| Literature DB >> 30536880 |
Atsumi Yamaki1, Rino Akiyama1, Chiaki Murakami1, Saki Takao1, Yuki Murakami1, Satoru Mizuno1, Daisuke Takahashi1, Sayaka Kado2, Akinobu Taketomi3, Yasuhito Shirai4, Kaoru Goto5, Fumio Sakane1.
Abstract
Diacylglycerol (DG) kinase (DGK), which phosphorylates DG to generate phosphatidic acid (PA), consists of ten isozymes (α-к). Recently, we identified a novel small molecule inhibitor, CU-3, that selectively inhibits the activity of the α isozyme. In addition, we newly obtained Compound A, which selectively and strongly inhibits type I DGKs (α, β, and γ). In the present study, we demonstrated that both CU-3 and Compound A induced apoptosis (caspase 3/7 activity and DNA fragmentation) and viability reduction of AKI melanoma cells. Liquid chromatography-mass spectrometry revealed that the production of 32:0- and 34:0-PA species was commonly attenuated by CU-3 and Compound A, suggesting that lower levels of these PA molecular species are involved in the apoptosis induction and viability reduction of AKI cells. We determined the effects of the DGKα inhibitors on several other cancer cell lines derived from refractory cancers. In addition to melanoma, the DGKα inhibitors enhanced caspase 3/7 activity and reduced the viability of hepatocellular carcinoma, glioblastoma, and pancreatic cancer cells, but not breast adenocarcinoma cells. Interestingly, Western blot analysis indicated that the DGKα expression levels were positively correlated with the sensitivity to the DGK inhibitors. Because both CU-3 and Compound A induced interleukin-2 production by T cells, it is believed that these two compounds can enhance cancer immunity. Taken together, our results suggest that DGKα inhibitors are promising anticancer drugs.Entities:
Keywords: apoptosis; cancer; diacylglycerol kinase (DGK); inhibitor; melanoma; phosphatidic acid (PA)
Year: 2018 PMID: 30536880 DOI: 10.1002/jcb.28288
Source DB: PubMed Journal: J Cell Biochem ISSN: 0730-2312 Impact factor: 4.429