Haojie Chen
Delivery of imiquimod to intestinal lymph nodes following oral administration
Chen, Haojie; Ji, Liuhang; Wong, Abigail; Chu, Yenju; Feng, Wanshan; Zhu, Yufei; Wang, Junting; Comeo, Eleonora; Kim, Dong-Hyun; Stocks, Michael J.; Gershkovich, Pavel
Authors
Liuhang Ji
Abigail Wong
Yenju Chu
Wanshan Feng
Yufei Zhu
Junting Wang
Eleonora Comeo
DONG-HYUN KIM Dong-hyun.Kim@nottingham.ac.uk
Associate Professor
MICHAEL STOCKS MICHAEL.STOCKS@NOTTINGHAM.AC.UK
Professor of Medicinal Chemistry and Drug Discovery
PAVEL GERSHKOVICH PAVEL.GERSHKOVICH@NOTTINGHAM.AC.UK
Associate Professor
Abstract
Intestinal lymph nodes are involved in the progression of colorectal cancer (CRC). Tumours suppress the activation of dendritic cells (DCs) in draining lymph nodes, diminishing anti-cancer immune response. Imiquimod (IMQ) facilitates DCs activation via toll-like receptor 7, suggesting that targeted delivery of IMQ to intestinal lymph nodes can improve the treatment of CRC. This study aims to enhance the delivery of IMQ to intestinal lymph nodes by a highly lipophilic prodrug approach. Amide prodrugs were synthesised by conjugating IMQ with saturated and unsaturated medium- to long-chain fatty acids. Their potential for intestinal lymphatic transport was assessed by their affinity to chylomicrons and solubility in long-chain triglycerides. Further selection of prodrug candidates was determined by resistance to enzymatic hydrolysis in intestinal lumen and release of IMQ in the lymphatics using fasting state simulated intestinal fluid supplemented with esterases, brush border enzyme vesicles and plasma. Key pharmacokinetic parameters and biodistribution in rats were assessed for the most promising compounds, prodrugs 5 and 8. The plasma concentration–time profile of IMQ following oral administration of the prodrugs was less erratic in comparison to the administration of unmodified IMQ. The lymph-to-plasma ratios of IMQ concentration increased 1.9- and 1.7-fold using prodrugs 5 and 8 in comparison to administration of unmodified IMQ, respectively. Importantly, the average concentration of IMQ in mesenteric lymph nodes (MLN) was 11.2- and 7.6-fold higher than in plasma following the administration of prodrugs 5 and 8, respectively. Additionally, the non-specific wide distribution of IMQ into various organs and tissues was reduced with prodrugs. This work suggests that the highly lipophilic prodrug approach can efficiently deliver IMQ to intestinal lymphatics. In addition, this study demonstrates the feasibility of an amide prodrug approach for intestinal lymphatic targeting.
Citation
Chen, H., Ji, L., Wong, A., Chu, Y., Feng, W., Zhu, Y., Wang, J., Comeo, E., Kim, D.-H., Stocks, M. J., & Gershkovich, P. (2024). Delivery of imiquimod to intestinal lymph nodes following oral administration. International Journal of Pharmaceutics, 667, Article 124895. https://doi.org/10.1016/j.ijpharm.2024.124895
Journal Article Type | Article |
---|---|
Acceptance Date | Oct 29, 2024 |
Online Publication Date | Oct 31, 2024 |
Publication Date | Dec 25, 2024 |
Deposit Date | Oct 30, 2024 |
Publicly Available Date | Nov 1, 2025 |
Journal | International Journal of Pharmaceutics |
Print ISSN | 0378-5173 |
Electronic ISSN | 1873-3476 |
Publisher | Elsevier |
Peer Reviewed | Peer Reviewed |
Volume | 667 |
Article Number | 124895 |
DOI | https://doi.org/10.1016/j.ijpharm.2024.124895 |
Keywords | Colorectal cancer; Intestinal lymphatic targeting; Immune oncology; Toll-like receptors agonists; Imiquimod; Lymph nodes; Lipophilic prodrugs |
Public URL | https://nottingham-repository.worktribe.com/output/41141393 |
Publisher URL | https://www.sciencedirect.com/science/article/pii/S0378517324011293?via%3Dihub |
Files
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Licence
https://creativecommons.org/licenses/by/4.0/
Publisher Licence URL
https://creativecommons.org/licenses/by/4.0/
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