学术探索
学术期刊
新闻热点
数据分析
智能评审

Probing the substrate specificity of hepatitis C virus NS3 serine protease by using synthetic peptides

被引:89
作者
Zhang, RM
Durkin, J
Windsor, WT
McNemar, C
Ramanathan, L
Le, HV
机构
来源
JOURNAL OF VIROLOGY | 1997年 / 71卷 / 08期
关键词
D O I
10.1128/JVI.71.8.6208-6213.1997
中图分类号
Q93 [微生物学];
学科分类号
071005 ; 100705 ;
摘要
We probed the substrate specificity of a recombinant noncovalent complex of the full-length hepatitis C virus (HCV) NS3 serine protease and NS4A cofactor, using a series of small synthetic peptides derived from the three trans-cleavage sites of the HCV nonstructural protein sequence. We observed a distinct cleavage site preference exhibited by the enzyme complex. The values of the turnover number (k(cat)) for the most efficient NS4A/4B, 4B/5A, and 5A/5B peptide substrates were 1.6, 11, and 8 min(-1), respectively, and the values for the corresponding Michaelis-Menten constants (K-m) were 280, 160, and 16 mu M, providing catalytic efficiency values (k(cat)/K-m) of 92, 1,130, and 8,300 M-1 s(-1). An alanine-scanning study for an NS5A/5B substrate (P6P4') revealed that P1 Cys and P3 Val were critical. Finally, substitutions at the scissile P1 Cys residue by homocysteine (Hcy), S-methylcysteine (Mcy), Ala, S-ethylcysteine (Ecy), Thr, Met, D-Cys, Ser, and penicillamine (Pen) produced progressively less efficient substrates, revealing a stringent stereochemical requirement for a Cys residue at this position.
引用
收藏
页码:6208 / 6213
页数:6
相关论文
共 49 条
[1]   THE NATURAL-HISTORY OF COMMUNITY-ACQUIRED HEPATITIS-C IN THE UNITED-STATES [J].
ALTER, MJ ;
MARGOLIS, HS ;
KRAWCZYNSKI, K ;
JUDSON, FN ;
MARES, A ;
ALEXANDER, WJ ;
HU, PY ;
MILLER, JK ;
GERBER, MA ;
SAMPLINER, RE ;
MEEKS, EL ;
BEACH, MJ .
NEW ENGLAND JOURNAL OF MEDICINE, 1992, 327 (27) :1899-1905
[2]   NONSTRUCTURAL PROTEIN-3 OF THE HEPATITIS-C VIRUS ENCODES A SERINE-TYPE PROTEINASE REQUIRED FOR CLEAVAGE AT THE NS3/4 AND NS4/5 JUNCTIONS [J].
BARTENSCHLAGER, R ;
AHLBORNLAAKE, L ;
MOUS, J ;
JACOBSEN, H .
JOURNAL OF VIROLOGY, 1993, 67 (07) :3835-3844
[3]   SUBSTRATE DETERMINANTS FOR CLEAVAGE IN CIS AND IN TRANS BY THE HEPATITIS-C VIRUS NS3 PROTEINASE [J].
BARTENSCHLAGER, R ;
AHLBORNLAAKE, L ;
YASARGIL, K ;
MOUS, J ;
JACOBSEN, H .
JOURNAL OF VIROLOGY, 1995, 69 (01) :198-205
[4]   COMPLEX-FORMATION BETWEEN THE NS3 SERINE-TYPE PROTEINASE OF THE HEPATITIS-C VIRUS AND NS4A AND ITS IMPORTANCE FOR POLYPROTEIN MATURATION [J].
BARTENSCHLAGER, R ;
LOHMANN, V ;
WILKINSON, T ;
KOCH, JO .
JOURNAL OF VIROLOGY, 1995, 69 (12) :7519-7528
[5]   KINETIC AND STRUCTURAL-ANALYSES OF HEPATITIS-C VIRUS POLYPROTEIN PROCESSING [J].
BARTENSCHLAGER, R ;
AHLBORNLAAKE, L ;
MOUS, J ;
JACOBSEN, H .
JOURNAL OF VIROLOGY, 1994, 68 (08) :5045-5055
[6]   Synthetic depsipeptide substrates for the assay of human hepatitis C virus protease [J].
Bianchi, E ;
Steinkuhler, C ;
Taliani, M ;
Urbani, A ;
De Francesco, R ;
Pessi, A .
ANALYTICAL BIOCHEMISTRY, 1996, 237 (02) :239-244
[7]   HEPATITIS-C VIRUS-RNA IN SOUTHERN AFRICAN BLACKS WITH HEPATOCELLULAR-CARCINOMA [J].
BUKH, J ;
MILLER, RH ;
KEW, MC ;
PURCELL, RH .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (05) :1848-1851
[8]   EVIDENCE THAT THE N-TERMINAL DOMAIN OF NONSTRUCTURAL PROTEIN NS3 FROM YELLOW-FEVER VIRUS IS A SERINE PROTEASE RESPONSIBLE FOR SITE-SPECIFIC CLEAVAGES IN THE VIRAL POLYPROTEIN [J].
CHAMBERS, TJ ;
WEIR, RC ;
GRAKOUI, A ;
MCCOURT, DW ;
BAZAN, JF ;
FLETTERICK, RJ ;
RICE, CM .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1990, 87 (22) :8898-8902
[9]   Structure of the human cytomegalovirus protease catalytic domain reveals a novel serine protease fold and catalytic triad [J].
Chen, P ;
Tsuge, H ;
Almassy, RJ ;
Gribskov, CL ;
Katoh, S ;
Vanderpool, DL ;
Margosiak, SA ;
Pinko, C ;
Matthews, DA ;
Kan, CC .
CELL, 1996, 86 (05) :835-843
[10]   ISOLATION OF A CDNA CLONE DERIVED FROM A BLOOD-BORNE NON-A, NON-B VIRAL-HEPATITIS GENOME [J].
CHOO, QL ;
KUO, G ;
WEINER, AJ ;
OVERBY, LR ;
BRADLEY, DW ;
HOUGHTON, M .
SCIENCE, 1989, 244 (4902) :359-362
12345