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New Treatments in Renal Cancer: The AhR Ligands

机译:肾癌的新疗法:AhR配体

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摘要

Kidney cancer rapidly acquires resistance to antiangiogenic agents, such as sunitinib, developing an aggressive migratory phenotype (facilitated by c-Metsignal transduction). The Aryl hydrocarbon receptor (AhR) has recently been postulated as a molecular target for cancer treatment. Currently, there are two antitumor agent AhR ligands, with activity against renal cancer, that have been tested clinically: aminoflavone (AFP 464, NSC710464) and the benzothiazole (5F 203) prodrug Phortress. Our studies investigated the action of AFP 464, the aminoflavone pro-drug currently used in clinical trials, and 5F 203 on renal cancer cells, specifically examining their effects on cell cycle progression, apoptosis and cell migration. Both compounds caused cell cycle arrest and apoptosis but only 5F 203 potently inhibited the migration of TK-10, Caki-1 and SN12C cells as well as the migration signal transduction cascade, involving c-Met signaling, in TK-10 cells. Current investigations are focused on the development of nano-delivery vehicles, apoferritin-encapsulated benzothiazoles 5F 203 and GW610, for the treatment of renal cancer. These compounds have shown improved antitumor effects against TK-10 cells in vitro at lower concentrations compared with a naked agent.
机译:肾脏癌迅速获得了对舒尼替尼等抗血管生成剂的耐药性,并发展了侵略性迁移表型(通过c-Metsignal转导)。最近,芳烃受体(AhR)被认为是治疗癌症的分子靶标。目前,已经有两种抗肿瘤药AhR配体具有抗肾癌的活性,并已在临床上进行了测试:氨基黄酮(AFP 464,NSC710464)和苯并噻唑(5F 203)前药Phortress。我们的研究调查了目前临床试验中使用的氨基黄酮前药AFP 464和5F 203对肾癌细胞的作用,特别研究了它们对细胞周期进程,细胞凋亡和细胞迁移的影响。两种化合物均导致细胞周期停滞和凋亡,但只有5F 203有效抑制TK-10细胞中TK-10,Caki-1和SN12C细胞的迁移以及涉及c-Met信号传导的迁移信号转导级联。当前的研究集中在用于肾癌治疗的纳米递送载体,载有铁铁蛋白包裹的苯并噻唑5F 203和GW610的开发上。与裸剂相比,这些化合物在较低浓度下在体外显示出对TK-10细胞的改善的抗肿瘤作用。

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