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使用氧梯度红细胞变形性测定法进行受控自动脱氧过程中镰状化的特征分析。

Characterization of Sickling During Controlled Automated Deoxygenation with Oxygen Gradient Ektacytometry.

作者信息

Rab Minke A E, van Oirschot Brigitte A, Bos Jennifer, Kanne Celeste K, Sheehan Vivien A, van Beers Eduard J, van Wijk Richard

机构信息

Laboratory of Clinical Chemistry and Hematology, University Medical Center Utrecht, Utrecht University; Van Creveldkliniek, University Medical Center Utrecht, Utrecht University;

Laboratory of Clinical Chemistry and Hematology, University Medical Center Utrecht, Utrecht University.

出版信息

J Vis Exp. 2019 Nov 5(153). doi: 10.3791/60213.

Abstract

In sickle cell disease (SCD), a single point mutation in the gene coding for beta-globin causes the production of abnormal hemoglobin S (HbS). When deoxygenated, HbS can polymerize, forming rigid rods of hemoglobin, resulting in the sickling of red blood cells (RBCs). These sickled RBCs have significantly reduced deformability, causing vaso-occlusion, which leads to numerous SCD-related clinical complications, including pain, stroke, and organ damage. RBC deformability is also reduced by RBC dehydration, resulting in dense red blood cells that are more likely to sickle. To date, there is not a single widely available, rapid, and reproducible laboratory assay capable of predicting the disease severity or directly monitoring the treatment effects for novel, non-fetal hemoglobin inducing therapies. In this study, we describe a protocol to measure RBC deformability as a function of pO2 that allows for the quantitation of sickling behavior in SCD patients. Oxygen gradient ektacytometry measures RBC deformability, expressed as the elongation index (EI), as a function of pO2. RBCs are exposed to a fixed shear stress of 30 Pa during one round of deoxygenation and reoxygenation. Six readout parameters are produced. Of these, the point of sickling (PoS), defined as the pO2 at which maximum EI (EImax) shows a 5% decrease, and minimum EI during deoxygenation (EImin) are the most informative, reflecting an individual patient's pO2 at which sickling starts and the minimal deformability of a patient's red blood cells, respectively. PoS is associated with an individual patient's hemoglobin affinity for oxygen, whereas EImin shows a strong correlation with fetal hemoglobin levels. We conclude that oxygen gradient ektacytometry is a promising technique to monitor the treatment of patients with SCD, as a biomarker for anti-sickling agents in clinical and preclinical trials, and an important tool to study sickling behavior of RBCs from individuals with SCD and sickle cell traits.

摘要

在镰状细胞病(SCD)中,编码β-珠蛋白的基因发生单点突变,导致异常血红蛋白S(HbS)的产生。当去氧时,HbS会聚合,形成血红蛋白刚性棒状物,导致红细胞(RBC)镰变。这些镰变的红细胞变形性显著降低,导致血管阻塞,进而引发许多与SCD相关的临床并发症,包括疼痛、中风和器官损伤。红细胞脱水也会降低红细胞变形性,导致红细胞密度增加,更容易发生镰变。迄今为止,尚无一种广泛可用、快速且可重复的实验室检测方法能够预测疾病严重程度或直接监测新型非胎儿血红蛋白诱导疗法的治疗效果。在本研究中,我们描述了一种测量红细胞变形性随氧分压(pO2)变化的方案,该方案可对SCD患者的镰变行为进行定量分析。氧梯度血细胞变形性测定法测量红细胞变形性,以伸长指数(EI)表示,作为pO2的函数。在一轮去氧和复氧过程中,红细胞暴露于30 Pa的固定剪切应力下。产生六个读出参数。其中,镰变点(PoS)定义为最大伸长指数(EImax)下降5%时的pO2,去氧过程中的最小伸长指数(EImin)最具信息量,分别反映个体患者镰变开始时的pO2和患者红细胞的最小变形性。PoS与个体患者的血红蛋白对氧的亲和力相关,而EImin与胎儿血红蛋白水平密切相关。我们得出结论,氧梯度血细胞变形性测定法是监测SCD患者治疗的一种有前景的技术,可作为临床和临床前试验中抗镰变药物的生物标志物,也是研究SCD患者和镰状细胞性状个体红细胞镰变行为的重要工具。

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