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末端脱氧核苷酸转移酶阳性亚群存在于大多数急性非淋巴细胞白血病中:对微小疾病检测的意义。

Terminal deoxynucleotidyl transferase positive subpopulations occur in the majority of ANLL: implications for the detection of minimal disease.

作者信息

Adriaansen H J, van Dongen J J, Kappers-Klunne M C, Hählen K, van 't Veer M B, Wijdenes-de Bresser J H, Holdrinet A C, Harthoorn-Lasthuizen E J, Abels J, Hooijkaas H

机构信息

Department of Immunology, University Hospital Dijkzigt/Erasmus University, Rotterdam, The Netherlands.

出版信息

Leukemia. 1990 Jun;4(6):404-10.

PMID:2359340
Abstract

A series of 60 acute nonlymphocytic leukemias (ANLL) was analyzed for the expression of terminal deoxynucleotidyl transferase (TdT). The detected TdT+ cells were studied in detail by use of double marker analyses for TdT and differentiation markers, such as myeloid markers (CD13 and CD33), B cell markers, T cell markers, and the precursor antigen CD34. In 15 (25%) of these leukemic cell samples, we found no TdT+ cells or low percentages of CD10+TdT+ cells; the latter probably represent precursor B cells. In the other 45 (75%) ANLL myeloid marker+TdT+ CD10- cells were detected, ranging from 0.1-10% (n = 24) or over 10% (n = 21) of mononuclear cells. Interestingly, a higher frequency of CD34 positivity was found on the TdT+ cells as compared to the TdT- cells, suggesting that the TdT+ cells represent an immature leukemic subpopulation. Therefore, it may be speculated that the TdT+ subpopulation contains the clonogenic ANLL cells. In two patients, in whom immunologic marker analysis was performed at initial diagnosis as well as at relapse, an expansion of the TdT+ subpopulation was documented at relapse, which may reflect a reduced differentiation capacity of the leukemic cells. Previous studies on a series of nonleukemic bone marrow and blood samples revealed that normal counterparts of myeloid marker+TdT+ cells are rare in bone marrow (less than 0.03%, if they occur at all) and that such cells are not detectable in blood. Therefore myeloid marker TdT double stainings may be useful to monitor the TdT+ leukemic subpopulation in patients with a TdT+ ANLL during and after chemotherapy. Our preliminary results on the follow-up of two such patients support this hypothesis.

摘要

对60例急性非淋巴细胞白血病(ANLL)进行了末端脱氧核苷酸转移酶(TdT)表达分析。通过对TdT与分化标志物(如髓系标志物(CD13和CD33)、B细胞标志物、T细胞标志物以及前体抗原CD34)进行双重标记分析,对检测到的TdT+细胞进行了详细研究。在这些白血病细胞样本中,有15例(25%)未发现TdT+细胞或CD10+TdT+细胞比例较低;后者可能代表前体B细胞。在另外45例(75%)ANLL中,检测到髓系标志物+TdT+CD10-细胞,占单核细胞的0.1 - 10%(n = 24)或超过10%(n = 21)。有趣的是,与TdT-细胞相比,TdT+细胞上CD34阳性频率更高,表明TdT+细胞代表一个不成熟的白血病亚群。因此,可以推测TdT+亚群包含克隆性ANLL细胞。在两名患者中,初诊及复发时均进行了免疫标志物分析,复发时记录到TdT+亚群扩大,这可能反映白血病细胞分化能力降低。先前对一系列非白血病骨髓和血液样本的研究表明,骨髓中髓系标志物+TdT+细胞的正常对应物很少见(如果存在,也少于0.03%),血液中无法检测到此类细胞。因此,髓系标志物与TdT双重染色可能有助于在化疗期间及化疗后监测TdT+ANLL患者的TdT+白血病亚群。我们对两名此类患者随访的初步结果支持这一假设。

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