| Literature DB >> 29227683 |
BinQing Wei1, Janet Gunzner-Toste1, Hui Yao2, Tao Wang2, Jing Wang2, Zijin Xu2, Jinhua Chen2, John Wai2, Jim Nonomiya1, Siao Ping Tsai1, Josefa Chuh1, Katherine R Kozak1, Yichin Liu1, Shang-Fan Yu1, Jeff Lau1, Guangmin Li1, Gail D Phillips1, Doug Leipold1, Amrita Kamath1, Dian Su1, Keyang Xu1, Charles Eigenbrot1, Stefan Steinbacher3, Rachana Ohri1, Helga Raab1, Leanna R Staben1, Guiling Zhao1, John A Flygare1, Thomas H Pillow1, Vishal Verma1, Luke A Masterson4, Philip W Howard4, Brian Safina1.
Abstract
Antibody-drug conjugates (ADCs) have become an important therapeutic modality for oncology, with three approved by the FDA and over 60 others in clinical trials. Despite the progress, improvements in ADC therapeutic index are desired. Peptide-based ADC linkers that are cleaved by lysosomal proteases have shown sufficient stability in serum and effective payload-release in targeted cells. If the linker can be preferentially hydrolyzed by tumor-specific proteases, safety margin may improve. However, the use of peptide-based linkers limits our ability to modulate protease specificity. Here we report the structure-guided discovery of novel, nonpeptidic ADC linkers. We show that a cyclobutane-1,1-dicarboxamide-containing linker is hydrolyzed predominantly by cathepsin B while the valine-citrulline dipeptide linker is not. ADCs bearing the nonpeptidic linker are as efficacious and stable in vivo as those with the dipeptide linker. Our results strongly support the application of the peptidomimetic linker and present new opportunities for improving the selectivity of ADCs.Entities:
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Year: 2017 PMID: 29227683 DOI: 10.1021/acs.jmedchem.7b01430
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446