低氧诱导因子1α对成肌分化中PGC-1β的影响及机制研究  被引量:1

Effects of hypoxia-inducible factor 1α on PGC-1β in myogenesis and the relevant mechanism

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作  者:卢芸[1] 刘月华 

机构地区:[1]同济大学口腔医学院正畸教研室.口腔生物医学及转化医学实验室,上海200072 [2]上海市口腔医院,上海200001

出  处:《临床口腔医学杂志》2015年第8期451-455,共5页Journal of Clinical Stomatology

基  金:国家自然科学基金项目(81271192)

摘  要:目的:研究低氧诱导因子HIF-1α在颏舌肌成肌分化和线粒体生物发生中的作用,探索可能的调控机制。方法:构建HIF-1α敲降质粒,慢病毒载体转染小鼠颏舌肌成肌细胞,设阴性对照组,用含2%马血清的分化培养基在低氧(1%O2)环境下诱导成肌细胞分化,western blot检测成肌细胞分化2、4、6 d,PGC-1β、AMPKα1、p AMPKα1的表达水平,免疫细胞化学染色观察低氧分化4 d时AMPK通道激活剂与阻滞剂对PGC-1β的表达影响,western blot定量分析。结果:1 HIF-1α敲降组的PGC-1β表达量高于对照组(P<0.05),且分化4 d时表达最高(P<0.05);2AMPKα1总蛋白表达量无明显差异,p AMPKα1的表达在HIF-1α敲降组远高于对照组(P<0.05)。3AMPK通路促进剂AICAR增加PGC-1β的表达(P<0.05),抑制剂Compound C明显抑制PGC-1β的表达(P<0.05)。结论:HIF-1α下调了低氧环境中PGC-1β的表达,PGC-1β的表达受AMPK通路的正向调节作用。Objective:To investigate the effects of HIF-1α on myogenic differentiation and mitochondrial biogenesis and the mechanism involved. Method:HIF-1α shRNA lentivirous was used to infect the myoblasts. Myoblasts was induced differentiation by 2%horse serum in hypoxia condition(1%O2) for 6 days,PGC-1β,AMPKα1 and pAMPKα1 were detect-ed through western-blot. Immunocytochemistry and western-blot were performed to detected the expression of PGC-1β after medication of AICAR or Compound C. Result: ①Compared with control myoblasts,the expression of PGC-1βwas higher in HIF-1α KO myoblasts during myogenesis (P 〈0.05),and highest in the fourth day. ②There is no significant differences in AMPKα1 (P 〉0.05). The expression of pAMPKα1 was significantly higher under hypoxia condition in HIF-1α KO group, compared with the control groups(P 〈0.05).③AICAR(activator of AMPK) increaed the expression of PGC-1β(P 〈0.05), while Compound C (inhibitor of AMPK) showed opposite effect (P〈0.05). Conclusion:HIF-1αdecreases the expression of PGC-1βunder hypoxia condition. The expression of PGC-1β is influenced by AMPK,which acts as a positively acting com-ponent.

关 键 词:低氧 低氧诱导因子1Α 过氧化物酶体增殖物激活受体γ协同刺激因子1β:AMP依赖的蛋白激酶 

分 类 号:Q786[生物学—分子生物学]

 

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