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Featured researches published by Thomas Kieckbusch.


Journal of drug assessment | 2013

Delivery characteristics of a low-resistance dry-powder inhaler used to deliver the long-acting muscarinic antagonist glycopyrronium

Paul Colthorpe; Thomas Voshaar; Thomas Kieckbusch; Erika Cuoghi; Juergen Jauernig

Abstract Objectives: The long-acting muscarinic antagonist (LAMA) glycopyrronium (NVA237) has recently been approved as a once-daily treatment for COPD. The objectives of this study were to determine the dose delivery characteristics of glycopyrronium and compare them with those of the LAMA tiotropium, both delivered by their respective capsule-based dry-powder inhalers (DPIs). Research design and methods: Seven inhalation profiles derived from patients with moderate and severe COPD were reproduced to determine the aerodynamic particle size distribution of glycopyrronium delivered by the Breezhaler device, a low-resistance DPI. Theoretical respiratory tract deposition was estimated using a semi-empirical model for healthy lungs. These results were compared with those of tiotropium delivered by the high-resistance HandiHaler device obtained in a previous study using the same set of inhalation profiles. Study limitations are that fine particle fraction (FPF) and particle size are generated by the inhalers are not a direct measure of lung deposition, and the bronchodilator effect of inhaled drugs does not depend solely upon the percentage of the total dose that reaches the lung. Results: The mean FPF (≤4.7 µm) was 42.6% of the nominal dose (which refers to the content of the capsule) for glycopyrronium and 9.8% for tiotropium while the mass median aerodynamic diameter (MMAD) was 2.8 µm and 3.9 µm for glycopyrronium and tiotropium, respectively. The mean estimated intrathoracic drug deposition as a percentage of the mean dose delivered to the Next Generation Impactor was 39% for glycopyrronium and 22% for tiotropium. Conclusions: The glycopyrronium capsule-based DPI delivered a higher FPF and greater and more consistent intrathoracic deposition irrespective of age and disease severity compared to the tiotropium capsule-based DPI, suggesting that it may be suitable for use by patients with a wide range of COPD severities.


Archive | 2007

Compositions of Glycopyrronium Salt for Inhalation

Barbara Haeberlin; Frank Stowasser; Wolfgang Wirth; Anton Baumberger; Stephan Abel; Sebastian Kaerger; Thomas Kieckbusch


Archive | 2013

Original article Delivery characteristics of a low-resistance dry-powder inhaler used to deliver the long- acting muscarinic antagonist glycopyrronium*

Paul Colthorpe; Thomas Voshaar; Thomas Kieckbusch; Erika Cuoghi; Juergen Jauernig


Archive | 2008

Process for preparing particulates of crystalline drug substance

Gerhard Muhrer; Thomas Kieckbusch; Dilraj Singh; Ranjit Thakur; Kurt Schaffluetzel; Norbert Rasenack


Archive | 2008

Verfahren zur herstellung eines partikulären und kristallinen wirkstoffes

Gerhard Muhrer; Thomas Kieckbusch; Dilraj Singh; Ranjit Thakur; Kurt Schaffluetzel; Norbert Rasenack


Archive | 2008

Procede de preparation de particules de substance medicamenteuse cristalline

Gerhard Muhrer; Thomas Kieckbusch; Dilraj Singh; Ranjit Thakur; Kurt Schaffluetzel; Norbert Rasenack


Archive | 2008

Process for preparing a particulate and crystalline drug substance

Gerhard Muhrer; Thomas Kieckbusch; Dilraj Singh; Ranjit Thakur; Kurt Schaffluetzel; Norbert Rasenack


Archive | 2008

Process for preparing a drug substance in crystalline particles and

Gerhard Muhrer; Thomas Kieckbusch; Dilraj Singh; Ranjit Thakur; Kurt Schaffluetzel; Norbert Rasenack


Archive | 2007

Composiciones de sal de glicopirronio para inhalación

Barbara Haeberlin; Frank Stowasser; Wolfgang Wirth; Anton Baumberger; Stephan Abel; Sebastian Kaerger; Thomas Kieckbusch


Archive | 2007

Formulierungen enthaltend glycopyrroniumsalz zur inhalation

Barbara Haeberlin; Frank Stowasser; Wolfgang Wirth; Anton Baumberger; Stephan Abel; Sebastian Kaerger; Thomas Kieckbusch

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