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首页> 外文期刊>Leukemia Research: A Forum for Studies on Leukemia and Normal Hemopoiesis >CD10 and CD19 fluorescence intensity of B-cell precursors in normal and leukemic bone marrow. Clinical characterization of CD10(+strong) and CD10(+weak) common acute lymphoblastic leukemia.
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CD10 and CD19 fluorescence intensity of B-cell precursors in normal and leukemic bone marrow. Clinical characterization of CD10(+strong) and CD10(+weak) common acute lymphoblastic leukemia.

机译:正常和白血病骨髓中B细胞前体的CD10和CD19荧光强度。 CD10(+ strong)和CD10(+ weak)常见急性淋巴细胞白血病的临床特征。

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摘要

In order to assess the age-related changes in CD10 and CD19 fluorescence intensity (FI) the present study analyzed by flow cytometry 56 sternal biopsies from 'normal' infants, children and adults undergoing cardiac surgery. The CD10(+weak) subset was predominant in all age groups, representing approximately 50% of the bone marrow (BM) lymphoid cells in children younger than 4 years. Both CD10+ subsets significantly decreased with age but their ratio did not differ significantly. Moreover, the intensity of CD10 and CD19 fluorescence in the strong and weak subsets did not vary with age. The CD19 intensity was significantly higher in CD10(+weak) than in CD10(+strong) cells. In addition, we classified as CD10(+weak) or CD10(+strong) the leukemic cells from BM aspirates of 117 patients with common acute lymphoblastic leukemia (cALL) (78 children and 39 adults). A higher frequency of cases expressing the CD19+ CD10(+strong) phenotype was observed both in children and adults. Children of the CD10(+weak) group tended to be older than those of the CD10(+strong) group (median = 7 vs. 4 years, P = 0.07), and presented a significantly higher frequency of splenomegaly (93.7 vs. 55%, P = 0.04), which was massive in about 60% of these cases. Among adults, a significantly higher frequency of cases expressing the CD10(+weak) phenotype was observed in females. No other clinical or biological difference was detected between the two groups either for children or adults. Concerning the treatment outcome, we did not observe significant differences in complete remission rate (CRR) or in disease free survival (DFS) among the 32 children and 28 adults analyzed. Finally, we compared the CD10 and CD19 intensity in normal and leukemic BM. Overexpression of either or both antigens in leukemic cells was observed in 42.4% of the cALL cases. In these cases, using cut off values of 110 afu for the CD10 FI and of 100 afu for the CD19 FI, the detection of leukemic cells was possible at levels of 0.2% based on CD10 analysis, of 0.6% based on CD19, and 0.02% when both antigens were overexpressed. In conclusion, we demonstrated that the heterogeneity of CD10 and CD19 fluorescence intensity is of no clinical relevance in cALL, although its study may be helpful for the diagnosis and the detection of minimal residual disease.
机译:为了评估与年龄相关的CD10和CD19荧光强度(FI)的变化,本研究通过流式细胞术对来自接受心脏手术的“正常”婴儿,儿童和成人的56胸骨活检进行了分析。 CD10(+弱)亚群在所有年龄组中均占主导地位,约占4岁以下儿童骨髓(BM)淋巴样细胞的50%。两种CD10 +亚型均随年龄显着下降,但其比例无显着差异。此外,强和弱子集中的CD10和CD19荧光强度不随年龄而变化。 CD10(+弱)中的CD19强度显着高于CD10(+强)细胞中。此外,我们将117例常见的急性淋巴细胞白血病(cALL)患者的BM抽吸物中的白血病细胞归类为CD10(+弱)或CD10(+ strong)(78名儿童和39名成人)。在儿童和成人中,观察到较高表达CD19 + CD10(+ strong)表型的病例。 CD10(+弱)组的孩子往往比CD10(+ strong)组的孩子大(中位数= 7 vs. 4岁,P = 0.07),脾肿大的频率明显更高(93.7 vs 55)。 %,P = 0.04),在这些案例中约有60%占很大比例。在成年人中,女性中观察到表达CD10(+弱)表型的病例的频率明显更高。在儿童或成人这两组之间未检测到其他临床或生物学差异。关于治疗结果,我们在分析的32名儿童和28名成人中,未观察到完全缓解率(CRR)或无病生存期(DFS)的显着差异。最后,我们比较了正常和白血病BM中的CD10和CD19强度。在42.4%的cALL病例中观察到白血病细胞中一种或两种抗原的过表达。在这些情况下,对于CD10 FI,使用110 afu的截止值,对于CD19 FI,使用100 afu的截止值,根据CD10分析,检测白血病细胞的水平为0.2%,基于CD19的检测水平为0.6%,而0.02两种抗原均过表达时的%。总之,我们证明了CD10和CD19荧光强度的异质性在cALL中没有临床意义,尽管其研究可能有助于诊断和发现最小残留病。

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