Litcius/Paper detail

A first-in-class fully modified version of miR-34a with outstanding stability, activity, and anti-tumor efficacy

Ahmed Mansour, Ikjot Singh Sohal, Shreyas G. Iyer, Kasireddy Sudarshan, Harish Kothandaraman, Nadia A. Lanman, Philip S. Low, Andrea L. Kasinski

2023Oncogene64 citationsDOIOpen Access PDF

Abstract

Altered by defects in p53, epigenetic silencing, and genomic loss, the microRNA miR-34a represents one of the most clinically relevant tumor-suppressive microRNAs. Without question, a striking number of patients with cancer would benefit from miR-34a replacement, if poor miR-34a stability, non-specific delivery, and delivery-associated toxicity could be overcome. Here, we highlight a fully modified version of miR-34a (FM-miR-34a) that overcomes these hurdles when conjugated to a synthetically simplistic ligand. FM-miR-34a is orders of magnitude more stable than a partially modified version, without compromising its activity, leading to stronger repression of a greater number of miR-34a targets. FM-miR-34a potently inhibited proliferation and invasion, and induced sustained downregulation of endogenous target genes for >120 h following in vivo delivery. In vivo targeting was achieved through conjugating FM-miR-34a to folate (FM-FolamiR-34a), which inhibited tumor growth leading to complete cures in some mice. These results have the ability to revitalize miR-34a as an anti-cancer agent, providing a strong rationale for clinical testing.

Topics & Concepts

microRNAIn vivoBiologyGene silencingDownregulation and upregulationCancer researchPsychological repressionEpigeneticsCancerBioinformaticsGeneGene expressionBiochemistryGeneticsMicroRNA in disease regulationRNA Interference and Gene DeliveryCircular RNAs in diseases