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人钠碘转运体基因转移后碘转运增强与滞留缺乏及低吸收剂量相关。

Enhanced iodide transport after transfer of the human sodium iodide symporter gene is associated with lack of retention and low absorbed dose.

作者信息

Haberkorn U, Kinscherf R, Kissel M, Kübler W, Mahmut M, Sieger S, Eisenhut M, Peschke P, Altmann A

机构信息

Department of Nuclear Medicine, University of Heidelberg, Heidelberg, Germany.

出版信息

Gene Ther. 2003 May;10(9):774-80. doi: 10.1038/sj.gt.3301943.

Abstract

Transfer of the sodium iodide symporter (hNIS) has been proposed as a new principle of cancer gene therapy. Using clinically relevant doses of (131)I for the treatment of NIS-expressing prostate carcinoma cells, we investigated the kinetics and the absorbed doses obtained in these tumors. hNIS-expressing cell lines accumulated up to 200 times more iodide when compared to wild-type cells. However, a rapid efflux of the radioactivity (80%) occurred during the first 20 min after replacement of the medium. In rats, the hNIS-expressing tumors accumulated up to 20 times more iodide when compared to contralateral transplanted wild-type tumors. After 24 h and doses of 550, 1200 or 2400 MBq/m(2) hNIS-expressing tumors lost 89, 89 and 91% of the initial activity, respectively. Dosimetric calculations showed that 1200 MBq/m(2) resulted in 3+/-0.5 Gy (wild-type tumor 0.15+/-0.1 Gy) and 2400 MBq/m(2) resulted in 3.1+/-0.9 Gy (wild-type tumor 0.26+/-0.02 Gy). Although transduction of the hNIS gene induces iodide transport in rat prostate adenocarcinoma a rapid efflux occurs, which leads to a low absorbed dose in genetically modified tumors. With regard to a therapeutic application additional conditions need to be defined leading to iodide trapping.

摘要

碘化钠同向转运体(hNIS)的转移已被提议作为癌症基因治疗的新原理。使用临床相关剂量的(131)I治疗表达NIS的前列腺癌细胞,我们研究了这些肿瘤中的动力学和吸收剂量。与野生型细胞相比,表达hNIS的细胞系积累的碘化物多高达200倍。然而,在更换培养基后的最初20分钟内,放射性迅速流出(80%)。在大鼠中,与对侧移植的野生型肿瘤相比,表达hNIS的肿瘤积累的碘化物多高达20倍。24小时后,给予550、1200或2400 MBq/m²剂量后,表达hNIS的肿瘤分别失去了初始活性的89%、89%和91%。剂量学计算表明,1200 MBq/m²导致3±0.5 Gy(野生型肿瘤为0.15±0.1 Gy),2400 MBq/m²导致3.1±0.9 Gy(野生型肿瘤为0.26±0.02 Gy)。尽管hNIS基因的转导在大鼠前列腺腺癌中诱导了碘化物转运,但会发生快速流出,这导致基因改造肿瘤中的吸收剂量较低。关于治疗应用,需要确定导致碘化物捕获的其他条件。

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