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Tissue iodoprotein formation during the peripheral metabolism of the thyroid hormones

机译:甲状腺激素周围代谢过程中组织碘蛋白的形成

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摘要

The formation of tissue iodoproteins during the peripheral metabolism of the thyroid hormones was examined by determining the concentration of nonethanol-extractable 125I (NE125I) in various tissues after the intravenous injection of 3,5,3′-triiodo-L-thyronine (T3-125I) and L-thyroxine-125I (T4-125I) in groups of rats with iodide-blocked thyroid glands. 3 days after T3-125I and 7 days after T4-125I injection the concentration of NE125I in the liver and kidney was 5-10 times greater than in plasma. Smaller but nonetheless significant concentrations of NE125I were demonstrated in skeletal and cardiac muscle. Hepatic subcellular fractionation studies revealed that the major portion of the liver NE125I was in the microsomal fraction. Lower concentrations of NE125I were present in the nuclear, mitochondrial, and soluble fractions. When similar studies were performed in groups of rats pretreated with phenobarbital, an increase in the metabolic clearance of T3-125I (30%) and T4-125I (100%) was observed along with a highly significant increase in the NE125I concentration of the liver and plasma. The increase in hepatic NE125I in these studies was primarily due to the microsomal component.Incubation of hepatic microsomes with T3-125I and T4-125I showed that NEI formation as well as deiodination appeared to obey simple Michaelis-Menten kinetics. Moreover, the maximal rate of both deiodination and NEI formation was increased when microsomes harvested from phenobarbital-treated rats were employed.These studies indicate that thyroid hormone metabolism results in the formation of structural and soluble tissue iodoproteins in addition to circulating iodoproteins. The rate of formation of these moieties in the liver and plasma appears to be related to the rate of hormone metabolism.
机译:通过测定静脉内注射后各种组织中非乙醇可提取的 125 I(NE 125 I)的浓度来检查甲状腺激素周围代谢过程中组织碘蛋白的形成注射3,5,3'-三碘-L-甲状腺素(T3- 125 I)和L-甲状腺素- 125 I(T4- 125 I)碘化物阻断的甲状腺大鼠组。 T3- 125 I注射后3天和T4- 125 I注射后7天,肝脏和肾脏中NE 125 I的浓度为5比血浆大-10倍。在骨骼肌和心肌中,NE 125 I的浓度较小但显着升高。肝亚细胞分级分离研究表明,肝脏NE 125 I的主要部分位于微粒体部分。核,线粒体和可溶性部分中NE 125 I的浓度较低。当在苯巴比妥预处理的大鼠组中进行类似研究时,T3- 125 I(30%)和T4- 125 I(100%)的代谢清除率增加)以及肝脏和血浆中NE 125 I的浓度显着增加。这些研究中肝NE 125 I的增加主要归因于微粒体成分。肝微粒体与T3- 125 I和T4- 125 的孵育sup>我表明,NEI的形成以及除碘作用似乎遵循简单的Michaelis-Menten动力学。此外,当使用苯巴比妥治疗的大鼠收集的微粒体时,脱碘和NEI形成的最大速率都增加了。这些研究表明,甲状腺激素代谢除了循环的碘蛋白外还导致结构性和可溶性组织碘蛋白的形成。这些部分在肝脏和血浆中的形成速率似乎与激素代谢速率有关。

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