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纯化的人白细胞介素2的体内给药。II. 重组白细胞介素2在体内的半衰期、免疫效应及外周淋巴细胞的扩增

In vivo administration of purified human interleukin 2. II. Half life, immunologic effects, and expansion of peripheral lymphoid cells in vivo with recombinant IL 2.

作者信息

Lotze M T, Matory Y L, Ettinghausen S E, Rayner A A, Sharrow S O, Seipp C A, Custer M C, Rosenberg S A

出版信息

J Immunol. 1985 Oct;135(4):2865-75.

PMID:2993418
Abstract

Purified recombinant human interleukin 2 (RIL 2) derived from E. coli containing the inserted gene encoding for IL 2 was administered to 20 patients with a variety of malignancies. Toxicity was dose related and included fever, chills, malaise, arthralgias, myalgias, and unexpectedly, weight gain related to marked fluid retention. All patients receiving more than 10(5) U/kg total cumulative dose developed evidence of fluid retention, and all patients requiring discontinuance of RIL 2 (11/20) received total doses of between 2.54 X 10(5) U/kg to 15.4 X 10(5) U/kg. The limiting dose with this preparation was 3000 U/kg/hr by continuous administration or 10(6) U/kg by bolus administration. IL 2 was rapidly cleared from the plasma, with a half life of 6.9 min, and a later delayed clearance was consistent with a two-compartment model, with slower release from the extravascular space back into the plasma compartment. A marked change in lymphoid cells in the periphery was noted with an early depletion of all lymphoid cells, followed by an expansion of such cells with continuous IL 2 administration. A twofold to 16-fold expansion of total lymphoid cells in the peripheral blood could be demonstrated. TAC+ cells representing up to 25% of the circulating peripheral blood mononuclear cells could be demonstrated with 3 wk of continuous RIL 2 administration. Interferon-gamma levels increased in patients treated with IL 2. Precursors of lymphokine-activated killer cells generated under standard conditions were depleted within 2 to 3 min after IL 2 administration, but repopulated the peripheral blood after 7 to 10 days of continuous IL 2 administration. No tumor regression was seen in any of the cancer patients treated with IL 2 alone.

摘要

将含有编码白细胞介素2(IL-2)插入基因的大肠杆菌来源的纯化重组人白细胞介素2(RIL-2)给予20例患有各种恶性肿瘤的患者。毒性与剂量相关,包括发热、寒战、不适、关节痛、肌痛,出乎意料的是,还包括与明显液体潴留相关的体重增加。所有接受总累积剂量超过10⁵U/kg的患者均出现液体潴留迹象,所有需要停用RIL-2的患者(11/20)接受的总剂量在2.54×10⁵U/kg至15.4×10⁵U/kg之间。该制剂的极限剂量为持续给药3000U/kg/小时或推注给药10⁶U/kg。IL-2从血浆中迅速清除,半衰期为6.9分钟,随后的延迟清除符合二室模型,从血管外间隙回流入血浆室的速度较慢。外周淋巴样细胞有明显变化,所有淋巴样细胞早期耗竭,随后随着持续给予IL-2此类细胞扩增。外周血中总淋巴样细胞可扩增2至16倍。连续给予RIL-2 3周后,可证明代表高达25%循环外周血单核细胞的TAC⁺细胞。接受IL-2治疗的患者中γ干扰素水平升高。在标准条件下产生的淋巴因子激活的杀伤细胞前体在给予IL-2后2至3分钟内耗竭,但在连续给予IL-2 7至10天后在外周血中重新出现。单独用IL-2治疗的癌症患者均未出现肿瘤消退。

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