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首页> 外文期刊>Nano letters >Thermostable luciferase from Luciola cruciate for imaging of carbon nanotubes and carbon nanotubes carrying doxorubicin using in vivo imaging system
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Thermostable luciferase from Luciola cruciate for imaging of carbon nanotubes and carbon nanotubes carrying doxorubicin using in vivo imaging system

机译:来自Luciola crucanate的热稳定荧光素酶,用于使用体内成像系统对碳纳米管和携带阿霉素的碳纳米管成像

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摘要

In the present study, we introduce a novel method for in vivo imaging of the biodistribution of single wall carbon nanotubes (SWNTs) labeled with recombinant thermo-stable Luciola cruciata luciferase (LcL). In addition, we highlight a new application for green fluorescent proteins in which they are utilized as imaging moieties for SWNTs. Carbon nanotubes show great positive potential compared to other drug nanocarriers with respect to loading capacity, cell internalization, and biodegradability. We have also studied the effect of binding mode (chemical conjugation and physical adsorption) on the chemiluminescence activity, decay rate, and half-life. We have shown that through proper chemical conjugation of LcL to CNTs, LcL remained biologically active for the catalysis of d-luciferin in the presence of ATP to release detectable amounts of photons for in vivo imaging. Chemiluminescence of LcL allows imaging of CNTs and their cargo in nonsuperficial locations at an organ resolution with no need of an excitation source. Loading LcL-CNTs with the antitumor antibiotic doxorubicin did not alter their biological activity for imaging. In vivo imaging of LcL-CNTs has been carried out using "IVIS spectrum" showing the uptake of LcL-CNTs by different organs in mice. We believe that the LcL-CNT system is an advanced powerful tool for in vivo imaging and therefore a step toward the advancement of the nanomedicine field.
机译:在本研究中,我们介绍了一种新型的体内重组单稳态碳纳米管荧光素酶(LcL)标记的单壁碳纳米管(SWNTs)生物分布成像的方法。此外,我们重点介绍了绿色荧光蛋白的新应用,其中绿色荧光蛋白被用作SWNTs的成像部分。与其他药物纳米载体相比,碳纳米管在负载能力,细胞内在化和生物降解性方面显示出巨大的积极潜力。我们还研究了结合模式(化学共轭和物理吸附)对化学发光活性,衰变速率和半衰期的影响。我们已经表明,通过LcL与CNT的适当化学偶联,LcL在ATP存在下对d-萤光素的催化具有生物活性,从而释放出可检测量的光子以用于体内成像。 LcL的化学发光可以在非表面位置以器官分辨率对CNT及其货物成像,而无需激发源。用抗肿瘤抗生素阿霉素加载LcL-CNT不会改变其成像的生物学活性。已经使用“ IVIS光谱”对LcL-CNT进行体内成像,显示了小鼠中不同器官对LcL-CNT的摄取。我们相信,LcL-CNT系统是用于体内成像的高级功能强大的工具,因此是朝着纳米医学领域发展的一步。

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