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Improved synthesis and biological evaluation of Tc‐99m radiolabeled AMO for miRNA imaging in tumor xenografts
Authors:Chao Ma  Ping Yan  Chunli Zhang  Huan Ma  Pan Hao  Xueqi Chen  Zhibing Zheng  Xiaojie Xu  Rongfu Wang
Affiliation:1. Department of Nuclear Medicine, Peking University First Hospital, Beijing, China;2. Laboratory of Computer‐aided Drug Design and Discovery, Beijing Institute of Pharmacology and Toxicology, Beijing, China;3. Department of Medical Molecular Biology, Beijing Institute of Biotechnology, Beijing, China
Abstract:MicroRNAs (miRNAs) have been considered as important biomarkers for malignant tumors. In this study, we introduced an improved 99mTc labeling method for noninvasive visualization of overexpressed miRNAs in tumor‐bearing mice. Anti‐miRNA‐21 oligonucleotide (AMO) with partial 2′‐O‐methyl and phosphorothioate modification was designed and chemically synthesized. After conjugated with NHS‐MAG3, AMO was labeled with 99mTc. Optimization was made to shorten reaction time and to improve labeling efficiency. Labeling efficiency was 97%, and specific activity was 2.78 MBq/ng. During 12 h, 99mTc‐AMO showed no significant degradation by gel electrophoresis. Its radiochemical purity was stable, between 95.8% and 99.1%. Further, 99mTc‐AMO decreased the level of miR‐21 and increased the expression of PTEN protein at cellular level, shown by qRT‐PCR and Western blot. Fluorescent protein labeled AMO displayed specific distribution and good stability in tumor cells. After the administration in tumor‐bearing mice, 99mTc‐AMO showed more radioactive uptake in the miR‐21 over‐expressed tumors than scramble control. Biodistribution results further proved the significant difference of tumor uptake between 99mTc‐AMO and 99mTc‐control. Therefore, this study presents an improved method with shorten time to prepare a 99mTc radiolabeled AMO. In addition, it supports the role of 99mTc‐AMO for noninvasive visualization of miR‐21 in malignant tumors.
Keywords:microRNA  molecular imaging  AMO  99mTc  radiolabel  SPECT
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