Improved oral bioavailability of BCS class 2 compounds by self nano-emulsifying drug delivery systems (SNEDDS): The underlying mechanisms for amiodarone and talinolol

Anna Elgart, Irina Cherniakov, Yanir Aldouby, Abraham J. Domb, Amnon Hoffman

Research output: Contribution to journalArticlepeer-review

85 Scopus citations

Abstract

Purpose: Superior bioavailability of BCS Class 2 compounds incorporated into SNEDDS was previously reported. This study aims to elucidate the underlying mechanisms accountable for this phenomenon. Methods: SNEDDS of amiodarone (AM) and talinolol were developed. Pharmacokinetic parameters were assessed in vivo. Effect on intestinal permeability, P-gp efflux and toxicity was evaluated in vitro (Caco-2) and ex vivo (Ussing). Solubilization was assessed in vitro (Dynamic Lipolysis Model). Effect on intraenterocyte metabolism was evaluated using CYP3A4 microsomes. Results: Oral administration of AM-SNEDDS and talinolol-SNEDDS resulted in higher and less variable AUC and Cmax. In vitro, higher talinolol-SNEDDS Papp indicated Pgp inhibition. Lipolysis of AM-SNEDDS resulted in higher AM concentration in the fraction available for absorption. Incubation of AM-SNEDDS with CYP3A4 indicated CYP inhibition. SNEDDS didn't alter mannitol Papp and TEER. SNEDDS effect was transient. Conclusions: Multiple mechanisms are accountable for improved bioavailability and reduced variability of Class-2 compounds by SNEDDS: increased solubilization, reduced intraenterocyte metabolism and reduced P-gp efflux. SNEDDS effect is reversible and doesn't cause intestinal tissue or cell damage. These comprehensive findings can be used for intelligent selection of drugs for which oral bioavailability will improve upon incorporation into SNEDDS, based on recognition of the drug's absorption barriers and the ability of SNEDDS to overcome them.

Original languageEnglish
Pages (from-to)3029-3044
Number of pages16
JournalPharmaceutical Research
Volume30
Issue number12
DOIs
StatePublished - Dec 2013
Externally publishedYes

Bibliographical note

Funding Information:
This study was in part supported by the Nofar Program of the Israel Ministry of Commerce and Trade.

Funding

This study was in part supported by the Nofar Program of the Israel Ministry of Commerce and Trade.

FundersFunder number
Israel Ministry of Commerce and Trade

    Keywords

    • P-gp efflux
    • first pass metabolism
    • intestinal absorption
    • intestinal solubilization
    • intra-enterocyte metabolism
    • lipophilic drugs
    • self emulsifying drug delivery systems

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