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Using FRET to measure the time it takes for a cell to destroy a virus

机译:用焦虑来测量细胞的时间摧毁一个病毒

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摘要

The emergence of viral nanotechnology over the preceding two decades has created a number of intellectually captivating possible translational applications; however, thein vitrofate of the viral nanoparticles in cells remains an open question. Herein, we investigate the stability and lifetime of virus-like particle (VLP) Q beta-a representative and popular VLP for several applications-following cellular uptake. By exploiting the available functional handles on the viral surface, we have orthogonally installed the known FRET pair, FITC and Rhodamine B, to gain insight of the particle's behaviorin vitro. Based on these data, we believe VLPs undergo aggregation in addition to the anticipated proteolysis within a few hours of cellular uptake.
机译:病毒纳米技术的出现前二十年创造了许多智力上迷人的可能的转化应用程序;病毒纳米颗粒在细胞仍然是开放的的问题。和病毒样颗粒的一生(车牌区域)βa代表数和流行的车牌区域随后细胞吸收。利用可用的功能处理病毒表面,垂直安装已知的烦恼,FITC和若丹明B粒子的behaviorin体外的了解。基于这些数据,我们相信一种经历聚合除了预期几个小时的细胞内蛋白水解作用吸收。

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