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High efficiency cell-specific targeting of cytokine activity

机译:细胞因子活性的高效细胞特异性靶向

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摘要

Systemic toxicity currently prevents exploiting the huge potential of many cytokines for medical applications. Here we present a novel strategy to engineer immunocytokines with very high targeting efficacies. The method lies in the use of mutants of toxic cytokines that markedly reduce their receptor-binding affinities, and that are thus rendered essentially inactive. Upon fusion to nanobodies specifically binding to marker proteins, activity of these cytokines is selectively restored for cell populations expressing this marker. This ‘activity-by-targeting’ concept was validated for type I interferons and leptin . In the case of interferon, activity can be directed to target cells in vitro and to selected cell populations in mice, with up to 1,000-fold increased specific activity. This targeting strategy holds promise to revitalize the clinical potential of many cytokines.
机译:目前,全身毒性阻止了许多细胞因子在医学应用中的巨大潜力的开发。在这里,我们提出了一种新的策略来设计具有很高靶向效率的免疫细胞因子。该方法在于使用毒性细胞因子的突变体,该突变体显着降低了它们的受体结合亲和力,因此使其基本上无活性。在与特异性结合标志物蛋白的纳米抗体融合后,针对表达该标志物的细胞群体选择性地恢复了这些细胞因子的活性。这种“针对目标的活动”概念已针对I型干扰素和瘦素进行了验证。在干扰素的情况下,可以将活性定向到体外靶细胞和小鼠中选定的细胞群,比活性最多提高1000倍。这种靶向策略有望振兴许多细胞因子的临床潜力。

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