Recombinant Human herpesvirus 1 Deneddylase UL36 (UL36), partial

1. The findings underline the roles of UL36USP-IFNAR2 interaction in counteracting the type I IFN-mediated signaling pathway and reveal a novel evasion mechanism of antiviral innate immunity by HSV-1. PMID: 29997210
2. UL36USP deubiquitinating activity supports HSV-1 virus replication during infection. PMID: 28348081
3. UL36 abrogates NF-kappaB activation by cleaving polyubiquitin chains from IkappaBalpha and therefore restricts proteasome-dependent degradation of IkappaBalpha and that DUB activity is indispensable for this process. PMID: 28031360
4. characterized 2 conserved tryptophan-acidic motifs in the central region of pUL36; results indicate the unique conserved tryptophan-acidic motifs in the central region of pUL36 are required for efficient targeting of progeny capsids to the membranes of secondary capsid envelop PMID: 27009950
5. UL36p-independent binding of capsids to organelles occurs prior to the function of UL36p in capsid envelopment. PMID: 26339048
6. an essential feature of UL36 is the existence in its central region of a stalk capable of connecting capsid and membrane across the tegument and that the ability to switch between monomeric and dimeric forms may help UL36 fulfill its multiple functions PMID: 25678705
7. Authors showed that in contrast to accepted models, the capsid vertex-specific component is not formed from pUL17 and pUL25 on their own but requires a contribution from pUL36. PMID: 25410861
8. In addition, immunoblot analysis suggested that failure to bind pUL37 affected the stability of pUL36. PMID: 24725933
9. These findings demonstrate that herpes simplex virus 1 ubiquitin-specific protease UL36 removes polyubiquitin chains on TRAF3 and counteracts the IFN-beta pathway. PMID: 23986588
10. Cytosolic herpes simplex virus capsids not only require binding inner tegument protein pUL36 but also pUL37 for active transport prior to secondary envelopment. PMID: 23186167
11. Nuclear localization signal in VP1-2(UL36) is essential for infection via capsid routing to the nuclear pore. PMID: 22718835
12. UL36 plays a major role in the tegumentation of the virion, providing a flexible scaffold to which other tegument proteins, including UL37, bind. PMID: 22345483
13. 2430 to 2893 of HSV1 pUL36, containing one binding site for the capsid protein pUL25, are sufficient to recruit pUL36 onto cytosolic capsids during assembly. PMID: 22258258
14. Interaction between VP1/2 and VP16 is important for viral assembly but is not essential for HSV-1 replication in cell culture. PMID: 22013045
15. Here the authors show that herpes simplex virus 1 VP1-2 ubiquitin-specific protease can act on itself and is important for stability. PMID: 21715485
16. A single mutation in the UL36 protein is responsible for virus temperature-sensitive entry and assembly defects. PMID: 21177812
17. The findings are interpreted to indicate that UL36 and UL37 are the components of the tufts and of the thin strands that extend from them. PMID: 20631146
18. For each HSV-1 mutant, analysis of purified deenveloped C capsids indicated that only in the absence of pUL36 was there a complete loss of capsid-bound pUL48, as well as pUL37 PMID: 19923173
19. Single changes to alanine of pUL36 residues F593 and E596 impaired binding of pUL37 with the greatest effect observed for the substitution E596A. PMID: 17651773
20. we propose a model in which after the herpes simplex virus (HSV) capsid docks at the nuclear pore, the tegument protein attached to the capsid must be cleaved by a serine or a cysteine protease in order for the DNA to be released into the nucleus. PMID: 18216103
21. These findings suggest that UL36p is necessary for HSV-1 anterograde transport. PMID: 18495763
22. cells infected with UL37/deltaUL36 virus showed that, in the absence of UL36, accumulation of UL37 at the Golgi complex was not evident. PMID: 18787001
23. these inner tegument proteins have differing functions, with pUL36 being essential during both the assembly and uptake stages of infection, while pUL37 is needed for the formation of virions but is not required during the initial stages of infection. PMID: 18971278

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KEGG: vg:2703357