4.5 Article

Regulation of the mTOR signaling network in hibernating thirteen-lined ground squirrels

期刊

JOURNAL OF EXPERIMENTAL BIOLOGY
卷 215, 期 10, 页码 1720-1727

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COMPANY BIOLOGISTS LTD
DOI: 10.1242/jeb.066225

关键词

Ictidomys tridecemlineatus; torpor-arousal cycle; translational control; Akt; 4EBP

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资金

  1. National Science and Engineering Research Council of Canada [6793]

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For many small mammals, survival over the winter months is a serious challenge because of low environmental temperatures and limited food availability. The solution for many species, such as thirteen-lined ground squirrels (Ictidomys tridecemlineatus), is hibernation, an altered physiological state characterized by seasonal heterothermy and entry into long periods of torpor that are interspersed with short arousals back to euthermia. During torpor, metabolic rate is strongly reduced to achieve major energy savings, and a coordinated depression of non-essential ATP-expensive functions such as protein synthesis takes place. This study examines the mammalian target of rapamycin (mTOR) signaling pathway, a crucial component of the insulin receptor network, over six stages of the torpor-arousal cycle of hibernation. Immunoblots showed that the phosphorylation state of mTOR(Ser2448) was strongly reduced in skeletal muscle (by 55%) during late torpor but increased by 200% during early arousal compared with euthermia. However, the phosphorylation state of this residue remained relatively constant in cardiac muscle during torpor but was enhanced during entrance into torpor and early arousal from torpor stages (by 2.9- and 3.2-fold, respectively). Phosphorylation states of upstream regulators of mTOR, p-Akt(Thr473) and p-TSC2(Thr1462), were also suppressed in skeletal muscle by 55 and 51%, respectively, during late torpor, as were selected downstream substrates - p-4E-BP1(Thr46) and p-S6(Ser235) contents dropped by 74 and 41%, respectively. Overall, the results indicate suppressed mTOR signaling in skeletal muscle, but not cardiac muscle, during torpor. By contrast, activation of mTOR and other components of the mTORC1 complex (p-PRAS40(Thr246) and G beta L) occurred during early arousal in both skeletal and cardiac muscle.

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