The AUTOTAC chemical biology platform for targeted protein degradation via the autophagy-lysosome system.
Chang Hoon JiHee Yeon KimMin Ju LeeAh Jung HeoDaniel Youngjae ParkSungsu LimSeulgi ShinSrinivasrao GanipisettiWoo Seung YangChang An JungKun Young KimEun Hye JeongSun Ho ParkSu Bin KimSu Jin LeeJeong Eun NaJi In KangHyung Min ChiHyun Tae KimYun Kyung KimBo Yeon KimYong Tae KwonPublished in: Nature communications (2022)
Targeted protein degradation allows targeting undruggable proteins for therapeutic applications as well as eliminating proteins of interest for research purposes. While several degraders that harness the proteasome or the lysosome have been developed, a technology that simultaneously degrades targets and accelerates cellular autophagic flux is still missing. In this study, we develop a general chemical tool and platform technology termed AUTOphagy-TArgeting Chimera (AUTOTAC), which employs bifunctional molecules composed of target-binding ligands linked to autophagy-targeting ligands. AUTOTACs bind the ZZ domain of the otherwise dormant autophagy receptor p62/Sequestosome-1/SQSTM1, which is activated into oligomeric bodies in complex with targets for their sequestration and degradation. We use AUTOTACs to degrade various oncoproteins and degradation-resistant aggregates in neurodegeneration at nanomolar DC 50 values in vitro and in vivo. AUTOTAC provides a platform for selective proteolysis in basic research and drug development.