Mirasol 病原体减少处理技术不会影响由储存血成分引起的体内两事件模型中的急性肺损伤。

Mirasol Pathogen Reduction Technology treatment does not affect acute lung injury in a two-event in vivo model caused by stored blood components.

机构信息

The Bonfils Blood Center, Denver, Colorado, USA.

出版信息

Vox Sang. 2010 May;98(4):525-30. doi: 10.1111/j.1423-0410.2009.01289.x. Epub 2009 Nov 25.

DOI:10.1111/j.1423-0410.2009.01289.x

PMID:19951305

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3132808/

Abstract

INTRODUCTION

Mirasol Pathogen Reduction Technology (PRT) treatment uses riboflavin and UV light to inactivate pathogens in blood components. Neutrophil [polymorphonuclear cells (PMN)] priming activity accumulates during routine storage of cellular blood components, and this activity has been implicated in transfusion-related acute lung injury (TRALI). We hypothesize that PRT-treatment of blood components affects the priming activity generated during storage of packed RBCs (PRBCs) or platelet concentrates (PCs), which can elicit ALI in vivo.

METHODS

Plasma, PRBCs and PCs were isolated from healthy donor's whole blood or by apheresis. Half of a collected unit was treated with PRT treatment and the remainder was left as an unmodified control. Supernatant was collected during storage of PCs and PRBCs and assayed for PMN priming activity and used as the second event in a two-event in vivo model of TRALI.

RESULTS

PRT treatment did not induce priming activity in plasma or affect the priming activity generated during storage of PCs or PRBCs as compared with the unmodified controls. The supernatants from stored, but not fresh, PCs and PRBCs did cause ALI as the second event in a two-event animal model of TRALI, which was unaffected by PRT treatment. We conclude that the PRT treatment does not induce priming activity in plasma nor does it affect the priming activity generated during storage of PCs or PRBCs or their ability to cause ALI as the second event in a two-event in vivo model of TRALI. Moreover, the amount of priming activity in TRIMA-isolated PCs was significantly less than SPECTRA-isolated PCs.

摘要

简介

Mirasol 病原体减少技术（PRT）处理使用核黄素和紫外线来灭活血液成分中的病原体。在常规储存细胞血液成分期间，中性粒细胞[多形核细胞（PMN）]的激活活性会累积，并且这种活性与输血相关的急性肺损伤（TRALI）有关。我们假设血液成分的 PRT 处理会影响储存期间产生的 PMN 激活活性，这些活性可能会在体内引发 ALI。

方法

从健康供体的全血或通过单采分离血浆、PRBC 和血小板浓缩物（PC）。收集的一半单位用 PRT 处理，另一半单位作为未修饰的对照。在储存 PC 和 PRBC 期间收集上清液，并检测 PMN 激活活性，用作 TRALI 两事件体内模型的第二个事件。

结果

与未修饰的对照相比，PRT 处理不会在血浆中诱导激活活性，也不会影响储存期间 PC 或 PRBC 中产生的激活活性。但是，储存而不是新鲜的 PC 和 PRBC 的上清液确实会在 TRALI 的两事件动物模型中引起 ALI，而 PRT 处理对其没有影响。我们得出结论，PRT 处理不会在血浆中诱导激活活性，也不会影响储存期间 PC 或 PRBC 中产生的激活活性，也不会影响它们在 TRALI 的两事件体内模型中作为第二个事件引起 ALI 的能力。此外，TRIMA 分离的 PC 中的激活活性明显少于 SPECTRA 分离的 PC。

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