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网织红细胞血红蛋白含量

Reticulocyte hemoglobin content.

作者信息

Ogawa Chie, Tsuchiya Ken, Maeda Kunimi

机构信息

Maeda Institute of Renal Research, 6F-1-403 Kosugi-cho, Nakahara-ku, Kawasaki, Kanagawa 211-0063, Japan; Biomarker Society, INC, 6F-1-403 Kosugi-cho, Nakahara-ku, Kawasaki, Kanagawa, Japan.

Department of Blood Purification, Tokyo Women's Medical University, 8-1 Kawadacho, Shinjuku-ku, Tokyo 162-8666, Japan; Biomarker Society, INC, 6F-1-403 Kosugi-cho, Nakahara-ku, Kawasaki, Kanagawa, Japan.

出版信息

Clin Chim Acta. 2020 May;504:138-145. doi: 10.1016/j.cca.2020.01.032. Epub 2020 Jan 31.

DOI:10.1016/j.cca.2020.01.032
PMID:32014518
Abstract

Iron deficiency leads to the suppression of hemoglobin (Hb) synthesis and induces metabolic disorders. In contrast, iron overload not only reduces the iron utilization efficiency but also induces oxidative stress. Iron metabolism in the body is closely regulated by hepcidin, a short peptide produced by the liver. Unfortunately, conventional iron indices may not always accurately reflect the iron status. For example, Hb concentration assessed using mature erythrocytes do not accurately reflect the real-time iron status due to their long lifespan. Reticulocytes are differentiated from erythroblasts after Hb synthesis and transform into mature erythrocytes in 1-2 days upon release into peripheral blood. Thus, Hb content in reticulocytes (Hb-ret) is more reflective of real-time Hb synthesis. Moreover, Hb-ret is affected only by the amount of iron intake as long as there is no hematopoietic disorder. Reticulocyte Hb content (CHr) can be accurately and inexpensively measured as Hb-ret by commercial H*3 or ADVIA hematology analyzers. CHr has been shown to be more effective than other indices of iron metabolism for the diagnosis of iron deficiency, for early detection of the therapeutic effects of iron therapy, and for differentiation of the beta thalassemia trait.

摘要

缺铁会导致血红蛋白(Hb)合成受到抑制,并引发代谢紊乱。相比之下,铁过载不仅会降低铁的利用效率,还会引发氧化应激。体内的铁代谢受到肝脏产生的一种短肽——铁调素的密切调控。遗憾的是,传统的铁指标可能并不总能准确反映铁状态。例如,使用成熟红细胞评估的Hb浓度并不能准确反映实时铁状态,因为它们的寿命较长。网织红细胞在Hb合成后从成红细胞分化而来,并在释放到外周血后1 - 2天内转化为成熟红细胞。因此,网织红细胞中的Hb含量(Hb-ret)更能反映实时Hb合成情况。此外,只要没有造血障碍,Hb-ret仅受铁摄入量的影响。通过商用H*3或ADVIA血液分析仪可将网织红细胞血红蛋白含量(CHr)作为Hb-ret进行准确且低成本的测量。CHr已被证明在诊断缺铁、早期检测铁治疗的疗效以及鉴别β地中海贫血特征方面比其他铁代谢指标更有效。

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