首页> 外文期刊>Journal of proteomics >Proteomic profiling of cellular responses to Carvedilol enantiomers in vascular smooth muscle cells by iTRAQ-coupled 2-D LC-MS/MS.
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Proteomic profiling of cellular responses to Carvedilol enantiomers in vascular smooth muscle cells by iTRAQ-coupled 2-D LC-MS/MS.

机译:通过iTRAQ耦合的二维LC-MS / MS,对血管平滑肌细胞中卡维地洛对映体的细胞反应进行蛋白质组学分析。

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摘要

Carvedilol is a third-generation beta-blocker, with the S-enantiomer being more active than the R-enantiomer. Clinically, it has been used in the treatment of hypertension, congestive heart failure and angina pectoris. Each enantiomer of Carvedilol exhibits differential pharmacological effects. However, the cellular effects of individual enantiomer are not well understood. To gain insights into how each enantiomer affects cells, we analysed differential protein expression levels in vascular smooth muscle cells (A7r5) incubated separately with S- and R-Carvedilol by iTRAQ-coupled 2-D LC-MS/MS approach. Thirteen proteins were identified with statistically significant changes in cells incubated with S-Carvedilol, while the changes of most proteins incubated with R-Carvedilol were less significant. Among these proteins, actin in aortic smooth muscle (ACTA2), calmodulin, S100-A6, S100-A10, S100-A11, thioredoxin, lactadherin and heat-shock protein 105 kDa were found to be closely relevant with the clinical effects of Carvedilol. Furthermore, the changes in protein levels were validated by Western blot. Our findings thus provided molecular evidence on a comprehensive protein profile on Carvedilol-cell interaction, which may shed new light in molecular events underlying Carvedilol treatment.
机译:卡维地洛是第三代β-受体阻滞剂,其中S-对映体比R-对映体更具活性。临床上,它已被用于治疗高血压,充血性心力衰竭和心绞痛。卡维地洛的每种对映异构体均显示出不同的药理作用。然而,单个对映异构体的细胞作用尚不十分清楚。为了深入了解每种对映异构体如何影响细胞,我们通过iTRAQ耦合2-D LC-MS / MS方法分析了分别与S-和R-卡维地洛孵育的血管平滑肌细胞(A7r5)中的差异蛋白表达水平。鉴定出13种蛋白质,与S-卡维地洛一起孵育的细胞具有统计学上的显着变化,而与R-卡维地洛一起孵育的大多数蛋白质的变化则不那么显着。在这些蛋白质中,发现主动脉平滑肌中的肌动蛋白(ACTA2),钙调蛋白,S100-A6,S100-A10,S100-A11,硫氧还蛋白,乳黏着蛋白和热激蛋白105 kDa与卡维地洛的临床疗效密切相关。此外,蛋白质水平的变化通过蛋白质印迹法得以证实。因此,我们的发现提供了有关卡维地洛与细胞相互作用的全面蛋白质谱的分子证据,这可能为卡维地洛治疗的分子事件提供了新的线索。

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