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病原体灭活对冷沉淀的影响:功能和定量评估

The effect of pathogen inactivation on cryoprecipitate: a functional and quantitative evaluation.

作者信息

Kamyszek Reed W, Foster Matthew W, Evans Brooke A, Stoner Keaton, Poisson Jessica, Srinivasan Amudan J, Thompson J Will, Moseley M Arthur, Mooberry Micah J, Welsby Ian J

机构信息

Department of Anesthesiology, University of Michigan, Ann Arbor, MI, United States of America.

Duke University School of Medicine, Durham, NC, United States of America.

出版信息

Blood Transfus. 2020 Nov;18(6):454-464. doi: 10.2450/2020.0077-20. Epub 2020 Aug 6.

Abstract

BACKGROUND

As a pooled donor blood product, cryoprecipitate (cryo) carries risks of pathogen transmission. Pathogen inactivation (PI) improves the safety of cryoprecipitate, but its effects on haemostatic properties remain unclear. This study investigated protein expression in samples of pathogen inactivated cryoprecipitate (PI-cryo) using non-targeted quantitative proteomics and in vitro haemostatic capacity of PI-cryo.

MATERIALS AND METHODS

Whole blood (WB)- and apheresis (APH)-derived plasma was subject to PI with INTERCEPT Blood System (Cerus Corporation, Concord, CA, USA) and cryo was prepared from treated plasma. Protein levels in PI-cryo and paired controls were quantified using liquid chromatography-tandem mass spectrometry. Functional haemostatic properties of PI-cryo were assessed using a microparticle (MP) prothrombinase assay, thrombin generation assay, and an in vitro coagulopathy model subjected to thromboelastometry.

RESULTS

Over 300 proteins were quantified across paired PI-cryo and controls. PI did not alter the expression of coagulation factors, but levels of platelet-derived proteins and platelet-derived MPs were markedly lower in the WB PI-cryo group. Compared to controls, WB (but not APH) cryo samples demonstrated significantly lower MP prothrombinase activity, prolonged clotting time, and lower clot firmness on thromboelastometry after PI. However, PI did not affect overall thrombin generation variables in either group.

DISCUSSION

Data from this study suggest that PI via INTERCEPT Blood System does not significantly impact the coagulation factor content or function of cryo but reduces the higher MP content in WB-derived cryo. PI-cryo products may confer benefits in reducing pathogen transmission without affecting haemostatic function, but further in vivo assessment is warranted.

摘要

背景

作为一种汇集的献血者血液制品,冷沉淀存在病原体传播风险。病原体灭活(PI)可提高冷沉淀的安全性,但其对止血特性的影响尚不清楚。本研究使用非靶向定量蛋白质组学研究病原体灭活冷沉淀(PI-冷沉淀)样本中的蛋白质表达以及PI-冷沉淀的体外止血能力。

材料与方法

使用INTERCEPT血液系统(美国加利福尼亚州康科德市赛鲁斯公司)对全血(WB)和单采(APH)血浆进行PI处理,并从处理后的血浆中制备冷沉淀。使用液相色谱-串联质谱法定量PI-冷沉淀和配对对照中的蛋白质水平。使用微粒(MP)凝血酶原酶测定、凝血酶生成测定以及体外凝血障碍模型通过血栓弹力图评估PI-冷沉淀的功能性止血特性。

结果

在配对的PI-冷沉淀和对照中对300多种蛋白质进行了定量。PI未改变凝血因子的表达,但WB PI-冷沉淀组中血小板衍生蛋白和血小板衍生MP的水平明显较低。与对照相比,WB(而非APH)冷沉淀样本在PI后显示出明显较低的MP凝血酶原酶活性、延长的凝血时间以及血栓弹力图上较低的凝块硬度。然而,PI对两组中的总体凝血酶生成变量均无影响。

讨论

本研究数据表明,通过INTERCEPT血液系统进行的PI不会显著影响冷沉淀的凝血因子含量或功能,但会降低WB来源冷沉淀中较高的MP含量。PI-冷沉淀产品可能在降低病原体传播方面具有益处且不影响止血功能,但需要进一步的体内评估。

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