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

机译:用于器官选择性mRNA递送和CRISPR-CAS基因编辑的膜稳定的可电离磷脂

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摘要

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.
机译:内体逃脱仍然是妨碍核酸治疗剂的进步的基本障碍。从包含生物膜的天然磷脂中获取灵感,我们报告了能够在体内递送信使RNA或mRNA /单引导RNA的多尾可电离磷脂(Iphos)的组合合成。优化的Iphos脂质由一种pH可切换的两性周和三个疏水性尾部组成,其在内体酸性环境中采用锥形形状,以促进膜六方转化和随后从底皮中释放的货物释放。结构 - 活性关系表明,Iphos化学结构可以控制体内疗效和器官选择性。 Iphos脂质与各种辅助脂质协同作用,以配制用于选择性器官靶向的多组分脂质纳米颗粒(称为IPLNP)。两性离子,可电离的阳离子和永久阳离子辅助脂质使组织选择性mRNA递送和CRISPR-CAS9基因在静脉内给药后(分别)在脾脏,肝脏和肺部(分别)后进行编辑。这种功能性磷脂的理性设计证明了基因编辑研究和治疗应用的大量价值。

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  • 来源
    《Nature Materials》 |2021年第5期|701-710|共10页
  • 作者单位

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

    The University of Texas Southwestern Medical Center Department of Biochemistry Simmons Comprehensive Cancer Center Dallas TX USA;

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