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儿童非综合征性δ 储存池缺陷患者的功能分类。

Functional Classification of Paediatric Patients with Non-syndromic Delta-Storage Pool Deficiency.

机构信息

Institute of Experimental Biomedicine, University Hospital Würzburg, Würzburg, Germany.

Practice for Pediatric Hematology and Hemostaseology, Munich, Germany.

出版信息

Hamostaseologie. 2019 Nov;39(4):383-391. doi: 10.1055/s-0038-1675574. Epub 2018 Nov 21.

Abstract

Storage pool disease (SPD) covers a group of platelet defects in which α- and/or delta-granules are reduced or cannot be secreted adequately in response to agonists. The detection of delta-granule release defects is hampered by a lack of fast and feasible tests. We aimed to implement a flow cytometry-based kinetic mepacrine assay to better identify and subgroup childhood patients with a mild to moderate bleeding diathesis and compare our method to established laboratory tests. We analysed 50 children with suspected SPD whose initial parameters were re-assessed in a second site visit. Mepacrine uptake and release patterns were correlated with CD63 exposure, platelet ADP/ATP release and content, and the bleeding score ascertained by the ISTH-BAT. Mepacrine release was overall significantly reduced in investigated patients compared with controls. Summarizing, our time-resolved approach proved to be a quick and inexpensive tool that was additionally able to distinguish between mepacrine uptake, mepacrine release, and combined defects. Classification of patients using such a kinetic assay makes it feasible to sensitively detect frequently missed SPD and to group these patients for further analyses and clinical correlations.

摘要

储存池病(SPD)涵盖了一组血小板缺陷,其中α-和/或δ-颗粒减少或不能对激动剂充分分泌。由于缺乏快速可行的检测方法,δ-颗粒释放缺陷的检测受到阻碍。我们旨在实施基于流式细胞术的米帕林动力学测定法,以更好地识别和亚组具有轻度至中度出血素质的儿童患者,并将我们的方法与既定的实验室检测进行比较。我们分析了 50 名疑似 SPD 的儿童,他们的初始参数在第二次现场访问中重新评估。米帕林摄取和释放模式与 CD63 暴露、血小板 ADP/ATP 释放和含量以及 ISTH-BAT 确定的出血评分相关。与对照组相比,研究患者的米帕林释放总体上显著降低。总之,我们的时间分辨方法被证明是一种快速且廉价的工具,此外还能够区分米帕林摄取、米帕林释放和联合缺陷。使用这种动力学测定法对患者进行分类,可以灵敏地检测到经常被遗漏的 SPD,并对这些患者进行进一步的分析和临床相关性分组。

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