体内分布
化学
小干扰RNA
正电子发射断层摄影术
体内
脂质体
荧光
临床前影像学
阳离子脂质体
荧光寿命成像显微镜
生物物理学
核糖核酸
核医学
体外
转染
生物化学
医学
光学
基因
物理
生物技术
生物
作者
Kentaro Hatanaka,Tomohiro Asai,Hiroyuki Koide,Eriya Kenjo,Takuma Tsuzuku,Norihiro Harada,Hideo Tsukada,Naoto Oku
摘要
Pharmacokinetic study of small interfering RNA (siRNA) is an important issue for the development of siRNAs for use as a medicine. For this purpose, a novel and favorable positron emitter-labeled siRNA was prepared by amino group-modification using N-succinimidyl 4-[fluorine-18] fluorobenzoate ([(18)F]SFB), and real-time analysis of siRNA trafficking was performed by using positron emission tomography (PET). Naked [(18)F]-labeled siRNA or cationic liposome/[(18)F]-labeled siRNA complexes were administered to mice, and differential biodistribution of the label was imaged by PET. The former was cleared quite rapidly from the bloodstream and excreted from the kidneys; but in contrast, the latter tended to accumulate in the lungs. We also confirmed the biodistribution of fluorescence-labeled naked siRNA and cationic liposome/siRNA complexes by use of a near-infrared fluorescence imaging system. As a result, a similar biodistribution was observed, although quantitative data were obtained only by planar positron imaging system (PPIS) analysis but not by fluorescence in vivo imaging. Our results indicate that PET imaging of siRNA provides important information for the development of siRNA medicines.
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