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STRUCTURE AT 2.5-A RESOLUTION OF CHEMICALLY SYNTHESIZED HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 PROTEASE COMPLEXED WITH A HYDROXYETHYLENE-BASED INHIBITOR

被引:235
作者
JASKOLSKI, M
TOMASSELLI, AG
SAWYER, TK
STAPLES, DG
HEINRIKSON, RL
SCHNEIDER, J
KENT, SBH
WLODAWER, A
机构
[1] NCI,FREDERICK CANC RES FACIL,MACROMOLEC STRUCT LAB,FREDERICK,MD 21701
[2] BASIC RES PROGRAM,ANAT BIOL LAB,CTR DEV,FREDERICK,MD 21702
[3] BOND UNIV,GRAD SCH SCI & TECHNOL,GOLD COAST,QLD 4229,AUSTRALIA
[4] UPJOHN CO,BIOPOLYMER CHEM UNIT,KALAMAZOO,MI 49001
[5] CALTECH,DIV BIOL,PASADENA,CA 91125
来源
BIOCHEMISTRY | 1991年 / 30卷 / 06期
关键词
D O I
10.1021/bi00220a023
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The crystal structure of a complex between chemically synthesized human immunodeficiency virus type 1 (HIV-1) protease and an octapeptide inhibitor has been refined to an R factor of 0.138 at 2.5-angstrom resolution. The substrate-based inhibitor, H-Val-Ser-Gln-Asn-Leu-PSI[CH(OH)CH2]Val-Ile-Val-OH (U-85548e) contains a hydroxyethylene isostere replacement at the scissile bond that is believed to mimic the tetrahedral transition state of the proteolytic reaction. This potent inhibitor has K(i) < 1 nM and was developed as an active-site titrant of the HIV-1 protease. The inhibitor binds in an extended conformation and is involved in beta-sheet interactions with the active-site floor and flaps of the enzyme, which form the substrate/inhibitor cavity. The inhibitor diastereomer has the S configuration at the chiral carbon atom of the hydroxyethylene insert, and the hydroxyl group is within H-bonding distance of the two active-site carboxyl groups in the enzyme dimer. The two subunits of the enzyme are related by a pseudodyad, which superposes them at a 178-degrees rotation. The main difference between the subunits is in the beta turns of the flaps, which have different conformations in the two monomers. The inhibitor has a clear preferred orientation in the active site and the alternative conformation, if any, is a minor one (occupancy of less than 30%). A new model of the enzymatic mechanism is proposed in which the proteolytic reaction is viewed as a one-step process during which the nucleophile (water molecule) and electrophile (an acidic proton) attack the scissile bond in a concerted manner.
引用
收藏
页码:1600 / 1609
页数:10
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