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首页> 外文期刊>Journal of proteomics >Proteomics and gene expression analyses of squalene-supplemented mice identify microsomal thioredoxin domain-containing protein 5 changes associated with hepatic steatosis.
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Proteomics and gene expression analyses of squalene-supplemented mice identify microsomal thioredoxin domain-containing protein 5 changes associated with hepatic steatosis.

机译:补充角鲨烯的小鼠的蛋白质组学和基因表达分析确定了与肝脂肪变性相关的含微粒体硫氧还蛋白域的蛋白质5变化。

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摘要

Squalene is an abundant hydrocarbon present in virgin olive oil. Previous studies showed that its administration decreased atherosclerosis and steatosis in male apoE-knock-out mice. To study its effects on microsomal proteins, 1g/kg/day of squalene was administered to those mice. After 10 weeks, hepatic fat content was assessed and protein extracts of microsomal enriched fractions from control and squalene-treated animals were analyzed by 2D-DIGE. Spots exhibiting significant differences were identified by peptide fingerprinting and MSMS analysis. Squalene administration modified the expression of thirty-one proteins involved in different metabolic functions and increased the levels of those involved in vesicle transport, protein folding and redox status. Only mRNA levels of 9 genes (Arg1, Atp5b, Cat, Hyou1, Nipsnap1, Pcca, Pcx, Pyroxd2, and Txndc5) paralleled these findings. No such mRNA changes were observed in wild-type mice receiving squalene. Thioredoxin domain-containing protein 5 (TXNDC5) protein and mRNA levels were significantly associated with hepatic fat content in apoE-ko mice. These results suggest that squalene action may be executed through a complex regulation of microsomal proteins, both at the mRNA and post-transcriptional levels and the presence of apoE may change the outcome. Txndc5 reflects the anti-steatotic properties of squalene and the sensitivity to lipid accumulation.
机译:角鲨烯是原始橄榄油中存在的丰富烃。先前的研究表明,在雄性apoE基因敲除小鼠中,其给药可减少动脉粥样硬化和脂肪变性。为了研究其对微粒体蛋白的作用,向这些小鼠施用1g / kg /天的角鲨烯。 10周后,评估肝脏脂肪含量,并通过2D-DIGE分析来自对照和角鲨烯处理的动物的微粒体富集级分的蛋白质提取物。通过肽指纹图谱和MSMS分析鉴定出表现出显着差异的斑点。角鲨烯的施用修饰了三十一种参与不同代谢功能的蛋白质的表达,并增加了参与囊泡转运,蛋白质折叠和氧化还原状态的蛋白质的水平。只有9个基因(Arg1,Atp5b,Cat,Hyou1,Nipsnap1,Pcca,Pcx,Pyroxd2和Txndc5)的mRNA水平与这些发现平行。在接受角鲨烯的野生型小鼠中未观察到此类mRNA变化。载有硫氧还蛋白域的蛋白5(TXNDC5)蛋白和mRNA水平与apoE-ko小鼠的肝脂肪含量显着相关。这些结果表明,角鲨烯作用可以通过在mRNA和转录后水平上对微粒体蛋白的复杂调节来执行,并且载脂蛋白E的存在可能改变结果。 Txndc5反映了角鲨烯的抗硬脂特性和对脂质积累的敏感性。

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