Alpha 2.0
Login Register
» Articles » PMID: 26175316

Amorphous Solid Dispersions: Utilization and Challenges in Drug Discovery and Development

Overview
Journal J Pharm Sci
Publisher Elsevier
Specialties Pharmacology
Pharmacy
Date 2015 Jul 16
PMID 26175316
Citations 50
Authors
Yan He
Chris Ho
Affiliations
Soon will be listed here.
Abstract

Amorphous solid dispersion (ASD) can accelerate a project by improving dissolution rate and solubility, offering dose escalation flexibility and excipient acceptance for toxicology studies, as well as providing adequate preclinical and clinical exposure. The prerequisite physicochemical properties for a compound to form a stable ASD are glass-forming ability and low-crystallization tendency, which can be assessed using computational tools and experimental methods. Polymer excipient screening by in silico miscibility prediction and experimental screening techniques is discussed. Improved technologies for polymer screening with minimal quantity of drug substance, and the scalability of ASD from bench to commercial are reviewed. Considerations of in vitro evaluations, preclinical animal selection, and the translation of the preclinical results to clinical studies are also discussed. Better understanding of how polymers improve the stability of the amorphous phase in the solid state and how ASD improves bioavailability have facilitated the applications of ASD ranging from discovery research to preclinical development and further to commercialization. With the understanding of how ASDs are currently used in the pharmaceutical industry and what challenges remain to be solved, ASD can be applied to solve drug formulation problems at given research and development stages.

Citing Articles

Towards Enhanced Solubility of Cannabidiol: Preparation and Evaluation of Cannabidiol Solid Dispersions Using Vacuum Compression Molding.

Cherif A, Deshmukh J, Sanil K, Taha I, Treffer D, Ashour E AAPS PharmSciTech. 2025; 26(3):83.

PMID: 40069513 DOI: 10.1208/s12249-025-03078-8.

Advancing the Physicochemical Properties and Therapeutic Potential of Plant Extracts Through Amorphous Solid Dispersion Systems.

Budiman A, Hafidz N, Azzahra R, Amaliah S, Sitinjak F, Rusdin A Polymers (Basel). 2025; 16(24.

PMID: 39771340 PMC: 11679451. DOI: 10.3390/polym16243489.

Improve Solubility and Develop Personalized Itraconazole Dosages via Forming Amorphous Solid Dispersions with Hydrophilic Polymers Utilizing HME and 3D Printing Technologies.

Huang L, Guo J, Li Y, Yang W, Ni W, Jia Y Polymers (Basel). 2024; 16(23).

PMID: 39684047 PMC: 11644310. DOI: 10.3390/polym16233302.

Impact of Hot-Melt Extrusion on Glibenclamide's Physical and Chemical States and Dissolution Behavior: Case Studies with Three Polymer Blend Matrices.

Zupan N, Yous I, Danede F, Verin J, Kouach M, Foulon C Pharmaceutics. 2024; 16(8).

PMID: 39204416 PMC: 11360095. DOI: 10.3390/pharmaceutics16081071.

From formulation to structure: 3D electron diffraction for the structure solution of a new indomethacin polymorph from an amorphous solid dispersion.

Leung H, Copley R, Lampronti G, Day S, Saunders L, Johnstone D IUCrJ. 2024; 11(Pt 5):744-748.

PMID: 39194259 PMC: 11364028. DOI: 10.1107/S2052252524008121.