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淋巴因子激活的杀伤(LAK)细胞现象。IV. LAK细胞克隆对来自自体和多种同种异体肿瘤的新鲜人肿瘤细胞的杀伤作用。

Lymphokine-activated killer (LAK) cell phenomenon. IV. Lysis by LAK cell clones of fresh human tumor cells from autologous and multiple allogeneic tumors.

作者信息

Rayner A A, Grimm E A, Lotze M T, Wilson D J, Rosenberg S A

出版信息

J Natl Cancer Inst. 1985 Jul;75(1):67-75.

PMID:2989604
Abstract

Activated killer cells are generated by the incubation of peripheral blood mononuclear leukocytes (PBL) in the lymphokine interleukin 2 (IL-2). Unseparated populations of these lymphokine-activated killer (LAK) cells lyse a variety of fresh noncultured human tumor targets, but they do not kill normal PBL. This study analyzed the generation and lytic specificity of LAK cell clones. Of 49 (84%) clones isolated by limiting-dilution techniques from a whole population of LAK cells, 41 manifested significant LAK cell activity. LAK cell clones had varied cell surface phenotypes. Clones with high and intermediate LAK cell activity were Leu 2+3-4+7-DR+Tac+ and Leu 2-3+4+7-DR+Tac+, respectively. Single LAK cell clones lysed multiple fresh human tumor targets including autologous sarcoma, 5 allogeneic sarcomas, and a colon cancer in addition to the cultured cell line K562. Autologous PBL were not lysed. Tumor targets were each lysed by multiple LAK cell clones. Sixteen subclones were derived from 5 of these LAK cell clones. These subclones had 99% or greater probability of being derived from a single cell. These subclones also exhibited lysis of multiple tumor targets. These findings suggest the existence of a shared determinant, expressed by multiple human tumors, which is recognized in common by multiple LAK cell clones.

摘要

通过在淋巴因子白细胞介素2(IL-2)中孵育外周血单核白细胞(PBL)可产生活化的杀伤细胞。这些淋巴因子活化的杀伤(LAK)细胞的未分离群体可裂解多种新鲜的未培养的人类肿瘤靶标,但它们不会杀伤正常的PBL。本研究分析了LAK细胞克隆的产生及其裂解特异性。通过有限稀释技术从整个LAK细胞群体中分离出的49个克隆(84%)中,有41个表现出显著的LAK细胞活性。LAK细胞克隆具有不同的细胞表面表型。具有高和中等LAK细胞活性的克隆分别为Leu 2+3-4+7-DR+Tac+和Leu 2-3+4+7-DR+Tac+。单个LAK细胞克隆可裂解多种新鲜的人类肿瘤靶标,包括自体肉瘤、5种异体肉瘤以及一种结肠癌,此外还可裂解培养的细胞系K562。自体PBL未被裂解。肿瘤靶标可被多个LAK细胞克隆裂解。从其中5个LAK细胞克隆中获得了16个子克隆。这些子克隆有99%或更高的概率源自单个细胞。这些子克隆也表现出对多种肿瘤靶标的裂解作用。这些发现表明存在一种由多种人类肿瘤表达的共同决定簇,它可被多个LAK细胞克隆共同识别。

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