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Investigating a Boronate-Affinity-Guided Acylation Reaction for Labelling Native Antibodies.

Avijit K AdakKuan-Ting HuangChien-Yu LiaoYuan-Jung LeeWen-Hua KuoYi-Ren HuoPei-Jhen LiYi-Ju ChenBo-Shiun ChenYu-Ju ChenKuo-Chu HwangWun-Shang Wayne ChangChun-Cheng Lin
Published in: Chemistry (Weinheim an der Bergstrasse, Germany) (2022)
The excellent molecular recognition capabilities of monoclonal antibodies (mAbs) have opened up exciting opportunities for biotherapeutic discovery. Taking advantage of the full potential of this tool necessitates affinity ligands capable of conjugating directly with small molecules to a defined degree of biorthogonality, especially when modifying natural Abs. Herein, a bioorthogonal boronate-affinity-based Ab ligand featuring a 4-(dimethylamino)pyridine and an S-aryl thioester to label full-length Abs is reported. The photoactivatable linker in the acyl donor facilitated purification of azide-labelled Ab (N 3 -Ab) was quantitatively cleaved upon brief exposure to UV light while retaining the original Ab activity. Click reactions enabled the precise addition of biotin, a fluorophore, and a pharmacological agent to the purified N 3 -Abs. The resulting immunoconjugate showed selectivity against targeted cells. Bioorthogonal traceless design and reagentless purification allow this strategy to be a powerful tool to engineer native antibodies amenable to therapeutic intervention.
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