Novel High-Drug-Loaded Amorphous Dispersion Tablets of Posaconazole; In Vivo and In Vitro Assessment

Deanna M Mudie; Aaron M Stewart; Nishant Biswas; Timothy J Brodeur; Kimberly B Shepard; Adam Smith; Michael M Morgen; John M Baumann; David T Vodak

doi:10.1021/acs.molpharmaceut.0c00471

Novel High-Drug-Loaded Amorphous Dispersion Tablets of Posaconazole; In Vivo and In Vitro Assessment

Mol Pharm. 2020 Dec 7;17(12):4463-4472. doi: 10.1021/acs.molpharmaceut.0c00471. Epub 2020 Sep 4.

Authors

Deanna M Mudie¹, Aaron M Stewart¹, Nishant Biswas¹, Timothy J Brodeur¹, Kimberly B Shepard¹, Adam Smith¹, Michael M Morgen¹, John M Baumann¹, David T Vodak¹

Affiliation

¹ Lonza Pharma and Biotech, Bend, Oregon 97703, United States.

PMID: 32835489
DOI: 10.1021/acs.molpharmaceut.0c00471

Abstract

Amorphous solid dispersions (ASDs) can increase the bioavailability of drugs with poor aqueous solubility. However, concentration-sustaining dispersion polymers (CSPs) incorporated in ASDs can result in low drug loading and, therefore, a large dosage-form size or multiple units to meet dose requirements, potentially decreasing patient compliance. To address this challenge, a high-loaded dosage-form (HLDF) architecture for ASDs was developed, in which a drug is first spray-dried with a high glass-transition temperature (T_g) dispersion polymer to facilitate high drug loading while maintaining physical stability. The ASD is then granulated with a CSP designed to extend supersaturation in solution. The HLDF differs from traditional ASD architectures in which the dispersion polymer inside the ASD acts as the CSP. By strategically combining two different polymers, one "inside" and one "outside" the ASD, solubilization performance, physical stability, and overall drug loading are maximized. This study demonstrates in vivo performance of the HLDF architecture using posaconazole as a model drug. Two sizes of HLDF tablets were tested in beagle dogs, along with traditional ASD architecture (benchmark) tablets, ASD tablets without a CSP, and a commercial crystalline oral suspension (Noxafil OS). HLDF tablets performed equivalently to the benchmark tablets, the smaller HLDF tablet being 40% smaller (by mass) than the benchmark tablet. The HLDF tablets doubled the blood plasma AUC relative to Noxafil OS. In line with the in vivo outcome, in vitro results in a multicompartment dissolution apparatus demonstrated similar area under the curve (AUC) values in the intestinal compartment for ASD tablets. However, the in vitro data underpredicted the relative in vivo AUC of Noxafil OS compared to the ASD tablets. This study demonstrated that the HLDF approach can increase drug loadings while achieving good performance for ASD drug products.

Keywords: absorption; amorphous solid dispersion; bioavailability enhancement; high drug loading; in vitro dissolution; weak base precipitation.

MeSH terms

Administration, Oral
Animals
Antifungal Agents / administration & dosage
Antifungal Agents / chemistry
Antifungal Agents / pharmacokinetics*
Area Under Curve
Biological Availability
Crystallization
Dogs
Drug Compounding / methods*
Drug Liberation
Models, Animal
Solubility
Spray Drying
Suspensions
Tablets
Triazoles / administration & dosage
Triazoles / chemistry
Triazoles / pharmacokinetics*

Substances

Antifungal Agents
Suspensions
Tablets
Triazoles
posaconazole