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比较表型分析揭示了 TRα 和 TRβ 的经典和非经典生理功能。

Comparative Phenotyping of Mice Reveals Canonical and Noncanonical Physiological Functions of TRα and TRβ.

机构信息

Department of Endocrinology, Diabetes and Metabolism and Division of Laboratory Research, University Hospital Essen, University of Duisburg-Essen, Essen 45147, Germany.

Research Unit NeuroBiology of Diabetes, Helmholtz Zentrum München, Neuherberg 85764, Germany.

出版信息

Endocrinology. 2024 Jul 1;165(8). doi: 10.1210/endocr/bqae067.

Abstract

Thyroid hormone (TH) effects are mediated through TH receptors (TRs), TRα1, TRβ1, and TRβ2. The TRs bind to the DNA and regulate expression of TH target genes (canonical signaling). In addition, they mediate activation of signaling pathways (noncanonical signaling). Whether noncanonical TR action contributes to the spectrum of TH effects is largely unknown. The aim of this study was to attribute physiological effects to the TR isoforms and their canonical and noncanonical signaling. We conducted multiparameter phenotyping in male and female TR knockout mice (TRαKO, TRβKO), mice with disrupted canonical signaling due to mutations in the TR DNA binding domain (TRαGS, TRβGS), and their wild-type littermates. Perturbations in senses, especially hearing (mainly TRβ with a lesser impact of TRα), visual acuity, retinal thickness (TRα and TRβ), and in muscle metabolism (TRα) highlighted the role of canonical TR action. Strikingly, selective abrogation of canonical TR action often had little phenotypic consequence, suggesting that noncanonical TR action sufficed to maintain the wild-type phenotype for specific effects. For instance, macrocytic anemia, reduced retinal vascularization, or increased anxiety-related behavior were only observed in TRαKO but not TRαGS mice. Noncanonical TRα action improved energy utilization and prevented hyperphagia observed in female TRαKO mice. In summary, by examining the phenotypes of TRα and TRβ knockout models alongside their DNA binding-deficient mutants and wild-type counterparts, we could establish that the noncanonical actions of TRα and TRβ play a crucial role in modulating sensory, behavioral, and metabolic functions and, thus, contribute to the spectrum of physiological TH effects.

摘要

甲状腺激素(TH)的作用是通过甲状腺激素受体(TRs)介导的,TRα1、TRβ1 和 TRβ2。TRs 与 DNA 结合并调节 TH 靶基因的表达(经典信号)。此外,它们还介导信号通路的激活(非经典信号)。非经典 TR 作用是否有助于 TH 作用谱尚不清楚。本研究旨在将生理作用归因于 TR 同工型及其经典和非经典信号。我们对雄性和雌性 TR 敲除小鼠(TRαKO、TRβKO)、由于 TR DNA 结合域突变而导致经典信号中断的小鼠(TRαGS、TRβGS)及其野生型同窝仔鼠进行了多参数表型分析。感觉障碍,特别是听力(主要是 TRβ,TRα 的影响较小)、视力、视网膜厚度(TRα 和 TRβ)和肌肉代谢(TRα)的改变突出了经典 TR 作用。引人注目的是,经典 TR 作用的选择性阻断通常对表型没有什么影响,这表明非经典 TR 作用足以维持特定作用的野生型表型。例如,巨红细胞性贫血、视网膜血管化减少或焦虑相关行为增加仅见于 TRαKO 小鼠,而不是 TRαGS 小鼠。非经典 TRα 作用可改善能量利用并预防女性 TRαKO 小鼠中观察到的过度摄食。总之,通过检查 TRα 和 TRβ 敲除模型及其 DNA 结合缺陷突变体和野生型对照的表型,我们可以确定 TRα 和 TRβ 的非经典作用在调节感觉、行为和代谢功能方面发挥着重要作用,从而有助于 TH 作用谱的生理作用。

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