FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4382502253> ?p ?o ?g. }

• W4382502253 abstract "ABSTRACT High-risk human papillomaviruses (PV) account for approximately 600,000 new cancers per year. The early protein E8^E2 is a conserved repressor of PV replication, whereas E4 is a late protein that arrests cells in G2 and collapses keratin filaments to facilitate virion release. While inactivation of the Mus musculus PV1 (MmuPV1) E8 start codon (E8-) increases viral gene expression, surprisingly, it prevents wart formation in FoxN1 nu/nu mice. To understand this surprising phenotype, the impact of additional E8^E2 mutations was characterized in tissue culture and mice. MmuPV1 and HPV E8^E2 similarly interact with cellular NCoR/SMRT-HDAC3 co-repressor complexes. Disruption of the splice donor sequence used to generate the E8^E2 transcript or E8^E2 mutants (mt) with impaired binding to NCoR/SMRT-HDAC3 activates MmuPV1 transcription in murine keratinocytes. These MmuPV1 E8^E2 mt genomes also fail to induce warts in mice. The phenotype of E8^E2 mt genomes in undifferentiated cells resembles productive PV replication in differentiated keratinocytes. Consistent with this, E8^E2 mt genomes induced aberrant E4 expression in undifferentiated keratinocytes. In line with observations for HPV, MmuPV1 E4-positive cells displayed a shift to the G2 phase of the cell cycle. In summary, we propose that in order to enable both expansion of infected cells and wart formation in vivo , MmuPV1 E8^E2 inhibits E4 protein expression in the basal keratinocytes that would otherwise undergo E4-mediated cell cycle arrest. IMPORTANCE Human papillomaviruses (PVs) initiate productive replication, which is characterized by genome amplification and expression of E4 protein strictly within suprabasal, differentiated keratinocytes. Mus musculus PV1 mutants that disrupt splicing of the E8^E2 transcript or abolish the interaction of E8^E2 with cellular NCoR/SMRT-HDAC3 co-repressor complexes display increased gene expression in tissue culture but are unable to form warts in vivo . This confirms that the repressor activity of E8^E2 is required for tumor formation and genetically defines a conserved E8 interaction domain. E8^E2 prevents expression of E4 protein in basal-like, undifferentiated keratinocytes and thereby their arrest in G2 phase. Since binding of E8^E2 to NCoR/SMRT-HDAC3 co-repressor is required to enable expansion of infected cells in the basal layer and wart formation in vivo , this interaction represents a novel, conserved, and potentially druggable target." @default.
• W4382502253 created "2023-06-30" @default.
• W4382502253 creator A5001393130 @default.
• W4382502253 creator A5031102468 @default.
• W4382502253 creator A5041510167 @default.
• W4382502253 creator A5066778878 @default.
• W4382502253 creator A5069219697 @default.
• W4382502253 creator A5088538875 @default.
• W4382502253 creator A5089035026 @default.
• W4382502253 date "2023-06-29" @default.
• W4382502253 modified "2023-09-23" @default.
• W4382502253 title "Mus musculus papillomavirus 1 E8^E2 represses expression of late protein E4 in basal-like keratinocytes via NCoR/SMRT-HDAC3 co-repressor complexes to enable wart formation <i>in vivo</i>" @default.
• W4382502253 cites W1574443991 @default.
• W4382502253 cites W1607774948 @default.
• W4382502253 cites W1801314933 @default.
• W4382502253 cites W1980382561 @default.
• W4382502253 cites W1984180468 @default.
• W4382502253 cites W1989247572 @default.
• W4382502253 cites W1995715600 @default.
• W4382502253 cites W2003053867 @default.
• W4382502253 cites W2011935281 @default.
• W4382502253 cites W2017473511 @default.
• W4382502253 cites W2029942202 @default.
• W4382502253 cites W2032572462 @default.
• W4382502253 cites W2037678482 @default.
• W4382502253 cites W2044568134 @default.
• W4382502253 cites W2048559665 @default.
• W4382502253 cites W2052516166 @default.
• W4382502253 cites W2061862766 @default.
• W4382502253 cites W2063287731 @default.
• W4382502253 cites W2066332001 @default.
• W4382502253 cites W2079003739 @default.
• W4382502253 cites W2088720253 @default.
• W4382502253 cites W2090130596 @default.
• W4382502253 cites W2108631426 @default.
• W4382502253 cites W2112125352 @default.
• W4382502253 cites W2113271936 @default.
• W4382502253 cites W2119814307 @default.
• W4382502253 cites W2122386593 @default.
• W4382502253 cites W2130530238 @default.
• W4382502253 cites W2133312492 @default.
• W4382502253 cites W2140687712 @default.
• W4382502253 cites W2146757491 @default.
• W4382502253 cites W2148904894 @default.
• W4382502253 cites W2149157897 @default.
• W4382502253 cites W2161325043 @default.
• W4382502253 cites W2317295289 @default.
• W4382502253 cites W2413989238 @default.
• W4382502253 cites W2528456062 @default.
• W4382502253 cites W2605365014 @default.
• W4382502253 cites W2770961338 @default.
• W4382502253 cites W2792074753 @default.
• W4382502253 cites W2898692674 @default.
• W4382502253 cites W2954274611 @default.
• W4382502253 cites W3005873106 @default.
• W4382502253 cites W3021820466 @default.
• W4382502253 cites W3024116083 @default.
• W4382502253 cites W3125724987 @default.
• W4382502253 cites W3199948235 @default.
• W4382502253 cites W3200677052 @default.
• W4382502253 cites W3202170749 @default.
• W4382502253 cites W4221015485 @default.
• W4382502253 cites W4221086434 @default.
• W4382502253 cites W4225401277 @default.
• W4382502253 cites W4309242681 @default.
• W4382502253 doi "https://doi.org/10.1128/mbio.00696-23" @default.
• W4382502253 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/37382436" @default.
• W4382502253 hasPublicationYear "2023" @default.
• W4382502253 type Work @default.
• W4382502253 citedByCount "0" @default.
• W4382502253 crossrefType "journal-article" @default.
• W4382502253 hasAuthorship W4382502253A5001393130 @default.
• W4382502253 hasAuthorship W4382502253A5031102468 @default.
• W4382502253 hasAuthorship W4382502253A5041510167 @default.
• W4382502253 hasAuthorship W4382502253A5066778878 @default.
• W4382502253 hasAuthorship W4382502253A5069219697 @default.
• W4382502253 hasAuthorship W4382502253A5088538875 @default.
• W4382502253 hasAuthorship W4382502253A5089035026 @default.
• W4382502253 hasBestOaLocation W43825022531 @default.
• W4382502253 hasConcept C104317684 @default.
• W4382502253 hasConcept C140704245 @default.
• W4382502253 hasConcept C150194340 @default.
• W4382502253 hasConcept C153911025 @default.
• W4382502253 hasConcept C158448853 @default.
• W4382502253 hasConcept C159047783 @default.
• W4382502253 hasConcept C2777074287 @default.
• W4382502253 hasConcept C29537977 @default.
• W4382502253 hasConcept C54355233 @default.
• W4382502253 hasConcept C81885089 @default.
• W4382502253 hasConcept C86803240 @default.
• W4382502253 hasConcept C95444343 @default.
• W4382502253 hasConceptScore W4382502253C104317684 @default.
• W4382502253 hasConceptScore W4382502253C140704245 @default.
• W4382502253 hasConceptScore W4382502253C150194340 @default.
• W4382502253 hasConceptScore W4382502253C153911025 @default.
• W4382502253 hasConceptScore W4382502253C158448853 @default.
• W4382502253 hasConceptScore W4382502253C159047783 @default.
• W4382502253 hasConceptScore W4382502253C2777074287 @default.
• W4382502253 hasConceptScore W4382502253C29537977 @default.
• W4382502253 hasConceptScore W4382502253C54355233 @default.

• next