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无配体甲状腺激素受体α控制 Xenopus tropicalis 的发育时间。

Unliganded thyroid hormone receptor α controls developmental timing in Xenopus tropicalis.

机构信息

Section on Molecular Morphogenesis, Program on Cell Regulation and Metabolism, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Endocrinology. 2015 Feb;156(2):721-34. doi: 10.1210/en.2014-1439. Epub 2014 Dec 2.

Abstract

Thyroid hormone (T3) affects adult metabolism and postembryonic development in vertebrates. T3 functions mainly via binding to its receptors (TRs) to regulate gene expression. There are 2 TR genes, TRα and TRβ, with TRα more ubiquitously expressed. During development, TRα expression appears earlier than T3 synthesis and secretion into the plasma. This and the ability of TRs to regulate gene expression both in the presence and absence of T3 have indicated a role for unliganded TR during vertebrate development. On the other hand, it has been difficult to study the role of unliganded TR during development in mammals because of the difficulty to manipulate the uterus-enclosed, late-stage embryos. Here we use amphibian development as a model to address this question. We have designed transcriptional activator-like effector nucleases (TALENs) to mutate the TRα gene in Xenopus tropicalis. We show that knockdown of TRα enhances tadpole growth in premetamorphic tadpoles, in part because of increased growth hormone gene expression. More importantly, the knockdown also accelerates animal development, with the knockdown animals initiating metamorphosis at a younger age and with a smaller body size. On the other hand, such tadpoles are resistant to exogenous T3 treatment and have delayed natural metamorphosis. Thus, our studies not only have directly demonstrated a critical role of endogenous TRα in mediating the metamorphic effect of T3 but also revealed novel functions of unliganded TRα during postembryonic development, that is, regulating both tadpole growth rate and the timing of metamorphosis.

摘要

甲状腺激素 (T3) 影响脊椎动物的成年代谢和胚胎后发育。T3 主要通过与其受体 (TRs) 结合来调节基因表达。有 2 个 TR 基因,TRα 和 TRβ,TRα 表达更为广泛。在发育过程中,TRα 的表达早于 T3 合成并分泌到血浆中。这一事实以及 TR 能够在存在和不存在 T3 的情况下调节基因表达,表明未结合的 TR 在脊椎动物发育中发挥作用。另一方面,由于难以操纵子宫内的晚期胚胎,因此很难在哺乳动物中研究未结合的 TR 在发育过程中的作用。在这里,我们使用两栖动物发育作为模型来解决这个问题。我们设计了转录激活因子样效应物核酸酶 (TALENs) 来突变 Xenopus tropicalis 的 TRα 基因。我们表明,TRα 的敲低增强了前变态期蝌蚪的生长,部分原因是生长激素基因表达增加。更重要的是,敲低也加速了动物的发育,敲低的动物在更年轻的年龄和更小的体型开始变态。另一方面,这些蝌蚪对外源性 T3 处理具有抗性,并且自然变态延迟。因此,我们的研究不仅直接证明了内源性 TRα 在介导 T3 的变态作用中的关键作用,而且还揭示了未结合的 TRα 在胚胎后发育中的新功能,即调节蝌蚪的生长速度和变态的时间。

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本文引用的文献

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Neuroendocrinology of amphibian metamorphosis.
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Efficient targeted gene disruption in Xenopus embryos using engineered transcription activator-like effector nucleases (TALENs).
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