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Immunophenotypic Profiling of Erythroid Progenitor-Derived Extracellular Vesicles in Diamond-Blackfan Anaemia: A New Diagnostic Strategy

机译:钻石-Blackfan贫血中类红细胞祖细胞外囊的免疫表型分析:一种新的诊断策略。

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摘要

Diamond-Blackfan Anaemia (DBA) is a rare inherited anaemia caused by heterozygous mutations in one of 13 ribosomal protein genes. Erythroid progenitors (BFU-E and CFU-E) in bone marrow (BM) show a proapoptotic phenotype. Suspicion of DBA is reached after exclusion of other forms of BM failure syndromes. To improve DBA diagnosis, which is confirmed by mutation analysis, we tested a new approach based on the study of extracellular vesicles (EVs) isolated from plasma by differential centrifugations and analysed by flow cytometry. We chose CD34, CD71 and CD235a markers to study erythroid EVs. We characterised the EVs immunophentoypic profiles of 13 DBA patients, 22 healthy controls and 16 patients with other haematological diseases. Among the three EVs clusters we found, only the CD34+/CD71low population showed statistically significant differences between DBA patients and controls (p< 0.05). The absence of this cluster is in agreement with the low levels of BFU-E found in DBA patients. The assessment of ROC curves demonstrated the potential diagnostic value of this population. We suggest that this assay may be useful to improve DBA diagnosis as a quicker and less invasive alternative to BM BFU-E culture analysis.
机译:Diamond-Blackfan贫血(DBA)是一种罕见的遗传性贫血,由13个核糖体蛋白基因之一的杂合突变引起。骨髓(BM)中的类红细胞祖细胞(BFU-E和CFU-E)显示出凋亡的表型。排除其他形式的BM衰竭综合征后,可疑DBA。为了提高突变分析所证实的DBA诊断,我们基于通过差速离心从血浆中分离出的细胞外囊泡(EV)并通过流式细胞仪进行分析的基础上,测试了一种新方法。我们选择了CD34,CD71和CD235a标记来研究类红细胞电动汽车。我们表征了13名DBA患者,22名健康对照和16名其他血液系统疾病患者的EV免疫表型特征。在我们发现的三个电动汽车集群中,只有CD34 + / CD71low人群在DBA患者和对照组之间显示出统计学上的显着差异(p <0.05)。该簇的缺乏与在DBA患者中发现的BFU-E水平低相符。 ROC曲线的评估证明了该人群的潜在诊断价值。我们建议,该测定法可能作为提高BM BFU-E文化分析的一种更快,侵入性较小的替代方法,可以改善DBA诊断。

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