Author:
Mikitiuk Michał,Barczyński Jan,Bielski Przemysław,Arciniega Marcelino,Błaszkiewicz Urszula,Hec Aleksandra,Lipińska Andrea D.,Rychłowski Michał,Holak Tad A.,Sitar Tomasz
Abstract
AbstractLysosome Targeting Chimeras (LYTACs) have recently been developed to facilitate lysosomal degradation of specific extracellular and transmembrane molecular targets. However, the LYTAC particles described to date are based on glycopeptide conjugates, which are difficult to prepare and produce on a large scale. Here we report the development of pure protein LYTACs based on the non-glycosylated IGF2 peptides, which can be readily produced in virtually any facility capable of monoclonal antibody production. These chimeras utilize the IGF2R/CI-M6PR pathway for lysosomal shuttling and, in our illustrative example, target programmed death ligand 1 (PD-L1), eliciting physiological effects analogous to immune checkpoint blockade. Results from in vitro assays significantly exceed the effects of anti-PD-L1 antibodies alone.
Publisher
Cold Spring Harbor Laboratory