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[缺铁性贫血中的红细胞生成]

[Erythropoiesis in iron deficiency].

作者信息

Dörmer P, Lau B

出版信息

Blut. 1977 Jun;34(6):453-64. doi: 10.1007/BF00996872.

Abstract

The kinetics of erythroblast proliferation were studied by means of quantitative 14C-autoradiography in 5 patients showing anemia due to infection or malignancy, in 7 patients suffering from iron deficiency anemia, and in two individuals with bleeding enemia. Compared with a group of 5 healthy persons a markedly reduced turnover of erythroblasts was found in the anemia due to infection, malignancy, and iron deficiency, whereas this turnover was normal or increased in the case of bleeding anemia. The reduction is caused by a progressively decreasing rate of erythroblast proliferation and maturation with advancing development into mature cells. No indications of a change in the number of cell divisions were found in the anemia of infection, malignancy, and of iron deficiency, nor was there evidence of an intramedullary death of nucleated red cell percursors. The imbalance between production and loss of red cells causing anemia shows a different pattern in the 3 groups of disease: In bleeding anemia the insufficiency of supply is not yet apparent from the rate of erythroblast turnover giving weight to the factor of blood loss. In anemia due to infection, malignancy, and iron deficiency the but moderately increased rate of red cell destruction cannot be compensated because of several impairments: The rate of erythroblast turnover is reduced, and, in addition, a moderate portion of maturing cells is destroyed, probably at the reticulocyte stage. As the most significant factor, the bone marrow is unable to compensate the anemia by an effective erythroblast hyperplasia. In iron deficiency this hyperplasia is inadequately low, in infection and malignancies, however, it is more or less missing.

摘要

通过定量¹⁴C放射自显影术研究了5例因感染或恶性肿瘤导致贫血的患者、7例缺铁性贫血患者以及2例出血性贫血患者的成红细胞增殖动力学。与5名健康人组成的对照组相比,发现因感染、恶性肿瘤和缺铁导致的贫血中,成红细胞的更新明显减少,而在出血性贫血中,这种更新正常或增加。这种减少是由于成红细胞增殖和成熟的速率随着向成熟细胞的发育而逐渐降低。在感染性贫血、恶性肿瘤性贫血和缺铁性贫血中,未发现细胞分裂数量有变化的迹象,也没有证据表明有核红细胞前体在骨髓内死亡。导致贫血的红细胞生成与丢失之间的失衡在3组疾病中表现出不同的模式:在出血性贫血中,从成红细胞更新速率来看,供应不足尚不明显,这突出了失血因素。在因感染、恶性肿瘤和缺铁导致的贫血中,红细胞破坏速率仅适度增加,但由于多种损害因素无法得到补偿:成红细胞更新速率降低,此外,一部分成熟细胞可能在网织红细胞阶段被破坏。最主要的因素是骨髓无法通过有效的成红细胞增生来补偿贫血。在缺铁性贫血中,这种增生程度过低,而在感染和恶性肿瘤中,增生或多或少缺失。

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