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靶向白细胞介素-2治疗后小鼠体内持久且可转移的肿瘤免疫

Long-lived and transferable tumor immunity in mice after targeted interleukin-2 therapy.

作者信息

Becker J C, Varki N, Gillies S D, Furukawa K, Reisfeld R A

机构信息

The Scripps Research Institute, Department of Immunology, La Jolla, California 92037, USA.

出版信息

J Clin Invest. 1996 Dec 15;98(12):2801-4. doi: 10.1172/JCI119107.

Abstract

A major goal of tumor immunotherapy is the induction of tumor-specific T cell responses that are effective in eradicating disseminated tumor, as well as mounting a persistent tumor-protective immunity. We demonstrate here that a genetically engineered fusion protein consisting of human/mouse chimeric anti-ganglioside GD2 antibody and human interleukin-2 is able to induce eradication of established B78-D14 melanoma metastases in immunocompetent syngeneic C57BL/6J mice. This therapeutic effect is mediated by host immune cells, particularly CD8+ T cells and is associated with the induction of a long-lived immunity preventing tumor growth in the majority of animals when challenged up to four months later with B78-D14 cells. This effect was tumor-specific, since no cross-protection against syngeneic, ganglioside GD2+ EL-4 thymoma cells was observed. Furthermore, this tumor-specific protection can be transmitted horizontally to naive, syngeneic SCID mice by passive transfer of CD8+ T lymphocytes derived from immune animals. These results suggest that antibody-targeted delivery of cytokines provides a means to elicit effective immune responses against established tumors in the immunotherapy of neoplastic disease.

摘要

肿瘤免疫疗法的一个主要目标是诱导肿瘤特异性T细胞反应,这种反应在根除播散性肿瘤以及建立持久的肿瘤保护性免疫方面是有效的。我们在此证明,一种由人/鼠嵌合抗神经节苷脂GD2抗体和人白细胞介素-2组成的基因工程融合蛋白能够在具有免疫活性的同基因C57BL/6J小鼠中诱导已建立的B78-D14黑色素瘤转移灶的根除。这种治疗效果由宿主免疫细胞介导,特别是CD8+T细胞,并且与诱导长期免疫相关,当在四个月后用B78-D14细胞攻击时,大多数动物能够预防肿瘤生长。这种效果是肿瘤特异性的,因为未观察到对同基因神经节苷脂GD2+EL-4胸腺瘤细胞的交叉保护作用。此外,通过被动转移来自免疫动物的CD8+T淋巴细胞,这种肿瘤特异性保护可以水平传递给同基因的幼稚SCID小鼠。这些结果表明,细胞因子的抗体靶向递送为肿瘤疾病免疫治疗中针对已建立肿瘤引发有效免疫反应提供了一种手段。

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