个人信息Personal Information
教授
博士生导师
硕士生导师
性别:男
毕业院校:中科院大连化学物理研究所
学位:博士
所在单位:化工海洋与生命学院
学科:药理学. 生物医学工程. 生物化学与分子生物学
办公地点:盘锦校区F03-312B
联系方式:大连理工大学生命科学与药学学院 辽宁省盘锦市辽东湾新区大工路2号 邮编:124221 电话: 0427-2631433
电子邮箱:yliu@dlut.edu.cn
Cadmium induces cell growth in A549 and HELF cells via autophagy-dependent glycolysis
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论文类型:期刊论文
发表时间:2020-08-01
发表刊物:TOXICOLOGY IN VITRO
收录刊物:PubMed、SCIE
卷号:66
页面范围:104834
ISSN号:0887-2333
关键字:Cadmium; Autophagy; Glycolysis; Cell cycle
摘要:Cadmium (Cd) is a pervasive harmful metal in the environment. It is a well-known inducer of tumorigenesis, but its mechanism is still unclear. We have previously reported that Cd-induced autophagy was apoptosis-dependent and prevents apoptotic cell death to ensure the growth of A549 cells. In this study, the mechanism was further investigated. Cd treatment increased glucose uptake and lactate release significantly. Meanwhile, the protein level of GLUT1 , HKII , PKM2 and LDHA increased in a time-dependent manner, indicating that Cd induced aerobic glycolysis in A549 and HELF cells. The inhibitors of autophagy, 3MA, and CQ, repressed Cd-induced glycolysis-related proteins, indicating that autophagy was involved in Cd-induced glycolysis in A549 and HELF cells. Knockdown of ATG4B or ATG5 by siATG4B and siATG5 decreased Cd-induced glycolysis, while overexpression of ATG4B enhanced glycolysis. These results demonstrated that Cd-induced glycolysis was autophagy-dependent. Then, glycolysis inhibitor, 2DG and siPKM2 could inhibit Cd-induced cell viability and cell cycle progression compared to only Cd treatment, indicating that glycolysis played an important role in Cd-induced cell growth. Finally, co-treatment of transfection of ATG4B-DNA plasmids with 2DG or siPKM2 further demonstrated that the autophagy-glycolysis axis played an important role in Cd-induced cell cycle progression. Taken together, our results suggested that Cd-induced glycolysis is autophagy-dependent and the autophagyglycolysis axis underlies the mechanism of Cd-induced cell growth in A549 and HELF cells.