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Understanding lymphatic drug delivery through chylomicron blockade: A retrospective and prospective analysis.

Authors :
Yousef, Malaz
Bou-Chacra, Nadia
Löbenberg, Raimar
Davies, Neal M.
Source :
Journal of Pharmacological & Toxicological Methods. Sep2024, Vol. 129, pN.PAG-N.PAG. 1p.
Publication Year :
2024

Abstract

Scientists have developed and employed various models to investigate intestinal lymphatic uptake. One approach involves using specific blocking agents to influence the chylomicron-mediated lymphatic absorption of drugs. Currently utilized models include pluronic L-81, puromycin, vinca alkaloids, colchicine, and cycloheximide. This review offers a thorough analysis of the diverse models utilized, evaluating existing reports while delineating the gaps in current research. It also explores pharmacokinetic related aspects of intestinal lymphatic uptake pathway and its blockage through the discussed models. Pluronic L-81 has a reversible effect, minimal toxicity, and unique mode of action. Yet, it lacks clinical reports on chylomicron pathway blockage, likely due to low concentrations used. Puromycin and vinca alkaloids, though documented for toxicity, lack information on their application in drug intestinal lymphatic uptake. Other vinca alkaloids show promise in affecting triglyceride profiles and represent possible agents to test as blockers. Colchicine and cycloheximide, widely used in pharmaceutical development, have demonstrated efficacy, with cycloheximide preferred for lower toxicity. However, further investigation into effective and toxic doses of colchicine in humans is needed to understand its clinical impact. The review additionally followed the complete journey of oral lymphatic targeting drugs from intake to excretion, provided a pharmacokinetic equation considering the intestinal lymphatic pathway for assessing bioavailability. Moreover, the possible application of urinary data as a non-invasive way to measure the uptake of drugs through intestinal lymphatics was illustrated, and the likelihood of drug interactions when specific blockers are employed in human subjects was underscored. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
10568719
Volume :
129
Database :
Academic Search Index
Journal :
Journal of Pharmacological & Toxicological Methods
Publication Type :
Academic Journal
Accession number :
179709093
Full Text :
https://doi.org/10.1016/j.vascn.2024.107548