COMPLEX-FORMATION BETWEEN THE NS3 SERINE-TYPE PROTEINASE OF THE HEPATITIS-C VIRUS AND NS4A AND ITS IMPORTANCE FOR POLYPROTEIN MATURATION

被引：200

作者：

BARTENSCHLAGER, R ^{[1
]}

LOHMANN, V ^{[1
]}

WILKINSON, T ^{[1
]}

KOCH, JO ^{[1
]}

机构：

[1] ROCHE PROD LTD,WELWYN GARDEN CIT AL7 3AY,HERTS,ENGLAND

来源：

JOURNAL OF VIROLOGY | 1995年 / 69卷 / 12期

关键词：

D O I：

10.1128/JVI.69.12.7519-7528.1995

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

Processing of the hepatitis C virus polyprotein is mediated by host cell signalases and at least two virally encoded proteinases. Of these, the serine-type proteinase encompassing the amino-terminal one-third of NS3 is responsible for cleavage at the four sites carboxy terminal of NS3. The activity of this proteinase is modulated by NS4A, a 54-amino-acid polyprotein cleavage product essential for processing at the NS3/4A, NS4A/4B, and NS4B/5A sites and enhancing cleavage efficiency between NS5A and NS5B. Using the vaccinia virus-T7 hybrid system to express hepatitis C virus polypeptides in BHK-21 cells, we studied the role of NS4A in proteinase activation. We found that the NS3 proteinase and NS4A form a stable complex when expressed as a single polyprotein or as separate molecules. Results from deletion mapping show that the minimal NS4A domain required for proteinase activation is located in the center of NS4A between amino acids 1675 and 1686 of the polyprotein. Amino acid substitutions within this domain destabilizing the NS3-NS4A complex also impair trans cleavage at the NS4A-dependent sites. Similarly, deletion of amino-terminal NS3 sequences impairs complex formation as well as cleavage at the NS4B/5A site but not at the NS4A-independent NS5A/5B site. These results suggest that a stable NS3-NS4A interaction is important for cleavage at the NS4A-dependent sites and that amino-terminal NS3 sequences and the central NS4A domain are directly involved in complex formation.

引用

页码：7519 / 7528

页数：10

共 43 条

[1] NS2B-3 PROTEINASE-MEDIATED PROCESSING IN THE YELLOW-FEVER VIRUS STRUCTURAL REGION - IN-VITRO AND IN-VIVO STUDIES
AMBERG, SM
NESTOROWICZ, A
MCCOURT, DW
RICE, CM
[J]. JOURNAL OF VIROLOGY, 1994, 68 (06) : 3794 - 3802
[2] DENGUE-2 VIRUS NS2B AND NS3 FORM A STABLE COMPLEX THAT CAN CLEAVE NS3 WITHIN THE HELICASE DOMAIN
ARIAS, CF
PREUGSCHAT, F
STRAUSS, JH
[J]. VIROLOGY, 1993, 193 (02) : 888 - 899
[3] A PROTEIN-FOLDING REACTION UNDER KINETIC CONTROL
BAKER, D
SOHL, JL
AGARD, DA
[J]. NATURE, 1992, 356 (6366) : 263 - 265
[4] NONSTRUCTURAL PROTEIN-3 OF THE HEPATITIS-C VIRUS ENCODES A SERINE-TYPE PROTEINASE REQUIRED FOR CLEAVAGE AT THE NS3/4 AND NS4/5 JUNCTIONS
BARTENSCHLAGER, R
AHLBORNLAAKE, L
MOUS, J
JACOBSEN, H
[J]. JOURNAL OF VIROLOGY, 1993, 67 (07) : 3835 - 3844
[5] KINETIC AND STRUCTURAL-ANALYSES OF HEPATITIS-C VIRUS POLYPROTEIN PROCESSING
BARTENSCHLAGER, R
AHLBORNLAAKE, L
MOUS, J
JACOBSEN, H
[J]. JOURNAL OF VIROLOGY, 1994, 68 (08) : 5045 - 5055
[6] MUTAGENESIS OF THE YELLOW-FEVER VIRUS NS2B PROTEIN - EFFECTS ON PROTEOLYTIC PROCESSING, NS2B-NS3 COMPLEX-FORMATION, AND VIRAL REPLICATION
CHAMBERS, TJ
NESTOROWICZ, A
AMBERG, SM
RICE, CM
[J]. JOURNAL OF VIROLOGY, 1993, 67 (11) : 6797 - 6807
[7] HEPATITIS-C - PROGRESS AND PROBLEMS
CUTHBERT, JA
[J]. CLINICAL MICROBIOLOGY REVIEWS, 1994, 7 (04) : 505 - &
[8] CLEAVAGE-SITE PREFERENCES OF SINDBIS VIRUS POLYPROTEINS CONTAINING THE NONSTRUCTURAL PROTEINASE - EVIDENCE FOR TEMPORAL REGULATION OF POLYPROTEIN PROCESSING INVIVO
DEGROOT, RJ
HARDY, WR
SHIRAKO, Y
STRAUSS, JH
[J]. EMBO JOURNAL, 1990, 9 (08) : 2631 - 2638
[9] DUBOISSON J, 1994, J VIROL, V68, P6147
[10] THE HEPATITIS-C VIRUS ENCODES A SERINE PROTEASE INVOLVED IN PROCESSING OF THE PUTATIVE NONSTRUCTURAL PROTEINS FROM THE VIRAL POLYPROTEIN PRECURSOR
ECKART, MR
SELBY, M
MASIARZ, F
LEE, C
BERGER, K
CRAWFORD, K
KUO, C
KUO, G
HOUGHTON, M
CHOO, QL
[J]. BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1993, 192 (02) : 399 - 406

← 1 2 3 4 5 →