首页> 外文期刊>Transfusion: The Journal of the American Association of Blood Banks >Infusible platelet membranes improve hemostasis in thrombocytopenic blood: experimental studies under flow conditions.
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Infusible platelet membranes improve hemostasis in thrombocytopenic blood: experimental studies under flow conditions.

机译:不可溶的血小板膜可改善血小板减少性血液的止血作用:在流动条件下的实验研究。

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BACKGROUND: The potential hemostatic effect of infusible platelet membranes (IPM; Cyplex, Cypress Bioscience) prepared from outdated human platelets is investigated. STUDY DESIGN AND METHODS: Increasing concentrations of IPM were added to blood samples anticoagulated with low-molecular-weight heparin, in which platelets and WBC counts had been experimentally reduced by a filtration procedure. Thrombocytopenic blood with IPM was circulated in a perfusion chamber at various shear rates (300, 600, and 1200/sec(-1)), and platelet and fibrin deposition on the surface of a damaged vessel was measured. Prothrombin fragments 1 and 2 (F1+2) levels were also monitored. RESULTS: Under conditions of severe thrombocytopenia (<6000 platelets/microL) IPM did not increase platelet deposition. However, a dose-dependent increase in fibrin deposition was observed with concentrations of IPM ranging from 0.5 to 2 mg per kg in perfusions at 300 and 600 per sec(-1) (p<0.05 vs. thrombocytopenic blood). Experimental studies performed under conditions of moderate thrombocytopenia and higher shear rates (25, 000-30,000 platelets/microL; at 600 and 1200/sec(-1)) showed that IPM concentrations equivalent to 0.5 or 1 mg per kg improved fibrin deposition (33.5 +/- 9.5% and 37.7 +/- 12.8%, respectively, vs. 22.7 +/- 5.2% in controls) and also promoted a moderate increase in platelet deposition, with a concomitant significant increase in the size of platelet aggregates (p<0.05). Exposure of thrombocytopenic blood to a damaged vessel resulted in an increase of F1+2 levels from 0.8 +/- 0.15 to 1.7 +/- 0.22 nM at 300 per sec(-1) and 1.94 +/- 0.46 nM at 600 per sec(-1). Postperfusion levels of F1+2 after the addition of IPM were always similar to levels in untreated controls. CONCLUSION: IPM promotes local procoagulant activity at sites of vascular damage under conditions of severe and moderate thrombocytopenia. IPM also appears to facilitate platelet cohesive functions under conditions of moderate thrombocytopenia.
机译:背景:研究了从过时的人类血小板制备的不溶性血小板膜(IPM; Cyplex,赛普拉斯生物科学)的潜在止血作用。研究设计和方法:向低分子量肝素抗凝的血液样本中添加IPM浓度的增加,其中通过过滤程序实验性地减少了血小板和WBC的数量。使用IPM的血小板减少血在灌注室中以不同的剪切速率(300、600和1200 / sec(-1))循环,并测量血小板和血纤蛋白在受损血管表面的沉积。还监测凝血酶原片段1和2(F1 + 2)的水平。结果:在严重血小板减少症(<6000血小板/微升)的情况下,IPM不会增加血小板沉积。然而,在300和600 sec(-1)的灌注中,IPM的浓度范围为0.5至2 mg / kg,观察到血纤蛋白沉积的剂量依赖性增加(p <0.05 vs.血小板减少性血液)。在中度血小板减少症和较高剪切速率(25、000-30,000血小板/微升;在600和1200 /秒(-1)下)下进行的实验研究表明,IPM浓度相当于每公斤0.5或1 mg可以改善纤维蛋白沉积(33.5分别为+/- 9.5%和37.7 +/- 12.8%,而对照组为22.7 +/- 5.2%),并且还促进了血小板沉积的适度增加,同时血小板聚集物的大小也显着增加(p < 0.05)。血小板减少血暴露于受损血管导致F1 + 2水平从300 sec(-1)从0.8 +/- 0.15增加到1.7 +/- 0.22 nM,在600 sec(1.9)则从1.94 +/- 0.46 nM增加( -1)。加入IPM后的F1 + 2灌流后水平始终与未经治疗的对照组相似。结论:在重度和中度血小板减少的情况下,IPM可促进血管损伤部位的局部促凝活性。 IPM在中度血小板减少症的情况下也似乎有助于血小板凝聚功能。

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