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首页> 外文期刊>Toxicology and Applied Pharmacology >Long-term mildronate treatment increased Proteobacteria level in gut microbiome, and caused behavioral deviations and transcriptome change in liver, heart and brain of healthy mice
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Long-term mildronate treatment increased Proteobacteria level in gut microbiome, and caused behavioral deviations and transcriptome change in liver, heart and brain of healthy mice

机译:长期季霉素治疗在肠道微生物组中增加植物细菌水平,并导致健康小鼠肝脏,心脏和脑中的行为偏差和转录组变化

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摘要

Mildronate is a cardiac and neuroprotective drug that is widely used in some countries. By inhibiting carnitine biosynthesis, mildronate impairs the fatty acids transport into mitochondria, thereby decreasing the beta-oxidation intensity. Since 2016, it has been prohibited by the World Anti-Doping Agency (WADA). However, the information on its safety and its influence on the athletes' health is scarce. There are no published studies on whether mildronate-induced long-term metabolism "rearrangement" may cause negative effects on high-metabolic-rate organs and on the whole organism. Here, we demonstrate that long-term mildronate treatment of healthy mice induced global metabolism change at the transcriptome level in liver, heart, and brain. Mildronate treatment also induced some behavioral changes such as anxiety-related behavior and diminished explorative behavior. We also found that mildronate induced a dysbiosis, as manifested by an increase in Proteobacteria level in gut microbiome. At the same time, the absence of a statistically significant increase in mouse strength and endurance procedures suggests that mildronate effect on productivity is negligible. The sum of our data suggests that long-term treatment of healthy mice with mildronate induces dysbiosis and behavioral deviations despite the effectiveness of mildronate for cardiac and neurological diseases. Thus, we suggest that long-term mildronate treatment is undesirable or at the very least should be accompanied by prebiotics treatments, but this issue should be studied further.
机译:偏态酸盐是一种心脏和神经保护药,广泛应用于一些国家。通过抑制肉碱生物合成,水仑酸盐将脂肪酸输送到线粒体中,从而降低β-氧化强度。自2016年以来,世界反兴奋剂机构(WADA)禁止。但是,关于其安全及其对运动员健康的影响的信息是稀缺的。没有发表的研究,有关水平诱导的长期新陈代谢“重排”可对高代谢速率器官和整个生物体产生负面影响。在这里,我们证明了对肝脏,心脏和大脑的转录组水平诱导健康小鼠的长期淡季酸盐治疗诱导全球代谢变化。偏碳酸盐处理还诱导了一些行为变化,如焦虑相关的行为和减少的探索性行为。我们还发现,季霉素诱导困难,如肠道微生物组中的植物细菌水平的增加表现出。同时,缺乏小鼠强度和耐久性程序的统计上显着提高表明,对生产率的效果不足,可以忽略不计。我们的数据的总和表明,尽管心脏和神经疾病的季酸盐恒定的有效性,但仍然诱导困难和行为偏差的长期治疗。因此,我们建议长期季戊烷处理是不希望的或至少应伴有益生元治疗,但应进一步研究这个问题。

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