期刊
ANGEWANDTE CHEMIE-INTERNATIONAL EDITION
卷 57, 期 33, 页码 10646-10650出版社
WILEY-V C H VERLAG GMBH
DOI: 10.1002/anie.201806053
关键词
bioconjugation; click chemistry; cysteine; protein engineering; site-specific labeling
资金
- French Government through the French National Research Agency (ANR) under the programs Investissements d'Avenir (IMAPPI Equipex)
- AAP Generique 2017 (project ZINELABEL)
- CNRS
- Universite de Bourgogne
- Conseil Regional de Bourgogne through the 3MIM program
- Conseil Regional de Bourgogne Franche-Comte through the Plan d'Action Regional pour l'Innovation (PARI)
- European Union through the PO FEDER-FSE Bourgogne program
Dual-labeled biomolecules constitute a new generation of bioconjugates with promising applications in therapy and diagnosis. Unfortunately, the development of these new families of biologics is hampered by the technical difficulties associated with their construction. In particular, the site specificity of the conjugation is critical as the number and position of payloads can have a dramatic impact on the pharmacokinetics of the bioconjugate. Herein, we introduce dichlorotetrazine as a trivalent platform for the selective double modification of proteins on cysteine residues. This strategy is applied to the dual labeling of albumin with a macrocyclic chelator for nuclear imaging and a fluorescent probe for fluorescence imaging.
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