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雏鸡胚胎发育过程中肝脏碘甲状腺原氨酸代谢的变化。

Changes in hepatic iodothyronine metabolism during ontogeny of the chick embryo.

作者信息

Borges M, LaBourene J, Ingbar S H

出版信息

Endocrinology. 1980 Dec;107(6):1751-61. doi: 10.1210/endo-107-6-1751.

Abstract

As a model of the changes in peripheral iodothyronine metabolism that occur during ontogeny, we have studied the metabolism of 125I-labeled T4 and several of its partially deiodinated derivatives by the liver of the chick embryo. Homogenates of livers obtained from chicks varying in embryonic age from 8 days to the time of hatching (20-21 days) were incubated with various iodothyronines, all labeled with 125I in their outer or phenolic ring. Rates and products of the reactions were analyzed by paper chromatography of whole homogenates. In livers from embryos of all ages studied, the addition of dithiothreitol (DTT; 2 mM) enhanced the rate of metabolism of the iodothyronines T4, T3, and rT3. Marked age-related changes in the metabolism of the iodothyronines were apparent; these were evident in the absence of DTT, but were most clearly seen in specimens to which DTT had been added. rT3 was degraded very rapidly, even in livers from 8-day-old embryos, but its rate of degradation increased progressively with increasing age of the embryo up to the time of hatching. Outer ring (5'-) monodeiodination, giving rise to 3,3'-diiodothyronine (3,3'-T2), was the predominant, and perhaps the sole, pathway of rT3 metabolism throughout this period of embryogenesis. Age-related changes in the metabolism of T4 and T3 were similar to one another, but differed greatly from those seen in the case of rT3. In specimens enriched with DTT, the rates of metabolism of T4 and T3 were moderately rapid in livers from 12-day-old embryos and then increased abruptly, remaining very rapid in livers from embryos through 18 days of age. Rapid degradation of T4 was not due to 5'-monodeiodination, since very little T3 was generated from T4. In addition, since results obtained were similar during incubations under air and N2, oxidative degradation of T4 was apparently not important. Rather, during this period, inner ring (5-) monodeiodination appeared to be by far the predominmant pathway of metabolism of both T4 and T3, leading to the formation of rT3 from T4 and 3,3'-T2 from T3. In livers from 19- and 20 day-old embryos, the latter obtained just before hatching, the overall metabolism of both T4 and T3 slowed abruptly and progressively owing to a decrease in the rate of 5-monodeiodination. Concomitantly, 5'-monodeiodination of T3 and T4 became more prominent, leading to increased generation of T3 from T4. These maturational changes in T4 and T3 metabolism coincided in time with penetration of the air sac by the embryo's beak and initiation of air breathing, a process termed internal pipping. Premature maturational changes in T4 and T3 metabolism, very similar to those that occurred spontaneously in 19- and especially 20-day-old embryos, were induced within 2 days by the single injection of 200 microgram hydrocortisone onto the allantoic membrane of immature embryos. It is concluded that hepatic iodothyronine metabolism in the immature embryo is directed so as to prevent the accumulation of T3 derived from T4...

摘要

作为个体发育过程中发生的外周甲状腺素代谢变化的模型,我们研究了鸡胚肝脏对125I标记的T4及其几种部分脱碘衍生物的代谢。将取自胚胎年龄从8天到孵化时(20 - 21天)不等的鸡的肝脏匀浆与各种甲状腺素一起孵育,所有甲状腺素在其外环或酚环上都标记有125I。通过对整个匀浆进行纸层析分析反应速率和产物。在所研究的所有年龄胚胎的肝脏中,加入二硫苏糖醇(DTT;2 mM)可提高甲状腺素T4、T3和反T3(rT3)的代谢速率。甲状腺素代谢存在明显的年龄相关变化;在没有DTT的情况下这些变化就很明显,但在添加了DTT的标本中最为明显。rT3降解非常迅速,即使在8日龄胚胎的肝脏中也是如此,但其降解速率随着胚胎年龄的增加直至孵化时逐渐增加。外环(5'-)单脱碘生成3,3'-二碘甲状腺原氨酸(3,3'-T2),是整个胚胎发育期间rT3代谢的主要途径,甚至可能是唯一途径。T4和T3代谢的年龄相关变化彼此相似,但与rT3的情况有很大不同。在富含DTT的标本中,12日龄胚胎肝脏中T4和T3的代谢速率适中,然后突然增加,在18日龄胚胎的肝脏中一直保持很快。T4的快速降解不是由于5'-单脱碘,因为从T4生成的T3很少。此外,由于在空气和氮气环境下孵育得到的结果相似,T4的氧化降解显然并不重要。相反,在此期间,内环(5-)单脱碘似乎是T4和T3代谢的主要途径,T4通过此途径生成rT3,T3通过此途径生成3,3'-T2。在19日龄和20日龄胚胎(孵化前获取)的肝脏中,由于5-单脱碘速率降低,T4和T3的整体代谢突然且逐渐减缓。与此同时,T3和T4的5'-单脱碘变得更加显著,导致从T4生成的T3增加。T4和T3代谢的这些成熟变化与胚胎喙穿透气囊并开始空气呼吸(一个称为内破壳的过程)在时间上相吻合。通过向未成熟胚胎的尿囊膜单次注射200微克氢化可的松,可在2天内诱导T4和T3代谢过早出现成熟变化,这些变化与19日龄尤其是20日龄胚胎中自发发生的变化非常相似。结论是,未成熟胚胎肝脏中的甲状腺素代谢是有导向性的,以防止由T4衍生的T3积累……

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