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Impact of exposure to low concentrations of nitric oxide on protein profile in murine and human pancreatic islet cells

机译:暴露于低浓度一氧化氮对鼠和人胰岛细胞蛋白质谱的影响

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摘要

Homeostatic levels of nitric oxide (NO) protect efficiently against apoptotic death in both human and rodent pancreatic beta cells, but the protein profile of this action remains to be determined. We have applied a 2 dimensional LC-MS-MALDI-TOF/TOF-based analysis to study the impact of protective NO in rat insulin-producing RINm5F cell line and in mouse and human pancreatic islets (HPI) exposed to serum deprivation condition. 24 proteins in RINm5F and 22 in HPI were identified to undergo changes in at least one experimental condition. These include stress response mitochondrial proteins (UQCRC2, VDAC1, ATP5C1, ATP5A1) in RINm5F cells and stress response endoplasmic reticulum proteins (HSPA5, PDIA6, VCP, GANAB) in HPI. In addition, metabolic and structural proteins, oxidoreductases and chaperones related with protein metabolism are also regulated by NO treatment. Network analysis of differentially expressed proteins shows their interaction in glucocorticoid receptor and NRF2-mediated oxidative stress response pathways and eNOS signaling. The results indicate that exposure to exogenous NO counteracts the impact of serum deprivation on pancreatic beta cell proteome. Species differences in the proteins involved are apparent.
机译:一氧化氮(NO)的体内稳态水平可有效防止人类和啮齿动物胰腺β细胞凋亡的死亡,但该作用的蛋白质谱仍有待确定。我们已应用基于二维LC-MS-MALDI-TOF / TOF的分析来研究保护性NO对大鼠胰岛素生产RINm5F细胞系以及暴露于血清剥夺条件的小鼠和人类胰岛(HPI)的影响。 RINm5F中的24种蛋白质和HPI中的22种蛋白质被确定在至少一种实验条件下发生了变化。这些包括RINm5F细胞中的应激反应线粒体蛋白(UQCRC2,VDAC1,ATP5C1,ATP5A1)和HPI中的应激反应内质网蛋白(HSPA5,PDIA6,VCP,GANAB)。另外,NO处理也调节与蛋白质代谢有关的代谢和结构蛋白,氧化还原酶和伴侣蛋白。差异表达蛋白质的网络分析显示了它们在糖皮质激素受体和NRF2介导的氧化应激反应途径以及eNOS信号传导中的相互作用。结果表明,暴露于外源NO抵消了血清剥夺对胰腺β细胞蛋白质组的影响。所涉及蛋白质的种类差异是显而易见的。

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