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[小细胞低色素性贫血]

[Microcytic and hypochromic anemias].

作者信息

Chrobák L

机构信息

Oddĕlení klinické hematologie Fakultní nemocnice, Hradec Králové.

出版信息

Vnitr Lek. 2001 Mar;47(3):166-74.

PMID:15635879
Abstract

In the majority of cases, microcytosis is the result of impaired hemoglobin synthesis. Disorders of iron metabolism and protoporphyrin and heme synthesis, as well as impaired globin synthesis, lead to defective hemoglobin production and to the generation of microcytosis and microcytic anemia. Iron deficiency anemie, anemia of chronic diseases, thalassemias, congenital sideroblastic anemias and homozygous HbE disease are the main representatives of microcytosis and microcytic anemias. Serum iron, total iron binding capacity, transferrin saturation, serum ferritin, serum transferrin receptor, transferrin receptor-ferritin index, and zinc-protoporhyrin concentration in erythrocytes are tests used for assessment of iron deficiency. The convention laboratory test for diagnosing iron deficiency is the measurement of serum ferritin. The most precise method for evaluating body iron stores is the examination for iron on aspirated bone marrow or marrow biopsy. Increased content of Hb A2 over 3.5% is diagnostic for beta-thalassemia. Presence of ringed sideroblasts is characteristic of sideroblastic anemias. Hemoglobin electrophoresis is required for the diagnosis of hemoglobinopathy E. The optimal therapeutic regimen in iron deficiency anemia used in this country is to administer 100 mg of elemental iron twice daily separately from meals. Ferrous sulphate (Ferronat Retard tbl. or Sorbifer Dulures tbl.) which are slow-releasing iron formulations are preferred because of their low cost, high bioavailability and low side-effects. Parenteral iron therapy is justified only in patients who cannot absorb iron, who have blood losses that exceed the maximal absorptive capacity of their intestinal tract or who are totally intolerant of oral iron. However, parenteral iron therapy may be associated with serious and even fatal side-effects.

摘要

在大多数情况下,小红细胞症是血红蛋白合成受损的结果。铁代谢、原卟啉和血红素合成紊乱,以及珠蛋白合成受损,会导致血红蛋白生成缺陷,进而引发小红细胞症和小细胞性贫血。缺铁性贫血、慢性病性贫血、地中海贫血、先天性铁粒幼细胞贫血和纯合子血红蛋白E病是小红细胞症和小细胞性贫血的主要代表类型。血清铁、总铁结合力、转铁蛋白饱和度、血清铁蛋白、血清转铁蛋白受体、转铁蛋白受体-铁蛋白指数以及红细胞中的锌原卟啉浓度是用于评估缺铁的检测指标。诊断缺铁的常规实验室检测是测定血清铁蛋白。评估体内铁储备最精确的方法是对抽吸的骨髓进行铁检查或骨髓活检。血红蛋白A2含量超过3.5%可诊断为β地中海贫血。环形铁粒幼细胞的存在是铁粒幼细胞贫血的特征。诊断血红蛋白病E需要进行血红蛋白电泳。该国治疗缺铁性贫血的最佳治疗方案是每天两次,每次100毫克元素铁,与餐分开服用。硫酸亚铁(缓释铁制剂Ferronat Retard tbl.或Sorbifer Dulures tbl.)因其成本低、生物利用度高和副作用小而更受青睐。仅在无法吸收铁、失血超过肠道最大吸收能力或完全不耐受口服铁的患者中,胃肠外铁疗法才是合理的。然而,胃肠外铁疗法可能会伴有严重甚至致命的副作用。

相似文献

1
[Microcytic and hypochromic anemias].[小细胞低色素性贫血]
Vnitr Lek. 2001 Mar;47(3):166-74.
2
Serum ferritin in beta-thalassemia trait.β地中海贫血特征患者的血清铁蛋白
Isr J Med Sci. 1978 Nov;14(11):1127-31.
3
Microcytic anemia.小细胞贫血
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4
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[The value of serum ferritin, serum iron and iron-binding capacity in the differential diagnosis of microcytic hypochromic anemia].[血清铁蛋白、血清铁及铁结合能力在小细胞低色素性贫血鉴别诊断中的价值]
Schweiz Med Wochenschr. 1982 Jan 2;112(1):13-7.
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Iron deficiency anemia.缺铁性贫血
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Automated measurement of red blood cell microcytosis and hypochromia in iron deficiency and beta-thalassemia trait.缺铁性贫血和β地中海贫血特征中红细胞小红细胞症和低色素症的自动测量
Arch Pathol Lab Med. 1992 Jan;116(1):84-9.
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[Iron deficiency anaemia: clinical presentation, biological diagnosis and management].[缺铁性贫血:临床表现、生物学诊断及管理]
Transfus Clin Biol. 2007 May;14(1):21-4. doi: 10.1016/j.tracli.2007.04.005. Epub 2007 May 11.
9
Red cell distribution width, free erythrocyte protoporphyrin, and England-Fraser index in the differential diagnosis of microcytosis due to iron deficiency or beta-thalassemia trait. A study of 200 cases of microcytic anemia.红细胞分布宽度、游离红细胞原卟啉及英格兰-弗雷泽指数在缺铁或β地中海贫血特征所致小红细胞症鉴别诊断中的应用。对200例小细胞性贫血的研究。
Hematol Pathol. 1991;5(1):33-6.
10
The measurement of free erythrocyte porphyrin (FEP) as a simple means of distinguishing iron deficiency from beta-thalassemia trait in subjects with microcytosis.测定游离红细胞卟啉(FEP)作为区分小细胞性贫血患者缺铁性贫血与β地中海贫血特征的一种简单方法。
J Lab Clin Med. 1975 Jan;85(1):113-9.