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流量校准以确定细胞衍生的微粒和血液成分的均一性。

Flow rate calibration to determine cell-derived microparticles and homogeneity of blood components.

作者信息

Noulsri Egarit, Lerdwana Surada, Kittisares Kulvara, Palasuwan Attakorn, Palasuwan Duangdao

机构信息

Research Division, Faculty of Medicine Siriraj Hospital, Mahidol University, Bangkok, Thailand.

Department of Research and Development, Faculty of Medicine Siriraj Hospital, Mahidol University, Bangkok, Thailand.

出版信息

Transfus Apher Sci. 2017 Aug;56(4):585-590. doi: 10.1016/j.transci.2017.07.016. Epub 2017 Jul 18.

Abstract

BACKGROUND

Cell-derived microparticles (MPs) are currently of great interest to screening transfusion donors and blood components. However, the current approach to counting MPs is not affordable for routine laboratory use due to its high cost.

AIM

The current study aimed to investigate the potential use of flow-rate calibration for counting MPs in whole blood, packed red blood cells (PRBCs), and platelet concentrates (PCs).

METHODS

The accuracy of flow-rate calibration was investigated by comparing the platelet counts of an automated counter and a flow-rate calibrator. The concentration of MPs and their origins in whole blood (n=100), PRBCs (n=100), and PCs (n=92) were determined using a FACSCalibur. The MPs' fold-changes were calculated to assess the homogeneity of the blood components.

RESULTS

Comparing the platelet counts conducted by automated counting and flow-rate calibration showed an r of 0.6 (y=0.69x+97,620). The CVs of the within-run and between-run variations of flow-rate calibration were 8.2% and 12.1%, respectively. The Bland-Altman plot showed a mean bias of -31,142platelets/μl. MP enumeration revealed both the difference in MP levels and their origins in whole blood, PRBCs, and PCs. Screening the blood components demonstrated high heterogeneity of the MP levels in PCs when compared to whole blood and PRBCs.

CONCLUSIONS

The results of the present study suggest the accuracy and precision of flow-rate calibration for enumerating MPs. This flow-rate approach is affordable for assessing the homogeneity of MPs in blood components in routine laboratory practice.

摘要

背景

细胞衍生的微粒(MPs)目前在筛选输血供体和血液成分方面备受关注。然而,由于成本高昂,目前计数MPs的方法不适用于常规实验室使用。

目的

本研究旨在探讨流速校准在全血、浓缩红细胞(PRBCs)和血小板浓缩物(PCs)中计数MPs的潜在用途。

方法

通过比较自动计数器和流速校准器的血小板计数来研究流速校准的准确性。使用FACSCalibur测定全血(n = 100)、PRBCs(n = 100)和PCs(n = 92)中MPs的浓度及其来源。计算MPs的倍数变化以评估血液成分的同质性。

结果

比较自动计数和流速校准得出的血小板计数,r为0.6(y = 0.69x + 97,620)。流速校准的批内和批间变异系数分别为8.2%和12.1%。Bland-Altman图显示平均偏差为-31,142个血小板/μl。MP计数揭示了全血、PRBCs和PCs中MP水平及其来源的差异。对血液成分进行筛选显示,与全血和PRBCs相比,PCs中MP水平具有高度异质性。

结论

本研究结果表明流速校准在计数MPs方面具有准确性和精密度。这种流速方法在常规实验室实践中评估血液成分中MPs的同质性方面是经济可行的。

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