Macrophage Reprogramming with Anti‐miR223‐Loaded Artificial Protocells Enhances In Vivo Cancer Therapeutic Potential

Paco López‐Cuevas; Can Xu; Charlotte E. Severn; Tiah C. L. Oates; Stephen J. Cross; Ashley M. Toye; Stephen Mann; Paul Martin

doi:10.1002/advs.202202717

Advanced Science (Dec 2022)

Macrophage Reprogramming with Anti‐miR223‐Loaded Artificial Protocells Enhances In Vivo Cancer Therapeutic Potential

Paco López‐Cuevas,
Can Xu,
Charlotte E. Severn,
Tiah C. L. Oates,
Stephen J. Cross,
Ashley M. Toye,
Stephen Mann,
Paul Martin

Affiliations

Paco López‐Cuevas: School of Biochemistry Biomedical Sciences Building University Walk University of Bristol Bristol BS8 1TD UK
Can Xu: Centre for Protolife Research School of Chemistry University of Bristol Bristol BS8 1TS UK
Charlotte E. Severn: School of Biochemistry Biomedical Sciences Building University Walk University of Bristol Bristol BS8 1TD UK
Tiah C. L. Oates: School of Biochemistry Biomedical Sciences Building University Walk University of Bristol Bristol BS8 1TD UK
Stephen J. Cross: Wolfson Bioimaging Facility Biomedical Sciences Building University Walk University of Bristol Bristol BS8 1TD UK
Ashley M. Toye: School of Biochemistry Biomedical Sciences Building University Walk University of Bristol Bristol BS8 1TD UK
Stephen Mann: Centre for Protolife Research School of Chemistry University of Bristol Bristol BS8 1TS UK
Paul Martin: School of Biochemistry Biomedical Sciences Building University Walk University of Bristol Bristol BS8 1TD UK

DOI: https://doi.org/10.1002/advs.202202717
Journal volume & issue: Vol. 9, no. 35
pp. n/a – n/a

Abstract

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Abstract Several immune cell‐expressed miRNAs (miRs) are associated with altered prognostic outcome in cancer patients, suggesting that they may be potential targets for development of cancer therapies. Here, translucent zebrafish (Danio rerio) is utilized to demonstrate that genetic knockout or knockdown of one such miR, microRNA‐223 (miR223), globally or specifically in leukocytes, does indeed lead to reduced cancer progression. As a first step toward potential translation to a clinical therapy, a novel strategy is described for reprogramming neutrophils and macrophages utilizing miniature artificial protocells (PCs) to deliver anti‐miRs against the anti‐inflammatory miR223. Using genetic and live imaging approaches, it is shown that phagocytic uptake of anti‐miR223‐loaded PCs by leukocytes in zebrafish (and by human macrophages in vitro) effectively prolongs their pro‐inflammatory state by blocking the suppression of pro‐inflammatory cytokines, which, in turn, drives altered immune cell‐cancer cell interactions and ultimately leads to a reduced cancer burden by driving reduced proliferation and increased cell death of tumor cells. This PC cargo delivery strategy for reprogramming leukocytes toward beneficial phenotypes has implications also for treating other systemic or local immune‐mediated pathologies.

Published in Advanced Science

ISSN: 2198-3844 (Online)
Publisher: Wiley
Country of publisher: Germany
LCC subjects: Science
Website: https://onlinelibrary.wiley.com/journal/21983844

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