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分化与功能障碍:甲状腺激素、脱碘酶与视网膜光感受器

Differentiation versus dysfunction: thyroid hormone, deiodinases and retinal photoreceptors.

作者信息

Ng Lily, Liu Ye, Cho Young-Wook, Liu Hong, Forrest Douglas

出版信息

Eur Thyroid J. 2025 Mar 12;14(2). doi: 10.1530/ETJ-24-0315. Print 2025 Apr 1.

Abstract

A growing body of evidence has established that thyroid hormone (triiodothyronine, T3) is a key factor in the differentiation and survival of the light-sensing photoreceptors in the retina. These functions include a critical role in generating the cone photoreceptor diversity that is required for color vision. Here, we review some of these functions of T3 and the critical mechanisms that regulate the T3 signal in the mammalian retina. The provision of T3, the active form of thyroid hormone, is determined by developmentally rising levels of T3 and its precursor T4 (thyroxine) in the circulation and by intrinsic control within the retina itself by deiodinase enzymes that deplete or amplify the available level of T3. Dynamic profiles of inactivating (DIO3) and activating (DIO2) deiodinases suggest that the T3 signal is progressively calibrated throughout early development, maturation and later functional maintenance of the retina. However, the benefits of T3 come at a cost: photoreceptors are susceptible to impairment and cell death when T3 signaling becomes imbalanced. These findings have implications regarding the influence of T3 in retinal diseases.

摘要

越来越多的证据表明,甲状腺激素(三碘甲状腺原氨酸,T3)是视网膜中感光光感受器分化和存活的关键因素。这些功能包括在产生色觉所需的视锥光感受器多样性方面发挥关键作用。在此,我们综述T3的一些功能以及调节哺乳动物视网膜中T3信号的关键机制。甲状腺激素的活性形式T3的供应,取决于循环中T3及其前体T4(甲状腺素)水平的发育性升高,以及视网膜自身通过脱碘酶进行的内在调控,这些脱碘酶会消耗或放大可用的T3水平。失活(DIO3)和激活(DIO2)脱碘酶的动态变化表明,在视网膜的早期发育、成熟及后期功能维持过程中,T3信号是逐步校准的。然而,T3带来益处的同时也有代价:当T3信号失衡时,光感受器易受损伤并发生细胞死亡。这些发现对T3在视网膜疾病中的影响具有启示意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cc1f/11906153/46145366002d/ETJ-24-0315fig1.jpg

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