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Dynamic Biodistribution of Extracellular Vesicles in Vivo Using a Multimodal Imaging Reporter

机译:动态多细胞体内囊泡的生物分布使用多模式成像记者。

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Extracellular vesicles (EVs) are nanosized vesicles released by normal and diseased cells as a novel form of intercellular communication and can serve as an effective therapeutic vehicle for genes and drugs. Yet, much remains unknown about the in vivo properties of EVs such as tissue distribution, blood levels, and urine clearance, important parameters that will define their therapeutic effectiveness and potential toxicity. Here we combined Gaussia luciferase and metabolic biotinylation to create a sensitive EV reporter (EV-GlucB) for multimodal imaging in vivo, as well as monitoring of EV levels in the organs and biofluids ex vivo after administration of EVs. Bioluminescence and fluorescence-mediated tomography imaging on mice displayed a predominant localization of intravenously administered EVs in the spleen followed by the liver. Monitoring EV signal in the organs, blood, and urine further revealed that the EVs first undergo a rapid distribution phase followed by a longer elimination phase via hepatic and renal routes within six hours, which are both faster than previously reported using dye-labeled EVs. Moreover, we demonstrate systemically injected EVs can be delivered to tumor sites within an hour following injection. Altogether, we show the EVs are dynamically processed in vivo with accurate spatiotemporal resolution and target a number of normal organs as well as tumors with implications for disease pathology and therapeutic design.
机译:细胞外囊泡(EVs)是正常细胞和患病细胞释放的纳米级囊泡,是细胞间通讯的一种新型形式,可以用作基因和药物的有效治疗载体。然而,关于电动汽车的体内特性(例如组织分布,血液水平和尿液清除)的许多未知因素仍然未知,这些重要参数将定义电动汽车的治疗效果和潜在毒性。在这里,我们结合了高斯荧光素酶和代谢生物素化技术,创建了一个敏感的EV报告基因(EV-GlucB),用于体内多模式成像,以及在施用EV后离体监测器官和生物流体中的EV水平。小鼠的生物发光和荧光介导的断层扫描成像显示,静脉内施用的EV主要集中在脾脏中,然后是肝脏。监测器官,血液和尿液中的EV信号后,进一步发现,这些EV首先在六个小时内通过肝和肾途径经历了快速分布阶段,然后经历了更长的消除阶段,这都比以前使用染料标记的EV所报道的要快。此外,我们证明全身注射的电动车可在注射后一小时内递送至肿瘤部位。总而言之,我们显示了电动汽车在体内以准确的时空分辨率动态处理,并靶向许多正常器官以及与疾病病理和治疗设计有关的肿瘤。

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