A SHORT-TERM STUDY OF THE SAFETY, PHARMACOKINETICS, AND EFFICACY OF RITONAVIR, AN INHIBITOR OF HIV-1 PROTEASE

被引：503

作者：

DANNER, SA

CARR, A

LEONARD, JM

LEHMAN, LM

GUDIOL, F

GONZALES, J

RAVENTOS, A

RUBIO, R

BOUZA, E

PINTADO, V

AGUADO, AG

DELOMAS, JG

DELGADO, R

BORLEFFS, JCC

HSU, A

VALDES, JM

BOUCHER, CAB

COOPER, DA

GIMENO, C

CLOTET, B

TOR, J

FERRER, E

MARTINEZ, PL

MORENO, S

ZANCADA, G

ALCAMI, J

NORIEGA, AR

PULIDO, F

GLASSMAN, HN

机构：

[1] ST VINCENTS HOSP,SYDNEY,NSW,AUSTRALIA

[2] ABBOTT LABS,ABBOTT PK,IL

[3] HOSP BELLVITGE PRINCIPES DE ESPANA,BARCELONA,SPAIN

[4] HOSP LA PAZ,MADRID,SPAIN

[5] HOSP GERMANS TRIAS & PUJOL,BARCELONA,SPAIN

[6] HOSP 12 OCTUBRE,MADRID,SPAIN

[7] HOSP GEN GREGORIO MARANON,MADRID,SPAIN

[8] HOSP RAMON Y CAJAL,MADRID,SPAIN

[9] HOSP CLIN VALENCIA,VALENCIA,SPAIN

[10] UNIV UTRECHT HOSP,UTRECHT,NETHERLANDS

来源：

NEW ENGLAND JOURNAL OF MEDICINE | 1995年 / 333卷 / 23期

关键词：

D O I：

10.1056/NEJM199512073332303

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Background. Reverse-transcriptase inhibitors have only moderate clinical efficacy against the human immunodeficiency virus type 1 (HIV-1). Ritonavir is an inhibitor of HIV-1 pretease with potent in vitro anti-HIV properties and good oral bioavailability. Methods. We evaluated the antiviral activity and safety of ritonavir in a double-blind, randomized, placebo-controlled phase 1 and 2 study of 84 HIV-positive patients with 50 or more CD4+ lymphocytes per cubic millimeter. The patients were randomly assigned to one of four regimens of ritonavir therapy, or to placebo for four weeks and then (by random assignment) to one of the ritonavir regimens. Results. During the first 4 weeks, increases in CD4+ lymphocyte counts and reductions in the log number of copies of HIV-1 RNA per milliliter of plasma were similar among the four dosage groups, but in the three lower-dosage groups there was a return to base-line levels by 16 weeks. After 32 weeks, in the seven patients in the highest-dosage group (600 mg of ritonavir every 12 hours), the median increase from base line in the CD4+ lymphocyte count was 230 cells per cubic millimeter, and the mean decrease in the plasma concentration of HIV-1 RNA (as measured by a branched-chain DNA assay) was 0.81 log (95 percent confidence interval, 0.40 to 1.22). In a subgroup of 17 patients in the two higher-dosage groups, RNA was also measured with an assay based on the polymerase chain reaction, and after eight weeks of treatment there was a mean maximal decrease in viral RNA of 1.94 log (95 percent confidence interval, 1.37 to 2.51). Adverse events included nausea, circumoral paresthesia, elevated hepatic aminotransferase levels, and elevated triglyceride levels. Ten withdrawals from the study were judged to be related to ritonavir treatment. Conclusions. In this short-term study, ritonavir was well tolerated and had potent activity against HIV-1, but its clinical benefits remain to be established.

引用

页码：1528 / 1533

页数：6

共 23 条

[1]

BILELLO JA, IN PRESS J CLIN INVE

[2] 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

[3] ZIDOVUDINE RESISTANCE AND HIV-1 DISEASE PROGRESSION DURING ANTIRETROVIRAL THERAPY [J].

DAQUILA, RT ;

JOHNSON, VA ;

WELLES, SL ;

JAPOUR, AJ ;

KURITZKES, DR ;

DEGRUTTOLA, V ;

REICHELDERFER, PS ;

COOMBS, RW ;

CRUMPACKER, CS ;

KAHN, JO ;

RICHMAN, DD .

ANNALS OF INTERNAL MEDICINE, 1995, 122 (06) :401-408

[4] THE HIV-1 PROTEASE AS A THERAPEUTIC TARGET FOR AIDS [J].

DEBOUCK, C .

AIDS RESEARCH AND HUMAN RETROVIRUSES, 1992, 8 (02) :153-164

[5] HIGH-DOSE NEVIRAPINE - SAFETY, PHARMACOKINETICS, AND ANTIVIRAL EFFECT IN PATIENTS WITH HUMAN-IMMUNODEFICIENCY-VIRUS INFECTION [J].

HAVLIR, D ;

CHEESEMAN, SH ;

MCLAUGHLIN, M ;

MURPHY, R ;

ERICE, A ;

SPECTOR, SA ;

GREENOUGH, TC ;

SULLIVAN, JL ;

HALL, D ;

MYERS, M ;

LAMSON, M ;

RICHMAN, DD .

JOURNAL OF INFECTIOUS DISEASES, 1995, 171 (03) :537-545

[6] 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

[7] DISTINCT CHANGES IN HIV TYPE-1 RNA VERSUS P24 ANTIGEN LEVELS IN SERUM DURING SHORT-TERM ZIDOVUDINE THERAPY IN ASYMPTOMATIC INDIVIDUALS WITH AND WITHOUT PROGRESSION TO AIDS [J].

JURRIAANS, S ;

WEVERLING, GJ ;

GOUDSMIT, J ;

BOOGAARD, J ;

BROK, M ;

VANSTRIJP, D ;

LANGE, J ;

KOOT, M ;

VANGEMEN, B .

AIDS RESEARCH AND HUMAN RETROVIRUSES, 1995, 11 (04) :473-479

[8]

KATLAMA C, 1995, 2 NAT C HUM RETR REL, P29

[9] QUANTITATION OF HUMAN-IMMUNODEFICIENCY-VIRUS BY CULTURE AND POLYMERASE CHAIN-REACTION IN RESPONSE TO DIDANOSINE AFTER LONG-TERM THERAPY WITH ZIDOVUDINE [J].

KATZENSTEIN, DA ;

WINTERS, M ;

BUBP, J ;

ISRAELSKI, D ;

WINGER, E ;

MERIGAN, TC .

JOURNAL OF INFECTIOUS DISEASES, 1994, 169 (02) :416-419

[10] ABT-538 IS A POTENT INHIBITOR OF HUMAN-IMMUNODEFICIENCY-VIRUS PROTEASE AND HAS HIGH ORAL BIOAVAILABILITY IN HUMANS [J].

KEMPF, DJ ;

MARSH, KC ;

DENISSEN, JF ;

MCDONALD, E ;

VASAVANONDA, S ;

FLENTGE, CA ;

GREEN, BE ;

FINO, L ;

PARK, CH ;

KONG, XP ;

WIDEBURG, NE ;

SALDIVAR, A ;

RUIZ, L ;

KATI, WM ;

SHAM, HL ;

ROBINS, T ;

STEWART, KD ;

HSU, A ;

PLATTNER, JJ ;

LEONARD, JM ;

NORBECK, DW .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (07) :2484-2488

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