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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >IL-7/anti-IL-7 mAb complexes augment cytokine potency in mice through association with IgG-Fc and by competition with IL-7R.
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IL-7/anti-IL-7 mAb complexes augment cytokine potency in mice through association with IgG-Fc and by competition with IL-7R.

机译:IL-7 /抗IL-7 mAb复合物可通过与IgG-Fc结合并与IL-7R竞争来增强小鼠的细胞因子效力。

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Interleukin-7 (IL-7) is essential to T-cell survival as well as homeostatic proliferation, and clinical trials that exploit the mitogenic effects of IL-7 have achieved success in treating human diseases. In mice, the in vivo potency of IL-7 improves dramatically when it is administered as a complex with the anti-IL-7 neutralizing monoclonal antibody clone M25. However, the mechanism whereby M25 augments IL-7 potency is unknown. We have analyzed the discrete contributions of the antibody constant (Fc) and IL-7-binding (Fab) domains to the mechanism. By engaging the neonatal Fc receptor the Fc domain extends the in vivo lifespan of IL-7/M25 complexes and accounts for the majority of their activity. Unexpectedly, the IL-7-neutralizing Fab domain provides an additional, albeit smaller, contribution, possibly by serving as a cytokine depot. This study is the first to demonstrate that the neutralizing aspect of the monoclonal antibody is directly involved in enhancing the potency of a cytokine with a single form of receptor. Lessons from the mechanism of IL-7/M25 complexes inform the design of next-generation cytokine therapeutics.
机译:白细胞介素7(IL-7)对T细胞存活以及稳态增殖至关重要,利用IL-7的促有丝分裂作用的临床试验已成功治疗人类疾病。在小鼠中,当与抗IL-7中和性单克隆抗体克隆M25配合使用时,IL-7的体内效力会大大提高。但是,M25增强IL-7效力的机制尚不清楚。我们已经分析了抗体恒定(Fc)和IL-7结合(Fab)结构域对该机制的离散贡献。通过接合新生儿Fc受体,Fc结构域延长了IL-7 / M25复合物的体内寿命,并占据了其大部分活性。出乎意料的是,中和IL-7的Fab结构域可能通过充当细胞因子库而提供了额外的,尽管较小的贡献。这项研究首次证明单克隆抗体的中和方面直接参与增强具有单一形式受体的细胞因子的效力。 IL-7 / M25复合物机理的经验教训为下一代细胞因子疗法的设计提供了参考。

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