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糖化白蛋白不是镰状细胞病炎症的有用生物标志物。

GlycA is not a useful biomarker of inflammation in sickle cell disease.

机构信息

Sickle Cell Branch, National Heart, Lung and Blood Institute, The National Institutes of Health, Bethesda, Maryland.

Royal Sussex County Hospital, Brighton, UK.

出版信息

Int J Lab Hematol. 2018 Dec;40(6):704-709. doi: 10.1111/ijlh.12907. Epub 2018 Aug 27.

DOI:10.1111/ijlh.12907
PMID:30152174
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6419740/
Abstract

INTRODUCTION

Sickle cell disease (SCD) is a multisystemic disorder, the pathology being driven by recurrent inflammation particularly during a vaso-occlusive crisis. GlycA, a composite measure of protein glycation, is a sensitive biomarker for disorders associated with vascular inflammation. We determined the utility of GlycA as a biomarker of inflammation in SCD.

METHODS

Stored plasma samples from patients with SCD recruited to two clinical studies were analyzed. One study encompasses 488 patient samples with SCD (HbSS, HbSβ and HbSC) at steady state and 52 race-matched, healthy controls. The other study included paired plasma samples during steady state and acute pain crisis from (HbSS) patients with SCD. Plasma GlycA was measured using a proton NMR on the Vantera Clinical Analyzer. We performed analysis comparing patients with SCD, healthy controls, and paired samples analysis.

RESULTS

The mean plasma GlycA level was lower in SCD compared with healthy controls (324.6 ± 70.4 μmol/L vs. 386.3 ± 74.6 μmol/L, P < 0.0001). Within the same patient, mean plasma GlycA during acute pain crisis was lower than steady state, although the difference was not significant (300.5 ± 36.3 μmol/L vs 314.2 ± 34.8 μmol/L, P = 0.020). Plasma GlycA correlated inversely with serum LDH (P = 0.009).

CONCLUSION

GlycA is not a suitable biomarker of inflammation in SCD. We surmise that its signal is confounded by hemolysis leading to a depletion of haptoglobin, one of the major plasma proteins included in the composite NMR signal. Hemolysis is further exacerbated during an acute pain crisis, hence the lower GlycA levels in crisis compared to steady state.

摘要

简介

镰状细胞病(SCD)是一种多系统疾病,其病理学由反复炎症驱动,特别是在血管阻塞性危象期间。GlycA 是一种蛋白质糖化的综合衡量指标,是一种与血管炎症相关疾病的敏感生物标志物。我们确定 GlycA 作为 SCD 炎症标志物的效用。

方法

分析了从参与两项临床研究的 SCD 患者中储存的血浆样本。一项研究包括 488 名 SCD 患者(HbSS、HbSβ 和 HbSC)的稳态和 52 名种族匹配的健康对照者的样本。另一项研究包括 SCD 患者在稳态和急性疼痛危机期间配对的血浆样本。使用 Vantera 临床分析仪上的质子 NMR 测量血浆 GlycA。我们进行了比较 SCD 患者、健康对照者和配对样本分析的分析。

结果

与健康对照组相比,SCD 患者的平均血浆 GlycA 水平较低(324.6±70.4 μmol/L 与 386.3±74.6 μmol/L,P<0.0001)。在同一患者中,急性疼痛危机期间的平均血浆 GlycA 低于稳态,尽管差异无统计学意义(300.5±36.3 μmol/L 与 314.2±34.8 μmol/L,P=0.020)。血浆 GlycA 与血清 LDH 呈负相关(P=0.009)。

结论

GlycA 不是 SCD 炎症的合适生物标志物。我们推测,由于血红蛋白的消耗,其信号受到溶血的干扰,血红蛋白是复合 NMR 信号中包含的主要血浆蛋白之一。在急性疼痛危机期间,溶血进一步加剧,因此与稳态相比,危机中的 GlycA 水平较低。

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