| Literature DB >> 33053221 |
Jing Gong1, Hong-Xia Wang1, Yeh-Hsing Lao1, Hanze Hu1, Naazanene Vatan1, Jonathan Guo1, Tzu-Chieh Ho1, Dantong Huang1, Mingqiang Li1,2, Dan Shao1,3, Kam W Leong1,4.
Abstract
Recent advances in CRISPR present attractive genome-editing toolsets for therapeutic strategies at the genetic level. Here, a liposome-coated mesoporous silica nanoparticle (lipoMSN) is reported as an effective CRISPR delivery system for multiplex gene-editing in the liver. The MSN provides efficient loading of Cas9 plasmid as well as Cas9 protein/guide RNA ribonucleoprotein complex (RNP), while liposome-coating offers improved serum stability and enhanced cell uptake. Hypothesizing that loss-of-function mutation in the lipid-metabolism-related genes pcsk9, apoc3, and angptl3 would improve cardiovascular health by lowering blood cholesterol and triglycerides, the lipoMSN is used to deliver a combination of RNPs targeting these genes. When targeting a single gene, the lipoMSN achieved a 54% gene-editing efficiency, besting the state-of-art Lipofectamine CRISPRMax. For multiplexing, lipoMSN maintained significant gene-editing at each gene target despite reduced dosage of target-specific RNP. By delivering combinations of targeting RNPs in the same nanoparticle, synergistic effects on lipid metabolism are observed in vitro and vivo. These effects, such as a 50% decrease in serum cholesterol after 4 weeks of post-treatment with lipoMSN carrying both pcsk9 and angptl3-targeted RNPs, could not be reached with a single gene-editing approach. Taken together, this lipoMSN represents a versatile platform for the development of efficient, combinatorial gene-editing therapeutics.Entities:
Keywords: CRISPR/Cas9; cardiovascular disease; gene therapy; multiplex gene editing; nanoparticles
Year: 2020 PMID: 33053221 PMCID: PMC8274731 DOI: 10.1002/adma.202003537
Source DB: PubMed Journal: Adv Mater ISSN: 0935-9648 Impact factor: 30.849