Post‐translational regulation of antiviral innate signaling

Zhang

Journal of Medical Virology

et al. 2019

Increasing evidence indicates ATP1B3, one of the regulatory subunits of Na+/K+‐ATPase, is involved in numerous viral propagations, such as HIV and EV71. However, the function and mechanism of ATP1B3 on hepatitis B virus (HBV) propagation is unknown. Here, we demonstrated that ATP1B3 overexpression reduced the quantity of hepatitis B surface antigen (HBsAg) and hepatitis B e antigen (HBeAg) in supernatants of HBV expression plasmids cotransfected HepG2 cells. Correspondingly, small interfering RNA and short hairpin RNA mediated ATP1B3 silencing promoted HBsAg and HBeAg expression in the supernatants of HBV expression plasmids transfected HepG2 cells. Mechanically, we reported that ATP1B3 expression could activate nuclear factor‐κB (NF‐κB) pathway by inducing the expression, phosphorylation, and nuclear import of P65 for the first time. And NF‐κB inhibitor (Bay11) impaired the restraint of ATP1B3 on HBV replication. This counteraction effect of Bay11 proved that ATP1B3‐induced NF‐κB activation was crucial for HBV restriction. Accordingly, we observed that anti‐HBV factors interferon‐α (IFN‐α) and interleukin‐6 (IL‐6) production were increased in HepG2 cells after the NF‐κB activation. It suggested that ATP1B3 suppressed HBsAg and HBeAg by NF‐κB/IFN‐α and NF‐κB/IL‐6 axis. Further experiments proved that ATP1B3 overexpression induced anti‐HBV factor BST‐2 expression by NF‐κB/IFN‐α axis in HepG2 cells but not HEK293T cells, and ATP1B3 silencing downregulated BST‐2 messenger RNA level in HepG2 cells. As an HBV restriction factor, BST‐2 cooperated with ATP1B3 to antagonize HBsAg but not HBeAg in HepG2 cells. Our work identified ATP1B3 as a novel candidate of HBV restrictor with unrevealed mechanism and we highlighted it might serve as a potential therapeutic molecule for HBV infection.

Section: Previous Evidence On the Relationship Between Nf-κb Activationmentioning

confidence: 99%

ATP1B3 cooperates with BST‐2 to promote hepatitis B virus restriction

Zhang

Journal of Medical Virology

et al. 2019

“…However, a variety of non-histone proteins, both cytoplasmic and nuclear, are now known to be HDAC substrates (Seto & Yoshida, 2014). HDACs work in equilibrium with histone acetyl transferases to control the acetylation level of proteins and influence diverse biological processes such as gene expression (Sterner & Berger, 2000), protein trafficking (Li & Yang, 2015), and the innate immune response (Zhou, He, Wang, & Ge, 2017). Consequently, the imbalance in protein acetylation due to aberrant function of HDACs or histone acetyl transferases contributes to multiple human diseases such as cancer (Liu, Li, Wu, & Cho, 2017), neurodegeneration (Cook, Stankowski, Carlomagno, Stetler, & Petrucelli, 2014), and infection (Jeng, Ali, & Ott, 2015;Song & Walley, 2016).…”

Section: Introductionmentioning

confidence: 99%

The Class IV human deacetylase, HDAC11, exhibits anti‐influenza A virus properties via its involvement in host innate antiviral response

Nutsford

Galvin

Ahmed

et al. 2018

Cellular Microbiology

Histone deacetylase 11 (HDAC11) is most recently discovered deacetylase. Here, we demonstrate that human HDAC11 exhibits anti‐influenza A virus (IAV) properties. We found that knockdown of HDAC11 expression augments IAV growth kinetics in human lung epithelial cells A549 by up to 1 log. One of the ways HDAC11 exerts its anti‐IAV function is by being a part of IAV‐induced host antiviral response. We found that the kinetics of both IAV‐ and interferon‐induced innate antiviral response is significantly delayed in HDAC11‐depleted cells. Further, in the absence of HDAC11 expression, there was a significant decrease in the expression of interferon‐stimulated genes—IFITM3, ISG15, and viperin—previously implicated in anti‐IAV function. One of the ways IAV antagonises HDAC11 is by downregulating its expression in host cells. We found that there was up to 93% reduction in HDAC11 transcript levels in A549 cells in response to IAV infection. HDAC11 is the smallest HDAC with majority of its polypeptide assigned to catalytic domain. Evolutionarily, it seems to be the least evolved and most closely related to common ancestral HDAC gene(s). Furthermore, HDAC11 has also been described as a deacylase. Therefore, our findings present exciting prospects for further investigations into significance of HDAC11 in virus infections.

“…Another goal of nucleic acid packaging into a particle lies in the presentation of viral nucleic acids leading to the activation of specific immune receptors which induce the synthesis of type I interferons (INF) and other cytokines triggering the antivirus response [49]. It has been demonstrated that long DNA and RNA molecules may be incorporated into VLPs.…”

Section: Natural Sources For Vlp Bioengineering and The Specificmentioning

confidence: 99%

“…Posttranslational protein modifications and covalent bonds between the modifying molecules and the functional groups in the polypeptide chains are of great importance for immune homeostasis during the antiviral response. The balance between phosphorylation, ubiquitination, methylation, acetylation, SUMOylation, ADP-ribosylation, and glutamilation of a certain antigen performs the fine adjustment of the host's antiviral response [49,58]. The structural proteins for VLP production when synthesized in the eukaryotic expression systems undergo a number of posttranslational modifications.…”

Section: Natural Sources For Vlp Bioengineering and The Specificmentioning

confidence: 99%

Virus-Like Particles as an Instrument of Vaccine Production

Syomin

Ilyin

2019

Mol Biol

The paper discusses the techniques which are currently implemented for vaccine production based on virus-like particles (VLPs). The factors which determine the characteristics of VLP monomers assembly are provided in detail. Analysis of the literature demonstrates that the development of the techniques of VLP production and immobilization of target antigens on their surface have led to the development of universal platforms which make it possible for virtually any known antigen to be exposed on the particle surface in a highly concentrated form. As a result, the focus of attention has shifted from the approaches to VLP production to the development of a precise interface between the organism's immune system and the peptides inducing a strong immune response to pathogens or the organism's own pathological cells. Immunome-specified methods for vaccine design and the prospects of immunoprophylaxis are discussed. Certain examples of vaccines against viral diseases and cancers are considered.