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小鼠α和β维甲酸受体以及一种主要在皮肤中表达的新型γ受体的克隆。

Cloning of murine alpha and beta retinoic acid receptors and a novel receptor gamma predominantly expressed in skin.

作者信息

Zelent A, Krust A, Petkovich M, Kastner P, Chambon P

机构信息

Laboratoire de Génétique Moléculaire des Eucaryotes du CNRS, Strasbourg, France.

出版信息

Nature. 1989 Jun 29;339(6227):714-7. doi: 10.1038/339714a0.

Abstract

In addition to having profound effects on embryonic pattern formation, retinoic acid (RA) has striking effects on differentiation and maintenance of epithelial cells in vivo and in vitro Skin is a major target organ for retinoids both in its normal and pathological states. The discovery of two human nuclear receptors for RA (hRAR alpha and hRAR beta) acting as transcriptional RA-inducible enhancer factors has provided a basis for understanding how RA controls gene expression. To investigate the specific role that RARs might play during development and in adult tissues, we have cloned the mouse RAR alpha and RAR beta (mRAR alpha and mRAR beta). Their amino-acid sequences are much more homologous to those of hRAR alpha and hRAR beta, respectively, than to each other, which suggests strongly that RAR alpha- and beta-subtypes have different functions. Most interestingly we have discovered a novel RAR subtype (mRAR gamma) whose expression in adult mouse seems to be highly restricted to skin, whereas RAR alpha and RAR beta are expressed in a variety of adult tissues. Furthermore, both mRAR alpha and mRAR gamma RNAs are readily detected in undifferentiated F9 embryocarcinoma (EC) cells, whereas mRAR beta messenger RNA is induced at least 30-fold in RA-differentiated F9 cells.

摘要

除了对胚胎模式形成有深远影响外,视黄酸(RA)在体内和体外对上皮细胞的分化和维持也有显著作用。皮肤无论是在正常状态还是病理状态下都是类视黄醇的主要靶器官。两种作为转录RA诱导增强因子的人类RA核受体(hRARα和hRARβ)的发现,为理解RA如何控制基因表达提供了基础。为了研究RARs在发育过程和成年组织中可能发挥的特定作用,我们克隆了小鼠RARα和RARβ(mRARα和mRARβ)。它们的氨基酸序列彼此之间的同源性,分别比与hRARα和hRARβ的同源性低得多,这强烈表明RARα和β亚型具有不同的功能。最有趣的是,我们发现了一种新的RAR亚型(mRARγ),其在成年小鼠中的表达似乎高度局限于皮肤,而RARα和RARβ在多种成年组织中表达。此外,在未分化的F9胚胎癌细胞中很容易检测到mRARα和mRARγ的RNA,而在RA分化的F9细胞中,mRARβ信使RNA至少诱导了30倍。

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