Preparation and characterization of BSA-loaded liraglutide and platelet fragment nanoparticle delivery system for the treatment of diabetic atherosclerosis.

J Nanobiotechnology · 2024

Last updated 2026-05-28

Researchers created a nanoparticle delivery system (BSA@LIR-PMF) to improve the effectiveness of liraglutide, a GLP-1 drug, for treating diabetic atherosclerosis. The nanoparticles had a drug loading rate of 7.96% and released about 77.06% of the drug within 24 hours. In lab and animal tests, the system reduced harmful cell activity linked to atherosclerosis and improved energy production in cells.

AI summary of the abstract below.

Journal	J Nanobiotechnology, 2024
Citations	7
Relative citation ratio	1.50
NIH percentile	64
Molecules	liraglutide
Conditions studied	Type 2 Diabetes, Cardiovascular Risk Reduction

Abstract

BACKGROUND: Diabetic atherosclerosis is one of the main causes of morbidity and mortality worldwide, but its therapeutic options are limited. Liraglutide (LIR), a synthetic analog of GLP-1 approved as an anti-obesity drug by the FDA, has been reported as a promising drug for diabetic atherosclerosis. However, the main problem with LIR is its use that requires regular parenteral injections, which necessitates the improvement of drug delivery for increased efficiency and minimization of injection numbers.

RESULTS: The objective of our present study was to prepare and characterize nanoparticles (BSA@LIR-PMF) for targeted drug delivery using LIR-encapsulated platelet membrane fragments (PMF) coated bovine serum albumin (BSA). We used various methods to characterize the prepared nanoparticles and evaluated their efficiency on diabetes-induced atherosclerosis in vitro and in vivo. The results showed that the nanoparticles were spherical and had good stability and uniform size with intact membrane protein structure. The loading and encapsulation rates (LR and ER) of BSA@LIR-PMF were respectively 7.96% and 85.56%, while the cumulative release rate was around 77.06% after 24 h. Besides, we also examined the impact of BSA@LIR-PMF on the proliferation, migration, phagocytosis, reactive oxygen species (ROS) levels, oxidative phosphorylation, glycolysis, lactate and ATP levels, and lipid deposition in the aortas. The results indicated that BSA@LIR-PMF could effectively inhibit ox-LDL-stimulated abnormal cell proliferation and migration, reduce the level of ROS and lactate concentration, and enhance the level of ATP, thereby improving oxidative phosphorylation in ox-LDL-treated cells.

CONCLUSION: BSA@LIR-PMF significantly inhibited diabetes-induced atherosclerosis. It was anticipated that the BSA@LIR-PMF nanoparticles might be used for treating diabetes-associated cardiovascular complications.

Verbatim abstract via PubMed 39180102 ↗

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