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原发性白血病前期综合征中的自然杀伤(NK)细胞活性和抗体依赖性细胞毒性(ADCC)

Natural killer (NK)-cell activity and antibody-dependent cellular cytotoxicity (ADCC) in primary preleukemic syndrome.

作者信息

Kerndrup G, Meyer K, Ellegaard J, Hokland P

出版信息

Leuk Res. 1984;8(2):239-47. doi: 10.1016/0145-2126(84)90147-4.

Abstract

In 13 patients with a multi-parameter based diagnosis of primary acquired preleukemic syndrome (PPS), natural killer (NK) cell activity and antibody-dependent cellular cytotoxicity (ADCC) were investigated on peripheral blood mononuclear cell (MNC) fractions. In all but two patients a defective NK activity was found. Lymphocyte-monocyte mixture experiments demonstrated that this was not due to suppressor monocytes. Furthermore, NK activity was defective when both myeloid and non-myeloid target cell lines were used. Addition of human leukocyte interferon to the NK cultures augmented the cytotoxicity, which exhibited the same kinetics as that of normal controls, but NK activity levels remained subnormal. These data strongly indicate that the decreased NK activity seen in the patients is due to a decreased number of circulating NK cells. In contrast ADCC was within the normal range both when MNC suspensions as well as when purified peripheral blood lymphocytes were used as effector cells thus ruling out subnormal lymphocyte ADCC masked by the presence of monocyte ADCC. These results demonstrate that PPS patients have a selective NK defect with an intact lymphocyte ADCC function. Whether this defect will prove to be valuable in the assessment of a malignant transformation in a given patient will await further longitudinal NK studies and clinical follow-up of the patients.

摘要

在13例基于多参数诊断为原发性获得性白血病前期综合征(PPS)的患者中,对外周血单个核细胞(MNC)组分的自然杀伤(NK)细胞活性和抗体依赖性细胞毒性(ADCC)进行了研究。除2例患者外,其余所有患者均发现NK活性缺陷。淋巴细胞-单核细胞混合实验表明,这并非由于抑制性单核细胞所致。此外,当使用髓系和非髓系靶细胞系时,NK活性均有缺陷。向NK培养物中添加人白细胞干扰素可增强细胞毒性,其表现出与正常对照相同的动力学,但NK活性水平仍低于正常。这些数据强烈表明,患者中观察到的NK活性降低是由于循环NK细胞数量减少所致。相比之下,当使用MNC悬液以及纯化的外周血淋巴细胞作为效应细胞时,ADCC均在正常范围内,从而排除了单核细胞ADCC的存在所掩盖的淋巴细胞ADCC低于正常的情况。这些结果表明,PPS患者存在选择性NK缺陷,而淋巴细胞ADCC功能完整。这种缺陷是否在评估特定患者的恶性转化中具有价值,有待进一步对患者进行纵向NK研究和临床随访。

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