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索拉非尼与天然酚类化合物联合作用对肝癌细胞的序列依赖性影响及可能的作用机制。

Sequence‑dependent effect of sorafenib in combination with natural phenolic compounds on hepatic cancer cells and the possible mechanism of action.

机构信息

Molecular Biology Program, Department of Biological Sciences, Faculty of Science, Kuwait University, 13060 Safat, State of Kuwait.

Department of Microbiology and Immunology, Faculty of Medicine, Kuwait University, 13060 Safat, State of Kuwait.

出版信息

Int J Mol Med. 2018 Sep;42(3):1695-1715. doi: 10.3892/ijmm.2018.3725. Epub 2018 Jun 8.

DOI:10.3892/ijmm.2018.3725
PMID:29901131
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6089756/
Abstract

Sorafenib (Nexavar, BAY43‑9006 or Sora) is the first molecular targeted agent that has exhibited significant therapeutic benefits in advanced hepatocellular carcinoma (HCC). However, not all HCC patients respond well to Sora and novel therapeutic strategies to optimize the efficacy of Sora are urgently required. Plant‑based drugs have received increasing attention owing to their excellent chemotherapeutic and chemopreventive activities; they are also well tolerated, non‑toxic, easily available and inexpensive. It is well known that certain biologically active natural products act synergistically with synthetic drugs used in clinical applications. The present study aimed to investigate whether a combination therapy with natural phenolic compounds (NPCs), including curcumin (Cur), quercetin (Que), kaempherol (Kmf) and resveratrol (Rsv), would allow a dose reduction of Sora without concomitant loss of its effectiveness. Furthermore, the possible molecular mechanisms of this synergy were assessed. The hepatic cancer cell lines Hep3b and HepG2 were treated with Sora alone or in combination with NPCs in concomitant, sequential, and inverted sequential regimens. Cell proliferation, cell cycle, apoptosis and expression of proteins associated with the cell cycle and apoptosis were investigated. NPCs markedly potentiated the therapeutic efficacy of Sora in a sequence‑, type‑, NPC dose‑ and cell line‑dependent manner. Concomitant treatment with Sora and Cur [sensitization ratio (SR)=28], Kmf (SR=18) or Que (SR=8) was associated with the highest SRs in Hep3b cells. Rsv markedly potentiated the effect of Sora (SR=17) on Hep3b cells when administered in a reverse sequential manner. By contrast, Rsv and Que did not improve the efficacy of Sora against HepG2 cells, while concomitant treatment with Cur (SR=10) or Kmf (SR=4.01) potentiated the cytotoxicity of Sora. Concomitant treatment with Sora and Cur or Kmf caused S‑phase and G2/M phase arrest of liver cancer cells and markedly induced apoptosis compared with mono‑treatment with Sora, Cur or Kmf. Concomitant treatment with Sora and Cur reduced the protein levels of cyclins A, B2 and D1, phosphorylated retinoblastoma and B‑cell lymphoma (Bcl) extra‑large protein. By contrast, Sora and Cur co‑treatment increased the protein levels of Bcl‑2‑associated X protein, cleaved caspase‑3 and cleaved caspase‑9 in a dose‑dependent manner. In conclusion, concomitant treatment with Sora and Cur or Kmf appears to be a potent and promising therapeutic approach that may control hepatic cancer by triggering cell cycle arrest and apoptosis. Additional studies are required to examine the potential of combined treatment with Sora and NPCs in human hepatic cancer and other solid tumor types in vivo.

摘要

索拉非尼(Nexavar、BAY43-9006 或 Sora)是首个在晚期肝细胞癌(HCC)中表现出显著治疗益处的分子靶向药物。然而,并非所有 HCC 患者对 Sora 反应良好,因此迫切需要新的治疗策略来优化 Sora 的疗效。植物药由于其出色的化疗和化学预防活性而受到越来越多的关注;它们还具有良好的耐受性、无毒、易于获得且价格低廉。众所周知,某些具有生物活性的天然产物与临床应用中的合成药物协同作用。本研究旨在探讨天然酚类化合物(NPCs),包括姜黄素(Cur)、槲皮素(Que)、山奈酚(Kmf)和白藜芦醇(Rsv)的联合治疗是否可以在不降低其有效性的情况下减少 Sora 的剂量。此外,还评估了这种协同作用的可能分子机制。将肝癌细胞系 Hep3b 和 HepG2 分别用 Sora 单独或与 NPC 联合治疗,采用同时、序贯和反序治疗方案。研究了细胞增殖、细胞周期、凋亡以及与细胞周期和凋亡相关的蛋白表达。NPCs 以序列、类型、NPC 剂量和细胞系依赖性方式显著增强了 Sora 的治疗效果。在 Hep3b 细胞中,Sora 与 Cur [增敏比(SR)=28]、Kmf(SR=18)或 Que(SR=8)同时治疗与最高的 SR 相关。当以反序方式给予 Rsv 时,Rsv 可显著增强 Sora 对 Hep3b 细胞的作用(SR=17)。相比之下,Rsv 和 Que 并不能提高 Sora 对 HepG2 细胞的疗效,而同时用 Cur(SR=10)或 Kmf(SR=4.01)治疗则增强了 Sora 的细胞毒性。Sora 与 Cur 或 Kmf 同时治疗导致肝癌细胞的 S 期和 G2/M 期停滞,并与 Sora、Cur 或 Kmf 单药治疗相比,明显诱导了细胞凋亡。Sora 与 Cur 同时治疗可降低 cyclin A、B2 和 D1、磷酸化视网膜母细胞瘤和 B 细胞淋巴瘤(Bcl)大蛋白的蛋白水平。相比之下,Sora 和 Cur 共同处理以剂量依赖性方式增加了 Bcl-2 相关 X 蛋白、裂解 caspase-3 和裂解 caspase-9 的蛋白水平。总之,Sora 与 Cur 或 Kmf 同时治疗似乎是一种有效且有前途的治疗方法,可通过触发细胞周期停滞和凋亡来控制肝癌。需要进一步研究以检查 Sora 和 NPCs 联合治疗在人类肝癌和其他实体肿瘤类型中的潜在应用。

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