在乌干达儿童的一项病例对照研究中,血红素-血红素结合蛋白轴失调与严重疟疾有关。
Dysregulation of the haem-haemopexin axis is associated with severe malaria in a case-control study of Ugandan children.
作者信息
Elphinstone Robyn E, Riley Frank, Lin Tian, Higgins Sarah, Dhabangi Aggrey, Musoke Charles, Cserti-Gazdewich Christine, Regan Raymond F, Warren H Shaw, Kain Kevin C
机构信息
Sandra Rotman Centre for Global Health, University Health Network-Toronto General Hospital, Toronto, ON, Canada.
Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, ON, Canada.
出版信息
Malar J. 2015 Dec 21;14:511. doi: 10.1186/s12936-015-1028-1.
BACKGROUND
Malaria is associated with haemolysis and the release of plasma haem. Plasma haem can cause endothelial injury and organ dysfunction, and is normally scavenged by haemopexin to limit toxicity. It was hypothesized that dysregulation of the haem-haemopexin pathway contributes to severe and fatal malaria infections.
METHODS
Plasma levels of haemin (oxidized haem), haemopexin, haptoglobin, and haemoglobin were quantified in a case-control study of Ugandan children with Plasmodium falciparum malaria. Levels at presentation were compared in children with uncomplicated malaria (UM; n = 29), severe malarial anaemia (SMA; n = 27) or cerebral malaria (CM; n = 31), and evaluated for utility in predicting fatal (n = 19) vs non-fatal (n = 39) outcomes in severe disease. A causal role for haemopexin was assessed in a pre-clinical model of experimental cerebral malaria (ECM), following disruption of mouse haemopexin gene (hpx). Analysis was done using Kruskall Wallis tests, Mann-Whitney tests, log-rank tests for survival, and repeated measures ANOVA.
RESULTS
In Ugandan children presenting with P. falciparum malaria, haemin levels were higher and haemopexin levels were lower in SMA and CM compared to children with UM (haemin, p < 0.01; haemopexin, p < 0.0001). Among all cases of severe malaria, elevated levels of haemin and cell-free haemoglobin at presentation were associated with subsequent mortality (p < 0.05). Compared to ECM-resistant BALB/c mice, susceptible C57BL/6 mice had lower circulating levels of haemopexin (p < 0.01), and targeted deletion of the haemopexin gene, hpx, resulted in increased mortality compared to their wild type littermates (p < 0.05).
CONCLUSIONS
These data indicate that plasma levels of haemin and haemopexin measured at presentation correlate with malaria severity and levels of haemin and cell-free haemoglobin predict outcome in paediatric severe malaria. Mechanistic studies in the ECM model support a causal role for the haem-haemopexin axis in ECM pathobiology.
背景
疟疾与溶血及血浆血红素的释放有关。血浆血红素可导致内皮损伤和器官功能障碍,通常由血红素结合蛋白清除以限制毒性。据推测,血红素-血红素结合蛋白途径的失调会导致严重和致命的疟疾感染。
方法
在一项针对乌干达恶性疟原虫疟疾儿童的病例对照研究中,对血浆中的高铁血红素(氧化血红素)、血红素结合蛋白、触珠蛋白和血红蛋白水平进行了定量分析。比较了单纯性疟疾(UM;n = 29)、严重疟疾贫血(SMA;n = 27)或脑型疟疾(CM;n = 31)患儿就诊时的水平,并评估其在预测严重疾病中致命(n = 19)与非致命(n = 39)结局方面的效用。在实验性脑型疟疾(ECM)的临床前模型中,通过破坏小鼠血红素结合蛋白基因(hpx)来评估血红素结合蛋白的因果作用。使用Kruskal Wallis检验、Mann-Whitney检验、生存对数秩检验和重复测量方差分析进行分析。
结果
在患有恶性疟原虫疟疾的乌干达儿童中,与单纯性疟疾患儿相比,严重疟疾贫血和脑型疟疾患儿的高铁血红素水平较高,血红素结合蛋白水平较低(高铁血红素,p < 0.01;血红素结合蛋白,p < 0.0001)。在所有严重疟疾病例中,就诊时高铁血红素和游离血红蛋白水平升高与随后的死亡率相关(p < 0.05)。与抗ECM的BALB/c小鼠相比,易感的C57BL/6小鼠循环中的血红素结合蛋白水平较低(p < 0.01),并且靶向缺失血红素结合蛋白基因hpx导致其死亡率高于野生型同窝小鼠(p < 0.05)。
结论
这些数据表明,就诊时测得的血浆高铁血红素和血红素结合蛋白水平与疟疾严重程度相关,高铁血红素和游离血红蛋白水平可预测儿童严重疟疾的结局。ECM模型中的机制研究支持血红素-血红素结合蛋白轴在ECM病理生物学中的因果作用。
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