Synergic Inhibition of Lung Carcinoma 95-D Cell Proliferation and Invasion by Combination with(—)-Epigallocatechin-3-Gallate and Ascorbic Acid

In this study, the anti-invasion effects of（-）-epigallocatechin-3-gallate（EGCG） mixed with ascorbic acid（Vc） on human lung carcinoma 95-D cells in vitro were examined and the synergism of the combination of EGCG and Vc was evaluated. Soft agar colony formation assay, cell migration assay, invasion assay, western blot analysis of NF-κB, in situ detection of cellular oxidative stress, and statistical analysis were assessed. The results showed that combining EGCG with Vc could inhibit clone forming rate of 95-D cell by 73.2%, reduce the migration ability of 95-D cell by 65.9%, and decrease the intracellular reactive oxygen species（ROS） level by 76.8%. The results of western blot proved that Vc enhanced the activity of EGCG in inhibiting NF-κB localization. It is speculated that the combination of EGCG and Vc can strongly suppress the proliferation and metastasis of lung carcinoma cells in a synergic manner, possibly with a mechanism associated with the scavenging of reactive oxygen species.

Separation of epigallocatechin-3-gallate from crude tea polyphenols by using Cellulose diacetate graft β-cyclodextrin copolymer asymmetric membrane

This study demonstrates a new Cellulose diacetate graft b-cyclodextrin(CDA-b-CD)copolymer asymmetric membrane prepared by a phase inversion technique for the separation of(–)-epigallocatechin-3-gallate(EGCG)from other polyphenols in crude tea.The graft copolymer,CDA-b-CD,was synthesized by pre-polymerization of cellulose diacetate(CDA)and 1,6-hexamethylene-diisocyanate(HDI),which was then grafted with b-cyclodextrin(b-CD).Surface and cross-section morphologies of the CDA-b-CD membranes were analyzed by using scanning electron microscopy(SEM).Fourier transform infrared spectroscopy(FT-IR)indicated that the b-CD was grafted onto the CDA by chemical bonding.The influences of the HDI/CDA mass ratio and the catalyst mass fraction on the b-CD graft yield were investigated.The optimum conditions of a HDI/CDA mass ratio of 0.35 g$g–1 and a catalyst mass fraction of 0.18 wt-%produced ab-CD graft yield of 26.51 wt-%.The effects of the b-CD graft yield and the concentration of the polymer cast solution on the separation of EGCG were also investigated.Under optimum conditions of a b-CD graft yield of 24.21 wt-%and a polymer concentration of 13 wt-%,the purity of EGCG increased from 26.51 to 86.91 wt-%.

Synergistic effects of tea polyphenols and ascorbic acid on human lung adenocarcinoma SPC-A-1 cells

Tea polyphenols have been shown to have anticancer activity in many studies.In the present study,we investigated effects of theaflavin-3-3'-digallate(TF3),one of the major theaflavin monomers in black tea,in combination with ascorbic acid(AA),a reducing agent,and(-)-epigallocatechin-3-gallate(EGCG),the main polyphenol presented in green tea,in combination with AA on cellular viability and cell cycles of the human lung adenocarcinoma SPC-A-1 cells.The 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyl tetrazolium bromide(MTT) assay showed that the 50% inhibition concentrations(IC50) of TF3,EGCG,and AA on SPC-A-1 cells were 4.78,4.90,and 30.62 μmol/L,respectively.The inhibitory rates of TF3 combined with AA(TF3+AA) and EGCG combined with AA(EGCG+AA) at a molar ratio of 1:6 on SPC-A-1 cells were 54.4% and 45.5%,respectively.Flow cytometry analysis showed that TF3+AA and EGCG+AA obviously increased the cell population in the G0/G1 phase of the SPC-A-1 cell cycle from 53.9% to 62.8% and 60.0%,respectively.TF3-treated cells exhibited 65.3% of the G0/G1 phase at the concentration of its IC50.Therefore,TF3+AA and EGCG+AA had synergistic inhibition effects on the proliferation of SPC-A-1 cells,and significantly held SPC-A-1 cells in G0/G1 phase.The results suggest that the combination of TF3 with AA or EGCG with AA enhances their anticancer activity.