Coronavirus, the King Who Wanted More Than a Crown: From Common to the Highly Pathogenic SARS-CoV-2, Is the Key in the Accessory Genes?

Chazal, Nathalie

doi:10.3389/fmicb.2021.682603

Cited by 11 publications

(13 citation statements)

References 309 publications

(382 reference statements)

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“…One example of homologous proteins in two different betacoronavirus lineages is the PDEs of merbecoviruses (NS2) and embecoviruses (NS4b); however, these proteins differ in that only NS4b contains an NLS and has a second function in host antagonism ( 21 , 22 , 28 – 31 , 50 ). The SARS-CoV-2 genome encodes sarbecovirus lineage-specific accessory proteins encoded in ORF3a, ORF3b, ORF6, ORF7a, and ORF9b, which have all been reported to be IFN antagonists ( 51 , 52 ). Most notably, the ORF6 encoded protein of SARS-CoV and SARS-CoV-2 blocks STAT1/STAT2 translocation into the nucleus, thus impairing induction of ISGs ( 53 , 54 ).…”

Section: Discussionmentioning

confidence: 99%

MERS-CoV endoribonuclease and accessory proteins jointly evade host innate immunity during infection of lung and nasal epithelial cells

Comar

Otter

Pfannenstiel

et al. 2022

Proc. Natl. Acad. Sci. U.S.A.

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Significance Middle East respiratory syndrome coronavirus (MERS-CoV) causes highly lethal respiratory disease. MERS-CoV encodes innate immune antagonists, including accessory proteins NS4a and NS4b, unique to the merbeco lineage of betacoronaviruses, and the nsp15 protein endoribonuclease (EndoU), conserved among all coronaviruses. While mutation of each antagonist protein alone has little effect on innate immunity, infections with recombinant MERS-CoVs with mutations of EndoU in combination with either NS4a or NS4b activate innate signaling pathways and are attenuated for replication. Our data indicate that EndoU and accessory proteins NS4a and NS4b together suppress innate immunity during MERS-CoV infection, to optimize viral replication. This is in contrast to SARS-CoV-2 which activates these pathways and is thus more vulnerable to host innate immune responses.

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Section: Discussionmentioning

confidence: 99%

MERS-CoV endoribonuclease and accessory proteins jointly evade host innate immunity during infection of lung and nasal epithelial cells

Comar

Otter

Pfannenstiel

et al. 2022

Proc. Natl. Acad. Sci. U.S.A.

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“…Assembly of new viral particles and exocytosis of the mature virions through the formation of double membraned vesicles (DMVs) completes the viral life cycle ( Hartenian et al, 2020 ; V’kovski et al, 2020 ). The roles of each of the viral structural/accessory protein and non-structural proteins (nsps) have been studied extensively ( Hartenian et al, 2020 ; V’kovski et al, 2020 ; Chazal, 2021 ). Targeting essential steps early in the process of viral replication has been the most successful strategy to stop CoV infection.…”

Section: Introductionmentioning

confidence: 99%

Inhibitors of SARS-CoV-2 PLpro

2022

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The emergence of SARS-CoV-2 causing the COVID-19 pandemic, has highlighted how a combination of urgency, collaboration and building on existing research can enable rapid vaccine development to fight disease outbreaks. However, even countries with high vaccination rates still see surges in case numbers and high numbers of hospitalized patients. The development of antiviral treatments hence remains a top priority in preventing hospitalization and death of COVID-19 patients, and eventually bringing an end to the SARS-CoV-2 pandemic. The SARS-CoV-2 proteome contains several essential enzymatic activities embedded within its non-structural proteins (nsps). We here focus on nsp3, that harbours an essential papain-like protease (PLpro) domain responsible for cleaving the viral polyprotein as part of viral processing. Moreover, nsp3/PLpro also cleaves ubiquitin and ISG15 modifications within the host cell, derailing innate immune responses. Small molecule inhibition of the PLpro protease domain significantly reduces viral loads in SARS-CoV-2 infection models, suggesting that PLpro is an excellent drug target for next generation antivirals. In this review we discuss the conserved structure and function of PLpro and the ongoing efforts to design small molecule PLpro inhibitors that exploit this knowledge. We first discuss the many drug repurposing attempts, concluding that it is unlikely that PLpro-targeting drugs already exist. We next discuss the wealth of structural information on SARS-CoV-2 PLpro inhibition, for which there are now ∼30 distinct crystal structures with small molecule inhibitors bound in a surprising number of distinct crystallographic settings. We focus on optimisation of an existing compound class, based on SARS-CoV PLpro inhibitor GRL-0617, and recapitulate how new GRL-0617 derivatives exploit different features of PLpro, to overcome some compound liabilities.

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“…In the last two decades, three novel Betacoronaviruses have entered human circulation from zoonotic sources and caused infections with high morbidity and mortality. This group includes the severe acute respiratory syndrome coronavirus (SARS-CoV), the Middle East respiratory syndrome coronavirus (MERS-CoV), and the SARS-CoV2 virus that appeared in late 2019 and caused the most devastating respiratory virus pandemic since the 1918 Spanish Flu (2)(3)(4)(5). The relatively genomes of Betacoronaviruses are ~30 kb and encode 4-5 structural proteins and 16 nonstructural proteins (Nsp1-16) (1,(6)(7)(8).…”

Section: Introductionmentioning

confidence: 99%

Nsp1 proteins of human coronaviruses HCoV-OC43 and SARS-CoV2 inhibit stress granule formation

Dolliver

Kleer

Bui-Marinos

et al. 2022

Preprint

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Stress granules (SGs) are cytoplasmic condensates that often form as part of the cellular antiviral response. Despite the growing interest in understanding the interplay between SGs and other biological condensates and viral replication, the role of SG formation during coronavirus infection remains poorly understood. Several proteins from different coronaviruses have been shown to suppress SG formation upon overexpression, but there are only a handful of studies analyzing SG formation in coronavirus-infected cells. To better understand SG inhibition by coronaviruses, we analyzed SG formation during infection with the human common cold coronavirus OC43 (HCoV-OC43) and the highly pathogenic SARS-CoV2. We did not observe SG induction in infected cells and both viruses inhibited eukaryotic translation initiation factor 2α (eIF2α) phosphorylation and SG formation induced by exogenous stress (e.g. sodium arsenite treatment). Furthermore, in SARS-CoV2 infected cells we observed a sharp decrease in the levels of SG-nucleating protein G3BP1. Ectopic overexpression of nucleocapsid (N) and non-structural protein 1 (Nsp1) from both HCoV-OC43 and SARS-CoV-2 inhibited SG formation. The Nsp1 proteins of both viruses inhibited arsenite-induced eIF2α phosphorylation, and the Nsp1 of SARS-CoV2 alone was sufficient to cause decrease in G3BP1 levels. This phenotype was dependent on the depletion of cytoplasmic mRNA mediated by Nsp1 and associated with nuclear retention of the SG-nucleating protein TIAR. To test the role of G3BP1 in coronavirus replication, we infected cells overexpressing EGFP-tagged G3BP1 with HCoV-OC43 and observed a significant decrease in infection compared to control cells expressing EGFP. The antiviral role of G3BP1 and the existence of multiple SG suppression mechanisms that are conserved between HCoV-OC43 and SARS-CoV2 suggest that SG formation may represent an important antiviral host defense that coronaviruses target to ensure efficient replication.

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Coronavirus, the King Who Wanted More Than a Crown: From Common to the Highly Pathogenic SARS-CoV-2, Is the Key in the Accessory Genes?

Cited by 11 publications

References 309 publications

MERS-CoV endoribonuclease and accessory proteins jointly evade host innate immunity during infection of lung and nasal epithelial cells

MERS-CoV endoribonuclease and accessory proteins jointly evade host innate immunity during infection of lung and nasal epithelial cells

Inhibitors of SARS-CoV-2 PLpro

Nsp1 proteins of human coronaviruses HCoV-OC43 and SARS-CoV2 inhibit stress granule formation

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