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Download Heterochromatin silencing at p53 target genes by a small viral protein.
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Heterochromatin silencing at p53 target genes by a small viral protein. p53 Revealed character as a tumor suppressor gene in 1989. Tumor suppressor protein. Encoded by the TP53 gene. Preventing tumor development. Inhibit overexpression of cell. Regulate to cell cycle. p53 pathway E1B-55K 55kDa protein. Encoded by E1B genomic region of adenovirus. Binds to p53 and functionally inactivates it. Inhibit cell death by apoptosis. ONYX-015 Oncolytic adenoviral therapy Deleted E1B-55K Trialed as a possible treatment for cancer. Be directly injected into a tumor. Combined with chemotherapy Result ▶Fig 1. p53 is induced and phosphorylated in ΔE1B-55k infection but p53 activity is dominantly suppressed. Result ▶Fig 1. p53 is induced and phosphorylated in ΔE1B-55k infection but p53 activity is dominantly suppressed. Result ▶Fig 2. E4-ORF3 inactivates p53 independently of E1B-55k and p53 degradation. Result ▶Fig 2. E4-ORF3 inactivates p53 independently of E1B-55k and p53 degradation. Result ▶Fig 3. E4-ORF3 induces heterochromatin formation and prevents p53-DNA binding at endogenous promoters. Result ▶Fig 3. E4-ORF3 induces heterochromatin formation and prevents p53-DNA binding at endogenous promoters. Result ▶Fig 3. E4-ORF3 induces heterochromatin formation and prevents p53-DNA binding at endogenous promoters. Result ▶Fig 4. E4-ORF3 forms a nuclear scaffold that specifies heterochromatin assembly and H3K9 trimethylation at p53 target promoters. Result ▶Fig 4. E4-ORF3 forms a nuclear scaffold that specifies heterochromatin assembly and H3K9 trimethylation at p53 target promoters. Result ▶Fig 5. p53 transcriptional targets are silenced selectively in the backdrop of global transcriptional changes that drive oncogenic cellular and viral replication. Result ▶Fig 5. p53 transcriptional targets are silenced selectively in the backdrop of global transcriptional changes that drive oncogenic cellular and viral replication. Discussion • p53 induction and phosphorylation is tantamount to p53 activity, which is the premise for several cancer therapies. • Identified, E4-ORF3, directing SUV39H1/2 H3K9me3 heterochromatin assembly at p53 target promoters to silence p53 activated transcription in response to genotoxic and oncogenic stress. Discussion • All of the known targets of E4-ORF3, PML, the MRN DNA damage/repair complex and Tif1α are subverted by tumor mutations. • Identification of E4-ORF3 changes the fundamental definition of how p53 is inactivated in adenovirus infected cells, which is a critical mechanistic insight that could now enable the rational development of true p53 tumor selective adenoviral therapies.
