与依诺肝素和血管性血友病因子抑制剂相比,P-选择素抑制在治疗上更能促进血栓溶解,并更好地预防静脉壁纤维化。
P-selectin inhibition therapeutically promotes thrombus resolution and prevents vein wall fibrosis better than enoxaparin and an inhibitor to von Willebrand factor.
作者信息
Diaz Jose A, Wrobleski Shirley K, Alvarado Christine M, Hawley Angela E, Doornbos Nichole K, Lester Patrick A, Lowe Suzan E, Gabriel Joy E, Roelofs Karen J, Henke Peter K, Schaub Robert G, Wakefield Thomas W, Myers Daniel D
机构信息
From the Section of Vascular Surgery, Department of Surgery, Conrad Jobst Vascular Research Laboratories (J.A.D., S.K.W., C.M.A., A.E.H., N.K.D., J.E.G., K.J.R., P.K.H., T.W.W., D.D.M.), Unit for Laboratory Animal Medicine (C.M.A., P.A.L., D.D.M.), and Department of Radiology (S.E.L.), University of Michigan, Ann Arbor; and Research and Development, Archemix Corporation, Cambridge, MA (R.G.S.).
出版信息
Arterioscler Thromb Vasc Biol. 2015 Apr;35(4):829-37. doi: 10.1161/ATVBAHA.114.304457. Epub 2015 Feb 5.
OBJECTIVE
Aptamers are oligonucleotides targeting protein-protein interactions with pharmacokinetic profiles and activity reversal options. Although P-selectin and von Willebrand factor (vWF) have been implicated in the development of venous thrombosis (VT), no studies have directly compared aptamer efficacy with standard of care in VT. In this study, ARC5692, an anti-P-selectin aptamer, and ARC15105, an anti-vWF aptamer, were compared with low-molecular-weight heparin, enoxaparin, to test the efficacy of P-selectin or vWF inhibition in promoting thrombus resolution and preventing vein wall fibrosis, in a baboon model of VT.
APPROACH AND RESULTS
Groups were as follows: treatment arm: animals received P-selectin or vWF aptamer inhibitors or enoxaparin (n=3 per group). Controls received no treatment (n=3). Prophylactic arm: animals received P-selectin inhibitor (n=4) or vWF inhibitor (n=3). Treatment arm: P-selectin-inhibitor demonstrated a significant improvement in vein recanalization by magnetic resonance venography (73% at day 21), and significantly decreased vein wall collagen, compared with all groups. Anti-P-selectin equaled enoxaparin in maintaining valve competency by ultrasound. All control animals had compromised valve competency post thrombosis. Prophylactic arm: animals receiving P-selectin and vWF inhibitors demonstrated improved vein recanalization by magnetic resonance venography versus controls (80% and 85%, respectively, at day 21). Anti-P-selectin protected iliac valve function better than anti-vWF, and both improved valve function versus controls. No adverse bleeding events were observed.
CONCLUSIONS
The P-selectin inhibitor aptamer promoted iliac vein recanalization, preserved valve competency, and decreased vein wall fibrosis. The results of this work suggest that P-selectin inhibition maybe an ideal target in the treatment and prophylaxis of deep VT, warranting clinical trials.
目的
适体是靶向蛋白质 - 蛋白质相互作用的寡核苷酸,具有药代动力学特征和活性逆转选项。尽管P - 选择素和血管性血友病因子(vWF)与静脉血栓形成(VT)的发生有关,但尚无研究直接比较适体在VT中的疗效与标准治疗方法。在本研究中,将抗P - 选择素适体ARC5692和抗vWF适体ARC15105与低分子量肝素依诺肝素进行比较,以在狒狒VT模型中测试抑制P - 选择素或vWF在促进血栓溶解和预防静脉壁纤维化方面的疗效。
方法与结果
分组如下:治疗组:动物接受P - 选择素或vWF适体抑制剂或依诺肝素(每组n = 3)。对照组不接受治疗(n = 3)。预防组:动物接受P - 选择素抑制剂(n = 4)或vWF抑制剂(n = 3)。治疗组:与所有组相比,P - 选择素抑制剂通过磁共振静脉造影显示静脉再通有显著改善(第21天为73%),且静脉壁胶原蛋白显著减少。抗P - 选择素在通过超声维持瓣膜功能方面与依诺肝素相当。所有对照动物在血栓形成后瓣膜功能均受损。预防组:接受P - 选择素和vWF抑制剂的动物通过磁共振静脉造影显示静脉再通较对照组有所改善(第21天分别为80%和85%)。抗P - 选择素比抗vWF更好地保护了髂静脉瓣膜功能,且两者均比对照组改善了瓣膜功能。未观察到不良出血事件。
结论
P - 选择素抑制剂适体促进了髂静脉再通,保留了瓣膜功能,并减少了静脉壁纤维化。这项工作的结果表明,抑制P - 选择素可能是治疗和预防深部VT的理想靶点,值得进行临床试验。
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