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Anti-esophagus cancer activity and mechanism of DN3,a novel natural diterpenoid derivative,as a dual inhibitor of glycolysis and oxidative phosphorylation
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作者 Yong-cheng MA Ying-li ZHU +4 位作者 Xia-xia FAN Ao JIA Ya-fei LI Bei-bei SHAO ai-feng wang 《中国药理学与毒理学杂志》 CAS CSCD 北大核心 2018年第4期297-297,共1页
OBJECTIVE To probe into the anti-esophagus cancer activity and mechanisms of DN3,a novel natural diterpenoid derivative.METHODS The anti-tumor activity in vitro of DN3 was evaluated by MTT,and by using human esophagea... OBJECTIVE To probe into the anti-esophagus cancer activity and mechanisms of DN3,a novel natural diterpenoid derivative.METHODS The anti-tumor activity in vitro of DN3 was evaluated by MTT,and by using human esophageal carcinoma cells xenografted into athymic mice model in vivo.The specific mechanisms of DN3,as a dual inhibitor of glycolysis and oxidative phos.phorylation(OXPHOS) were explored through cell and molecular biology techniques.For instance,the manner of cancer cell death induced by DN3 was characterized by hoechst33342,FITC-Annexin V/PI staining and flow cytometric analysis,then these changes of glucose consumption,glucose uptake and lactate production in glycolysis,as well as oxygen consumption rate(OCR) and ATP content in OXPHOS caused by DN3 were performed separately through related kits and SeahorseBioscience XF24 Extra.cellular Flux Analyzer.Furthermore,in order to obtain a clear understanding of the inhibition of DN3 to glycolysis and OXPHOS,these regulatory factors were investigated by Western blot,such as PI3K/AKT,c-Myc and p53 of glycolysis,Bax and HK2 of mitochondrial function.RESULTS DN3 inhibited the growth of esophagus cancer cell EC9706,EC109 and EC1 cells in a dose and time dependent manner,but showed no significant effects on human esophageal epithelial cells(HEECs).DN3 caused significant G2/M arrest of esophagus cancer cell lines and induced apoptosis of these cell lines,which indicated DN3 inhibited the growth of esophagus cancer cell through blocking cell cycle and inducing apoptosis in a dose and time-dependent manner.Importantly,8 μM DN3 decreased the extracellular acidification rate(ECAR) by 45% in EC109,which indicated glycolysis was inhibited by DN3.Mean.while,DN3 decreased the oxygen consumption rate(OCR) and the OCR linked to intracellular ATP production in EC109 cells,but that was not obvious in HEECs,so which indicated that DN3 could selec.tively block OXPHOS of cancer cells.In addition,the accumulation of reactive oxygen species(ROS)and the drop of mitochondrial membrane potential(MMP) were also observed in EC109 incubated by DN3,which suggested mitochondrial biological function was disturbed.Furthermore,the expression of PI3K/AKT,c-Myc and HK2 related to glycolysis were down-regulated by DN3,but the p53 and Bax were up-regulated in esophageal carcinoma cells.The changes of these enzymes accounted for the decreased glycolysisand OXPHOS in esophageal carcinoma cells treated by DN3.CONCLUSION The new compound DN3 has a strong anti-esophageal carcinoma activity,and it is tolerable that DN3 is seen as a dual inhibitor of glycolysis and oxidative phosphorylation. 展开更多
关键词 天然二萜衍生物 食管癌 治疗方法 临床分析
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Antitumor activityand mechanism of JD20,a newly synthetic analog of natural ent-kaurane diterpenoid
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作者 Ying-li ZHU Xia-xia FAN +4 位作者 Ya-fei LI Ao JIA Bei-bei SHAO ai-feng wang Yong-cheng MA 《中国药理学与毒理学杂志》 CAS CSCD 北大核心 2018年第4期346-346,共1页
OBJECTIVE To study the anti-tumor activity and molecular mechanism of natural diter.pene derivative JD20 in vitro.METHODS Screening the sensitive of gastric carcinoma cell lines to JD20 by cytotoxicity test for 24 h.C... OBJECTIVE To study the anti-tumor activity and molecular mechanism of natural diter.pene derivative JD20 in vitro.METHODS Screening the sensitive of gastric carcinoma cell lines to JD20 by cytotoxicity test for 24 h.Cell morphology was evaluated by using DAPI.After staining of can.cer cells with PI or annexin V-FITC/PI respectively,the cell cycle and apoptosis induced by JD20 were detectded by flow cytometry.The change in cell membrane potential was detected by JC-1 test kit.Western blot method was used to detect the apoptosis-related protein.RESULTS The novel natural kaurane diterpene derivative JD20 had a significant inhibitory effect on tumor cells and was particularly active on gastric cancer cell lines HGC-27(IC50=4.72±1.37 μmol·L-1) and MGC-803(IC50=7.36±0.86 μmol·L^(-1)).Further studies found that JD20 resulted in thecell cycle arrest in the G2/M phase,and induced a significant apoptosis in HGC-27.In addition,JD20 also caused the drop of mitochondrial membrane potential of HGC-27 within a short time(3 h).Furthermore,the Western blotting analysis showed that JD20 could induce the up-regulation of p53,Bax and Bim protein expression in gastric can.cer cells,and the releasing of cytochrome c from the mitochondria into the cytoplasm,as well as the ac.tivation of casepase-9/3.CONCLUSION The natural kaurane diterpene derivative JD20 can inhibit the proliferation of various human cancer cells by blocking the cell cycle and inducing apoptosis,and its mechanism of inducing apoptosis may be related to the mitochondria-mediated apoptosis pathway. 展开更多
关键词 细胞色素 线粒体 治疗方法 临床分析
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Metabolic heterogeneity of gastric cancer cell lines
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作者 Xia-xia FAN Ying-li ZHU +5 位作者 Bei-bei SHAO Lu-lu LI Ya-fei LI Ao JIA ai-feng wang Yong-cheng MA 《中国药理学与毒理学杂志》 CAS CSCD 北大核心 2018年第4期278-279,共2页
OBJECTIVE Gastric cancer is one of the most common malignant tumors,and the incidence rate is the highest in all kinds of tumors in China.However,it remains unclear that how signifi.cantly gastric cells are dependent ... OBJECTIVE Gastric cancer is one of the most common malignant tumors,and the incidence rate is the highest in all kinds of tumors in China.However,it remains unclear that how signifi.cantly gastric cells are dependent on glycolysis,and which type of gastric cells are sensitive to glycolysis inhibition.In this study,several kind of gastric cancer cell lines were used as the research object,and the metabolic characteristics of different cell lines were systematically analyzed to provide theoretical support for the accurate treatment of gastric cancer.METHODS We examined the energy metabolism of four gastric cancer cell lines(MGC-803,SGC-7901,HGC-27 and BGC-823) by using glycolysis inhibitor,2-deoxy-D-glucose(2-DG) and inhibitor of oxidative phosphorylation,oligomycin.Oxygen consumption rates(OCR) and L-lactate were also measured with an XF96 Analyzer(Seahorse Biosciences) to deter.mine the significance of metabolism of oxidative phosphorylation and aerobic glycolysisin gastric cells.In addition,western blot was used to detect the contribution of AMP-activated protein kinase(AMPK),and anti-apoptotic proteins(Bcl-2 and survivin) to clarify the mechanism of death or survival of gastric cancer cells treated by 2-DG or oligomycin.RESULTS In this study,it was shown that the growth of gastric cell lines were suppressed by 2-DG.However,the sensitivity to 2-DG was quite different among cell lines:IC 50 of 2-DG was from 3.28 mmol·L^(-1)(MGC-803) to 15.57 mmol·L^(-1)(BGC-823).MGC-803 was relatively sensitive to 2-DG(IC 50:3.28 mmol·L^(-1)),consumed more glucose and produced more lactate(waste product of glycolysis) than the three other cell lines.Consequently,MGC-803 could be more dependent on glycolysis than other cell lines,which was further confirmed by the fact that glucose(+) FCS(-) medium showed more growth and survival than glucose(-) FCS(+) medium.Alternatively,BGC-823,most resistant to 2-DG(IC50:15.57 mmol · L-1),was most sensitive to oligomycin,and showed more growth and survival in glucose(-) FCS(+) medium than in glucose(+) FCS(-) medium.Thus,we had reasons to think BGC-823 cells depended on oxidative phosphorylation for energy production.In BGC-823,AMPK,which is activated when ATP becomes limiting,was rapidly phosphorylated by 2-DG,and expression of Bcl-2 was augmented,which might result in resistance to 2-DG.Interestingly,AMPK phosphorylation and augmentation of Bcl-2 expression by 2-DG were not observed in MGC-803,which is 2-DG sensitive.CONCLUSION There is a large metabolic difference between gastric cancer cell lines,which will facilitate the future gastric cancer therapy by targeting metabolic pathways. 展开更多
关键词 胃癌 恶性肿瘤 治疗方法 临床分析
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Electrical and thermal transport properties of kagome metals AV3Sb5(A=K,Rb,Cs) 被引量:1
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作者 Xin-Run Mi Kun-Ya Yang +5 位作者 Yu-Han Gan Long Zhang ai-feng wang Yi-Sheng Chai Xiao-Yuan Zhou Ming-Quan He 《Tungsten》 EI CSCD 2023年第3期300-316,共17页
The interplay between lattice geometry,band topology and electronic correlations in the newly discovered kagome compounds AV3Sb5(A=K,Rb,Cs) makes this family a novel playground to investigate emergent quantum phenomen... The interplay between lattice geometry,band topology and electronic correlations in the newly discovered kagome compounds AV3Sb5(A=K,Rb,Cs) makes this family a novel playground to investigate emergent quantum phenomena,such as unconventional superconductivity,chiral charge density wave and electronic nematicity.These exotic quantum phases naturally leave nontrivial fingerprints in transport properties of AV3Sb5,both in electrical and thermal channels,which are prominent probes to uncover the underlying mechanisms.In this brief review,we highlight the unusual electrical and thermal transport properties observed in the unconventional charge ordered state of A V3Sb5,including giant anomalous Hall,anomalous Nernst,ambipolar Nernst and anomalous thermal Hall effects.Connections of these anomalous transport properties to time-reversal symmetry breaking,topological and multiband fermiology,as well as electronic nematicity,are also discussed.Finally,a perspective together with challenges of this rapid growing field are given. 展开更多
关键词 Kagome superconductors Charge density wave Anomalous Hall effect Anomalous Nernst effect Ambipolar Nernst Effect Anomalous thermal Hall effect
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The Impulsive Solution for a Semi-linear Singularly Perturbed Differential-difference Equation 被引量:1
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作者 ai-feng wang Mei XU Ming-kang NI 《Acta Mathematicae Applicatae Sinica》 SCIE CSCD 2016年第2期333-342,共10页
The impulsive solution for a semi-linear singularly perturbed differential-difference equation is studied. Using the methods of boundary function and fractional steps, we construct the formula asymptotic expansion of ... The impulsive solution for a semi-linear singularly perturbed differential-difference equation is studied. Using the methods of boundary function and fractional steps, we construct the formula asymptotic expansion of the problem. At the same time, Based on sewing techniques, the existence of the smooth impulsive solution and the uniform validity of the asymptotic expansion are proved. 展开更多
关键词 singularly perturbed differential-difference equation delay argument asymptotic expansion im-pulsive solution boundary function
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