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Targeting of pertechnetate imaging of HepG2 hepatocellular carcinoma through the transduction of the survivin promoter controls the sodium iodide symporter

机译:通过转导survivin启动子靶向靶向HepG2肝细胞癌的高net酸酯成像可控制碘化钠同向转运蛋白

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摘要

Currently, the intratumoral (i.t.) injection of adenovirus-mediated cancer gene therapy has been reported in numerous investigations. However, the intravenous (i.v.) injection of adenovirus is more suited for disseminated tumors and distant metastatic lesions. The survivin promoter, which has tumor-selective capability, was used to construct an adenoviral vector, and its feasibility to carry the sodium iodide symporter (NIS) gene for potential tumor-targeting transfection into carcinoma was evaluated in this study. An in vitro cellular assay using HepG2 hepatocellular carcinoma (HCC) cells exhibited iodide uptake after infection with Ad-Sur-NIS, and the uptake reached a maximum level at 30 min. The effective half-life of I efflux from Ad-Sur-NIS infected HepG2 cells was 16.67 ± 1.08 min. Moreover, in vivo transfection of Ad-Sur-NIS via i.v. injection induced more effective transfection and, accordingly, induced higher uptake of pertechnetate in HCC xenograft tumors than did the non-specific transfection of Ad-CMV-NIS (i.v.) (P<0.05), indicating possible selective NIS gene-transfecting image strategies by the survivin promoter.
机译:目前,在许多研究中已经报道了瘤内(i.t.)注射腺病毒介导的癌症基因疗法。然而,腺病毒的静脉内(i.v.)注射更适合于扩散的肿瘤和远处的转移性病变。使用具有肿瘤选择能力的survivin启动子构建腺病毒载体,并评估了其携带碘化钠共转运蛋白(NIS)基因用于潜在的靶向肿瘤转染至癌的可行性。使用Ad-Sur-NIS感染后,使用HepG2肝细胞癌(HCC)细胞进行的体外细胞测定显示碘化物吸收,并且在30分钟时吸收达到最高水平。来自被Ad-Sur-NIS感染的HepG2细胞的I外排的有效半衰期为16.67±1.08分钟。此外,通过静脉内体内转染Ad-Sur-NIS。与Ad-CMV-NIS的非特异性转染相比,注射HSC诱导的HCC异种移植瘤更有效转染,并因此诱导更高的高tech酸盐摄取(iv)(P <0.05),表明可能有选择性的NIS基因转染图像策略survivin启动子。

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