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老年大鼠甲状腺激素给药后能量平衡调节的改变。

Altered regulation of energy homeostasis in older rats in response to thyroid hormone administration.

机构信息

1Endocrinology Research Unit, Mayo Clinic, 200 First Street SW, Rochester, MN 55905, USA.

出版信息

FASEB J. 2014 Mar;28(3):1499-510. doi: 10.1096/fj.13-239806. Epub 2013 Dec 16.

Abstract

Hyperthyroidism causes increased energy intake and expenditure, although anorexia and higher weight loss have been reported in elderly individuals with hyperthyroidism. To determine the effect of age on energy homeostasis in response to experimental hyperthyroidism, we administered 200 μg tri-iodothyronine (T3) in 7- and 27-mo-old rats for 14 d. T3 increased energy expenditure (EE) in both the young and the old rats, although the old rats lost more weight (147 g) than the young rats (58 g) because of the discordant effect of T3 on food intake, with a 40% increase in the young rats, but a 40% decrease in the old ones. The increased food intake in the young rats corresponded with a T3-mediated increase in the appetite-regulating proteins agouti-related peptide, neuropeptide Y, and uncoupling protein 2 in the hypothalamus, but no increase occurred in the old rats. Evidence of mitochondrial biogenesis in response to T3 was similar in the soleus muscle and heart of the young and old animals, but less consistent in old plantaris muscle and liver. Despite the comparable increase in EE, T3's effect on mitochondrial function was modulated by age in a tissue-specific manner. We conclude that older rats lack compensatory mechanisms to increase caloric intake in response to a T3-induced increase in EE, demonstrating a detrimental effect of age on energy homeostasis.

摘要

甲状腺功能亢进症导致能量摄入和消耗增加,尽管有报道称老年甲状腺功能亢进症患者会出现厌食和更高的体重减轻。为了确定年龄对实验性甲状腺功能亢进症时能量平衡的影响,我们在 7 个月大和 27 个月大的大鼠中给予 200μg 三碘甲状腺原氨酸(T3),持续 14 天。T3 增加了年轻和老年大鼠的能量消耗(EE),尽管老年大鼠(147g)比年轻大鼠(58g)体重减轻更多,这是由于 T3 对食物摄入的影响不一致,年轻大鼠的食物摄入量增加了 40%,而老年大鼠的食物摄入量减少了 40%。年轻大鼠的食物摄入量增加与下丘脑调节食欲的蛋白质刺鼠相关肽、神经肽 Y 和解偶联蛋白 2 的 T3 介导增加相对应,但老年大鼠则没有。年轻和老年动物的比目鱼肌和心脏对 T3 的反应中,线粒体生物发生的证据相似,但在老年动物的跖肌和肝脏中则不那么一致。尽管 EE 的增加相当,但 T3 对线粒体功能的影响在组织特异性方面受到年龄的调节。我们得出结论,老年大鼠缺乏补偿机制来增加热量摄入以响应 T3 诱导的 EE 增加,这表明年龄对能量平衡有不利影响。

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