Bioavailability of a lipidic formulation of curcumin in healthy human volunteers

Yogesh B. Pawar, Bhushan Munjal, Saurabh Arora, Manoj Karwa, Gunjan Kohli, Jyoti K. Paliwal, Arvind K. Bansal

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37 Scopus citations

Abstract

Numerous publications have reported the significant pharmacodynamic activity of Curcumin (CRM) despite low or undetectable levels in plasma. The objective of the present study was to perform a detailed pharmacokinetic evaluation of CRM after the oral administration of a highly bioavailable lipidic formulation of CRM (CRM-LF) in human subjects. Cmax, Tmaxand AUC0-∞; were found to be 183.35 ± 37.54 ng/mL, 0.60 ± 0.05 h and 321.12 ± 25.55 ng/mL respectively, at a dose of 750 mg. The plasma profile clearly showed three distinct phases, viz., absorption, distribution and elimination. A close evaluation of the primary pharmacokinetic parameters provided valuable insight into the behavior of the CRM after absorption by CRM-LF. CRM-LF showed a lag time (Tlag) of 0.18 h (around 12 min). Pharmacokinetic modeling revealed that CRM-LF followed a two-compartment model with first order absorption, lag time and first order elimination. A high absorption rate constant (K01 4.51/h) signifies that CRM-LF ensured rapid absorption of the CRM into the central compartment. This was followed by the distribution of CRM from the central to peripheral compartment (K12 2.69/h). The rate of CRM transfer from the peripheral to central compartment (K21 0.15/h) was slow. This encourages higher tissue levels of CRM as compared with plasma levels. The study provides an explanation of the therapeutic efficacy of CRM, despite very low/undetectable levels in the plasma.

Original languageEnglish (US)
Pages (from-to)517-530
Number of pages14
JournalPharmaceutics
Volume4
Issue number4
DOIs
StatePublished - Dec 2012
Externally publishedYes

Keywords

  • Absorption
  • Bioavailability
  • Curcumin
  • Pharmacokinetic modeling

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