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人类大颗粒淋巴细胞(LGL)产生多种淋巴因子的能力:白细胞介素2、干扰素和集落刺激因子。

Capacity of human large granular lymphocytes (LGL) to produce multiple lymphokines: interleukin 2, interferon, and colony stimulating factor.

作者信息

Kasahara T, Djeu J Y, Dougherty S F, Oppenheim J J

出版信息

J Immunol. 1983 Nov;131(5):2379-85.

PMID:6195261
Abstract

Human large granular lymphocytes (LGL), which are known to be responsible for natural killer (NK) cell activity, also produced a variety of lymphokines including interleukin 2 (IL 2), colony stimulating factor (CSF), and interferon (IFN) in response to phytohemagglutinin (PHA) or concanavalin A (Con A). Human peripheral blood LGL, which were purified by removal of monocytes adhering to plastic flasks and nylon columns, followed by separation on a discontinuous Percoll gradient, and additional treatment with anti-OKT3 and Leu-M1 plus complement, were more potent producers of these lymphokines than unseparated mononuclear cells (MNC), nylon column-eluted cells, or purified T lymphocytes. Moreover, IL 2 production by LGL could be further distinguished in that it was not enhanced by the addition of macrophages or macrophage-derived factor, i.e., IL 1, whereas addition of macrophages did potentiate IL 2 production by T lymphocytes. Further analysis of cells in the LGL population using various monoclonal antibodies revealed that removal of cells with OKT11 or AF-10, a monoclonal antibody against human HLA-DR antigen, decreased IL 2 production, whereas removal of OKT8+, OKM1+, Leu-M1+, or Leu-7+ cells led to enhanced IL 2 production. The LGL population is therefore heterogeneous and includes at least three functionally and phenotypically distinct subsets. An atypical T cell subset (OKT3-, Leu-1-, OKT11+) rather than the myeloid subset of LGL (Leu-M1+ or OKMI+) was the source of LGL-derived IL 2, whereas the latter subset and/or another subset of OKT8+ cells appear to regulate this IL 2 production. In addition to performing NK activity, LGL on a per cell basis seem to be more effective than T lymphocytes in producing lymphokines, namely, IL2, CSF, and IFN.

摘要

已知人类大颗粒淋巴细胞(LGL)负责自然杀伤(NK)细胞活性,其在受到植物血凝素(PHA)或刀豆球蛋白A(Con A)刺激后,还会产生多种淋巴因子,包括白细胞介素2(IL 2)、集落刺激因子(CSF)和干扰素(IFN)。通过去除附着在塑料瓶和尼龙柱上的单核细胞进行纯化,然后在不连续的Percoll梯度上分离,并使用抗OKT3和Leu-M1加补体进行额外处理,得到的人类外周血LGL比未分离的单核细胞(MNC)、尼龙柱洗脱细胞或纯化的T淋巴细胞更能有效地产生这些淋巴因子。此外,LGL产生IL 2的情况可以进一步区分,即添加巨噬细胞或巨噬细胞衍生因子(即IL 1)并不能增强其产生,而添加巨噬细胞确实能增强T淋巴细胞产生IL 2的能力。使用各种单克隆抗体对LGL群体中的细胞进行进一步分析发现,去除表达OKT11或AF-10(一种针对人类HLA-DR抗原的单克隆抗体)的细胞会降低IL 2的产生,而去除OKT8 +、OKM1 +、Leu-M1 +或Leu-7 +细胞会导致IL 2产生增加。因此,LGL群体是异质性的,至少包括三个功能和表型不同的亚群。非典型T细胞亚群(OKT3 -、Leu-1 -、OKT11 +)而非LGL的髓样亚群(Leu-M1 +或OKMI +)是LGL衍生的IL 2的来源,而后者亚群和/或另一个OKT8 +细胞亚群似乎调节这种IL 2的产生。除了执行NK活性外,单个LGL细胞在产生淋巴因子(即IL2、CSF和IFN)方面似乎比T淋巴细胞更有效。

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