Determination of the rate of monomer interchange in a ligand-bound homodimeric protein from NOESY cross peaks: Application to the HIV protease/KNI-529 complex

被引:11
作者
Katoh, E
Yamazaki, T [1 ]
Kiso, Y
Wingfield, PT
Stahl, SJ
Kaufman, JD
Torchia, DA
机构
[1] Natl Inst Agrobiol Resources, Struct Biol Unit, Tsukuba, Ibaraki 3058602, Japan
[2] Kyoto Pharmaceut Univ, Dept Med Chem, Yamashima Ku, Kyoto 6078414, Japan
[3] Natl Inst Dent & Craniofacial Res, Mol Struct Biol Unit, NIAMSD, Prot Express Lab,NIH, Bethesda, MD 20892 USA
来源
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY | 1999年 / 121卷 / 11期
关键词
D O I
10.1021/ja984041v
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
引用
收藏
页码:2607 / 2608
页数:2
相关论文
共 16 条
[1]   STRUCTURE OF HIV-1 PROTEASE WITH KNI-272, A TIGHT-BINDING TRANSITION-STATE ANALOG CONTAINING ALLOPHENYLNORSTATINE [J].
BALDWIN, ET ;
BHAT, TN ;
GULNIK, S ;
LIU, BS ;
TOPOL, IA ;
KISO, Y ;
MIMOTO, T ;
MITSUYA, H ;
ERICKSON, JW .
STRUCTURE, 1995, 3 (06) :581-590
[2]   A HETERONUCLEAR CORRELATION EXPERIMENT FOR SIMULTANEOUS DETERMINATION OF N-15 LONGITUDINAL DECAY AND CHEMICAL-EXCHANGE RATES OF SYSTEMS IN SLOW EQUILIBRIUM [J].
FARROW, NA ;
ZHANG, OW ;
FORMANKAY, JD ;
KAY, LE .
JOURNAL OF BIOMOLECULAR NMR, 1994, 4 (05) :727-734
[3]   Flexibility and function in HIV protease: Dynamics of the HIV-1 protease bound to the asymmetric inhibitor kynostatin 272 (KNI-272) [J].
Freedberg, DI ;
Wang, YX ;
Stahl, SJ ;
Kaufman, JD ;
Wingfield, PT ;
Kiso, Y ;
Torchia, DA .
JOURNAL OF THE AMERICAN CHEMICAL SOCIETY, 1998, 120 (31) :7916-7923
[4]   INVESTIGATION OF EXCHANGE PROCESSES BY 2-DIMENSIONAL NMR-SPECTROSCOPY [J].
JEENER, J ;
MEIER, BH ;
BACHMANN, P ;
ERNST, RR .
JOURNAL OF CHEMICAL PHYSICS, 1979, 71 (11) :4546-4553
[5]   ACTIVE HUMAN IMMUNODEFICIENCY VIRUS PROTEASE IS REQUIRED FOR VIRAL INFECTIVITY [J].
KOHL, NE ;
EMINI, EA ;
SCHLEIF, WA ;
DAVIS, LJ ;
HEIMBACH, JC ;
DIXON, RAF ;
SCOLNICK, EM ;
SIGAL, IS .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1988, 85 (13) :4686-4690
[6]   RATIONAL DESIGN OF POTENT, BIOAVAILABLE, NONPEPTIDE CYCLIC UREAS AS HIV PROTEASE INHIBITORS [J].
LAM, PYS ;
JADHAV, PK ;
EYERMANN, CJ ;
HODGE, CN ;
RU, Y ;
BACHELER, LT ;
MEEK, JL ;
OTTO, MJ ;
RAYNER, MM ;
WONG, YN ;
CHANG, CH ;
WEBER, PC ;
JACKSON, DA ;
SHARPE, TR ;
ERICKSONVIITANEN, S .
SCIENCE, 1994, 263 (5145) :380-384
[7]   Molecular basis of resistance to HIV-1 protease inhibition:: A plausible hypothesis [J].
Luque, I ;
Todd, MJ ;
Gómez, J ;
Semo, N ;
Freire, E .
BIOCHEMISTRY, 1998, 37 (17) :5791-5797
[8]   FLEXIBILITY AND FUNCTION IN HIV-1 PROTEASE [J].
NICHOLSON, LK ;
YAMAZAKI, T ;
TORCHIA, DA ;
GRZESIEK, S ;
BAX, A ;
STAHL, SJ ;
KAUFMAN, JD ;
WINGFIELD, PT ;
LAM, PYS ;
JADHAV, PK ;
HODGE, CN ;
DOMAILLE, PJ ;
CHANG, CH .
NATURE STRUCTURAL BIOLOGY, 1995, 2 (04) :274-280
[9]   DISULFIDE BOND ISOMERIZATION IN BPTI AND BPTI(G36S) - AN NMR-STUDY OF CORRELATED MOBILITY IN PROTEINS [J].
OTTING, G ;
LIEPINSH, E ;
WUTHRICH, K .
BIOCHEMISTRY, 1993, 32 (14) :3571-3582
[10]   HUMAN-IMMUNODEFICIENCY-VIRUS - PROTEASE UNINHIBITED [J].
RICHMAN, DD .
NATURE, 1995, 374 (6522) :494-494
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