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Clinical Review on Features and Cytogenetic Patterns in Adult Acute Myeloid Leukemia with Lymphoid Markers

 

作者: CuneoAntonio,   FerrantAugustin,   LouisJean,   BoogaertsMarc,   DemuynckHilde,   BoslyAndre,   DoyenChantal,   CarliM. Gretel,   PivaNadia,   CastoldiGianluigi,   StulMichel,   CinPaola Dal,   CassimanJean Jacques,   Van Den BergheHerman,  

 

期刊: Leukemia&Lymphoma  (Taylor Available online 1993)
卷期: Volume 9, issue 4-5  

页码: 285-291

 

ISSN:1042-8194

 

年代: 1993

 

DOI:10.3109/10428199309148525

 

出版商: Taylor&Francis

 

关键词: Hybrid acute Leukemia;chromosome;immunophenotype

 

数据来源: Taylor

 

摘要:

Cytogenetic patterns in correlation with cytologic, biomolecular and clinical findings were studied in 45 adult patients with AML expressing at least one of the following lymphoid associated markers (LM): CD2, CD7, CD10, CD19, CD22, TdT. Four cytogenetic groups were recognized: group I, including 8 patients with 11q23 rearrangements; group II including S patients with the Ph chromosome; group III, with 19 patients and aberrations of the“myeloid type”including 4 cases with aberrations of chromosome 13, 3 cases with lq and 7q anomalies, 2 cases with trisomy 1 lq; group IV, including 13 patients with normal karyotype.Patients showing extensive lineage infidelity were encountered more frequently in cytogenetic groups I and II than in groups III and IV. Two of 4 cases with aberrations of chromosome 13 showed two or more lymphoid features either at immunophenotyping or at biomolecular analysis of the configuration of lg and TCR genes. Patients with 1 Iq23 rearrangements and with the Ph chromosome were generally young, presented with high WBC count and had low complete remission rate. Survival in Ph chromosome positive patients was uniformly short. We conclude that, although there is no cytogenetic anomaly specific for AML with LM, chromosome findings may be clinically relevant in AML with LM. A morphologic, immunologic and cytogenetic classification of AML with LM may constitute a working basis for future studies aimed at a better definiton of clinicopathological features and optimal treatment strategy for these leukemias.

 

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