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浸润肿瘤的单核细胞的功能分析。II. 从不同组织获得的单核细胞产生参与细胞毒性细胞生成的辅助因子的差异能力。

Functional analysis of mononuclear cells infiltrating into tumors. II. Differential ability of mononuclear cells obtained from various tissues to produce helper factors that are involved in the generation of cytotoxic cells.

作者信息

Uede T, Kohda H, Ibayashi Y, Osawa H, Diamantstein T, Kikuchi K

出版信息

J Immunol. 1985 Nov;135(5):3243-51.

PMID:3900205
Abstract

The requirement of CGF in the generation of cytotoxic cells against syngeneic tumor cells (T-9) and in the rejection of transplanted T-9 cells has been investigated. Spleen cells obtained from sensitized rats showed strong cytotoxicity against 51Cr-labeled T-9 cells upon incubation with CGF for 48 hr. Human recombinant IL 2 and rat IFN failed to generate cytotoxic cells from spleen cells of sensitized rats. CGF are produced by spleen cells upon inoculation of T-9 cells into sensitized rats as a host in vivo immune response. Production of CGF preceded the appearance of cytotoxic cells in regional lymph node and tumor tissues. In those rats, inoculated tumor cells were eventually rejected. In contrast, spleen cells failed to produce CGF upon inoculation of T-9 cells in unsensitized rats. Cytotoxic cells were not detected in unsensitized rats, and inoculated tumor grew in those rats. Thus, CGF is likely to be involved in the generation of cytotoxic cells and in the rejection of inoculated syngeneic tumor cells. A Mono Q anion-exchange column with an FPLC system allowed the chromatographic separation of CGF from IL 1, IL 2, IL 3, and CSF.

摘要

研究了CGF在针对同基因肿瘤细胞(T-9)产生细胞毒性细胞以及排斥移植的T-9细胞中的需求。从致敏大鼠获得的脾细胞在与CGF孵育48小时后,对51Cr标记的T-9细胞表现出强烈的细胞毒性。人重组IL-2和大鼠IFN未能从致敏大鼠的脾细胞中产生细胞毒性细胞。CGF是在将T-9细胞接种到致敏大鼠作为宿主后,由脾细胞产生的一种体内免疫反应。CGF的产生先于区域淋巴结和肿瘤组织中细胞毒性细胞的出现。在那些大鼠中,接种的肿瘤细胞最终被排斥。相反,在未致敏大鼠中接种T-9细胞后,脾细胞未能产生CGF。在未致敏大鼠中未检测到细胞毒性细胞,接种的肿瘤在这些大鼠中生长。因此,CGF可能参与细胞毒性细胞的产生以及接种的同基因肿瘤细胞的排斥。带有FPLC系统的Mono Q阴离子交换柱允许从IL-1、IL-2、IL-3和CSF中对CGF进行色谱分离。

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