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通过瘤内注射表达人白细胞介素-2的组织不相容细胞对自发性犬黑色素瘤和猫纤维肉瘤进行基因治疗。

Gene therapy of spontaneous canine melanoma and feline fibrosarcoma by intratumoral administration of histoincompatible cells expressing human interleukin-2.

作者信息

Quintin-Colonna F, Devauchelle P, Fradelizi D, Mourot B, Faure T, Kourilsky P, Roth C, Mehtali M

机构信息

Ecole Vétérinaire d'Alfort, Maisons-Alfort, France.

出版信息

Gene Ther. 1996 Dec;3(12):1104-12.

PMID:8986437
Abstract

The production of human interleukin-2 (hIL-2) local to the tumor site by engineered histoincompatible cells has been shown in various murine models to promote a strong immune response leading to tumor growth inhibition or rejection. To assess whether this strategy would be similarly applicable for treatment of primary neoplastic cells, two naturally occurring tumors were used as preclinical models; the highly metastatic melanoma of the dog and the low metastatic fibrosarcoma of the cat. We demonstrate that both cats and dogs when treated by tumor surgery, radiotherapy and repeated local injections of xenogeneic Vero cells secreting high levels of hIL-2 relapse less frequently and survive longer than control animals treated by surgery and radiotherapy alone. Local secretion of hIL-2 by the xenogeneic cells is shown to be necessary for the induction of an optimal antitumor effect. Moreover, the safety of the procedure was demonstrated in both animal models and through extensive toxicological analysis performed in rats. These results confirm for the first time to our knowledge the safety and therapeutic potential of a gene transfer strategy in animals with spontaneous metastatic and nonmetastatic tumors.

摘要

在各种小鼠模型中已表明,通过工程改造的组织不相容细胞在肿瘤部位产生人白细胞介素-2(hIL-2)可促进强烈的免疫反应,从而导致肿瘤生长抑制或排斥。为了评估该策略是否同样适用于原发性肿瘤细胞的治疗,使用了两种天然发生的肿瘤作为临床前模型;犬的高转移性黑色素瘤和猫的低转移性纤维肉瘤。我们证明,与仅接受手术和放疗的对照动物相比,接受肿瘤手术、放疗并反复局部注射分泌高水平hIL-2的异种Vero细胞治疗的猫和犬复发频率更低,存活时间更长。异种细胞局部分泌hIL-2被证明是诱导最佳抗肿瘤效果所必需的。此外,在动物模型以及通过在大鼠中进行的广泛毒理学分析都证明了该程序的安全性。据我们所知,这些结果首次证实了基因转移策略在患有自发性转移性和非转移性肿瘤的动物中的安全性和治疗潜力。

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