip Gole; Ilias Jimidar; Hans Wim Pieter Vermeersch
PURPOSE The physical compatibility of the new cephalosporin ceftobiprole medocaril with 70 other drugs during simulated Y-site injection was studied. METHODS Ceftobiprole was reconstituted with sterile water for injection. Dilutions of ceftobiprole 2 mg/mL (as ceftobiprole medocaril 2.67 mg/mL) were prepared in 5% dextrose injection, 0.9% sodium chloride injection, and lactated Ringers injection. For testing compatibility with the other drugs, a 5-mL sample of the ceftobiprole 2-mg/mL admixtures was combined with a 5-mL sample of the other drug either undiluted or diluted with one of the three vehicles. Each combination was prepared in duplicate, switching the order of drug addition, and kept at room temperature. At intervals up to four hours after preparation, samples were examined visually and with the aid of a Tyndall beam and measured with a turbidimeter and a particle sizer and counter. Compatibility with propofol was evaluated by checking for emulsion separation and particles after centrifugation. RESULTS In all three vehicles, ceftobiprole was compatible with 31 other drugs and incompatible with 32. With 7 drugs, compatibility was dependent on the vehicle used. Signs of incompatibility included the presence of visible and subvisible particles, haze, and turbidity. No incompatibilities were related to the order of mixing. CONCLUSION Of the 70 drugs evaluated for compatibility with ceftobiprole 2 mg/ mL (as medocaril) in 5% dextrose injection, 0.9% sodium chloride injection, and lactated Ringers injection, 31 were found to be compatible and 32 were found to be incompatible in all three of the infusion solutions. For 7 of the drugs, compatibility was dependent on which infusion solution was used. Ceftobiprole medocaril should not be simultaneously administered via a Y site with drugs with which it was shown to be incompatible.
Journal of Chromatography A | 2003
Stefanie Leonard; Rául Capote; Nils Germonprez; Luc Van Puyvelde; Norbert De Kimpe; Hans Wim Pieter Vermeersch; Jan Rosier; Louis Maes; Eugene Roets; Jos Hoogmartens
A liquid chromatographic method was developed for the separation of six related triterpenoid saponins in Maesa balansae extracts with different purity, active against leishmaniasis. As stationary phase a Hypersil BDS C18 column (3 microm), 100 x 4.6 mm was used. The mobile phase was a mixture of methanol, acetonitrile, 5% (m/v) ammonium acetate, pH 6.5 and water. A linear gradient was developed for the analysis of crude extracts. An isocratic method was developed to analyze purified samples that mainly contained saponins 3 and 4, the most active saponins. The isocratic LC method was optimized and the robustness was evaluated with an experimental design. The method showed good selectivity, repeatability, linearity and sensitivity.
Archive | 2003
Hans Wim Pieter Vermeersch; Daniel Joseph Christiaan Thoné; Luc Donné Marie-Louise Janssens
Electrophoresis | 2005
Stefanie Leonard; Ann Van Schepdael; Tímea Iványi; István Lázár; Jan Rosier; Marc Vanstockem; Hans Wim Pieter Vermeersch
Archive | 2008
Dilip J. Gole; Ketan Amin; Llias M. Jimidar; Hans Wim Pieter Vermeersch; Michael Tran
Aaps Pharmscitech | 2011
Magali B. Hickey; Sara Waggener; Dilip Gole; Ilias Jimidar; Hans Wim Pieter Vermeersch; Poe Ratanabanangkoon; Arjen P. Tinke; Örn Almarsson
Archive | 2003
S. Leonard; Hans Wim Pieter Vermeersch; Ann Van Schepdael; Jos Hoogmartens
Archive | 2003
Hans Wim Pieter Vermeersch; Daniel Joseph Christiaan Thoné; Luc Donné Marie-Louise Janssens
Archive | 2003
Hans Wim Pieter Vermeersch; Daniel Joseph Christiaan Thoné; Luc Donné Marie-Louise Janssens; Piet Tom Bert Paul Wigernick
Archive | 2003
Hans Wim Pieter Vermeersch; Daniel Joseph Christiaan Thoné; Luc Donné Marie-Louise Janssens; Piet Bert Paul Wigerinck