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Thrombosomes: a platelet‐derived hemostatic agent for control of noncompressible hemorrhage

血栓弹性成像 止血剂 血小板 止血 人口 医学 凝血酶 凝结 药理学 免疫原性 不利影响 化学 免疫学 内科学 抗原 环境卫生
作者
G. Michael Fitzpatrick,Richard O. Cliff,Narendra N. Tandon
出处
期刊:Transfusion [Wiley]
卷期号:53 (S1) 被引量:56
标识
DOI:10.1111/trf.12043
摘要

Background Uncontrolled hemorrhage is responsible for ∼80% of the potentially survivable deaths in combat and over 40% of early mortality in the under 65 age group in the United States. Providing an easily used infusible hemostatic agent to first responders could significantly reduce these fatalities. We report on an infusible lyophilized platelet‐derived hemostatic agent stabilized with trehalose and polysucrose prior to and during lyophilization. Study Design and Methods Characterization included determining the particle population size range, surface marker expression GPIb, GPIIbIIIa, and Annexin V binding. Function was assessed by aggregation, thromboelastography, and thrombin generation. Pharmacokinetics, biodistribution, and immunogenicity established using Indium 111 labeled Thrombosomes in healthy N ew Z ealand white rabbits ( NZWRs ), efficacy in thrombocytopenic NZWR , and safety in NZWRs , canines, and nonhuman primates. Results Thrombosomes retained GPIIbIIIa expression (98.71% ± 0.18 of the rehydrated particles), a reduced expression of GPIb (47.77% ± 6.65), and Annexin V binding (86.05% ± 2.65). Aggregation to all agonists except thrombin in buffer (78.15% ± 2.5) was <50%. Thrombin generation and thromboelastography results demonstrated a concentration gradient that was consistent from lot to lot. There were no observed adverse events in any safety study and blood loss was reduced by >80% in the thrombocytopenic ear bleed model. Conclusion Our in vitro characterization studies in conjunction with preclinical animal safety and efficacy studies demonstrated lot consistency in manufacturing, maintenance of hemostatic functions of Thrombosomes, safety at high dose concentrations, and the potential to provide an effective hemostatic agent at the site of injury.
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