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The p40 Subunit of Interleukin (IL)-12 Promotes Stabilization and Export of the p35 Subunit

机译:白介素(IL)-12的p40亚基促进p35亚基的稳定和输出

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摘要

IL-12 is a 70-kDa heterodimeric cytokine composed of the p35 and p40 subunits. To maximize cytokine production from plasmid DNA, molecular steps controlling IL-12p70 biosynthesis at the posttranscriptional and posttranslational levels were investigated. We show that the combination of RNA/codon-optimized gene sequences and fine-tuning of the relative expression levels of the two subunits within a cell resulted in increased production of the IL-12p70 heterodimer. We found that the p40 subunit plays a critical role in enhancing the stability, intracellular trafficking, and export of the p35 subunit. This posttranslational regulation mediated by the p40 subunit is conserved in mammals. Based on these findings, dual gene expression vectors were generated, producing an optimal ratio of the two subunits, resulting in a ∼1 log increase in human, rhesus, and murine IL-12p70 production compared with vectors expressing the wild type sequences. Such optimized DNA plasmids also produced significantly higher levels of systemic bioactive IL-12 upon in vivo DNA delivery in mice compared with plasmids expressing the wild type sequences. A single therapeutic injection of an optimized murine IL-12 DNA plasmid showed significantly more potent control of tumor development in the B16 melanoma cancer model in mice. Therefore, the improved IL-12p70 DNA vectors have promising potential for in vivo use as molecular vaccine adjuvants and in cancer immunotherapy.
机译:IL-12是由p35和p40亚基组成的70 kDa异二聚体细胞因子。为了使质粒DNA的细胞因子产量最大化,研究了在转录后和翻译后水平控制IL-12p70生物合成的分子步骤。我们表明RNA /密码子优化的基因序列和细胞内两个亚基的相对表达水平的微调的组合导致IL-12p70异二聚体的生产增加。我们发现,p40亚基在增强p35亚基的稳定性,细胞内运输和出口中起着关键作用。由p40亚基介导的这种翻译后调节在哺乳动物中是保守的。基于这些发现,产生了双基因表达载体,产生了两个亚基的最佳比例,与表达野生型序列的载体相比,人类,恒河猴和鼠类IL-12p70的产量增加了约1个对数。与表达野生型序列的质粒相比,在小鼠体内体内DNA递送时,这种优化的DNA质粒还产生显着更高水平的全身生物活性IL-12。优化的鼠IL-12 DNA质粒的单次治疗性注射在小鼠的B16黑色素瘤癌症模型中显示出对肿瘤发展的更有效控制。因此,改进的IL-12p70 DNA载体在体内用作分子疫苗佐剂和癌症免疫治疗方面具有广阔的前景。

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