Pui C H, Rivera G K, Hancock M L, Raimondi S C, Sandlund J T, Mahmoud H H, Ribeiro R C, Furman W L, Hurwitz C A, Crist W M
Department of Hematology-Oncology, St Jude Children's Research Hospital, Memphis, TN 38101.
Leukemia. 1993 Jan;7(1):35-40.
The independent significance of CD10 expression in childhood acute lymphoblastic leukemia (ALL) is uncertain because most studies have not adjusted for other risk features, such as age and immunophenotype, or for treatment effects. We reassessed the clinical importance of CD10 expression in patients who received highly effective contemporary treatment. CD10 antigen was detected in blast cells from 384 of 408 patients (94%) with B-lineage ALL and 36 of 90 (40%) with T-cell ALL. In the B-lineage subgroup, CD10 expression was associated with favorable presenting features: age > or = 1 year, lower leukocyte count (< 50 x 10(9)/l), and leukemic cell DNA index > or = 1.16 or hyperdiploidy > 50 chromosomes. One-half of the patients with CD10- B-lineage ALL had 11q23 chromosomal abnormalities. Separate analysis of the marker in T-cell ALL revealed no differences between CD10+ and CD10- cases in clinical features or karyotypic patterns, with the exception of a lower frequency of central nervous system leukemia and a higher frequency of 9p abnormalities in the former subgroup. CD10+ T-cell cases were also significantly more likely than CD10- cases to coexpress CD21, CD1, CD4, or CD8. Lack of CD10 expression was independently associated with an adverse prognosis in T-cell ALL (p = 0.02). However, for the larger subgroup of patients with B-lineage ALL, CD10 expression has no independent prognostic significance.
CD10表达在儿童急性淋巴细胞白血病(ALL)中的独立意义尚不确定,因为大多数研究未对其他风险特征(如年龄和免疫表型)或治疗效果进行校正。我们重新评估了接受高效现代治疗的患者中CD10表达的临床重要性。在408例B系ALL患者中的384例(94%)和90例T细胞ALL患者中的36例(40%)的原始细胞中检测到CD10抗原。在B系亚组中,CD10表达与良好的就诊特征相关:年龄≥1岁、白细胞计数较低(<50×10⁹/L)、白血病细胞DNA指数≥1.16或超二倍体>50条染色体。一半的CD10⁻ B系ALL患者存在11q23染色体异常。对T细胞ALL中该标志物的单独分析显示,CD10⁺和CD10⁻病例在临床特征或核型模式上无差异,但前者亚组中枢神经系统白血病的发生率较低,9p异常的发生率较高。CD10⁺ T细胞病例也比CD10⁻病例更有可能共表达CD21、CD1、CD4或CD8。CD10表达缺失与T细胞ALL的不良预后独立相关(p = 0.02)。然而,对于更大的B系ALL患者亚组,CD10表达没有独立的预后意义。
