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Assessment of the Higher-Order Structure of Formulated Monoclonal Antibody Therapeutics by 2D Methyl Correlated NMR and Principal Component Analysis

机译:评估的高阶结构制定由2 d单克隆抗体疗法甲基核磁共振相关和主成分分析

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摘要

Characterization of the higher-order structure (HOS) of protein therapeutics, and in particular of monoclonal antibodies, by 2D 1H-13C methyl correlated NMR has been demonstrated as precise and robust. Such characterization can be greatly enhanced when collections of spectra are analyzed using multivariate approaches such as principal component analysis (PCA), allowing for the detection and identification of small structural differences in drug substance that may otherwise fall below the limit of detection of conventional spectral analysis. A major limitation to this approach is the presence of aliphatic signals from formulation or excipient components, which result in spectral interference with the protein signal of interest; however, the recentlydescribed Selective £xcipient deduction and Removal (SIERRA) filter greatly reduces this issue. Here we will outline how basic 2D ~1H-~(13)C methyl-correlated NMR may be combined with the SIERRA approach to collect ‘clean’ NMR spectra of formulated monoclonal antibody therapeutics (i.e., drug substance spectra free of interfering component signals), and how series of such spectra may be used for HOS characterization by direct PCA of the series spectral matrix.
机译:描述的高阶结构累积量的蛋白质疗法,特别是的单克隆抗体,通过2 d 1 h-13c甲基相关核磁共振已经证明是准确的和鲁棒性。增强当集合的光谱进行了分析使用多元主体等方法成分分析(PCA),允许的小结构的探测和识别不同的药物可能其他的物质低于常规的检测极限光谱分析。方法是脂肪族的存在的信号从配方或赋形剂组件导致光谱干扰蛋白质感兴趣的信号;recentlydescribed选择性£xcipient扣除和删除(塞拉利昂)滤波器大大减少问题。~ 1 h - ~ (13) C methyl-correlated NMR可能的总和SIERRA方法收集‘干净’NMR光谱的单克隆抗体制定治疗(例如,免费药物质谱干扰分量信号),以及系列这样的光谱可以用于累积量直接PCA特征的系列谱矩阵。

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