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达那唑治疗骨髓增生异常综合征。

Danazol treatment of myelodysplastic syndromes.

作者信息

Stadtmauer E A, Cassileth P A, Edelstein M, Abrahm J, Schreiber A D, Nowell P C, Cines D B

机构信息

Department of Medicine, University of Pennsylvania School of Medicine, Philadelphia.

出版信息

Br J Haematol. 1991 Apr;77(4):502-8. doi: 10.1111/j.1365-2141.1991.tb08617.x.

DOI:10.1111/j.1365-2141.1991.tb08617.x
PMID:1827346
Abstract

Peripheral cytopenias are common in patients with myelodysplastic syndromes. We previously successfully treated three such patients with improvement of some cytopenias with the impeded androgen danazol. To confirm this finding and elucidate the mechanism of response, we treated an additional 22 patients with myelodysplasia with oral danazol (600-800 mg daily) for 3-12 months. Eleven of 22 evaluable patients taking danazol met our criteria for improvement of peripheral counts, mainly thrombocytopenia. Chromosome analysis, marrow culture studies and serial bone marrow biopsies revealed no alteration of the abnormal clone or normal haematopoiesis in patients on danazol therapy. This suggested that improvement in blood counts was not related to modulation of ineffective haematopoiesis. Investigation of the thrombocytopenia in these patients revealed that most patients presented with markedly elevated platelet associated IgG (PAIgG), elevated plasma platelet-bindable IgG (PBIgG), and an elevated number of monocyte Fc gamma receptors. Treatment with danazol was associated with a decline in monocyte Fc gamma receptor number without significantly altering the elevated PAIgG or PBIgG levels. These results are similar to our observations in patients treated with danazol for chronic idiopathic thrombocytopenia purpura (ITP). Our data suggest that a component of the thrombocytopenia occurring in patients with myelodysplasia may be due to enhanced peripheral blood cell destruction by abnormal macrophages. Danazol may modulate cytopenia by decreasing the number of monocyte Fc gamma receptors. Danazol treatment was associated with minimal toxicity, but clinically meaningful responses were rare.

摘要

外周血细胞减少在骨髓增生异常综合征患者中很常见。我们之前成功治疗了3例此类患者,使用受阻雄激素达那唑后部分血细胞减少情况有所改善。为了证实这一发现并阐明反应机制,我们用口服达那唑(每日600 - 800毫克)治疗了另外22例骨髓发育异常患者,疗程为3至12个月。在22例可评估的服用达那唑的患者中,有11例达到了外周血细胞计数改善的标准,主要是血小板减少症。染色体分析、骨髓培养研究及系列骨髓活检显示,接受达那唑治疗的患者异常克隆或正常造血功能无改变。这表明血细胞计数的改善与无效造血的调节无关。对这些患者血小板减少症的研究发现,大多数患者血小板相关IgG(PAIgG)显著升高、血浆血小板可结合IgG(PBIgG)升高以及单核细胞Fcγ受体数量增加。达那唑治疗与单核细胞Fcγ受体数量减少相关,而PAIgG或PBIgG升高水平无显著改变。这些结果与我们在用达那唑治疗慢性特发性血小板减少性紫癜(ITP)患者中的观察结果相似。我们的数据表明,骨髓发育异常患者出现的血小板减少症部分可能是由于异常巨噬细胞对外周血细胞破坏增强所致。达那唑可能通过减少单核细胞Fcγ受体数量来调节血细胞减少。达那唑治疗的毒性极小,但临床上有意义的反应很少见。

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Danazol treatment of myelodysplastic syndromes.达那唑治疗骨髓增生异常综合征。
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