WEAK BINDING OF VX-478 TO HUMAN PLASMA-PROTEINS AND IMPLICATIONS FOR ANTI-HUMAN-IMMUNODEFICIENCY-VIRUS THERAPY

被引:73
作者
LIVINGSTON, DJ [1 ]
PAZHANISAMY, S [1 ]
PORTER, DJT [1 ]
PARTALEDIS, JA [1 ]
TUNG, RD [1 ]
PAINTER, GR [1 ]
机构
[1] BURROUGHS WELLCOME CO, RES TRIANGLE PK, NC 27709 USA
来源
JOURNAL OF INFECTIOUS DISEASES | 1995年 / 172卷 / 05期
关键词
D O I
10.1093/infdis/172.5.1238
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
VX-478 is a potent inhibitor of human immunodeficiency virus type 1 (HIV-1) protease (K-i, 0.6 nM) and of HIV-1 replication in antiviral assays (IC90, 80 nM). The fractional binding of VX-478 to human plasma and to purified plasma proteins was determined by equilibrium dialysis and difference UV spectrophotometry. Binding to alpha(1)-acid glycoprotein (89% at 2 mu m total drug concentration, K-d of 4 mu M) accounts for its fractional binding in plasma (93%). Stopped-flow spectrophotometry methods showed that binding is a reversible two-step process. The measured dissociation rate constant approaches 100 s(-1). The antiviral effect of VX-478 was determined in the presence of 45% human plasma, in which the IC90 increased by 1.5-fold compared with control experiments in the presence of 15% fetal bovine serum. The effects of protein binding on the antiviral activity of VX-478 are minor, as expected for a weak drug-protein interaction.
引用
收藏
页码:1238 / 1245
页数:8
相关论文
共 31 条
[1]  
BABA M, 1993, BIOCHEM PHARMACOL, V45, P2507
[2]   REDUCTION OF THE IN-VITRO ACTIVITY OF A77003, AN INHIBITOR OF HUMAN-IMMUNODEFICIENCY-VIRUS PROTEASE, BY HUMAN SERUM ALPHA(1) ACID GLYCOPROTEIN [J].
BILELLO, JA ;
BILELLO, PA ;
PRICHARD, M ;
ROBINS, T ;
DRUSANO, GL .
JOURNAL OF INFECTIOUS DISEASES, 1995, 171 (03) :546-551
[3]   IN-VIVO EMERGENCE OF HIV-1 VARIANTS RESISTANT TO MULTIPLE PROTEASE INHIBITORS [J].
CONDRA, JH ;
SCHLEIF, WA ;
BLAHY, OM ;
GABRYELSKI, LJ ;
GRAHAM, DJ ;
QUINTERO, JC ;
RHODES, A ;
ROBBINS, HL ;
ROTH, E ;
SHIVAPRAKASH, M ;
TITUS, D ;
YANG, T ;
TEPPLER, H ;
SQUIRES, KE ;
DEUTSCH, PJ ;
EMINI, EA .
NATURE, 1995, 374 (6522) :569-571
[4]  
DANNER SA, 1993, 9 INT C AIDS 4 STD W
[5]  
Darke P L, 1994, Adv Pharmacol, V25, P399, DOI 10.1016/S1054-3589(08)60438-X
[6]   HUMAN-IMMUNODEFICIENCY-VIRUS PROTEASE - A TARGET FOR AIDS THERAPY [J].
DEBOUCK, C ;
METCALF, BW .
DRUG DEVELOPMENT RESEARCH, 1990, 21 (01) :1-17
[7]   L-735,524 - THE DESIGN OF A POTENT AND ORALLY BIOAVAILABLE HIV PROTEASE INHIBITOR [J].
DORSEY, BD ;
LEVIN, RB ;
MCDANIEL, SL ;
VACCA, JP ;
GUARE, JP ;
DARKE, PL ;
ZUGAY, JA ;
EMINI, EA ;
SCHLEIF, WA ;
QUINTERO, JC ;
LIN, JH ;
CHEN, IW ;
HOLLOWAY, MK ;
FITZGERALD, PMD ;
AXEL, MG ;
OSTOVIC, D ;
ANDERSON, PS ;
HUFF, JR .
JOURNAL OF MEDICINAL CHEMISTRY, 1994, 37 (21) :3443-3451
[8]  
FISCHL MA, 1995, 2ND NAT C HUM RETR R
[9]   IMPORTANCE OF PROTEIN-BINDING FOR THE INTERPRETATION OF SERUM OR PLASMA DRUG CONCENTRATIONS [J].
GREENBLATT, DJ ;
SELLERS, EM ;
KOCHWESER, J .
JOURNAL OF CLINICAL PHARMACOLOGY, 1982, 22 (5-6) :259-263
[10]   RAPID TURNOVER OF PLASMA VIRIONS AND CD4 LYMPHOCYTES IN HIV-1 INFECTION [J].
HO, DD ;
NEUMANN, AU ;
PERELSON, AS ;
CHEN, W ;
LEONARD, JM ;
MARKOWITZ, M .
NATURE, 1995, 373 (6510) :123-126
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