OBJECTIVE: FTY720 is a potent drug for multiple sclerosis treatment. To biologically address its possible applications to more generalized diseases with aberrant inflammation, we are testing whether FTY720 can function as a lymphocyte cell cycle blocker and activation suppressor via a concanavalin A (ConA)-mediated mouse lymphocyte pan-activation model. METHODS: Mouse lymphocytes were obtained from lymph nodes and subjected to ConA and/or FTY720 treatment. Cell viability was assayed by MTT and mitochondrial assays. Early and late activation, cell cycle, proliferation and intracellular Ca(2+) concentration ([Ca(2+)](i)) were analyzed by flow cytometry. RESULTS: At concentrations of less than 500 nM, FTY720 significantly down-regulated both CD69 and CD25 expressions of T cells, as well as inhibiting proliferation of activated lymphocytes. In addition, FTY720 blocked the ConA-induced mitogenesis, exhibiting lymphocyte G(0)/G(1) phase cell cycle arrest with significant reduction of cells in S and G(2)/M phases. Meanwhile, a significant decline in [Ca(2+)](i) was observed. The correlation of [Ca(2+)](i) and cell cycle arrest were validated by employing a [Ca(2+)](i) inhibitor SK&F 96365 and testing with and without FTY720 treatment. CONCLUSION: We demonstrated that FTY720 induces G(0)/G(1) phase cell cycle arrest, resulting in proliferation inhibition upon lymphocyte pan-activation, which may be related to reduction of overall intracellular Ca(2+) load.
OBJECTIVE:FTY720 is a potent drug for multiple sclerosis treatment. To biologically address its possible applications to more generalized diseases with aberrant inflammation, we are testing whether FTY720 can function as a lymphocyte cell cycle blocker and activation suppressor via a concanavalin A (ConA)-mediated mouse lymphocyte pan-activation model. METHODS:Mouse lymphocytes were obtained from lymph nodes and subjected to ConA and/or FTY720 treatment. Cell viability was assayed by MTT and mitochondrial assays. Early and late activation, cell cycle, proliferation and intracellular Ca(2+) concentration ([Ca(2+)](i)) were analyzed by flow cytometry. RESULTS: At concentrations of less than 500 nM, FTY720 significantly down-regulated both CD69 and CD25 expressions of T cells, as well as inhibiting proliferation of activated lymphocytes. In addition, FTY720 blocked the ConA-induced mitogenesis, exhibiting lymphocyte G(0)/G(1) phase cell cycle arrest with significant reduction of cells in S and G(2)/M phases. Meanwhile, a significant decline in [Ca(2+)](i) was observed. The correlation of [Ca(2+)](i) and cell cycle arrest were validated by employing a [Ca(2+)](i) inhibitor SK&F 96365 and testing with and without FTY720 treatment. CONCLUSION: We demonstrated that FTY720 induces G(0)/G(1) phase cell cycle arrest, resulting in proliferation inhibition upon lymphocyte pan-activation, which may be related to reduction of overall intracellular Ca(2+) load.
Authors: Adam C Yopp; Shuang Fu; Shaun M Honig; Gwendalyn J Randolph; Yaozhong Ding; Nancy R Krieger; Jonathan S Bromberg Journal: J Immunol Date: 2004-07-15 Impact factor: 5.422
Authors: Volker Brinkmann; Andreas Billich; Thomas Baumruker; Peter Heining; Robert Schmouder; Gordon Francis; Shreeram Aradhye; Pascale Burtin Journal: Nat Rev Drug Discov Date: 2010-10-29 Impact factor: 84.694
Authors: R Fujii; T Kanai; Y Nemoto; S Makita; S Oshima; R Okamoto; K Tsuchiya; T Totsuka; M Watanabe Journal: Am J Physiol Gastrointest Liver Physiol Date: 2006-03-30 Impact factor: 4.052