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首页> 外文期刊>FEBS letters. >Mass spectrometry for the biophysical characterization of therapeutic monoclonal antibodies
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Mass spectrometry for the biophysical characterization of therapeutic monoclonal antibodies

机译:质谱法用于治疗性单克隆抗体的生物物理表征

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摘要

Monoclonal antibodies (mAbs) are powerful therapeutics, and their characterization has drawn considerable attention and urgency. Unlike small-molecule drugs (150-600 Da) that have rigid structures, mAbs (~150 kDa) are engineered proteins that undergo complicated folding and can exist in a number of low-energy structures, posing a challenge for traditional methods in structural biology. Mass spectrometry (MS)-based biophysical characterization approaches can provide structural information, bringing high sensitivity, fast turnaround, and small sample consumption. This review outlines various MS-based strategies for protein biophysical characterization and then reviews how these strategies provide structural information of mAbs at the protein level (intact or top-down approaches), peptide, and residue level (bottom-up approaches), affording information on higher order structure, aggregation, and the nature of antibody complexes.
机译:单克隆抗体(mAbs)是强大的治疗方法,其表征引起了相当大的关注和紧迫性。与具有刚性结构的小分子药物(150-600 Da)不同,mAb(〜150 kDa)是经过工程改造的蛋白,会经历复杂的折叠并可能以许多低能结构存在,这对结构生物学的传统方法提出了挑战。基于质谱(MS)的生物物理表征方法可提供结构信息,带来高灵敏度,快速周转和少量样品消耗。这篇综述概述了各种基于MS的蛋白质生物物理表征策略,然后回顾了这些策略如何在蛋白质水平(完整或自上而下的方法),肽和残基水平(自下而上的方法)提供mAb的结构信息,从而提供信息抗体复合物的高阶结构,聚集和性质。

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