Clinical pharmacology of higher dose eptifibatide in percutaneous coronary intervention (the PRIDE study)

被引：60

作者：

Tcheng, JE

Talley, JD

O'Shea, JC

Gilchrist, IC

Kleiman, NS

Grines, CL

Davidson, CJ

Lincoff, AM

Califf, RM

Jennings, LK

Kitt, MM

Lorenz, TJ

机构：

[1] Duke Clin Res Inst, Durham, NC USA

[2] Univ Arkansas Med Sci, Little Rock, AR 72205 USA

[3] Penn State Univ, Hershey, PA USA

[4] Methodist Hosp, Houston, TX 77030 USA

[5] William Beaumont Hosp, Royal Oak, MI 48072 USA

[6] Northwestern Univ, Sch Med, Chicago, IL USA

[7] Cleveland Clin, Cleveland, OH 44106 USA

[8] Univ Tennessee, Memphis, TN USA

[9] COR Therapeut, San Francisco, CA USA

来源：

AMERICAN JOURNAL OF CARDIOLOGY | 2001年 / 88卷 / 10期

关键词：

D O I：

10.1016/S0002-9149(01)02041-0

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

This study describes the dose-exploration phase of the PRIDE trial, an investigation of the clinical pharmacology of higher dose eptifibatide in patients who underwent elective percutaneous coronary intervention (PCI). Outcomes of treatment with the platelet glycoprotein IIb/IIIa inhibitors were dependent upon proper dosing selection. In this multicenter, placebo-controlled clinical study, 127 patients were randomized 1:1:2:2 into 1 of the following treatment groups: placebo; eptifibatide as a 135 mug/kg bolus followed by a 0.75 mug/kg/min infusion; eptifibatide as a 180 mug/kg bolus with a 2.0 mug/kg/min infusion; or eptifibatide as a 250 mug/kg bolus with a 3.0 mug/kg/min infusion. Light transmission aggregometry was used to determine platelet aggregation in response to 20 muM adenosine diphosphate, and platelet receptor occupancy was also determined. Eptifibatide exhibited linear pharmacokinetics over the dose range studied. Inhibition of platelet aggregation was greater in samples collected in sodium citrate compared with those collected in D-phenylalanyl-L-prolyl-L-arginine chloromethyl ketone. The 180/2.0 dosing regimen achieved 90% inhibition of platelet aggregation immediately (5 minutes) and at steady state (8 to 24 hours). At 1hour, mean inhibition of platelet aggregation was 80%. Eptifibatide exhibited dose-dependent pharmacodynamics that were dependent upon choice of anticoagulant. A 180 mug/kg bolus followed by a 2.0 mug/kg/min infusion at steady state achieved >80% inhibition of platelet aggregation. With the single-bolus regimen, however, there was an early loss of the inhibition of platelet aggregation before steady state was reached. Additional dose-exploration studies may further optimize eptifibatide dosing. (C) by Excerpta Medica, Inc.

引用

页码：1097 / 1102

页数：6

共 24 条

[1]

BORN GVR, 1963, J PHYSIOL-LONDON, V168, P178, DOI 10.1113/jphysiol.1963.sp007185

[2] USE OF A MONOCLONAL-ANTIBODY DIRECTED AGAINST THE PLATELET GLYCOPROTEIN IIB/IIIA RECEPTOR IN HIGH-RISK CORONARY ANGIOPLASTY [J].

CALIFF, RM ;

SHADOFF, N ;

VALETT, N ;

BATES, E ;

GALEANA, A ;

KNOPF, W ;

SHAFTEL, J ;

BENDER, MJ ;

AVERSANO, T ;

RAQUENO, J ;

GURBEL, P ;

COWFER, J ;

COHEN, M ;

CROSS, P ;

BITTL, J ;

EDDINGS, K ;

TAYLOR, M ;

DEROSA, K ;

HATTEL, L ;

COOPER, L ;

ESHELMAN, B ;

FINTEL, D ;

NIEMYSKI, P ;

KLEIN, L ;

KENNEDY, H ;

THORNTON, T ;

KEREIAKES, D ;

MARTIN, L ;

ANDERSON, L ;

HIGBY, N ;

ELLIS, S ;

BREZINA, K ;

GEORGE, B ;

CHAPEKIS, A ;

SMITH, D ;

ANWAR, A ;

GERBER, TL ;

PRITCHARD, GL ;

MYLER, R ;

SHAW, R ;

MURPHY, M ;

WARD, K ;

MADIGAN, NP ;

BLANKENSHIP, J ;

HALBERT, M ;

FLANAGAN, C ;

TANNENBAUM, M ;

POLICH, M ;

STEVENSON, C ;

TCHENG, J .

NEW ENGLAND JOURNAL OF MEDICINE, 1994, 330 (14) :956-961

[3]

COLLEN D, 1994, THROMB HAEMOSTASIS, V71, P95

[4] ABOLITION OF INVIVO PLATELET THROMBUS FORMATION IN PRIMATES WITH MONOCLONAL-ANTIBODIES TO THE PLATELET GPIIB-IIIA RECEPTOR - CORRELATION WITH BLEEDING-TIME, PLATELET-AGGREGATION, AND BLOCKADE OF GPIIB-IIIA RECEPTORS [J].

COLLER, BS ;

FOLTS, JD ;

SMITH, SR ;

SCUDDER, LE ;

JORDAN, R .

CIRCULATION, 1989, 80 (06) :1766-1774

[5] LIGAND AND CATION-BINDING ARE DUAL FUNCTIONS OF A DISCRETE SEGMENT OF THE INTEGRIN BETA(3) SUBUNIT - CATION DISPLACEMENT IS INVOLVED IN LIGAND-BINDING [J].

DSOUZA, SE ;

HAAS, TA ;

PIOTROWICZ, RS ;

BYERSWARD, V ;

MCGRATH, DE ;

SOULE, HR ;

CIERNIEWSKI, C ;

PLOW, EF ;

SMITH, JW .

CELL, 1994, 79 (04) :659-667

[6] RAPID AND SUSTAINED CORONARY-ARTERY RECANALIZATION WITH COMBINED BOLUS INJECTION OF RECOMBINANT TISSUE-TYPE PLASMINOGEN-ACTIVATOR AND MONOCLONAL ANTIPLATELET GPIIB/IIIA ANTIBODY IN A CANINE PREPARATION [J].

GOLD, HK ;

COLLER, BS ;

YASUDA, T ;

SAITO, T ;

FALLON, JT ;

GUERRERO, JL ;

LEINBACH, RC ;

ZISKIND, AA ;

COLLEN, D .

CIRCULATION, 1988, 77 (03) :670-677

[7]

Hanrath P, 1997, CIRCULATION, V96, P1445

[8] IMMEDIATE AND REVERSIBLE PLATELET INHIBITION AFTER INTRAVENOUS ADMINISTRATION OF A PEPTIDE GLYCOPROTEIN IIB/IIIA INHIBITOR DURING PERCUTANEOUS CORONARY INTERVENTION [J].

HARRINGTON, RA ;

KLEIMAN, NS ;

KOTTKEMARCHANT, K ;

LINCOFF, AM ;

TCHENG, JE ;

SIGMON, KN ;

JOSEPH, D ;

RIOS, G ;

TRAINOR, K ;

ROSE, D ;

GREENBERG, CS ;

KITT, MM ;

TOPOL, EJ ;

CALIFF, RM .

AMERICAN JOURNAL OF CARDIOLOGY, 1995, 76 (17) :1222-1227

[9]

JOHNSTON GI, 1988, THROMB HAEMOSTASIS, V59, P54

[10]

KOUNS WC, 1990, J BIOL CHEM, V265, P20594

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