Synergistic effects of resveratrol with gemcitabine in pancreatic cancer chemotherapy by inhibiting the c-Met/PARP1 axis

Shuai Wu, Jiaqiang Ren, Weikun Qian, M. Gong, Jie Li, Tao Qin, Simei Zhang, Wunai Zhang, Hao Sun, Zheng Wu, Zheng Wang, Qingyong Ma, Wanxing Duan
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Abstract

Pancreatic cancer is a highly malignant tumor of the digestive tract with a dismal prognosis. A key challenge of pancreatic cancer is its resistance to chemotherapy. The c-Met/PARP1 axis plays an important role in the therapeutic resistance of breast cancer and hepatocellular carcinoma. Therefore, this study aims to explore potential therapeutic targets for improving chemotherapy for pancreatic cancer and the underlying mechanisms. Gemcitabine-resistant pancreatic cancer cell lines were constructed by our laboratory using a continuous low-concentration gemcitabine induction method. The proliferation and apoptosis of combination therapy were examined using flow cytometry and comet assay. Synergistic effects of two drugs were determined by Chou-Talalay's combination index (CI). The interactions between proteins were predicted using the AutoDock model and detected through Coimmunoprecipitation assays. The combination of resveratrol and gemcitabine inhibited proliferation and promoted apoptosis of pancreatic cancer cells. We found that c-Met and PARP1 were highly expressed in gemcitabine-resistant pancreatic cancer cells. However, resveratrol inhibited their expression and improved the effectiveness of gemcitabine-induced DNA damage. In addition, our data demonstrated that resveratrol and gemcitabine had synergistic effects (CI < 1). Furthermore, the protein interactions between c-Met and PARP1 were attenuated after the early stage of resveratrol intervention. Using AutoDock models, we predicted the potential binding sites where resveratrol could impact the protein interaction between c-Met (tyrosine kinase domain) and PARP1 (CAT domain). Our results suggested that the synergistic effects of resveratrol with gemcitabine depend on the c-Met/PAPR1 axis. Using resveratrol as a combined chemotherapy agent may have clinical benefits for patients with refractory pancreatic cancer.
白藜芦醇与吉西他滨通过抑制 c-Met/PARP1 轴在胰腺癌化疗中产生协同效应
胰腺癌是一种预后不良的高度恶性消化道肿瘤。胰腺癌的一个主要挑战是对化疗的耐药性。c-Met/PARP1 轴在乳腺癌和肝细胞癌的耐药性中起着重要作用。因此,本研究旨在探索改善胰腺癌化疗的潜在治疗靶点及其内在机制。 本实验室采用连续低浓度吉西他滨诱导方法构建了吉西他滨耐药胰腺癌细胞系。采用流式细胞术和彗星试验检测了联合疗法的增殖和凋亡情况。通过 Chou-Talalay 联合指数(CI)确定两种药物的协同效应。使用 AutoDock 模型预测了蛋白质之间的相互作用,并通过免疫共沉淀试验进行了检测。 白藜芦醇和吉西他滨的联合用药抑制了胰腺癌细胞的增殖并促进了其凋亡。我们发现,c-Met和PARP1在吉西他滨耐药的胰腺癌细胞中高表达。然而,白藜芦醇抑制了它们的表达,并改善了吉西他滨诱导的DNA损伤的有效性。此外,我们的数据表明,白藜芦醇和吉西他滨具有协同作用(CI < 1)。此外,在白藜芦醇干预的早期阶段,c-Met 和 PARP1 之间的蛋白质相互作用有所减弱。我们利用AutoDock模型预测了白藜芦醇可能影响c-Met(酪氨酸激酶结构域)和PARP1(CAT结构域)之间蛋白质相互作用的潜在结合位点。 我们的结果表明,白藜芦醇与吉西他滨的协同作用取决于 c-Met/PAPR1 轴。使用白藜芦醇作为联合化疗药物可能会对难治性胰腺癌患者产生临床疗效。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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