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OK-432(化脓性链球菌)激活自然杀伤细胞的机制。I. 自然杀伤细胞趋化因子的自发释放以及在受到自然杀伤细胞靶细胞刺激后自然杀伤细胞趋化因子产生的增加。

Mechanism of NK activation by OK-432 (Streptococcus pyogenes). I. Spontaneous release of NKCF and augmentation of NKCF production following stimulation with NK target cells.

作者信息

Bonavida B, Katz J, Hoshino T

出版信息

Cell Immunol. 1986 Oct 1;102(1):126-35. doi: 10.1016/0008-8749(86)90331-x.

Abstract

The biological response modifier OK-432 (Picibanil) (manufactured in Japan) is produced by lyophilization of cultures of the low virulent Su strain of group A Streptococcus pyogenes of human origin. This preparation has been shown to have multiple effects on the immune system and has been used as an anti-cancer therapeutic agent in man. It has been shown that OK-432 augments the cytotoxic activity of human natural killer (NK) cells. We have proposed that natural killer cytotoxic factors (NKCF) derived from NK cells play a role in the mechanism of NK cell-mediated cytotoxicity (CMC). The present study investigates the underlying mechanism of the OK-432-mediated enhancement of NK activity by determining whether OK-432 has an effect on the induction and activity of NKCF produced by NK cells. Treatment of peripheral blood lymphocytes (PBL) with OK-432 for 20 hr and wash resulted in significant augmentation of NK CMC and this enhancement was dependent on the concentration of OK-432 used. Coculture of the OK-432-treated PBL with U937 resulted in a several-fold enhanced production of NKCF in the supernatant. The NKCF produced were similar to those produced by untreated effector cells in that they had the same NK target specificity for lysis. The time kinetics of stimulation of PBL with OK-432 for optimal production of NKCF was found to be 8-12 hr. It was also observed that culture of OK-432-treated PBL in the absence of stimulator cells spontaneously release significant amounts of NKCF into the supernatant. The supernatant containing NKCF was tested for interleukin 2 (IL-2) activity using an IL-2-dependent HT-2 line. It was found that there was no direct correlation between the levels of NKCF and IL-2 activity. The results of this study demonstrate that OK-432 stimulates NK cells to produce NKCF in the presence or absence of stimulator cells. The optimum concentration of OK-432-induced augmentation of NK CMC paralleled that seen for optimum NKCF production, suggesting that one mode of action of OK432 is to enhance NKCF production in a manner reminiscent of IFN and IL-2. The results also point out that OK-432 acts by a mechanism independent of the action of IL-2.

摘要

生物反应调节剂OK-432(沙培林)(日本生产)是通过冻干源自人类的A组化脓性链球菌低毒力Su菌株的培养物而制成的。这种制剂已被证明对免疫系统有多种作用,并已在人体中用作抗癌治疗剂。研究表明,OK-432可增强人类自然杀伤(NK)细胞的细胞毒性活性。我们曾提出,源自NK细胞的自然杀伤细胞毒性因子(NKCF)在NK细胞介导的细胞毒性(CMC)机制中发挥作用。本研究通过确定OK-432是否对NK细胞产生的NKCF的诱导和活性有影响,来探究OK-432介导的NK活性增强的潜在机制。用OK-432处理外周血淋巴细胞(PBL)20小时并洗涤后,NK CMC显著增强,且这种增强取决于所用OK-432的浓度。将经OK-432处理的PBL与U937共培养,导致上清液中NKCF的产生增加了几倍。所产生的NKCF与未处理的效应细胞产生的NKCF相似,因为它们对裂解具有相同的NK靶标特异性。发现用OK-432刺激PBL以实现NKCF最佳产生的时间动力学为8 - 12小时。还观察到,在没有刺激细胞的情况下培养经OK-432处理的PBL会自发地将大量NKCF释放到上清液中。使用依赖IL-2的HT-2细胞系检测含有NKCF的上清液的白细胞介素2(IL-2)活性。发现NKCF水平与IL-2活性之间没有直接相关性。本研究结果表明,无论有无刺激细胞,OK-432均可刺激NK细胞产生NKCF。OK-432诱导NK CMC增强的最佳浓度与最佳NKCF产生的浓度平行,这表明OK432的一种作用方式是以类似于干扰素和IL-2的方式增强NKCF的产生。结果还指出,OK-432的作用机制独立于IL-2的作用机制。

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