Serpin mechanism of hepatitis C virus nonstructural 3 (NS3) protease inhibition - Induced fit as a mechanism for narrow specificity

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dc.contributor.author Richer, M. J.
dc.contributor.author Juliano, Luiz [UNIFESP]
dc.contributor.author Hashimoto, C.
dc.contributor.author Jean, F.
dc.date.accessioned 2016-01-24T12:37:03Z
dc.date.available 2016-01-24T12:37:03Z
dc.date.issued 2004-03-12
dc.identifier http://dx.doi.org/10.1074/jbc.M313852200
dc.identifier.citation Journal of Biological Chemistry. Bethesda: Amer Soc Biochemistry Molecular Biology Inc, v. 279, n. 11, p. 10222-10227, 2004.
dc.identifier.issn 0021-9258
dc.identifier.uri http://repositorio.unifesp.br/handle/11600/27674
dc.description.abstract Hepatitis C virus (HCV) nonstructural 3 (NS3) serine protease disrupts important cellular antiviral signaling pathways and plays a pivotal role in the proteolytic maturation of the HCV polyprotein precursor. This recent discovery has fostered the search for NS3 protease inhibitors. However, the enzyme's unusual induced fit behavior and peculiar molecular architecture have imposed considerable obstacles to the development of small molecule inhibitors. in this article, we demonstrate that such unique induced fit behavior and the chymotrypsin-like catalytic domain can provide the structural plasticity necessary to generate protein-based inhibitors of the NS3 protease. We took advantage of the macromolecular scaffold of a Drosophila serpin, SP6, which intrinsically supports chymotrypsin-like enzyme inhibition, to design a novel class of potent and selective inhibitors. We show that altering the SP6 reactive site loop (RSL) resulted in the development of the first effective (K-i of 34 nM) and selective serpin, SP6(EVC/S), directed at the NS3 protease. SP6(EVC/S) operates as a suicide substrate inhibitor, and its partitioning between the complex-forming and proteolytic pathways for the NS3 protease is HCV NS4A cofactor-dependent and - specific. Once bound to the protease active site, SP6(EVC/S) partitions with equal probability to undergo proteolysis by NS3 at the C-terminal site of the engineered RSL, (P-6) Glu-Ile-( P-4) Val-Met-Thr-(P-1) Cys- down arrow-(P-1') Ser, or to form a covalent acyl-enzyme complex characteristic of cognate protease-serpin pairs. Our results also reveal a novel cofactor-induced serpin mechanism of enzyme inhibition that could be explored for developing effective and selective inhibitors of other important induced fit viral proteases of the Flaviviridae family such as the West Nile virus NS3 endoprotease. en
dc.format.extent 10222-10227
dc.language.iso eng
dc.publisher Amer Soc Biochemistry Molecular Biology Inc
dc.relation.ispartof Journal of Biological Chemistry
dc.rights Acesso aberto
dc.title Serpin mechanism of hepatitis C virus nonstructural 3 (NS3) protease inhibition - Induced fit as a mechanism for narrow specificity en
dc.type Artigo
dc.contributor.institution Univ British Columbia
dc.contributor.institution Universidade Federal de São Paulo (UNIFESP)
dc.contributor.institution Yale Univ
dc.description.affiliation Univ British Columbia, Dept Microbiol & Immunol, Vancouver, BC V6T 1Z3, Canada
dc.description.affiliation Escola Paulista Med, Dept Biophys, BR-04044020 São Paulo, Brazil
dc.description.affiliation Yale Univ, Sch Med, Dept Cell Biol, New Haven, CT 06520 USA
dc.description.affiliationUnifesp Escola Paulista Med, Dept Biophys, BR-04044020 São Paulo, Brazil
dc.identifier.doi 10.1074/jbc.M313852200
dc.description.source Web of Science
dc.identifier.wos WOS:000220050400069



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