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Microparticle content of plasma for transfusion is influenced by the whole blood hold conditions: pre-analytical considerations for proteomic investigations

机译:用于输血的血浆的微粒含量受到全血的影响:蛋白质组学调查的分析前考虑

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摘要

Microparticles (MPs) are shed from normal blood cells and may contribute to the coagulation potential of plasma. Transfusion of fresh frozen plasma (FFP) is used to correct coagulopathies and blood loss in trauma or major surgery. The role of MPs in FFP clinical efficacy is unknown. Regulations that govern the preparation of FFP vary in different countries. The aim of this study was to determine the effect of whole blood (WB)-hold conditions before FFP preparation on the MP profile. WB units were held at room temperature (RT) or combination of RT and refrigeration for up to 24hr before FFP preparation. The MP content in thawed FFP was measured to reflect transfusion practice. The absolute number of MPs in FFP increased with longer WB hold time. Refrigeration of WB may also promote increased generation of MPs. In particular the number of platelet-derived and phosphatidylserine-containing MPs, which are known to have procoagulant properties, increased. Lipid peroxidation increased with longer WB-hold time. Donor-related factors appear to govern lipid peroxidation levels. Holistic proteomic and coagulant analyses of FFP MPs is warranted. Such information could guide the choice of the optimal handling conditions of WB and the most relevant quality control procedures for FFP.
机译:微粒(MPs)从正常血细胞中脱落,可能有助于血浆凝结。新鲜冷冻血浆(FFP)的输血用于纠正创伤或大手术中的凝血病和失血。 MP在FFP临床疗效中的作用尚不清楚。有关FFP制备的法规在不同国家有所不同。这项研究的目的是确定FFP制备前全血(WB)保持条件对MP分布的影响。在准备FFP之前,将WB单元在室温(RT)或RT与冷藏的组合下放置24小时。测量融化的FFP中的MP含量以反映输血实践。随着白平衡保持时间的延长,FFP中MP的绝对数量增加。 WB的冷藏也可能促进MP的产生。特别地,已知具有促凝血特性的血小板衍生的和含磷脂酰丝氨酸的MP的数量增加。脂质过氧化随着WB保持时间的延长而增加。供体相关因素似乎控制脂质过氧化水平。对FFP MP进行整体蛋白质组学和凝血分析是必要的。这些信息可以指导选择WB的最佳处理条件以及最相关的FFP质量控制程序。

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