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首页> 外文期刊>Disease markers >The Relationship between Clinical Feature, Complex Immunophenotype, Chromosome Karyotype, and Outcome of Patients with Acute Myeloid Leukemia in China
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The Relationship between Clinical Feature, Complex Immunophenotype, Chromosome Karyotype, and Outcome of Patients with Acute Myeloid Leukemia in China

机译:中国急性髓细胞性白血病患者临床特征,复杂免疫表型,染色体核型与结果的关系

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Mixed phenotype acute leukemia (MPAL) is a complex entity expressing both lymphoid and myeloid immunophenotyping. In the present study, 47 MPAL, 60 lymphoid antigen-positive acute myeloid leukemia (Ly+AML), and 90 acute myeloid leukemia with common myeloid immunophenotype (Ly−AML) patients were investigated. We found that, in MPAL patients, there were high proportions of blast cells in bone marrow and incidence of hepatosplenomegaly, lymphadenopathy, and Philadelphia chromosome. The overall survival (OS) and relapse-free survival (RFS) in MPAL patients were significantly shorter than those in Ly+AML and Ly−AML. With regard to the patients with normal karyotype only, the OS and RFS of MPAL were significantly lower than those of the Ly+AML and Ly−AML; but there were no significant differences in OS and RFS among the patients with complex karyotype. The OS rates of 3 groups with complex karyotype were lower than those of patients with normal karyotype. In Cox multivariate analysis, complex karyotype was an independent pejorative factor for both OS and RFS. Therefore, MPAL is confirmed to be a poor-risk disease while Ly+AML does not impact prognosis. Complex karyotype is an unfavorable prognosis factor in AML patients with different immunophenotype. Mixed immunophenotype and complex karyotype increase the adverse risk when they coexist.
机译:混合表型急性白血病(MPAL)是表达淋巴样和髓样免疫表型的复杂实体。在本研究中,研究了47例MPAL,60例淋巴样抗原阳性的急性髓性白血病(Ly + AML)和90例具有常见髓样免疫表型(Ly-AML)的急性髓性白血病。我们发现,在MPAL患者中,骨髓中的原始细胞比例很高,肝脾肿大,淋巴结病和费城染色体的发生率也很高。 MPAL患者的总生存期(OS)和无复发生存期(RFS)明显短于Ly + AML和Ly-AML。仅对于核型正常的患者,MPAL的OS和RFS显着低于Ly + AML和Ly-AML。但复杂核型患者的OS和RFS无明显差异。 3组复杂核型的OS率低于正常核型患者。在Cox多变量分析中,复杂的核型是OS和RFS的独立贬义因子。因此,MPAL被证实是一种低危疾病,而Ly + AML不影响预后。在具有不同免疫表型的AML患者中,复杂的核型是不利的预后因素。免疫表型和复杂核型混合存在时,会增加不良反应。

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