《口腔颌面外科杂志》 ›› 2024, Vol. 34 ›› Issue (4): 276-281. doi: 10.12439/kqhm.1005-4979.2024.04.004

• 基础研究 • 上一篇    下一篇

索拉非尼抑制口腔鳞状细胞癌细胞的自噬、增殖及迁移

熊建哲(), 张昊, 余伟()   

  1. 十堰市人民医院(湖北医药学院附属人民医院)口腔科,十堰 442000
  • 收稿日期:2023-02-03 接受日期:2023-10-09 出版日期:2024-08-28 发布日期:2024-08-26
  • 通讯作者: 余伟,副主任医师. E-mail: yuweikouqiang@163.com
  • 作者简介:
    熊建哲,医师. E-mail:
  • 基金资助:
    十堰市科技局科研项目(21Y51)

Sorafenib tosylate inhibits autophagy, proliferation and migration of oral squamous cell carcinoma

XIONG Jianzhe(), ZHANG Hao, YU Wei()   

  1. Department of Stomatology, Shiyan People's Hospital (Affiliated People's Hospital of Hubei Medical University), Shiyan 442000, China
  • Received:2023-02-03 Accepted:2023-10-09 Online:2024-08-28 Published:2024-08-26

摘要:

目的:研究甲苯磺酸索拉非尼(Sorafenib tosylate,ST)对口腔鳞状细胞癌(oral squamous cell carcinoma,OSCC)CAL-27细胞自噬、增殖、迁移的影响。方法:采用不同浓度的索拉非尼处理CAL-27细胞,使用CCK-8法和细胞克隆形成实验检测其增殖活性;通过细胞划痕实验检测其对CAL-27细胞迁移能力的影响;通过蛋白质印迹法检测Beclin1、LC3B、PCNA的表达。用自噬激活剂雷帕霉素(rapamycin,RA)预处理CAL-27细胞,检测激活自噬后索拉非尼对CAL-27细胞增殖、迁移和Beclin-1、LC3B、PCNA表达的影响。结果:与对照组相比,索拉非尼可显著抑制CAL-27的细胞增殖和迁移;索拉非尼使Beclin-1和PCNA表达下降、LC3B的胞质形式LC3Ⅰ和LC3B的脂质形式LC3Ⅱ的表达上升;但用RA预处理CAL-27细胞激活自噬后,索拉非尼对CAL-27细胞的增殖、迁移的抑制作用被削弱,Beclin-1和PCNA的表达上升,LC3B的胞质形式LC3Ⅰ和LC3B的脂质形式LC3Ⅱ的表达下降。结论:索拉非尼可能通过下调Beclin-1抑制自噬,从而抑制CAL-27细胞的增殖和迁移,为OSCC提供潜在的治疗策略。

关键词: 口腔鳞状细胞癌, 自噬, 增殖, 迁移, 索拉非尼

Abstract:

Objective: To study the effect of Sorafenib tosylate (ST) on autophagy, proliferation and migration of CAL-27 cells in oral squamous cell carcinoma (OSCC). Methods: The CAL-27 cells were treated with different concentrations of ST, and their proliferation activity was detected by CCK-8 and cell clone formation assay; the effect of the CAL-27 cells migration was detected by cell wound scratch assay; the expressions of Beclin1, LC3B and PCNA were detected by western blotting. The CAL-27 cells were pretreated with the autophagy activator rapamycin, and the effects of ST on the proliferation, migration and expression of Beclin1, LC3B and PCNA in CAL-27 cells were detected after activation of autophagy. Results: Compared with the control group, ST significantly inhibited the proliferation and migration of the CAL-27 cells. ST decreased the expressions of Beclin-1, PCNA and increased the expressions of the cytoplasmic form LC3Ⅰ and the lipid form LC3Ⅱ of LC3B. However, when the CAL-27 cells were pretreated with RA to activate autophagy, the inhibitory effect of ST on proliferation and migration of the CAL-27 cells were weakened, the expressions of Beclin-1 and PCNA were increased, and the expressions of the cytoplasmic form LC3Ⅰ and the lipid form LC3Ⅱ of LC3B were decreased. Conclusion: ST may inhibit the proliferation and migration of CAL-27 cells by down-regulating Beclin-1, and inhibiting autophagy. Inhibition of autophagy may be a potential therapeutic strategy for OSCC.

Key words: oral squamous cell carcinoma, autophagy, proliferation, migration, Sorafenib tosylate

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