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凝血酶特异性抑制剂阿加曲班对纤维蛋白凝块相关凝血酶激活血小板的抑制作用。

Inhibition by Argatroban, a specific thrombin inhibitor, of platelet activation by fibrin clot-associated thrombin.

作者信息

Lunven C, Gauffeny C, Lecoffre C, O'Brien D P, Roome N O, Berry C N

机构信息

Cardiovascular Dept., Blood and Vessel Pharmacology Group, Bagneux, France.

出版信息

Thromb Haemost. 1996 Jan;75(1):154-60.

PMID:8713795
Abstract

Clot-associated thrombin retains amidolytic activity, and is resistant to inhibition by heparin, but not to low molecular weight thrombin inhibitors. We show that clot-associated thrombin induces platelet aggregation, is resistant to heparin:antithrombin III, less so to recombinant hirudin (rHV2Lys47) but not to argatroban, an active-site directed thrombin inhibitor. Fibrin clots prepared with human fibrinogen and thrombin were used to aggregate rabbit washed platelets assessed by single platelet counting, thromboxane B2 (TXB2) immunoassay and scanning electron microscopy. Fibrin clots decreased platelet counts, and released TXB2. Electron microscopy showed platelet aggregates on the clot surface. Argatroban concentration-dependently inhibited such aggregation with IC50s of 21 nM and 13 nM versus aggregation and TXB2 release respectively. The IC50s of Argatroban against fluid-phase thrombin producing similar aggregation were 12 nM (aggregation) and 33 nM (TXB2). rHV2Lys47 was less active against clot-induced aggregation (IC50 = 1.8 nM) than against fluid-phase thrombin (IC50 = 0.06 nM). Heparin had an IC50 of 0.02 mU/ml against aggregation induced by fluid-phase thrombin, but much greater concentrations are required to inhibit clot-induced aggregation (IC50 = 48 mU/ml). These data provide a basis for the superiority of direct-acting thrombin inhibitors over heparin in platelet rich thrombi.

摘要

与凝块相关的凝血酶保留酰胺水解活性,对肝素抑制具有抗性,但对低分子量凝血酶抑制剂敏感。我们发现,与凝块相关的凝血酶可诱导血小板聚集,对肝素-抗凝血酶III具有抗性,对重组水蛭素(rHV2Lys47)的抗性较小,但对活性位点导向的凝血酶抑制剂阿加曲班敏感。用人纤维蛋白原和凝血酶制备的纤维蛋白凝块用于聚集兔洗涤血小板,通过单血小板计数、血栓素B2(TXB2)免疫测定和扫描电子显微镜进行评估。纤维蛋白凝块可降低血小板计数,并释放TXB2。电子显微镜显示凝块表面有血小板聚集物。阿加曲班浓度依赖性地抑制这种聚集,对聚集和TXB2释放的IC50分别为21 nM和13 nM。阿加曲班对产生类似聚集的液相凝血酶的IC50分别为12 nM(聚集)和33 nM(TXB2)。rHV2Lys47对凝块诱导的聚集(IC50 = 1.8 nM)的活性低于对液相凝血酶(IC50 = 0.06 nM)的活性。肝素对液相凝血酶诱导的聚集的IC50为0.02 mU/ml,但抑制凝块诱导的聚集需要更高的浓度(IC50 = 48 mU/ml)。这些数据为直接作用的凝血酶抑制剂在富含血小板血栓中优于肝素提供了依据。

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