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慢性髓性白血病髓系细胞和祖细胞上N-CAM(CD56)黏附分子的异常表达

Abnormal expression of N-CAM (CD56) adhesion molecule on myeloid and progenitor cells from chronic myeloid leukemia.

作者信息

Lanza F, Bi S, Castoldi G, Goldman J M

机构信息

LRF Centre for Adult Leukaemia, RPMS, Hammersmith Hospital, London, UK.

出版信息

Leukemia. 1993 Oct;7(10):1570-5.

PMID:7692192
Abstract

Bone marrow and peripheral blood samples from 36 patients with Philadelphia chromosome positive chronic myelogenous leukemia (Ph+ CML) (30 in chronic phase, four in accelerated phase, and two in blastic crisis) were tested with two CD56 monoclonal antibodies (My31 and Eric 1) using the Facscan flow cytometer. Two- and three-color fluorescence experiments indicated that CD13+/CD33+ myeloid cells from 19 out of the 36 patients were positive for CD56 in 12-77% of the cells. In contrast, no CD56 positivity was documented in myeloid cells from bone marrow (BM) of healthy donors. Immunocytochemical staining (APAAP technique) of CML peripheral blood (PB) and BM slides showed that CD56 expression was detectable from the myelocyte stage with the strongest staining in the metamyelocyte stage. Neutrophils were negative both by flow cytometry and APAAP analysis. In individual CML patients, an increasing number of CD56+ cells were recovered with progressively higher density cuts (1.065-1.077 g/ml), supporting the concept that the antigen level tends to increase during myeloid differentiation. Furthermore, 19% of CML patients coexpressed CD56 and CD34 antigens in 10-45% of the CD34+ cells. The myeloid nature of CD56+/CD34+ CML cells has been ascertained by granulocyte-macrophage colony-forming unit (CFU-GM) assays on CD56+ cells sorted on FACS. Furthermore, in six out of eight CML patients in whom we performed a comparative BM and PB analysis, we found that the CD56 expression was brighter and the number of positive cells significantly higher in the peripheral blood myeloid cells as compared to their BM counterpart. In short-term liquid cultures, low doses (50 U/ml) of alpha interferon down-regulated the CD56 expression in CML cells, accompanied by a significant reduction of the Ph positivity. In conclusion, the expression of CD56 on CML myeloid elements seems to represent an aberrant phenomenon which could affect the cell homing mechanisms and, probably, the pattern of tumor cell dissemination. In patients with CD56+ CML, its detection could be further used as a means of monitoring patients undergoing bone marrow transplantation, since its reappearance is associated with early relapse of the disease.

摘要

采用流式细胞仪,使用两种CD56单克隆抗体(My31和Eric 1)对36例费城染色体阳性慢性粒细胞白血病(Ph + CML)患者(慢性期30例、加速期4例、急变期2例)的骨髓和外周血样本进行检测。双色和三色荧光实验表明,36例患者中有19例的CD13 + / CD33 + 髓系细胞中,12% - 77%的细胞CD56呈阳性。相比之下,健康供者骨髓(BM)中的髓系细胞未发现CD56阳性。对CML外周血(PB)和BM涂片进行免疫细胞化学染色(APAAP技术)显示,从髓细胞阶段即可检测到CD56表达,在晚幼粒细胞阶段染色最强。中性粒细胞通过流式细胞术和APAAP分析均为阴性。在个别CML患者中,随着密度梯度离心(1.065 - 1.077 g/ml)密度的增加,回收的CD56 + 细胞数量增多,支持了抗原水平在髓系分化过程中趋于增加的观点。此外,19%的CML患者在10% - 45%的CD34 + 细胞中共表达CD56和CD34抗原。通过对FACS分选的CD56 + 细胞进行粒细胞 - 巨噬细胞集落形成单位(CFU - GM)检测,确定了CD56 + / CD34 + CML细胞的髓系性质。此外,在我们进行比较BM和PB分析的8例CML患者中的6例中,我们发现外周血髓系细胞中的CD56表达比其BM对应细胞更亮,阳性细胞数量显著更高。在短期液体培养中,低剂量(50 U/ml)的α干扰素可下调CML细胞中的CD56表达,同时Ph阳性显著降低。总之,CML髓系成分上CD56的表达似乎代表一种异常现象,可能影响细胞归巢机制,也可能影响肿瘤细胞播散模式。在CD56 + CML患者中,其检测可进一步用作监测接受骨髓移植患者的手段,因为其再次出现与疾病早期复发相关。

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