Hyperthermia-Induced In Situ Drug Amorphization by Superparamagnetic Nanoparticles in Oral Dosage Forms

Shaquib Rahman Ansari; Nele-Johanna Hempel; Shno Asad; Peter Svedlindh; Christel A S Bergström; Korbinian Löbmann; Alexandra Teleki

doi:10.1021/acsami.2c03556

Hyperthermia-Induced In Situ Drug Amorphization by Superparamagnetic Nanoparticles in Oral Dosage Forms

ACS Appl Mater Interfaces. 2022 May 18;14(19):21978-21988. doi: 10.1021/acsami.2c03556. Epub 2022 Apr 22.

Authors

Shaquib Rahman Ansari¹, Nele-Johanna Hempel², Shno Asad¹, Peter Svedlindh³, Christel A S Bergström⁴, Korbinian Löbmann², Alexandra Teleki¹

Affiliations

¹ Department of Pharmacy, Science for Life Laboratory, Uppsala University, Uppsala 75123, Sweden.
² Department of Pharmacy, University of Copenhagen, Copenhagen 2100, Denmark.
³ Department of Materials Science and Engineering, Uppsala University, Uppsala 75103, Sweden.
⁴ The Swedish Drug Delivery Center, Department of Pharmacy, Uppsala University, Uppsala 75123, Sweden.

Abstract

Superparamagnetic iron oxide nanoparticles (SPIONs) generate heat upon exposure to an alternating magnetic field (AMF), which has been studied for hyperthermia treatment and triggered drug release. This study introduces a novel application of magnetic hyperthermia to induce amorphization of a poorly aqueous soluble drug, celecoxib, in situ in tablets for oral administration. Poor aqueous solubility of many drug candidates is a major hurdle in oral drug development. A novel approach to overcome this challenge is in situ amorphization of crystalline drugs. This method facilitates amorphization by molecular dispersion of the drug in a polymeric network inside a tablet, circumventing the physical instability encountered during the manufacturing and storage of conventional amorphous solid dispersions. However, the current shortcomings of this approach include low drug loading, toxicity of excipients, and drug degradation. Here, doped SPIONs produced by flame spray pyrolysis are compacted with polyvinylpyrrolidone and celecoxib and exposed to an AMF in solid state. A design of experiments approach was used to investigate the effects of SPION composition (Zn_0.5Fe_2.5O₄ and Mn_0.5Fe_2.5O₄), doped SPION content (10-20 wt %), drug load (30-50 wt %), and duration of AMF (3-15 min) on the degree of drug amorphization. The degree of amorphization is strongly linked to the maximum tablet temperature achieved during the AMF exposure (r = 0.96), which depends on the SPION composition and content in the tablets. Complete amorphization is achieved with 20 wt % Mn_0.5Fe_2.5O₄ and 30 wt % celecoxib in the tablets that reached the maximum temperature of 165.2 °C after 15 min of AMF exposure. Furthermore, manganese ferrite exhibits no toxicity in human intestinal Caco-2 cell lines. The resulting maximum solubility of in situ amorphized celecoxib is 5 times higher than that of crystalline celecoxib in biorelevant intestinal fluid. This demonstrates the promising capability of SPIONs as enabling excipients to magnetically induce amorphization in situ in oral dosage forms.

Keywords: amorphous solid dispersions; in situ drug amorphization; magnetic hyperthermia; oral drug delivery; superparamagnetic nanoparticles.

MeSH terms

Caco-2 Cells
Celecoxib / chemistry
Excipients / chemistry
Humans
Hyperthermia, Induced*
Magnetic Iron Oxide Nanoparticles
Nanoparticles* / chemistry
Solubility
Tablets

Substances

Excipients
Tablets
Celecoxib