Applying Material Science Principles to Chemical Stability: Modelling Solid State Autoxidation in Mifepristone Containing Different Degrees of Crystal Disorder

Jayant Iyer; Lucy M Morgan; Pamela Harrison; Adrian Davis; Andrew Ray; Stefan Mitsche; Ferdinand Hofer; Isha Saraf; Amrit Paudel

doi:10.1016/j.xphs.2023.03.020

Applying Material Science Principles to Chemical Stability: Modelling Solid State Autoxidation in Mifepristone Containing Different Degrees of Crystal Disorder

J Pharm Sci. 2023 Sep;112(9):2463-2482. doi: 10.1016/j.xphs.2023.03.020. Epub 2023 Apr 7.

Authors

Jayant Iyer¹, Lucy M Morgan², Pamela Harrison³, Adrian Davis², Andrew Ray⁴, Stefan Mitsche⁵, Ferdinand Hofer⁵, Isha Saraf¹, Amrit Paudel⁶

Affiliations

¹ Research Center Pharmaceutical Engineering GmbH (RCPE), Graz 8010, Austria.
² Pfizer Worldwide Research, Development and Medical, Sandwich, Kent, CT13 9NJ, UK.
³ Oral Product Development, Pharmaceutical Technology and Development, operations, AstraZeneca, Macclesfield SK10 2NA, UK.
⁴ New Modalities & Parenteral Development, Pharmaceutical Technology & Development, Operations, AstraZeneca, Macclesfield SK10 2NA, UK.
⁵ FELMI ZFE-Austrian Center for Electron Microscopy and Nanoanalysis Graz University of Technology, Graz 8010, Austria.
⁶ Research Center Pharmaceutical Engineering GmbH (RCPE), Graz 8010, Austria; Graz University of Technology, Institute of Process and Particle Engineering, Graz 8010, Austria. Electronic address: amrit.paudel@rcpe.at.

PMID: 37031865
DOI: 10.1016/j.xphs.2023.03.020

Abstract

Ball-milling and harsh manufacturing processes often generate crystal disorder which have practical implications on the physical and chemical stabilities of solid drugs during subsequent storage, transport, and handling. The impact of the physical state of solid drugs, containing different degrees/levels of crystal disorder, on their autoxidative stability under storage has not been widely investigated. This study investigates the impact of differing degrees of crystal disorder on the autoxidation of Mifepristone (MFP) to develop a predictive (semi-empirical) stability model. Crystalline MFP was subjected to different durations of ambient ball milling, and the resulting disorder/ amorphous content was quantified using a partial least square (PLS) regression model based on Raman spectroscopy data. Samples of MFP milled to generate varying levels of disorder were subjected to a range of (accelerated) stability conditions, and periodically sampled to examine their recrystallization and degradation extents. Crystallinity was monitored by Raman spectroscopy, and the degradation was evaluated by liquid chromatography. The analyses of milled samples demonstrated a competition between recrystallization and degradation via autoxidation of MFP, to different extents depending on stability conditions/exposure time. The degradation kinetics were analyzed by accounting for the preceding amorphous content, and fitted with a diffusion model. An extended Arrhenius equation was used to predict the degradation of stored samples under long-term (25°C/60% RH) and accelerated (40°C/75% RH, 50°C/75% RH) stability conditions. This study highlights the utility of such a predictive stability model for identifying the autoxidative instability in non-crystalline/partially crystalline MFP, owing to the degradation of the amorphous phases. This study is particularly useful for identifying drug-product instability by leveraging the concept of material sciences.

Keywords: Amorphous; Autoxidation; Crystal disorder; Mifepristone; Partially crystalline; Solid-state degradation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Calorimetry, Differential Scanning
Crystallization
Drug Stability
Materials Science*
Mifepristone*

Substances

Mifepristone