Reprogramming Tumor-associated Dendritic Cells in Vivo Using MiRNA Mimetics Triggers Protective Immunity Against Ovarian Cancer

Overview

Journal Cancer Res

Specialty Oncology

Date 2012 Feb 7

PMID 22307839

Citations 94

Authors

Juan R Cubillos-Ruiz

Jason R Baird

Amelia J Tesone

Melanie R Rutkowski

Uciane K Scarlett

Ana L Camposeco-Jacobs

Jorge Anadon-Arnillas

Noah M Harwood

Murray Korc

Steven N Fiering

Lorenzo F Sempere

Jose R Conejo-Garcia

Affiliations

Soon will be listed here.

Abstract

Modulating the activity of miRNAs provides opportunities for novel cancer interventions. However, low bioavailability and poor cellular uptake are major challenges for delivering miRNA mimetics specifically to tumor cells. Here, we took advantage of the spontaneous enhanced endocytic activity of ovarian cancer-associated dendritic cells (DC) to selectively supplement the immunostimulatory miRNA miR-155. In vivo processing of nanoparticles carrying oligonucleotide duplexes mimicking the bulged structure of endogenous pre-miRNA (but not siRNA-like oligonucleotides) dramatically augmented miR-155 activity without saturating the RNA-induced silencing complex. Endogenous processing of synthetic miR-155 favored Ago2 and, to a lesser extent, Ago4 loading, resulting in genome-wide transcriptional changes that included silencing of multiple immunosuppressive mediators. Correspondingly, tumor-infiltrating DCs were transformed from immunosuppressive to highly immunostimulatory cells capable of triggering potent antitumor responses that abrogated the progression of established ovarian cancers. Our results show both the feasibility and therapeutic potential of supplementing/replenishing miRNAs in vivo using nonviral approaches to boost protective immunity against lethal tumors. Thus, we provide a platform, an optimized design, and a mechanistic rationale for the clinical testing of nonviral miRNA mimetics.

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