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视黄酸和甲状腺激素通过共同的反应元件诱导基因表达。

Retinoic acid and thyroid hormone induce gene expression through a common responsive element.

作者信息

Umesono K, Giguere V, Glass C K, Rosenfeld M G, Evans R M

机构信息

Howard Hughes Medical Institute, La Jolla, California.

出版信息

Nature. 1988 Nov 17;336(6196):262-5. doi: 10.1038/336262a0.

Abstract

Studies of steroid receptors have led to the identification of a superfamily of ligand-inducible regulatory proteins that includes receptors for thyroid hormones and retinoic acid. This family of receptors regulates gene expression through binding to short cis-acting sequences referred to as hormone-response elements. Identification of a functional retinoic acid responsive element is crucial to our understanding of the mechanisms by which retinoic acid receptors activate gene expression and regulate cell differentiation. One impediment to such a study is the absence of any identified gene whose transcription is directly dependent on the receptor-hormone complex. Because the DNA-binding domains of the retinoic acid and thyroid hormone receptors are highly related (62% identical in their amino acid sequences), we have investigated the possibility that the retinoic acid receptor could activate gene expression through a thyroid hormone response element. We now report that a human retinoic acid receptor expressed from cloned complementary DNA or the endogenous retinoic acid receptor present in F9 teratocarcinoma cells can activate gene expression from promoters fused to a natural or synthetic thyroid hormone response element. The product translated in vitro from the human retinoic acid receptor cDNA can bind to a thyroid hormone response element with high affinity. The unexpected implication of these findings is that retinoic acid and thyroid hormones, acting through their respective receptors, could control overlapping gene networks involved in the regulation of vertebrate morphogenesis and homeostasis.

摘要

对类固醇受体的研究已导致鉴定出一类配体诱导性调节蛋白超家族,其中包括甲状腺激素和视黄酸的受体。该受体家族通过与称为激素反应元件的短顺式作用序列结合来调节基因表达。鉴定功能性视黄酸反应元件对于我们理解视黄酸受体激活基因表达并调节细胞分化的机制至关重要。此类研究的一个障碍是缺乏任何转录直接依赖于受体 - 激素复合物的已鉴定基因。由于视黄酸受体和甲状腺激素受体的DNA结合结构域高度相关(其氨基酸序列62%相同),我们研究了视黄酸受体是否可以通过甲状腺激素反应元件激活基因表达的可能性。我们现在报告,从克隆的互补DNA表达的人视黄酸受体或存在于F9畸胎瘤细胞中的内源性视黄酸受体可以激活与天然或合成甲状腺激素反应元件融合的启动子的基因表达。从人视黄酸受体cDNA体外翻译的产物可以高亲和力结合甲状腺激素反应元件。这些发现的意外含义是,视黄酸和甲状腺激素通过它们各自的受体,可能控制参与脊椎动物形态发生和体内平衡调节的重叠基因网络。

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