Small-molecule targeted recruitment of a nuclease to cleave an oncogenic RNA in a mouse model of metastatic cancer

Author:

Costales Matthew G.,Aikawa Haruo,Li Yue,Childs-Disney Jessica L.,Abegg Daniel,Hoch Dominic G.,Pradeep Velagapudi Sai,Nakai Yoshio,Khan Tanya,Wang Kye Won,Yildirim Ilyas,Adibekian Alexander,Wang Eric T.,Disney Matthew D.ORCID

Abstract

As the area of small molecules interacting with RNA advances, general routes to provide bioactive compounds are needed as ligands can bind RNA avidly to sites that will not affect function. Small-molecule targeted RNA degradation will thus provide a general route to affect RNA biology. A non–oligonucleotide-containing compound was designed from sequence to target the precursor to oncogenic microRNA-21 (pre–miR-21) for enzymatic destruction with selectivity that can exceed that for protein-targeted medicines. The compound specifically binds the target and contains a heterocycle that recruits and activates a ribonuclease to pre–miR-21 to substoichiometrically effect its cleavage and subsequently impede metastasis of breast cancer to lung in a mouse model. Transcriptomic and proteomic analyses demonstrate that the compound is potent and selective, specifically modulating oncogenic pathways. Thus, small molecules can be designed from sequence to have all of the functional repertoire of oligonucleotides, including inducing enzymatic degradation, and to selectively and potently modulate RNA function in vivo.

Funder

HHS | National Institutes of Health

HHS | NIH | NIH Office of the Director

American Chemical Society

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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