Characterization and Inhibition of SARS-Coronavirus Main Protease

Liang, Po‐Huang

doi:10.2174/156802606776287090

Cited by 87 publications

(69 citation statements)

References 67 publications

(107 reference statements)

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“…It has the potential to inhibit the two proteases of SARS-CoV that are responsible for virus maturation (Lindner et al, 2005;Liang, 2006) (Barnard et al, 2006). Therefore, the compound was evaluated for efficacy against SARS-CoV replication in the mouse as an i.p.…”

Section: In Vivo Activitymentioning

confidence: 99%

Evaluation of Immunomodulators, Interferons and Known in Vitro SARS-CoV Inhibitors for Inhibition of SARS-Cov Replication in BALB/c Mice

Barnard

Day

Bailey

et al. 2006

Antivir Chem Chemother

208

193

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IFN-α-n3) did not significantly reduce lung virus titres in mice. Anti-inflammatory agents, chloroquine, amodiaquin and pentoxifylline, were also inactive in vivo, suggesting that although they may be useful in ameliorating the hyperinflammatory response induced by the virus infection, they will not significantly reduce the replication of the virus, the inducer of inflammatory response. Thus, anti-inflammatory agents may only be useful in treating virus lung infections if used in combination with agents that inhibit virus replication. In summary, the data suggest that induction of IFN by mismatched dsRNA or actual treatment with exogenous IFN-α can inhibit SARS-CoV replication in the lungs of mice.

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Section: In Vivo Activitymentioning

confidence: 99%

Evaluation of Immunomodulators, Interferons and Known in Vitro SARS-CoV Inhibitors for Inhibition of SARS-Cov Replication in BALB/c Mice

Barnard

Day

Bailey

et al. 2006

Antivir Chem Chemother

208

193

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“…The catalytic dyad Cys148-His41 and the substrate binding site of pro are located on the interface of Domain I and II, which is identified by the bound inhibitor N3 (Fig. 1B) (Liang, 2006;Lee et al, 2009). Although the inhibitory effect of inhibitor N3 to HCoV-EMC 3CL pro is not extremely good, it presents good pharmaceutical properties with comparable inhibitory activity (Fig.…”

mentioning

confidence: 99%

The newly emerged SARS-Like coronavirus HCoV-EMC also has an “Achilles’ heel”: current effective inhibitor targeting a 3C-like protease

et al. 2013

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“…Protease inhibitors have also been reviewed elsewhere (Liang, 2006;Ramajayam et al, 2011). In addition to its role in proteolytic processing of the viral polymerase, PLP2 is also involved in host evasion.…”

Section: Common Inhibitors Of Corona and Picornavirusesmentioning

confidence: 99%

How Prepared Are We to Control Severe Acute Respiratory Syndrome in Future

Bhardwaj¹

2013

American Journal of Virology

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No non-human reservoirs for smallpox-and polio-viruses has contributed to the success of worldwide eradication of smallpox and a significant control of poliomyelitis. Most emerging and re-emerging viruses including SARS Coronavirus (SARS-CoV), have animal reservoirs and therefore,they impose a constant threat of host jump leading tooutbreaksin humans. It is desirable to be ready for control of infections that are caused by zoonotic pathogens, even after an outbreak has ended. This literature review is a compilation of advances made so far for diagnosis and treatment of SARS.

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Characterization and Inhibition of SARS-Coronavirus Main Protease

Cited by 87 publications

References 67 publications

Evaluation of Immunomodulators, Interferons and Known in Vitro SARS-CoV Inhibitors for Inhibition of SARS-Cov Replication in BALB/c Mice

Evaluation of Immunomodulators, Interferons and Known in Vitro SARS-CoV Inhibitors for Inhibition of SARS-Cov Replication in BALB/c Mice

The newly emerged SARS-Like coronavirus HCoV-EMC also has an “Achilles’ heel”: current effective inhibitor targeting a 3C-like protease

How Prepared Are We to Control Severe Acute Respiratory Syndrome in Future

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