| Literature DB >> 29957841 |
Ling Xu1,2, Tianshu Guo1,2, Xiujuan Qu1,2, Xuejun Hu3, Ye Zhang1,2, Xiaofang Che1,2, Huicong Song1,2, Jing Gong1,2, Rui Ma1,2, Ce Li1,2, Yibo Fan1,2, Yanju Ma1,2, Kezuo Hou1,2, Peihong Wu1,2, Hang Dong1,2, Yunpeng Liu1,2.
Abstract
β-Elemene, an anti-cancer drug extracted from traditional Chinese medicinal herb, showed anti-tumor effects on gastric cancer cells. Our previous studies reported gastric cancer cells are insensitive to TRAIL. However, whether β-elemene could enhance anti-cancer effects of TRAIL on gastric cancer cells is unknown. In our present study, β-elemene prevented gastric cancer cell viability in dose-dependent manner, and when combined with TRAIL, obviously inhibited proliferation and promoted apoptosis in gastric cancer cells. Compared to β-elemene or TRAIL alone, treatment with β-elemene and TRAIL obviously promoted DR5 clustering as well as translocation of Caspase-8, DR5 and FADD into lipid rafts. This led to cleavage of Caspase-8 and the formation of death-inducing signaling complex (DISC) in lipid rafts. The cholesterol-sequestering agent nystatin partially reversed DR5 clustering and DISC formation, preventing apoptosis triggered by the combination of β-elemene and TRAIL. Our results suggest that β-elemene increases the sensitivity of gastric cancer cells to TRAIL partially by promoting the formation of DISC in lipid rafts.Entities:
Keywords: DISC; TRAIL; apoptosis; gastric cancer; β-elemene
Mesh:
Substances:
Year: 2018 PMID: 29957841 DOI: 10.1002/cbin.11023
Source DB: PubMed Journal: Cell Biol Int ISSN: 1065-6995 Impact factor: 3.612