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  2. Membrane-destabilizing ionizable phospholipids for organ-selective mRNA delivery and CRISPR-Cas gene editing

Membrane-destabilizing ionizable phospholipids for organ-selective mRNA delivery and CRISPR-Cas gene editing

  • Nat Mater. 2021 May;20(5):701-710. doi: 10.1038/s41563-020-00886-0.
Shuai Liu # 1 Qiang Cheng # 1 Tuo Wei 1 Xueliang Yu 1 Lindsay T Johnson 1 Lukas Farbiak 1 Daniel J Siegwart 2
Affiliations

Affiliations

  • 1 The University of Texas Southwestern Medical Center, Department of Biochemistry, Simmons Comprehensive Cancer Center, Dallas, TX, USA.
  • 2 The University of Texas Southwestern Medical Center, Department of Biochemistry, Simmons Comprehensive Cancer Center, Dallas, TX, USA. Daniel.Siegwart@UTSouthwestern.edu.
  • # Contributed equally.
Abstract

Endosomal escape remains a fundamental barrier hindering the advancement of nucleic acid therapeutics. Taking inspiration from natural Phospholipids that comprise biological membranes, we report the combinatorial synthesis of multi-tailed ionizable Phospholipids (iPhos) capable of delivering messenger RNA or mRNA/single-guide RNA for gene editing in vivo. Optimized iPhos lipids are composed of one pH-switchable zwitterion and three hydrophobic tails, which adopt a cone shape in endosomal acidic environments to facilitate membrane hexagonal transformation and subsequent cargo release from endosomes. Structure-activity relationships reveal that iPhos chemical structure can control in vivo efficacy and organ selectivity. iPhos lipids synergistically function with various helper lipids to formulate multi-component lipid nanoparticles (called iPLNPs) for selective organ targeting. Zwitterionic, ionizable cationic and permanently cationic helper lipids enable tissue-selective mRNA delivery and CRISPR-Cas9 gene editing in spleen, liver and lungs (respectively) following intravenous administration. This rational design of functional Phospholipids demonstrates substantial value for gene editing research and therapeutic applications.

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