Savage D, Lindenbaum J
Medicine (Baltimore). 1986 Sep;65(5):322-38. doi: 10.1097/00005792-198609000-00005.
In order to develop a diagnostic approach to the common problem of anemia associated with alcoholism, 121 chronic alcoholics admitted to a general medical service with a low hematocrit were evaluated. Multiple contributing causes of anemia were present in most patients. Megaloblastic marrow change was found in 33.9% of patients, sideroblastic change in 23.1%, absent iron stores in 13.2%, aggregated macrophage iron in 81.0%, and acute blood loss in 24.8%. The MCV was of little value in predicting the presence of megaloblastic change unless markedly elevated (greater than 110 fl). In 15 of 41 patients with megaloblastic marrow morphology (36.6%) the MCV was normal or low. Among 40 patients with MCV values between 100 and 110 fl, megaloblastic change was not present in the bone marrow smears of 24 (60.0%). Neutrophil hypersegmentation was 95% specific but only 78% sensitive for megaloblastic change; in contrast, the presence of macroovalocytosis was 90% sensitive but only 68% specific. Serum lactic dehydrogenase, plasma folate, and erythrocyte folate levels had such low sensitivities and specificities for megaloblastic change as to be of little predictive value. Hematologic responses to folic acid were often inadequate in patients with megaloblastic morphologic changes, apparently because of associated acute and chronic illness. Our findings are consistent with the hypothesis that 2 mechanisms account for the development of megaloblastic hematopoiesis in alcoholics: induction of folate deficiency and a direct toxic effect of alcohol on erythroid precursors independent of folate depletion, as reflected by the presence of normal plasma and erythrocyte folate levels in several patients with megaloblastic change. In no patient was sideroblastic change the sole apparent cause of anemia. Megaloblastic hematopoiesis and aggregated macrophage iron frequently accompanied sideroblastic change. Examination of the blood smear revealed siderocytes in one-third of patients with sideroblastic marrows and dimorphic erythrocyte morphology in the majority. Dimorphic blood smears, however, were neither sensitive nor specific for sideroblastic change. Serum iron concentrations were usually not elevated in the group with sideroblastic abnormalities. In predicting marrow iron stores, serum iron and iron-binding capacity concentrations were often non-diagnostic or misleading. Serum ferritin levels less than 100 ng/ml, however, showed 100% sensitivity and 95% specificity for absent marrow iron stores despite the frequent presence of abnormal liver function. On the basis of our findings, practical guidelines have been formulated for the evaluation and therapy of anemia in alcohol
为了制定针对酒精中毒相关常见贫血问题的诊断方法,对121名因血细胞比容低而入住综合内科的慢性酒精中毒患者进行了评估。大多数患者存在多种导致贫血的因素。33.9%的患者出现巨幼细胞性骨髓改变,23.1%出现环形铁粒幼细胞改变,13.2%铁储存缺乏,81.0%出现聚集的巨噬细胞铁,24.8%出现急性失血。除非显著升高(大于110 fl),平均红细胞体积(MCV)对预测巨幼细胞性改变的存在价值不大。在41例具有巨幼细胞性骨髓形态的患者中,有15例(36.6%)的MCV正常或偏低。在40例MCV值在100至110 fl之间的患者中,24例(60.0%)的骨髓涂片未出现巨幼细胞性改变。中性粒细胞核分叶过多对巨幼细胞性改变的特异性为95%,但敏感性仅为78%;相比之下,大卵圆形红细胞的存在敏感性为90%,但特异性仅为68%。血清乳酸脱氢酶、血浆叶酸和红细胞叶酸水平对巨幼细胞性改变的敏感性和特异性很低,几乎没有预测价值。具有巨幼细胞性形态改变的患者对叶酸的血液学反应往往不足,显然是由于伴有急慢性疾病。我们的研究结果与以下假设一致,即酒精中毒患者巨幼细胞性造血的发生有两种机制:叶酸缺乏的诱导以及酒精对红系前体细胞的直接毒性作用,与叶酸缺乏无关,这一点在一些有巨幼细胞性改变的患者中血浆和红细胞叶酸水平正常得到了体现。在任何患者中,环形铁粒幼细胞改变都不是贫血的唯一明显原因。巨幼细胞性造血和聚集的巨噬细胞铁常与环形铁粒幼细胞改变同时出现。血液涂片检查显示,三分之一有环形铁粒幼细胞性骨髓的患者出现铁粒幼红细胞,大多数患者出现双形红细胞形态。然而,双形血涂片对环形铁粒幼细胞改变既不敏感也不特异。环形铁粒幼细胞异常组的血清铁浓度通常不升高。在预测骨髓铁储存方面,血清铁和铁结合能力浓度常常无法诊断或产生误导。然而,血清铁蛋白水平低于100 ng/ml对骨髓铁储存缺乏显示出100%的敏感性和95%的特异性,尽管肝功能异常很常见。基于我们的研究结果,已制定了酒精中毒患者贫血评估和治疗的实用指南
