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Published November 27, 2000 | public
Journal Article

Modulation of early growth response (EGR) transcription factor-dependent gene expression by using recombinant adenovirus

Abstract

Early growth response (EGR) transcription factors link initial cytoplasmic events to long-term alterations of cellular gene expression and are induced by various stimuli. To test their roles in cell physiology, we constructed adenoviral recombinants encoding NGFI-A binding protein 2 (NAB2, a repressor of EGR1, EGR2, and EGR3), EGR1, NAB-insensitive EGR1(I293F) (EGR1∗), EGR2, and the NAB-binding, repressive domain 1 (R1) of EGR1. These viruses regulated EGR-dependent expression of GFP and luciferase reporter genes in heterologous expression assays. Infection of a myoblast cell line with EGR1 and EGR1∗ adenovirus induced the endogenous gene for platelet-derived growth factor A chain (PDGF-A). In addition, in neuroblastoma cells, the two novel EGR1 target genes EGR3 and NAB2 were identified by using adenoviral transfer of EGR1 and EGR1∗. Our results demonstrate that recombinant adenovirus is useful to regulate heterologous and endogenous EGR target gene expression, and suggest that EGR transcription factors can autoregulate themselves.

Additional Information

© 2000 Elsevier. Received 16 June 2000, Revised 15 September 2000, Accepted 28 September 2000, Available online 4 December 2000. We thank Dr Jeffrey Milbrandt and Dr John Svaren for providing A2ProLuc and the cDNAs for EGR1, EGR1∗, EGR2, NAB2, R1, and R1∗, Dr Barbara J. Wold and Dr Jeong Kyo Yoon for the sGFP cDNA, Anita Buchli for the Neuro-2a cells, Susanne Erb for the C2C12 cells, Dr Hanns Möhler and Laura Huopaniemi for supporting the TaqMan PCR, and Dr John Svaren and Dr Sondra Schlesinger for helpful discussions and comments on the manuscript. This work was supported by the Swiss National Science Foundation (grant no. 31-57′125.99 to MUE, and fellowship no. 823A-053469 to CML), the National Institute of Mental Health (grant to ND), and by the Donald E. and Delia B. Baxter Foundation (fellowship to MUE).

Additional details

Created:
August 21, 2023
Modified:
October 20, 2023