靶向c-kit通过减弱干性、上皮-间质转化和获得性耐药来抑制吉非替尼耐药的非小细胞肺癌细胞的生长和侵袭。
Targeting c-kit inhibits gefitinib resistant NSCLC cell growth and invasion through attenuations of stemness, EMT and acquired resistance.
作者信息
Zhou Yueling, Wang Li, Sun Zhen, Zhang Jie, Wang Xiujie
机构信息
Laboratory of Experimental Oncology, State Key Laboratory of Biotherapy/Collaborative Innovation Center for Biotherapy, West China Hospital, West China Clinical Medical School, Sichuan University Chengdu 610041, China.
出版信息
Am J Cancer Res. 2020 Dec 1;10(12):4251-4265. eCollection 2020.
EGFR tyrosine kinase inhibitors (TKIs) are the first-line drugs for NSCLC. But, the acquired resistance limited their efficacy, so that the patients deteriorate eventually. Therefore, it is necessary to clarify the mechanism of the acquired resistance and overcome it for effective NSCLC therapy. In this experimental study, a stable gefitinib resistant lung adenocarcinoma cell line (PC9/GR) infected with shRNA-c-kit-homo-1386 were established; c-kit siRNA and c-kit inhibitors were used to block c-kit signaling; the acquired resistance of PC9/GR cells and the effects of c-kit siRNA and c-kit inhibitors on the growth and invasion of PC9/GR cells were investigated with CCK-8 assay, colony formation and cell invasion assays ; the tumor growth inhibition effects of c-kit inhibitors on PC9/GR cell generated tumors were tested ; the mechanisms involved in the acquired resistance reverse, growth and invasion inhibition effects of c-kit siRNA and c-kit inhibitors on PC9/GR cells were evaluated with qRT-PCR, Western blot and immunohistochemistry staining. The proliferation, colony formation, and invasion of PC9/GR cells were decreased by c-kit siRNA and inhibitors significantly; c-kit inhibitors suppressed the tumor growth of PC9/GR cell generated tumors . In the stable shRNA-c-kit transfected PC9/GR cells, the protein expressions of c-kit signaling and stemness phenotype related proteins, including ALDH1A1, Oct4, Sox2 and ABCG2 were decreased, and EMT phenotype related protein expressions including vimentin, N-cadherin, and Slug, were downregulated and with upregulation of E-cadherin; c-kit inhibitors reduced stemness phenotype related protein expressions, downregulated EMT phenotype related protein expressions including vimentin, N-cadherin, and Slug, with upregulation of E-cadherin, and the stemness related protein expressions of c-kit, ALDH1A1, ABCG2 and EMT-related proteins of vimentin and slug were decreased in the imatinib treated tumor tissues. The findings of this study indicated that c-kit signaling mediated the acquired gefitinib resistance, cell growth, invasion, stemness and EMT phenotype of PC9/GR cells. Targeting c-kit signaling with c-kit siRNA and small molecule c-kit inhibitors might overcome the acquired gefitinib resistance, and inhibit PC9/GR cell growth in and in .
表皮生长因子受体酪氨酸激酶抑制剂(TKIs)是用于非小细胞肺癌(NSCLC)的一线药物。但是,获得性耐药限制了它们的疗效,最终导致患者病情恶化。因此,有必要阐明获得性耐药的机制并克服它,以实现有效的NSCLC治疗。在本实验研究中,建立了用shRNA-c-kit-homo-1386感染的稳定的吉非替尼耐药肺腺癌细胞系(PC9/GR);使用c-kit siRNA和c-kit抑制剂阻断c-kit信号传导;采用CCK-8法、集落形成实验和细胞侵袭实验研究PC9/GR细胞的获得性耐药以及c-kit siRNA和c-kit抑制剂对PC9/GR细胞生长和侵袭的影响;检测c-kit抑制剂对PC9/GR细胞产生的肿瘤的生长抑制作用;采用qRT-PCR、蛋白质免疫印迹法和免疫组织化学染色评估c-kit siRNA和c-kit抑制剂逆转PC9/GR细胞获得性耐药、抑制其生长和侵袭的相关机制。c-kit siRNA和抑制剂显著降低了PC9/GR细胞的增殖、集落形成和侵袭能力;c-kit抑制剂抑制了PC9/GR细胞产生的肿瘤的生长。在稳定转染shRNA-c-kit的PC9/GR细胞中,c-kit信号传导以及干性表型相关蛋白(包括醛脱氢酶1A1、八聚体结合转录因子4、性别决定区Y框蛋白2和ATP结合盒转运蛋白G2)的蛋白表达降低,上皮-间质转化(EMT)表型相关蛋白(包括波形蛋白、N-钙黏蛋白和锌指蛋白Snail)的表达下调,而E-钙黏蛋白表达上调;c-kit抑制剂降低了干性表型相关蛋白的表达,下调了包括波形蛋白、N-钙黏蛋白和锌指蛋白Snail在内的EMT表型相关蛋白的表达,同时E-钙黏蛋白表达上调,并且在伊马替尼治疗的肿瘤组织中,c-kit、醛脱氢酶1A1、ATP结合盒转运蛋白G2的干性相关蛋白表达以及波形蛋白和锌指蛋白Snail的EMT相关蛋白表达均降低。本研究结果表明,c-kit信号传导介导了PC9/GR细胞对吉非替尼的获得性耐药、细胞生长、侵袭、干性和EMT表型。用c-kit siRNA和小分子c-kit抑制剂靶向c-kit信号传导可能克服PC9/GR细胞对吉非替尼的获得性耐药,并在体内和体外抑制PC9/GR细胞生长。
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