| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 4752411 | Biomaterials | 2017 | 15 Pages |
â¢Thrombolytic therapies use I.V.-administration of plasminogen activating drugs.â¢Off-target action of thrombolytic drugs can cause significant hemorrhagic risks.â¢Clot-targeted delivery of drugs can increase thrombolytic efficacy and reduce risks.â¢Platelet microparticles (PMPs) inspire design of clot-targeted drug delivery system.â¢PMP-inspired nanovesicles (PMINs) render targeted thrombolysis with systemic safety.
Intravascular administration of plasminogen activators is a clinically important thrombolytic strategy to treat occlusive vascular conditions. A major issue with this strategy is the systemic off-target drug action, which affects hemostatic capabilities and causes substantial hemorrhagic risks. This issue can be potentially resolved by designing technologies that allow thrombus-targeted delivery and site-specific action of thrombolytic drugs. To this end, leveraging a liposomal platform, we have developed platelet microparticle (PMP)-inspired nanovesicles (PMINs), that can protect encapsulated thrombolytic drugs in circulation to prevent off-target uptake and action, anchor actively onto thrombus via PMP-relevant molecular mechanisms and allow drug release via thrombus-relevant enzymatic trigger. Specifically, the PMINs can anchor onto thrombus via heteromultivalent ligand-mediated binding to active platelet integrin GPIIb-IIIa and P-selectin, and release the thrombolytic payload due to vesicle destabilization triggered by clot-relevant enzyme phospholipase-A2. Here we report on the evaluation of clot-targeting efficacy, lipase-triggered drug release and resultant thrombolytic capability of the PMINs in vitro, and subsequently demonstrate that intravenous delivery of thrombolytic-loaded PMINs can render targeted fibrinolysis without affecting systemic hemostasis, in vivo, in a carotid artery thrombosis model in mice. Our studies establish significant promise of the PMIN technology for safe and site-targeted nanomedicine therapies in the vascular compartment.
Graphical abstractDownload high-res image (348KB)Download full-size image
