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胸腺醌通过摄取/外排基因调节使人类结直肠癌细胞对伊马替尼敏感。

Thymoquinone chemosensitizes human colorectal cancer cells to imatinib via uptake/efflux genes modulation.

机构信息

Pharmacology Unit, Department of Cancer Biology, National Cancer Institute, Cairo University, Cairo, Egypt.

Department of Pharmacology and Toxicology, Faculty of Pharmacy, Ahram Canadian University, Giza, Egypt.

出版信息

Clin Exp Pharmacol Physiol. 2021 Jun;48(6):911-920. doi: 10.1111/1440-1681.13476. Epub 2021 Mar 29.

DOI:10.1111/1440-1681.13476
PMID:33783002
Abstract

Imatinib (IM) is a pharmaceutical drug that inhibits tyrosine kinase enzymes that are responsible for the activation of many proteins by signal transduction cascades as c-Abl, c-Kit and the platelet-derived growth factor (PDGF) receptor. Thymoquinone (TQ) is an active constituent of Nigella sativa seeds. Thymoquinone benefits are attributed to its medicinal uses as antioxidant, anticancer and antimicrobial agent. This study aimed to investigate the impact of using TQ with IM in the HCT human colorectal cancer cell line model. The HCT cells were treated with IM or/and TQ in non-constant ratios, in which the fixed concentrations of TQ (5, 10 or 20 µmol/L) were co-treated with various concentrations of IM (7.5-120 µmol/L) for 24, 48 and 72 hours. Imatinib-TQ interaction was analysed using CompuSyn software. The IC values for IM were 105, 72 μmol/L after 48 and 72 hours, respectively, and were significantly reduced to 7.3, 7 and 5.5 μmol/L after combination with TQ (10 μmol/L) and to 5.8, 5.6 and 4.6 μmol/L after combination with TQ (20 μmol/L) to 24, 48 and 72 hours, respectively. The combination index (CI) and dose reduction index (DRI) values indicate a significant synergism in HCT-116 cells at different treatment time points. Thymoquinone significantly enhances the cellular uptake of IM in HCT cells in a time and concentration-dependent manner. A significant downregulation in ATP-binding cassette (ABC) subfamily B member 1 (ABCB1), ABC subfamily G member 2 (ABCG2) and human organic cation transporter 1 (hOCT1) genes was observed in the cells exposed to IM+TQ combination as compared to IM alone, which resulted in a substantial elevation in uptake/efflux ratio in combination group. In conclusion, TQ potentiates IM efficacy on HCT cells via uptake/efflux genes modulation.

摘要

伊马替尼(IM)是一种抑制酪氨酸激酶酶的药物,这些酶通过信号转导级联反应负责激活许多蛋白质,如 c-Abl、c-Kit 和血小板衍生生长因子(PDGF)受体。百里醌(TQ)是黑种草种子的一种活性成分。百里醌的益处归因于其作为抗氧化剂、抗癌和抗菌剂的药用用途。本研究旨在探讨在 HCT 人结直肠癌细胞模型中使用 TQ 与 IM 的联合应用的影响。将 HCT 细胞用 IM 或/和 TQ 以非恒定比例处理,其中固定浓度的 TQ(5、10 或 20μmol/L)与各种浓度的 IM(7.5-120μmol/L)共同处理 24、48 和 72 小时。使用 CompuSyn 软件分析 IM-TQ 相互作用。IM 的 IC 值分别为 48 和 72 小时后的 105 和 72μmol/L,与 TQ(10μmol/L)联合后显著降低至 7.3、7 和 5.5μmol/L,与 TQ(20μmol/L)联合后降低至 5.8、5.6 和 4.6μmol/L 至 24、48 和 72 小时。组合指数(CI)和剂量减少指数(DRI)值表明在不同的治疗时间点,HCT-116 细胞中存在显著的协同作用。TQ 以时间和浓度依赖的方式显著增加 HCT 细胞中 IM 的细胞摄取。与单独使用 IM 相比,暴露于 IM+TQ 组合的细胞中 ABC 亚家族 B 成员 1(ABCB1)、ABC 亚家族 G 成员 2(ABCG2)和人有机阳离子转运蛋白 1(hOCT1)基因的下调显著,导致组合组中的摄取/流出比显著升高。总之,TQ 通过摄取/流出基因调节增强 IM 对 HCT 细胞的疗效。

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