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首页> 外文期刊>Nucleic Acids Research >Retinoic acid receptor alpha 1 variants, RAR alpha 1 Delta B RAR alpha 1 Delta BC, define a new class of nuclear receptor isoforms
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Retinoic acid receptor alpha 1 variants, RAR alpha 1 Delta B RAR alpha 1 Delta BC, define a new class of nuclear receptor isoforms

机译:维甲酸受体α1变体,RARα1Delta B,RARα1Delta BC,定义了一类新的核受体同工型

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摘要

Retinoic acid (RA) binds and activates retinoid X receptor (RXR)/retinoic acid receptor (RAR) heterodimers, which regulate the transcription of genes that have retinoic acid response elements (RARE). The RAR isotypes (alpha, beta and gamma) are comprised of six regions designated A-F. Two isoforms of RAR alpha, 1 and 2, have been identified in humans, which have different A regions generated by differential promoter usage and alternative splicing. We have isolated two new splice variants of RAR alpha1 from human B lymphocytes. In one of these variants, exon 2 is juxtaposed to exon 5, resulting in an altered reading frame and a stop codon. This variant, designated RAR alpha1 DeltaB, does not code for a functional receptor. In the second variant, exon 2 is juxtaposed to exon 6, maintaining the reading frame. This isoform, designated RAR alpha1 Delta BC, retains most of the functional domains of RAR alpha1, but omits the transactivation domain AF-1 and the DNA-binding domain. Consequently, it does not bind nor transactivate RARE on its own. Nevertheless, RAR alpha1 Delta BC interacts with RXR alpha and, as an RXR alpha /RAR alpha1 Delta BC heterodimer, transactivates the DR5 RARE upon all-trans-RA binding. The use of RAR- and RXR-specific ligands shows that, whereas transactivation of the DR5 RARE through the RXR alpha /RAR alpha1 heterodimer is mediated only by RAR ligands, transactivation through the RXR alpha /RAR alpha1 Delta BC heterodimer is mediated by RAR and RXR ligands. Whilst RAR alpha1 has a broad tissue distribution, RAR alpha1 Delta BC has a more heterogeneous distribution, but with significant expression in myeloid cells. RAR alpha1 Delta BC is an infrequent example of a functional nuclear receptor which deletes the DNA-binding domain.
机译:视黄酸(RA)结合并激活类视黄醇X受体(RXR)/视黄酸受体(RAR)异二聚体,后者调节具有视黄酸反应元件(RARE)的基因的转录。 RAR同种型(α,β和γ)由六个指定为A-F的区域组成。在人类中已经鉴定出RAR alpha的两个同工型1和2,它们具有不同的A区,这些A区是通过不同的启动子用法和选择性剪接产生的。我们从人B淋巴细胞中分离了RAR alpha1的两个新剪接变体。在这些变体中的一种中,外显子2与外显子5并列,导致改变的阅读框和终止密码子。命名为RAR alpha1 DeltaB的此变体不编码功能性受体。在第二变体中,外显子2与外显子6并列,维持阅读框。这种同种型称为RAR alpha1 Delta BC,保留了RAR alpha1的大部分功能域,但省略了反式激活域AF-1和DNA结合域。因此,它不会单独绑定或激活RARE。然而,RAR alpha1 Delta BC与RXR alpha相互作用,并且作为RXR alpha / RAR alpha1 Delta BC异二聚体,在全反式RA结合后可激活DR5 RARE。 RAR和RXR特异性配体的使用表明,尽管通过RXR alpha / RAR alpha1异二聚体介导的DR5 RARE的反式激活仅由RAR配体介导,但通过RXR alpha / RAR alpha1 Delta BC异源二聚体的反式激活是由RAR和RXR配体。尽管RAR alpha1具有较宽的组织分布,但RAR alpha1 Delta BC具有较不均匀的分布,但在髓样细胞中具有明显的表达。 RAR alpha1 Delta BC是删除核糖核酸结合结构域的功能性核受体的罕见例子。

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