Biological Function and Application of Picornaviral 2B Protein: A New Target for Antiviral Drug Development

Li, Zengbin; Zou, Zixiao; Jiang, Zeju; Huang, Xiaotian; Liu, Qiong

doi:10.3390/v11060510

Cited by 17 publications

(22 citation statements)

References 107 publications

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“…The CVB3 proteins, 2B and 3A, are both involved in the disruption of the secretory pathway of infected cells and cause rearrangements of cellular membranes contributing to the formation of ROs [ 11 , 12 ]. Furthermore, protein 2B is known to form homotetramers, which act as viroporins and increase membrane permeability, e.g., for Ca 2+ ions [ 17 ]. Protein 3A was previously also described as a viroporin, but it is not as well characterized as protein 2B in this regard [ 18 ].…”

Section: Resultsmentioning

confidence: 99%

Coxsackievirus B3 Exploits the Ubiquitin-Proteasome System to Facilitate Viral Replication

Voß

Braun

Bredow

et al. 2021

Viruses

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Infection by RNA viruses causes extensive cellular reorganization, including hijacking of membranes to create membranous structures termed replication organelles, which support viral RNA synthesis and virion assembly. In this study, we show that infection with coxsackievirus B3 entails a profound impairment of the protein homeostasis at virus-utilized membranes, reflected by an accumulation of ubiquitinylated proteins, including K48-linked polyubiquitin conjugates, known to direct proteins to proteasomal degradation. The enrichment of membrane-bound ubiquitin conjugates is attributed to the presence of the non-structural viral proteins 2B and 3A, which are known to perturb membrane integrity and can cause an extensive rearrangement of cellular membranes. The locally increased abundance of ubiquitinylated proteins occurs without an increase of oxidatively damaged proteins. During the exponential phase of replication, the oxidative damage of membrane proteins is even diminished, an effect we attribute to the recruitment of glutathione, which is known to be required for the formation of infectious virus particles. Furthermore, we show that the proteasome contributes to the processing of viral precursor proteins. Taken together, we demonstrate how an infection with coxsackievirus B3 affects the cellular protein and redox homeostasis locally at the site of viral replication and virus assembly.

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Section: Resultsmentioning

confidence: 99%

Coxsackievirus B3 Exploits the Ubiquitin-Proteasome System to Facilitate Viral Replication

Voß

Braun

Bredow

et al. 2021

Viruses

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“…In EMCV this is a 128-amino acid protein, whereas in TMEV it is a short 14–15-amino acid peptide [ 54 ]. 2B encodes a viroporin, which increases cell permeability and thereby can induce viral release and host cell apoptosis [ 57 ]. On the other hand, 2B* has no known function and the main role of frameshifting is thought to be the down-regulation of the other proteins encoded downstream of the frameshift site [ 58 ].…”

Section: Unusual Gene Expression Strategies Employed By the Cardiovirusesmentioning

confidence: 99%

Insights from structural studies of the cardiovirus 2A protein

Caliskan

Hill

2022

Bioscience Reports

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Cardioviruses are single-stranded RNA viruses of the family Picornaviridae. In addition to being the first example of internal ribosome entry site utilization, cardioviruses also employ a series of alternative translation strategies, such as Stop-Go translation and programmed ribosome frameshifting. Here, we focus on cardiovirus 2A protein, which is not only a primary virulence factor, but also exerts crucial regulatory functions during translation, including activation of viral ribosome frameshifting and inhibition of host cap-dependent translation. Only recently, biochemical and structural studies have allowed us to close the gaps in our knowledge of how cardiovirus 2A is able to act in diverse translation-related processes as a novel RNA-binding protein. This review will summarize these findings, which ultimately may lead to the discovery of other RNA-mediated gene expression strategies across a broad range of RNA viruses.

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“…In addition, the CVB3 viroporin suppresses the cell death stimuli actinomycin D and cycloheximide that would usually activate caspase-3, but a clear connection between Ca 2+ -level manipulation induced by the viroporin and the inhibition of cell death stimuli has still to be established [147]. On the other hand, high concentrations of Ca 2+ in mitochondria lead to initiation of the intrinsic apoptotic pathway by releasing cytochrome c and activating caspase-9 which in turn activates caspase-3 and -7 [150,153,154]. Moreover, CVB3-induced myocarditis in mice exerts ER stress that promotes apoptosis and other cell death mechanisms.…”

Section: Enteroviruses (Cvb3)mentioning

confidence: 99%

“…Thus, viroporins exert extensive effects on ion homeostasis manipulating apoptosis and inflammation signaling. Drugs, siRNA, or shRNA that can inhibit viroporin activity and expression are shown to decrease viral titer in several picornavirus-infected cells [153]. CVB3 and EV71 can additionally regulate miRNAs which has pro-apoptotic effects: CVB3 upregulates miRNA-34a in infected rodent cardiomyocytes [159].…”

Section: Enteroviruses (Cvb3)mentioning

confidence: 99%

Virus-Host Interactions of Enteroviruses and Parvovirus B19 in Myocarditis

Peischard

Strutz‐Seebohm

et al. 2021

Cell Physiol Biochem

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Viral diseases are a major threat to modern society and the global health system. It is therefore of utter relevance to understand the way viruses affect the host as a basis to find new treatment solutions. The understanding of viral myocarditis (VMC) is incomplete and effective treatment options are lacking. This review will discuss the mechanism, effects, and treatment options of the most frequent myocarditis-causing viruses namely enteroviruses such as Coxsackievirus B3 (CVB3) and Parvovirus B19 (PVB19) on the human heart. Thereby, we focus on: 1. Viral entry: CVB3 use Coxsackievirus-Adenovirus-Receptor (CAR) and Decay Accelerating Factor (DAF) to enter cardiac myocytes while PVB19 use the receptor globoside (Gb4) to enter cardiac endothelial cells. 2. Immune system responses: The innate immune system mediated by activated cardiac toll-like receptors (TLRs) worsen inflammation in CVB3-infected mouse hearts. Different types of cells of the adaptive immune system are recruited to the site of inflammation that have either protective or adverse effects during VMC. 3. Autophagy: CVB3 evades autophagosomal degradation and misuses the autophasomal pathway for viral replication and release. 4. Viral replication sites: CVB3 promotes the formation of double membrane vesicles (DMVs), which it uses as replication sites. PVB19 uses the host cell nucleus as the replication site and uses the host cell DNA replication system. 5. Cell cycle manipulation: CVB3 attenuates the cell cycle at the G1/S phase, which promotes viral transcription and replication. PVB19 exerts cell cycle arrest in the S phase using its viral endonuclease activity. 6. Regulation of apoptosis: Enteroviruses prevent apoptosis during early stages of infection and promote cell death during later stages by using the viral proteases 2A and 3C, and viroporin 2B. PVB19 promotes apoptosis using the non-structural proteins NS1 and the 11 kDa protein. 7. Energy metabolism: Dysregulation of respiratory chain complex expression, activity and ROS production may be altered in CVB3- and PVB19-mediated myocarditis. 8. Ion channel modulation: CVB3-expression was indicated to alter calcium and potassium currents in Xenopus laevis oocytes and rodent cardiomyocytes. The phospholipase 2-like activity of PVB19 may alter several calcium, potassium and sodium channels. By understanding the general pathophysiological mechanisms of well-studied myocarditis-linked viruses, we might be provided with a guideline to handle other less-studied human viruses.

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Biological Function and Application of Picornaviral 2B Protein: A New Target for Antiviral Drug Development

Cited by 17 publications

References 107 publications

Coxsackievirus B3 Exploits the Ubiquitin-Proteasome System to Facilitate Viral Replication

Coxsackievirus B3 Exploits the Ubiquitin-Proteasome System to Facilitate Viral Replication

Insights from structural studies of the cardiovirus 2A protein

Virus-Host Interactions of Enteroviruses and Parvovirus B19 in Myocarditis

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