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Synthetic high-density lipoproteins loaded with an antiplatelet drug for efficient inhibition of thrombosis in mice

机译:含有抗血小板药物的合成高密度脂蛋白,用于有效抑制小鼠血栓形成的血栓形成

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Antiplatelet agents offer a desirable approach to thrombosis prevention through the reduction of platelet reactivity. However, major bleeding events greatly attenuate the clinical outcomes of most antithrombotic agents. Therefore, the development of safer and more effective strategies to prevent vascular occlusion and avoid bleeding is urgently needed. A reconstituted nanoparticle, synthetic high-density lipoprotein (sHDL), which mimics the native HDL, has been established as clinically safe and is easily manufactured on a large scale. In this study, we propose that the delivery of the antiplatelet drug ML355, a selective inhibitor of 12(S)-lipoxygenase (12-LOX), by sHDL will efficiently inhibit thrombosis by targeting ML355 to the intended site of action, improving the pharmaceutical profile and harnessing the innate antithrombotic efficacy of the sHDL carrier. Our data show that ML355-sHDL exhibits more potent inhibition of thrombus formation in both small arterioles and larger arteries in mice without impairing the normal hemostasis in vivo.
机译:抗血小板剂通过降低血小板反应性提供了血栓形成预防的理想方法。然而,主要出血事件大大衰减了大多数抗血栓形成剂的临床结果。因此,迫切需要发展更安全,更有效的策略,以防止血管闭塞和避免出血。重构的纳米粒子,用于模仿天然HDL的合成高密度脂蛋白(SHDL),已经在临床安全地建立,并且易于大规模制造。在该研究中,通过SHDL提出抗血小板药物ML355的递送12(S)-LIPOxygenase(12-LOX)的选择性抑制剂,通过靶向ML355至预定的作用部位,改善药物,有效地抑制血栓形成,改善药物轮廓并利用SHDL载体的先天抗血栓形成效果。我们的数据表明,ML355-SHDL在小鼠中表现出更有效的血栓形成血栓形成,而不会损害体内正常的止血。

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