4.7 Article

Modulation of Gastrointestinal Mucus Properties with Ionic Liquids for Drug Delivery

Journal

ADVANCED HEALTHCARE MATERIALS
Volume 10, Issue 13, Pages -

Publisher

WILEY
DOI: 10.1002/adhm.202002192

Keywords

diffusion; ionic liquids; mucosal; mucus; viscosity

Funding

  1. School of Engineering and Applied Sciences at the Harvard University

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Studies have shown that choline-based ionic liquids can significantly enhance the absorption of macromolecular drugs in the gastrointestinal tract by reducing drug interactions with mucus or disrupting the mucus layer, potentially improving the success rate of oral drug delivery.
The mucus barrier lining the gastrointestinal tract poses a significant barrier to the oral delivery of macromolecular drugs. Successful approaches to overcoming this barrier have primarily focused on reducing drug and carrier interactions with mucus or disrupting the mucus layer directly. Choline-based ionic liquids (ILs) such as choline geranate and choline glycolate (CGLY) have recently been shown to be effective in enhancing the intestinal absorption of macromolecules such as insulin and immunoglobulin (IgG), respectively. Herein, the use of choline-based ILs as mucus-modulating agents for safely improving drug penetration through mucus is described. Choline-based ILs significantly increase the diffusion rates of cationic dextrans through mucin solution. Choline-maleic acid (CMLC 2:1) enhances the diffusion of 4 kDa cationic dextran in mucin solution by more than fourfold when compared to phosphate-buffered saline control. Choline-based ILs also reduce mucus viscosity without significantly impacting the native mucus gel structure. In vitro studies in a mucus-secreting coculture model with Caco-2 and HT29MTX-E12 cells further demonstrate the effectiveness of ILs in improving transport of cationic molecules in the presence of secreted mucus. This work demonstrates the potential for choline-based ionic liquids to be used as nondestructive mucus-modulating agents for enabling enhanced oral delivery of macromolecular drugs.

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