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人类T细胞亚群产生α-淋巴毒素。

Production of alpha-lymphotoxin by human T-cell subsets.

作者信息

Leopardi E, Rosenau W

出版信息

Cell Immunol. 1984 Jan;83(1):73-82. doi: 10.1016/0008-8749(84)90226-0.

Abstract

Human T cells were isolated from peripheral blood lymphocytes (PBL) and sensitized to allogeneic PBL in a one-way mixed-lymphocyte culture. These sensitized T cells were fractionated on the basis of their possession of Fc receptors for IgG (TG+) or IgM (TM+), or the absence of both IgG and IgM receptors (TG-M-). When restimulated with alloantigen of the same derivation, TG+, TM+, and TG-M- cells yielded almost equal amounts of cytotoxin. Anti-alpha-lymphotoxin serum neutralized most of this cytotoxic activity indicating that alpha-lymphotoxin (alpha-LT) constituted most of this activity. Although TG-M- cells function as effectors in allogeneic cytotoxicity, TG+ cells lyse IgG-coated targets in an antibody-dependent cell-mediated cytotoxic (ADCC) reaction, which has been shown to be mediated in part by alpha-LT. Whether TM+ cells can be cytotoxic is not clear. In addition, freshly isolated human T-cell subsets were stimulated with phytohemagglutinin-P (PHA-P). After PHA stimulation, TG+, TM+, and TG-M- cells produced similar amounts of soluble cytotoxin, which was largely neutralized by anti-alpha-LT. The TG+ cells incorporated less thymidine than the TM+ or TG-M- cells. Likewise, OKT4+ and OKT8+ subsets, isolated with the aid of monoclonal OKT8 or OKT4 antibody and complement, yielded lymphotoxin after stimulation with PHA. It is shown that all T-cell subsets, as defined here, can produce lymphotoxin. Furthermore, depending on the assay system, cytotoxicity can be clearly demonstrated in all of these subsets, except in TM+ cells, where positive and negative results have been reported.

摘要

从外周血淋巴细胞(PBL)中分离出人T细胞,并在单向混合淋巴细胞培养中使其对同种异体PBL致敏。这些致敏T细胞根据其是否拥有针对IgG的Fc受体(TG+)或IgM的Fc受体(TM+),或同时缺乏IgG和IgM受体(TG-M-)进行分离。当用相同来源的同种异体抗原再次刺激时,TG+、TM+和TG-M-细胞产生的细胞毒素量几乎相等。抗α-淋巴毒素血清中和了大部分这种细胞毒性活性,表明α-淋巴毒素(α-LT)构成了这种活性的大部分。尽管TG-M-细胞在同种异体细胞毒性中起效应细胞的作用,但TG+细胞在抗体依赖性细胞介导的细胞毒性(ADCC)反应中裂解IgG包被的靶标,已证明该反应部分由α-LT介导。TM+细胞是否具有细胞毒性尚不清楚。此外,用植物血凝素-P(PHA-P)刺激新鲜分离的人T细胞亚群。PHA刺激后,TG+、TM+和TG-M-细胞产生相似量的可溶性细胞毒素,其大部分被抗α-LT中和。TG+细胞掺入的胸腺嘧啶核苷比TM+或TG-M-细胞少。同样,借助单克隆OKT8或OKT4抗体和补体分离的OKT4+和OKT8+亚群在PHA刺激后产生淋巴毒素。结果表明,本文所定义的所有T细胞亚群都能产生淋巴毒素。此外,根据检测系统的不同,除TM+细胞(关于其细胞毒性的结果有阳性和阴性报道)外,所有这些亚群都能清楚地显示出细胞毒性。

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