The human severe acute respiratory syndrome coronavirus (SARS-CoV) 8b protein is distinct from its counterpart in animal SARS-CoV and down-regulates the expression of the envelope protein in infected cells

Keng, Choong Tat; Choi, Yook-Wah; Welkers, Matthijs R.A.; Chan, Daphne Z. L.; Shen, Shuo; Lim, Seng Gee; Hong, Wanjin; Tan, Yee‐Joo

doi:10.1016/j.virol.2006.06.026

Cited by 55 publications

(92 citation statements)

References 35 publications

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“…Although SARS-CoV 8b gene product could be expressed in vivo when cloned directly behind a promoter [11][12][13]; the expression of 8a and 8b in SARS-CoVinfected cells is still controversial [9,10,13]. As shown above, we were unable to detect the protein expression of sgRNA 8 with the 5 0 viral leader sequence, which corroborated with a recent report on ORF8 expression [13].…”

Section: Resultssupporting

confidence: 91%

“…Ten sgRNAs have been identified [5] and the SARS-CoV accessory proteins 3a, 3b, 6,7a, and 7b can be detected in infected cells or SARS patients besides structural proteins [7,8], while the expression of 8a and 8b is controversial [9][10][11][12][13]. Elucidation of the regulatory mechanism in the translation is important for understanding the pathogenesis of SARS-CoV; however, it is hard to compare the differential translation of sgRNAs because the steady-state level of viral proteins in infected cells reflects the sum of transcription, translation, and the relative stabilities of these transcriptional and translational products.…”

Section: Resultsmentioning

confidence: 99%

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Translational control of the subgenomic RNAs of severe acute respiratory syndrome coronavirus

et al. 2009

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The 3'-one-third of the severe acute respiratory syndrome coronavirus (SARS-CoV) genome contains genes for four essential structural proteins and eight virus-specific genes. The expression of this genomic information of SARS-CoV involves synthesis of a nested set of subgenomic RNAs (sgRNAs). In this study, we showed that the translational levels of 10 SARS-CoV sgRNAs including the two low-abundance sgRNAs 2-1 and 3-1 varied considerably in translation reporter assays. We also demonstrated that the initiator AUG codon of sgRNA-8 was silent and the repressive control was most likely positioned in the upstream untranslated region (UTR) of sgRNA-8. The initiator AUG codons of most sgRNAs are in poor Kozak contexts and the translation of truncated proteins from downstream AUG codons by leaky scanning was common in our experimental settings. No significant correlation was found between complexity of 5'-UTR and the sequence context of AUG codon with the level of translation of SARS-CoV sgRNAs. These results will be helpful for further studies to reveal the biological functions and translation regulatory mechanisms of sgRNAs in the coronavirus life cycle and pathogenesis.

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Section: Resultssupporting

confidence: 91%

Section: Resultsmentioning

confidence: 99%

Translational control of the subgenomic RNAs of severe acute respiratory syndrome coronavirus

et al. 2009

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“…ORF8b encodes an 84-aa polypeptide and residues 9-84 are identical to the C-terminal of 8ab (Oostra et al, 2007). Whereas Keng et al have demonstrated by indirect immunofluorescence that 8a and 8b are expressed in SARS-CoVinfected Vero E6 cells, Oostra et al were unable to detect 8b in SARS-CoV-infected Vero E6 cells (Oostra et al, 2007;Keng et al, 2006). Although there is no data regarding the expression of 8a or 8b in vivo, Chen et al have identified anti-p8a antibodies in two out of 37 patients with SARS (Chen et al, 2007).…”

Section: Sars-cov P7bmentioning

confidence: 99%

Accessory proteins of SARS-CoV and other coronaviruses

et al. 2014

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The huge RNA genome of SARS coronavirus comprises a number of open reading frames that code for a total of eight accessory proteins. Although none of these are essential for virus replication, some appear to have a role in virus pathogenesis. Notably, some SARS-CoV accessory proteins have been shown to modulate the interferon signaling pathways and the production of pro-inflammatory cytokines. The structural information on these proteins is also limited, with only two (p7a and p9b) having their structures determined by X-ray crystallography. This review makes an attempt to summarize the published knowledge on SARS-CoV accessory proteins, with an emphasis on their involvement in virus-host interaction. The accessory proteins of other coronaviruses are also briefly discussed. This paper forms part of a series of invited articles in Antiviral Research on "From SARS to MERS: 10 years of research on highly pathogenic human coronaviruses" (see Introduction by Hilgenfeld and Peiris (2013)).

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“…Not only do in vitro and in vivo studies show that ORF8ab is ubiquitinated, but both ORF8a and ORF8b also binds to monoubiquitin and polyubiquitin, suggesting the potential involvement of these proteins in the pathogenesis of SARS-CoV [116]. ORF8ab interacts with SARS-CoV proteins S, M, ORF3a and ORF7a [118], all of which have been shown to be structural proteins. …”

Section: Sars Accessory Proteinsmentioning

confidence: 99%

“…ORF8b down-regulates the expression of SARS-CoV E, a process that could be inhibited by the addition of proteasome inhibitors [116]. For this reason, E is not detectable in SARS-CoV-infected cells that are expressing high levels of ORF8b [118]. Similarly to ORF6, overexpression of ORF8b in mammalian cells also induces DNA synthesis.…”

Section: Sars Accessory Proteinsmentioning

confidence: 99%

The Role of Severe Acute Respiratory Syndrome (SARS)-Coronavirus Accessory Proteins in Virus Pathogenesis

McBride

Fielding

2012

Viruses

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A respiratory disease caused by a novel coronavirus, termed the severe acute respiratory syndrome coronavirus (SARS-CoV), was first reported in China in late 2002. The subsequent efficient human-to-human transmission of this virus eventually affected more than 30 countries worldwide, resulting in a mortality rate of ~10% of infected individuals. The spread of the virus was ultimately controlled by isolation of infected individuals and there has been no infections reported since April 2004. However, the natural reservoir of the virus was never identified and it is not known if this virus will re-emerge and, therefore, research on this virus continues. The SARS-CoV genome is about 30 kb in length and is predicted to contain 14 functional open reading frames (ORFs). The genome encodes for proteins that are homologous to known coronavirus proteins, such as the replicase proteins (ORFs 1a and 1b) and the four major structural proteins: nucleocapsid (N), spike (S), membrane (M) and envelope (E). SARS-CoV also encodes for eight unique proteins, called accessory proteins, with no known homologues. This review will summarize the current knowledge on SARS-CoV accessory proteins and will include: (i) expression and processing; (ii) the effects on cellular processes; and (iii) functional studies.

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The human severe acute respiratory syndrome coronavirus (SARS-CoV) 8b protein is distinct from its counterpart in animal SARS-CoV and down-regulates the expression of the envelope protein in infected cells

Cited by 55 publications

References 35 publications

Translational control of the subgenomic RNAs of severe acute respiratory syndrome coronavirus

Translational control of the subgenomic RNAs of severe acute respiratory syndrome coronavirus

Accessory proteins of SARS-CoV and other coronaviruses

The Role of Severe Acute Respiratory Syndrome (SARS)-Coronavirus Accessory Proteins in Virus Pathogenesis

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