一种β - d -木糖苷,伊立帕尔,在预防大鼠溶栓后再血栓形成中的有益作用。

Haemostasis Pub Date : 1998-11-01 DOI:10.1159/000022448
P Chicaud, J R Rademakers, J Millet
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引用次数: 7

摘要

采用改良的Umetsu模型,研究了新型口服活性β - d -木糖苷静脉抗血栓药Iliparcil对大鼠溶栓治疗后再血栓形成的影响。该药物在溶栓治疗前口服给药,溶栓治疗包括肝素和尿激酶(H/U)分别以37.5和70000 IU/kg联合给药。再咬合时间从生理盐水组的3.9 min增加到注射H/U后的10.5 min。注射h /U前4 h给药Iliparcil (30 mg/kg,口服),与单独给药h /U相比,再咬合时间增加250% (p < 0.001)。同样,在血栓诱导前5分钟静脉注射硫酸皮丹(DS) (3 mg/kg),也增加了再闭塞的时间(与单独使用H/U相比,增加了300%;P < 0.001)。研究还表明,即使肝素剂量减少,髂骨parcil或DS治疗后再闭塞的次数仍然增加。这些结果表明,从β - d -木糖苷家族衍生的抗血栓产品可以与溶栓治疗联合使用,而不是肝素,后者会导致并发症和副作用。
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The beneficial effect of a beta-D-xyloside, Iliparcil, in the prevention of postthrombolytic rethrombosis in the rat.

The effect of Iliparcil, a new orally active beta-D-xyloside venous antithrombotic, was studied on the rethrombosis following thrombolytic therapy in rats, using a modified Umetsu model. The drug was administered by oral route prior to thrombolytic therapy, which consisted of administering a combination of heparin and urokinase (H/U) at 37.5 and 70,000 IU/kg, respectively. Time to reocclusion increased from 3.9 min with saline to 10.5 min following H/U injection. When Iliparcil (30 mg/kg, oral route) was administered 4 h before H/U injection, the time to reocclusion was increased by 250% compared with H/U alone (p < 0.001). Similarly, dermatan sulfate (DS), administered intravenously (3 mg/kg) 5 min before thrombus induction, also increased the time to reocclusion (300% compared with H/U alone; p < 0.001). It was also shown that times to reocclusion following Iliparcil or DS treatments were still increased even when heparin dosage was decreased. These results suggest that an antithrombotic product derived from the beta-D-xyloside family could be advantageously used in combination with thrombolytic treatment instead of heparin, which causes complications and side effects.

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