For
atherosclerosis (AS) management, a therapeutic drug intervention
is the most widely used strategy. However, there are some problems
such as low location specificity, high intake, and side effects. Nanomedicine
can prolong the half-life of drug solubilization, reduce toxic and
side effects, and improve the distribution of drug objects. Herein,
to overcome the challenges, an erythrocyte-based “plug and
play” nanoplatform was developed by incorporating the vascular
cell adhesion molecule-1 (VCAM-1) targeting and the acid stimulus
responsibility. After the function moieties conjugated with DSPE-PEG,
the targeting peptide and the acid-sensitive prodrug were conveniently
integrated into red blood cells’ surface for enhancing target
AS drug delivery and controlling local drug release. As a proof of
principle, a plug and play nanoplatform with targeted drug delivery
and acid-control drug release is demonstrated, achieving a marked
therapeutic effect for AS.
Nanomedicines represent the new promise strategies for treating atherosclerosis (AS). Because they enhance drug bioavailability and have lower side effects. Nevertheless, nanomedicines have several challenges with these advantages, including a...
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