The PROTACtable genome.
Melanie SchneiderChris J RadouxAndrew HerculesDavid OchoaIan DunhamLykourgos-Panagiotis ZalmasGerhard HesslerSven RufVeerabahu ShanmugasundaramMichael M HannPam J ThomasMarkus A QueisserAndrew B BenowitzKris BrownAndrew R LeachPublished in: Nature reviews. Drug discovery (2021)
Proteolysis-targeting chimeras (PROTACs) are an emerging drug modality that may offer new opportunities to circumvent some of the limitations associated with traditional small-molecule therapeutics. By analogy with the concept of the 'druggable genome', the question arises as to which potential drug targets might PROTAC-mediated protein degradation be most applicable. Here, we present a systematic approach to the assessment of the PROTAC tractability (PROTACtability) of protein targets using a series of criteria based on data and information from a diverse range of relevant publicly available resources. Our approach could support decision-making on whether or not a particular target may be amenable to modulation using a PROTAC. Using our approach, we identified 1,067 proteins of the human proteome that have not yet been described in the literature as PROTAC targets that offer potential opportunities for future PROTAC-based efforts.
Keyphrases
- small molecule
- protein protein
- decision making
- endothelial cells
- systematic review
- genome wide
- amino acid
- electronic health record
- binding protein
- human health
- big data
- healthcare
- cancer therapy
- induced pluripotent stem cells
- quality improvement
- drug induced
- drug delivery
- health information
- machine learning
- data analysis
- artificial intelligence