儿童中度再生障碍性贫血的预后。

Z Khatib, J Wilimas, W Wang
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引用次数: 0

摘要

目的:为了帮助管理新诊断的中度再生障碍性贫血(MAA)儿童,我们回顾了过去12年来在我院就诊的中度再生障碍性贫血(MAA)儿童的临床病程和预后,并将其与重度再生障碍性贫血(SAA)儿童进行了比较。患者和方法:MAA定义为骨髓细胞减少和至少两个细胞系细胞减少,但不属于严重范围。有12个孩子符合这些标准。在同一时间间隔内观察了28名患有SAA的儿童。MAA患者如果进展为SAA,则使用抗胸腺细胞球蛋白和/或环孢素进行免疫调节。结果:5例MAA患者在诊断后的中位间隔18个月进展为SAA。其他7例患者在诊断后<或= 6个月不需要治疗或仅接受输血。MAA患者的生存期明显优于免疫调节治疗的SAA患者(p = 0.022)。所有MAA患者中位随访时间为7年,且不依赖输血;目前只有一名患者接受治疗。MAA患儿残留的血液学异常包括血小板减少、白细胞减少和巨噬细胞增多。结论:在这个小系列的MAA患儿中,结果非常好,明显好于SAA患者;一半以上的患者只接受少量治疗或不接受治疗就康复了。进展为SAA的患者对治疗反应良好。需要更大的前瞻性研究来确定MAA的自然历史。
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Outcome of moderate aplastic anemia in children.

Purpose: In order to assist in the management of newly diagnosed children with moderate aplastic anemia (MAA) we reviewed the clinical course and outcome of children with MAA seen at our institution over the past 12 years and compared them with children with severe aplastic anemia (SAA).

Patients and methods: MAA was defined as having a hypocellular bone marrow and cytopenia in at least two cell lines not in the severe range. Twelve children met these criteria. Twenty-eight children with SAA were seen during the same interval. Patients with MAA were treated with immunomodulation with antithymocyte globulin and/or cyclosporine if they progressed to SAA.

Results: Five patients with MAA progressed to SAA at a median interval of 18 months from diagnosis. The other seven patients required no therapy or only received transfusions for < or = 6 months after diagnosis. The survival of the patients with MAA was significantly better than that of patients with SAA treated with immunomodulation (p = 0.022). All patients with MAA are alive at a median follow up of 7 years and are transfusion independent; only one patient currently receives therapy. Residual hematologic abnormalities in children with MAA included thrombocytopenia, leukopenia, and macrocytosis.

Conclusions: In this small series of children with MAA the outcome was excellent and significantly better than in patients with SAA; more than half recovered with minimal or no therapy. Patients who progressed to SAA responded well to treatment. A larger prospective study is needed to conclusively define the natural history of MAA.

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