Targeting a proteolytic neo-epitope of CUB-domain containing protein 1 in RAS-driven cancer

Author:

Lim Shion A.,Zhou JieORCID,Martinko Alexander J.,Wang Yung-Hua,Filippova Ekaterina V.,Steri Veronica,Wang Donghui,Remesh Soumya G.,Liu Jia,Hann Byron,Kossiakoff Anthony A.,Evans Michael J.ORCID,Leung Kevin K.ORCID,Wells James A.

Abstract

AbstractA central challenge for any therapeutic is targeting diseased over normal cells. Proteolysis is frequently upregulated in disease and can generate proteoforms with unique neo-epitopes. We hypothesize that targeting proteolytic neo-epitopes can enable more effective and safer treatments, reflecting a conditional layer of disease-specific regulation. Here, we characterized the precise proteolytic isoforms of CUB domain containing protein 1 (CDCP1), a protein overexpressed and specifically cleaved in RAS-driven cancers. We validated that the N-terminal and C-terminal fragments of CDCP1 remain associated after proteolysis in vitro and on the surface of pancreatic cancer cells. Using a differential phage display strategy, we generated exquisitely selective recombinant antibodies that target cells harboring cleaved CDCP1 and not the full-length form using antibody-drug conjugates or a bi-specific T-cell engagers. We show tumor-specific localization and anti-tumor activity in a syngeneic pancreatic tumor model having superior safety profiles compared to a pan-CDCP1-targeting antibody. Our studies show proteolytic neo-epitopes can provide an orthogonal “AND” gate for disease-specific targeting.One-Sentence SummaryAntibody-based targeting of neo-epitopes generated by disease-associated proteolysis improves the therapeutic index

Publisher

Cold Spring Harbor Laboratory

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