A chemical probe based on the PreQ1 metabolite enables transcriptome-wide mapping of binding sites

Balaratnam, Sumirtha; Rhodes, Curran A.; Bume, Desta Doro; Connelly, Colleen M.; Lai, Christopher C.; Kelley, James A.; Yazdani, Kamyar; Homan, Philip J.; Incarnato, Danny; Numata, T.; Schneekloth, John S.

doi:10.1038/s41467-021-25973-x

Cited by 26 publications

(23 citation statements)

References 74 publications

(92 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Cellular target validation methods for RNA have been recently developed based on covalent bond formation with 65 , 131 – 133 , or cleavage of, the target 65 . One covalent method, chemical cross-linking and isolation by pull-down (Chem-CLIP; Fig.…”

Section: Target Validation and Selectivity Of Rna-targeting Small Mol...mentioning

confidence: 99%

“…Quantitative PCR with reverse transcription (RT–qPCR) or RNA-seq and subsequent statistical analysis are used to analyse the enrichment of RNA targets in the pulled-down fraction, as compared with the starting lysate. Although the exact protocol may vary depending upon the chemistry of cross-linking 133 and purification modules, the fundamental idea of Chem-CLIP remains unchanged: transformation of dynamic reversible binding to covalent bonds by cross-linking and amplifying the signal by pull-down enrichment. Chem-CLIP experiments are completed side by side with a probe that lacks the RNA-binding module, controlling for nonspecific reaction of the cross-linking module.…”

Section: Target Validation and Selectivity Of Rna-targeting Small Mol...mentioning

confidence: 99%

“…Such data are key to inform lead optimization. Intriguingly, fragment mapping and Chem-CLIP 108 , 133 , 274 , in combination with RNA structure prediction programs such as ScanFold, can provide insight into ligandable cellular RNA structures; biologically silent interactions inform cellular RNAs amenable to targeting by small-molecule-induced degradation.…”

Section: The Future Of Small-molecule Targeting Of Rnamentioning

confidence: 99%

“…Cellular target validation methods for RNA have been recently developed based on covalent bond formation with 65,[131][132][133] , or cleavage of, the target 65 (for example, biotin or an alkyne) 65 . The RNA-binding module drives target engagement, bringing the cross-linking module into proximity to the RNA such that they react either directly (electrophilic in the case of chlorambucil) or upon irradiation (diazirine).…”

Section: Covalent Bond Formation To Measure Direct Target Engagementmentioning

confidence: 99%

See 3 more Smart Citations

Targeting RNA structures with small molecules

Childs‐Disney

Yang

Gibaut

et al. 2022

Nat Rev Drug Discov

251

219

View full text Add to dashboard Cite

RNA adopts 3D structures that confer varied functional roles in human biology and dysfunction in disease. Approaches to therapeutically target RNA structures with small molecules are being actively pursued, aided by key advances in the field including the development of computational tools that predict evolutionarily conserved RNA structures, as well as strategies that expand mode of action and facilitate interactions with cellular machinery. Existing RNA-targeted small molecules use a range of mechanisms including directing splicing — by acting as molecular glues with cellular proteins (such as branaplam and the FDA-approved risdiplam), inhibition of translation of undruggable proteins and deactivation of functional structures in noncoding RNAs. Here, we describe strategies to identify, validate and optimize small molecules that target the functional transcriptome, laying out a roadmap to advance these agents into the next decade.

show abstract

Section: Target Validation and Selectivity Of Rna-targeting Small Mol...mentioning

confidence: 99%

Section: Target Validation and Selectivity Of Rna-targeting Small Mol...mentioning

confidence: 99%

Section: The Future Of Small-molecule Targeting Of Rnamentioning

confidence: 99%

Section: Covalent Bond Formation To Measure Direct Target Engagementmentioning

confidence: 99%

See 2 more Smart Citations

Targeting RNA structures with small molecules

Childs‐Disney

Yang

Gibaut

et al. 2022

Nat Rev Drug Discov

251

219

View full text Add to dashboard Cite

show abstract

“…Little is known about the RNA off-target interactions of protein-targeted drugs in vivo, especially for clinically approved drugs. Investigation of small molecule-RNA interactions has been carried out recently via photocrosslinking (diazirine) 7,8 , alkylation (chlorambucil) 9,10 , in-line probing 11 , and SHAPE 12 , and these have emerged as useful tools to identify RNA-ligand interactions in vitro and recently in cultured cells 13 . Although elegant, application of these methods in vivo is potentially limited by transcriptional effects during prolonged probe treatment 14 , cellular damage by ultraviolet irradiation 15,16 , and nucleobase biases [17][18][19] .…”

mentioning

confidence: 99%

Pervasive Transcriptome Interactions of Protein-Targeted Drugs

Fang

Velema

Lee

et al. 2022

Preprint

View full text Add to dashboard Cite

The off-target toxicity of drugs targeted to proteins imparts substantial health and economic costs. Proteome interaction studies can reveal off-target effects with unintended proteins; however, little attention has been paid to intracellular RNAs as potential off targets that may contribute to toxicity. To begin to assess this, we developed a reactivity-based RNA profiling (RBRP) methodology, and applied it to uncover transcriptome interactions of a set of FDA-approved small-molecule drugs in vivo. We show that these protein-targeted drugs pervasively interact with the human transcriptome and can exert unintended biological effects on RNA function. In addition, we show that many off-target interactions occur at RNA loci associated with protein binding and structural changes, allowing us to generate hypotheses to infer the biological consequences of RNA off-target binding. The results suggest that rigorous characterization of drugs’ transcriptome interactions may help assess target specificity and avoid toxicity and clinical failures.

show abstract