| Literature DB >> 26315561 |
Joong-Jae Lee1, Hyo-Jung Choi2, Misun Yun3, YingJin Kang4, Ji-Eun Jung2, Yiseul Ryu1, Tae Yoon Kim1, Young-Je Cha4, Hyun-Soo Cho5, Jung-Joon Min6, Chul-Woong Chung7, Hak-Sung Kim8.
Abstract
Targeted therapy based on protein-drug conjugates has attracted significant attention owing to its high efficacy and low side effects. However, efficient and stable drug conjugation to a protein binder remains a challenge. Herein, a chemoenzymatic method to generate highly stable and homogenous drug conjugates with high efficiency is presented. The approach comprises the insertion of the CaaX sequence at the C-terminal end of the protein binder, prenylation using farnesyltransferase, and drug conjugation through an oxime ligation reaction. MMAF and an EGFR-specific repebody are used as the antitumor agent and protein binder, respectively. The method enables the precisely controlled synthesis of repebody-drug conjugates with high yield and homogeneity. The utility of this approach is illustrated by the notable stability of the repebody-drug conjugates in human plasma, negligible off-target effects, and a remarkable antitumor activity in vivo. The present method can be widely used for generating highly homogeneous and stable PDCs for targeted therapy.Entities:
Keywords: cancer; drug delivery; oxime ligation; prenylation; protein-drug conjugates
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Year: 2015 PMID: 26315561 DOI: 10.1002/anie.201505964
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336