在动脉血流条件下,组织因子诱导的凝血触发血小板血栓形成的效率与纤维性胶原蛋白相同。

U Orvim, H E Roald, R W Stephens, N Roos, K S Sakariassen
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引用次数: 51

摘要

血管壁组织因子(TF)在启动血栓形成中的相对重要性尚不明确。相比之下,血管壁胶原已被充分证明是血栓形成的有效诱导剂。我们比较了人TF/磷脂表面与由人III型胶原纤维组成的表面在静脉和动脉血流条件下触发天然血液血栓形成的效力。一种商业制剂,Thromborel S,被用作人TF的来源。该制剂的生化表征显示少量的FVII, FIX和FX蛋白。这些蛋白的凝血活性仅与FVII蛋白相关,尽管其活性非常低。在单阶段凝血试验中使用抗TF抗体的研究表明,血栓的促凝活性主要是TF的结果。TF与磷脂的摩尔比为1:2 × 10(7)。在平行板灌注室装置中,在Thermanox盖上涂覆的Thromborel S或胶原原纤维可以触发从膝前静脉直接抽取的流动的非抗凝人血液中的血栓形成。在100 S -1的壁剪切速率下,1:50的血小板相关性S稀释得到最大的纤维蛋白沉积(90%的表面覆盖率)。然而,用单克隆抗TF抗体预处理TF表面可使纤维蛋白沉积减少93% (P < 0.001)。因此,在该血流系统中,TF对于血栓S表面的促凝活性也是必不可少的。在较高的壁剪切速率下(650和2600s-1),纤维蛋白沉积较少,但纤维蛋白网上血小板血栓形成明显增加。(摘要删节250字)
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Tissue factor-induced coagulation triggers platelet thrombus formation as efficiently as fibrillar collagen at arterial blood flow conditions.

The relative importance of vessel wall tissue factor (TF) in initiating thrombogenesis is not well defined. In contrast, vessel wall collagens have been well documented as potent inducers of thrombus formation. We compared the potency of a human TF/phospholipid surface with that of a surface consisting of human type III collagen fibrils in triggering thrombus formation in native human blood at venous and arterial blood flow conditions. A commercial preparation, Thromborel S, was used as a source of human TF. Biochemical characterization of this preparation revealed small amounts of FVII, FIX, and FX proteins. Coagulant activity of these proteins was associated with the FVII protein only, although it was a very low activity. Studies with anti-TF antibodies in a one-stage clotting assay showed that the procoagulant activity of Thromborel was mainly a result of TF. The molar ratio of TF to phospholipid was 1:2 x 10(7). Thrombus formation in flowing nonanticoagulated human blood drawn directly from an antecubital vein was triggered by either Thromborel S or collagen fibrils coated on Thermanox coverslips in a parallel-plate perfusion chamber device. A 1:50 Thromborel S dilution gave maximal fibrin deposition (90% surface coverage) at a wall shear rate of 100 s-1. However, pretreatment of the TF surface with a monoclonal anti-TF antibody reduced this fibrin deposition by 93% (P < .001). Thus, TF was essential for the procoagulant activity of the Thromborel S surface in this flow system also. At higher wall shear rates (650 and 2600s-1), less fibrin was deposited, but the platelet thrombus formation on the fibrin mesh increased dramatically.(ABSTRACT TRUNCATED AT 250 WORDS)

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