Barzegar Mansoureh, Ma Shuang, Zhang Chao, Chen Xin, Gu Ying, Shang Chaowei, Jiang Xiaojuan, Yang Jiao, Nathan Cherie-Ann, Yang Shengyong, Huang Shile
Department of Biochemistry and Molecular Biology, Louisiana State University Health Sciences Center, 1501 Kings Highway, Shreveport, LA 71130-3932, USA.
State Key Laboratory of Biotherapy and Cancer Center/Collaborative Innovation Center of Biotherapy, West China Hospital, West China Medical School, Sichuan University, Chengdu, Sichuan 610041, China.
Br J Cancer. 2017 Oct 10;117(8):1154-1163. doi: 10.1038/bjc.2017.298. Epub 2017 Sep 5.
Overexpression of epidermal growth factor receptor (EGFR) occurs in approximately 90% of head and neck squamous cell carcinoma (HNSCC), and is correlated with poor prognosis. Thus, targeting EGFR is a promising strategy for treatment of HNSCC. Several small molecule EGFR inhibitors have been tested in clinical trials for treatment of HNSCC, but none of them are more effective than the current chemotherapeutic drugs. Thus, it is urgently needed to develop novel EGFR inhibitors for HNSCC treatment.
By screening an in-house focused library containing approximately 650 000 known kinase inhibitors and kinase inhibitor-like compounds containing common kinase inhibitor core scaffolds, we identified SKLB188 as a lead compound for inhibition of EGFR. The anticancer effects of SKLB188 on HNSCC cells were investigated by in vitro cell growth, cell cycle and apoptosis assays, as well as in vivo FaDu xenograft mouse model. Molecular docking, in vitro kinase profiling and western blotting were performed to characterise EGFR as the molecular target.
SKLB188 inhibited HNSCC cell proliferation by inducing G cell cycle arrest, which was associated with downregulating the expression of Cdc25A, cyclins D1/A and cyclin-dependent kinases (CDK2/4), and upregulating the expression of cyclin-dependent kinase (CDK) inhibitors (p21 and p27), leading to decreased phosphorylation of Rb. SKLB188 also induced caspase-dependent apoptosis of HNSCC cells by downregulating the expression of Mcl-1 and survivin. Molecular docking revealed that SKLB188 could bind to the kinase domain of EGFR through hydrogen bonds and hydrophobic interactions. In vitro kinase assay showed that SKLB188 inhibited the activity of a recombinant human EGFR very potently (IC=5 nM). Western blot analysis demonstrated that SKLB188 inhibited the phosphorylation of EGFR and its downstream targets, extracellular signal-regulated protein kinases 1 and 2 (Erk1/2) and Akt in the cells. In addition, SKLB188 dose-dependently inhibited FaDu xenograft growth in nude mice, and concurrently inhibited the phosphorylation of Erk1/2 and Akt in the tumours.
SKLB188 potently inhibits the growth of HNSCC cells in vitro and in vivo by targeting EGFR signalling. The results provide a basis for further clinical investigation of SKLB188 as a targeted therapy for HNSCC. Our findings may open a new avenue for development of novel EGFR inhibitors for treatment of HNSCC and other cancers.
表皮生长因子受体(EGFR)在约90%的头颈部鳞状细胞癌(HNSCC)中过表达,且与预后不良相关。因此,靶向EGFR是治疗HNSCC的一种有前景的策略。几种小分子EGFR抑制剂已在治疗HNSCC的临床试验中进行了测试,但它们均不比目前的化疗药物更有效。因此,迫切需要开发用于治疗HNSCC的新型EGFR抑制剂。
通过筛选一个内部聚焦文库,该文库包含约650000种已知激酶抑制剂和含有常见激酶抑制剂核心骨架的激酶抑制剂样化合物,我们鉴定出SKLB188作为抑制EGFR的先导化合物。通过体外细胞生长、细胞周期和凋亡测定以及体内FaDu异种移植小鼠模型研究了SKLB188对HNSCC细胞的抗癌作用。进行分子对接、体外激酶谱分析和蛋白质印迹以将EGFR表征为分子靶点。
SKLB188通过诱导G期细胞周期停滞抑制HNSCC细胞增殖,这与下调Cdc25A、细胞周期蛋白D1/A和细胞周期蛋白依赖性激酶(CDK2/4)的表达以及上调细胞周期蛋白依赖性激酶(CDK)抑制剂(p21和p27)的表达相关,导致Rb磷酸化减少。SKLB188还通过下调Mcl-1和survivin的表达诱导HNSCC细胞的半胱天冬酶依赖性凋亡。分子对接显示SKLB188可通过氢键和疏水相互作用与EGFR的激酶结构域结合。体外激酶测定表明SKLB188非常有效地抑制重组人EGFR的活性(IC = 5 nM)。蛋白质印迹分析表明SKLB188抑制细胞中EGFR及其下游靶点细胞外信号调节蛋白激酶1和2(Erk1/2)以及Akt的磷酸化。此外,SKLB188剂量依赖性地抑制裸鼠中FaDu异种移植瘤的生长,并同时抑制肿瘤中Erk1/2和Akt的磷酸化。
SKLB188通过靶向EGFR信号通路在体外和体内有效抑制HNSCC细胞的生长。这些结果为进一步临床研究SKLB188作为HNSCC的靶向治疗提供了依据。我们的发现可能为开发用于治疗HNSCC和其他癌症的新型EGFR抑制剂开辟一条新途径。
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