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不同纯度的凝血因子 VIII 浓缩物中所含的血管性血友病因子支持来自异质性血管性血友病患者组的血样中的血小板黏附。

von Willebrand factor contained in factor VIII concentrates of different purities supports platelet adhesion in blood samples from a heterogeneous group of patients with von Willebrand disease.

作者信息

Escolar G, Carretero M, Magallón M, Quintana M, Arnau C, Castillo R, Aznar-Salatti J

机构信息

Servicio de Hemoterapia y Hemostasia, Facultad de Medicina, Universidad de Barcelona, Spain.

出版信息

Haematologica. 1998 Nov;83(11):1009-14.

PMID:9864923
Abstract

BACKGROUND AND OBJECTIVE

Plasma derived FVIII-VWF concentrates in which the VWF structure is reasonably maintained are recommended as substitutive therapy in VWD. Our aim was to assess platelet deposition and binding to subendothelial structures of VWF present in FVIII concentrates.

DESIGN AND METHODS

Cryoprecipitate (CRY), intermediate-purity (IPC), or high-purity (HPC) FVIII concentrates were added in vitro to citrated blood samples from 11 patients affected by different subtypes of VWD, with the aim of normalizing VWF levels. Measurements of VWF:Ag, ristocetin cofactor (RiCof) activities, FVIII coagulant activity (FVIII:C), and platelet interaction with subendothelium under flow conditions (Baumgartner's perfusion method, computer-assisted morphometry, shear rate 1000 s-1, 10 min, 37 degrees C) were determined. Binding of VWF to the luminal surface of the perfused vessels was assessed by immunofluorescence microscopy. Paired t-test statistics were performed.

RESULTS

Addition of FVIII-VWF preparations raised VWF:Ag from baseline (BSL) values of 0.3 (SD 0.2) to averages of 1.4 (SD 0.5, p < 0.001), 1.2 (SD 0.6, p < 0.001), and 0.4 (SD 0.3) IU mL-1 after CRY, IPC, and HPC, respectively. A positive labeling for VWF was observed by immunofluorescence in vessels perfused with blood containing any of the concentrates. Platelet adhesion of 13.2 (SD 7.6), 22.4 (SD 10.8), 24.8 (SD 7.8, p < 0.03), or 22.5 (SD 4.8)% was measured in BSL, CRY, IPC, or HPC tests, respectively.

INTERPRETATION AND CONCLUSIONS

Our observations support the hypothesis above the mechanisms involved in the beneficial effects of commercial concentrates in von Willebrand disease: the VWF in these concentrates has functional capacity to bind to subendothelium and to support platelet adhesion.

摘要

背景与目的

推荐使用能合理维持血管性血友病因子(VWF)结构的血浆源性FVIII - VWF浓缩物作为血管性血友病(VWD)的替代疗法。我们的目的是评估血小板在FVIII浓缩物中VWF与内皮下结构的沉积及结合情况。

设计与方法

将冷沉淀(CRY)、中纯度(IPC)或高纯度(HPC)FVIII浓缩物体外添加至11例不同亚型VWD患者的枸橼酸化血样中,以使VWF水平正常化。测定VWF:Ag、瑞斯托霉素辅因子(RiCof)活性、FVIII凝血活性(FVIII:C),以及在流动条件下(鲍姆加特纳灌注法,计算机辅助形态测量,剪切速率1000 s-1,10分钟,37℃)血小板与内皮下的相互作用。通过免疫荧光显微镜评估VWF与灌注血管腔表面的结合情况。进行配对t检验统计分析。

结果

添加FVIII - VWF制剂后,VWF:Ag从基线(BSL)值0.3(标准差0.2)分别升至CRY、IPC和HPC后的平均值1.4(标准差0.5,p < 0.001)、1.2(标准差0.6,p < 0.001)和0.4(标准差0.3)IU/mL。在灌注含有任何一种浓缩物血液的血管中,通过免疫荧光观察到VWF呈阳性标记。在BSL、CRY、IPC或HPC试验中,分别测得血小板黏附率为13.2(标准差7.6)、22.4(标准差10.8)、24.8(标准差7.8,p < 0.03)或22.5(标准差4.8)%。

解读与结论

我们的观察结果支持上述关于商业浓缩物对血管性血友病有益作用机制的假设:这些浓缩物中的VWF具有与内皮下结合并支持血小板黏附的功能能力。

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