| Literature DB >> 30180286 |
Hans-Georg Lerchen1, Sven Wittrock2, Beatrix Stelte-Ludwig1, Anette Sommer2, Sandra Berndt2, Nils Griebenow3, Anne-Sophie Rebstock4, Sarah Johannes1, Yolanda Cancho-Grande1, Christoph Mahlert1, Simone Greven1, Carsten Terjung1.
Abstract
The number of cytotoxic payload classes successfully employed in antibody-drug conjugates (ADCs) is still rather limited. The identification of ADC payloads with a novel mode of action will increase therapeutic options and potentially increase the therapeutic window. Herein, we describe the utilization of kinesin spindle protein inhibitors (KSPi) as a novel payload class providing highly potent ADCs against different targets, for instance HER-2 or TWEAKR/Fn14. Aspects of technical optimization include the development of different linker attachment sites, the stabilization of ADC linkage to avoid payload deconjugation and finally, the tailor-made design of active metabolites with a long lasting intracellular exposure in the tumor matching the mode of action of KSP inhibition. These KSPi-ADCs are highly potent and selective in vitro and demonstrate in vivo efficacy in a broad panel of tumor models including complete regressions in a patient-derived urothelial cancer model.Entities:
Keywords: ADC; bioconjugate; cancer; cytotoxicity; drug discovery
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Year: 2018 PMID: 30180286 DOI: 10.1002/anie.201807619
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336