Evidence for prevention of death and myocardial infarction with platelet membrane glycoprotein IIb/IIIa receptor blockade by abciximab (c7E3 Fab) among patients with unstable angina undergoing percutaneous coronary revascularization

被引：171

作者：

Lincoff, AM

Califf, RM

Anderson, KM

Weisman, HF

Aguirre, FV

Kleiman, NS

Harrington, RA

Topol, EJ

机构：

[1] DUKE UNIV, MED CTR, DURHAM, NC USA

[2] CENTOCOR INC, MALVERN, PA 19355 USA

[3] ST LOUIS UNIV, ST LOUIS, MO 63103 USA

[4] BAYLOR COLL MED, HOUSTON, TX 77030 USA

[5] METHODIST HOSP, HOUSTON, TX 77030 USA

来源：

JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY | 1997年 / 30卷 / 01期

关键词：

D O I：

10.1016/S0735-1097(97)00110-1

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Objectives. We sought to evaluate whether patients with unstable angina undergoing coronary intervention derive particular clinical benefit from potent platelet inhibition. Background. Plaque rupture and platelet aggregation are pathogenetic professes common to unstable angina and ischemic complications of percutaneous coronary intervention. Methods. Of the 2,099 patients undergoing a coronary intervention in the Evaluation of 7E3 in Preventing Ischemic Complications (EPIC) trial, 489 were enrolled with the diagnosis of unstable angina and randomized to receive placebo, an abciximab (c7E3) bolus immediately before the intervention or an abciximab bolus followed by a 12 h infusion. The primary endpoint aas a composite of death, myocardial infarction (MI) or urgent repeat revascularization within 30 days of randomization. The occurrence of death, MI or any revascularization within 6 months was also assessed. Results. Compared with placebo, the bolus and infusion of abciximab resulted in a 62% reduction in the rate of the primary end point (12.8% vs. 4.8%, p = 0.012) among patients with unstable angina, due primarily to a reduction in the incidences of death (3.2% vs. 1.2%, p = 0.164) and MI (9% vs. 1.8%, p = 0.004). By 6 months, cumulative death and MI were further reduced by abciximab (6.6% vs. 1.8%, p = 0.018 and 11.1% vs. 2.4%, p = 0.002, respectively). The magnitude of the risk reduction with abciximab was greater among the patients with unstable angina than among other patients in the EPIC trial without unstable angina for the end points of death (interaction: p = 0.008 at 30 days, p = 0.002 at 6 months) and MI (interaction: p = 0.004 at 30 days, p = 0.003 at 6 months). Conclusions. The syndrome of unstable angina identifies patients who will experience particularly marked reductions in the risk of death and MI with abciximab during coronary intervention. (C) 1997 by the American College of Cardiology.

引用

页码：149 / 156

页数：8

共 34 条

[1] BLEEDING COMPLICATIONS WITH THE CHIMERIC ANTIBODY TO PLATELET GLYCOPROTEIN IIB/IIIA INTEGRIN IN PATIENTS UNDERGOING PERCUTANEOUS CORONARY INTERVENTION [J].

AGUIRRE, FV ;

TOPOL, EJ ;

FERGUSON, JJ ;

ANDERSON, K ;

BLANKENSHIP, JC ;

HEUSER, RR ;

SIGMON, K ;

TAYLOR, M ;

GOTTLIEB, R ;

HANOVICH, G ;

ROSENBERG, M ;

DONOHUE, TJ ;

WEISMAN, HF ;

CALIFF, RM .

CIRCULATION, 1995, 91 (12) :2882-2890

[2] COLLABORATIVE OVERVIEW OF RANDOMIZED TRIALS OF ANTIPLATELET THERAPY .1. PREVENTION OF DEATH, MYOCARDIAL-INFARCTION, AND STROKE BY PROLONGED ANTIPLATELET THERAPY IN VARIOUS CATEGORIES OF PATIENTS [J].

ALTMAN, R ;

CARRERAS, L ;

DIAZ, R ;

FIGUEROA, E ;

PAOLASSO, E ;

PARODI, JC ;

CADE, JF ;

DONNAN, G ;

EADIE, MJ ;

GAVAGHAN, TP ;

OSULLIVAN, EF ;

PARKIN, D ;

RENNY, JTG ;

SILAGY, C ;

VINAZZER, H ;

ZEKERT, F ;

ADRIAENSEN, H ;

BERTRANDHARDY, JM ;

BRAN, M ;

DAVID, JL ;

DRICOT, J ;

LAVENNEPARDONGE, E ;

LIMET, R ;

LOWENTHAL, A ;

MORIAU, M ;

SCHAPIRA, S ;

SMETS, P ;

SYMOENS, J ;

VERHAEGHE, R ;

VERSTRAETE, M ;

ATALLAH, A ;

BARNETT, H ;

BATISTA, R ;

BLAKELY, J ;

CAIRNS, JA ;

COTE, R ;

CROUCH, J ;

EVANS, G ;

FINDLAY, JM ;

GENT, M ;

LANGLOIS, Y ;

LECLERC, J ;

NORRIS, J ;

PINEO, GF ;

POWERS, PJ ;

ROBERTS, R ;

SCHWARTZ, L ;

SICURELLA, J ;

TAYLOR, W ;

THEROUX, P .

BMJ-BRITISH MEDICAL JOURNAL, 1994, 308 (6921) :81-100

[3] ADJUNCTIVE THROMBOLYTIC THERAPY DURING ANGIOPLASTY FOR ISCHEMIC REST ANGINA - RESULTS OF THE TAUSA TRIAL [J].

AMBROSE, JA ;

ALMEIDA, OD ;

SHARMA, SK ;

TORRE, SR ;

MARMUR, JD ;

ISRAEL, DH ;

RATNER, DE ;

WEISS, MB ;

HJEMDAHLMONSEN, CE ;

MYLER, RK ;

MOSES, J ;

UNTERECKER, WJ ;

GRUNWALD, AM ;

GARRETT, JS ;

COWLEY, MJ ;

ANWAR, A ;

SOBOLSKI, J .

CIRCULATION, 1994, 90 (01) :69-77

[4]

[Anonymous], 1994, Circulation, V89, P1545

[5] OUTCOME OF PERCUTANEOUS TRANSLUMINAL CORONARY ANGIOPLASTY IN SUBSETS OF UNSTABLE ANGINA-PECTORIS - A REPORT OF THE 1985-1986 NATIONAL-HEART,-LUNG,-AND-BLOOD-INSTITUTE PERCUTANEOUS TRANSLUMINAL CORONARY ANGIOPLASTY REGISTRY [J].

BENTIVOGLIO, LG ;

DETRE, K ;

YEH, WL ;

WILLIAMS, DO ;

KELSEY, SF ;

FAXON, DP .

JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY, 1994, 24 (05) :1195-1206

[6] TREATMENT WITH BIVALIRUDIN (HIRULOG) AS COMPARED WITH HEPARIN DURING CORONARY ANGIOPLASTY FOR UNSTABLE OR POSTINFARCTION ANGINA [J].

BITTL, JA ;

STRONY, J ;

BRINKER, JA ;

AHMED, WH ;

MECKEL, CR ;

CHAITMAN, BR ;

MARAGANORE, J ;

DEUTSCH, E ;

ADELMAN, B .

NEW ENGLAND JOURNAL OF MEDICINE, 1995, 333 (12) :764-769

[7] DIAGNOSING AND MANAGING UNSTABLE ANGINA [J].

BRAUNWALD, E ;

JONES, RH ;

MARK, DB ;

BROWN, J ;

BROWN, L ;

CHEITLIN, MD ;

CONCANNON, CA ;

COWAN, M ;

EDWARDS, C ;

FUSTER, V ;

GOLDMAN, L ;

GREEN, LA ;

GRINES, CL ;

LYTLE, BW ;

MCCAULEY, KM ;

MUSHLIN, AI ;

ROSE, GC ;

SMITH, EE ;

SWAIN, JA ;

TOPOL, EJ ;

WILLERSON, JT .

CIRCULATION, 1994, 90 (01) :613-622

[8] ASPIRIN, SULFINPYRAZONE, OR BOTH IN UNSTABLE ANGINA - RESULTS OF A CANADIAN MULTICENTER TRIAL [J].

CAIRNS, JA ;

GENT, M ;

SINGER, J ;

FINNIE, KJ ;

FROGGATT, GM ;

HOLDER, DA ;

JABLONSKY, G ;

KOSTUK, WJ ;

MELENDEZ, LJ ;

MYERS, MG ;

SACKETT, DL ;

SEALEY, BJ ;

TANSER, PH .

NEW ENGLAND JOURNAL OF MEDICINE, 1985, 313 (22) :1369-1375

[9] 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

[10]

COLLER BS, 1985, BLOOD, V66, P1456

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