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首页> 外文期刊>Scandinavian journal of clinical and laboratory investigation. >Potential of whole blood coagulation reconstitution by desmopressin and fibrinogen under conditions of hypothermia and acidosis--an in vitro study using rotation thrombelastometry.
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Potential of whole blood coagulation reconstitution by desmopressin and fibrinogen under conditions of hypothermia and acidosis--an in vitro study using rotation thrombelastometry.

机译:在体温过低和酸中毒的情况下,去氨加压素和纤维蛋白原重构全血的潜力-使用旋转血栓弹性测定法进行的体外研究。

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BACKGROUND: Desmopressin (DDAVP) and fibrinogen improve platelet function and clot stability. We investigated the influence of DDAVP and fibrinogen on whole blood coagulation in an in vitro model of hypothermia and acidosis. METHODS: After IRB approval and written consent blood samples were taken from 10 healthy volunteers. Samples were prepared with hydrochloric acid to maintain--beside normal pH--reduced pH ( approximately 7.2) and severely reduced pH ( approximately 7.0), and were assigned to four treatment groups: addition of either isotonic saline for compensation of dilutional effects (ISO), desmopressin (DDAVP+), fibrinogen (FIB+), or both substances (DDAVP+FIB+). Baseline was ISO at 37 degrees C and normal pH. Remaining samples were incubated for 30 min and measured at 32 degrees . Rotation thrombelastometry (ROTEM) after extrinsically activation and fibrin polymerization was tested. Repeated measures ANOVA were performed (p < 0.05). RESULTS: Hypothermia and acidosis synergistically impaired whole blood coagulation. DDAVP+ normalized maximum clot firmness (MCF) at normal pH. Coagulation time (CT) was not affected. FIB+ normalized MCF at pH 7.35 and pH 7.2. CT was normalized independently of pH. DDAVP+FIB+ did not show additional effects to FIB+. Fibrin polymerization was increased by FIB+ and DDAVP+FIB+ independently of pH. DDAVP+ did not alter fibrin polymerization. CONCLUSION: DDAVP and fibrinogen increased whole blood coagulation under hypothermia. Acidosis diminished this effect. Thus, acidosis should be corrected first and then both substances could be used for bridging until normothermia can be achieved. In combination, the effects of fibrinogen were overwhelming DDAVP effects. Thus, combined administration did not show any benefit compared to fibrinogen administration alone.
机译:背景:去氨加压素(DDAVP)和纤维蛋白原可改善血小板功能和血凝块稳定性。我们在体外低温和酸中毒的体外模型中研究了DDAVP和纤维蛋白原对全血凝固的影响。方法:在IRB批准并获得书面同意后,从10名健康志愿者那里采集了血液样本。用盐酸制备样品,以维持pH值(正常pH值以下),降低的pH值(约7.2)和严重降低的pH值(约7.0),并分为四个处理组:添加等渗盐水以补偿稀释效应(ISO ),去氨加压素(DDAVP +),纤维蛋白原(FIB +)或两种物质(DDAVP + FIB +)。基准是在37摄氏度和正常pH下的ISO。其余样品孵育30分钟,并在32度下测量。在外部激活和纤维蛋白聚合后,进行旋转血栓弹性测定(ROTEM)。重复进行方差分析(p <0.05)。结果:体温过低和酸中毒协同损害全血凝结。 DDAVP +标准化了正常pH下的最大凝块硬度(MCF)。凝血时间(CT)不受影响。 FIB +在pH 7.35和pH 7.2下归一化MCF。 CT的标准化与pH无关。 DDAVP + FIB +对FIB +没有显示其他作用。 FIB +和DDAVP + FIB +可以独立于pH值增加血纤蛋白的聚合反应。 DDAVP +不会改变纤维蛋白的聚合。结论:DDAVP和纤维蛋白原可增加体温过低下的全血凝结。酸中毒减弱了这种作用。因此,应首先纠正酸中毒,然后可以将两种物质都用于桥接,直到达到正常体温。结合起来,纤维蛋白原的作用压倒了DDAVP的作用。因此,与单独施用纤维蛋白原相比,联合施用未显示任何益处。

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