| Literature DB >> 30689149 |
Jin Jin1,2, Yujia Zhao1,2, Wan Guo1,2, Bingrong Wang1,2, Yigang Wang1, Xinyuan Liu1,3, Chuanlian Xu4,5.
Abstract
Thiocoraline, a depsipeptide bisintercalator with potent antitumor activity, was first isolated from marine actinomycete Micromonospora marina. It possesses an intense toxicity to MCF-7 cells at nanomolar concentrations in a dose-dependent manner evaluated by MTT assay and crystal violet staining. We established a human breast thiocoraline-resistant cancer subline of MCF-7/thiocoraline (MCF-7/T) to investigate the expression variation of breast cancer resistance proteins (BCRP) and its subsequent influence on drug resistance. Colony-forming assay showed that the MCF-7 cells proliferated faster than the MCF-7/T cells in vitro. Western blot analysis demonstrated that thiocoraline increased the phosphorylation of Akt. Additionally, the sensitivity of tumor cells to thiocoraline was reduced with a concurrent rise in phosphorylation level of Akt and of BCRP expression.These studies indicated that thiocoraline probably mediated the drug resistance via PI3K/Akt/BCRP signaling pathway. MK-2206 dihydrochloride, a selective phosphorylation inhibitor of Akt, significantly decreased MCF-7 cell viability under exposure to thiocoraline compared to the control. However, it was not obviously able to decrease MCF-7/T cell viability when cells were exposed to thiocoraline.Entities:
Keywords: BCRP; MCF-7; MK-2206 dihydrochloride; Multidrug resistance; PI3K/Akt/BCRP signaling pathway; Thiocoraline
Year: 2019 PMID: 30689149 PMCID: PMC6368516 DOI: 10.1007/s10616-019-00301-w
Source DB: PubMed Journal: Cytotechnology ISSN: 0920-9069 Impact factor: 2.058