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儿童t(8;21)(q22;q22)急性髓系白血病的独特免疫表型特征

Distinctive immunophenotypic features of t(8;21)(q22;q22) acute myeloblastic leukemia in children.

作者信息

Hurwitz C A, Raimondi S C, Head D, Krance R, Mirro J, Kalwinsky D K, Ayers G D, Behm F G

机构信息

Department of Pathology, St Jude Children's Research Hospital, Memphis, TN 38101-0318.

出版信息

Blood. 1992 Dec 15;80(12):3182-8.

PMID:1467524
Abstract

Thirty cases of newly diagnosed pediatric acute myeloblastic leukemia (AML) with French-American-British (FAB) M2 morphology were analyzed with cytogenetics and a comprehensive panel of monoclonal antibodies reactive with lymphoid-, natural killer (NK)-cell-, and myeloid-associated antigens. The t(8;21)(q22;q22), or t(8;21;V)(q22;q22;V), translocation was identified in 16 of the 30 cases. Cases with the t(8;21) did not differ significantly from the remaining M2 cases with respect to expression of CD11b, CD13, CD14, CD15, CD33, CD34, CD36, CD41a, CD42b, CDw65, TdT, or HLA-DR. Expression of the B-cell antigen CD19 was detected in 13 of the 16 t(8;21) cases (81%), but in only 1 of the 14 (7%) other M2 cases (P = .00006). Expression of the CD56 NK-cell antigen was also significantly more frequent among t(8;21) cases (63% v 14%; P = .01). Coexpression of CD19 and CD56 was found only in the t(8;21) group (9 of 16 cases, P = .0009). Furthermore, this phenotype was not found in 48 evaluable cases of de novo AML of the FAB M1, M3, M4, M5, or M7 subtypes. The 14 M2 AML cases lacking the t(8;21) commonly expressed CD2 (n = 5) or CD7 (n = 8). However, no case with the t(8;21) expressed either antigen (P = .01 and .0005, respectively). Thus, the t(8;21) biologic subgroup of pediatric M2 AML has distinct immunophenotypic characteristics that distinguish it from other types of de novo AML.

摘要

采用细胞遗传学和一组全面的与淋巴样、自然杀伤(NK)细胞及髓系相关抗原反应的单克隆抗体,对30例新诊断的具有法美英(FAB)M2形态学特征的儿童急性髓细胞白血病(AML)进行分析。在30例病例中,有16例检测到t(8;21)(q22;q22)或t(8;21;V)(q22;q22;V)易位。t(8;21)病例在CD11b、CD13、CD14、CD15、CD33、CD34、CD36、CD41a、CD42b、CDw65、TdT或HLA-DR表达方面与其余M2病例无显著差异。在16例t(8;21)病例中有13例(81%)检测到B细胞抗原CD19表达,但在14例其他M2病例中仅1例(7%)有表达(P = 0.00006)。CD56 NK细胞抗原在t(8;21)病例中的表达也明显更常见(63%对14%;P = 0.01)。CD19和CD56共表达仅在t(8;21)组中发现(16例中有9例,P = 0.0009)。此外,在48例可评估的FAB M1、M3、M4、M5或M7亚型的初发AML病例中未发现此表型。14例缺乏t(

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