| Literature DB >> 25643134 |
Magdalena Dorywalska1, Pavel Strop1, Jody A Melton-Witt1, Adela Hasa-Moreno1, Santiago E Farias1, Meritxell Galindo Casas1, Kathy Delaria1, Victor Lui1, Kris Poulsen1, Carole Loo1, Stellanie Krimm1, Gary Bolton1, Ludivine Moine2, Russell Dushin2, Thomas-Toan Tran1, Shu-Hui Liu1, Mathias Rickert1, Davide Foletti1, David L Shelton1, Jaume Pons1, Arvind Rajpal1.
Abstract
The systemic stability of the antibody-drug linker is crucial for delivery of an intact antibody-drug conjugate (ADC) to target-expressing tumors. Linkers stable in circulation but readily processed in the target cell are necessary for both safety and potency of the delivered conjugate. Here, we report a range of stabilities for an auristatin-based payload site-specifically attached through a cleavable valine-citrulline-p-aminobenzylcarbamate (VC-PABC) linker across various sites on an antibody. We demonstrate that the conjugation site plays an important role in determining VC-PABC linker stability in mouse plasma, and that the stability of the linker positively correlates with ADC cytotoxic potency both in vitro and in vivo. Furthermore, we show that the VC-PABC cleavage in mouse plasma is not mediated by Cathepsin B, the protease thought to be primarily responsible for linker processing in the lysosomal degradation pathway. Although the VC-PABC cleavage is not detected in primate plasma in vitro, linker stabilization in the mouse is an essential prerequisite for designing successful efficacy and safety studies in rodents during preclinical stages of ADC programs. The divergence of linker metabolism in mouse plasma and its intracellular cleavage offers an opportunity for linker optimization in the circulation without compromising its efficient payload release in the target cell.Entities:
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Year: 2015 PMID: 25643134 DOI: 10.1021/bc5005747
Source DB: PubMed Journal: Bioconjug Chem ISSN: 1043-1802 Impact factor: 4.774