| Literature DB >> 33456361 |
Xiaoyan Jiang1,2, Jing Yuan1, Yingyu Dou1, Da Zeng1, Songshu Xiao1.
Abstract
Previous studies have found that LPS and FRA1 play opposite roles in cervical cancer. In addition, LPS functions by regulating the expression of FRA1 in many disease models, but there is currently no study of their relationship in the energy metabolism of tumor cells. This study, therefore, investigates the effects of LPS on FRA1-mediated glucose metabolism and the possible mechanisms it may have in cervical cancer cells. We constructed FRA1 stable overexpressing/ empty vector cervical cancer cell lines, where glucose consumption, the level of lactic acid production and the expression of energy metabolism related molecules were detected under the stimulation of LPS. At the same time, the changes in proliferation ability of cervical cancer cells were detected. We discovered that LPS promotes glucose consumption, lactic acid production, pentose phosphate bypass, and inhibits aerobic oxidation, by inhibiting the expression of FRA1; and that LPS promotes the growth of cervical cancer cells. Our results indicate that LPS affects the proliferation and glucose metabolism of cervical cancer cells through the FRA1/MDM2/p53 pathway. © The author(s).Entities:
Keywords: FRA1; LPS; cervical cancer; metabolism
Year: 2021 PMID: 33456361 PMCID: PMC7807182 DOI: 10.7150/ijms.47360
Source DB: PubMed Journal: Int J Med Sci ISSN: 1449-1907 Impact factor: 3.738