Human Coronavirus 229E Papain-Like Proteases Have Overlapping Specificities but Distinct Functions in Viral Replication

Ziebuhr, John; Schelle, Barbara; Karl, Nadja; Minskaia, Ekaterina; Bayer, Sonja; Siddell, Stuart G.; Gorbalenya, Alexander E.; Thiel, Volker

doi:10.1128/jvi.02091-06

Cited by 54 publications

(57 citation statements)

References 67 publications

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“…As discussed recently by Catic et al [28], it remains to be shown if these enzymes truly act as deubiquitinating enzymes in vivo. In vivo, however, the SARS-CoV PLpro is part of nsp3 localized to the membrane-bound viral replicase complex [29]. Deubiquitination of host substrate(s) in the context of a SARS-CoV infection, however, remains to be demonstrated.…”

Section: Resultsmentioning

confidence: 99%

Selectivity in ISG15 and ubiquitin recognition by the SARS coronavirus papain-like protease

Lindner

Lytvyn

et al. 2007

Archives of Biochemistry and Biophysics

149

172

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The severe acute respiratory syndrome coronavirus papain-like protease (SARS-CoV PLpro) carries out N-terminal processing of the viral replicase polyprotein, and also exhibits Lys48-linked polyubiquitin chain debranching and ISG15 precursor processing activities in vitro. Here, we used SDS-PAGE and fluorescence-based assays to demonstrate that ISG15 derivatives are the preferred substrates for the deubiquitinating activity of the PLpro. With k(cat)/K(M) of 602,000 M(-1)s(-1), PLpro hydrolyzes ISG15-AMC 30- and 60-fold more efficiently than Ub-AMC and Nedd8-AMC, respectively. Data obtained with truncated ISG15 and hybrid Ub/ISG15 substrates indicate that both the N- and C-terminal Ub-like domains of ISG15 contribute to this preference. The enzyme also displays a preference for debranching Lys48- over Lys63-linked polyubiquitin chains. Our results demonstrate that SARS-CoV PLpro can differentiate between ubiquitin-like modifiers sharing a common C-terminal sequence, and that the debranching activity of the PLpro is linkage type selective. The potential structural basis for the demonstrated specificity of SARS-CoV PLpro is discussed.

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Section: Resultsmentioning

confidence: 99%

Selectivity in ISG15 and ubiquitin recognition by the SARS coronavirus papain-like protease

Lindner

Lytvyn

et al. 2007

Archives of Biochemistry and Biophysics

149

172

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“…Human coronavirus NL63 (HCoV-NL63) PL1 pro processes Nsp1↓2 while the PL2 pro processes the other two cleavage sites, Nsp2↓3 and Nsp3↓4 (Table 2; Chen et al, 2007). Both PL1 pro and PL2 pro of HCoV 229E can cleave Nsp1↓2 and 2↓ 3 (Table 2); however, the PL1 pro is more efficient in cleaving Nsp1↓2 while the PL2 pro is more efficient with respect to the latter site (Ziebuhr et al, 2007). Some viruses, such as SARS-CoV, MERS-CoV, and IBV, comprise only one functional PL2 pro to process all three cleavage sites ( Table 2).…”

Section: Papain-like Protease 1 Domainmentioning

confidence: 99%

Nsp3 of coronaviruses: Structures and functions of a large multi-domain protein

2018

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The multi-domain non-structural protein 3 (Nsp3) is the largest protein encoded by the coronavirus (CoV) genome, with an average molecular mass of about 200 kD. Nsp3 is an essential component of the replication/transcription complex. It comprises various domains, the organization of which differs between CoV genera, due to duplication or absence of some domains. However, eight domains of Nsp3 exist in all known CoVs: the ubiquitin-like domain 1 (Ubl1), the Glu-rich acidic domain (also called "hypervariable region"), a macrodomain (also named "X domain"), the ubiquitin-like domain 2 (Ubl2), the papain-like protease 2 (PL2), the Nsp3 ectodomain (3Ecto, also called "zinc-finger domain"), as well as the domains Y1 and CoV-Y of unknown functions. In addition, the two transmembrane regions, TM1 and TM2, exist in all CoVs. The three-dimensional structures of domains in the N-terminal two thirds of Nsp3 have been investigated by X-ray crystallography and/or nuclear magnetic resonance (NMR) spectroscopy since the outbreaks of Severe Acute Respiratory Syndrome coronavirus (SARS-CoV) in 2003 as well as Middle-East Respiratory Syndrome coronavirus (MERS-CoV) in 2012. In this review, the structures and functions of these domains of Nsp3 are discussed in depth.

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“…The homologous enzyme, PLP2, from the human coronavirus 229E, has been shown to be critical to 229E viral replication 13. In addition, recent studies have shown that human deubiquitinating enzymes are potential anticancer drug-design targets.…”

Section: Introductionmentioning

confidence: 99%

Severe Acute Respiratory Syndrome Coronavirus Papain-like Novel Protease Inhibitors: Design, Synthesis, Protein−Ligand X-ray Structure and Biological Evaluation

et al. 2010

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The design, synthesis, X-ray crystal structure, molecular modeling, and biological evaluation of a series of new generation SARS-CoV PLpro inhibitors are described. A new lead compound 3 (6577871) was identified via high-throughput screening of a diverse chemical library. Subsequently, we carried out lead optimization and structure-activity studies to provide a series of improved inhibitors that show potent PLpro inhibition and antiviral activity against SARS-CoV infected Vero E6 cells. Interestingly, the (S)-Me inhibitor 15h (enzyme IC50 = 0.56 μM; antiviral EC50 = 9.1 μM) and the corresponding (R)-Me 15g (IC50 = 0.32 μM; antiviral EC50 = 9.1 μM) are the most potent compounds in this series, with nearly equivalent enzymatic inhibition and antiviral activity. A protein-ligand X-ray structure of 15g-bound SARS-CoV PLpro and a corresponding model of 15h docked to PLpro provide intriguing molecular insight into the ligand-binding site interactions.

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Human Coronavirus 229E Papain-Like Proteases Have Overlapping Specificities but Distinct Functions in Viral Replication

Cited by 54 publications

References 67 publications

Selectivity in ISG15 and ubiquitin recognition by the SARS coronavirus papain-like protease

Selectivity in ISG15 and ubiquitin recognition by the SARS coronavirus papain-like protease

Nsp3 of coronaviruses: Structures and functions of a large multi-domain protein

Severe Acute Respiratory Syndrome Coronavirus Papain-like Novel Protease Inhibitors: Design, Synthesis, Protein−Ligand X-ray Structure and Biological Evaluation

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