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成人及儿童急性早幼粒细胞白血病的免疫表型:与形态学、PML基因断点类型及临床结果的相关性。一项对196例病例的意大利合作研究。

Immunophenotype of adult and childhood acute promyelocytic leukaemia: correlation with morphology, type of PML gene breakpoint and clinical outcome. A cooperative Italian study on 196 cases.

作者信息

Guglielmi C, Martelli M P, Diverio D, Fenu S, Vegna M L, Cantù-Rajnoldi A, Biondi A, Cocito M G, Del Vecchio L, Tabilio A, Avvisati G, Basso G, Lo Coco F

机构信息

Dipartimento di Biotecnologie Cellulari ed Ematologia, Università degli Studi La Sapienza, Roma, Italy.

出版信息

Br J Haematol. 1998 Sep;102(4):1035-41. doi: 10.1046/j.1365-2141.1998.00871.x.

Abstract

Acute promyelocytic leukaemia (APL), characterized by a specific PML-RARalpha fusion gene resulting from translocation t(15;17) and by a high response rate to differentiation therapy with all-trans retinoic acid, presents clinical (varying WBC counts, age and treatment outcome), morphological (hypergranular M3 and hypogranular M3V) and molecular (three isoforms of PML breakpoint) heterogeneity. We correlated leukaemic immunophenotype with these aspects in 196 molecularly confirmed APLs (63 children and 133 adults) in Italy. The bcr3 isoform (P = 0.05) and FAB M3V (P = 0.05) were more frequent in children. We confirmed in APL an immunophenotype characterized by frequent expression of CD13, CD33 and CD9 and rare expression of HLA-DR, CD10, CD7 and CD11b. However, we recognized CD2 in 28%, CD34 in 23% and CD19 in 11% of cases and demonstrated by double labelling that CD34 and CD2 may be co-expressed. CD2, CD34 and CD19 were significantly intercorrelated, and variably associated to other features: CD2 and CD34 with PML bcr3 (P < 0.001 and P < 0.001, respectively) and with M3V (P < 0.001 and P = 0.002), whereas only CD19 was directly correlated with WBC counts and only CD2 positively influenced CR rate (logistic model) and event-free survival (Cox model). We conclude that immunophenotype plays a role in the determination of the biological and clinical heterogeneity of childhood and adult APL.

摘要

急性早幼粒细胞白血病(APL)的特征是由t(15;17)易位产生特定的PML-RARα融合基因,且对全反式维甲酸分化疗法有较高的反应率,它存在临床(白细胞计数、年龄和治疗结果各异)、形态学(颗粒增多的M3型和颗粒减少的M3V型)和分子(PML断点的三种异构体)异质性。我们在意大利对196例经分子确诊的APL患者(63例儿童和133例成人)的白血病免疫表型与这些方面进行了相关性研究。bcr3异构体(P = 0.05)和FAB M3V型(P = 0.05)在儿童中更为常见。我们证实APL的免疫表型特征为CD13、CD33和CD9表达频繁,而HLA-DR、CD10、CD7和CD11b表达罕见。然而,我们在28%的病例中识别出CD2,23%的病例中识别出CD34,11%的病例中识别出CD19,并通过双重标记证明CD34和CD2可能共表达。CD2、CD34和CD19显著相互关联,并与其他特征存在不同程度的关联:CD2和CD34与PML bcr3(分别为P < 0.001和P < 0.001)以及M3V(分别为P < 0.001和P = 0.002)相关,而只有CD19与白细胞计数直接相关,只有CD2对完全缓解率(逻辑模型)和无事件生存期(Cox模型)有正向影响。我们得出结论,免疫表型在儿童和成人APL的生物学和临床异质性的决定中起作用。

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