RNA Control via Redox‐Responsive Acylation

Author:

Guo Junsong1,Chen Siqin1,Onishi Yoshiyuki2,Shi Qi1,Song Yangyang3,Mei Hui2,Chen Leilei3,Kool Eric T.2ORCID,Zhu Ru‐Yi1ORCID

Affiliation:

1. Department of Chemistry National University of Singapore 4 Science Drive 2 Singapore 117544 Singapore

2. Department of Chemistry Stanford University Stanford CA 94305 USA

3. Cancer Science Institute of Singapore National University of Singapore 14 Medical Dr Singapore 117599 Singapore

Abstract

AbstractIncorporating stimuli‐responsive components into RNA constructs provides precise spatiotemporal control over RNA structures and functions. Despite considerable advancements, the utilization of redox‐responsive stimuli for the activation of caged RNAs remains scarce. In this context, we present a novel strategy that leverages post‐synthetic acylation coupled with redox‐responsive chemistry to exert control over RNA. To achieve this, we design and synthesize a series of acylating reagents specifically tailored for introducing disulfide‐containing acyl adducts into the 2′‐OH groups of RNA (“cloaking”). Our data reveal that these acyl moieties can be readily appended, effectively blocking RNA catalytic activity and folding. We also demonstrate the traceless release and reactivation of caged RNAs (“uncloaking”) through reducing stimuli. By employing this strategy, RNA exhibits rapid cellular uptake, effective distribution and activation in the cytosol without lysosomal entrapment. We anticipate that our methodology will be accessible to laboratories engaged in RNA biology and holds promise as a versatile platform for RNA‐based applications.

Funder

National University of Singapore

National Institutes of Health

Publisher

Wiley

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