flt3 -内串联重复在儿童t(8;21)急性髓性白血病患者中的应用

Machiko Kawamura , Hidefumi Kaku , Tateki Ito , Nobuaki Funata , Tomohiko Taki , Akira Shimada , Yasuhide Hayashi
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引用次数: 8

摘要

诊断为t(8;21)-急性髓性白血病(AML)的患者目前被认为预后良好,但这些患者中约有一半复发。flt3 -内部串联重复(ITD)通常被认为与AML预后不良密切相关,但在t(8;21)-AML患者中很少报道。神经细胞粘附分子(CD56)的表达也与t(8;21)-AML患者的完全缓解持续时间和生存时间显著缩短有关。据报道,表达CD56的t(8;21)-AML患者表现出更高的粒细胞肉瘤(GS)发病率,t(8;21)-AML合并GS的预后不如单纯这种易位的AML。在这里,我们报告了一个15岁的女孩患有t(8;21)-AML,同时表达CD56和FLT3-ITD。该患者行非亲属供体骨髓移植后病情完全缓解,但复发时出现GS压迫胆总管所致梗阻性黄疸,无骨髓侵犯。尸检显示胃粘膜多发结节,并侵犯胰腺头部。为了更早地发现复发,我们建议在诊断和血液缓解时检查cd56阳性t(8;21)-AML患者是否存在GS是有用的。尽管t(8;21)-AML在儿科患者中与FLT3- itd同时发生的可能性较小,但本报告建议应分析这些患者的预后因素,包括FLT3和KIT基因以及表面标记物CD56。
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FLT3-internal tandem duplication in a pediatric patient with t(8;21) acute myeloid leukemia

Patients diagnosed with t(8;21)-acute myeloid leukemia (AML) are currently considered to have good prognoses, but about half of these patients relapse. FLT3-internal tandem duplication (ITD) is generally thought to be strongly associated with poor prognosis in AML, but is rarely reported in patients with t(8;21)-AML. Expression of the neural cell-adhesion molecule (CD56) is also associated with a significantly shorter complete remission duration and survival in patients with t(8;21)-AML. Patients with t(8;21)-AML expressing CD56 have been reported to exhibit a higher incidence of granulocytic sarcoma (GS), and t(8;21)-AML with GS results in a less favorable prognosis than AML with this translocation alone. Here, we report on a 15-year-old girl with t(8;21)-AML having both CD56 expression and FLT3-ITD. This patient underwent unrelated donor bone marrow transplantation and achieved complete remission, but thereafter presented with obstructive jaundice caused by GS compression of the common bile duct without bone marrow invasion at relapse. Autopsy revealed multiple nodules of the stomach membrane and invasion into the head of the pancreas. For earlier detection of relapse, we suggest that it would be useful to examine existence of GS in CD56-positive t(8;21)-AML patients at diagnosis and hematologic remission. Even though t(8;21)-AML is less likely to co-occur with FLT3-ITD in pediatric patients, this report suggests that prognostic factors, including FLT3 and KIT genes and the surface marker CD56, should be analyzed in these patients.

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