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Multifunctional nanocarrier based on clay nanotubes for efficient intracellular siRNA delivery and gene silencing.

机译:基于粘土纳米管的多功能纳米载波高效细胞内siRNA递送和基因沉默。

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RNA interference-mediated gene silencing relating to disease has recently emerged as a powerful method in gene therapy. Despite the promises, effective transport of siRNA with minimal side effects remains a challenge. Halloysites are cheap and naturally available aluminosilicate clay nanotubes with high mechanical strength and biocompatibility. In this study, a novel multifunctional nanocarrier based on functionalized halloysite nanotubes (f-HNTs) has been developed via electrostatic layer-by-layer assembling approach for loading and intracellular delivery of therapeutic antisurvivin siRNA and simultaneously tracking their intracellular transport, in which PEI-modified HNTs are used as gene vector, antisurvivin siRNA as gene therapeutic agent, and mercaptoacetic acid-capped CdSe quantum dots as fluorescent labeling probes. The successful assembly of the f-HNTs-siRNA complexes was systematically characterized by transmission electron microscopy (TEM), UV-visible spectrophotometry, Zeta potential measurement, fluorescence spectrophotometry, and electrochemical impedance spectroscopy. Confocal microscopy, biological TEM, and flow cytometry studies revealed that the complexes enabled the efficient intracellular delivery of siRNA for cell-specific gene silencing. MTT assays exhibited that the complexes can enhance antitumor activity. Furthermore, Western blot analysis showed that f-HNTs-mediated siRNA delivery effectively knocked down gene expression of survivin and thereby decreased the levels of target proteins of PANC-1 cells. Therefore, this study suggested that the synthesized f-HNTs were a new effective drug delivery system for potential application in cancer gene therapy.
机译:RNA干扰介导的疾病与疾病有关的基因沉默在基因疗法中成为一种强大的方法。尽管有承诺,但副副作用的有效运输仍然是一个挑战。 HolloySites具有便宜的,天然可用的铝硅酸盐粘土纳米管,具有高机械强度和生物相容性。在该研究中,通过静电层逐层组装方法开发了一种基于官能化的霍氏铁矿石纳米管(F-HNT)的新型多功能纳米载波,用于加载和细胞内递送治疗性抗肌肉素siRNA,同时跟踪其细胞内运输,其中PEI-改性HNT用作基因载体,抗肌病素SiRNA作为基因治疗剂,以及氟乙酸封端的CDSE量子点作为荧光标记探针。通过透射电子显微镜(TEM),UV可见分光光度法,Zeta电位测量,荧光分光光度法和电化学阻抗光谱学和电化学阻抗光谱和电化学阻抗光谱和电化学阻抗光谱和电化学阻抗光谱学的成功组装。共聚焦显微镜,生物学TEM和流式细胞术研究表明,复合物使得SiRNA的高效细胞内递送用于细胞特异性基因沉默。 MTT测定表明,复合物可以增强抗肿瘤活性。此外,Western印迹分析表明,F-HNT介导的siRNA递送有效地击落了Survivin的基因表达,从而降低了Panc-1细胞的靶蛋白水平。因此,该研究表明,合成的F-HNT是一种新的有效药物递送系统,用于癌症基因治疗中的潜在应用。

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