在体内用白细胞介素-2治疗后,肿瘤患者淋巴细胞的体外T细胞反应降低,同时白细胞介素-2反应增强。

J A Hank, J A Sosman, P C Kohler, R Bechhofer, B Storer, P M Sondel
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引用次数: 0

摘要

在两种不同的临床方案中接受白细胞介素-2 (IL-2)治疗的癌症患者外周血淋巴细胞被评估其对IL-2、同种异体抗原和PHA的体外反应。体内IL-2诱导对IL-2的体外增殖反应增强,而对植物血凝素(PHA)和同种异体抗原的体外增殖反应减弱。体内IL-2也抑制了同种异体诱导的细胞毒性T细胞反应。我们检查了体外对PHA和IL-2的增殖反应动力学,发现在体外暴露的2周内,虽然体内IL-2诱导的淋巴细胞对PHA的反应在任何时候都被抑制,但对IL-2的反应比IL-2治疗前获得的淋巴细胞对IL-2的反应更早达到峰值,并且更高。这些对抗原诱导的T细胞反应与IL-2诱导的非特异性增殖和细胞毒性反应的对比作用表明,在用于增强抗原特异性T细胞反应或作为免疫增强剂与疫苗联合使用时,IL-2给药的剂量和时间的重要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Depressed in vitro T cell responses concomitant with augmented interleukin-2 responses by lymphocytes from cancer patients following in vivo treatment with interleukin-2.

Peripheral blood lymphocytes obtained from cancer patients receiving interleukin-2 (IL-2) on two separate clinical protocols were evaluated for their in vitro responses to IL-2, alloantigens, and PHA. IL-2 in vivo induced enhanced in vitro proliferative responses to IL-2 and diminished in vitro proliferative responses to phytohemagglutinin (PHA) and alloantigens. Alloinduced cytotoxic T cell responses were also depressed following in vivo IL-2. We examined the kinetics of the in vitro proliferative response to PHA and IL-2 and found that while the response of lymphocytes primed in vivo with IL-2 to PHA was depressed at all times during the 2 week in vitro exposure, the response to IL-2 peaked earlier and higher than did the response to IL-2 by lymphocytes obtained prior to IL-2 therapy. These contrasting effects on antigen-induced T cell responses vs. IL-2 induced nonspecific proliferative and cytotoxic responses suggest the importance of dose and timing of IL-2 administration when used to enhance antigen-specific T cell responses or as an immune enhancing agent combined with vaccines.

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