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首页> 外文期刊>Molecular cancer therapeutics >Targeting AKT with Oridonin Inhibits Growth of Esophageal Squamous Cell Carcinoma In Vitro and Patient-Derived Xenografts In Vivo
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Targeting AKT with Oridonin Inhibits Growth of Esophageal Squamous Cell Carcinoma In Vitro and Patient-Derived Xenografts In Vivo

机译:靶向AKT与oridonin抑制在体外体外和患者衍生的异种移植物中食管鳞状细胞癌的生长

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摘要

Overexpression or activation of AKT is very well known to control cell growth, survival, and gene expression in solid tumors. Oridonin, an inflammatory medical and diterpenoid compound isolated from Rabdosia rubescens, has exhibited various pharmacologic and physiologic properties, including antitumor, antibacterial, and anti-inflammatory effects. In this study, we demonstrated that oridonin is an inhibitor of AKT and suppresses proliferation of esophageal squamous cell carcinoma (ESCC) in vitro and in vivo. The role of AKT in ESCC was studied using immuno-histochemical analysis of a tumor microarray, the effect of AKT knockdown on cell growth, and treatment of cells with MK-2206, an AKT inhibitor. Oridonin blocked AKT kinase activity and interacted with the ATP-binding pocket of AKT. It inhibited growth of KYSE70, KYSE410, and KYSE450 esophageal cancer cells in a time- and concentration-dependent manner. Oridonin induced arrest of cells in the G2-M cell-cycle phase, stimulated apoptosis, and increased expression of apoptotic biomarkers, including cleaved PARP, caspase-3, caspase-7, and Bims in ESCC cell lines. Mechanistically, we found that oridonin diminished the phosphorylation and activation of AKT signaling. Furthermore, a combination of oridonin and 5-fluorouracil or cisplatin (clinical chemotherapeutic agents) enhanced the inhibition of ESCC cell growth. The effects of oridonin were verified in patient-derived xenograft tumors expressing high levels of AKT. In summary, our results indicate that oridonin acts as an AKT inhibitor to suppress the growth of ESCC by attenuating AKT signaling. Mol Cancer Ther; 17(7); 1540-53. (C) 2018 AACR.
机译:众所周知,AKT的过度表达或激活是控制细胞生长,生存和基因表达在实体肿瘤中。 Oridonin,从Rabdosia Rubescens分离的炎症医疗和二萜类化合物,表现出各种药理和生理性质,包括抗肿瘤,抗菌和抗炎作用。在这项研究中,我们证明Oridonin是AKT的抑制剂,并在体外和体内抑制食管鳞状细胞癌(ESCC)的增殖。使用肿瘤微阵列的免疫组织化学分析研究了AKT在ESCC中的作用,AKT敲低对细胞生长的影响,以及AKT抑制剂的MK-2206的细胞的处理。 Oridonin阻断AKT激酶活性并与AKT的ATP结合口袋相互作用。它抑制Kyse70,Kyse410和Kyse450以时期和浓度依赖性方式的生长。 Oridonin诱导在G2-M细胞周期阶段,刺激的细胞凋亡和凋亡生物标志物的表达增加,包括切割的PARP,Caspase-3,Caspase-7和ESCC细胞系中的BIM的细胞增加。机械地,我们发现奥利替素减少了Akt信号传导的磷酸化和激活。此外,奥利替素和5-氟尿嘧啶或顺铂(临床化学治疗剂)的组合增强了ESCC细胞生长的抑制。在表达高水平Akt的患者衍生的异种移植肿瘤中验证了奥里替尼的效果。总之,我们的结果表明,奥利替林作为AKT抑制剂通过衰减AKT信号传导来抑制ESCC的生长。 mol癌症; 17(7); 1540-53。 (c)2018年AACR。

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  • 来源
    《Molecular cancer therapeutics》 |2018年第7期|共14页
  • 作者

    Song Mengqiu; Liu Xuejiao; Liu Kangdong; Zhao Ran; Huang Hai; Shi Yuanyuan; Zhang Man; Zhou Silei; Xie Hua; Chen Hanyong; Li Yin; Zheng Yan; Wu Qiong; Liu Fangfang; Li Enmin; Bode Ann M.; Dong Zigang; Lee Mee-Hyun;

  • 作者单位

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

    China US Henan Hormel Canc Inst 127 Dongming Rd Zhengzhou 450008 Henan Peoples R China;

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

    China US Henan Hormel Canc Inst 127 Dongming Rd Zhengzhou 450008 Henan Peoples R China;

    China US Henan Hormel Canc Inst 127 Dongming Rd Zhengzhou 450008 Henan Peoples R China;

    China US Henan Hormel Canc Inst 127 Dongming Rd Zhengzhou 450008 Henan Peoples R China;

    China US Henan Hormel Canc Inst 127 Dongming Rd Zhengzhou 450008 Henan Peoples R China;

    Chinese Acad Sci Shanghai Inst Mat Med Div Antitumor Pharmacol State Key Lab Drug Res Shanghai;

    Univ Minnesota Hormel Inst 801 16th Ave NE Austin MN 55912 USA;

    Zhengzhou Univ Henan Canc Hosp Dept Thorac Surg Affiliated Canc Hosp Zhengzhou Henan Peoples;

    Zhengzhou Univ Henan Canc Hosp Dept Thorac Surg Affiliated Canc Hosp Zhengzhou Henan Peoples;

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

    Shantou Univ Dept Biochem &

    Mol Biol Med Coll Shantou Guangdong Peoples R China;

    Univ Minnesota Hormel Inst 801 16th Ave NE Austin MN 55912 USA;

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

    Zhengzhou Univ Sch Basic Med Sci Dept Pathophysiol Zhengzhou Henan Peoples R China;

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  • 正文语种 eng
  • 中图分类 肿瘤学;
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