首页> 外文期刊>Cytokine >IL-15:IL-15 receptor alpha superagonist complex: high-level co-expression in recombinant mammalian cells, purification and characterization.
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IL-15:IL-15 receptor alpha superagonist complex: high-level co-expression in recombinant mammalian cells, purification and characterization.

机译:IL-15:IL-15受体α超激动剂复合物:在重组哺乳动物细胞中高水平共表达,纯化和鉴定。

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摘要

IL-15, a promising cytokine for treating cancer and viral diseases, is presented in trans by the IL-15 receptor (IL-15R) alpha-chain to the IL-15Rbetagammac complex displayed on the surface of T cells and natural killer (NK) cells. We previously reported that an asparagine to aspartic acid substitution at amino acid 72 (N72D) of IL-15 provides a 4-5-fold increase in biological activity compared to the native molecule. In this report, we describe Chinese hamster ovary (CHO) cell expression of a soluble complex (IL-15 N72D:IL-15RalphaSu/Fc) consisting of the IL-15 N72D superagonist and a dimeric IL-15Ralpha sushi domain-IgG1 Fc fusion protein. A simple but readily scalable affinity and ion exchange chromatography method was developed to highly purify the complex having both IL-15 binding sites fully occupied. The immunostimulatory effects of this complex were confirmed using cell proliferation assays. Treatment of mice with a single intravenous dose of IL-15N72D:IL-15RalphaSu/Fc resulted in a significant increase in CD8+ T cells and NK cells that was not observed following IL-15 treatment. Pharmacokinetic analysis indicated that the complex has a 25-h half-life in mice which is considerably longer than <40-min half-life of IL-15. Thus, the enhanced activity of the IL-15N72D:IL-15RalphaSu/Fc complex is likely the result of the increased binding activity of IL-15N72D to IL-15Rbetagammac, optimized cytokine trans-presentation by the IL-15RalphaSu domain, the dimeric nature of the cytokine domain and its increased in vivo half-life compared to IL-15. These findings indicate that this IL-15 superagonist complex could serve as a superior immunostimulatory therapeutic agent.
机译:IL-15是一种有望用于治疗癌症和病毒性疾病的细胞因子,它通过IL-15受体(IL-15R)α链反式呈现给T细胞和自然杀伤分子(NK)表面上显示的IL-15Rbetagammac复合物) 细胞。我们先前曾报道,与天然分子相比,IL-15的氨基酸72(N72D)处的天冬酰胺取代天冬氨酸可提供4-5倍的生物学活性。在此报告中,我们描述了由IL-15 N72D超激动剂和二聚体IL-15Ralpha Sushi结构域-IgG1 Fc融合物组成的可溶性复合物(IL-15 N72D:IL-15RalphaSu / Fc)的中国仓鼠卵巢(CHO)细胞表达蛋白。开发了一种简单但易于扩展的亲和力和离子交换色谱方法,以高度纯化具有两个IL-15结合位点均被占据的复合物。使用细胞增殖测定法证实了该复合物的免疫刺激作用。用单次静脉注射剂量的IL-15N72D:IL-15RalphaSu / Fc处理小鼠会导致IL-8治疗后未观察到CD8 + T细胞和NK细胞显着增加。药代动力学分析表明,该复合物在小鼠中具有25小时的半衰期,这比IL-15的<40分钟半衰期要长得多。因此,IL-15N72D:IL-15RalphaSu / Fc复合物活性的增强可能是由于IL-15N72D与IL-15Rbetagammac的结合活性增强,IL-15RalphaSu结构域优化的细胞因子反式呈递,二聚体性质的结果。与IL-15相比,细胞因子结构域的抗衰老作用及其增加的体内半衰期。这些发现表明,该IL-15超激动剂复合物可以用作优良的免疫刺激治疗剂。

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