自然杀伤细胞和基因治疗:基因转染优化效应细胞功能和靶向基因产物进入肿瘤转移的潜力。

Natural immunity Pub Date : 1994-03-01
R H Goldfarb, T L Whiteside, P H Basse, W C Lin, N Vujanovic, R B Herberman
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引用次数: 0

摘要

荧光标记的过继转移白细胞介素(IL)-2激活的自然杀伤细胞(A-NK)能够选择性地积聚在已建立的肺或肝转移瘤中,与肿瘤细胞和/或微血管内皮细胞结合。在动物模型和临床中,A-NK细胞也显示出抗转移治疗的作用。转染细胞因子或可能的其他分子的基因有可能提高效应细胞的治疗效力和功效。通过基因转染诱导IL-2和/或其他细胞因子的自分泌,有望增强其抗转移活性,同时避免高剂量细胞因子的全身毒性。基因治疗的一种替代或补充策略是用细胞毒性分子基因转染A-NK细胞,选择性地将其靶向转移部位。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Natural killer cells and gene therapy: potential of gene transfection for optimizing effector cell functions and for targeting gene products into tumor metastases.

Fluorescently labeled, adoptively transferred interleukin (IL)-2 activated natural killer (A-NK) cells have the ability to selectively accumulate within established pulmonary or hepatic metastases, binding to tumor cells and/or to microvascular endothelial cells. A-NK cells have also been shown to exert antimetastatic therapy in animal models and in the clinic. Transfection of genes for cytokines or possibly other molecules has the potential to improve the therapeutic potency and efficacy of the effector cells. Gene transfection to induce autocrine production of IL-2 and/or other cytokines is expected to augment their antimetastatic activities, while avoiding toxicity from systemic administration of high doses of cytokines. An alternative or complementary strategy for gene therapy is to transfect A-NK cells with genes for cytotoxic molecules, to selectively target them to metastatic sites.

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