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首页> 外文期刊>The Journals of Gerontology Series A: Biological Sciences and Medical Sciences >Alterations in Oxygen Consumption, Respiratory Quotient, and Heat Production in Long-Lived GHRKO and Ames Dwarf Mice, and Short-Lived bGH Transgenic Mice
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Alterations in Oxygen Consumption, Respiratory Quotient, and Heat Production in Long-Lived GHRKO and Ames Dwarf Mice, and Short-Lived bGH Transgenic Mice

机译:长寿命GHRKO和Ames矮小鼠和短寿命bGH转基因小鼠的耗氧量,呼吸商和产热量的变化

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摘要

Growth hormone (GH) signaling influences longevity in mice, with decreased GH signaling associated with longer life span and increased GH signaling with shortened life span. A proposed mechanism through which GH signaling influences life span postulates that decreased GH signaling lowers metabolic rate, thus slowing aging by decreasing production of damaging free radicals. The influence of altered GH signaling on metabolism was tested by monitoring oxygen consumption (VO2), respiratory quotient (RQ), and heat production in long-lived GH receptor knockout (GHRKO) and Ames dwarf mice, and short-lived bovine GH-overexpressing transgenic (bGH TG) mice. Intriguingly, both GHRKO and Ames dwarf mice have increased VO2 and heat per gram body weight, and decreased RQ, whereas bGH TG mice have decreased VO2 and heat per gram body weight and increased RQ. In conclusion, decreased GH signaling associates with increased metabolism per body weight and may beneficially affect mitochondrial flexibility by increasing the capacity for fat oxidation; generally, GH excess produces opposite metabolic effects.
机译:生长激素(GH)信号会影响小鼠的寿命,GH信号的降低与寿命的延长相关,而GH信号的增加则寿命的缩短。 GH信号转导影响寿命的拟议机制假定降低的GH信号转导降低了代谢速率,从而通过减少有害自由基的产生而减缓了衰老。通过监测长寿GH受体敲除(GHRKO)和Ames矮小鼠的耗氧量(VO 2 ),呼吸商(RQ)和产热量来测试GH信号改变对代谢的影响,和短寿命的牛GH高表达转基因(bGH TG)小鼠。有趣的是,GHRKO和Ames矮小鼠均具有每克体重VO 2 和热量增加,RQ降低,而bGH TG小鼠均具有每克体重VO 2 和热量减少重量和增加的RQ。总之,减少的GH信号传导与每单位体重的新陈代谢增加有关,并可能通过增加脂肪氧化能力而有益地影响线粒体的柔韧性。通常,过量的GH产生相反的代谢作用。

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