白细胞介素-2和白细胞介素-4在恶性肿瘤患者中的免疫调节作用。

Journal of immunotherapy with emphasis on tumor immunology : official journal of the Society for Biological Therapy Pub Date : 1996-01-01 DOI:10.1097/00002371-199601000-00008

T Olencki, J Finke, R Tubbs, L Tuason, T Greene, D McLain, S J Swanson, P Herzog, J Stanley, M Edinger, G T Budd, R M Bukowski

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引用次数: 12

摘要

同时给予重组白细胞介素-2 (il -2)和重组人白细胞介素-4 (rHuIL-4)进行I期试验，以评估该细胞因子组合的毒性以及临床和免疫效果。39例符合条件的难治性恶性肿瘤患者接受了8种不同剂量水平(1A至3B)的治疗:1-3剂量的rIL-2[3.0、12.0和48.0 × 10(6) IU/m(2)静脉注射，每周3次(TIW)]和A-C剂量的rHuIL-4(40、120和400 μ g/m(2) s.c TIW)。这两种细胞因子的毒性是中等的，与单独使用il -2的毒性相当。由于缺乏足够的rHuIL-4，该组合未达到最大耐受剂量(MTD)，但至少为48.0 × 10(6) IU/m(2)的rhuil -2和120 μ g/m(2)的rHuIL-4。两名黑色素瘤患者有部分反应。免疫效应包括绝对淋巴细胞数量、CD3- /CD56+/ CD2+、总CD56+、CD8+和CD16c+淋巴细胞亚群随着rIL-2剂量水平的增加而增加，但与rHuIL-4剂量水平无关。外周血中自然杀伤(NK)细胞的增加伴随着NK对K562靶点的裂解活性高于基线的增加;然而，没有观察到淋巴因子激活杀手(LAK)活性(Daudi靶标)的增加。CD3+、CD4+和CD3+/CD25+/HLA-Dr+ t细胞亚群也增加，这些增加与rIL-2和rRuIL-4剂量的增加有关。最后，在6例患者中的4例中，连续肿瘤活检显示肿瘤细胞上主要组织相容性复合体(MHC) I类或II类抗原表达增加，或细胞因子治疗期间t细胞浸润增加，或两者兼有。本试验表明，rIL-2和rHuIL-4可同时给药，毒性可接受。免疫学结果显示，与ril -2相关的CD56+和CD16c+淋巴细胞和NK活性增加，有趣的是，LAK活性没有增加。这些发现提示rHuIL-4在体内对ril -2相关效应具有调节作用。

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Immunomodulatory effects of interleukin-2 and interleukin-4 in patients with malignancy.

A phase I trial of simultaneously administered recombinant interleukin-2 (rIL-2) and recombinant human IL-4 (rHuIL-4) was conducted to evaluate the toxicity and the clinical and immunologic effects of this cytokine combination. Thirty-nine eligible patients with refractory malignancy were treated at eight different dose levels (1A to 3B): 1-3 of rIL-2 [3.0, 12.0, and 48.0 x 10(6) IU/m(2) i.v. three times weekly (TIW)] and A-C of rHuIL-4 (40, 120, and 400 mu g/m(2) s.c. TIW). The toxicity of these two cytokines was moderate and was comparable with that seen with rIL-2 alone. The maximal tolerated dose (MTD) of the combination was not reached because of lack of sufficient rHuIL-4 but is at least 48.0 x 10(6) IU/m(2) of rIL-2 and 120 mu g/m(2) of rHuIL-4. Two patients with melanoma had partial responses. The immunologic effects included increases in absolute lymphocyte numbers, and the CD3- /CD56+/ CD2+, total CD56+, CD8+, and CD16c+ lymphocyte subsets with increasing rIL-2 dose levels, but not with rHuIL-4. This increase in natural killer (NK) cells in the peripheral blood was accompanied by an increase over baseline in NK lytic activity against K562 targets; however, concomitant increases in lymphokine-activated killer (LAK) activity (Daudi targets) were not seen. The CD3+, CD4+, and CD3+/CD25+/HLA-Dr+ T-cell subsets also increased, and these increases were related to both increasing rIL-2 and rRuIL-4 doses. Finally, in four of six patients, serial tumor biopsies demonstrated increases in major histocompatibility complex (MHC) class I or II antigen expression on tumor cells or increasing T-cell infiltrates during cytokine therapy or both. This trial demonstrated that rIL-2 and rHuIL-4 can be administered simultaneously with acceptable toxicity. The immunologic findings demonstrated the expected rIL-2-associated increases of CD56+ and CD16c+ lymphocytes and NK activity, and interestingly, no development of LAK activity. These findings suggest regulatory effects of rHuIL-4 on rIL-2-related effects in vivo.

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Journal of immunotherapy with emphasis on tumor immunology : official journal of the Society for Biological Therapy

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