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通过逆转录病毒介导在体内递送白细胞介素4基因根除大鼠恶性胶质瘤。

Eradication of rat malignant gliomas by retroviral-mediated, in vivo delivery of the interleukin 4 gene.

作者信息

Benedetti S, Bruzzone M G, Pollo B, DiMeco F, Magrassi L, Pirola B, Cirenei N, Colombo M P, Finocchiaro G

机构信息

Laboratory of Neuro-Oncology and Gene Therapy, Istituto Nazionale Neurologico Besta, Milano, Italy.

出版信息

Cancer Res. 1999 Feb 1;59(3):645-52.

PMID:9973213
Abstract

Overexpression of interleukin 4 (IL-4) can impair the tumorigenicity of glioma cells, but direct evidence of its antitumor efficacy after in vivo gene transfer into malignant gliomas has not been provided. To test this, we first injected into the brain of Sprague Dawley rats a 1:1 mixture of C6 rat glioblastoma cells and psi2.L4SN20 or E86.L4SN50 retroviral producer cells (RPCs), secreting 20 and 50 ng of IL-4/5 x 10(5) cells/48 h, respectively. Twenty-seven and 56% of rats receiving injections with these low- or medium-level IL-4 RPCs, respectively, survived tumor injection, whereas control rats died in about 1 month. E86.L4SN50 RPCs coinjected with 9L gliosarcoma cells into syngeneic Fischer 344 rats yielded similar results. A novel IL-4 RPC clone expressing higher levels of IL-4, E86.L4SN200, coinjected with 9L cells increased to 75% the fraction of long-term survivors and induced tumor regression in 50% of rats when injected into established 9L gliosarcomas. Cured rats developed an immunological memory because they rejected a challenge of wild-type 9L cells into the contralateral hemisphere. Magnetic resonance imaging was used to monitor 9L and C6 gliomas and gave direct evidence for tumor rejection in treated rats. Immunohistology showed inflammatory infiltrates in IL-4-treated tumors in which CD8+ T lymphocytes were more abundant, although CD4+ T lymphocytes, B lymphocytes, and macrophages were also present. Overall, these findings suggest that IL-4 gene transfer is a new, promising approach for treating malignant gliomas.

摘要

白细胞介素4(IL-4)的过表达可损害胶质瘤细胞的致瘤性,但尚未提供其在体内基因转移至恶性胶质瘤后抗肿瘤疗效的直接证据。为了验证这一点,我们首先将C6大鼠胶质母细胞瘤细胞与分别分泌20 ng和50 ng IL-4/5×10⁵细胞/48 h的psi2.L4SN20或E86.L4SN50逆转录病毒生产细胞(RPC)按1:1的混合物注入Sprague Dawley大鼠脑内。分别接受这些低水平或中等水平IL-4 RPC注射的大鼠中,27%和56%在肿瘤注射后存活,而对照大鼠在约1个月内死亡。将E86.L4SN50 RPC与9L胶质肉瘤细胞共同注入同基因的Fischer 344大鼠中也得到了类似结果。一个表达更高水平IL-4的新型IL-4 RPC克隆E86.L4SN200与9L细胞共同注入时,长期存活者的比例增加到75%,并且在注入已形成的9L胶质肉瘤时,50%的大鼠出现肿瘤消退。治愈的大鼠产生了免疫记忆,因为它们拒绝了对侧半球野生型9L细胞的攻击。磁共振成像用于监测9L和C6胶质瘤,并为治疗大鼠中的肿瘤排斥提供了直接证据。免疫组织学显示,在IL-4治疗的肿瘤中有炎性浸润,其中CD8⁺T淋巴细胞更为丰富,尽管也存在CD4⁺T淋巴细胞、B淋巴细胞和巨噬细胞。总体而言,这些发现表明IL-4基因转移是一种治疗恶性胶质瘤的新的、有前景的方法。

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