Effect to Therapy of Sodium-Iodine Symporter Expression by Alpha-Ray Therapeutic Agent via Sodium/Iodine Symporter

α射线治疗剂通过钠/碘同向转运蛋白对钠/碘同向转运蛋白表达的治疗作用

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Abstract

This study confirmed the effect of sodium/iodine symporter (NIS) expression on existing drugs by in vitro and in vivo tests using cultured cell lines. The tumor growth inhibitory effect of sodium astatide ([(211)At]NaAt) was evaluated by in vitro and in vivo tests using human thyroid cancer cells (K1, K1/NIS and K1/NIS-DOX). NIS expression in cancer cells was controlled using the Tet-On system. [(131)I]NaI was used as control existing drug. From the results of the in vitro studies, the mechanism of [(211)At]NaAt uptake into thyroid cancer cells is mediated by NIS, analogous to [(131)I]NaI, and the cellular uptake rate correlates with the expression level of NIS. [(211)At]NaAt's ability to inhibit colony formation was more than 10 times that of [(131)I]NaI per becquerel (Bq), and [(211)At]NaAt's DNA double-strand breaking (DSB) induction was more than ten times that of [(131)I]NaI per Bq, and [(211)At]NaAt was more than three times more cytotoxic than [(131)I]NaI (at 1000 kBq each). In vivo studies also showed that the tumor growth inhibitory effect of [(211)At]NaAt depended on NIS expression and was more than six times that of [(131)I]NaI per Bq.

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