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影响冷冻肝素化血浆稳定性的因素的表征

Characterization of factors affecting the stability of frozen heparinized plasma.

作者信息

Palmer D S, Rosborough D, Perkins H, Bolton T, Rock G, Ganz P R

机构信息

Ottawa Centre, Canadian Red Cross, Blood Transfusion Service, Ontario, Canada.

出版信息

Vox Sang. 1993;65(4):258-70. doi: 10.1111/j.1423-0410.1993.tb02165.x.

Abstract

The use of heparin rather than citrate as primary anticoagulant has been shown to significantly improve the initial activity, stability and recovery of factor VIII:C from human plasma, cryoprecipitates or factor VIII concentrates if the plasma was initially frozen at -80 degrees C and subsequently stored at this temperature. If frozen and stored at progressively warmer temperatures however, increasing amounts of insoluble protein aggregates, termed storage precipitates (SPs), were recovered in the thawed plasma and cryoprecipitate fractions. Plasma recovery by centrifugation at 7,000 g for 7 min [Method I (MI)], 2 x 10 min (MII) or 15 min (MIII) had little effect on SP formation after 1 month at any storage temperature. After 4 months at -20 degrees C, more SP was recovered from MIII plasma whereas at -40 degrees C, more SP was recovered from MI plasma. Also, the preparation method had little or no effect on factor VIII:C activity at equivalent storage times or temperatures. A trend towards improved factor VIII recoveries was noted at lower freezing and storage temperatures however. SP formation was associated with reduced fibrinogen levels in the recovered plasma without loss of antithrombin-III or increased fibrinopeptide-A. Western blots showed polymerization of A alpha or gamma-chains of fibrinogen. SP formation was reduced or eliminated with factor XIII inhibitors, antibody to the active factor XIII a subunit or adjustment of heparinized plasma to 5-10 mM sodium citrate before initial freezing and storage. Although plasma factor VIII:C recoveries were only slightly affected at these citrate concentrations under most conditions, its recovery in cryoprecipitates was substantially improved owing to the reduction or absence of SPs.

摘要

如果血浆最初在-80℃冷冻并随后在此温度下储存,已表明使用肝素而非柠檬酸盐作为主要抗凝剂可显著提高从人血浆、冷沉淀或因子VIII浓缩物中获得的因子VIII:C的初始活性、稳定性和回收率。然而,如果在逐渐升高的温度下冷冻和储存,在解冻的血浆和冷沉淀部分中会回收越来越多的不溶性蛋白质聚集体,称为储存沉淀物(SPs)。在任何储存温度下,通过在7000g离心7分钟[方法I(MI)]、2×10分钟(MII)或15分钟(MIII)进行血浆回收,对1个月后的SP形成影响很小。在-20℃储存4个月后,从MIII血浆中回收的SP更多,而在-40℃时,从MI血浆中回收的SP更多。此外,在相同的储存时间或温度下,制备方法对因子VIII:C活性几乎没有影响。然而,在较低的冷冻和储存温度下,观察到因子VIII回收率有提高的趋势。SP的形成与回收血浆中纤维蛋白原水平降低有关,而抗凝血酶III没有损失或纤维蛋白肽A没有增加。蛋白质免疫印迹显示纤维蛋白原的Aα或γ链发生聚合。在初始冷冻和储存前,使用因子 XIII抑制剂、活性因子 XIII a亚基抗体或将肝素化血浆调节至5-10 mM柠檬酸钠可减少或消除SP的形成。尽管在大多数情况下,这些柠檬酸盐浓度下血浆因子VIII:C回收率仅受到轻微影响,但由于SP的减少或不存在,其在冷沉淀中的回收率显著提高。

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