Pure red cell aplasia evolving through the hyperfibrotic myelodysplastic syndrome to the acute myeloid leukemia: some pathogenetic aspects.

Hematology and cell therapy Pub Date : 1999-02-01 DOI:10.1007/s00282-999-0027-5

N Suvajdzic, D Marisavljevic, V Jovanovic, M Pantic, D Sefer, M Colovic

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引用次数: 6

Abstract

The authors report a 58-year-old female who originally presented with acquired pure red cell aplasia (PRCA). At diagnosis, the karyotype was normal, the serum erythropoietin level was highly elevated and no T-cell mediated inhibition of erythropoiesis was demonstrated in coculture studies. Conventional immunosuppressive therapy proved ineffective. A year later a diagnosis of hyperfibrotic myelodysplastic syndrome was assessed. The sequential bone marrow examinations in the course of the three years showed a progressive increase in bone marrow fibrosis, erythroid hyperplasia and dysmegakaryocytopoiesis, terminating in the acute myeloid leukemia. This sequence of the events included the appearance of del(5)(q13q33), four years after setting a diagnosis of PRCA. The authors suggest that the absence of both cytogenetic abnormality and the signs of dyshematopoiesis at the diagnosis of PRCA does not exclude ultimately a "clonal" category of the disease. Thus, repeated hematological and cytogenetical reevaluations are recommended.

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纯红细胞发育不全，从增生性骨髓增生异常综合征发展到急性髓性白血病:一些发病方面。

作者报告了一位58岁的女性，她最初表现为获得性纯红细胞发育不全(PRCA)。诊断时，核型正常，血清促红细胞生成素水平高，共培养研究未发现t细胞介导的红细胞生成抑制。常规免疫抑制治疗无效。一年后诊断为增生性骨髓增生异常综合征。三年间的连续骨髓检查显示骨髓纤维化、红细胞增生和巨核异常增生逐渐增加，最终发展为急性髓性白血病。这一系列事件包括在诊断为PRCA四年后出现del(5)(q13q33)。作者认为，在诊断PRCA时没有细胞遗传学异常和造血障碍的迹象，并不能最终排除该疾病的“克隆”类别。因此，建议反复进行血液学和细胞遗传学重新评估。

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Hematology and cell therapy

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