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Cytochrome b5 reductase and the control of lipid metabolism and healthspan

机译:细胞色素 b 5 还原酶与脂质代谢和健康期的控制

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Cytochrome b5 reductases (CYB5R) are required for the elongation and desaturation of fatty acids, cholesterol synthesis and mono-oxygenation of cytochrome P450 enzymes, all of which are associated with protection against metabolic disorders. However, the physiological role of CYB5R in the context of metabolism, healthspan and aging remains ill-defined. We generated CYB5R-overexpressing flies (CYB5R-OE) and created a transgenic mouse line overexpressing CYB5R3 (CYB5R3-Tg) in the C57BL/6J background to investigate the function of this class of enzymes as regulators of metabolism and age-associated pathologies. Gender- and/or stage-specific induction of CYB5R, and pharmacological activation of CYB5R with tetrahydroindenoindole extended fly lifespan. Increased expression of CYB5R3 was associated with significant improvements in several metabolic parameters that resulted in modest lifespan extension in mice. Diethylnitrosamine-induced liver carcinogenesis was reduced in CYB5R3-Tg mice. Accumulation of high levels of long-chain polyunsaturated fatty acids, improvement in mitochondrial function, decrease in oxidative damage and inhibition of chronic pro-inflammatory pathways occurred in the transgenic animals. These results indicate that CYB5R represents a new target in the study of genes that regulate lipid metabolism and healthspan.
机译:细胞色素b 5 还原酶(CYB5R)是脂肪酸的延伸和去饱和,胆固醇合成和细胞色素P450酶的单加氧反应所必需的,所有这些都与预防代谢紊乱有关。但是,CYB5R在代谢,健康期和衰老过程中的生理作用仍然不清楚。我们在C57BL / 6J背景中产生了CYB5R过表达的果蝇(CYB5R-OE),并创建了一个过表达CYB5R3(CYB5R3-Tg)的转基因小鼠品系,以研究此类酶作为代谢和与年龄相关的病理调节剂的功能。 CYB5R的性别和/或阶段特异性诱导,以及四氢茚并吲哚的CYB5R药理活化延长了果蝇的寿命。 CYB5R3表达的增加与一些代谢参数的显着改善有关,这些代谢参数导致小鼠的寿命延长适度。在CYB5R3-Tg小鼠中,二乙基亚硝胺诱导的肝癌发生减少。在转基因动物中积累了高水平的长链多不饱和脂肪酸,改善了线粒体功能,降低了氧化损伤,并抑制了慢性促炎途径。这些结果表明CYB5R代表了调控脂质代谢和健康跨度的基因研究的新目标。

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