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In vitro-in vivo evaluation of lipid based formulations of the CETP inhibitors CP-529,414 (torcetrapib) and CP-532,623.

Claire L McEvoy, Natalie L Trevaskis, Glenn A Edwards, Michael E Perlman, Catherine M Ambler, Mary C Mack, Barbara Brockhurst, Christopher J H Porter

European journal of pharmaceutics and biopharmaceutics : official journal of Arbeitsgemeinschaft für Pharmazeutische Verfahrenstechnik e.V 2014 Nov


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  • cholesterol ester transfer proteins (2)
  • cp 529, 414 (1)
  • cp 532, 623 (6)
  • cross over studies (1)
  • dogs (3)
  • lipid (8)
  • male (1)
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  • quinolines (2)
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    The present study investigated the use of lipid based drug delivery systems to enhance the oral bioavailability of the CETP inhibitors CP-532,623 and torcetrapib. A series of self-emulsifying lipid based drug delivery systems (SEDDS) were assembled and examined using an in vitro lipid digestion model to evaluate patterns of drug precipitation under simulated intestinal conditions. Drug exposure after oral administration of the same formulations was subsequently assessed in beagle dogs. CP-532,623 was maintained in a solubilised state during dispersion of most formulations in simulated intestinal fluid, however, solubilisation capacity was reduced to various degrees upon in vitro digestion. Administration of SEDDS formulations to beagle dogs resulted in moderate differences in plasma AUC when compared to the differences in solubilisation observed in vitro. Similar trends were observed for torcetrapib. In all cases, however, in vivo exposure of CP-532,623 was greatly enhanced by administration in lipid based drug delivery systems when compared to a powder formulation. Some correlation between in vitro solubilisation and in vivo drug exposure (AUC) was evident; however, this was not linear. The data suggest that for highly lipophilic drugs such as CP-532,623 in vitro digestion data may be a conservative in vitro indicator of utility and that good exposure may be evident even for formulations that result in significant drug precipitation during in vitro digestion. Copyright © 2014 Elsevier B.V. All rights reserved.

    Citation

    Claire L McEvoy, Natalie L Trevaskis, Glenn A Edwards, Michael E Perlman, Catherine M Ambler, Mary C Mack, Barbara Brockhurst, Christopher J H Porter. In vitro-in vivo evaluation of lipid based formulations of the CETP inhibitors CP-529,414 (torcetrapib) and CP-532,623. European journal of pharmaceutics and biopharmaceutics : official journal of Arbeitsgemeinschaft für Pharmazeutische Verfahrenstechnik e.V. 2014 Nov;88(3):973-85

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    PMID: 25152213

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