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Antitumoral action of icaritin in LNCaP prostate cancer cells by regulating PEA3/HER2/AR signaling  期刊论文  

  • 编号:
    3d410076-974f-4d5b-8536-1394821a48d9
  • 作者:
  • 语种:
    English
  • 期刊:
    ANTI-CANCER DRUGS ISSN:0959-4973 2016 年 27 卷 10 期 (944 - 952) ; NOV
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  • 摘要:

    Human epidermal growth factor receptor type 2 (HER2) and androgen receptor (AR) are critical factors for prostate cancer (PCa) progression. These factors regulate tumor cell survival and proliferation, and remain as crucial drivers of castration-resistant PCa progression. Icaritin (ICT) is a prenyl flavonoid derived from the Epimedium genus, which has many biological and pharmacological effects. Using androgen-sensitive human prostate carcinoma LNCaP cell lines, we found that 35g/ml of ICT could inhibit more than 50% of cell proliferation, induce cell apoptosis, and lead to a strong G1 phase arrest by targeting cyclin-related proteins and suppressing the ability of cell invasion. Moreover, ICT exerts its potent anticancer efficacy by inducing polyomavirus enhancer activator 3 (PEA3) to inhibit the aberrantly activated HER2/AR signaling. In addition, after PEA3 expression was silenced by specific small-interference RNA, we found that both the ICT-inhibited effect on LNCaP cell proliferation and the ICT-induced cell apoptosis rate decreased. These results provide alternative mechanisms for the antitumor actions of ICT, indicating that ICT might be a promising therapeutic agent, as well as a preventive agent, for hormone therapy-resistant PCa.

  • 推荐引用方式
    GB/T 7714:
    Hu Jimeng,Zhu Wenhui,Wei Bingbing, et al. Antitumoral action of icaritin in LNCaP prostate cancer cells by regulating PEA3/HER2/AR signaling [J].ANTI-CANCER DRUGS,2016,27(10):944-952.
  • APA:
    Hu Jimeng,Zhu Wenhui,Wei Bingbing,Wen Hui,&Jiang Haowen.(2016).Antitumoral action of icaritin in LNCaP prostate cancer cells by regulating PEA3/HER2/AR signaling .ANTI-CANCER DRUGS,27(10):944-952.
  • MLA:
    Hu Jimeng, et al. "Antitumoral action of icaritin in LNCaP prostate cancer cells by regulating PEA3/HER2/AR signaling" .ANTI-CANCER DRUGS 27,10(2016):944-952.
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