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体内给予白细胞介素2可增强同种反应性细胞毒性T淋巴细胞和驻留自然杀伤细胞的生成。

In vivo interleukin 2 administration augments the generation of alloreactive cytolytic T lymphocytes and resident natural killer cells.

作者信息

Hefeneider S H, Conlon P J, Henney C S, Gillis S

出版信息

J Immunol. 1983 Jan;130(1):222-7.

PMID:6600178
Abstract

Interleukin 2 (IL 2) is a T cell growth factor that has been shown to modulate several in vitro immune responses. Produced by T cells, the lymphokine has been highly purified and used in a series of in vivo studies to examine the effect of IL 2 on murine cytotoxic T cell (CTL) and natural killer (NK) cell reactivity. By employing an immunization protocol known to generate CTL activity against allogeneic tumors, in vivo administration of highly purified IL 2, either in concert, with or 2 days after, tumor administration, resulted in an augmented CTL response as compared to effector cells harvested from untreated, alloimmunized control animals. Characterization of the effector cells responsible for the augmented cytolytic activity showed them to be of the T cell lineage and to be specific for the appropriate immunizing tumor cell. Furthermore, we were able to demonstrate that administration of purified IL 2 to naive, non-antigen-challenged recipients resulted in substantial potentiation of NK cell activity. The augmented cytolytic reactivity was mediated by NK cells as evidenced by effector cell lysis of NK-susceptible but not NK-insusceptible tumor targets. The results of these studies suggest IL 2 functions in vivo as an immune response regulator and may have a beneficial effect as an in vivo immunopotentiator.

摘要

白细胞介素2(IL - 2)是一种T细胞生长因子,已被证明可调节多种体外免疫反应。这种淋巴因子由T细胞产生,已被高度纯化,并用于一系列体内研究,以检验IL - 2对小鼠细胞毒性T细胞(CTL)和自然杀伤(NK)细胞反应性的影响。通过采用一种已知能产生针对同种异体肿瘤的CTL活性的免疫方案,在肿瘤接种时或接种后2天同时给予高度纯化的IL - 2,与从未经处理的同种免疫对照动物收获的效应细胞相比,CTL反应增强。对负责增强细胞溶解活性的效应细胞的表征表明,它们属于T细胞谱系,并且对适当的免疫肿瘤细胞具有特异性。此外,我们能够证明,向未接触过抗原的幼稚受体给予纯化的IL - 2会导致NK细胞活性大幅增强。增强的细胞溶解反应性由NK细胞介导,这可通过效应细胞对NK敏感但对NK不敏感的肿瘤靶标的裂解来证明。这些研究结果表明,IL - 2在体内作为一种免疫反应调节剂发挥作用,并且作为体内免疫增强剂可能具有有益效果。

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