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Balancing the pharmacokinetics and pharmacodynamics of interferon-α2b and human serum albumin fusion protein by proteolytic or reductive cleavage increases its in vivo therapeutic efficacy

机译:通过蛋白水解或还原裂解平衡干扰素-α2b和人血清白蛋白融合蛋白的药代动力学和药效动力学可提高其体内治疗功效

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摘要

Human serum albumin (HSA) fusion (Albufusion) technology has evolved to be a general strategy to increase the in vivo half-lives of therapeutic proteins. However, because of the steric hindrance effect of HSA, conventional Albufusion technology improves the pharmacokinetics (PK) at the cost of pharmacodynamics (PD). To achieve balanced PK and PD of interferon-α2b (IFN-α2b) and HSA fusion protein, protease cleavage sites or disulfide linkage that enabled releasing of intact IFN-α2b with full activity was introduced between these two moieties. Nonreleasable and releasable fusion proteins showed similar cell surface receptor binding affinities; however, releasable fusion proteins exhibited release efficiency proportional increase of in vitro antiviral and antiproliferative activities. The release rate also had a profound impact on the in vivo pharmaceutical properties of fusion proteins. Releasable fusion proteins with intermediate release rate had the most balanced PK and PD, which translated into improved therapeutic efficacy in the HT29 human colon cancer xenograft model. Releasable Albufusion (rAlbufusion) allows tailored design of the PK/PD profile and greatly extends the utility of conventional Albufusion technology.
机译:人血清白蛋白(HSA)融合(Albufusion)技术已发展成为增加治疗性蛋白体内半衰期的一般策略。但是,由于HSA的空间位阻效应,传统的Albufusion技术以药效学(PD)为代价提高了药代动力学(PK)。为了实现干扰素-α2b(IFN-α2b)和HSA融合蛋白的PK和PD平衡,在这两个部分之间引入了蛋白酶裂解位点或二硫键,使完整的IFN-α2b能够完全释放。不可释放和可释放融合蛋白显示出相似的细胞表面受体结合亲和力。然而,可释放的融合蛋白表现出的释放效率与体外抗病毒和抗增殖活性成比例地增加。释放速率也对融合蛋白的体内药物性质产生深远影响。具有中等释放速率的可释放融合蛋白具有最平衡的PK和PD,在HT29人结肠癌异种移植模型中转化为更高的治疗效果。可释放的Albufusion(rAlbufusion)允许对PK / PD曲线进行量身定制的设计,并大大扩展了传统Albufusion技术的实用性。

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