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Critical reagent characterization and re-evaluation to ensure long-term stability: two case studies

机译:关键试剂表征和重新评估,以确保长期稳定性:两种案例研究

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摘要

Characterization of critical reagents can mitigate adverse impact to ligand-binding assay performance. We investigated the conjugation conditions of a bispecific protein to SULFO-TAG NHS-Ester (TM) ruthenium to resolve a steady increase in ligand-binding assay background signal. Functional and biophysical attributes in stability samples revealed low pH (4.0) conjugation and formulation buffers were key to decrease aggregate formation. We also identified pH-specific (3.0) purification conditions to reduce aggregate levels from 37% to <5% of a mouse IgG3 reagent antibody. These case studies support the utility of biophysical and functional characterization of critical reagents as a proactive approach to maintain long-term stability and provide the basis for our recommendations a risk-based approach to establish re-evaluation intervals for traditional and novel reagents.
机译:关键试剂的表征可以减轻对配体结合分析性能的不利影响。我们研究了双特异性蛋白质与磺基标记NHS酯(TM)钌的结合条件,以解决配体结合分析背景信号的稳定增加。稳定性样品的功能和生物物理特性表明,低pH(4.0)共轭和配方缓冲液是减少聚集形成的关键。我们还确定了pH特异性(3.0)纯化条件,以将小鼠IgG3试剂抗体的聚集水平从37%降至<5%。这些案例研究支持将关键试剂的生物物理和功能表征作为维持长期稳定性的主动方法,并为我们的建议提供了基础,即基于风险的方法,以建立传统和新型试剂的重新评估间隔。

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