Deregulation of HDAC5 by Viral Interferon Regulatory Factor 3 Plays an Essential Role in Kaposi's Sarcoma-Associated Herpesvirus-Induced Lymphangiogenesis

Chen

Journal of Medical Virology

et al. 2018

Background and purpose Kaposi's sarcoma–associated herpes virus (KSHV) vIL‐6 is sufficient to induce lymphatic reprogramming of vascular endothelial cells, which is a key event in Kaposi's sarcoma (KS) development. This study was aimed to investigate the effect of Chinese herb oroxylin A on lymphatic reprogramming and neovascularization by KSHV vIL‐6 in vitro and in vivo. Methods The lymphatic‐phenotype endothelial cell line was generated by lentiviral KSHV vIL‐6 infection. Cell viability and apoptosis were determined by MTT assay or flow cytometry with annexin V/propidium iodide staining. Migration, invasion, and neovascularization of the vIL‐6‐expressing lymphatic‐phenotype endothelial cells were determined by wound healing assay, transwell chamber assay, microtubule formation assay, and chick chorioallantoic membrane assay, respectively. Quantitative polymerase chain reaction and Western blot analysis were used to test the expression of Prox1, VEGFR3, podoplanin, LYVE‐1, and PPARγ in cells. Co‐localization of Prox1 and PPARγ was determined by immunofluorescence. Ubiquitination of Prox1 was detected by in vivo ubiquitination assay. Results The lymphatic‐phenotype endothelial cell line expressing KSHV vIL‐6 was successfully generated. Oroxylin A induced cellular invasion abrogation, apoptosis induction, and neovascularization inhibition of the vIL‐6‐expressing endothelial cells. Mechanically, oroxylin A elevated PPARγ expression, which in turn interacted with and facilitated Prox1 to undergo ubiquitinational degradation, and subsequently leads to VEGFR3, LYVE‐1, and podoplanin reduction. Conclusion Through modulating PPARγ/Prox1 axis, oroxylin A inhibits lymphatic reprogramming and neovascularization of KSHV vIL‐6. Thus, oroxylin A may serve as a candidate for the treatment of KS as well as other aggressive angiomas.

mentioning

confidence: 59%

“…Lymphatic reprogramming plays a pivotal role in KS development . In the present study, we successfully established a lymphatic‐phenotype endothelial cell line by transduction of KSHV vIL‐6 gene into the HUVECs.…”

Section: Discussionmentioning

confidence: 93%

Oroxylin A inhibits Kaposi's sarcoma‐associated herpes virus (KSHV) vIL‐6–mediated lymphatic reprogramming of vascular endothelial cells through modulating PPARγ/Prox1 axis

Chen

Journal of Medical Virology

et al. 2018

“…No specific SIRT6 inhibitor (small compound) is available; the SIRT6-KSHV DNA might be an effective target for developing an interfering molecule for infection prevention or therapeutic purposes. Interestingly, a recent study found that the KSHV-encoded protein viral interferon regulatory factor 3, which interacts with HDAC5, contributes to KSHV-induced lymphangiogenesis, which is related to KSHV-caused malignancy (35). Therefore, studies on the relationship between HDAC/SIRT and KSHV might also result in an understanding of how KSHV causes cancer.…”

Section: Discussionmentioning

confidence: 99%

Sirtuin 6 Attenuates Kaposi's Sarcoma-Associated Herpesvirus Reactivation by Suppressing Ori-Lyt Activity and Expression of RTA

Armstrong

Seto

et al. 2019

J Virol

Kaposi's sarcoma-associated herpesvirus (KSHV; also called human herpesvirus 8 ), upon being reactivated, causes serious diseases in immunocompromised individuals. Its reactivation, especially how the cellular regulating mechanisms play roles in KSHV gene expression and viral DNA replication, is not fully understood. In searching for the cellular factors that regulate KSHV gene expression, we found that several histone deacetylases (HDACs) and sirtuins (SIRTs), including HDACs 2, 7, 8, and 11 and SIRTs 4 and 6, repress KSHV ori-Lyt promoter activity. Interestingly, the nuclear protein SIRT6 presents the greatest inhibitory effect on ori-Lyt promoter activity. A more detailed investigation revealed that SIRT6 exerts repressive effects on multiple promoters of KSHV. As a consequence of inhibiting the KSHV promoters, SIRT6 not only represses viral protein production but also inhibits viral DNA replication, as investigated in a KSHV-containing cell line, SLK-iBAC-gfpK52. Depletion of the SIRT6 protein using small interfering RNA could not directly reactivate KSHV from SLK-iBAC-gfpK52 cells but made the reactivation of KSHV by use of a small amount of the reactivator (doxycycline) more effective and enhanced viral DNA replication in the KSHV infection system. We performed DNA chromatin immunoprecipitation (ChIP) assays for SIRT6 in the SLK-iBAC-gfpK52 cell line to determine whether SIRT6 interacts with the KSHV genome in order to exhibit regulatory effects. Our results suggest that SIRT6 interacts with KSHV ori-Lyt and ORF50 promoters. Furthermore, the SIRT6-KSHV DNA interaction is significantly negated by reactivation. Therefore, we identified a cellular regulator, SIRT6, that represses KSHV replication by interacting with KSHV DNA and inhibiting viral gene expression. IMPORTANCE Kaposi's sarcoma-associated herpesvirus (KSHV) is a pathogen causing cancer in the immune-deficient population. The reactivation of KSHV from latency is important for it to be carcinogenic. Our finding that SIRT6 has inhibitory effects on KSHV reactivation by interacting with the viral genome and suppressing viral gene expression is important because it might lead to a strategy of interfering with KSHV reactivation. Overexpression of SIRT6 repressed the activities of several KSHV promoters, leading to reduced gene expression and DNA replication by KSHV in a KSHV bacterial artificial chromosome-containing cell line. Depletion of SIRT6 favored reactivation of KSHV from SLK-iBACV-gfpK52 cells. More importantly, we reveal that SIRT6 interacts with KSHV DNA. Whether the interaction of SIRT6 with KSHV DNA occurs at a global level will be further studied in the future. Downloaded fromfor the pORF50 promoter), as shown in Fig. 8B. We found that SIRT6 interacts with KSHV DNA in both the latent (without Dox) and lytic (with Dox) phases. However, the DNA-SIRT6 interaction was decreased when the KSHV latency was reactivated. This suggests that the interaction of SIRT6 with KSHV DNA is important for the maintenance of viral latency. In summary, cellular ...

“…KSHV oncogenesis is, in part, attributed to genes expressed during latency. Viral FLICE inhibitory protein (vFLIP or K13), is a latently expressed gene that was originally identified as an inhibitor of apoptosis, due to the presence of tandem death effector domains 8,9 . vFLIP is a potent activator of NFκB signaling and this activity is dependent on interaction with IKKߛ 10-12 . vFLIP has also been shown to promote NFκB signaling through upregulation of IKKߝ and CADM1 and inhibition of the SAP18/HDAC1 complex resulting in activation of NFκB via acetylation of p65 [13][14][15] .…”

Section: Introductionmentioning

confidence: 99%

Novel functions of Kaposi’s sarcoma herpesvirus viral FLICE inhibitory protein

Herold

Ruffin

Mitchell

et al. 2019

Preprint

KSHV vFLIP is a potent activator of NFκB signaling and an inhibitor of apoptosis and autophagy. Inhibition of vFLIP function and NFκB signaling promotes viral reactivation. Here we provide evidence for a novel function of vFLIP in promoting NFߢB signaling through inhibition of the DUB activity of the negative regulator, A20. We demonstrate interaction of vFLIP with the Itch/A20 ubiquitin editing complex. We have identified a SUMO interaction motif in vFLIP that is required for NFκB activation. We observed a decrease in vFLIP induced NFκB when the SIM in vFLIP was mutated. Small molecule inhibition of SUMOylation resulted in a dose dependent increase lytic reactivation and virus production. Our results suggest a role for SUMO in mediating vFLIP function and provide evidence for vFLIP modulation of the negative regulation of NFκB signaling by A20. Our results provide further insight into the function of vFLIP and SUMO in the regulation of NFκB signaling and the latent lytic transition.