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Using heat conduction microcalorimetry to study thermal aggregation kinetics of proteins

机译:使用热导微量热法研究蛋白质的热聚集动力学

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摘要

The thermally induced irreversible aggregation of a monoclonal antibody in different pH buffers was investigated using different techniques such as micro-differential scanning calorimetry (micro-DSC), size exclusion HPLC (SEC) and isothermal microcalorimetry. The kinetics of aggregation of the protein was analyzed in terms of a Lumry-Eyring model proceeding via a non-native conformational state. The rate constants and reaction enthalpies of unfolding and consequent aggregation were obtained by fitting the isothermal microcalorimetric and SEC data based on proposed aggregation mechanisms. The consistency of rate constants obtained via isothermal microcalorimetry and SEC indicates it is possible to deconvolute the observed microcalorimetry power-time data obtained from thermally induced protein aggregation.
机译:使用微差示扫描量热法(micro-DSC),体积排阻HPLC(SEC)和等温微量量热法等不同技术研究了在不同pH缓冲液中单克隆抗体的热诱导不可逆聚集。根据通过非天然构象状态进行的Lumry-Eyring模型,分析了蛋白质聚集的动力学。通过基于提出的聚集机制拟合等温微量热法和SEC数据,获得了展开和随后聚集的速率常数和反应焓。通过等温微量热法和SEC获得的速率常数的一致性表明,可以对从热诱导蛋白质聚集获得的观测微量热法功率时间数据进行反卷积。

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