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Heparin antagonizes cisplatin resistance of A2780 ovarian cancer cells by affecting the Wnt signaling pathway

机译:肝素通过影响Wnt信号通路拮抗A2780卵巢癌细胞的顺铂耐药性

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摘要

Low molecular weight heparin (LMWH), the guideline based drug for prophylaxis and treatment of cancer-associated thrombosis, was recently shown to sensitize cisplatin resistant A2780cis human ovarian cancer cells for cisplatin cytotoxicity upon 24 h pretreatment with 50 mu g x mL(-1) of the LMWH tinzaparin in vitro, equivalent to a therapeutic dosage. Thereby, LMWH induced sensitization by transcriptional reprogramming of A2780cis cells via not yet elucidated mechanisms that depend on cellular proteoglycans. Here we aim to illuminate the underlying molecular mechanisms of LMWH in sensitizing A2780cis cells for cisplatin. Using TCF/LEF luciferase promotor assay (Top/Flash) we show that resistant A2780cis cells possess a threefold higher Wnt signaling activity compared to A2780 cells. Furthermore, Wnt pathway blockade by FH535 leads to higher cisplatin sensitivity of A2780cis cells. Glypican-3 (GPC3) is upregulated in A2780cis cells in response to LMWH treatment, probably as counter-regulation to sustain the high Wnt activity against LMWH. Hence, LMWH reduces the cisplatin-induced rise in Wnt activity and TCF-4 expression in A2780cis cells, but keeps sensitive A2780 cells unaffected. Consequently, Wnt signaling pathway appears as primary target of LMWH in sensitizing A2780cis cells for cisplatin toxicity. Considering the outstanding role of LMWH in clinical oncology, this finding appears as promising therapeutic option to hamper chemoresistance.
机译:低分子量肝素(LMWH)是预防和治疗癌症相关血栓形成的基于指南的药物,最近被证明可以在50μg g mL(-1)预处理24小时后使顺铂耐药A2780cis卵巢癌细胞对顺铂细胞毒性敏感。 LMWH替扎肝素在体外的剂量等于治疗剂量。因此,LMWH通过尚未阐明的依赖细胞蛋白聚糖的机制,通过A2780cis细胞的转录重编程诱导了致敏作用。在这里,我们旨在阐明在使A2780cis细胞对顺铂敏感的过程中LMWH的潜在分子机制。使用TCF / LEF荧光素酶启动子分析(顶部/快速),我们显示抗性A2780cis细胞比A2780细胞具有高三倍的Wnt信号传导活性。此外,FH535对Wnt途径的阻断导致A2780cis细胞对顺铂的敏感性更高。响应LMWH处理,A2780cis细胞中的Glypican-3(GPC3)被上调,可能是为了维持Wnt对LMWH的高活性而进行的反调节。因此,LMWH减少了顺铂诱导的A2780cis细胞中Wnt活性和TCF-4表达的增加,但使敏感的A2780细胞不受影响。因此,在使A2780cis细胞对顺铂毒性敏感的过程中,Wnt信号通路似乎是LMWH的主要靶标。考虑到LMWH在临床肿瘤学中的杰出作用,这一发现似乎是有希望阻止化学耐药性的治疗选择。

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