(303d) Generation of Amorphous Dispersions through a Continuous Manufacturing Train to Enable Direct Compression of Reduced Tablet Size Amorphous Dosage Units | AIChE

(303d) Generation of Amorphous Dispersions through a Continuous Manufacturing Train to Enable Direct Compression of Reduced Tablet Size Amorphous Dosage Units

Authors 

Schenck, L., Merck & Co, Inc.
Nie, H., Merck
Coelho, A., New Jersey Institute of Technology
Dalton, C., Merck
Dvorak, H., University of Kentucky
Elkhabaz, A., Merck & Co, Inc.
Fahy, M., Merck & Co, Inc.
Ormes, J. D., Merck & Co., Inc.
Parker, A. S., Purdue University
Punia, A., Merck & Co, Inc.
Rowe, J., Bristol-Myers Squibb
Smith, D., Merck & Co, Inc.
Stroman, N. A., Merck & Co, Inc.
Wang, M., Merck & Co, Inc.
Wareham, L., Merck Sharp & Dohme Corp.
Amorphous solid dispersions (ASDs) are an attractive option to improve the bioavailability of poorly water-soluble compounds. However, the material attributes of ASDs can present formulation and processability challenges, which are often mitigated by the addition of excipients albeit at the expense of tablet size. In this work, a continuous ASD manufacturing train combining co-precipitation and thin film evaporation (TFE) was used to generate high bulk-density co-precipitated amorphous dispersion (cPAD). The cPAD/TFE material was directly compressed into tablets at amorphous solid dispersion loadings up to 89 wt%, representing a greater than 60% reduction in tablet size relative to formulated tablets containing spray dried intermediate (SDI). This high ASD loading was possible due to densification of the amorphous dispersion during drying by TFE. Pharmacokinetic performance of the TFE-isolated, co-precipitated dispersion was shown to be equivalent to an SDI formulation. These data highlight the downstream advantages of this novel ASD manufacturing pathway to facilitate reduced tablet size via high ASD loading in directly compressed tablets.