Gadd45β is an inducible coactivator of transcription that facilitates rapid liver growth in mice
Jianmin Tian, Haiyan Huang, Barbara Hoffman, Dan A. Liebermann, Giovanna M. Ledda-Columbano, Amedeo Columbano, Joseph Locker
Jianmin Tian, Haiyan Huang, Barbara Hoffman, Dan A. Liebermann, Giovanna M. Ledda-Columbano, Amedeo Columbano, Joseph Locker
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Research Article Hepatology

Gadd45β is an inducible coactivator of transcription that facilitates rapid liver growth in mice

Abstract

The growth arrest and DNA damage–inducible 45 (Gadd45) proteins act in many cellular processes. In the liver, Gadd45b (encoding Gadd45β) is the gene most strongly induced early during both compensatory regeneration and drug-induced hyperplasia. The latter response is associated with the dramatic and rapid hepatocyte growth that follows administration of the xenobiotic TCPOBOP (1,4-bis[2-(3,5)-dichoropyridyloxy] benzene), a ligand of the nuclear receptor constitutive androstane receptor (CAR). Here, we have shown that Gadd45b–/– mice have intact proliferative responses following administration of a single dose of TCPOBOP, but marked growth delays. Moreover, early transcriptional stimulation of CAR target genes was weaker in Gadd45b–/– mice than in wild-type animals, and more genes were downregulated. Gadd45β was then found to have a direct role in transcription by physically binding to CAR, and TCPOBOP treatment caused both proteins to localize to a regulatory element for the CAR target gene cytochrome P450 2b10 (Cyp2b10). Further analysis defined separate Gadd45β domains that mediated binding to CAR and transcriptional activation. Although baseline hepatic expression of Gadd45b was broadly comparable to that of other coactivators, its 140-fold stimulation by TCPOBOP was striking and unique. The induction of Gadd45β is therefore a response that facilitates increased transcription, allowing rapid expansion of liver mass for protection against xenobiotic insults.

Authors

Jianmin Tian, Haiyan Huang, Barbara Hoffman, Dan A. Liebermann, Giovanna M. Ledda-Columbano, Amedeo Columbano, Joseph Locker

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Figure 4

Transcriptional coactivation by Gadd45β.

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Transcriptional coactivation by Gadd45β. (A) Direct binding of CAR to Ga...
(A) Direct binding of CAR to Gadd45β. A plasmid expressing a GST-binding domain fused to full-length Gadd45β was expressed in E. coli. Fusion protein or a control GST-binding domain protein was bound to glutathione agarose beads and then incubated with 35S-CAR prepared by cell free translation. After wash, the bound protein was eluted and resolved by acrylamide gel electrophoresis. The control lane contained a 20% input fraction. (B) Comparison of coactivation by Gadd45β and Ncoa1. Cotransfection experiments were set up with a limiting amount of CAR expression plasmid (10 ng) to display maximal coactivation. (C) Inhibition of coactivation by ketoconazole (25 μM). Transfection assays used 10 ng CAR, 100 ng Ncoa1, or Gadd45β expression plasmids. (D) Intrinsic activation by DNA-bound Gadd45β. A plasmid expressing a Gal4-DBD fused to the N terminus of full-length Gadd45β was cotransfected with a Gal4 site LUC reporter, with and without ketoconazole. The strong generic activator Gal4-VP16 (100 ng) is also shown for comparison. (BD) Data are mean ± SD of duplicate assays in HepG2 cells.