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新型小鼠血小板输血模型的表征。

Characterization of a novel mouse platelet transfusion model.

机构信息

Department of Pathology and Cell Biology, Columbia University Irving Medical Center, New York, New York, USA.

出版信息

Vox Sang. 2024 Jul;119(7):702-711. doi: 10.1111/vox.13642. Epub 2024 Apr 21.

DOI:10.1111/vox.13642
PMID:38643983
Abstract

BACKGROUND AND OBJECTIVES

Platelet transfusions are increasing with medical advances. Based on FDA criteria, platelet units are assessed by in vitro measures; however, it is not known how platelet processing and storage duration affect function in vivo. Our study's aim was to develop a novel platelet transfusion model stored in mouse plasma that meets FDA criteria adapted to mice, and transfused fresh and stored platelets are detectable in clots in vivo.

STUDY DESIGN AND METHODS

Platelet units stored in mouse plasma were prepared using a modified platelet-rich plasma (PRP) collection protocol. Characteristics of fresh and stored units, including pH, cell count, in vitro measures of activity, including activation and aggregation, and post-transfusion recovery (PTR), were determined. Lastly, a tail transection assay was conducted using mice transfused with fresh or stored units, and transfused platelets were identified by confocal imaging.

RESULTS

Platelet units had acceptable platelet and white cell counts and were negative for bacterial contamination. Fresh and 1-day stored units had acceptable pH; the platelets were activatable by thrombin and adenosine diphosphate, agreeable with thrombin, had acceptable PTR, and were present in vivo in clots of recipients after tail transection. In contrast, 2-day stored units had clinically unacceptable quality.

CONCLUSION

We developed mouse platelets for transfusion analogous to human platelet units using a modified PRP collection protocol with maximum storage of 1 day for an 'old' unit. This provides a powerful tool to test how process modifications and storage conditions affect transfused platelet function in vivo.

摘要

背景与目的

随着医学的进步,血小板输注量不断增加。根据 FDA 标准,血小板单位通过体外测量进行评估;然而,尚不清楚血小板处理和储存时间如何影响体内功能。我们的研究目的是开发一种新的血小板输注模型,该模型在满足 FDA 标准的情况下在鼠血浆中储存,适应于小鼠,并可在体内血栓中检测到新鲜和储存的血小板。

研究设计与方法

使用改良的富含血小板血浆(PRP)采集方案制备储存在鼠血浆中的血小板单位。测定新鲜和储存单位的特性,包括 pH 值、细胞计数、体外活性测量,包括激活和聚集,以及输注后恢复(PTR)。最后,通过尾切断试验用新鲜或储存单位输注小鼠,并通过共聚焦成像鉴定输注的血小板。

结果

血小板单位的血小板和白细胞计数可接受,且无细菌污染。新鲜和 1 天储存的单位 pH 值可接受;血小板可被凝血酶和二磷酸腺苷激活,与凝血酶一致,具有可接受的 PTR,并且在接受者的血栓中在体内存在于接受者的血栓中。相比之下,2 天储存的单位质量不佳。

结论

我们使用改良的 PRP 采集方案开发了类似于人类血小板单位的用于输注的小鼠血小板,最大储存时间为 1 天,对于“旧”单位。这为测试处理方式的改变和储存条件如何影响体内输注血小板的功能提供了有力工具。

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1
Characterization of a novel mouse platelet transfusion model.新型小鼠血小板输血模型的表征。
Vox Sang. 2024 Jul;119(7):702-711. doi: 10.1111/vox.13642. Epub 2024 Apr 21.
2
Characterization of a Novel Mouse Platelet Transfusion Model.
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Permanent lesions of stored platelets correlate to pH and cell count while reversible lesions do not.储存血小板的永久性损伤与pH值和细胞计数相关,而可逆性损伤则不然。
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PLoS One. 2021 May 11;16(5):e0250120. doi: 10.1371/journal.pone.0250120. eCollection 2021.
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Effects of storage time on quantitative and qualitative platelet function after transfusion.储存时间对输血后血小板定量和定性功能的影响。
Anesthesiology. 1995 Dec;83(6):1167-72. doi: 10.1097/00000542-199512000-00006.
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Resveratrol preserves the function of human platelets stored for transfusion.白藜芦醇可维持用于输血的储存人血小板的功能。
Br J Haematol. 2016 Mar;172(5):794-806. doi: 10.1111/bjh.13862. Epub 2015 Dec 18.
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Evaluation of platelet function using the in vitro bleeding time and corrected count increment of transfused platelets. Comparison between platelet concentrates derived from pooled buffy coates and apheresis.使用体外出血时间和输注血小板校正计数增加值评估血小板功能。比较来自混合白膜层和单采血小板的浓缩血小板。
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