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胚胎期鸡肝脏、肾脏、大脑和血液中细胞内甲状腺激素浓度的动态变化及调节

Dynamics and regulation of intracellular thyroid hormone concentrations in embryonic chicken liver, kidney, brain, and blood.

作者信息

Reyns G E, Venken K, Morreale de Escobar G, Kühn E R, Darras V M

机构信息

Laboratory of Comparative Endocrinology, Zoological Instistute, K.U. Leuven, Naamsestraat 61, Leuven B-3000, Belgium.

出版信息

Gen Comp Endocrinol. 2003 Oct 15;134(1):80-7. doi: 10.1016/s0016-6480(03)00220-x.

Abstract

The intracellular thyroid hormone (TH) availability is influenced by different metabolic pathways. We investigated the relationship between tissue and plasma TH levels as well as the correlation with changes of deiodination and sulfation during chicken embryonic development. From day 14 until day 19, T3 remains unchanged in liver and kidney in spite of increasing plasma T4 and T3 levels and a slightly increased T4 availability in these tissues. During this period, the T3 breakdown capacity by type III deiodinase (D3) is high in liver but low in kidney. The TH inactivation capacity of type I deiodinase (D1), with production of inactive rT3 instead of T3, in kidney seems to be potentiated by the sulfation pathway. A sharp rise in T3 and T4 is detected in all tissues examined when the embryo switches to lung respiration. The same day, T4 content in liver is sharply enhanced and sulfation activity is decreased. So, T4 availability in liver is increased while a declined D3 activity allows for the accumulation of hepatic T3. The increase in renal T3 and T4 are more closely related to plasma TH profiles and a lack of correlation with the changes in renal D1 and D3 activity suggests that T4 and T3 content in this organ is strongly dependent on direct uptake from the blood. Despite much lower T4 levels, T3 levels in brain are in the same range as in liver and kidney and intracellular T3 even exceeds the T4 levels towards the end of development. The rise in TH content coincides with a drop in D3 activity, low sulfation activity and an increased T3 production capacity via type II deiodinase (D2). In conclusion, the current study describes the dynamics of intracellular TH concentrations in liver, kidney, and brain during chicken development and investigates their relationship with circulating TH levels and changes of deiodinases and sulfotransferases. The clear differences in intracellular TH profiles among the different tissues demonstrate that circulating levels are not necessarily representative for the local TH changes. Some of the changes in intracellular TH availability can be linked to changes in local deiodination and sulfation capacities, but the importance of these enzyme systems in relation to other factors, such as hormone uptake, differs between liver, kidney, and brain.

摘要

细胞内甲状腺激素(TH)的可利用性受不同代谢途径的影响。我们研究了鸡胚胎发育过程中组织与血浆TH水平之间的关系,以及与脱碘和硫酸化变化的相关性。从第14天到第19天,尽管血浆T4和T3水平升高,且这些组织中T4的可利用性略有增加,但肝脏和肾脏中的T3保持不变。在此期间,肝脏中III型脱碘酶(D3)分解T3的能力较高,而肾脏中则较低。肾脏中I型脱碘酶(D1)将T4转化为无活性的反式T3(rT3)而非T3的TH失活能力似乎因硫酸化途径而增强。当胚胎转向肺呼吸时,在所有检测的组织中均检测到T3和T4急剧上升。同一天,肝脏中的T4含量急剧增加,硫酸化活性降低。因此,肝脏中T4的可利用性增加,而D3活性下降使得肝脏中T3得以积累。肾脏中T3和T4的增加与血浆TH水平更为密切相关,且与肾脏中D1和D3活性的变化缺乏相关性,这表明该器官中T4和T3的含量强烈依赖于从血液中的直接摄取。尽管T4水平低得多,但大脑中的T3水平与肝脏和肾脏中的处于同一范围,并且在发育末期细胞内T3甚至超过了T4水平。TH含量的上升与D3活性下降、低硫酸化活性以及通过II型脱碘酶(D2)产生T3的能力增加相吻合。总之,本研究描述了鸡发育过程中肝脏、肾脏和大脑中细胞内TH浓度的动态变化,并研究了它们与循环TH水平以及脱碘酶和硫酸转移酶变化的关系。不同组织中细胞内TH谱的明显差异表明,循环水平不一定代表局部TH的变化。细胞内TH可利用性的一些变化可与局部脱碘和硫酸化能力的变化相关联,但这些酶系统相对于其他因素(如激素摄取)的重要性在肝脏、肾脏和大脑之间有所不同。

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