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Solubility and dissolution enhancement strategies: current understanding and recent trends

Journal

DRUG DEVELOPMENT AND INDUSTRIAL PHARMACY
Volume 41, Issue 6, Pages 875-887

Publisher

TAYLOR & FRANCIS LTD
DOI: 10.3109/03639045.2014.971027

Keywords

Amorphous solid dispersion; bioavailability; dissolution rate; formulation strategies; particle size reduction; poor solubility; salts

Funding

  1. St. John's University

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Identification of lead compounds with higher molecular weight and lower aqueous solubility has become increasingly prevalent with the advent of high throughput screening. Poor aqueous solubility of these lipophilic compounds can drastically affect the dissolution rate and subsequently the drug absorbed in the systemic circulation, imposing a significant burden of time and money during drug development process. Various pre-formulation and formulation strategies have been applied in the past that can improve the aqueous solubility of lipophilic compounds by manipulating either the crystal lattice properties or the activity coefficient of a solute in solution or both, if possible. However, despite various strategies available in the armor of formulation scientist, solubility issue still remains an overriding problem in the drug development process. It is perhaps due to the insufficient conceptual understanding of solubility and dissolution phenomenon that hinders the judgment in selecting suitable strategy for improving aqueous solubility and/or dissolution rate. This article, therefore, focuses on (i) revisiting the theoretical and mathematical concepts associated with solubility and dissolution, (ii) their application in making rationale decision for selecting suitable pre-formulation and formulation strategies and (iii) the relevant research performed in this field in past decade.

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