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Combining different design strategies for rational affinity maturation of the MICA-NKG2D interface

机译:结合不同的设计策略以实现MICA-NKG2D接口的合理亲和力成熟

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摘要

We redesigned residues on the surface of MICA, a protein that binds the homodimeric immunoreceptor NKG2D, to increase binding affinity with a series of rational, incremental changes. A fixed-backbone RosettaDesign protocol scored a set of initial mutations, which we tested by surface plasmon resonance for thermodynamics and kinetics of NKG2D binding, both singly and in combination. We combined the best four mutations at the surface with three affinity-enhancing mutations below the binding interface found with a previous design strategy. After curating design scores with three cross-validated tests, we found a linear relationship between free energy of binding and design score, and to a lesser extent, enthalpy and design score. Multiple mutants bound with substantial subadditivity, but in at least one case full additivity was observed when combining distant mutations. Altogether, combining the best mutations from the two strategies into a septuple mutant enhanced affinity by 50-fold, to 50 nM, demonstrating a simple, effective protocol for affinity enhancement.
机译:我们重新设计了MICA表面的残基,MICA是一种与同源二聚体免疫受体NKG2D结合的蛋白质,可通过一系列合理的增量变化来增加结合亲和力。固定骨干RosettaDesign协议对一组初始突变进行了评分,我们通过表面等离振子共振对NKG2D结合的热力学和动力学进行了单独或组合的测试。我们将表面上最好的四个突变与以前设计策略中发现的结合界面下方的三个亲和力增强突变结合在一起。在通过三个交叉验证的测试确定设计分数之后,我们发现了结合自由能与设计分数之间的线性关系,在较小程度上,焓与设计分数之间也存在线性关系。多个突变体具有实质性的亚可加性结合,但在至少一种情况下,结合远处的突变可观察到完全可加性。总而言之,将两种策略中的最佳突变组合成一个七肽突变体,可使亲和力提高50倍,达到50 nM,这证明了一种简单,有效的亲和力增强方案。

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