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依那西普中二硫键的结构-功能关系。

The structure-function relationship of disulfide bonds in etanercept.

机构信息

Sandoz Biopharmaceuticals, Sandoz GmbH, Biochemiestraße 10, 6250, Kundl, Austria.

Technical Development Biosimilars, Biologics Technical Development and Manufacturing, Novartis, Sandoz GmbH, Biochemiestraße 10, 6250, Kundl, Austria.

出版信息

Sci Rep. 2017 Jun 21;7(1):3951. doi: 10.1038/s41598-017-04320-5.

Abstract

Etanercept is a TNFα receptor Fc fusion protein used for the treatment of rheumatic disease and psoriasis. Physicochemical and functional investigation of process fractions during development of the etanercept biosimilar GP2015 (Erelzi) revealed a correlation between reduced potency and incorrect disulfide bridging between specific cysteines in the receptor domain. This novel structure-function relationship was found to be the molecular basis for reduced potency in recent Enbrel batches, which exhibit higher levels of incorrect disulfide bridging. Interestingly, incorrect disulfide bridging was found to be reversible under serum-like redox conditions, restoring potency to normal levels. This redox dependent reversibility suggests that these variants are likely not relevant for clinical efficacy once the drug enters the bloodstream. Nonetheless, incorrect disulfide bridging in etanercept represents a new quality attribute that is critical for biopharmaceutical functionality and should thus be carefully monitored and controlled to guarantee patient safety.

摘要

依那西普是一种 TNFα 受体 Fc 融合蛋白,用于治疗风湿性疾病和银屑病。在依那西普生物类似药 GP2015(Erelzi)的开发过程中,对工艺馏分进行理化性质和功能研究,揭示了效力降低与受体结构域中特定半胱氨酸之间错误二硫键形成之间存在相关性。这种新的结构-功能关系是最近 Enbrel 批次效力降低的分子基础,这些批次表现出更高水平的错误二硫键形成。有趣的是,在类似于血清的氧化还原条件下,发现错误二硫键形成是可逆的,将效力恢复到正常水平。这种依赖于氧化还原的可逆性表明,一旦药物进入血液,这些变体可能与临床疗效无关。尽管如此,依那西普中的错误二硫键代表了一个新的质量属性,对于生物制药功能至关重要,因此应仔细监测和控制,以保证患者安全。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b227/5479810/797bab4a3c70/41598_2017_4320_Fig1_HTML.jpg

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