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低温下棕色脂肪组织产热能力增加及其对叙利亚仓鼠从冬眠中觉醒的贡献。

Increased thermogenic capacity of brown adipose tissue under low temperature and its contribution to arousal from hibernation in Syrian hamsters.

机构信息

Department of Physiology, Asahikawa Medical University, Japan.

出版信息

Am J Physiol Regul Integr Comp Physiol. 2012 Jan 1;302(1):R118-25. doi: 10.1152/ajpregu.00053.2011. Epub 2011 Oct 12.

DOI:10.1152/ajpregu.00053.2011
PMID:21993529
Abstract

Brown adipose tissue (BAT) is thought to play a significant physiological role during arousal when body temperature rises from the extremely low body temperature that occurs during hibernation. The dominant pathway of BAT thermogenesis occurs through the β(3)-adrenergic receptor. In this study, we investigated the role of the β(3)-adrenergic system in BAT thermogenesis during arousal from hibernation both in vitro and in vivo. Syrian hamsters in the hibernation group contained BAT that was significantly greater in overall mass, total protein, and thermogenic uncoupling protein-1 than BAT from the warm-acclimated group. Although the ability of the β(3)-agonist CL316,243 to induce BAT thermogenesis at 36°C was no different between the hibernation and warm-acclimated groups, its maximum ratio over the basal value at 12°C in the hibernation group was significantly larger than that in the warm-acclimated group. Forskolin stimulation at 12°C produced equivalent BAT responses in these two groups. In vivo thermogenesis was assessed with the arousal time determined by the time course of BAT temperature or heart rate. Stimulation of BAT by CL316,243 significantly shortened the time of arousal from hibernation compared with that induced by vehicle alone, and it also induced arousal in deep hibernating animals. The β(3)-antagonist SR59230A inhibited arousal from hibernation either in part or completely. These results suggest that BAT in hibernating animals has potent thermogenic activity with a highly effective β(3)-receptor mechanism at lower temperatures.

摘要

棕色脂肪组织(BAT)被认为在唤醒时发挥重要的生理作用,此时体温从冬眠时的极低体温升高。BAT 产热的主要途径是通过β(3)-肾上腺素能受体。在这项研究中,我们研究了β(3)-肾上腺素能系统在冬眠唤醒期间对 BAT 产热的作用,包括在体外和体内的作用。冬眠组的叙利亚仓鼠的 BAT 在总质量、总蛋白和解偶联蛋白-1 方面明显大于适应温暖组的 BAT。虽然 36°C 时β(3)激动剂 CL316,243 诱导 BAT 产热的能力在冬眠组和适应温暖组之间没有差异,但在 12°C 时其最大比值高于适应温暖组。在这两组中,12°C 时的 forskolin 刺激产生了等效的 BAT 反应。通过 BAT 温度或心率的时间过程来评估体内产热,唤醒时间被确定为 BAT 产热的评估指标。与单独使用载体相比,CL316,243 刺激 BAT 显著缩短了从冬眠中唤醒的时间,并且它还能诱导深度冬眠的动物醒来。β(3)拮抗剂 SR59230A 部分或完全抑制了从冬眠中醒来。这些结果表明,冬眠动物的 BAT 在较低温度下具有很强的产热活性和高度有效的β(3)受体机制。

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