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Anticancer Mechanism of Curcumin on Human Glioblastoma

机译:抗癌机制姜黄素对人胶质细胞瘤的抗癌机制

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摘要

Glioblastoma (GBM) is the most malignant brain tumor and accounts for most adult brain tumors. Current available treatment options for GBM are multimodal, which include surgical resection, radiation, and chemotherapy. Despite the significant advances in diagnostic and therapeutic approaches, GBM remains largely resistant to treatment, with a poor median survival rate between 12 and 18 months. With increasing drug resistance, the introduction of phytochemicals into current GBM treatment has become a potential strategy to combat GBM. Phytochemicals possess multifarious bioactivities with multitarget sites and comparatively marginal toxicity. Among them, curcumin is the most studied compound described as a potential anticancer agent due to its multi-targeted signaling/molecular pathways properties. Curcumin possesses the ability to modulate the core pathways involved in GBM cell proliferation, apoptosis, cell cycle arrest, autophagy, paraptosis, oxidative stress, and tumor cell motility. This review discusses curcumin’s anticancer mechanism through modulation of Rb, p53, MAPK, P13K/Akt, JAK/STAT, Shh, and NF-κB pathways, which are commonly involved and dysregulated in preclinical and clinical GBM models. In addition, limitation issues such as bioavailability, pharmacokinetics perspectives strategies, and clinical trials were discussed.
机译:Glioblastoma(GBM)是最恶毒的脑肿瘤,也是大多数成年脑肿瘤的患者。 GBM的当前可用治疗方案是多式联算的,包括手术切除,辐射和化疗。尽管诊断和治疗方法的显着进展,但GBM仍然对治疗仍然很耐药,中位数差12至18个月之间。随着耐药性的增加,将植物化学的引入当前的GBM治疗成为打击GBM的潜在策略。植物化学品具有多种生物活体,具有多元位点和比较边际毒性。其中,由于其多目标信号/分子途径性能,姜黄素是作为潜在的抗癌剂描述的最多研究的化合物。姜黄素具有调节GBM细胞增殖,细胞凋亡,细胞周期停滞,自噬,缓喂剂,氧化应激和肿瘤细胞运动的核心途径的能力。本综述讨论姜黄素的抗癌机制通过调制RB,P53,MAPK,P13K / AKT,JAK / Stat,SHH和NF-κB途径,通常涉及并在临床前和临床GBM模型中进行了失调。此外,还讨论了诸如生物利用度,药代动力学观点策略和临床试验之类的限制问题。

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