Inhibition of the Inositol Requiring Protein 1α- X-Box Binding Protein-1 Pathway as a Promising Therapeutic Target for Human Prostate Cancer

A. Khalil, A. Alghadi, Rahaf M. T. Shahen, Jehad W. Elasad, K. Jawasreh
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Abstract

Prostate cancer (PCa) has been associated with endoplasmic reticulum stress (ERS) which activates the inositol requiring protein 1α- X-box binding protein-1 (IREα-XBP-1) pathway. The aim of the study was to investigate the role of this pathway in three human PCa cell lines (LNCaP, PC-3, and DU-145) by evaluating the expression of XBP-1 and glucose-regulated protein 78 (GRP78) genes. The effect of two ERS inducers (Thapsigargin, Tg and tunicamycin, Tm) alone and in combination with an inhibitor of the IRE1α RNase inhibitor (STF-083010) on expression profiling was followed using Quantitative-PCR. In vitro treatment of PCa cells with ERS inducers upregulated expression of XBP-1 gene. STF-083010 inhibited IRE1α-induced splicing of the gene and increased cytotoxicity. Inhibition of IRE1α RNase activity significantly decreased expression of chaperon protein GRP78. The results confirm and extend the concept that selective targeting of IRE1α-XBP-1 pathway might be a novel therapeutic approach that curbs PCa cell progression.
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抑制肌醇需求蛋白1α- X-Box结合蛋白1途径作为人类前列腺癌的有希望的治疗靶点
前列腺癌(PCa)与内质网应激(ERS)有关,内质网应激激活了肌醇需要蛋白1α- X-box结合蛋白-1 (IREα-XBP-1)途径。本研究的目的是通过评估XBP-1和葡萄糖调节蛋白78 (GRP78)基因的表达,探讨该途径在三种人PCa细胞系(LNCaP、PC-3和DU-145)中的作用。采用定量pcr方法观察两种ERS诱导剂(Thapsigargin, Tg和tunicamycin, Tm)单独使用和与IRE1α RNase抑制剂(STF-083010)联合使用对表达谱的影响。体外用ERS诱导剂处理PCa细胞可上调XBP-1基因的表达。STF-083010抑制ire1 α-诱导的基因剪接,增加细胞毒性。抑制IRE1α RNase活性可显著降低伴侣蛋白GRP78的表达。结果证实并扩展了选择性靶向IRE1α-XBP-1通路可能是抑制PCa细胞进展的新治疗方法的概念。
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