Curcumol Enhances the Sensitivity of Gastric Cancer to Cisplatin Resistance by Inducing Ferroptosis Through the P62/KEAP1/NRF2 Pathway.

IF 2.9 3区 医学 Q2 INTEGRATIVE & COMPLEMENTARY MEDICINE Integrative Cancer Therapies Pub Date : 2024-01-01 DOI:10.1177/15347354241294043
Tongfei Feng, Yanlin Zhou, Xiangying Mao, Xiaowei Rui, Lijun Cai
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Abstract

Background: Chemoresistance represented one of the challenges in the treatment of advanced gastric cancer (GC). Curcumol (CUR) was found to have a certain sensitizing effect on chemoresistance, although the mechanism was not yet fully understood. Purpose: To clarify the ability of CUR to intervene in the sensitivity of GC cells to Cisplatin (CDDP) by regulating the induction of ferroptosis through the P62/KEAP1/NRF2 pathway. Methods: An in vitro resistant cell line was established and treated with CUR for intervention. The synergy was evaluated using synergyfinder3.0 software. The impact of the combined use of CUR and CDDP on the proliferation, migration, and invasion of resistant GC cells was determined. The effect of CUR on ferroptosis in resistant GC cell lines was evaluated by measuring changes in reactive oxygen species (ROS) levels, malondialdehyde (MDA) levels, iron ion levels, and the ratio of reduced glutathione (GSH) to oxidized glutathione (GSSG). Western blotting was used to verify the expression changes of the ferroptosis-related indicator GPX4 and the differential expression of the antioxidant-related pathway P62/KEAP1/NRF2, validating the mechanism by which CUR induces ferroptosis in resistant GC cells. In vivo validation was performed using a xenograft mouse model. Results: The evaluation by synergy3.0 revealed a synergistic effect between CUR and CDDP. After treatment with CUR and CDDP, resistant GC cell lines exhibited reduced proliferation, migration, and invasion capabilities. Furthermore, the resistant GC cell lines underwent ferroptosis, with significant changes observed in ferroptosis-related indicators such as ROS, MDA, iron ions, and GSH/GSSG. The ferroptosis-related targets Glutathione Peroxidase 4 (GPX4) and the antioxidant pathway P62/KEAP1/NRF2 signaling pathway also showed significant changes. In in vivo validation, the combination of CUR and CDDP inhibited the growth of subcutaneous tumors and was found to be associated with the inhibition of subcutaneous xenografts and the GPX4 and P62/KEAP1/NRF2 signaling pathways. Conclusion: This study first revealed that CUR enhanced the sensitivity of cisplatin-resistant GC cells to CDDP by inducing ferroptosis. The combination of CUR and CDDP induces ferroptosis in cisplatin-resistant GC through the P62/KEAP1/NRF2 pathway.

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姜黄素通过P62/KEAP1/NRF2途径诱导铁突变,从而增强胃癌对顺铂耐药的敏感性
背景:化疗耐药性是晚期胃癌(GC)治疗过程中面临的挑战之一。研究发现莪术醇(CUR)对化疗耐药性有一定的增敏作用,但其机制尚未完全明了。目的:阐明莪术醇通过 P62/KEAP1/NRF2 通路调节铁变态反应的诱导,从而干预 GC 细胞对顺铂 (CDDP) 的敏感性。研究方法建立体外耐药细胞系并用 CUR 进行干预。使用 synergyfinder3.0 软件评估协同作用。确定了联合使用 CUR 和 CDDP 对耐药 GC 细胞的增殖、迁移和侵袭的影响。通过测量活性氧(ROS)水平、丙二醛(MDA)水平、铁离子水平以及还原型谷胱甘肽(GSH)与氧化型谷胱甘肽(GSSG)之比的变化,评估了 CUR 对耐药性 GC 细胞株铁变态反应的影响。利用 Western 印迹技术验证了铁变态反应相关指标 GPX4 的表达变化以及抗氧化相关途径 P62/KEAP1/NRF2 的差异表达,从而验证了 CUR 在耐药性 GC 细胞中诱导铁变态反应的机制。利用异种移植小鼠模型进行了体内验证。结果:synergy3.0 评估显示,CUR 和 CDDP 具有协同效应。经 CUR 和 CDDP 处理后,耐药 GC 细胞株的增殖、迁移和侵袭能力均有所下降。此外,耐药 GC 细胞株发生了铁变态反应,与铁变态反应相关的指标,如 ROS、MDA、铁离子和 GSH/GSSG 都发生了显著变化。与铁变态反应相关的靶点谷胱甘肽过氧化物酶4(GPX4)和抗氧化通路P62/KEAP1/NRF2信号通路也发生了显著变化。在体内验证中,CUR 和 CDDP 的组合抑制了皮下肿瘤的生长,并发现这与抑制皮下异种移植以及 GPX4 和 P62/KEAP1/NRF2 信号通路有关。结论本研究首次发现 CUR 通过诱导铁变态反应增强了顺铂耐药 GC 细胞对 CDDP 的敏感性。CUR和CDDP联合使用可通过P62/KEAP1/NRF2途径诱导顺铂耐药GC的铁突变。
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来源期刊
Integrative Cancer Therapies
Integrative Cancer Therapies 医学-全科医学与补充医学
CiteScore
4.80
自引率
3.40%
发文量
78
审稿时长
>12 weeks
期刊介绍: ICT is the first journal to spearhead and focus on a new and growing movement in cancer treatment. The journal emphasizes scientific understanding of alternative medicine and traditional medicine therapies, and their responsible integration with conventional health care. Integrative care includes therapeutic interventions in diet, lifestyle, exercise, stress care, and nutritional supplements, as well as experimental vaccines, chrono-chemotherapy, and other advanced treatments. Contributors are leading oncologists, researchers, nurses, and health-care professionals.
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