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How the thyroid controls metabolism in the rat: different roles for triiodothyronine and diiodothyronines.

机译:甲状腺如何控制大鼠的新陈代谢:三碘甲状腺素和碘甲状腺素的作用不同。

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摘要

1. Although the first evidence of a relationship between the thyroid and metabolism was reported in 1895, the mechanism by which thyroid hormones influence resting metabolic rate in whole animals is still poorly understood. This paper reports an attempt to test whether diiodothyronines (T2s) and triiodothyronine (T3) have different roles in the control of resting metabolism (RM). 2. Changes in resting metabolic rate were measured in hypothyroid rats treated acutely (25 micrograms (100 g body weight)-1) either with one of the T2s or with T3. Injection of T3 induced an increase of about 35% in RM that started 25-30 h after the injection and lasted until 5-6 days after the injection, the maximal value being observed at 50-75 h. The injection of T2s evoked a temporally different pattern of response. The increases in RM started 6-12 h after the injection, had almost disappeared after 48 h, and the maximal stimulation was observed at 28-30 h. 3. When actinomycin D (an inhibitor of protein synthesis) and T3 were given together, the stimulation of RM was almost completely abolished. The simultaneous injection of actinomycin D and either of the T2s, on the other hand, did not cause any attenuation of the stimulation seen with the T2s alone. 4. Following chronic treatment (3 weeks) with either T3 or T2s there was a stimulation of organ growth only after the administration of T3. 5. Chronic administration of either T2s or T3 to hypothyroid rats significantly enhanced the oxidative capacity of each of the tissues considered. In the case of T2s the stimulation was almost the same whether it was expressed as an increase in specific activity or total tissue activity. In the case of T3 the increases were, in the main, secondary to the hypertrophic or hyperplastic effect. 6. These results indicate that T2s and T3 exert different effects on RM. The effects of T2s are rapid and possibly mediated by their direct interaction with mitochondria. Those of T3 are slower and more prolonged, and at least partly attributable to a modulation of the cellularity of tissues that are metabolically very active.
机译:1.尽管在1895年报道了甲状腺与代谢之间关系的第一个证据,但对甲状腺激素影响整个动物静息代谢率的机制仍知之甚少。本文报道了尝试检测二碘甲状腺素(T2s)和三碘甲状腺素(T3)在控制静止代谢(RM)中是否具有不同作用的尝试。 2.在急性甲状腺功能减退的大鼠(25微克(100克体重)-1)中,用一种T2s或T3治疗,测量其静息代谢率的变化。注射T3导致RM的增加约35%,从注射后25-30小时开始,一直持续到注射后5-6天,在50-75小时观察到最大值。 T2的注入引起了时间上不同的响应模式。 RM的增加在注射后6-12小时开始,在48小时后几乎消失,在28-30小时观察到最大刺激。 3.当放线菌素D(蛋白质合成抑制剂)和T3一起使用时,RM的刺激作用几乎完全被消除。另一方面,同时注射放线菌素D和两个T2中的任何一个,都不会导致单独使用T2中看到的刺激作用减弱。 4.用T3或T2进行慢性治疗(3周)后,仅在施用T3后才刺激器官生长。 5.对甲状腺功能减退的大鼠长期施用T2或T3可以显着增强所考虑的每个组织的氧化能力。在T2s的情况下,无论刺激表现为比活性或总组织活性的增加,几乎都是相同的。在T3的情况下,增加主要是继发于肥厚或增生的作用。 6.这些结果表明,T2和T3对RM的作用不同。 T2的作用是快速的,可能是由于它们与线粒体的直接相互作用介导的。 T3的那些较慢且更长,并且至少部分归因于代谢非常活跃的组织的细胞性的调节。

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