Intra-articular bioactivity of a p38 MAPK inhibitor and development of an extended-release system

  • Eur J Pharm Biopharm. 2015 Jun;93:110-7. doi: 10.1016/j.ejpb.2015.03.017.
Julie Pradal  1 Maria-Fernanda Zuluaga  1 Pierre Maudens  1 Jean-Marc Waldburger  2 Christian Alexander Seemayer  3 Eric Doelker  1 Cem Gabay  2 Olivier Jordan  1 Eric Allémann  4
Affiliations
  • 1. School of Pharmaceutical Sciences, University of Geneva, University of Lausanne, Geneva, Switzerland.
  • 2. Division of Rheumatology, Department of Internal Medicine, University Hospital and Department of Pathology and Immunology, University of Geneva, School of Medicine, Switzerland.
  • 3. Novartis Pharma AG, Postfach, Basel, Switzerland.
  • 4. School of Pharmaceutical Sciences, University of Geneva, University of Lausanne, Geneva, Switzerland. Electronic address: [email protected].
Abstract

In the treatment of arthritic diseases, oral or systemic administration of anti-inflammatory substances, such as p38 MAPK inhibitors, is hampered by numerous side effects. To overcome them, formulations of rapid and extended drug delivery systems were studied in intra-articular administration. For the first time, VX-745, a highly selective p38 MAPK Inhibitor, demonstrated in vivo bioactivity, similar to dexamethasone activity, following intra-articular administration in an antigen-induced arthritic (AIA) mouse model. The in vitro bioactivity of VX-745 was also shown on synoviocytes, reducing the IL-6 concentration. Process and formulation parameters (i.e., polymer concentration, aqueous/organic phase ratio, emulsification speed and process, and evaporation pressure) and particle characterisation (i.e., drug loading, size of particle, and surface aspect) were extensively examined to produce optimised formulations. Indeed, a burst release provides a rapid saturation of intracellular p38 MAPK to relieve patients from pain and inflammation. Then, drug diffusion would be sufficient to maintain an effective dose over 2-3 months. This study confirms the effectiveness of encapsulated p38 MAPK inhibitors in extended drug delivery systems and seems to be a promising strategy for intra-articular treatment.

Keywords
Drug delivery system; Intra-articular; Liposomes; Long-term release; Microparticles; P38 MAPK inhibitors; PLA; PLGA.
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