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Nanoparticle-mediated cytoplasmic delivery of proteins to target cellular machinery

机译:纳米粒子介导的蛋白向靶细胞机械的细胞质传递

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Despite recent advances in nanomaterial-based delivery systems, their applicability as carriers of cargo, especially proteins for targeting cellular components and manipulating cell function, is not wellunderstood. Herein, we demonstrate the ability of hydrophobic silica nanoparticles to deliver proteins, including enzymes and antibodies, to a diverse set of mammalian cells, including human cancer cells and rat stem cells, while preserving the activity of the biomolecule post-delivery. Specifically, we have explored the delivery and cytosolic activity of hydrophobically functionalized silica nanoparticle-protein conjugates in a human breast cancer cell line (MCF-7) and rat neural stem cells (NSCs) and elucidated the mechanism of cytosolic transport. Importantly, the proteins were delivered to the cytosol without extended entrapment in the endosomes, which facilitated the retention of biological activity of the delivered proteins. As a result, delivery of ribonuclease A (RNase A) and the antibody to phospho-Akt (pAkt) resulted in the initiation of cell death. Delivery of control protein conjugates (e.g., those containing green fluorescent protein or goat antirabbit IgG) resulted in minimal cell death, indicating that the carrier-mediated toxicity was low. The results presented here provide insight into the design of nanomaterials as protein carriers that enable control of cell function.
机译:尽管基于纳米材料的递送系统最近取得了进展,但人们对它们作为货物载体,特别是靶向细胞成分和操纵细胞功能的蛋白质的适用性还没有很好的理解。在本文中,我们证明了疏水性二氧化硅纳米颗粒能够将蛋白质(包括酶和抗体)传递到多种多样的哺乳动物细胞(包括人类癌细胞和大鼠干细胞)中,同时保留生物分子在传递后的活性。具体来说,我们已经探索了疏水化功能化二氧化硅纳米粒子-蛋白质偶联物在人乳腺癌细胞系(MCF-7)和大鼠神经干细胞(NSCs)中的递送和胞质活性,并阐明了胞质转运的机制。重要的是,蛋白被递送到胞质溶胶而没有延长的内体包埋,这促进了被递送蛋白的生物学活性的保留。结果,递送核糖核酸酶A(RNase A)和针对磷酸化Akt的抗体(pAkt)导致细胞死亡的开始。对照蛋白偶联物(例如,含有绿色荧光蛋白或山羊抗兔IgG的那些)的递送导致最小的细胞死亡,表明载体介导的毒性低。本文介绍的结果提供了对纳米材料设计的洞察力,这些材料可作为能够控制细胞功能的蛋白质载体。

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