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Optimizing antibody affinity and stability by the automated design of the variable light-heavy chain interfaces

机译:通过可变轻链链界面的自动化设计优化抗体亲和力和稳定性

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摘要

Antibodies developed for research and clinical applications may exhibit suboptimal stability, expressibility, or affinity. Existing optimization strategies focus on surface mutations, whereas natural affinity maturation also introduces mutations in the antibody core, simultaneously improving stability and affinity. To systematically map the mutational tolerance of an antibody variable fragment (Fv), we performed yeast display and applied deep mutational scanning to an anti-lysozyme antibody and found that many of the affinity-enhancing mutations clustered at the variable light-heavy chain interface, within the antibody core. Rosetta design combined enhancing mutations, yielding a variant with tenfold higher affinity and substantially improved stability. To make this approach broadly accessible, we developed AbLIFT, an automated web server that designs multipoint core mutations to improve contacts between specific Fv light and heavy chains (). We applied AbLIFT to two unrelated antibodies targeting the human antigens VEGF and QSOX1. Strikingly, the designs improved stability, affinity, and expression yields. The results provide proof-of-principle for bypassing laborious cycles of antibody engineering through automated computational affinity and stability design.
机译:为研究和临床应用而开发的抗体可能表现出次优的稳定性,可表达性或亲和力。现有的优化策略专注于表面突变,而自然亲和力成熟也会在抗体核心中引入突变,同时提高稳定性和亲和力。为了系统地绘制抗体可变片段(Fv)的突变耐受性,我们进行了酵母展示,并对抗溶菌酶抗体进行了深层突变扫描,发现许多亲和力增强突变都聚集在可变轻链界面上,在抗体核心内。 Rosetta设计结合了增强的突变,产生的亲和力提高了十倍,稳定性大大提高。为了使这种方法广泛可用,我们开发了一种自动Web服务器AbLIFT,该服务器设计了多点核心突变,以改善特定Fv轻链和重链之间的联系。我们将AbLIFT应用于针对人抗原VEGF和QSOX1的两种无关抗体。引人注目的是,这些设计提高了稳定性,亲和力和表达产量。结果为通过自动计算亲和力和稳定性设计绕过抗体工程的繁重循环提供了原理证明。

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