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Ultrafast Structural Dynamics of the Photocleavage of Protein Hybrid Nanoparticles

机译:蛋白质杂化纳米粒子光解的超快结构动力学。

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摘要

Protein-coated gold nanoparticles in suspension are excited by intense laser pulses to mimic the light-induced effect on biomolecules that occur In photothermal laser therapy with nanoparticles as photosensitizer. Ultrafast X-ray scattering employed to access the nanoscale structural modifications of the protein-nanoparticle hybrid reveals that the protein shell Is expelled as a whole without denaturation at a laser fluence that coincides with the bubble formation threshold. In this ultrafast heating mediated by the nanoparticles, time-resolved scattering data show that proteins are not denatured in terms of secondary structure even at much higher temperatures than the static thermal denaturation temperature, probably because time Is too short for the proteins to unfold and the temperature stimulus has vanished before this motion sets in. Consequently the laser pulse length has a strong influence on whether the end result is the ligand detachment (for example drug delivery) or biomaterial degradation.
机译:悬浮液中被蛋白质包裹的金纳米颗粒被强激光脉冲激发,以模仿光诱导的对生物分子的作用,这种作用发生在使用纳米颗粒作为光敏剂的光热激光治疗中。用于访问蛋白质-纳米粒子杂物的纳米级结构修饰的超快X射线散射揭示,蛋白质外壳作为一个整体被排出,而激光通量与气泡形成阈值一致则不变性。在这种由纳米颗粒介导的超快加热中,时间分辨散射数据表明,即使在比静态热变性温度高得多的温度下,蛋白质也不会在二级结构上变性,这可能是因为时间太短了,无法展开并且在这种运动开始之前,温度刺激就消失了。因此,激光脉冲的长度对最终结果是配体脱离(例如药物输送)还是生物材料降解有很大影响。

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