Reprogramming of Protein-Targeted Small-Molecule Medicines to RNA by Ribonuclease Recruitment.
Peiyuan ZhangXiaohui LiuDaniel AbeggToru TanakaYuquan TongRaphael I BenhamouJared T BaisdenGogce CrynenSamantha M MeyerMichael D CameronArnab K ChatterjeeAlexander AdibekianJessica L Childs-DisneyMatthew D DisneyPublished in: Journal of the American Chemical Society (2021)
Reprogramming known medicines for a novel target with activity and selectivity over the canonical target is challenging. By studying the binding interactions between RNA folds and known small-molecule medicines and mining the resultant dataset across human RNAs, we identified that Dovitinib, a receptor tyrosine kinase (RTK) inhibitor, binds the precursor to microRNA-21 (pre-miR-21). Dovitinib was rationally reprogrammed for pre-miR-21 by using it as an RNA recognition element in a chimeric compound that also recruits RNase L to induce the RNA's catalytic degradation. By enhancing the inherent RNA-targeting activity and decreasing potency against canonical RTK protein targets in cells, the chimera shifted selectivity for pre-miR-21 by 2500-fold, alleviating disease progression in mouse models of triple-negative breast cancer and Alport Syndrome, both caused by miR-21 overexpression. Thus, targeted degradation can dramatically improve selectivity even across different biomolecules, i.e., protein versus RNA.
Keyphrases
- small molecule
- cell proliferation
- long non coding rna
- tyrosine kinase
- protein protein
- long noncoding rna
- nucleic acid
- cancer therapy
- endothelial cells
- binding protein
- stem cells
- epidermal growth factor receptor
- mouse model
- cell therapy
- signaling pathway
- case report
- drug delivery
- cell death
- bone marrow
- cell cycle arrest
- dna binding