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首页> 外文期刊>Molecular and Cellular Endocrinology >Think globally: act locally. New insights into the local regulation of thyroid hormone availability challenge long accepted dogmas.
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Think globally: act locally. New insights into the local regulation of thyroid hormone availability challenge long accepted dogmas.

机译:放眼全球:在当地行动。对甲状腺激素可利用性的局部调节的新见识挑战了公认的教条。

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摘要

Recent evidence derived from transgenic mouse models and findings in humans with mutations affecting thyroid hormone (TH) metabolism have convincingly supported a model of TH signalling in which regulated local adjustment of active TH concentrations is far more important than circulating plasma hormone levels. Although this theory was put forward several years ago and has been supported by significant, but inherently indirect evidence, recent insights from targeted deletion of the genes encoding deiodinase (Dio) isozymes have revived this model and greatly increased our understanding of TH metabolism. However, gene targeting proved to be a double edged sword, since the overall model was supported, but several predictions are apparently not consistent with the new experimental evidence. Human genetics further provided additional exciting data on the physiological role of Dio isozymes that need to be incorporated into any model of TH biology. The recent identification of mutations in the T3 plasma membrane transporter MCT8 has sparked new interest in the role of TH in brain function, since affected patients suffered from psychomotor retardation. Moreover, selenium (Se) and TH physiology have finally been unequivocally connected by newly identified inherited defects in a gene involved in selenoprotein biosynthesis. Finally, a link between Dio expression and energy metabolism has been delineated in mice that may hold great promise for the management of the adiposity pandemic.
机译:从转基因小鼠模型获得的最新证据以及在人类中影响甲状腺激素(TH)代谢突变的发现令人信服地支持了TH信号传导模型,其中对活性TH浓度的调节局部调节远比循环血浆激素水平重要。尽管该理论是在几年前提出的,并得到了重要但固有的间接证据的支持,但是针对性删除编码脱碘酶(Dio)同工酶的基因的最新见解使该模型得以复兴,并极大地增进了我们对TH代谢的理解。然而,由于支持了整体模型,因此基因靶向被证明是一把双刃剑,但是一些预测显然与新的实验证据不一致。人类遗传学进一步提供了有关Dio同工酶的生理作用的其他令人兴奋的数据,需要将其纳入任何TH生物学模型中。 T3质膜转运蛋白MCT8中突变的最新发现激发了TH在脑功能中的作用的新兴趣,因为受影响的患者患有精神运动障碍。此外,硒(Se)和TH的生理学最终已被新确定的涉及硒蛋白生物合成的基因中的遗传缺陷明确地联系在一起。最后,已经在小鼠中描述了Dio表达与能量代谢之间的联系,这可能对控制肥胖大流行具有广阔的前景。

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