RISKS OF GASTROINTESTINAL-BLEEDING DURING SECONDARY PREVENTION OF VASCULAR EVENTS WITH ASPIRIN - ANALYSIS OF GASTROINTESTINAL-BLEEDING DURING THE UK-TIA TRIAL

被引：114

作者：

SLATTERY, J

WARLOW, CP

SHORROCK, CJ

LANGMAN, MJS

机构：

[1] UNIV BIRMINGHAM, QUEEN ELIZABETH HOSP, DEPT MED, BIRMINGHAM B15 2TH, W MIDLANDS, ENGLAND

[2] WESTERN GEN HOSP, DEPT CLIN NEUROSCI, EDINBURGH, MIDLOTHIAN, SCOTLAND

来源：

GUT | 1995年 / 37卷 / 04期

关键词：

ASPIRIN; HEMORRHAGE; GASTROINTESTINAL;

D O I：

10.1136/gut.37.4.509

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

From 1979 to 1985 2435 patients having had transient ischaemic attacks (TIAs) or minor ischaemic strokes, were enrolled in the UK TIA trial and were randomised to receive either aspirin 300 mg, daily or aspirin 1200 mg or placebo. Analysis of reported upper gastrointestinal bleeding events (defined as haematemesis or melaena, or both) showed a risk of bleeding in a dose dependent manner, odds ratios (95% CI) for 300 mg of aspirin=3.3 (1.2 to 9.0) and for 1200 mg=6.4 (2.5 to 16.5) and, as would be expected, an increased risk of hospitalisation because of bleeding also in a dose dependent manner, odds ratio=3.6 (0.7 to 17.2) for 300 mg and 8.7 (2.0 to 37.6) for 1200 mg. Further analysis suggested greater risks of bleeding from duodenal ulcers than gastric ulcers and that bleeding is more likely early in the course of treatment with aspirin used as secondary prevention. There was also an increased risk of lower gastrointestinal bleeding, defined as fresh blood per rectum for both doses of aspirin, odds ratio 1.8 (0.5 to 6.1) for 300 mg of aspirin, and 1.5 (0.4 to 5.3) for 1200 mg of aspirin.

引用

页码：509 / 511

页数：3

共 14 条

[1] 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

[2]

[Anonymous], 1988, LANCET, V2, P349

[3]

[Anonymous], 1988, Br Med J (Clin Res Ed), V296, P316

[4]

GARDNER MJ, 1989, STATISTICS CONFIDENC

[5] GASTRIC ADAPTATION - STUDIES IN HUMANS DURING CONTINUOUS ASPIRIN ADMINISTRATION [J].

GRAHAM, DY ;

SMITH, JL ;

SPJUT, HJ ;

TORRES, E .

GASTROENTEROLOGY, 1988, 95 (02) :327-333

[6] NONSTEROIDAL ANTIINFLAMMATORY DRUG-USE AND INCREASED RISK FOR PEPTIC-ULCER DISEASE IN ELDERLY PERSONS [J].

GRIFFIN, MR ;

PIPER, JM ;

DAUGHERTY, JR ;

SNOWDEN, M ;

RAY, WA .

ANNALS OF INTERNAL MEDICINE, 1991, 114 (04) :257-263

[7] FINAL REPORT ON THE ASPIRIN COMPONENT OF THE ONGOING PHYSICIANS HEALTH STUDY [J].

HENNEKENS, CH .

NEW ENGLAND JOURNAL OF MEDICINE, 1989, 321 (03) :129-135

[8] EPIDEMIOLOGIC EVIDENCE ON THE ASSOCIATION BETWEEN PEPTIC-ULCERATION AND ANTIINFLAMMATORY DRUG-USE [J].

LANGMAN, MJS .

GASTROENTEROLOGY, 1989, 96 (02) :640-646

[9] USE OF ANTI-INFLAMMATORY DRUGS BY PATIENTS ADMITTED WITH SMALL OR LARGE BOWEL PERFORATIONS AND HEMORRHAGE [J].

LANGMAN, MJS ;

MORGAN, L ;

WORRALL, A .

BRITISH MEDICAL JOURNAL, 1985, 290 (6465) :347-349

[10] RISKS OF BLEEDING PEPTIC-ULCER ASSOCIATED WITH INDIVIDUAL NONSTEROIDAL ANTIINFLAMMATORY DRUGS [J].

LANGMAN, MJS ;

WEIL, J ;

WAINWRIGHT, P ;

LAWSON, DH ;

RAWLINS, MD ;

LOGAN, RFA ;

MURPHY, M ;

VESSEY, MP ;

COLINJONES, DG .

LANCET, 1994, 343 (8905) :1075-1078

← 1 2 →