Improved variants of SrtA for site-specific conjugation on antibodies and proteins with high efficiency

改进的 SrtA 变体,用于高效地与抗体和蛋白质进行位点特异性结合

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作者:Long Chen, Justin Cohen, Xiaoda Song, Aishan Zhao, Zi Ye, Christine J Feulner, Patrick Doonan, Will Somers, Laura Lin, Peng R Chen

Abstract

Sortase mediated ligation is a highly specific platform for conjugation that relies on the specificity of the transpeptidase Sortase A (SrtA) for short peptide sequences (LPXTG and GGG). SrtA retains its specificity while accepting a wide range of potential substrates, but its broad use is limited by the wild-type enzyme's poor kinetics, which require large amounts of SrtA and extended reaction times for efficient conjugation. Prior explorations have aimed to improve the kinetics of SrtA with limited success. Herein we describe the discovery of further improved SrtA variants with increased efficiency for the conjugation reaction, and demonstrate their robustness in labelling proteins and antibodies in a site-specific manner. Our variants require significantly lower amounts of enzyme than WT SrtA and can be used to attach small molecules to the N or C-terminus of the heavy or light chain in antibodies with excellent yields. These improved variants can also be used for highly efficient site-specific PEGylation.

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