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体内白细胞介素-2治疗诱导的淋巴因子激活的杀伤活性:CD2和leu19抗原表达增加但CD16抗原表达阴性的淋巴细胞起主要作用。

Lymphokine-activated killer activity induced by in vivo interleukin 2 therapy: predominant role for lymphocytes with increased expression of CD2 and leu19 antigens but negative expression of CD16 antigens.

作者信息

Weil-Hillman G, Fisch P, Prieve A F, Sosman J A, Hank J A, Sondel P M

机构信息

Department of Human Oncology, University of Wisconsin, Madison.

出版信息

Cancer Res. 1989 Jul 1;49(13):3680-8.

PMID:2471587
Abstract

The phenotype and function of lymphocytes from cancer patients treated with repetitive weekly cycles of continuous i.v. infusions of recombinant interleukin 2 (IL-2) were examined. Peripheral blood lymphocytes (PBL) obtained after IL-2 therapy showed an increased percentage of cells bearing the CD16 and leu19 markers which are associated with natural killer cells. These PBL mediated significantly increased levels of IL-2-dependent lymphokine-activated killer (LAK) activity against the Daudi cell line. Depletion of CD16+ cells from PBL obtained after in vivo IL-2 caused only slight inhibition of their LAK activity or their proliferative response to IL-2 in vitro. This indicates that CD16+ cells are involved but play only a minor role in these responses. In contrast, depletion of leu19+ cells, from PBL activated in vivo with IL-2, virtually abrogated their LAK activity and their proliferative response to IL-2. Two-color flow cytometry studies showed that a leu19+/CD16- population was expanded by in vivo IL-2 therapy and was responsible for the majority of LAK activity by in vivo-activated PBL. Moreover, this CD16- population showed an increased density of leu19 and CD2 (E rosette receptor) antigens when compared to the resting PBL obtained prior to IL-2 treatment. These data show that the predominant population mediating in vitro LAK activity, induced by in vivo IL-2 therapy, consists of activated natural killer cells with a high density of leu19 and CD2 antigens but negative for the CD16 antigen.

摘要

对接受每周重复静脉持续输注重组白细胞介素2(IL-2)治疗的癌症患者的淋巴细胞的表型和功能进行了研究。IL-2治疗后获得的外周血淋巴细胞(PBL)显示,携带与自然杀伤细胞相关的CD16和leu19标记的细胞百分比增加。这些PBL介导的针对Daudi细胞系的IL-2依赖性淋巴因子激活的杀伤细胞(LAK)活性水平显著提高。体内IL-2治疗后获得的PBL中CD16+细胞的耗竭仅轻微抑制其LAK活性或其体外对IL-2的增殖反应。这表明CD16+细胞参与其中,但在这些反应中仅起次要作用。相反,体内用IL-2激活后的PBL中leu19+细胞的耗竭几乎消除了它们的LAK活性和对IL-2的增殖反应。双色流式细胞术研究表明,体内IL-2治疗可使leu19+/CD16-群体扩增,并负责体内激活的PBL的大部分LAK活性。此外,与IL-2治疗前获得的静息PBL相比,该CD16-群体显示leu19和CD2(E玫瑰花结受体)抗原密度增加。这些数据表明,体内IL-2治疗诱导的介导体外LAK活性的主要群体由具有高密度leu19和CD2抗原但CD16抗原呈阴性的活化自然杀伤细胞组成。

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Lymphokine-activated killer activity induced by in vivo interleukin 2 therapy: predominant role for lymphocytes with increased expression of CD2 and leu19 antigens but negative expression of CD16 antigens.体内白细胞介素-2治疗诱导的淋巴因子激活的杀伤活性:CD2和leu19抗原表达增加但CD16抗原表达阴性的淋巴细胞起主要作用。
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