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刘竟成

作品数:5 被引量:6H指数:1
供职机构:北京大学化学与分子工程学院化学生物学系更多>>
发文基金:国家自然科学基金更多>>
相关领域:医药卫生生物学理学更多>>

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ROS在钒化合物抗脂解和激活糖代谢信号通路中的作用
于游刘竟成杨晓改王夔
关键词:钒化合物脂解糖代谢
从钒化合物生物效应的多样性看其作用机制被引量:5
2009年
本文对近年来关于钒化合物不同生物效应机制的研究进展进行了总结,着重于其类胰岛素和抗癌效应的信号转导机制以及两者之间的相关性。同时,基于钒化合物对磷酸转移反应的干预以及对细胞氧化还原状态的调节,讨论了钒化合物多样化的生物效应是否具有一个共同作用机制的可能性,并提出了未来钒化合物研究方向和所面临的挑战。
杨晓改王琴刘竟成王夔
关键词:抗癌钒化合物
Role of vanadyl acetylacetonate-induced elevation of reactive oxygen species in the regulation of lipolysis and glucose metabolism in 3T3L1 adipocytes
2015年
In the present study, we investigated the role of reactive oxygen species(ROS) elevation induced by an anti-diabetic vanadium compound, vanadyl acetylacetonate(VO(acac)2), in the regulation of lipolysis and glucose metabolism using differentiated 3T3L1 adipocytes as a model system. By confocal laser scanning microscopy, we found that VO(acac)2 induced ROS generation under high glucose stimulation, and the pretreatment of NADPH oxidase inhibitors could significantly reduce the elevated ROS level. Meanwhile, the decreased phosphorylated levels of AKT and the two key modulators of lipolysis(HSL and perilipin) were observed by western blot analysis. We also found that the contents of glycerol release were further reduced as well. In addition, the levels of key regulatory proteins, AS160 and GSK3β, in glucose metabolism pathway were correspondingly reduced. These findings demonstrated that ROS induced by vanadium compounds could act as a metabolic signal to activate AKT pathway to inhibit lipolysis and promote glucose transport and glycogen synthesis rather than by direct action by themselves. Our study contributed to elucidate the anti-diabetic effects of vanadium compounds and provided a theoretical basis for the further development of new vanadium complexes in the prevention and therapeutics of diabetes.
李逸刘竟成于游卞卫霞胡霞杨晓改
关键词:LIPOLYSIS
Bis(acetylacetonato)-oxidovanadium(Ⅳ) inhibits isoproterenol-induced lipolysis in insulin-resistant 3T3-L1 adipocytes by reducing phosphorylation of perilipin and hormone-sensitive lipase被引量:1
2016年
Insulin resistance is characterized as one of crucial pathological changes in type 2 diabetes mellitus(T2DM), and dyslipidaemia is frequently detected in T2DM. A variety of vanadium compounds have been studied as drug candidates for diabetes based on their insulin-like action. However, few studies focus on their antilipolytic effect. In the present study, we established an insulin-resistant model in 3T3-L1 adipocytes to mimic pathological conditions of T2DM according to a well-established method by the treatment of high concentrations of glucose and insulin, which was validated by oil red O staining and the decreased levels of phosphorylated Akt, AS160 and GSK3 after insulin treatment. The results demonstrated that bis(acetylacetonato)-oxidovanadium(Ⅳ)(VO(acac)_2) could inhibit isoproterenol-stimulated lipolysis through the reduction of the phosphorylated HSL and perilipin levels in both insulin-sensitive and insulin-resistant 3T3-L1 adipocytes. Moreover, although the levels of phosphorylated Akt induced by VO(acac)_2 were decreased, the rates of lipolytic inhibition were not significantly altered compared with those under insulin-sensitive condition, indicating that the anti-lipolytic effect of VO(acac)_2 might also function in an Akt-independent way in insulin-resistant adipocytes. Our work here help elucidate the anti-diabetic effects of vanadium compounds. It may not only shed light on the utility of vanadium-based compounds as potential anti-diabetic drugs but also serve as a useful screening model for new anti-diabetic drugs.
胡霞刘竟成于游卞卫霞杨晓改
关键词:LIPOLYSIS
难溶性稀土物种引起生物学效应的机制
由于稀土的物理和化学性质异于其它重金属物种,在对其进行毒理学评价实,应注重对其作用方式、靶器官以及敏感生物标志物的确定。实际上,目前对于稀土引起的生物效应的机理的了解仍是欠缺的,主要原因在于稀土特殊的化学性质以及形成难溶...
杨晓改马孝杰范云周刘会雪黄慧霞付丽娟刘竟成冯敏
关键词:毒性效应分子机制
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