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重组α干扰素对肺癌患者自然杀伤细胞和抗体依赖的细胞介导的细胞毒性作用的影响:一项II期试验的结果

Effect of recombinant alpha interferon on NK and ADCC function in lung cancer patients: results from a phase II trial.

作者信息

Hokland P, Hokland M, Olesen B K, Ernst P

出版信息

J Interferon Res. 1984 Fall;4(4):561-9. doi: 10.1089/jir.1984.4.561.

Abstract

During a phase II trial of recombinant IFN-alpha given in doses of 50 X 10(6) units/m2 three times per week to lung cancer patients, 13 patients were evaluated longitudinally in NK and ADCC assays and in immunofluorescence tests enumerating the number of cells reactive with the new N901 NK-cell antibody. An increase in NK-cell activity could be demonstrated when values before and 24 h after the first injection of IFN were compared, but simultaneously the enhancing effect of IFN-alpha on NK-cells added to in vitro cultures was abolished, probably as a result of preactivation of NK cells in vivo. After 2-4 weeks of treatment, the majority of patients exhibited a pronounced decrease in NK-cell activity while still retaining the inability to be boosted by IFN added in vitro. Investigations with the NK antibody N901 showed that the initial increase in NK activity appeared concomitantly with an increase in the number of N901 positive cells, indicating that the mechanism behind this increase was an increase in the number of circulating NK cells. In contrast, the decrease in NK activity mentioned above was not followed by a similar decrease in the number of N901+ cells, and it was concluded that this decrease might be attributable to either an exhaustion phenomenon or to an induction of a refractory state of peripheral blood NK cells. When measuring ADCC activity, increases in lytic activity were seen only in patients in whom they could be attributed to non-IgG-dependent (NK-like) mechanisms. These data are discussed in relation to other clinical trials using leukocyte or recombinant IFN-alpha.

摘要

在一项针对肺癌患者的II期试验中,给予重组干扰素-α,剂量为50×10⁶单位/m²,每周三次。对13名患者进行了纵向评估,包括自然杀伤细胞(NK)和抗体依赖细胞介导的细胞毒性(ADCC)检测,以及免疫荧光测试,以确定与新型N901 NK细胞抗体反应的细胞数量。比较首次注射干扰素前和注射后24小时的值时,可以证明NK细胞活性增加,但同时,添加到体外培养物中的干扰素-α对NK细胞的增强作用被消除,这可能是由于体内NK细胞的预激活。治疗2 - 4周后,大多数患者的NK细胞活性显著下降,同时仍无法被体外添加的干扰素增强。使用NK抗体N901的研究表明,NK活性的最初增加与N901阳性细胞数量的增加同时出现,这表明这种增加背后的机制是循环NK细胞数量的增加。相比之下,上述NK活性的下降并没有伴随着N901⁺细胞数量的类似下降,得出的结论是,这种下降可能归因于耗竭现象或外周血NK细胞难治状态的诱导。在测量ADCC活性时,仅在那些其裂解活性可归因于非IgG依赖性(NK样)机制的患者中观察到裂解活性增加。这些数据与使用白细胞或重组干扰素-α的其他临床试验相关进行了讨论。

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