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Engineering a bacterial sialyltransferase for di-sialylation of a therapeutic antibody

Org Biomol Chem. 2020; 
Mingqun Wang, Yue Wang, Kaimeng Liu, Xiaodong Dou, Zhenming Liu, Liangren Zhang, Xin-Shan Ye
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Plasmid DNA Preparation … Terminal truncation of Psp2,6ST (16–511)-His 6 A366G. Psp2,6ST (16–511)-His 6 A366G gene (Genscript, Nanjing in China) harbored in the plasmid pET-22b(+) was used as a template for the terminal truncation study. DNA sequencing verified the truncations … Get A Quote

摘要

Terminal α-2,6-sialylation of N-glycans is a humanized glycosylation that affects the properties and efficacy of therapeutic glycoproteins. Fc di-sialylation (a biantennary N-glycan with two α-2,6-linked sialic acids) of IgG antibodies imparts them with enhanced anti-inflammatory activity and other roles. However, the microheterogeneity of N-glycoforms presents a challenge for therapeutic development. Therefore, controlled sialylation has drawn considerable attention, but direct access to well-defined di-sialylated antibodies remains limited. Herein, a one-pot three-enzyme protocol was developed by engineering a bacterial sialyltransferase to facilitate the modification of therapeutic antibodies with N-acetyl... More

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