Exploring Bioequivalence of Dexketoprofen Trometamol Drug Products with the Gastrointestinal Simulator (GIS) and Precipitation Pathways Analyses

Marival Bermejo; Gislaine Kuminek; Jozef Al-Gousous; Alejandro Ruiz-Picazo; Yasuhiro Tsume; Alfredo Garcia-Arieta; Isabel González-Alvarez; Bart Hens; Gregory E Amidon; Nair Rodriguez-Hornedo; Gordon L Amidon; Deanna Mudie

doi:10.3390/pharmaceutics11030122

Exploring Bioequivalence of Dexketoprofen Trometamol Drug Products with the Gastrointestinal Simulator (GIS) and Precipitation Pathways Analyses

Pharmaceutics. 2019 Mar 15;11(3):122. doi: 10.3390/pharmaceutics11030122.

Authors

Marival Bermejo^{1

2}, Gislaine Kuminek³, Jozef Al-Gousous^{4

5}, Alejandro Ruiz-Picazo⁶, Yasuhiro Tsume^{7

8}, Alfredo Garcia-Arieta⁹, Isabel González-Alvarez¹⁰, Bart Hens^{11

12}, Gregory E Amidon¹³, Nair Rodriguez-Hornedo¹⁴, Gordon L Amidon¹⁵, Deanna Mudie^{16

17}

Affiliations

¹ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. mbermejo@goumh.umh.es.
² Department Engineering Pharmacy Section, Miguel Hernandez University, San Juan de Alicante, 03550 Alicante, Spain. mbermejo@goumh.umh.es.
³ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. gkuminek@umich.edu.
⁴ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. jalgouso@umich.edu.
⁵ Department of Biopharmaceutics and Pharmaceutical Technology, Johannes Gutenberg Universität Mainz, D-55099 Mainz, Germany. jalgouso@umich.edu.
⁶ Department Engineering Pharmacy Section, Miguel Hernandez University, San Juan de Alicante, 03550 Alicante, Spain. alejandroruizpicazo@gmail.com.
⁷ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. ytsume@umich.edu.
⁸ Merck and Co., Inc., 126 E Lincoln Ave, Rahway, NJ 07065, USA. ytsume@umich.edu.
⁹ Service on Pharmacokinetics and Generic Medicines, Division of Pharmacology and Clinical Evaluation, Department of Human Use Medicines, Spanish Agency for Medicines and Health Care Products, 28022 Madrid, Spain. agarciaa@aemps.es.
¹⁰ Department Engineering Pharmacy Section, Miguel Hernandez University, San Juan de Alicante, 03550 Alicante, Spain. isabel.gonzalez@goumh.umh.es.
¹¹ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. barthens@umich.edu.
¹² Department of Pharmaceutical and Pharmacological Sciences, KU Leuven, Herestraat 49, 3000 Leuven, Belgium. barthens@umich.edu.
¹³ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. geamidon@umich.edu.
¹⁴ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. nrh@umich.edu.
¹⁵ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. glamidon@umich.edu.
¹⁶ Department of Pharmaceutical Sciences, College of Pharmacy, University of Michigan, Ann Arbor, MI 48109, USA. deanna.mudie@lonza.com.
¹⁷ Drug Product Development and Innovation, Lonza Pharma and Biotech, Bend, OR 97703, USA. deanna.mudie@lonza.com.

Abstract

The present work aimed to explain the differences in oral performance in fasted humans who were categorized into groups based on the three different drug product formulations of dexketoprofen trometamol (DKT) salt-Using a combination of in vitro techniques and pharmacokinetic analysis. The non-bioequivalence (non-BE) tablet group achieved higher plasma C_max and area under the curve (AUC) than the reference and BE tablets groups, with only one difference in tablet composition, which was the presence of calcium monohydrogen phosphate, an alkalinizing excipient, in the tablet core of the non-BE formulation. Concentration profiles determined using a gastrointestinal simulator (GIS) apparatus designed with 0.01 N hydrochloric acid and 34 mM sodium chloride as the gastric medium and fasted state simulated intestinal fluids (FaSSIF-v1) as the intestinal medium showed a faster rate and a higher extent of dissolution of the non-BE product compared to the BE and reference products. These in vitro profiles mirrored the fraction doses absorbed in vivo obtained from deconvoluted plasma concentration⁻time profiles. However, when sodium chloride was not included in the gastric medium and phosphate buffer without bile salts and phospholipids were used as the intestinal medium, the three products exhibited nearly identical concentration profiles. Microscopic examination of DKT salt dissolution in the gastric medium containing sodium chloride identified that when calcium phosphate was present, the DKT dissolved without conversion to the less soluble free acid, which was consistent with the higher drug exposure of the non-BE formulation. In the absence of calcium phosphate, however, dexketoprofen trometamol salt dissolution began with a nano-phase formation that grew to a liquid⁻liquid phase separation (LLPS) and formed the less soluble free acid crystals. This phenomenon was dependent on the salt/excipient concentrations and the presence of free acid crystals in the salt phase. This work demonstrated the importance of excipients and purity of salt phase on the evolution and rate of salt disproportionation pathways. Moreover, the presented data clearly showed the usefulness of the GIS apparatus as a discriminating tool that could highlight the differences in formulation behavior when utilizing physiologically-relevant media and experimental conditions in combination with microscopy imaging.

Keywords: dexketoprofen; gastrointestinal absorption; gastrointestinal simulator; in vitro dissolution; liquid–liquid phase separation; microscopy imaging; oral absorption.

Abstract

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