Synapse - Genome-wide analysis of Pax8 binding provides new insights into thyroid functions

Genome-wide analysis of Pax8 binding provides new insights into thyroid functions Journal Article

Authors:	Ruiz-Llorente, S.; de Pau, E. C. S.; Sastre-Perona, A.; Montero-Conde, C.; Gomez-Lopez, G.; Fagin, J. A.; Valencia, A.; Pisano, D. G.; Santisteban, P.
Article Title:	Genome-wide analysis of Pax8 binding provides new insights into thyroid functions
Abstract:	Background: The transcription factor Pax8 is essential for the differentiation of thyroid cells. However, there are few data on genes transcriptionally regulated by Pax8 other than thyroid-related genes. To better understand the role of Pax8 in the biology of thyroid cells, we obtained transcriptional profiles of Pax8-silenced PCCl3 thyroid cells using whole genome expression arrays and integrated these signals with global cis-regulatory sequencing studies performed by ChIP-Seq analysis. Results: Exhaustive analysis of Pax8 immunoprecipitated peaks demonstrated preferential binding to intragenic regions and CpG-enriched islands, which suggests a role of Pax8 in transcriptional regulation of orphan CpG regions. In addition, ChIP-Seq allowed us to identify Pax8 partners, including proteins involved in tertiary DNA structure (CTCF) and chromatin remodeling (Sp1), and these direct transcriptional interactions were confirmed in vivo. Moreover, both factors modulate Pax8-dependent transcriptional activation of the sodium iodide symporter (Nis) gene promoter. We ultimately combined putative and novel Pax8 binding sites with actual target gene expression regulation to define Pax8-dependent genes. Functional classification suggests that Pax8-regulated genes may be directly involved in important processes of thyroid cell function such as cell proliferation and differentiation, apoptosis, cell polarity, motion and adhesion, and a plethora of DNA/protein-related processes.Conclusion: Our study provides novel insights into the role of Pax8 in thyroid biology, exerted through transcriptional regulation of important genes involved in critical thyrocyte processes. In addition, we found new transcriptional partners of Pax8, which functionally cooperate with Pax8 in the regulation of thyroid gene transcription. Besides, our data demonstrate preferential location of Pax8 in non-promoter CpG regions. These data point to an orphan CpG island-mediated mechanism that represents a novel role of Pax8 in the transcriptional output of the thyrocyte. © 2012 Ruiz-Llorente et al.; licensee BioMed Central Ltd.
Keywords:	controlled study; promoter region; genetics; nonhuman; protein function; cell proliferation; animal cell; animal; cytology; metabolism; animals; gene targeting; cell function; apoptosis; cell line; small interfering rna; protein binding; rna, small interfering; genetic association; genome-wide association study; cell motion; rna interference; in vivo study; cell differentiation; hela cell; hela cells; transfection; gene expression regulation; genome analysis; drug antagonism; transcription regulation; genetic transfection; microarray analysis; chromatin immunoprecipitation; cpg island; cpg islands; promoter regions, genetic; nucleotide sequence; rat; transcription factor sp1; sp1 transcription factor; cell polarity; binding site; gene control; genome; dna structure; binding sites; rats; gene silencing; thyroid gland; cell adhesion; repressor protein; repressor proteins; chromatin assembly and disassembly; protein dna interaction; paired box transcription factor; paired box transcription factors; sp1; thyroid function; sodium iodide symporter; transcription factor pax8; pax8; chip-seq; cotransporter; symporters; thyroid cell; expression arrays; ctcf; ccctc-binding factor; pax8 protein, rat; transcription factor ctcf
Journal Title:	BMC Genomics
Volume:	13
Issue:	1
ISSN:	1471-2164
Publisher:	Biomed Central Ltd
Date Published:	2012-04-24
Start Page:	147
Language:	English
DOI:	10.1186/1471-2164-13-147
PUBMED:	22531031
PROVIDER:	scopus
PMCID:	PMC3403905
DOI/URL:	http://www.scopus.com/inward/record.url?eid=2-s2.0-84862216535&partnerID=40&md5=13fabb23d8442daaf5741e77ff404777
Notes:	--- - "Cited By (since 1996): 1" - "Export Date: 28 January 2013" - "CODEN: BGMEE" - "Molecular Sequence Numbers: GENBANK: GSE26938;" - "Source: Scopus"

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