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首页> 外文期刊>Journal of Neuroimmunology: Official Bulletin of the Research Committee on Neuroimmunology of the World Federation of Neurology >IL-10 gene transfer to intracranial 9L glioma: tumor inhibition and cooperation with IL-2.
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IL-10 gene transfer to intracranial 9L glioma: tumor inhibition and cooperation with IL-2.

机译:IL-10基因转移到颅内9L神经胶质瘤:肿瘤抑制和与IL-2的合作。

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摘要

This study examines the effects of interleukin-10 (IL-10) and combination IL-10 + IL-2 gene transfer on experimental brain tumor growth in vivo. 9L gliosarcoma cells were engineered to stably express murine IL-10 (9L-IL-10 cells) and implanted subcutaneously or to the caudate/putamen of syngeneic rats. The growth of tumors expressing IL-10 was substantially reduced compared to that of control tumors (p < 0.05). Intracranial tumors expressing IL-10 and IL-2 were established by co-implanting 9L-IL-10 cells with endothelial cells engineered to express IL-2. At 14 days post-implantation, tumors expressing IL-10 + IL-2 were 99% smaller than control-transfected tumors (p < 0.0001). This extent of anti-tumor effect could not be achieved by expression of IL-10 or IL-2 alone within tumors. Neither IL-10 nor a combination of IL-10 + IL-2 gene delivery inhibited tumor growth in severe combined immunodeficient (SCID-Beige) mice (p > 0.05). Immunohistochemical analysis revealed that IL-10 + IL-2 gene delivery markedly increased T-cell infiltration within the striatum ipsilateral to tumor cell implantation. These findings establish that IL-10 expression, particularly in combination with IL-2 expression, can have significant immune-dependent anti-tumor actions within intracranial gliomas.
机译:这项研究检查了白介素10(IL-10)和IL-10 + IL-2组合基因转移对体内实验性脑肿瘤生长的影响。将9L胶质肉瘤细胞改造成稳定表达鼠类IL-10(9L-IL-10细胞),然后皮下植入或植入到同系大鼠的尾状/丘状。与对照肿瘤相比,表达IL-10的肿瘤的生长明显减少(p <0.05)。通过将9L-IL-10细胞与经过工程改造以表达IL-2的内皮细胞共植入,可以建立表达IL-10和IL-2的颅内肿瘤。植入后第14天,表达IL-10 + IL-2的肿瘤比对照转染的肿瘤小99%(p <0.0001)。通过在肿瘤内单独表达IL-10或IL-2不能达到这种程度的抗肿瘤作用。 IL-10或IL-10 + IL-2基因递送的组合均不能抑制严重的联合免疫缺陷(SCID-Beige)小鼠的肿瘤生长(p> 0.05)。免疫组织化学分析显示,IL-10 + IL-2基因的递送显着增加了肿瘤细胞植入同侧纹状体内T细胞的浸润。这些发现建立了IL-10表达,特别是与IL-2表达组合,在颅内神经胶质瘤内可以具有重要的免疫依赖性抗肿瘤作用。

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