Increased bioavailability of a P-gp substrate: Co-release of etoposide and zosuquidar from amorphous solid dispersions

Rasmus Blaaholm Nielsen; Bjarke Strøm Larsen; René Holm; Ils Pijpers; Jan Snoeys; Ulla Gro Nielsen; Ingunn Tho; Carsten Uhd Nielsen

doi:10.1016/j.ijpharm.2023.123094

Increased bioavailability of a P-gp substrate: Co-release of etoposide and zosuquidar from amorphous solid dispersions

Int J Pharm. 2023 Jul 25:642:123094. doi: 10.1016/j.ijpharm.2023.123094. Epub 2023 May 30.

Authors

Rasmus Blaaholm Nielsen¹, Bjarke Strøm Larsen², René Holm¹, Ils Pijpers³, Jan Snoeys³, Ulla Gro Nielsen¹, Ingunn Tho², Carsten Uhd Nielsen⁴

Affiliations

¹ Department of Physics, Chemistry and Pharmacy, University of Southern Denmark, Campusvej 55, DK-5230 Odense, Denmark.
² Department of Pharmacy, University of Oslo, Sem Sælands vei 3, NO-0371 Oslo, Norway.
³ Drug Metabolism and Pharmacokinetics, Janssen R&D, Johnson & Johnson, Turnhoutseweg 30, BE-2340 Beerse, Belgium.
⁴ Department of Physics, Chemistry and Pharmacy, University of Southern Denmark, Campusvej 55, DK-5230 Odense, Denmark. Electronic address: cun@sdu.dk.

PMID: 37263451
DOI: 10.1016/j.ijpharm.2023.123094

Abstract

P-glycoprotein (P-gp) inhibitors, like zosuquidar, partly increase oral bioavailability of P-gp substrates, such as etoposide. Here, it was hypothesised that co-release of etoposide and zosuquidar from amorphous solid dispersions (ASDs) may further increase oral etoposide bioavailability. This was envisioned through simultaneous co-release and subsequent spatiotemporal association of etoposide and zosuquidar in the small intestinal lumen. To further achieve this, ASDs of etoposide and zosuquidar in polyvinylpyrrolidone (PVP), hydroxypropylmethyl cellulose (HPMC) 5, and HPMC 4 k were prepared by freeze-drying. From these ASDs, etoposide release was fastest from PVP, then HPMC 5 and slowest from HPMC 4. Release from PVP and HPMC5 resulted in stable supersaturations of etoposide. In transcellular permeability studies across MDCKII-MDR1 cell monolayers, the accumulated amount of etoposide increased 3.7-4.9-fold from amorphous etoposide or when incorporated into PVP- or HPMC 5-based ASDs, compared to crystalline etoposide. In vivo, the oral bioavailability in Sprague Dawley rats increased from 1.0 to 2.4-3.4 %, when etoposide was administered as amorphous drug or in ASDs. However, when etoposide and zosuquidar were co-administered, the oral bioavailability increased further to 8.2-18 %. Interestingly, a distinct increase in oral etoposide bioavailability to 26 % was observed when etoposide and zosuquidar were co-administration in HPMC5-based ASDs. The supersaturation of etoposide as well as the simultaneous co-release of etoposide and zosuquidar in the small intestinal lumen may explain the observed bioavailability increase. Overall, this study suggested that simultaneous co-release of an amorphous P-gp substrate and inhibitor may be a novel and viable formulation strategy to increase the bioavailability P-gp substrates.

Keywords: Amorphous solid dispersion; Etoposide; Hydroxypropylmethyl cellulose (HPMC); In vivo; Oral bioavailability; P-glycoprotein; Polyvinylpyrrolidone (PVP); Zosuquidar; Zosuquidar (LY-335979).

MeSH terms

Animals
Biological Availability
Etoposide
Hypromellose Derivatives / chemistry
Pharmaceutical Preparations / chemistry
Povidone* / chemistry
Rats
Rats, Sprague-Dawley
Solubility

Substances

Etoposide
Pharmaceutical Preparations
Povidone
Hypromellose Derivatives