未分离肝素、低分子量肝素及两者联合释放总组织因子和游离组织因子途径抑制剂的疗效。

Haemostasis Pub Date : 1998-09-01 DOI:10.1159/000022436
R Altman, A Scazziota, J Rouvier
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引用次数: 24

摘要

未分级肝素(UFH)通过抗凝血酶III增加凝血酶和激活因子X的失活来发挥其抗凝血特性。除此之外,内皮细胞释放的组织因子途径抑制剂(TFPI)对肝素的抗血栓活性也很重要。5名健康志愿者皮下注射4种不同的肝素制剂,间隔1周:(1)UFH 2500 IU固定剂量(FixUFH),(2)低分子肝素(LMWH) 1 mg/kg体重,(3)LMWH调整剂量加UFH 2500 IU固定剂量(ComHep)和(4)UFH 2500 IU/10 kg体重(UFHvar)。分别于术前、术后1、2、4、6、12、24 h抽取血浆。FixUFH不影响总TFPI和游离TFPI的浓度。低分子肝素注射后1 h总TFPI由74 ~ 124 ng/ml升高(p < 0.01), ComHep注射后1 h总TFPI由82 ~ 144 ng/ml升高(p < 0.01), UFHvar注射后1 h总TFPI由91 ~ 113 ng/ml升高(p < 0.05)。与基线相比,所有观测值在峰值处均显著升高(+/- 2 h, p < 0.01)。在2和4 h, UFHvar产生的游离TFPI(74.5和70.5 ng/ml)显著高于低分子肝素(42.8和38.0 ng/ml) (p < 0.001和p < 0.01)。与FixUFH相比,UFHvar和ComHep在2、4和6 h时使游离TFPI升高,但LMWH无统计学意义(p < 0.05)。01). 我们得出结论,在相当的治疗剂量下,皮下UFHvar释放的游离TFPI比低分子肝素和ComHep更多。在4、6和12小时的血液样本中发现低分子肝素和低剂量UFH之间的协同作用。
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Efficacy of unfractionated heparin, low molecular weight heparin and both combined for releasing total and free tissue factor pathway inhibitor.

Unfractionated heparin (UFH) exerts its anticoagulant properties by increasing the inactivation of thrombin and activated factor X by antithrombin III. Apart from this main action release of tissue factor pathway inhibitor (TFPI) from endothelial cells could also be important for the antithrombotic activity of heparins. Four different heparin preparations were injected subcutaneously into 5 healthy volunteers 1 week apart: (1) UFH 2,500 IU fix dose (FixUFH), (2) 1 mg/kg body weight of low molecular weight heparin (LMWH), (3) the combined LMWH-adjusted dose plus UFH 2,500 IU fix dose (ComHep) and (4) UFH 2,500 IU/10 kg body weight (UFHvar). Plasma samples were drawn before and 1, 2, 4, 6, 12 and 24 h afterwards. FixUFH did not affect the concentration of total and free TFPI. Total TFPI increased in the 1st hour after LMWH injection from 74 to 124 ng/ml (p < 0.01), after ComHep from 82 to 144 ng/ml (p < 0.01), and after UFHvar from 91 to 113 ng/ml (p < 0.05). All observed elevations were significant at the peak value (+/- 2 h, p < 0.01 compared with baselines). The increase of free TFPI produced by UFHvar (74.5 and 70.5 ng/ml) was significantly higher than with LMWH (42.8 and 38.0 ng/ml) at 2 and 4 h (p < 0.001 and p < 0.01, respectively). UFHvar and ComHep but not LMWH produced a statistically significant increase of free TFPI compared with FixUFH at 2, 4 and 6 h (p < 0. 01). We concluded that at comparable therapeutic doses, subcutaneous UFHvar released more free TFPI than LMWH and ComHep. A synergism between LMWH and low dose of UFH was found in 4-, 6- and 12-hour blood samples.

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