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加纳儿童可溶性CD163水平与疟疾严重程度

Levels of soluble CD163 and severity of malaria in children in Ghana.

作者信息

Kusi Kwadwo A, Gyan Ben A, Goka Bamenla Q, Dodoo Daniel, Obeng-Adjei George, Troye-Blomberg Marita, Akanmori Bartholomew D, Adjimani Jonathan P

机构信息

Immunology Department, Noguchi Memorial Institute for Medical Research, P.O. Box LG581, University of Ghana, Legon, Ghana.

出版信息

Clin Vaccine Immunol. 2008 Sep;15(9):1456-60. doi: 10.1128/CVI.00506-07. Epub 2008 Jul 16.

Abstract

CD163 is an acute-phase-regulated monocyte/macrophage membrane receptor expressed late in inflammation. It is involved in the haptoglobin-mediated removal of free hemoglobin from plasma, has been identified as a naturally soluble plasma glycoprotein with potential anti-inflammatory properties, and is possibly linked to an individual's haptoglobin phenotype. High levels of soluble CD163 (sCD163) in a malaria episode may therefore downregulate inflammation and curb disease severity. In order to verify this, the relationships between sCD163 levels, malaria severity, and selected inflammatory mediators (tumor necrosis factor alpha [TNF-alpha], interleukin-6 [IL-6], and IL-10) were assessed by enzyme-linked immunosorbent assay using plasma samples obtained from pediatric malaria patients with uncomplicated malaria (UM [n = 38]), cerebral malaria (CM [n = 52]), and severe malarial anemia (SA [n = 55]) during two consecutive malaria transmission seasons (2002 and 2003). Median sCD163 levels were higher in UM (11.9 microg/ml) patients than in SA (7.7 microg/ml; P = 0.010) and CM (8.0 microg/ml; P = 0.031) patients. Levels of sCD163 were also higher in all patient groups than in a group of 81 age-matched healthy controls. The higher sCD163/TNF-alpha ratio in UM patients, coupled with the fact that sCD163 levels correlated with TNF-alpha levels in UM patients but not in CM and SA patients, suggests inflammatory dysregulation in the complicated cases. The study showed that sCD163 levels are elevated during acute malaria. High sCD163 levels in UM patients may be due to the induction of higher-level anti-inflammatory responses, enabling them to avoid disease complications. It is also possible that UM patients simply lost their CD163 receptors from macrophages in inflammatory sites while complicated-malaria patients still had their receptors attached to activated macrophages, reflecting ongoing and higher-level inflammation associated with complicated malaria.

摘要

CD163是一种急性期调节的单核细胞/巨噬细胞膜受体,在炎症后期表达。它参与触珠蛋白介导的从血浆中清除游离血红蛋白的过程,已被鉴定为一种具有潜在抗炎特性的天然可溶性血浆糖蛋白,并且可能与个体的触珠蛋白表型有关。因此,疟疾发作时高水平的可溶性CD163(sCD163)可能会下调炎症反应并抑制疾病严重程度。为了验证这一点,在2002年和2003年这两个连续的疟疾传播季节,使用从患有非复杂性疟疾(UM [n = 38])、脑型疟疾(CM [n = 52])和严重疟疾贫血(SA [n = 55])的儿科疟疾患者获得的血浆样本,通过酶联免疫吸附测定法评估了sCD163水平、疟疾严重程度与选定的炎症介质(肿瘤坏死因子α [TNF-α]、白细胞介素-6 [IL-6]和IL-10)之间的关系。UM患者(11.9微克/毫升)的sCD163水平中位数高于SA患者(7.7微克/毫升;P = 0.010)和CM患者(8.0微克/毫升;P = 0.031)。所有患者组的sCD163水平也高于81名年龄匹配健康对照者组成的组。UM患者中较高的sCD163/TNF-α比值,以及sCD163水平在UM患者中与TNF-α水平相关但在CM和SA患者中不相关这一事实,表明复杂病例中存在炎症失调。该研究表明,急性疟疾期间sCD163水平升高。UM患者中sCD163水平较高可能是由于诱导了更高水平的抗炎反应,使他们能够避免疾病并发症。也有可能UM患者只是在炎症部位的巨噬细胞上失去了他们的CD163受体,而复杂疟疾患者的受体仍附着在活化的巨噬细胞上,这反映了与复杂疟疾相关的持续且更高水平的炎症。

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