SARS-CoV (severe acute respiratory syndrome-associated coronavirus) caused infection of ~8000 people and death of ~800 patients around the world during the 2003 outbreak. In addition, picornaviruses such as enterovirus, coxsackievirus and rhinovirus also can cause life-threatening diseases. Replication of picornaviruses and coronaviruses requires 3Cpro (3C protease) and 3CLpro (3C-like protease) respectively, which are structurally analogous with chymotrypsin-fold, but the former is a monomer and the latter is dimeric due to an extra third domain for dimerization. Subtle structural differences in the S2 and S3 pockets of these proteases make inhibitors selective, but some dual inhibitors have been discovered. Our findings as summarized in the present review provide new potential anti-coronavirus and anti-picornavirus therapeutic agents and a clue to convert 3CLpro inhibitors into 3Cpro inhibitors and vice versa.
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October 2011
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Conference Article|
September 21 2011
Recent development of 3C and 3CL protease inhibitors for anti-coronavirus and anti-picornavirus drug discovery Available to Purchase
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R. Ramajayam;
R. Ramajayam
1Institute of Biological Chemistry, Academia Sinica, Taipei 11529, Taiwan
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Kian-Pin Tan;
Kian-Pin Tan
1Institute of Biological Chemistry, Academia Sinica, Taipei 11529, Taiwan
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Po-Huang Liang
Po-Huang Liang
1
1Institute of Biological Chemistry, Academia Sinica, Taipei 11529, Taiwan
1To whom correspondence should be addressed (email [email protected]).
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Publisher: Portland Press Ltd
Received:
May 13 2011
Online ISSN: 1470-8752
Print ISSN: 0300-5127
© The Authors Journal compilation © 2011 Biochemical Society
2011
Biochem Soc Trans (2011) 39 (5): 1371–1375.
Article history
Received:
May 13 2011
Citation
R. Ramajayam, Kian-Pin Tan, Po-Huang Liang; Recent development of 3C and 3CL protease inhibitors for anti-coronavirus and anti-picornavirus drug discovery. Biochem Soc Trans 1 October 2011; 39 (5): 1371–1375. doi: https://doi.org/10.1042/BST0391371
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