2009
DOI: 10.1073/pnas.0901521106
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Human papillomavirus 16 E7 inactivator of retinoblastoma family proteins complements human cytomegalovirus lacking UL97 protein kinase

Abstract: Several different families of DNA viruses encode proteins that inactivate the cellular retinoblastoma tumor suppressor protein (pRb), which normally functions to bind E2F transcription factors and restrict expression of genes necessary for cellular processes including DNA replication. Human cytomegalovirus (HCMV) UL97, a protein kinase functionally orthologous to cellular cyclin-dependent kinases, phosphorylates pRb on inactivating residues during HCMV infection. To assess if such phosphorylation is biological… Show more

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Cited by 35 publications
(82 citation statements)
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“…Following this, PCR primers with sequences to facilitate homologous recombination into the viral genome (see supplemental Table S1 at our website, https://coen.med.harvard.edu) were used to amplify the D/N GFP-lamin A sequence containing the ISce-AphAI (KanaR) region from the plasmid pGFP-dhead-caax-KanS. The PCR product was gel purified and electroporated into GS1783 cells harboring either WT_E7 AD169rv (16) or WT AD169rv BAC. Kanamycin-resistant integrates were resolved by heat shock and L-(ϩ)-arabinose induction of I-SceI, and the resulting BACs were sequenced to confirm the introduced changes.…”
Section: Methodsmentioning
confidence: 99%
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“…Following this, PCR primers with sequences to facilitate homologous recombination into the viral genome (see supplemental Table S1 at our website, https://coen.med.harvard.edu) were used to amplify the D/N GFP-lamin A sequence containing the ISce-AphAI (KanaR) region from the plasmid pGFP-dhead-caax-KanS. The PCR product was gel purified and electroporated into GS1783 cells harboring either WT_E7 AD169rv (16) or WT AD169rv BAC. Kanamycin-resistant integrates were resolved by heat shock and L-(ϩ)-arabinose induction of I-SceI, and the resulting BACs were sequenced to confirm the introduced changes.…”
Section: Methodsmentioning
confidence: 99%
“…Kanamycin-resistant integrates were resolved by heat shock and L-(ϩ)-arabinose induction of I-SceI, and the resulting BACs were sequenced to confirm the introduced changes. For the WT HCMV construct (WT LMN ⌬H/C AD169rv), the mutated GFPlamin A sequences were cloned under the control of a duplicated UL97 promoter (described previously [16]) in the unique short (U S ) region of the HCMV genome within an intergenic locus between US9 and US10 by replacing the previously described human papillomavirus E7 gene cloned in that region (16). For the UL97 null (⌬97) HCMV construct (⌬97 LMN ␣-helical "rod" domains flanked by the head and tail domains, with a CaaX domain at the carboxyl terminus that is a site for isoprenylation.…”
Section: Methodsmentioning
confidence: 99%
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