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首页> 外文期刊>Journal of Hepatology: The Journal of the European Association for the Study of the Liver >Methyl donor deficiency impairs fatty acid oxidation through PGC-1α hypomethylation and decreased ER-α, ERR-α, and HNF-4α in the rat liver
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Methyl donor deficiency impairs fatty acid oxidation through PGC-1α hypomethylation and decreased ER-α, ERR-α, and HNF-4α in the rat liver

机译:甲基供体不足会通过PGC-1α甲基化不足而损害脂肪酸氧化,并降低大鼠肝脏中的ER-α,ERR-α和HNF-4α

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Background & Aims: Folate and cobalamin are methyl donors needed for the synthesis of methionine, which is the precursor of S-adenosylmethionine, the substrate of methylation in epigenetic, and epigenomic pathways. Methyl donor deficiency produces liver steatosis and predisposes to metabolic syndrome. Whether impaired fatty acid oxidation contributes to this steatosis remains unknown. Methods: We evaluated the consequences of methyl donor deficient diet in liver of pups from dams subjected to deficiency during gestation and lactation. Results: The deprived rats had microvesicular steatosis, with increased triglycerides, decreased methionine synthase activity, S-adenosylmethionine, and S-adenosylmethionine/S-adenosylhomocysteine ratio. We observed no change in apoptosis markers, oxidant and reticulum stresses, and carnityl-palmitoyl transferase 1 activity, and a decreased expression of SREBP-1c. Impaired beta-oxidation of fatty acids and carnitine deficit were the predominant changes, with decreased free and total carnitines, increased C14:1/C16 acylcarnitine ratio, decrease of oxidation rate of palmitoyl-CoA and palmitoyl-l-carnitine and decrease of expression of novel organic cation transporter 1, acylCoA-dehydrogenase and trifunctional enzyme subunit alpha and decreased activity of complexes I and II. These changes were related to lower protein expression of ER-α, ERR-α and HNF-4α, and hypomethylation of PGC-1α co-activator that reduced its binding with PPAR-α, ERR-α, and HNF-4α. Conclusions: The liver steatosis resulted predominantly from hypomethylation of PGC1-α, decreased binding with its partners and subsequent impaired mitochondrial fatty acid oxidation. This link between methyl donor deficiency and epigenomic deregulations of energy metabolism opens new insights into the pathogenesis of fatty liver disease, in particular, in relation to the fetal programming hypothesis.
机译:背景与目的:叶酸和钴胺素是甲硫氨酸合成所需的甲基供体,甲硫氨酸是S-腺苷甲硫氨酸的前体,是表观遗传途径和表观基因组途径中甲基化的底物。甲基供体缺乏会导致肝脏脂肪变性,并易患代谢综合征。脂肪酸氧化受损是否会导致脂肪变性尚不清楚。方法:我们评估了在妊娠和哺乳期间营养不良的水坝幼崽肝脏中甲基供体缺乏饮食的后果。结果:剥夺的大鼠微囊脂肪变性,甘油三酸酯增加,蛋氨酸合酶活性降低,S-腺苷甲硫氨酸和S-腺苷甲硫氨酸/ S-腺苷同型半胱氨酸比。我们没有观察到细胞凋亡标志物,氧化和网状应激,肉碱基-棕榈酰转移酶1活性和SREBP-1c的表达减少的变化。脂肪酸的β-氧化受损和肉碱缺乏是主要变化,游离和总肉碱减少,C14:1 / C16酰基肉碱比例增加,棕榈酰-CoA和棕榈酰-1-肉碱的氧化率降低,且其表达降低。新型有机阳离子转运蛋白1,酰基辅酶A脱氢酶和三功能酶亚基α和复合物I和II活性降低。这些变化与ER-α,ERR-α和HNF-4α的蛋白表达降低以及PGC-1α共激活剂的低甲基化降低了其与PPAR-α,ERR-α和HNF-4α的结合有关。结论:肝脂肪变性主要是由于PGC1-α的甲基化不足,与其伴侣的结合减少以及随后的线粒体脂肪酸氧化受损所致。甲基供体缺乏与能量代谢的表观基因组失调之间的这种联系为脂肪肝疾病的发病机理提供了新的见识,尤其是与胎儿编程假说相关的观点。

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