IF 5.8
3区 材料科学
Q1 CHEMISTRY, MULTIDISCIPLINARY
引用次数: 0
摘要
CRISPR-Cas9已成为一种高效且可定制的基因组编辑工具,在治疗肺癌KRAS突变方面大有可为。在这项研究中,我们介绍了一种名为 C14-PEI 的新型胶束复合物,它能有效地共同递送 Cas9 mRNA 和 sgRNA,从而切除肺癌细胞中突变的 KRAS 等位基因。C14-PEI 是由 1,2-epoxytetradecane 和支链 PEI 600 Da 通过开环反应合成的。C14-PEI 的临界胶束浓度(CMC)约为 20.86 ± 0.15 mg/L,表明它能够在低浓度下形成稳定的胶束。C14-PEI 通过静电作用将 mRNA 有效地包裹到胶束簇中。当质量比为 8(w/w 8)时,C14-PEI 配方表现出有利的特性,eGFP mRNA 的封装效率高达 99%,与未处理的细胞相比,eGFP 在 A549 细胞中的表达量增加了 130 倍,这表明胶束具有强大的递送和表达能力。重要的是,使用细胞内还原四唑盐进行的毒性测试显示,C14-PEI 没有明显的细胞毒性,这突出表明了 C14-PEI 的生物相容性。琼脂糖凝胶电泳也证实,C14-PEI 在共包被 Cas9 mRNA 和 sgRNA 方面也表现出很高的效率。当 sgRNA 与 Cas9 mRNA 的摩尔比为 10 时,经 T7 内切酶 I(T7EI)测定,胶束复合物成功地介导了对突变 KRAS 的切割,切割效率超过 60%。数字液滴聚合酶链式反应(ddPCR)进一步表明,以编辑的基因拷贝数衡量,基因编辑效率在 w/w 4 组为 48.5%,在 w/w 8 组为 37.8%。用含有靶向 KRAS G12S 突变的 Cas9 mRNA 和 sgRNA 的 C14-PEI 胶束团处理 A549 细胞,可显著削弱其迁移能力并提高细胞凋亡率。这些研究结果表明,C14-PEI 能有效破坏 KRAS 信号通路,从而减少肿瘤细胞的增殖并增强细胞的死亡。本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Novel Micelleplex for Tumour-Targeted Delivery of CRISPR-Cas9 against KRAS-Mutated Lung Cancer
CRISPR-Cas9 has emerged as a highly effective and customizable genome editing tool, holding significant promise for the treatment of KRAS mutations in lung cancer. In this study, we introduce a novel micelleplex, named C14-PEI, designed to co-deliver Cas9 mRNA and sgRNA efficiently to excise the mutated KRAS allele in lung cancer cells. C14-PEI is synthesised from 1,2-epoxytetradecane and branched PEI 600 Da via a ring-opening reaction. The resulting C14-PEI has a critical micelle concentration (CMC) of approximately 20.86 ± 0.15 mg/L, indicating its ability to form stable micelles at low concentrations. C14-PEI efficiently encapsulates mRNA into micelleplexes through electrostatic interactions. When the mass ratio is 8 (w/w 8), the C14-PEI formulation exhibits conducive properties, which showed encapsulation efficiency of eGFP mRNA at 99% and led to a 130-fold increase in eGFP expression in A549 cells compared to untreated cells, demonstrating the robust delivery and expression capability of the micelleplexes. Importantly, toxicity tests using intracellular reduction of a tetrazolium salt revealed no significant cytotoxicity, underscoring the biocompatibility of C14-PEI. C14-PEI also shows high efficiency in co-encapsulating Cas9 mRNA and sgRNA, as confirmed by agarose gel electrophoresis. At an sgRNA to Cas9 mRNA molar ratio of 10, the micelleplexes successfully mediate the cutting of mutated KRAS with an indel efficiency exceeding 60%, as determined by the T7 Endonuclease I (T7EI) assay. Digital droplet PCR (ddPCR) further demonstrates that the gene editing efficiency, measured by edited gene copies, is 48.5% in the w/w 4 group and 37.8% in the w/w 8 group. Treatment with C14-PEI micelleplexes containing Cas9 mRNA and sgRNA targeting the KRAS G12S mutation significantly impairs the migration capability of A549 cells and increases apoptosis rates. These findings suggest that C14-PEI effectively disrupts KRAS signalling pathways, leading to reduced tumor cell proliferation and enhanced cell death.
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来源期刊
Nanoscale
CHEMISTRY, MULTIDISCIPLINARY-NANOSCIENCE & NANOTECHNOLOGY
CiteScore
12.10
自引率
3.00%
发文量
1628
审稿时长
1.6 months
期刊介绍:
Nanoscale is a high-impact international journal, publishing high-quality research across nanoscience and nanotechnology. Nanoscale publishes a full mix of research articles on experimental and theoretical work, including reviews, communications, and full papers.Highly interdisciplinary, this journal appeals to scientists, researchers and professionals interested in nanoscience and nanotechnology, quantum materials and quantum technology, including the areas of physics, chemistry, biology, medicine, materials, energy/environment, information technology, detection science, healthcare and drug discovery, and electronics.
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