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Pooled endogenous protein tagging and recruitment for systematic profiling of protein function

Yevgeniy V. Serebrenik, Deepak Mani, Timothé Maujean, George M. Burslem, Ophir Shalem

2024Cell Genomics16 citationsDOIOpen Access PDF

Abstract

The emerging field of induced proximity therapeutics, which involves designing molecules to bring together an effector and target protein-typically to induce target degradation-is rapidly advancing. However, its progress is constrained by the lack of scalable and unbiased tools to explore effector-target protein interactions. We combine pooled endogenous gene tagging using a ligand-binding domain with generic small-molecule-based recruitment to screen for induction of protein proximity. We apply this methodology to identify effectors for degradation in two orthogonal screens: using fluorescence to monitor target levels and a cellular growth that depends on the degradation of an essential protein. Our screens revealed new effector proteins for degradation, including previously established examples, and converged on members of the C-terminal-to-LisH (CTLH) complex. We introduce a platform for pooled induction of endogenous protein-protein interactions to expand our toolset of effector proteins for protein degradation and other forms of induced proximity.

Topics & Concepts

EndogenyProfiling (computer programming)Protein functionComputational biologyBiologyComputer scienceBiochemistryGeneOperating systemProtein Degradation and InhibitorsUbiquitin and proteasome pathwaysAdvanced Proteomics Techniques and Applications
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