| Literature DB >> 29534146 |
Gaomei Chang1,2, Jiayi Zheng3, Wenqin Xiao1,2, Shuaikang Chang1,2, Qing Wei3, Huiqun Wu1,2, Yi Tao1,2, Guang Yang1,2, Bingqian Xie1,2, Xiucai Lan1,2, Yingcong Wang1,2, Dandan Yu1,2, Liangning Hu1,2, Yongsheng Xie1,2, Wenxuan Bu1,2, Yuanyuan Kong1,2, Bojie Dai4, Jun Hou1,2, Jumei Shi1,2.
Abstract
MCT-1 (multiple copies in T-cell lymphoma-1), a novel oncogene, was originally identified in T-cell lymphoma. A recent study has demonstrated that MCT-1 is highly expressed in 85% of diffuse large B-cell lymphomas (DLBCL). PKC (protein kinase C) plays an essential role in signal transduction for multiple biologically active substances for activating cellular functions and proliferation. In this study, we found that the mRNA and protein expression levels of MCT-1 were visibly decreased after knocking down PKC by siRNA in SUDHL-4 and OCI-LY8 DLBCL cell lines. A selective PKC inhibitor, sotrastaurin, effectively inhibited cell proliferation and induced cell apoptosis in a dose- and time-dependent manner. Meanwhile, we also observed that the cell cycle was arrested in the G1 phase in sotrastaurin-treated cells. In addition, MCT-1 was down-regulated in the sotrastaurin treatment group in vivo. Furthermore, we demonstrated that the PKC inhibitor sotrastaurin induced cell apoptosis and cell cycle arrest in DLBCL cells potentially through regulating the expression of MCT-1. Our data suggest that targeting PKC may be a potential therapeutic approach for lymphomas and related malignancies that exhibit high levels of MCT-1 protein.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29534146 DOI: 10.1093/abbs/gmy021
Source DB: PubMed Journal: Acta Biochim Biophys Sin (Shanghai) ISSN: 1672-9145 Impact factor: 3.848