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甲状腺激素受体亚型的负向和正向转录调控。

Negative and positive transcriptional regulation by thyroid hormone receptor isoforms.

作者信息

Rentoumis A, Chatterjee V K, Madison L D, Datta S, Gallagher G D, Degroot L J, Jameson J L

机构信息

Thyroid Unit, Massachusetts General Hospital, Boston 02114.

出版信息

Mol Endocrinol. 1990 Oct;4(10):1522-31. doi: 10.1210/mend-4-10-1522.

DOI:10.1210/mend-4-10-1522
PMID:2284000
Abstract

Multiple forms of human thyroid hormone (T3) receptor have been identified, including true receptors that bind T3 (alpha 1 and beta) and a splicing variant (alpha 2) that does not bind T3. The alpha 1- and beta-receptors activate transcription through interactions with positive thyroid response elements (TREs). The alpha 2 variant is unable to activate transcription and has been reported to inhibit alpha 1 or beta stimulation of positive TREs, a property referred to as dominant negative activity. In this report we have performed studies to assess the functional properties of different members of the thyroid receptor family with regard to both positive and negative transcriptional regulation. The alpha 1-, alpha 2-, and beta-receptors were each coexpressed in JEG-3 cells with either TreTKCAT (CAT = chloramphenicol acetyltransferase), a reporter gene that contains a positive TRE, or TSH alpha CAT, a negatively regulated reporter gene. The alpha 1 and beta isoforms stimulated transcription of TreTKCAT and inhibited TSH alpha CAT transcription in a T3-dependent manner, whereas the alpha 2 variant was inactive. When coexpressed with alpha 1- or beta-receptors, alpha 2 inhibited regulation of positive TREs, but the effects of alpha 2 were modest and only occurred when relatively high doses of receptor were transfected. The alpha 2-receptor variant did not affect negative regulation by alpha 1- or beta-receptors. Thus, in both positive and negative regulation, thyroid hormone receptor isoforms that bind T3 (alpha 1, beta) are functional, whereas the alpha 2 isoform, which does not bind T3, is not functional.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

已鉴定出多种形式的人甲状腺激素(T3)受体,包括与T3结合的真正受体(α1和β)以及不与T3结合的剪接变体(α2)。α1和β受体通过与正向甲状腺反应元件(TRE)相互作用来激活转录。α2变体无法激活转录,据报道它会抑制α1或β对正向TRE的刺激,这种特性被称为显性负活性。在本报告中,我们进行了研究,以评估甲状腺受体家族不同成员在正向和负向转录调控方面的功能特性。α1、α2和β受体分别在JEG - 3细胞中与TreTKCAT(CAT = 氯霉素乙酰转移酶,一种含有正向TRE的报告基因)或TSHαCAT(一种负向调控的报告基因)共表达。α1和β异构体以T3依赖的方式刺激TreTKCAT的转录并抑制TSHαCAT的转录,而α2变体无活性。当与α1或β受体共表达时,α₂抑制正向TRE的调控,但α2的作用较小,且仅在转染相对高剂量受体时才会出现。α2受体变体不影响α1或β受体的负向调控。因此,在正向和负向调控中,与T3结合的甲状腺激素受体异构体(α1、β)具有功能,而不与T3结合α2异构体则无功能。(摘要截短于250字)

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