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首页> 外文期刊>ACS nano >Nanomotor-Enabled pH-Responsive Intracellular Delivery of Caspase-3: Toward Rapid Cell Apoptosis
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Nanomotor-Enabled pH-Responsive Intracellular Delivery of Caspase-3: Toward Rapid Cell Apoptosis

机译:使纳米运动的pH-响应Caspase-3的细胞内递送:朝向快速细胞凋亡

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摘要

Direct and efficient intracellular delivery of enzymes to cytosol holds tremendous therapeutic potential while remaining an unmet technical challenge. Herein, an ultrasound (US)-propelled nanomotor approach and a high-pH-responsive delivery strategy are reported to overcome this challenge using caspase-3 (CASP-3) as a model enzyme. Consisting of a gold nanowire (AuNW) motor with a pH-responsive polymer coating, in which the CASP-3 is loaded, the resulting nanomotor protects the enzyme from release and deactivation prior to reaching an intracellular environment. However, upon entering a cell and exposure to the higher intracellular pH, the polymer coating is dissolved, thereby directly releasing the active CASP-3 enzyme to the cytosol and causing rapid cell apoptosis. In vitro studies using gastric cancer cells as a model cell line demonstrate that such a motion-based active delivery approach leads to remarkably high apoptosis efficiency within a significantly shorter time and with a lower amount of CASP-3 compared to other control groups not involving US-propelled nanomotors. For instance, the reported nanomotor system can achieve 80% apoptosis of human gastric adenocarcinoma cells within only 5 min, which dramatically outperforms other CASP-3 delivery approaches. These results indicate that the US-propelled nanomotors may act as a powerful vehicle for cytosolic delivery of active therapeutic proteins, which would offer an attractive means to enhance the current landscape of intracellular protein delivery and therapy. While CASP-3 is selected as a model protein in this study, the same nanomotor approach can be readily applied to a variety of different therapeutic proteins.
机译:直接和高效的细胞内递送酶至细胞溶质溶解巨大的治疗潜力,同时留下了未满足的技术挑战。在此,据报道,超声(US) - 营收的纳米培养物方法和高pH响应递送策略克服使用Caspase-3(Casp-3)作为模型酶的这种挑战。由具有pH-响应聚合物涂层的金纳米线(AUNW)电动机组成,其中加载CASP-3,得到的纳米电机在达到细胞内环境之前保护酶免受释放和失活。然而,在进入细胞并暴露于较高的细胞内pH时,将聚合物涂层溶解,从而直接将活性CASP-3酶释放到胞浆溶胶并引起快速细胞凋亡。使用胃癌细胞作为模型细胞的体外研究表明,这种基于运动的活性递送方法在明显较短的时间内具有显着高的细胞凋亡效率,并且与不涉及我们的其他对照组相比,较低的Casp-3。 - 纳米纳米热管。例如,报告的纳米电机系统只能在5分钟内实现人胃腺癌细胞的80%凋亡,这显着优于其他Casp-3递送方法。这些结果表明,美国推进的纳米热剂可以作为活性治疗蛋白的细胞源递送的强大载体,这将提供一种有吸引力的方法,以增强细胞内蛋白质递送和治疗的当前景观。虽然在该研究中选择CasP-3作为模型蛋白质,但可以容易地应用于同一纳米电机方法以各种不同的治疗蛋白质。

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