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在患有血红蛋白病的成年人中存在具有胎儿表型的 F 细胞,这限制了流式细胞术用于定量胎儿母体出血的应用。

The presence of F cells with a fetal phenotype in adults with hemoglobinopathies limits the utility of flow cytometry for quantitation of fetomaternal hemorrhage.

机构信息

Institute of Haematology, Royal Prince Alfred Hospital, Camperdown, New South Wales, Australia.

出版信息

Cytometry B Clin Cytom. 2018 Jul;94(4):695-698. doi: 10.1002/cyto.b.21598. Epub 2017 Nov 16.

DOI:10.1002/cyto.b.21598
PMID:29072803
Abstract

BACKGROUND

Detection and quantitation of fetomaternal hemorrhage (FMH) can be difficult in patients with pre-existing elevations of HbF, such as those with hemoglobinopathies. The aim of this study was to evaluate the utility of dual-color flow cytometry with the Fetal Cell Count Kit (FCCK) in differentiating adult and fetal HbF in this population, as compared to flow cytometry (FC) using HbF alone.

METHODS

Peripheral blood was obtained from normal adults and patients with hemoglobinopathies (β-thalassemia and sickle cell disease), including a small number of pregnant females. Cord blood was used to spike some samples with 5% fetal cells. Analysis by single color (HbF) and dual-color (HbF and carbonic anhydrase) FC was performed on these samples. Fetal cells were defined as those with high HbF fluorescence on single-color FC, and those that were HbF + CA- using the FCCK. The quantity of fetal cells detected by each technique was compared.

RESULTS

Forty-six adult patients were included. In non-pregnant adults with hemoglobinopathies, a population of red cells with a fetal cell phenotype were detected by both techniques. The dual-color method reported lower quantities of these cells. In nineteen samples spiked with cord blood the FCCK consistently underestimated the quantity of fetal cells.

CONCLUSIONS

Patients with β-thalassemia and sickle cell disease have a population of HbF-containing cells which are phenotypically similar to fetal cells. Even with dual-color flow cytometry (FCCK), the detection and quantification of FMH by flow cytometry in this population remains difficult. © 2017 International Clinical Cytometry Society.

摘要

背景

在存在血红蛋白 F(HbF)升高的患者中,例如患有血红蛋白病的患者,检测和定量胎儿母体出血(FMH)可能很困难。本研究的目的是评估双荧光素标记流式细胞术(dual-color flow cytometry)联合胎儿细胞计数试剂盒(Fetal Cell Count Kit,FCCK)在该人群中与单独使用 HbF 的流式细胞术(flow cytometry,FC)相比,用于区分成人和胎儿 HbF 的效用。

方法

从正常成年人和血红蛋白病(β-地中海贫血和镰状细胞病)患者中获得外周血,包括少数孕妇。用脐带血对一些样本进行 5%胎儿细胞的掺入。对这些样本进行单染(HbF)和双染(HbF 和碳酸酐酶)FC 分析。通过单染 FC 检测到 HbF 荧光强度高的胎儿细胞,以及 FCCK 检测到的 HbF+CA-的细胞定义为胎儿细胞。比较每种技术检测到的胎儿细胞数量。

结果

共纳入 46 例成年患者。在非妊娠血红蛋白病患者中,两种技术均检测到具有胎儿细胞表型的红细胞群体。双染法报告的这些细胞数量较低。在 19 个掺入脐带血的样本中,FCCK 始终低估了胎儿细胞的数量。

结论

β-地中海贫血和镰状细胞病患者存在一群表型上类似于胎儿细胞的含 HbF 细胞。即使使用双荧光素标记流式细胞术(FCCK),该人群中通过流式细胞术检测和定量 FMH 仍然很困难。 © 2017 国际临床细胞化学学会。

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