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Blood soluble drag-reducing polymers prevent lethality from hemorrhagic shock in acute animal experiments

机译:在急性动物实验中,可溶血的减阻聚合物可防止因失血性休克致死

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Over the past several decades, blood-soluble drag reducing polymers (DRPs) have been shown to significantly enhance hemodynamics in various animal models when added to blood at nanomolar concentrations. In the present study, the effects of the DRPs on blood circulation were tested in anesthetized rats exposed to acute hemorrhagic shock. The animals were acutely resuscitated either with a 2.5% dextran solution (Control) or using the same solution containing 0.0005% or 5 parts per million (ppm) concentration of one of two blood soluble DRPs: high molecular weight (MW = 3500 kDa) polyethylene glycol (PEG-3500) or a DRP extracted from Aloe vera (AVP). An additional group of animals was resuscitated with 0.0075% (75 ppm) polyethylene glycol of molecular weight of 200 kDa (PEG-200), which possesses no drag-reducing ability. All of the animals were observed for two hours following the initiation of fluid resuscitation or until they expired. We found that infusion of the DRP solutions significantly improved tissue perfusion, tissue oxygenation, and two-hour survival rate, the latter from 19% (Control) and 14% (PEG-200) to 100% (AVP) and 100% (PEG-3500). Furthermore, the Control and PEG-200 animals that survived required three times more fluid to maintain their blood pressure than the AVP and PEG-3500 animals. Several hypotheses regarding the mechanisms underlying these observed beneficial hemodynamic effects of DRPs are discussed. Our findings suggest that the drag-reducing polymers warrant further investigation as a potential clinical treatment for hemorrhagic shock and possibly other microcirculatory disorders.
机译:在过去的几十年中,已证明当以纳摩尔浓度添加到血液中时,可溶于血液的减阻聚合物(DRP)可显着增强各种动物模型的血液动力学。在本研究中,在暴露于急性失血性休克的麻醉大鼠中测试了DRP对血液循环的影响。用2.5%右旋糖酐溶液(对照)或使用含有0.0005%或百万分之5(ppm)浓度的两种可溶DRP之一的相同溶液对动物进行急性复苏:高分子量(MW = 3500 kDa)聚乙烯乙二醇(PEG-3500)或从芦荟(AVP)中提取的DRP。另一组动物用0.0075%(75 ppm)分子量为200 kDa的聚乙二醇(PEG-200)进行复苏,该聚乙烯不具有减阻能力。在开始液体复苏后或直到它们死亡之前,观察所有动物两个小时。我们发现输注DRP溶液可显着改善组织灌注,组织氧合和2小时生存率,后者从19%(对照)和14%(PEG-200)增至100%(AVP)和100%(PEG) -3500)。此外,存活下来的对照动物和PEG-200动物需要的液体维持其血压的压力是AVP和PEG-3500动物的三倍。讨论了有关这些观察到的DRP有益血流动力学作用基础的机制的一些假设。我们的发现表明,减阻聚合物应作为出血性休克和其他微循环障碍的潜在临床治疗方法进行进一步研究。

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