Transglutaminase 2 mediates transcriptional regulation through BAF250a polyamination.

Genes Genomics

Department of Biochemistry and Molecular Biology, Seoul National University College of Medicine, 103 Daehak-ro, Jongno-gu, Seoul, 03080, Korea.

Published: April 2021

AI Article Synopsis

  • Transglutaminase 2 (TG2) plays a crucial role in cellular stress responses by modifying proteins, influencing processes like apoptosis and inflammation.
  • Through a yeast two-hybrid assay, this study identified BAF250a, part of the chromatin remodeling complex, as a TG2-interacting protein.
  • The findings demonstrate that TG2 enhances transcriptional activity via polyamine incorporation into BAF250a, affecting the expression of glucocorticoid response genes in hepatocytes.

Article Abstract

Background: Transglutaminase 2 (TG2) mediates protein modifications by crosslinking or by incorporating polyamine in response to oxidative or DNA-damaging stress, thereby regulating apoptosis, extracellular matrix formation, and inflammation. The regulation of transcriptional activity by TG2-mediated histone serotonylation or by Sp1 crosslinking may also contribute to cellular stress responses.

Objective: In this study, we attempted to identify TG2-interacting proteins to better understand the role of TG2 in transcriptional regulation.

Methods: Using a yeast two-hybrid assay to screen a HeLa cell cDNA library, we found that TG2 bound BAF250a, a core subunit of the cBAF chromatin remodeling complex, through an interaction between the TG2 barrel 1 and BAF250a C-terminal domains.

Results: TG2 was pulled down with a GST-BAF250a C-term fusion protein. Moreover, TG2 and BAF250a were co-fractionated using P11 chromatography, and co-immunoprecipitated. A transamidation reaction showed that TG2 mediated incorporation of polyamine into BAF250a. In glucocorticoid response-element reporter-expressing cells, TG2 overexpression increased the luciferase reporter activity in a transamidation-dependent manner. In addition, a comparison of genome-wide gene expression between wild-type and TG2-deficient primary hepatocytes in response to dexamethasone treatment showed that TG2 further enhanced or suppressed the expression of dexamethasone-regulated genes that were identified by a gene ontology enrichment analysis.

Conclusion: Thus, our results indicate that TG2 regulates transcriptional activity through BAF250a polyamination.

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Source
http://dx.doi.org/10.1007/s13258-021-01055-6DOI Listing

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