Covalent Ligand Screening Uncovers a RNF4 E3 Ligase Recruiter for Targeted Protein Degradation Applications

Ward, Carl C.; Kleinman, Jordan I.; Brittain, Scott M.; Lee, Patrick S.; Chung, Clive Yik‐Sham; Kim, Kenneth; Petri, Yana; Thomas, Jason R.; Tallarico, John A.; McKenna, Jeffrey M.; Schirle, Markus; Nomura, Daniel K.

doi:10.1021/acschembio.8b01083

Cited by 252 publications

(200 citation statements)

References 49 publications

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“…These molecules are generally larger and more flexible than typical drug-like compounds, which can translate into poor membrane permeability and liability to efflux pumps 39,42,43 . While covalent binding to E3 ligases is acceptable 31,44 , PROTACs binding covalently to the protein target probably lose the substoichiometric nature of their mechanism 45 . Finally, what percentage of a target protein should be degraded to trigger a phenotypic response probably depends on the target and the readout, but needs to be systematically investigated.…”

Section: Progress and Lessons Learnedmentioning

confidence: 99%

Targeted protein degradation: expanding the toolbox

Schapira

Calabrese

Bullock

et al. 2019

Nat Rev Drug Discov

657

539

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Proteolysis-targeting chimeras (PROTACs) and related molecules that induce targeted protein degradation by the ubiquitin-proteasome system represent a new therapeutic modality and are the focus of great interest, owing to potential advantages over traditional occupancy-based inhibitors with respect to dosing, side effects, drug resistance and modulating 'undruggable' targets. However, the technology is still maturing, and the design elements for successful PROTAC-based drugs are currently being elucidated. Importantly, fewer than 10 of the more than 600 E3 ubiquitin ligases have so far been exploited for targeted protein degradation, and expansion of knowledge in this area is a key opportunity. Here, we briefly discuss lessons learned about targeted protein degradation in chemical biology and drug discovery and systematically review the expression profile, domain architecture and chemical tractability of human E3 ligases that could expand the toolbox for PROTAC discovery. Recent crystal structures of ternary complexes have advanced the understanding of the structural mechanism of PROTACs. Structural studies on VHL and CRBN show that these Cullin-RING E3 ligases (CRLs) form large, modular, U-shaped complexes in which adaptor proteins mediate the interaction between the substrate-binding element (VHL or CRBN) and Cullin scaffolds that bind the RING-domain protein RBX1, leading to the recruitment of a ubiquitinconjugated E2 (refs 9,46,47,48,49,50,51,52) (Fig. 2a,b). The U shape leads to proximal positioning of the E2 and substrate proteins, allowing targeted ubiquitin transfer. The architecture of these large complexes is expected to provide an extended ubiquitylation radius that can accommodate multiple ubiquitylation sites on substrates with diverse sizes and shapes 47,52. In particular, given

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Section: Progress and Lessons Learnedmentioning

confidence: 99%

Targeted protein degradation: expanding the toolbox

Schapira

Calabrese

Bullock

et al. 2019

Nat Rev Drug Discov

657

539

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“…In previous works investigating the direct targets of parthenolide, multiple studies have revealed unique ligandable and functional cysteines within their respective proteins that could be targeted to influence cellular signaling and pathogenicity. Recent studies have shown that activity-based protein profiling (ABPP)-based chemoproteomic platforms can be utilized to uncover unique and functional druggable hotspots and modalities that can be accessed by covalently-acting small-molecules and natural products that may not be obvious using standard drug discovery paradigms (Backus et al, 2016;Bateman et al, 2017;Grossman et al, 2017;Hacker et al, 2017;Spradlin et al, 2018;Ward et al, 2018).…”

Section: Main Textmentioning

confidence: 99%

Parthenolide Covalently Targets and Inhibits Focal Adhesion Kinase in Breast Cancer Cells

Berdan¹,

Ho²,

Lehtola³

et al. 2019

Preprint

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Parthenolide, a natural product from the feverfew plant and member of the large family of sesquiterpene lactones, exerts multiple biological and therapeutic activities including anti-inflammatory and anti-cancer effects. Herein, we further study parthenolide mechanism of action using activity-based protein profiling (ABPP)-based chemoproteomic platforms to map additional covalent targets engaged by parthenolide in human breast cancer cells. We find that parthenolide, as well as other related exocyclic methylene lactonecontaining sesquiterpenes, covalently modify cysteine 427 (C427) of focal adhesion kinase 1 (FAK1) leading to impairment of FAK1-dependent signaling pathways and breast cancer cell proliferation, survival, and motility.These studies reveal a novel functional target exploited by members of a large family of anticancer natural products.

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“…TRH 1-23 (2, Table 2) is a promising RNF4 inhibitor that was recently identified in an activity-based protein profiling (ABPP) screen. An analog of TRH 1-23, named CCW-16 3, was found to be a more a potent RNF4 inhibitor, exhibiting an IC 50 of 1.8 μM [63]. Von Hippel-Lindau (VHL) E3 Ubiquitin Ligase is one of the few E3 ligases, including cereblon, VHL, MDM2, and cIAP, that have been successfully exploited in targeted protein degradation strategies [71,72].…”

Section: Ring-type E3 Ligase Inhibitorsmentioning

confidence: 99%

Small molecules that target the ubiquitin system

Baker

Ovaa

2020

Biochemical Society Transactions

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Eukaryotic life depends upon the interplay between vast networks of signaling pathways composed of upwards of 109–1010 proteins per cell. The integrity and normal operation of the cell requires that these proteins act in a precise spatial and temporal manner. The ubiquitin system is absolutely central to this process and perturbation of its function contributes directly to the onset and progression of a wide variety of diseases, including cancer, metabolic syndromes, neurodegenerative diseases, autoimmunity, inflammatory disorders, infectious diseases, and muscle dystrophies. Whilst the individual components and the overall architecture of the ubiquitin system have been delineated in some detail, how ubiquitination might be successfully targeted, or harnessed, to develop novel therapeutic approaches to the treatment of disease, currently remains relatively poorly understood. In this review, we will provide an overview of the current status of selected small molecule ubiquitin system inhibitors. We will further discuss the unique challenges of targeting this ubiquitous and highly complex machinery, and explore and highlight potential ways in which these challenges might be met.

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Covalent Ligand Screening Uncovers a RNF4 E3 Ligase Recruiter for Targeted Protein Degradation Applications

Cited by 252 publications

References 49 publications

Targeted protein degradation: expanding the toolbox

Targeted protein degradation: expanding the toolbox

Parthenolide Covalently Targets and Inhibits Focal Adhesion Kinase in Breast Cancer Cells

Small molecules that target the ubiquitin system

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