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长链酰基辅酶 A 是否负责冬眠 13 线地松鼠中线粒体代谢的抑制?

Are long chain acyl CoAs responsible for suppression of mitochondrial metabolism in hibernating 13-lined ground squirrels?

机构信息

Department of Biology, University of Western Ontario, London, ON N6A5B8, Canada.

Department of Biology, University of Western Ontario, London, ON N6A5B8, Canada.

出版信息

Comp Biochem Physiol B Biochem Mol Biol. 2014 Apr;170:50-7. doi: 10.1016/j.cbpb.2014.02.002. Epub 2014 Feb 20.

Abstract

Hibernation in 13-lined ground squirrels (Ictidomys tridecemlineatus) is associated with a substantial suppression of whole-animal metabolism. We compared the metabolism of liver mitochondria isolated from torpid ground squirrels with those from interbout euthermic (IBE; recently aroused from torpor) and summer euthermic conspecifics. Succinate-fuelled state 3 respiration, calculated relative to mitochondrial protein, was suppressed in torpor by 48% and 44% compared with IBE and summer, respectively. This suppression remains when respiration is expressed relative to cytochrome c oxidase activity. We hypothesized that this suppression was caused by inhibition of succinate transport at the dicarboxylate transporter (DCT) by long-chain fatty acyl CoAs that may accumulate during torpor. We predicted, therefore, that exogenous palmitoyl CoA would inhibit respiration in IBE more than in torpor. Palmitoyl CoA inhibited respiration ~70%, in both torpor and IBE. The addition of carnitine, predicted to reverse palmitoyl CoA suppression by facilitating its transport into the mitochondrial matrix, did not rescue the respiration rates in IBE or torpor. Liver mitochondrial activities of carnitine palmitoyl transferase did not differ among IBE, torpor and summer animals. Although palmitoyl CoA inhibits succinate-fuelled respiration, this suppression is likely not related exclusively to inhibition of the DCT, and may involve additional mitochondrial transporters such as the adenine-nucleotide transporter.

摘要

冬眠的 13 行地松鼠(Ictidomys tridecemlineatus)与整个动物代谢的显著抑制有关。我们比较了来自冬眠地松鼠、清醒期(最近从冬眠中苏醒)和夏季同物种的肝线粒体的代谢。与 IBE 和夏季相比,琥珀酰辅酶 A 驱动的状态 3 呼吸,相对于线粒体蛋白计算,在冬眠中分别被抑制了 48%和 44%。当呼吸相对于细胞色素 c 氧化酶活性表达时,这种抑制仍然存在。我们假设这种抑制是由长链脂肪酸辅酶 A 在二羧酸转运蛋白(DCT)处抑制琥珀酸转运引起的,这些物质可能在冬眠期间积累。因此,我们预测外源性棕榈酰辅酶 A 会比在冬眠中更抑制 IBE 中的呼吸。棕榈酰辅酶 A 抑制 IBE 和冬眠中的呼吸约 70%。添加肉碱,预计通过促进其进入线粒体基质来逆转棕榈酰辅酶 A 的抑制,但不能挽救 IBE 或冬眠中的呼吸速率。IBE、冬眠和夏季动物的肉碱棕榈酰转移酶的肝线粒体活性没有差异。虽然棕榈酰辅酶 A 抑制琥珀酸驱动的呼吸,但这种抑制可能不仅仅与 DCT 的抑制有关,还可能涉及其他线粒体转运蛋白,如腺嘌呤核苷酸转运蛋白。

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