Vašeková Petra, Szépe Peter, Marcinek Ján, Balhárek Tomáš, Plank Lukáš
Vnitr Lek. 2016 Fall;62(9):692-697.
Megaloblastic anemia (MA) represents a subtype of macrocytic anemia caused by impaired DNA synthesis, mostly due to folate and vitamin B12 deficiency. Its mildest forms lead to macrocytosis without concomitant anemia, but more severe forms to thrombocytopenia and/or leucopenia as well. In majority of the cases, the diagnosis of MA dose not represent a serious clinical problem, however, other causes of macrocytosis including myelodysplastic syndrome (MDS) must be excluded.
In the period 2004-2015 we identified in our registry 126 consecutive bone marrow (BM) biopsies of patients with cytopenia/s in peripheral blood and suspicion either on MA or MDS of refractory anemia (RA) type. We performed a retrospective analysis of BM biopsies focused on evaluation of parameters useful for the differential diagnosis, as represented by (a) cellularity and proportions of BM precursors, (b) and their topography, (c) presence of maturation defects and dysplastic changes, (d) grade and extent of myelofibrosis, (e) iron deposits and (f) presence of "inflammatory" response in BM. Histological analyses were supported by immunohistochemical examinations.
The series consisted of biopsies of 126 patients (61 men and 65 women) with average age 63 (14-88 years) - almost all patients (121/126) presented with anemia. Based on the findings we distinguished three diagnostic groups - MA (31 patients), MDS-RA (39) and bioptically unclasifiable case ("DIF DG" - 56 patients). Abnormalities of the BM cellularity were observed in 81 % and of topography in 73 % of all cases respectively. Megalobastic differentiation of erythropoesis was detected in 79 % and diagnostic dysplastic changes in 25 % of all biopsy cases. In 29 % of all biopsies ring sideroblasts were present, megakaryocytic nuclear lobulisation defects density changes were found in 61 % of all patients. In 14 % of all biopsies the BM myelofibrosis was absent, in contrast 5 % of the biopsies showed severe diffuse fibrosis. "Inflammatory" response was developed in 44 % of all biopsies. Iron deposits were absent in 26 %, decreased in 35 % and increased in 33 % of all the cases.
From the point of view of histopathologist it seems to be difficult to distinguish BM hematopoietic changes in patients with MA and MDS-RA respectivelly, as histological examinations allowed determination of a definitive and correct diagnosis in about 55% of the cases. The crucial problem represents a decision whether the observed changes really result from the development of a clonal disease.Key words: megaloblastic anemia - megaloblastic differentiation - refractory anemia.
巨幼细胞贫血(MA)是大细胞性贫血的一种亚型,由DNA合成受损引起,主要原因是叶酸和维生素B12缺乏。其最轻微的形式会导致大细胞增多而无伴随贫血,但更严重的形式还会导致血小板减少和/或白细胞减少。在大多数情况下,MA的诊断并非严重的临床问题,然而,必须排除包括骨髓增生异常综合征(MDS)在内的其他大细胞增多的原因。
在2004年至2015年期间,我们在登记处确定了126例连续的骨髓(BM)活检病例,这些患者外周血有血细胞减少,且怀疑患有MA或难治性贫血(RA)型MDS。我们对BM活检进行了回顾性分析,重点评估有助于鉴别诊断的参数,包括(a)BM前体细胞的细胞密度和比例,(b)它们的拓扑结构,(c)成熟缺陷和发育异常变化的存在,(d)骨髓纤维化的程度和范围,(e)铁沉积,以及(f)BM中“炎症”反应的存在。组织学分析得到免疫组织化学检查的支持。
该系列包括126例患者(61名男性和65名女性)的活检,平均年龄63岁(14 - 88岁) - 几乎所有患者(121/126)都有贫血。根据研究结果,我们区分出三个诊断组 - MA(31例患者),MDS - RA(39例)和活检无法分类的病例(“DIF DG” - 56例患者)。分别在81%的所有病例中观察到BM细胞密度异常,73%的病例中观察到拓扑结构异常。在79%的活检病例中检测到红细胞生成的巨幼样分化,25%的病例中有诊断性发育异常变化。在所有活检病例的29%中存在环形铁粒幼细胞,61%的患者中发现巨核细胞核分叶缺陷密度变化。在所有活检病例的14%中未发现BM骨髓纤维化,相反,5%的活检显示严重弥漫性纤维化。44%的活检出现“炎症”反应。在所有病例中,26%没有铁沉积,35%铁沉积减少,而33%铁沉积增加。
从组织病理学家的角度来看,似乎很难分别区分MA和MDS - RA患者的BM造血变化,因为组织学检查仅能在约55%的病例中确定明确且正确的诊断。关键问题在于判断观察到的变化是否真的是由克隆性疾病的发展引起的。关键词:巨幼细胞贫血 - 巨幼样分化 - 难治性贫血
