首页> 外文期刊>The Journal of Experomental Medicine >Lymphokine-activated killer cell phenomenon. Lysis of natural killer-resistant fresh solid tumor cells by interleukin 2-activated autologous human peripheral blood lymphocytes.
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Lymphokine-activated killer cell phenomenon. Lysis of natural killer-resistant fresh solid tumor cells by interleukin 2-activated autologous human peripheral blood lymphocytes.

机译:淋巴因子激活杀伤细胞现象。白细胞介素2-活化的自体外周血淋巴细胞裂解天然杀伤新鲜固体肿瘤细胞的裂解。

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Activation in lectin-free interleukin 2 (IL-2) containing supernatants of peripheral blood mononuclear leukocytes (PBL) from cancer patients or normal individuals resulted in expression of cytotoxicity toward 20 of 21 natural killer (NK)-resistant fresh solid tumor cells tested. Fresh solid tumor cells were resistant to NK-mediated lysis in 10 autologous patients' PBL-tumor interactions, and from 17 normal individuals tested against 13 allogeneic fresh tumors. Culture of PBL in IL-2 for 2-3 d was required for the lymphokine activated killers (LAK) to be expressed, and lytic activity toward a variety of NK-resistant fresh and cultured tumor targets developed in parallel. Autologous IL-2 was functional in LAK activation, as well as interferon-depleted IL-2 preparations. Irradiation of responder PBL before culture in IL-2 prevented LAK development. Precursors of LAK were present in PBL depleted of adherent cells and in NK-void thoracic duct lymphocytes, suggesting that the precursor is neither a monocyte nor an NK cell. LAK effectors expressed the serologically defined T cell markers of OKT.3, Leu-1, and 4F2, but did not express the monocyte/NK marker OKM-1. Lysis of autologous fresh solid tumors by LAK from cancer patients' PBL was demonstrated in 85% of the patient-fresh tumor combinations. Our data present evidence that the LAK system is a phenomenon distinct from either NK or CTL systems that probably accounts for a large number of reported nonclassical cytotoxicities. The biological role of LAK cells is not yet known, although it is suggested that these cells may be functional in immune surveillance against human solid tumors.
机译:从癌症患者的外周血单核白细胞(PBL)的外周血单核白细胞上清液(IL-2)的活化活化导致在2111个天然杀伤(NK) - 售后新鲜固体肿瘤细胞中的细胞毒性表达细胞毒性。新鲜的固体肿瘤细胞在10名自体患者的PBL肿瘤相互作用中耐受NK介导的裂解,并且从17个对13个同种异体新鲜肿瘤测试的正常个体。淋巴因子活化杀伤者(LAK)需要表达2-3d的IL-2中的PBL培养物,并达到与平行开发的各种NK抗性新鲜和培养的肿瘤靶标的裂变活动。自体IL-2在LAK活化中具有功能性,以及干扰素耗尽的IL-2制剂。 IL-2中培养前的响应PBL辐照防止LAK开发。 Lak的前体存在于粘附细胞和NK-void胸道淋巴细胞中的PBL中,表明前体既不是单核细胞也不是NK细胞。 LAK效应器表达OKT.3,Leu-1和4F2的血清学定义的T细胞标志物,但没有表达单核细胞/ NK标记OKM-1。患有癌症患者PBL的LAK裂解自体新鲜实体肿瘤的裂解,85%的患者新鲜肿瘤组合。我们的数据存在证据表明LAK系统是与NK或CTL系统不同的现象,可能可能占大量报告的非生物症细胞毒性。 LAK细胞的生物学作用尚不清楚,尽管建议这些细胞可能在免疫监测中对人体固体肿瘤的功能性。

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