To investigate the inhibitory effects of Ginsenoside Rbl (GRbl) on apoptosis caused by Herpes Simplex Virus-1 (HSV-1) in Human Glioma Cells (U251), U251 cells were infected by HSV-1 at a multiplicity of infectio...To investigate the inhibitory effects of Ginsenoside Rbl (GRbl) on apoptosis caused by Herpes Simplex Virus-1 (HSV-1) in Human Glioma Cells (U251), U251 cells were infected by HSV-1 at a multiplicity of infection of 5 and GRbl, GRbl+HSV-1, HSV-1 and control groups. MTT and cell apoptosis assays were used to detect the inhibitory effects of GRbl on the apoptosis of U251 cells that caused by HSV-1 infection for various concentrations of drug and virus treatments by MTT assay. We found that in the 400 μg/mL GRb 1 and 400 μg/mL GRbl+HSV-1 groups, MTT values were higher than control group at all times (P〈0.05). Moreover, the apoptosis rate in the 400 μg/mL GRbl+HSV-1 group was lower than the HSV-1 group (P〈0. 05). These results confirmed that, at appropriate concentrations, GRbl could inhibit nerve cell apoptosis in HSV-1 infections.展开更多
OBJECTIVE To explore the potential neurotrophic effect of bone marrow stromal cells (BMSCs) on cell proliferation and committed neuronal differentiation of ventral mesencephalic precursors (VMPs) in vitro. METHODS...OBJECTIVE To explore the potential neurotrophic effect of bone marrow stromal cells (BMSCs) on cell proliferation and committed neuronal differentiation of ventral mesencephalic precursors (VMPs) in vitro. METHODS Ventral mesencephalic precursors from Ell inbred rat embryos and BMSCs from adult rats were cultured both separately and in co-culture. After a 7-day incubation in vitro, three conditioned culture media were obtained, termed VMP or common medium, BMSC medium, and BMSC±VMP medium. Ventral mesen- cephalic precursors cells were cultured in each of these media and the effects on proliferation and VMP differentiation were assessed. The relative yield of TH± cells was calculated and compared by immunocytochemical staining. RESULTS After a 7-day culture and induction of VMPs, the total cell counts were increased by (44.13±4.75)-fold (common), (60.63±5.25)-fold (BMSC), and (64.00±7.63)-fold (BMSC±VMP). The proportions of TH+ cells were (18.76±5.20)%, (23.49±4.10)%, and (28.08± 5.42)%, respectively, with statistically significant differences among the treatment groups. CONCLUSION BMSCs release factors that promote the proliferation of VMPs and facilitate the committed differentiation of VMPs into dopaminergic neurons.展开更多
基金Supported by National Natural Science Foundation of China(Grant No.81070501 and 30770105)Shandong Provincial Outstanding Medical Academic Professional Program
文摘To investigate the inhibitory effects of Ginsenoside Rbl (GRbl) on apoptosis caused by Herpes Simplex Virus-1 (HSV-1) in Human Glioma Cells (U251), U251 cells were infected by HSV-1 at a multiplicity of infection of 5 and GRbl, GRbl+HSV-1, HSV-1 and control groups. MTT and cell apoptosis assays were used to detect the inhibitory effects of GRbl on the apoptosis of U251 cells that caused by HSV-1 infection for various concentrations of drug and virus treatments by MTT assay. We found that in the 400 μg/mL GRb 1 and 400 μg/mL GRbl+HSV-1 groups, MTT values were higher than control group at all times (P〈0.05). Moreover, the apoptosis rate in the 400 μg/mL GRbl+HSV-1 group was lower than the HSV-1 group (P〈0. 05). These results confirmed that, at appropriate concentrations, GRbl could inhibit nerve cell apoptosis in HSV-1 infections.
基金This work was supported by grants from Natural Science Foundation of Jiangsu Province (No.BK2004043)
文摘OBJECTIVE To explore the potential neurotrophic effect of bone marrow stromal cells (BMSCs) on cell proliferation and committed neuronal differentiation of ventral mesencephalic precursors (VMPs) in vitro. METHODS Ventral mesencephalic precursors from Ell inbred rat embryos and BMSCs from adult rats were cultured both separately and in co-culture. After a 7-day incubation in vitro, three conditioned culture media were obtained, termed VMP or common medium, BMSC medium, and BMSC±VMP medium. Ventral mesen- cephalic precursors cells were cultured in each of these media and the effects on proliferation and VMP differentiation were assessed. The relative yield of TH± cells was calculated and compared by immunocytochemical staining. RESULTS After a 7-day culture and induction of VMPs, the total cell counts were increased by (44.13±4.75)-fold (common), (60.63±5.25)-fold (BMSC), and (64.00±7.63)-fold (BMSC±VMP). The proportions of TH+ cells were (18.76±5.20)%, (23.49±4.10)%, and (28.08± 5.42)%, respectively, with statistically significant differences among the treatment groups. CONCLUSION BMSCs release factors that promote the proliferation of VMPs and facilitate the committed differentiation of VMPs into dopaminergic neurons.
