Han Bing, Yu Yi-Qun, Yang Qi-Lian, Shen Chun-Ying, Wang Xiao-Juan
Department of Pharmacy, Minhang Hospital, Fudan University, Shanghai, China.
Oncotarget. 2017 Sep 16;8(49):86227-86239. doi: 10.18632/oncotarget.21043. eCollection 2017 Oct 17.
In the present study, we demonstrate that Kaempferol inhibited survival and proliferation of established human hepatocellular carcinoma (HCC) cell lines (HepG2, Huh-7, BEL7402, and SMMC) and primary human HCC cells. Kaempferol treatment in HCC cells induced profound AMP-activated protein kinase (AMPK) activation, which led to Ulk1 phosphorylation, mTOR complex 1 inhibition and cell autophagy. Autophagy induction was reflected by Beclin-1/autophagy gene 5 upregulation and p62 degradation as well as light chain 3B (LC3B)-I to LC3B-II conversion and LC3B puncta formation. Inhibition of AMPK, via AMPKα1 shRNA or dominant negative mutation, reversed above signaling changes. AMPK inhibition also largely inhibited Kaempferol-induced cytotoxicity in HCC cells. Autophagy inhibition, by 3-methyaldenine or Beclin-1 shRNA, also protected HCC cells from Kaempferol. Kaempferol downregulated melanoma antigen 6, the AMPK ubiquitin ligase, causing AMPKα1 stabilization and accumulation. We conclude that Kaempferol inhibits human HCC cells via activating AMPK signaling.
在本研究中,我们证明了山奈酚可抑制已建立的人肝癌(HCC)细胞系(HepG2、Huh-7、BEL7402和SMMC)以及原代人肝癌细胞的存活和增殖。在肝癌细胞中,山奈酚处理可诱导强烈的AMP激活蛋白激酶(AMPK)激活,进而导致Ulk1磷酸化、mTOR复合物1抑制和细胞自噬。自噬诱导表现为Beclin-1/自噬基因5上调、p62降解以及轻链3B(LC3B)-I向LC3B-II的转化和LC3B斑点形成。通过AMPKα1短发夹RNA(shRNA)或显性负突变抑制AMPK,可逆转上述信号变化。AMPK抑制也在很大程度上抑制了山奈酚诱导的肝癌细胞毒性。通过3-甲基腺嘌呤或Beclin-1 shRNA抑制自噬,也可保护肝癌细胞免受山奈酚的影响。山奈酚下调黑色素瘤抗原6(一种AMPK泛素连接酶),导致AMPKα1稳定和积累。我们得出结论,山奈酚通过激活AMPK信号通路抑制人肝癌细胞。
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