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Differential scanning fluorimetry based assessments of the thermal and kinetic stability of peptide-MHC complexes

机译:基于差示扫描荧光法的肽-MHC复合物热和动力学稳定性评估

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摘要

Measurements of thermal stability by circular dichroism (CD) spectroscopy have been widely used to assess the binding of peptides to MHC proteins, particularly within the structural immunology community. Although thermal stability assays offer advantages over other approaches such as IC50 measurements, CD-based stability measurements are hindered by large sample requirements and low throughput. Here we demonstrate that an alternative approach based on differential scanning fluorimetry (DSF) yields results comparable to those based on CD for both class I and class II complexes. As they require much less sample, DSF-based measurements reduce demands on protein production strategies and are amenable for high throughput studies. DSF can thus not only replace CD as a means to assess peptide/MHC thermal stability, but can complement other peptide-MHC binding assays used in screening, epitope discovery, and vaccine design. Due to the physical process probed, DSF can also uncover complexities not observed with other techniques. Lastly, we show that DSF can also be used to assess peptide/MHC kinetic stability, allowing a single experimental setup to probe both binding equilibria and kinetics.
机译:通过圆二色性(CD)光谱测量热稳定性已广泛用于评估肽与MHC蛋白的结合,特别是在结构免疫学界。尽管热稳定性分析提供了优于其他方法(例如IC50测量)的优势,但基于CD的稳定性测量受到样品需求量大和通量低的困扰。在这里,我们证明了基于差示扫描荧光法(DSF)的替代方法产生的结果可与基于CD的I类和II类络合物相媲美。由于它们需要的样品少得多,因此基于DSF的测量减少了对蛋白质生产策略的要求,适合进行高通量研究。因此,DSF不仅可以代替CD作为评估肽/ MHC热稳定性的手段,而且可以补充筛选,表位发现和疫苗设计中使用的其他肽-MHC结合测定。由于探究了物理过程,DSF还可以发现其他技术未发现的复杂性。最后,我们证明DSF也可用于评估肽/ MHC动力学稳定性,从而允许进行单个实验设置以探究结合平衡和动力学。

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