Literature DB >> 20702774

IRF2BP2 is a skeletal and cardiac muscle-enriched ischemia-inducible activator of VEGFA expression.

Allen C T Teng1, Drew Kuraitis, Shelley A Deeke, Ali Ahmadi, Stephen G Dugan, Brian L M Cheng, Matthew G Crowson, Patrick G Burgon, Erik J Suuronen, Hsiao-Huei Chen, Alexandre F R Stewart.   

Abstract

We sought to identify an essential component of the TEAD4/VGLL4 transcription factor complex that controls vascular endothelial growth factor A (VEGFA) expression in muscle. A yeast 2-hybrid screen was used to clone a novel component of the TEAD4 complex from a human heart cDNA library. We identified interferon response factor 2 binding protein 2 (IRF2BP2) and confirmed its presence in the TEAD4/VGLL4 complex in vivo by coimmunoprecipitation and mammalian 2-hybrid assays. Coexpression of IRF2BP2 with TEAD4/VGLL4 or TEAD1 alone potently activated, whereas knockdown of IRF2BP2 reduced, VEGFA expression in C(2)C(12) muscle cells. Thus, IRF2BP2 is required to activate VEGFA expression. In mouse embryos, IRF2BP2 was ubiquitously expressed but became progressively enriched in the fetal heart, skeletal muscles, and lung. Northern blot analysis revealed high levels of IRF2BP2 mRNA in adult human heart and skeletal muscles, but immunoblot analysis showed low levels of IRF2BP2 protein in skeletal muscle, indicating post-transcriptional regulation of IRF2BP2 expression. IRF2BP2 protein levels are markedly increased by ischemia in skeletal and cardiac muscle compared to normoxic controls. IRF2BP2 is a novel ischemia-induced coactivator of VEGFA expression that may contribute to revascularization of ischemic cardiac and skeletal muscles.

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Year:  2010        PMID: 20702774     DOI: 10.1096/fj.10-167049

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  32 in total

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3.  A novel transcription complex that selectively modulates apoptosis of breast cancer cells through regulation of FASTKD2.

Authors:  Kay T Yeung; Sharmistha Das; Jin Zhang; Alejandro Lomniczi; Sergio R Ojeda; Chong-Feng Xu; Thomas A Neubert; Herbert H Samuels
Journal:  Mol Cell Biol       Date:  2011-03-28       Impact factor: 4.272

4.  Transcription of the human EAP1 gene is regulated by upstream components of a puberty-controlling Tumor Suppressor Gene network.

Authors:  Johanna K Mueller; Ines Koch; Alejandro Lomniczi; Alberto Loche; Tomke Rulfs; Juan M Castellano; Wieland Kiess; Sergio Ojeda; Sabine Heger
Journal:  Mol Cell Endocrinol       Date:  2011-12-19       Impact factor: 4.102

5.  Mutation in IRF2BP2 is responsible for a familial form of common variable immunodeficiency disorder.

Authors:  Michael D Keller; Rahul Pandey; Dong Li; Joseph Glessner; Lifeng Tian; Sarah E Henrickson; Ivan K Chinn; Linda Monaco-Shawver; Jennifer Heimall; Cuiping Hou; Frederick G Otieno; Soma Jyonouchi; Leonard Calabrese; Joris van Montfrans; Jordan S Orange; Hakon Hakonarson
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6.  Hypothalamic EAP1 (enhanced at puberty 1) is required for menstrual cyclicity in nonhuman primates.

Authors:  Gregory A Dissen; Alejandro Lomniczi; Sabine Heger; Tanaya L Neff; Sergio R Ojeda
Journal:  Endocrinology       Date:  2011-11-29       Impact factor: 4.736

7.  Pits and CtBP Control Tissue Growth in Drosophila melanogaster with the Hippo Pathway Transcription Repressor Tgi.

Authors:  Joseph H A Vissers; Lucas G Dent; Colin M House; Shu Kondo; Kieran F Harvey
Journal:  Genetics       Date:  2020-03-02       Impact factor: 4.562

Review 8.  VGLL4 is a transcriptional cofactor acting as a novel tumor suppressor via interacting with TEADs.

Authors:  Xiaochong Deng; Lin Fang
Journal:  Am J Cancer Res       Date:  2018-06-01       Impact factor: 6.166

9.  Sex differences in gene expression in response to ischemia in the human left ventricular myocardium.

Authors:  Gregory Stone; Ashley Choi; Oliva Meritxell; Joshua Gorham; Mahyar Heydarpour; Christine E Seidman; Jon G Seidman; Sary F Aranki; Simon C Body; Vincent J Carey; Benjamin A Raby; Barbara E Stranger; Jochen D Muehlschlegel
Journal:  Hum Mol Genet       Date:  2019-05-15       Impact factor: 6.150

10.  Cdk5 disruption attenuates tumor PD-L1 expression and promotes antitumor immunity.

Authors:  R Dixon Dorand; Joseph Nthale; Jay T Myers; Deborah S Barkauskas; Stefanie Avril; Steven M Chirieleison; Tej K Pareek; Derek W Abbott; Duncan S Stearns; John J Letterio; Alex Y Huang; Agne Petrosiute
Journal:  Science       Date:  2016-07-21       Impact factor: 47.728

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