首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >In Vivo Hydrodynamic Delivery of cDNA Encoding IL-2:Rapid,Sustained Redistribution,Activation of Mouse NK Cells,and Therapeutic Potential in the Absence of NKT Cells
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In Vivo Hydrodynamic Delivery of cDNA Encoding IL-2:Rapid,Sustained Redistribution,Activation of Mouse NK Cells,and Therapeutic Potential in the Absence of NKT Cells

机译:编码IL-2的cDNA的体内流体动力学传递:快速,持续的重新分布,小鼠NK细胞的活化以及在缺少NKT细胞的情况下的治疗潜力

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In the present study,we have tested the ability of hydrodynamically delivered IL-2 cDNA to modulate the number and function of murine leukocyte subsets in different organs and in mice of different genetic backgrounds,and we have evaluated effects of this mode of gene delivery on established murine tumor metastases.Hydrodynamic administration of the IL-2 gene resulted in the rapid and transient production of up to 160 ng/ml IL-2 in the serum.The appearance of IL-2 was followed by transient production of IFN-gamma and a dramatic and sustained increase in NK cell numbers and NK-mediated cytolytic activity in liver and spleen leukocytes.In addition,significant increases in other lymphocyte subpopulations(e.g.,NKT,T,and B cells)that are known to be responsive to IL-2 were observed following IL-2 cDNA plasmid delivery.Finally,hydrodynamic delivery of only 4 mug of the IL-2 plasmid to mice bearing established lung and liver metastases was as effective in inhibiting progression of metastases as was the administration of large amounts(100,000 IU/twice daily)of IL-2 protein.Studies performed in mice bearing metastatic renal cell tumors demonstrated that the IL-2 cDNA plasmid was an effective treatment against liver metastasis and moderately effective against lung metastasis.Collectively,these results demonstrate that hydrodynamic delivery of relatively small amounts of IL-2 cDNA provides a simple and inexpensive method to increase the numbers of NK and NKT cells,to induce the biological effects of IL-2 in vivo for use in combination with other biological agents,and for studies of its antitumor activity.
机译:在本研究中,我们测试了水动力传递的IL-2 cDNA调节不同器官和不同遗传背景的小鼠中鼠白细胞亚群的数量和功能的能力,并评估了这种基因传递方式对小鼠白细胞的作用。建立了小鼠肿瘤转移瘤.IL-2基因的水力给药导致血清中迅速和瞬时产生高达160 ng / ml的IL-2.IL-2出现后,瞬时产生IFN-γ和肝和脾白细胞中NK细胞数量和NK介导的溶细胞活性的持续显着增加。此外,已知对IL-有反应的其他淋巴细胞亚群(例如NKT,T和B细胞)显着增加。 IL-2 cDNA质粒递送后观察到2个。最后,仅4杯IL-2质粒对携带已确定的肺和肝转移的小鼠进行流体动力学递送对抑制转移的进展同样有效。 s是施用大量(每天100,000 IU /天两次)的IL-2。在患有转移性肾细胞瘤的小鼠中进行的研究表明,IL-2 cDNA质粒可有效治疗肝转移,对肺转移具有中度治疗总的来说,这些结果表明,相对少量的IL-2 cDNA的流体动力学递送提供了一种简单且廉价的方法来增加NK和NKT细胞的数量,从而在体内诱导IL-2的生物学效应,从而与其他生物制剂,以及用于研究其抗肿瘤活性。

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