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  4. Competitive promoter-associated matrix attachment region binding of the Arid3a and Cux1 transcription factors
 
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2017
Journal Article
Title

Competitive promoter-associated matrix attachment region binding of the Arid3a and Cux1 transcription factors

Abstract
Arid3a/Bright/Dril1 is a B cell-specific transactivator that regulates immunoglobulin heavy chain (IgH) gene transcription by binding promoter and enhancer-associated matrix attachment regions (MARs) within the IgH gene locus. Promoter MAR-mediated Arid3a transactivation is antagonized by direct competition of MAR binding by Cux1/CDP-a ubiquitously expressed repressor originally termed NF-mNR. We report that the NF-mNR complex includes Arid3a in B cells but not in non-B cells through mobility shift assays. The binding activity of NF-mNR and Arid3a in B cells is reciprocally altered during the cell division cycle and by the B cell mitogen lipopolysaccharide LPS. LPS treatment had no effect on Arid3a localization but increased its total abundance within the nucleus and cytoplasm. We show that this increased level of Arid3a is capable of displacing Cux from the MARs to facilitate IgH gene transcription. Finally, we showed that the MARs (termed Bf150 and Tx125) associated with the VH1 rearranged variable region expressed in the S107 murine plasmacytoma, can repress reporter gene transcription in non-B cells and that they can relieve the repression mediated by Em enhancer in B cells. These results have significant implications for early human development and demonstrate that MARs in IgH locus, NF-µNR and Arid3a regulate IgH gene expression in a concerted fashion. This paves the way for future studies examining the misregulation of this pathway in pediatric disease.
Author(s)
Kim, Dongkyoon
Atreca, Inc., Redwood City, CA 94063, USA
Schmidt, Christian
Fraunhofer-Institut für Angewandte Polymerforschung IAP  
Brown, Mark A.
Colorado State University, Fort Collins, CO 80523, USA
Tucker, Haley
University of Texas at Austin, Austin, TX 78715, USA
Journal
Diseases  
Open Access
File(s)
Download (1.72 MB)
Rights
CC BY 4.0: Creative Commons Attribution
DOI
10.3390/diseases5040034
10.24406/publica-r-250792
Additional link
Full text
Language
English
Fraunhofer-Institut für Angewandte Polymerforschung IAP  
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