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牛磺酸增强分化的C2C12肌管中铁相关蛋白的表达并减少脂质过氧化。

Taurine Enhances Iron-Related Proteins and Reduces Lipid Peroxidation in Differentiated C2C12 Myotubes.

作者信息

Seidel Ulrike, Lüersen Kai, Huebbe Patricia, Rimbach Gerald

机构信息

Institute of Human Nutrition and Food Science, University of Kiel, 24118 Kiel, Germany.

出版信息

Antioxidants (Basel). 2020 Oct 31;9(11):1071. doi: 10.3390/antiox9111071.

Abstract

Taurine is a nonproteinogenic amino sulfonic acid in mammals. Interestingly, skeletal muscle is unable to synthesize taurine endogenously, and the processing of muscular taurine changes throughout ageing and under specific pathophysiological conditions, such as muscular dystrophy. Ageing and disease are also associated with altered iron metabolism, especially when there is an excess of labile iron. The present study addresses the question of whether taurine connects cytoprotective effects and redox homeostasis in a previously unknown iron-dependent manner. Using cultured differentiated C2C12 myotubes, the impact of taurine on markers of lipid peroxidation, redox-sensitive enzymes and iron-related proteins was studied. Significant increases in the heme protein myoglobin and the iron storage protein ferritin were observed in response to taurine treatment. Taurine supplementation reduced lipid peroxidation and BODIPY oxidation by ~60 and 25%, respectively. Furthermore, the mRNA levels of redox-sensitive heme oxygenase the total cellular glutathione content were lower in taurine-supplemented cells than they were in the control cells. We suggest that taurine may inhibit the initiation and propagation of lipid peroxidation by lowering basal levels of cellular stress, perhaps through reduction of the cellular labile iron pool.

摘要

牛磺酸是哺乳动物体内一种非蛋白质ogenic氨基酸磺酸。有趣的是,骨骼肌无法内源性合成牛磺酸,并且肌肉中牛磺酸的代谢在整个衰老过程以及特定病理生理条件下(如肌肉萎缩症)会发生变化。衰老和疾病还与铁代谢改变有关,尤其是在存在过量不稳定铁的情况下。本研究探讨了牛磺酸是否以前所未知的铁依赖性方式将细胞保护作用与氧化还原稳态联系起来的问题。使用培养的分化C2C12肌管,研究了牛磺酸对脂质过氧化标志物、氧化还原敏感酶和铁相关蛋白的影响。观察到,牛磺酸处理后,血红素蛋白肌红蛋白和铁储存蛋白铁蛋白显著增加。补充牛磺酸分别使脂质过氧化和BODIPY氧化降低了约60%和25%。此外,补充牛磺酸的细胞中氧化还原敏感的血红素加氧酶的mRNA水平和细胞总谷胱甘肽含量低于对照细胞。我们认为,牛磺酸可能通过降低细胞应激的基础水平来抑制脂质过氧化的起始和传播,这可能是通过减少细胞不稳定铁池来实现的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4dc3/7693586/0ab0987523b9/antioxidants-09-01071-sch001.jpg

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