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Papers In Press, published online ahead of print February 9, 2005
Vet. Microbiology, WCVM, University of Saskatchewan, Saskatoon, Saskatchewan S7N5B4
Corresponding Author: vikram.misra{at}usask.ca
Host cell factor (HCF) was initially discovered as a cellular co-factor required for the activation of herpes simplex virus immediate early gene expression by the virion associated transactivator VP16. HCF also participates in a variety of cellular processes although the mechanism of its action is not known. VP16 binds to HCF through a four amino acid motif (EHAY), which closely resembles the HCF binding domain of two cellular basic leucine-zipper proteins Luman and Zhangfei. Luman is a powerful transcription factor that, in transient expression assays, activates promoters containing cyclic AMP or unfolded protein response elements (UPRE). In contrast, Zhangfei neither binds consensus recognition elements for basic leucine-zipper proteins nor does it activate promoters containing them. Here we show that Zhangfei suppresses the ability of Luman to activate transcription. HCF appeared to be required for efficient suppression. A mutant of Zhangfei, which was unable to bind HCF, was impaired in its ability to suppress Luman. Zhangfei did not suppress ATF6, a transcription factor closely related to Luman but which does not bind HCF, unless the HCF-binding motif of Luman was grafted on to it. Zhangfei inhibited the HCF-dependant activation of a UPRE containing promoter by a Gal4-Luman fusion protein but was unable to inhibit the HCF-independent activation by Gal4-Luman of a promoter that contained Gal4 binding motifs. Binding of HCF by Zhangfei was required for the co-localization of Luman and Zhangfei to nuclear domains, suggesting that HCF might target the proteins to a common location.
J. Biol. Chem, 10.1074/jbc.M500728200
Submitted on January 20, 2005
Revised on February 7, 2005
Accepted on February 9, 2005
Zhangfei is a potent and specific inhibitor of the Host cell factor-binding transcription factor luman
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