Tumour Suppression by Targeted Intravenous Non-viral CRISPRa Using Dendritic Polymers

Overview

Journal Chem Sci

Publisher Royal Society of Chemistry

Specialty Chemistry

Date 2019 Oct 8

PMID 31588320

Citations 26

Authors

Jessica A Kretzmann

Cameron W Evans

Colette Moses

Anabel Sorolla

Amy L Kretzmann

Edina Wang

Diwei Ho

Mark J Hackett

Benjamin F Dessauvagie

Nicole M Smith

Andrew D Redfern

Charlene Waryah

Marck Norret

K Swaminathan Iyer

Pilar Blancafort

Affiliations

Soon will be listed here.

Abstract

Aberrant gene expression is a hallmark of cancer. Although transcription is traditionally considered 'undruggable', the development of CRISPR-associated protein 9 (Cas9) systems offers enormous potential to rectify cancer-associated transcriptional abnormalities in malignant cells. However delivery of this technology presents a critical challenge to overcome in order to realize clinical translation for cancer therapy. In this article we demonstrate for the first time, a fully synthetic strategy to enable CRISPR-mediated activation (CRISPRa) of tumour suppressor genes using a targeted intravenous approach. We show this highly efficient transcriptional activation of two model tumour suppressor genes, Mammary Serine Protease Inhibitor (MASPIN, ) and cysteine-rich 61/connective tissue growth factor/nephroblastoma-overexpressed 6 (, ), in a mouse model of breast cancer. In particular, we demonstrate that targeted intravenous delivery of can be achieved using a novel nanoscale dendritic macromolecular delivery agent, with negligible toxicity and long lasting therapeutic effects, outlining a targeted effective formulation with potential to treat aggressive malignancies.

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