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慢性病贫血:病理生理学与实验室诊断

Anemia of chronic disease: pathophysiology and laboratory diagnosis.

作者信息

Thomas Christian, Thomas Lothar

机构信息

Urologische Klinik und Poliklinik der Universität Mainz, Mainz, Germany.

出版信息

Lab Hematol. 2005;11(1):14-23. doi: 10.1532/LH96.04049.

Abstract

Classic iron deficiency (ID) does not represent a challenge for the laboratory and physicians. The anemia that accompanies infection, inflammation, and cancer, commonly termed anemia of chronic disease (ACD), features apparently normal or increased iron stores. However, 20% of these patients have iron-restricted erythropoiesis (functional ID), an imbalance between the iron requirements of the erythroid marrow and the actual iron supply. Functional ID leads to a reduction in red cell hemoglobiniza-tion, causing hypochromic microcytic anemia. The diagnosis of functional ID in real time is based on measuring the hemoglobin content of reticulocytes. An examination of the biochemical markers of iron metabolism demonstrates weaknesses in the diagnosis of functional ID. We developed a diagnostic plot for the assessment of iron status in ACD and the detection of advancing ID in patients with ID, ACD, and the combined state of functional ID and ACD. The plot indicates the correlation between a marker of the iron supply for erythropoiesis (ie, the ratio of the soluble transferrin receptor value to the logarithm of the ferritin value) and the reticulocyte hemoglobin content and functions as a marker of iron demand. The diagnostic plot shows good selectivity for assessing the iron status of disease-specific anemias such as classic ID, end-stage renal failure, cancer-related anemia, and the anemia of infection and inflammation. The therapeutic implications of the diagnostic plot are to differentiate patients who should be administered oral iron supplements, recombinant human erythropoietin (r-HuEPO), or a combination of r-HuEPO and iron. The response of erythropoiesis to r-HuEPO depends on the iron supply and the proliferation of erythropoiesis. The lack of an increase or a decrease in reticulocyte hemoglobin levels indicates a nonresponder to r-HuEPO or functional ID.

摘要

典型的缺铁(ID)对实验室和医生来说并不构成挑战。伴随感染、炎症和癌症出现的贫血,通常称为慢性病贫血(ACD),其特征是铁储备明显正常或增加。然而,这些患者中有20%存在铁限制的红细胞生成(功能性ID),即红系骨髓的铁需求与实际铁供应之间的失衡。功能性ID会导致红细胞血红蛋白化减少,引起低色素小细胞性贫血。功能性ID的实时诊断基于测量网织红细胞的血红蛋白含量。对铁代谢生化标志物的检查表明在功能性ID的诊断方面存在不足。我们开发了一种诊断图,用于评估ACD患者的铁状态以及检测ID、ACD以及功能性ID与ACD合并状态患者中进展性ID。该图显示了红细胞生成铁供应标志物(即可溶性转铁蛋白受体值与铁蛋白值对数之比)与网织红细胞血红蛋白含量之间的相关性,并作为铁需求的标志物发挥作用。诊断图在评估特定疾病贫血(如典型ID、终末期肾衰竭、癌症相关贫血以及感染和炎症性贫血)的铁状态方面具有良好的选择性。诊断图的治疗意义在于区分应给予口服铁补充剂(、重组人促红细胞生成素(r-HuEPO)或r-HuEPO与铁联合使用的患者。红细胞生成对r-HuEPO的反应取决于铁供应和红细胞生成的增殖情况。网织红细胞血红蛋白水平未升高或降低表明对r-HuEPO无反应或存在功能性ID。

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