Thorne LB et al. (2008), Protein expression of the transcriptional regul...

XB-ART-36201

J Mol Histol 2008 Feb 01;391:15-24. doi: 10.1007/s10735-007-9116-3.

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Protein expression of the transcriptional regulator MI-ER1 alpha in adult mouse tissues.

Thorne LB , McCarthy PL , Paterno GD , Gillespie LL .

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MI-ER1 is a novel transcriptional regulator that plays a critical role in embryonic development and is differentially expressed in breast carcinoma. The MI-ER1 protein sequence is highly conserved among species, with 95% identity between mouse and humans and 72% between Xenopus and mouse. There are two major protein isoforms, MI-ER1alpha and MI-ER1beta, which differ in the sequence of their C-terminus. MI-ER1alpha is of particular interest because it contains a consensus LXXLL nuclear receptor interaction motif and the current study was undertaken to determine the expression pattern of MI-ER1alpha protein in adult mouse tissues. Immunohistochemical analysis of paraffin-embedded tissue using an MI-ER1alpha-specific antibody revealed that the majority of mouse adult tissues examined showed very weak or no immunoreactivity; these included tissues of the lung, liver, intestine, uterus, spleen, lymph node, bladder as well as skeletal muscle. Interestingly, a subset of endocrine tissues displayed intense staining for MI-ER1alpha. Specifically, the islets of Langerhans, the zona glomerulosa and medulla of the adrenal gland, the ovary and the hypothalamus were intensely stained. In addition, both anterior and posterior pituitary showed moderate immunoreactivity, as did the parafollicular cells of the thyroid gland and Leydig cells and spermatids in the testes. Negative endocrine tissues included follicular cells of the thyroid gland and the X zone of the adrenal cortex. A few non-endocrine tissues displayed moderate immunoreactivity; these included all tubules and collecting ducts in the kidney, myocardial and endocardial layers of the heart, the hippocampal formation, pyramidal neurons in the cortex and the ductal epithelium of the mammary gland. In all cases, MI-ER1alpha immunoreactivity was cytoplasmic. This study represents the first immunohistochemical analysis of MI-ER1alpha expression in mammals and our data suggest that this transcriptional regulator plays a role in specific endocrine pathways.

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Species referenced: Xenopus
Genes referenced: mier1

References [+] :

Aasland, The SANT domain: a putative DNA-binding domain in the SWI-SNF and ADA complexes, the transcriptional co-repressor N-CoR and TFIIIB. 1996, Pubmed

Aasland, The SANT domain: a putative DNA-binding domain in the SWI-SNF and ADA complexes, the transcriptional co-repressor N-CoR and TFIIIB. 1996, Pubmed
Bielohuby, Growth analysis of the mouse adrenal gland from weaning to adulthood: time- and gender-dependent alterations of cell size and number in the cortical compartment. 2007, Pubmed
Ding, Human MI-ER1 alpha and beta function as transcriptional repressors by recruitment of histone deacetylase 1 to their conserved ELM2 domain. 2003, Pubmed , Xenbase
Ding, The SANT domain of human MI-ER1 interacts with Sp1 to interfere with GC box recognition and repress transcription from its own promoter. 2004, Pubmed
Heery, A signature motif in transcriptional co-activators mediates binding to nuclear receptors. 1997, Pubmed
Hirokawa, Electron microscopic observations on postnatal development of the X zone in mouse adrenal cortex. 1974, Pubmed
Hishikawa, Molecular histochemical analysis of estrogen receptor alpha and beta expressions in the mouse ovary: in situ hybridization and Southwestern histochemistry. 2003, Pubmed
Hörlein, Ligand-independent repression by the thyroid hormone receptor mediated by a nuclear receptor co-repressor. 1995, Pubmed
Jiao, A simple and sensitive antigen retrieval method for free-floating and slide-mounted tissue sections. 1999, Pubmed
Keegan, Recent insights into organogenesis of the adrenal cortex. 2002, Pubmed
Muramatsu, Estrogen receptors: how do they control reproductive and nonreproductive functions? 2000, Pubmed
Pascual-Le Tallec, The mineralocorticoid receptor: a journey exploring its diversity and specificity of action. 2005, Pubmed
Paterno, Molecular cloning of human er1 cDNA and its differential expression in breast tumours and tumour-derived cell lines. 1998, Pubmed , Xenbase
Paterno, Genomic organization of the human mi-er1 gene and characterization of alternatively spliced isoforms: regulated use of a facultative intron determines subcellular localization. 2002, Pubmed , Xenbase
Paterno, cDNA cloning of a novel, developmentally regulated immediate early gene activated by fibroblast growth factor and encoding a nuclear protein. 1997, Pubmed , Xenbase
Post, Nuclear localization signals in the Xenopus FGF embryonic early response 1 protein. 2001, Pubmed , Xenbase
Sanyal, Differential regulation of the orphan nuclear receptor small heterodimer partner (SHP) gene promoter by orphan nuclear receptor ERR isoforms. 2002, Pubmed
Sertznig, Present concepts and future outlook: function of peroxisome proliferator-activated receptors (PPARs) for pathogenesis, progression, and therapy of cancer. 2007, Pubmed
Solari, The Caenorhabditis elegans genes egl-27 and egr-1 are similar to MTA1, a member of a chromatin regulatory complex, and are redundantly required for embryonic patterning. 1999, Pubmed
Teplitsky, Proline365 is a critical residue for the activity of XMI-ER1 in Xenopus embryonic development. 2003, Pubmed , Xenbase
Thorne, Cloning and characterization of the mouse ortholog of mi-er1. 2005, Pubmed , Xenbase
Wilkinson-Berka, COX-2 inhibition and retinal angiogenesis in a mouse model of retinopathy of prematurity. 2003, Pubmed