Abstract
During adenovirus infection, the emphasis of gene expression switches from early genes to late genes in a highly regulated manner. Two gene products, L4-22K and L4-33K, contribute to this switch by activating the major late transcription unit (MLTU) and regulating the splicing of its transcript. L4-22K and L4-33K expression is driven initially by a recently described L4 promoter (L4P) embedded within the MLTU that is activated by early and intermediate viral factors: E1A, E4 Orf3, and IVa2. Here we show that this promoter is also significantly activated by the cellular stress response regulator, p53. Exogenous expression of p53 activated L4P in reporter assays, while depletion of endogenous p53 inhibited the induction of L4P by viral activators. Chromatin immunoprecipitation studies showed that p53 associates with L4P and that during adenovirus type 5 (Ad5) infection, this association peaks at 12 h postinfection, coinciding with the phase of the infectious cycle when L4P is active, and is then lost as MLP activation commences. p53 activation of L4P is significant during Ad5 infection, since depletion of p53 prior to infection of either immortalized or normal cells led to severely reduced late gene expression. The association of p53 with L4P is transient due to the action of products of L4P activity (L4-22K/33K), which establish a negative feedback loop that ensures the transient activity of L4P at the start of the late phase and contributes to an efficient switch from early- to late-phase virus gene expression.
Highlights
During adenovirus infection, the emphasis of gene expression switches from early genes to late genes in a highly regulated manner
It has previously been reported that adenovirus type 5 (Ad5) L4 promoter (L4P) activity is increased by transfection of fragmented DNA, indicating that this promoter is responsive to at least one cellular factor that is involved in the response to double-strand breaks (DSB) [16]
We have demonstrated that the human tumor suppressor protein p53 contributes to this control by regulating the activity of the L4 promoter, L4P, and entry into the late phase of the Ad5 life cycle
Summary
The emphasis of gene expression switches from early genes to late genes in a highly regulated manner. Upon activation of the MLP, L4-22K and L4-33K contribute to the correct expression of the full repertoire of adenovirus late proteins by influencing the splicing of the MLTU pre-mRNA [10,11,12]; L4-22K cooperates with IVa2 to promote packaging of viral DNA into nascent capsids [7]. Both L422K- and L4-33K-deficient viruses display defects in late gene expression and efficiency of packaging [13,14,15], emphasizing the importance of these proteins for efficient replication at multiple levels. Wright and Leppard infection, E1B-55K acts in conjunction with E4 Orf and cellular cullin 5, among other cellular proteins, to degrade p53 and other cellular targets in a proteasome-dependent manner [26,27,28]
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