2015
DOI: 10.1128/jvi.00403-15
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Studies on the Contribution of Human Cytomegalovirus UL21a and UL97 to Viral Growth and Inactivation of the Anaphase-Promoting Complex/Cyclosome (APC/C) E3 Ubiquitin Ligase Reveal a Unique Cellular Mechanism for Downmodulation of the APC/C Subunits APC1, APC4, and APC5

Abstract: Human cytomegalovirus (HCMV) deregulates the cell cycle by several means, including inactivation of the anaphase-promoting complex/cyclosome (APC/C) E3 ubiquitin ligase. Viral proteins UL97 and UL21a, respectively, affect the APC/C by phosphorylation of APC/C coactivator Cdh1 and by inducing the degradation of subunits APC4 and APC5, which along with APC1 form the APC/C platform subcomplex. The aim of this study was to further characterize the mechanism of APC/C inactivation and define the relative contributio… Show more

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Cited by 19 publications
(17 citation statements)
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References 51 publications
(60 reference statements)
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“…Overall, our data argue in favor of a model of the HCMV terminase as a multiprotein complex in which the individual subunits stabilize each other upon assembly. Such a setting was also proposed for other CMV protein complexes, namely, for the murine CMV (MCMV) US22 protein family (60) and for the HCMV major and small capsid proteins (18), as well as for the cellular anaphase-promoting complex, a multiprotein assembly targeted by HCMV (61).…”
Section: Discussionmentioning
confidence: 99%
“…Overall, our data argue in favor of a model of the HCMV terminase as a multiprotein complex in which the individual subunits stabilize each other upon assembly. Such a setting was also proposed for other CMV protein complexes, namely, for the murine CMV (MCMV) US22 protein family (60) and for the HCMV major and small capsid proteins (18), as well as for the cellular anaphase-promoting complex, a multiprotein assembly targeted by HCMV (61).…”
Section: Discussionmentioning
confidence: 99%
“…From a comparison with our previous study of HCMV-induced protein degradation between 2-24 h (10), seven proteins were degraded with high confidence throughout early and late infection ( Figures 1C, 1D). These proteins included HLTF and Anaphase Promoting Complex subunits 1 and 5 (ANAPC1/5), whose degradation by HCMV has been well characterised (10,19). The effector of necroptosis MLKL was the most significantly downregulated protein at 48 h of HCMV infection and was among proteins most significantly rescued by addition of MG132 ( Figure 1B).…”
Section: Host Proteins Targeted For Degradation At 48 H Of Hcmv Infecmentioning
confidence: 99%
“…Entry of the infected cell into mitosis is regulated HCMV pUL21a which limits Cyclin A levels and subsequently CCNB1 levels ( Fig 9A) [55]. Expressions of pUL97 and pUL21a also inactivated APC/C during infection (Fig 9B and 9C) [56][57][58][59]. However, the reason for APC/C inactivation and how it contributes to HCMV replication remain unknown.…”
Section: Defining the Contribution Of Apc/c Degradation To Mitotic Comentioning
confidence: 99%
“…This perturbation resulted in increased oscillations with an eventual mitotic collapse defined by reduced MPF, LMNAP and PTTG1T and elevated APC/CT (Fig 9E). By a different mechanism, HCMV pUL21 also mediates the degradation of subunits APC1, APC4 and APC5 resulting in the inactivation of APC/C ( Fig 9C) [56,57]. For this mechanism, we increased the rate constant k d15.1 resulting in decreased oscillations and a mitotic collapse exhibiting elevated levels of MPF, CCNB1, PTTG1T and LMNAP ( Fig 9B).…”
Section: Defining the Contribution Of Apc/c Degradation To Mitotic Comentioning
confidence: 99%
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