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Synthesis of site-specific Fab-drug conjugates using ADP-ribosyl cyclases

Protein Sci. 2024-04; 
Hyo Sun Kim, Kimia Hariri, Xiao-Nan Zhang, Liang-Chieh Chen, Benjamin B Katz, Hua Pei, Stan G Louie, Yong Zhang
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Proteins, Expression, Isolation and Analysis … 5 days, media were collected and loaded through Protein G resins (GenScript, NJ) for purification. Eluted … Protein concentrations were measured with a Nanodrop 2000C spectrometer. … Get A Quote

摘要

Targeted delivery of small-molecule drugs via covalent attachments to monoclonal antibodies has proved successful in clinic. For this purpose, full-length antibodies are mainly used as drug-carrying vehicles. Despite their flexible conjugation sites and versatile biological activities, intact immunoglobulins with conjugated drugs, which feature relatively large molecular weights, tend to have restricted tissue distribution and penetration and low fractions of payloads. Linking small-molecule therapeutics to other formats of antibody may lead to conjugates with optimal properties. Here, we designed and synthesized ADP-ribosyl cyclase-enabled fragment antigen-binding (Fab) drug conjugates (ARC-FDCs) by utilizing ... More

關鍵詞

CD38, antibody, antibody-drug conjugate, protein engineering, targeted delivery
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