Michelle R. Duncan, Joanne M. Lee, Mark P. Warchol
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引用次数: 87
Abstract
This paper explores the use of surfactants as a pharmaceutical excipient to reduce adsorptive losses of protein/peptide drugs. The predominant adsorption mechanism for protein/peptide drugs is shown to change with the surface and conditions of study. In the presence of surfactants, where the surfactant-surface interaction is greater than the surface-protein/peptide interaction, drug adsorption is reduced and/or eliminated. Anionic (sodium dodecyl sulfate), cationic (dodecyltrimethylammonium chloride and benzalkonium chloride) and nonionic surfactants (Polysorbate 20 and Poloxamer 188) are evaluated as possible protein/peptide adsorption controlling excipients. For protein/peptide adsorption onto glass, where an electrostatic interaction predominates, only the most hydrophobic surfactants (Polysorbate 20 and benzalkonium chloride) were significantly effective. Protein/peptide adsorption to polypropylene, where a hydrophobic/dehydration mechanism predominates, allows additional surface-active agents to be effective in reducing drug adsorption.
期刊介绍:
The International Journal of Pharmaceutics is the third most cited journal in the "Pharmacy & Pharmacology" category out of 366 journals, being the true home for pharmaceutical scientists concerned with the physical, chemical and biological properties of devices and delivery systems for drugs, vaccines and biologicals, including their design, manufacture and evaluation. This includes evaluation of the properties of drugs, excipients such as surfactants and polymers and novel materials. The journal has special sections on pharmaceutical nanotechnology and personalized medicines, and publishes research papers, reviews, commentaries and letters to the editor as well as special issues.
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