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Absorbance and redox based approaches for measuring free heme and free hemoglobin in biological matrices

机译:基于吸光度和氧化还原的方法来测量生物基质中的游离血红素和游离血红蛋白

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摘要

Cell-free heme (CFH) and hemoglobin (Hb) have emerged as distinct mediators of acute injury characterized by inflammation and microcirculatory dysfunction in hemolytic conditions and critical illness. Several reports have shown changes in Hb and CFH in specific pathophysiological settings. Using PBS, plasma from patients with sickle cell disease, acute respiratory distress syndrome (ARDS) patients and supernatants from red cells units, we found that commonly used assays and commercially available kits do not distinguish between CFH and Hb. Furthermore, they suffer from a variety of false-positive interferences and limitations (including from bilirubin) that lead to either over- or underestimation of CFH and/or Hb. Moreover, commonly used protocols to separate CFH and Hb based on molecular weight (MWt) are inefficient due to CFH hydrophobicity. In this study, we developed and validated a new approach based on absorbance spectrum deconvolution with least square fitting analyses that overcomes these limitations and simultaneously measures CFH and Hb in simple aqueous buffers, plasma or when associated with red cell derived microvesicles. We show how incorporating other plasma factors that absorb light over the visible wavelength range (specifically bilirubin), coupled with truncating the wavelength range analyzed, or addition of mild detergent significantly improves fits allowing measurement of oxyHb, CFH and metHb with >90% accuracy. When this approach was applied to samples from SCD patients, we observed that CFH levels are higher than previously reported and of similar magnitude to Hb.
机译:无细胞血红素(CFH)和血红蛋白(Hb)已成为急性损伤的独特介质,其特征为溶血条件和危重疾病中的炎症和微循环功能障碍。一些报告显示在特定的病理生理环境中血红蛋白和CFH的变化。使用PBS,镰状细胞病患者的血浆,急性呼吸窘迫综合征(ARDS)患者的血浆和红细胞单位的上清液,我们发现常用的检测方法和市售试剂盒无法区分CFH和Hb。此外,它们遭受各种假阳性干扰和局限性(包括胆红素),导致CFH和/或Hb的高估或低估。此外,由于CFH疏水性,基于分子量(MWt)分离CFH和Hb的常用方案效率低下。在这项研究中,我们开发并验证了一种基于最小二乘拟合分析的基于吸收光谱解卷积的新方法,该方法克服了这些限制,并同时在简单的水性缓冲液,血浆中或与红细胞衍生的微囊泡相关联时测量CFH和Hb。我们展示了如何结合吸收在可见光波长范围内吸收光的其他血浆因子(特别是胆红素),并截短所分析的波长范围,或添加温和的清洁剂如何显着改善拟合度,从而能够以> 90%的精度测量oxyHb,CFH和metHb。当这种方法应用于来自SCD患者的样品时,我们观察到CFH水平高于以前报道的水平,与Hb相似。

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