Platelet-mimicking procoagulant nanoparticles augment hemostasis in animal models of bleeding

血小板 磷脂酰丝氨酸 止血 纤维蛋白 体内 凝结 凝血酶 医学 血小板活化 免疫学 化学 生物 磷脂 外科 生物化学 内科学 生物技术
作者
Ujjal D. S. Sekhon,Kelsey L. Swingle,Aditya Girish,Norman Luc,de la Fuente M,Jurgis Alvikas,Shannon Haldeman,Adnan Hassoune,Kaisal Shah,Youjoung Kim,Steven J. Eppell,Jeffrey R. Capadona,Andrew J. Shoffstall,Matthew D. Neal,Wei Li,Marvin T. Nieman,Anirban Sen Gupta
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science (AAAS)]
卷期号:14 (629) 被引量:44
标识
DOI:10.1126/scitranslmed.abb8975
摘要

Treatment of bleeding disorders using transfusion of donor-derived platelets faces logistical challenges due to their limited availability, high risk of contamination, and short (5 to 7 days) shelf life. These challenges could be potentially addressed by designing platelet mimetics that emulate the adhesion, aggregation, and procoagulant functions of platelets. To this end, we created liposome-based platelet-mimicking procoagulant nanoparticles (PPNs) that can expose the phospholipid phosphatidylserine on their surface in response to plasmin. First, we tested PPNs in vitro using human plasma and demonstrated plasmin-triggered exposure of phosphatidylserine and the resultant assembly of coagulation factors on the PPN surface. We also showed that this phosphatidylserine exposed on the PPN surface could restore and enhance thrombin generation and fibrin formation in human plasma depleted of platelets. In human plasma and whole blood in vitro, PPNs improved fibrin stability and clot robustness in a fibrinolytic environment. We then tested PPNs in vivo in a mouse model of thrombocytopenia where treatment with PPNs reduced blood loss in a manner comparable to treatment with syngeneic platelets. Furthermore, in rat and mouse models of traumatic hemorrhage, treatment with PPNs substantially reduced bleeding and improved survival. No sign of systemic or off-target thrombotic risks was observed in the animal studies. These findings demonstrate the potential of PPNs as a platelet surrogate that should be further investigated for the management of bleeding.
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